Nitsbin I Medicine 2nd Edition Final Revised 1

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ptilina

Copyright © 2016/2023
All rights reserved

Copyright © 2016/2023

All rights reserved


Preface i

Commemoration
This book is in memory of Dr. Habtamu Animaw,
who lost his life suddenly, due to unknown cause,
two months before his graduation, in paqume 03,
2012 E.C, while working his internship ward
activity, at University of Gondar Hospital.
May his soul Rest in peace.

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Nitsbin (ንጽቢን) Bedside oriented Internal medicine 2nd edition
Preface ii

“Your single comment is constructive for the next revised edition”

Comments here

❖ Email
[email protected]
❖ Telegram
 https://t.me/Nitsbinteam
Follow the channel for Updates
 https://t.me/Nitsbin21orit

2nd edition

Nitsibin(ንጽቢን)

Internal medicine

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Nitsbin (ንጽቢን) Bedside oriented Internal medicine 2nd edition
Preface iii

Preface
Nitsbin means ‘‘Book of art’’ in Geez language (ንጽቢን በልሳነ ግእዝ ‘‘የጥበብ መጽሐፍ’’ ማለት ነው
። ሐኪም ማለትም ሐከመ = ጥበበኛ ሆነ ፣ ብልሃተኛ ሆነ ከሚለው የግእዝ ግስ ተገኝቷል ። ሐኪም ማለት
ጥበበኛ ከሆነ፤ ሕክምና ማለት ደግሞ ጥበብ ይሆናልና ይህን ቃል ወደድን). We also prefer this name
because “Medicine is not only a Science; it is also an art” as said by Paracelsus. So,
Nitsbin means ‘‘book of medicine’’ indirectly.

The book is made on common Medical cases & approaches by Ethiopian Junior medical
doctors (GP) to be used as a quick reference & guide. The aim of Nitsbin is to enable &
equip medical students with the basic & necessary medical knowledge, skills & approaches
to patients in a very short period of time. We hope that, it will be important also for junior
medical and health science practitioners.

Nitsbin is a modified form of my previous bedside note ‘‘Internal medicine long and short
case notes by Mulualem.G (ኦሪት)’’ which was prepared in 2010 E.C during my 4th year (C-I)
attachment. I was considering only for myself and it was in hand written form. But I found
that most of students need a short-revised note for Clinical case approach and it was
necessary to revise the hand written note in to short and precise book with the intension of
collecting & comprising common medical cases in one place for easy access for
undergraduates and junior medical and health science practitioners.
We recommend you to read Standard books first and use Nitsbin as revision. Otherwise
depending only on Nitsbin is strongly forbidden.

Nitsbin has two major parts; long cases (containing 16 chapters including case report
sample) & short cases (containing 27 chapters).
Long cases contain important information on how to approach patients. Like;
✓ Some basic Information for taking history (clinical features, cause and risk factors,
complications, DDx…)
✓ Pertinent physical examination findings
✓ Sample histories for each case
✓ Investigations to be done & what is expected from each investigation considering
availability in Ethiopia and cost effectiveness.
✓ Discussion about the case & management
✓ Case reporting format for bedside, round, exam and case discussion
Short cases mainly contain
✓ Exam oriented physical examination techniques and possible findings
✓ DDX, IX and management principles of common physical examination findings
✓ Common medical procedures with indication, contraindication, complication of a
procedure, principle of management and result analysis with YouTube video link for
each procedure.
✓ Common Emergency and OPD cases
✓ CXR Interpretation
✓ Basics of ECG and ECG interpretation
✓ Basics about rational use of antibiotics
✓ Symptoms and signs in Amharic (የበሽታ ምልክቶች አማርኛ ትርጉም)
✓ Anatomical body parts in Amharic (የሰውነት አካል ክፍሎች አማርኛ ትርጉም)
✓ Common Laboratory Investigations with practical points and procedures (plus you tube
video link)
✓ Reference Intervals for Laboratory Tests

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Nitsbin (ንጽቢን) Bedside oriented Internal medicine 2nd edition
Acknowledgment iv

Acknowledgment

I thank God first and most for everything that had been and that ever will be, it
is all by the will of God.

I would like to acknowledge Dr. Asmare Walle and Dr. Robel Dibaba (Co-Author’s)
for their contribution in the preparation of Nitsbin Bedside oriented Internal medicine
1st edition. If it was not for you, I know that book wouldn’t never been real. Lastly
with effortful contribution of co-authors, we prepared Nitsbin as a ‘’Bedside oriented
book’’ depending on our clinical year attachment experiences.

The development and revision of Nitsbin 2nd edition for Medical and health
science students, junior practioners in Ethiopia is based on Harrison 21st edition,
UpToDate 2018, and National Guidelines on Clinical and Programmatic Management
focusing on detail management based on users’ comment.

I would also like to acknowledge the cover page designer Mr. Tadele
Tesfaye (Phone number: +251 91 881 2871. Email: [email protected].
Telegram: https://t.me/Tadele_tesfaye )

Lastly, I would also like to recognize the contributions of the following experts for
their detailed review both during development and materializing revised version.

NAME CONTRIBUTIONS AREA OF SPECIALTY AND


ORGANIZATION
Dr. Meaza Seyoum (MD+) Long Case Internist, Addis Alem
o Chapter 6; Stroke (የጭንቅላት ደም ስርበሽታ፣ እስትሮክ) Primary Hospital
o Chapter 7; Paraplegia (ከወገብ በታች ሽባነት)
o Chapter 8; Meningitis (ማጅራት ገትር)
Short cases
o Chapter 1, 1.4 Nervous system examination
o Chapter 2, 2.1 LP (Lumbar puncture)
o Chapter 7; Nervous System Related Disorders and
Infections
Dr. Elisabeth Awoke (MD+, Long Case Consultant Internist,
Assistant professor of Internal o Chapter 11; AKI/Acute kidney injury/and CKD/ Bahirdar University, TGSH
medicine) Chronic kidney disease (የኩላሊት በሽታ)
o Chapter 12; Glomerular disease (Nephrotic
syndrome/NS/ and Nephritic syndrome/Nts/)
Short cases
o Chapter 10; UTI (የሽንት ቧንቧ ልክፍት/ኢንፌክሽን/)
o Chapter 14; Fluid and electrolyte disturbance

Dr. Assefa Makuannent (MD+) Long Case Internist,


o Chapter 2; Cor pulmonale and Chronic lung Addis Alem Primary
disorders Hospital

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Nitsbin (ንጽቢን) Bedside oriented Internal medicine 2nd edition
Acknowledgment v

o Chapter 3; TB/Tuberculosis/ (የሳንባ ነቀርሳ ፣ ቲቢ)


o Chapter 4; Lung cancer (የሳንባ ካንሰር)
Short cases
o Chapter 1, 1.1 Respiratory System
o Chapter 2, 2.2 Pleural tap (thoracentesis)
o Chapter 8; Respiratory related disorders and
infections
o Chapter 21; Interpretation of Chest X – Ray (የደረት
ራጅ ማንበብ)
Dr. Segenet Bizuneh, (MD+, Long Case Consultant Internist,
Assistant professor of Internal o Chapter 1; Heart failure (ልብ ድካም) Approach and University of Gondar
medicine) management part
Dr. Kidan Mihret (MD+) Pediatrics DM and DKA Case management Pediatrician, Addis Alem
Primary Hospital
Dr. Melkam Desta (MD+) Pediatrics DM and DKA Case management Pediatrician, Addis Alem
Primary Hospital
For 3rd Edition Long Case
o Other Cardiac Disorders
Short cases
o Chapter 1, 1.2 Cardiovascular System examination
o Chapter 3; Shock
o Chapter 22; Basics of ECG and ECG interpretation
For 3rd edition Long Case
o Chapter 5; RVI (ኤች አይ ቪ ኤዲስ)
o Chapter 13; Leishmaniasis (ካላዛር/ጓቋ//ድባ/ እና
ቁንጭር)
Short cases
o Chapter 9; GI related disorders and infections
o Chapter 11; Acute febrile illness (AFI)
o Chapter16; STI (የአባላዘር በሽታ)
o Chapter 17; Sepsis
o Chapter 20; Miscellaneous
For 3rd edition Long Case
o Chapter 9; CLD/ Chronic liver disease/ (የጉበት በሽታ)
o Chapter 10; DM /Diabetes Mellitus/ (የስኳር በሽታ)
Short cases
o Chapter 1, 1.3 Abdominal examination
o Chapter 2, 2.3 Peritoneal tap (paracentesis)
o Chapter15; Dyslipidemia and metabolic syndrome
o Chapter18; Thyroid Hormone Disorders
For 3rd edition Short cases
o Chapter 12; MSS Related disorders and infections
o Chapter 19; Poisoning, Drug Overdose, and
Envenomation

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Nitsbin (ንጽቢን) Bedside oriented Internal medicine 2nd edition
Acknowledgment vi

For 3rd edition Long Case


o Chapter 14; Leukaemia (የደም ካንሰር)
o Chapter 15; Lymphomas (የደም ካንሰር)
Short cases
o Chapter 13; Hematologic Disorders

Dr. Mulualem Gashaw (GP)

Author

Type writing & internal page design

University of Gondar, 2016/2024

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Nitsbin (ንጽቢን) Bedside oriented Internal medicine 2nd edition
Contributors vii

Contributors

Author

Dr. Mulualem Gashaw/ኦሪት/, MD


General practitioner (GP)
Class of hakim 2020
University of Gondar, College of
Medicine and Health Science

Co-Author’s of 1st Edition

Dr. Robel Dibaba, MD


Dr. Asmare Walle, MD
General practitioner (GP)
General practitioner (GP)
Class of Hakim 2020
Class of Hakim 2019
University of Gondar,
Addis Ababa University
College of Medicine and
College of health sciences / TASH
Health science

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Nitsbin (ንጽቢን) Bedside oriented Internal medicine 2nd edition
Comments on 1st edition viii

Comments on 1st edition

➡️ Keep the good work up My brothers. I saw Nitsbin and it’s a good start. Keep
rolling forward

Dr. Mezigebu Diress


2nd year Internal medicine Resident (R2)
Bahirdar University, TGSH

➡️ I am glad to get you here. My appreciation goes regarding your writing in


Nitsbin. An excellent and examplary text in our Ethiopian medical students.

Fiseha Guadie
C-III (5th year) Medical Student
Debretabor university medical and Health science college
Owner of @nisirhikimna Telegram page

➡️ hello doctor! I am a C1 medical student at jimma universty medical center and I


want to say thank you a lot for your book Nitsbin. It’s really great work. Me and my
friends (I can say all clinical students) are enjoying it. So I want you to know that
it's loved and being used.

Desalegn Bile
C-I medical Student
Jimma University Medical College

➡️ Here is my COMMENT ON NTSBIN INTERNAL MEDICINE! First of all, I would


like thank u for your great effort on this edition starting from the Idea up to the end.
And you well don it indeed. and I'm very happy and surprised by this book. You
tried all your best and you invested your time and capacity. Because this book
highly attracted me and my friends and I think it may also attract the others. the
reference books you have used is another quality of this book. Otherwise I HAVE
NO WORD AND IDEA ON THE NEGATIVE COMMENT FOR NOW.

C-II medical Student


Debre birhan University Medical and Health science College

➡️ hi Dr. mulie. I am from HU medical school. I personally cannot thank you enough
for the book u prepared (Nitsbin IM). It is helping a lot of students here.

Abdulmalik Argani Hussein


C - II Medical student
Harommaya University medical and Health science college

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Nitsbin (ንጽቢን) Bedside oriented Internal medicine 2nd edition
Comments on 1st edition ix

➡️ My name is Hanchalu Alemayehu, C I medical student at yekatit 12 Hospital


medical college. I got your telegram from Nitsbin text book. Really really I appreciate
you and thanks God to have people like you. Stay blessed.

Hanchalu Alemayehu,
C I medical student
yekatit 12 Hospital medical college.

➡️Greetings. My name is Bruk Kifle, and I'm currently a medical student finishing up
the last of my major clinical rotations. Although I use standard text to read and
study from, just before the clinical session starts, I review the cases from the typical
med student short note (medstar, fanos,...) What I found from this note just left me
amazed. The attention to detail and the detailed explanation (need the want arise)
was nice. What got me most was Part II of the text, chapter 8. Symptoms and
signs in amharic. This is what I want most, wow to translate some key things to our
own setup. I aspire and hope to see you (those who participated) come up with
something even better.

Biruk Kifle
C-II Medical Student
ECHLI (Ethiopian catholic higher learning institute)

➡️ Dr. Did you know that here in our medical school all medicine, public health, anesthesia
and other health students use Nitsbin book for C1 and C2 attachments. It is our favorite.
Khelif Abddushkur Mohammed
4th Year HO
Wolkitie University

➡️ ባንታለም እባላለሁ ጤና መኮንን (HO) ነው የተማርኩት እና ያንተን short note በደንብ


አድርገን ነበር ስንጠቀመው የነበር። የሚገርምህ በግቢው ከ Medicine እስከ other health ነበር
የምንጠቀመው። አንድ ቀን ሥላንተ ሲወራ እኔም ነበርኩና በቃ የሌለ ደሥ አለኝ። እውነት
እልሃለሁ ሁሉም አንድ ነገር Comment ማድረግ ይፈልግ ነበር ። እሱም ትንሽ የእጅ ጽሑፍ
ሥለሆነ አንዳንድ ቦታ የማይታይ ነበር እና ምናለ ይህን በ PDF አድርጎ እንደገና ቢአዘጋጀው እኮ
ይበልጥ ያምር ነበር የሚል ነበር። እናም አሁን እንደዚህ ተዘጋጅቶ መቅረቡ አጀብ ያሥብላል ።
በጣም ነው የማከብርህ ዶክተር በርታ።
Bantalem Azmeraw
Health officer
UOG

➡️ ሰላም እንዴት ናቹህ ። Nitsbin(ንጽቢን) በማለት እየሰራቹህት ላለው ሥራ ልትመሠገኑ


ይገባል። ብዙ ልፋት ነው ያቀለላቹህልን ። በርቱ በዚሁ ቀጥሉ። Nitsbin Hand out ከሁሉም በላይ
በጣም ነው የረዳኝ። እስከመቼውም ከእኔጋ የሚቆይ ይሆናል። በጣም አመሠግናለሁ በርቱ

Dawit Mekonnen
C-II (5th year) Medical Student
Wachemo University

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Nitsbin (ንጽቢን) Bedside oriented Internal medicine 2nd edition
Comments on 1st edition x

➡️ ሰላም ዶ/ር በጣም አድናቂህ ነኝ ፡፡ መጽሐፉን እየተጠቀምኩበት ነው ፤ በጣም ቆንጆ ነው ፤ ደስ


ይላል በጣም ፤ እናመሰግናለን ፤ በርታ እግዚአብሔር ያበርታክ

Tsegaye abebe
C-II (5th year) Medical Student
Dilla University

➡️ Hey DOCTOR, I am a public health officer student at UoG. Your book ''Nitsbin'‘
helped me a lot in my internal medicine attachment. I have no words to admire you
and your book. I want to say thank you for your book. May GOD bless you and your
relatives.

Bekalu Temesgen
PHO student
UOG

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Nitsbin (ንጽቢን) Bedside oriented Internal medicine 2nd edition
What is new in 2nd edition xi

What is new in 2nd edition

Approach part of some long cases incorporated for best patient approach of
students and physicians with detailed modification of discussion part such as;
o Leukemia
o Lymphoma
o Glomerular disease
Majority if cases updated with recent guidelines and Harrison 21st edition. For
example
o ARF and RHD updated from National NCD guideline 2021
o HTN and DM Updated from National NCD guideline 2021 and CRITICAL
CARE POCKET GUIDE, FMOH, Ethiopia, 2022
o DM Updated from National Training on DM for Health Care Workers,
Participant’s Manual (Draft Revised Version) Addis Ababa January 2021
o HTN updated from NATIONAL TRAINING ON HYPERTENSIONFOR HEALTH
CARE WORKERS IN ETHIOPIA: Participant’s Manual October, 2021, Addis
Ababa, Ethiopia
o MANAGEMENT OF HYPERTENSION IN SPECIAL CLINICAL CONDITIONS
(comorbidities) added in 2nd edition
o ACS Updated from CRITICAL CARE POCKET GUIDE, FMOH, Ethiopia,
2022
o Peak Expiratory Flow (PEF) added in Diagnosis of asthma
o ILD Completely Modified from Harrison 21st edition and UpToDate 2018
o Cholera Updated from National Guideline for CHOLERA SURVEILLANCE
AND OUTBREAK RESPONSE 3rd edition, 2022
o Malaria Updated from Malaria Case Management Training Manual for Health
Professionals in Ethiopia, January 2022, FMOH
o First line TB treatment adult and pediatric dosing chart using body weight
bands (Table) Added in TB management
WHO RISK-BASED CVD MANAGEMENT PROTOCOL IN ETHIOPIA, added from
National NCD guideline 2021
Asthma exacerbations classified from Mild, moderate and severe to mild, moderate,
severe and life threatening
Chapter 2 (Chronic Lung disorders and Cor pulmonale rearranged for coherence
and better understanding for readers)
Majority of cases are evaluated by senior experts.
Long cases Updated to 16 chapters
Short cases rearranged to 27 chapters
New cases in 2nd edition
o DM and Hypertension Follow Up Form
o Pediatrics DM and DKA Case Management
o IBD
o Thrombocytopenia in hospitalized patients

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Nitsbin (ንጽቢን) Bedside oriented Internal medicine 2nd edition
What is new in 2nd edition xii

o ITP
o Dyslipidemia and metabolic syndrome
o Noradrenaline/Norepinephrine/ drip preparation
o Bell’s Palsy
o Parkinson’s Disease
o Adrenal Crisis
o Constipation
o Lupus nephritis
o Management of metalophosphate poisoning
o Fluid Management of DKA in CHF, CKD, HTN and CLD patients
o Shock and Pulmonary edema Management when they happen together
o Refractory Shock, Dual vasopressors in refractory shock
o COVID -19
o Anthrax (ቁርባ)
o Rabies (የእብድ ውሻ በሽታ)
o Filariasis, Lymphatic (Elephantiasis)/ዝሆኔ/

Table; Updated Examples in Nitsbin 2nd edition

S.N Case (Chapter) Nitsbin 1st edition Nitsbin 2nd edition


1. ATP Management BPG given 600,000 IU, IM stat BPG given 600,000 IU, IM stat
FOR those <27KG FOR those <30KG
Amoxicillin, 500mg, PO, BID For 10 Amoxicillin, 500mg, PO, TID for
days 10 days
2. HTN Urgency Nifedipine (Immediate release, short Nifedipine (Immediate release, short
management acting), 20mg, Sublingual, q 20 to acting), 20mg, PO, q 20 to 30min,
30min, until target achieved until target achieved

In most setups of Ethiopia, Nifedipine; The trend of using Sublingual


Immediate release, 20mg, Sublingual, is nifedipine for HTN Urgency in most
the preferred management principle for setups of Ethiopia should be
hypertensive urgency, may repeat with avoided
a 20 mg dose in 20 minutes if needed
3. RVI Screening PICT PITC (Provider initiated testing
and counseling)
Stat pack → Abon → SD bioline
One step → 1st response →
Unigold
4. Amoebae Metronidazole, 500-750mg P.O., TID Metronidazole, 500-750mg P.O., TID
Management for 5-7 days. for 7-10 days.
5. DM; Polyuria Polyuria considered when there is Polyuria considered when there is
definitio consistent elimination of an abnormally consistent elimination of >3 liters
n large volume of urine, > 2000ml/24hr per day (>3000ml/24hr) or if not

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Nitsbin (ንጽቢን) Bedside oriented Internal medicine 2nd edition
What is new in 2nd edition xiii

quantified a history of increase


in urination frequency with
increase in volume of urine)
DKA Keep NPO No NPO rather Encourage
Manage feeding
ment Urine Ketone and Glucose every
4hrs Urine Ketone and Glucose every
2hrs
RI (regular insulin) 10 IU, IV and
10 IU, IM Stat RI (regular insulin) 10 IU, IV stat
only

If lab not available: 2 vials of


KCL in every bag of fluid once
urine output is adequate (>50
ml/hr)
Sliding RBS (in Mg/dl) Regular insulin RBS (in Regular insulin dose
scale dose (IU), IV Mg/dl) (IU), IV route
route
For thin For For thin For obese
and obese and and
insulin- and insulin- insulin-
sensitive
sensitive insuli resistant
pt
pt n- pt
resist
ant pt
≤ 180 Omit omit 181 – 200 Omit omit
181 – 230 1 2 201 – 250 2 2

231 – 280 2 4 251 – 300 3 4

281 – 330 3 6 301 – 350 4 6

331 – 380 4 8 351 – 400 5 8

381 – 430 5 10 401 – 450 6 10

431 – 480 6 451 – 500 7

481 – 530 7 501 – 550 8

531 – 580 8 551 – 600 9

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Nitsbin (ንጽቢን) Bedside oriented Internal medicine 2nd edition
What is new in 2nd edition xiv

581 – 600 9 >600 (High) 10

>600 (High) 10

* Most experts recommend 1 IU


increment for each 50 mg/dl
increment from 180
* Minimum threshold of RBS to add
insulin varies from setup to setup.
For example, 180, 200 and 250.
We recommend to use threshold
starting from 200 (i.e. < 200 →
omit, 201 – 250 → 1 IU….)
* This table is from Harrison 21st
edition
6. Mixed The recommended first line treatment The recommended first-line
case for mixed infection is Coartem (AL) treatment for mixed infection is
(P.F + and single dose primaquine Coartem (AL) and primaquine
P.V) radical cure for 14 days.
manage Alternative; quinine for 7 days +
ment Primaquine for 14 days The second line treatment for both
P. falciparum and P. vivax is
Dihydro artemisinin-piperaquine
(DHA-PPQ) instead of oral quinine.
HMS Chloroquine 300mg, PO, weekly for 3 Chloroquine 500mg (2tab), PO,
Malaria
manage to 6 months. weekly for 6 months.
ment
Weekly and daily dosing’s are said to Weekly and daily dosing’s are said
be equally effective to be equally effective

Follow up every 3 months (with


CBC and spleen size…
abdominal U/S)
Severe Once a patient has received at least Once a patient has received at
malaria 24h of parenteral therapy and can least 24h of parenteral therapy and
manage tolerate oral therapy, complete can tolerate oral therapy, complete
ment treatment with full (3days) course of treatment with full (3days) course of
artemether + lumefantrine (AL) second line drug (Dihydro
artemisinin piperaquine (DHA-PPQ)
Malaria AL is indicated in first trimester In all trimesters, give Artemether-
manage pregnancy only if this is the only lumefantrine (AL) For the treatment
ment treatment available for P. falciparum of Falciparum malaria in pregnancy
during malaria.
pregna
P. falciparum or mixed infection in 2nd
ncy
or 3rd trimester will be treated with
AL.

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IM Artemether should only be used IM Artemether is the second option,


during the first trimester of (IV/IM artesunate (preferred)), while
pregnancy when IV/IM artesunate Quinine (IV or IM) may be
(preferred) and IV/IM quinine are both considered as the last option.
unavailable.
7. Relapsing fever Procaine penicillin, 400,000-800,000- Procaine penicillin, 400,000-
management unit I.M. stat. 600,000-unit I.M. stat.

Tetracycline hydrochloride, 500mg Tetracycline hydrochloride, 250 -


P.O. daily for 2 days 500mg P.O. daily for 2 days

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Acronyms & Abbreviations

✓ +ve… positive ✓ JVP…jugular venous pressure


✓ -ve… negative ✓ LABA … long acting β2-agonists
✓ 2ry… Secondary ✓ LAP… Lymphadenopathy
✓ a.k.a…. Also known as ✓ LBBB… Left bundle branch block
✓ AAA… abdominal aortic aneurism ✓ LDH… Lactate dehydrogenase
✓ ABG… arterial blood gases ✓ LDL… Low density lipoprotein
✓ ACE-I… angiotensin converting enzyme inhibitors ✓ LFT… liver function test
✓ ADA… Adenosine deaminase ✓ LGS… Lymphoglandular system
✓ AF/AFib …. Atrial fibrillation ✓ LL… lower limb
✓ AFI… Acute febrile illness ✓ LLSB… left lower sternal border
✓ AI… Apical impulse ✓ LMNL… Lower motor neuron lesion
✓ AKI…. Acute kidney injury ✓ LMWH… Low molecular weight heparin
✓ ARB’s… Angiotensin- II receptor Blockers (RAAS ✓ LOC…Loss of consciousness
blocking agents) ✓ LP… Lumbar puncture
✓ ARDS…. Acute respiratory distress syndrome ✓ LSHF … left sided heart failure
✓ ARF… Acute rheumatic fever ✓ LVH… left ventricular hypertrophy
✓ ASA… acetyl salicylic acid (Aspirin) ✓ MCL… mid clavicular line
✓ ASAP…As soon as possible ✓ MDI… metered dose inhaler
✓ ASD… Atrial septal defect ✓ Mgt…management
✓ ASL… acutely sick looking ✓ M. HCT… Manual hematocrit
✓ ASO… anti streptolysin O ✓ MI… myocardial infarction
✓ Ass’t…. Assessment ✓ MND… Motor neuron disease
✓ AVM… Arteriovenous malformations ✓ MRSA… Methicillin resistant staph aureus
✓ BAL… Broncho alveolar lavage ✓ MS… Multiple sclerosis
✓ BF… Blood film ✓ MSP… Multiple sexual partner
✓ BID… two times per day, every 12 hr (lat. bis in ✓ MSS… Musculoskeletal system
die) ✓ MSSA… Methicillin sensitive staph aureus
✓ BM… Bone marrow ✓ NHL… No Hodgkin lymphoma
✓ BNP… Brain natriuretic peptide ✓ NIS… Non icteric sclera
✓ BSS… Brown Sequard syndrome ✓ NR…. Non-reactive
✓ BUN… blood urea nitrogen ✓ NS… Nervous system
✓ C.C… chief compliant ✓ NSAID’s… Non-steroidal anti-inflammatory drugs
✓ C/F… Clinical feature ✓ OCS … oral corticosteroid
✓ CBC… complete blood cell count ✓ OGTT… oral glucose tolerance test
✓ CCB’s… Calcium channel blockers ✓ OI… opportunistic infection
✓ CF… Cystic fibrosis ✓ P/E… physical examination
✓ CHD…. Congenital heart Disease ✓ PC… Pink conjunctiva
✓ CHF…. Congestive heart failure ✓ PCKD… polycystic kidney disease
✓ CKD…. Chronic kidney disease ✓ PCV… polycythaemia vera
✓ CLD… Chronic liver disease ✓ PDA… Patent Ductus arteriosus
✓ CLL… Chronic lymphocytic leukaemia ✓ PE… pulmonary embolism
✓ CML… Chronic myelogenous leukaemia ✓ PICT… Provider initiated counselling and testing
✓ CMP…Cardiomyopathy (currently changed to PITC)
✓ Cmn … Common ✓ PKDL… post kalazar dermal leishmaniasis
✓ CN… Cranial nerve ✓ PLE… Protein losing enteropathy
✓ CNS… Central Nervous system ✓ PM/PB… Peripheral morphology/ peripheral blood
✓ CO…cardiac out put smear

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✓ COPD…chronic obstructive Pulmonary disease ✓ PND… paroxysmal nocturnal dyspnoea


✓ CRMVHD… chronic rheumatic multi valvular heart ✓ PO… by mouth (lat. Per Os)
disease ✓ PRN… Per need or as needed
✓ CSF… Cerebrospinal fluid ✓ Pt…. Patient
✓ CSL… chronically sick looking ✓ PTE… pulmonary thromboembolism
✓ CT… computed tomography ✓ QD… daily, once per day (lat. Quaque in die)
✓ CVS… Cardiovascular system ✓ QID… four times per day, every 6 hr (lat. quarter
✓ CXN… complications in die)
✓ CXR… chest X-ray (chest radiography) ✓ r/o… rule out
✓ DBP… diastolic blood pressure ✓ RAAS… Renin Angiotensin aldosterone system
✓ DDX…. differential diagnosis ✓ RBBB… Right bundle branch block
✓ DIC… Disseminated intravascular coagulation ✓ RBS… random blood sugar level
✓ DM… Diabetic Mellitus ✓ RES… Reticuloendothelial system
✓ DRE… Digital rectal examination ✓ RF… risk factor
✓ DTR…Deep tender reflex ✓ RFT… Renal function test
✓ DVHD… degenerative valvular Heart Disease ✓ RHD…. Rheumatic heart Disease
✓ DVT… deep vein thrombosis ✓ RS… Respiratory system
✓ Dx …. Diagnosis ✓ RSHF … Right sided heart failure
✓ EBV… Epstein-barr virus ✓ RSHF… right sided heart failure
✓ ECG…. Electrocardiography ✓ RV … right ventricle (right ventricular)
✓ Echo… echocardiography ✓ RVHD… Rheumatic valvular Heart Disease
✓ ED… Emergency department ✓ SABA… Short acting β2-agonists
✓ EDS… Ehlers-Danlos syndrome ✓ SAH… Subarachnoid haemorrhage
✓ ESRD…. End stage renal disease ✓ SaO2/SO2/SPO2… Saturation of oxygen
✓ FBS… Fasting blood sugar level ✓ SBP... systolic blood pressure / spontaneous
✓ FND… Focal neurologic deficit bacterial peritonitis
✓ FSGS… Focal segmental glomerulosclerosis ✓ SCC… Squamous cell carcinoma
✓ GBS… Generalized body swelling ✓ SCD… sudden cardiac death
✓ GBS… Guillain barre syndrome ✓ SDH… subdural haematoma
✓ GCS… Glasgow coma scale ✓ SLE… systemic lupus erythematosus
✓ GCS… Glucocorticosteroid ✓ SOB…. Shortness of breath
✓ GUS… Genitourinary system ✓ Ssx… Syndrome
✓ HAART / ART… Highly active antiretroviral ✓ TB… Tuberculosis
therapy / antiretroviral therapy ✓ TFT… Thyroid function test
✓ HBA1c… glycosylated haemoglobin ✓ TGA … transposition of great arteries
✓ HCC… Hepatocellular carcinoma ✓ TIA … transient ischaemic attack
✓ HCMP… Hypertrophic cardiomyopathy ✓ TID… three times per day, every 8 hr (lat. ter in
✓ HDL… High density lipoprotein die)
✓ HEENT… Heed, ears, eyes, nose and throat ✓ TM… transverse myelitis
✓ HF… Heart Failure ✓ TTP… Thrombotic thrombocytopenic purpura
✓ Hgb… Haemoglobin ✓ TVLS… Total vertical liver span
✓ HGIF… High grade intermittent fever ✓ U/A… Urine analysis
✓ HHD…hypertensive Heart Disease ✓ U/L… Unit per litre
✓ HL… Hodgkin lymphoma ✓ U/S… Ultrasound
✓ HMS… Hyperactive malarial splenomegaly ✓ UL… Upper limb
✓ HPI… history of present illness ✓ UMNL… Upper motor neuron lesion
✓ HRCT… high resolution computed tomography ✓ UOP… Urine out put
✓ HSS… Hepatosplenic schistosomiasis ✓ VHD… Valvular Heart Disease
✓ HSV… Herpes simplex virus ✓ VL… Visceral leishmaniasis
✓ HTN… hypertension ✓ VTE… Venous thromboembolism
✓ Hx… history

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✓ HZV… Herpes zoster virus


✓ ICH … Intra cranial hemorrhage
✓ ICP… Intracranial pressure
✓ ICS … Inter costal space/ inhalational
corticosteroid
✓ IDA… Iron deficiency anaemia
✓ IDSA… Infectious disease society of America
✓ IE… infective endocarditis
✓ IHD… Ischemic heart disease
✓ ILD…Interstitial lung disease
✓ IM… intra muscular injection
✓ IM… Infectious mononucleosis
✓ IP… Incubation period
✓ IPF… Idiopathic pulmonary fibrosis
✓ IRIS… Immune reconstitute inflammatory
syndrome
✓ IS… Integumentary system
✓ IU… International unit
✓ IV… intravenous injection

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Table of contents

Contents page
Preface ................................................................................................................................................. iii
Acknowledgment ................................................................................................................................ iv
Contributors ........................................................................................................................................ vii
Comments on 1st edition ............................................................................................................... viii
What is new in 2nd edition ............................................................................................................. xi
Acronyms & Abbreviations .............................................................................................................xvi
Table of contents .............................................................................................................................xix
Part I; Long cases ............................................................................................................................. 1
Mysteries of best physician's about patient approach ............................................................ 2
Chapter 1; Heart failure (ልብ ድካም) and Other Cardiac Disorders .................................... 3
1.1 Heart Failure/HF/ .............................................................................................................. 20
1.1.1 Management of heart failure ................................................................................. 27
1.2 Acute Rheumatic Fever(ARF) & Rheumatic heart disease (RHD) .................... 38
1.2.1. Acute rheumatic Fever (ARF) .................................................................................. 38
1.2.2. Rheumatic Heart Disease (RHD) ............................................................................ 51
1.3 Valvular heart disease (VHD) ....................................................................................... 59
1.4 Atherosclerotic cardiovascular diseases ..................................................................... 69
1.4.1 Ischemic heart disease (IHD) ............................................................................... 69
1.4.1.1 Acute coronary syndrome (ACS) ................................................................. 72
1.4.1.2 Chronic coronary syndrome........................................................................... 87
1.4.2 Peripheral Arterial Disease (Chronic Arterial Insufficiency) .......................... 90
1.4.3 Arterial occlusion (acute limb ischemia) ............................................................ 93
1.5 Hypertension (የደም ግፊት) and HHD .......................................................................... 95
1.5.1 MANAGEMENT OF HYPERTENSION IN SPECIAL CLINICAL CONDITIONS ............ 116
1.5.2 Hypertensive crisis ...................................................................................................... 120
1.5.3 Hypertensive heart disease (HHD)......................................................................... 125
1.6 Infective endocarditis (IE)............................................................................................. 126
1.7 Arrhythmia ......................................................................................................................... 135
1. Tachyarrhythmias ............................................................................................................ 136
2. Bradycardia (Bradyarrhythmia) .................................................................................... 145
Cardiac arrest (የልብ ምት መቋረጥ) ..................................................................................... 147
Cardioversion and Defibrillation .......................................................................................... 149

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1.8 Pericarditis ........................................................................................................................ 151


1.9 Cardiomyopathy (CMP) and myocarditis ................................................................. 160
1.10 Acute HF (Cardiogenic shock and Pulmonary edema)................................... 174
1.10. 1 Cardiogenic shock................................................................................................... 175
1.10.2 Pulmonary edema ..................................................................................................... 176
1.10.2.1 ARDS (Acute respiratory distress syndrome) ............................................ 181
1.11 WHO risk based CVD (Cardiovascular disease) Management in Ethiopia
190
1.12. DM and Hypertension Follow Up Form ................................................................... 202
Chapter 2; Chronic lung disorders and Cor pulmonale...................................................... 204
2.1 Obstructive Lung diseases........................................................................................... 223
2.1.1 COPD (Chronic obstructive pulmonary disease) ........................................... 223
2.1.1.1 Exacerbations of COPD ............................................................................... 238
2.1.2 Asthma ....................................................................................................................... 242
2.2 Restrictive lung disease................................................................................................ 242
2.2.1 ILD (Interstitial Lung disease) ............................................................................. 242
2.3 Suppurative lung diseases ........................................................................................... 262
2.3.1 Bronchiectasis .......................................................................................................... 262
2.3.2 Lung Abscess .......................................................................................................... 268
2.4. Cor pulmonale and Pulmonary Hypertension......................................................... 275
Chapter 3; TB/Tuberculosis/ (የሳንባ ነቀርሳ ፣ ቲቢ) ................................................................. 281
3.1 Pulmonary TB .................................................................................................................. 295
3.2 Extra Pulmonary TB ...................................................................................................... 298
3.3 RVI-TB Coinfection......................................................................................................... 307
3.4 Management of TB ........................................................................................................ 307
3.5 Baby of a mother with Active tuberculosis............................................................. 312
3.6 Drug resistant TB ........................................................................................................... 317
Chapter 4; Lung cancer (የሳንባ ካንሰር) ..................................................................................... 319
Chapter 5; RVI (ኤችአይቪ ኤዲስ) ................................................................................................ 330
5.1. HIV/AIDS ........................................................................................................................... 344
5.2. Treatment of RVI............................................................................................................ 348
5.2.1. Antiretroviral treatment failure ............................................................................. 352
5.2.2. Monitoring ARV Treatment .................................................................................. 358
5.3. IRIS (Immune reconstitution inflammatory syndrome) ......................................... 358
5.4. Post-exposure prophylaxis (PEP) and Pre-exposure prophylaxis /PrEP/....... 361

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5.5. PMTCT and treatment of RVI exposed infant ..................................................... 364


5.6. Opportunistic infections (OI’s) ..................................................................................... 366
5.6.1. Respiratory system OI’s ....................................................................................... 369
5.6.1.1. RIV - TB coinfection...................................................................................... 369
5.6.1.2. Pneumonia in RVI patient............................................................................ 378
5.6.2. Gastrointestinal (GI) opportunistic diseases .................................................... 381
5.6.2.1. Candida infection ............................................................................................ 382
5.6.2.2. Aphthous stomatitis/ aphthous ulcer ......................................................... 384
5.6.2.3. Necrotizing Gingivitis ..................................................................................... 384
5.6.2.4. Herpes simplex (HSV1)/Herpes Labialis/ ................................................. 385
5.6.2.5. Diarrhea in HIV patients............................................................................... 385
5.6.2.6. Peri-anal problems ......................................................................................... 387
5.6.3. CNS opportunistic diseases................................................................................. 388
5.6.3.1. CNS Toxoplasmosis ....................................................................................... 389
5.6.3.2. Cryptococcal meningitis................................................................................. 392
5.6.3.3. Peripheral neuropathies ................................................................................ 396
5.6.4. Cutaneous disorders related to RVI infection ................................................ 397
5.6.4.1. varicella-zoster (Chicken Pox) /ጉድፍ/ ....................................................... 400
5.6.4.2. Herpes zoster (shingles) /አልማዝ ባለጭራ ................................................ 401
5.6.4.3. Pruritic papular eruption (PPE)................................................................... 406
5.6.5. Kaposi sarcoma (KS) ............................................................................................ 407
5.6.6. RVI - VL co infection ............................................................................................ 407
Chapter 6; Stroke (የጭንቅላት ደም ስር በሽታ፣ እስትሮክ) ........................................................ 408
6.1 Ischemic stroke ............................................................................................................... 426
6.2 Hemorrhagic stroke (Intracranial hemorrhage) ....................................................... 435
6.3. Management of Stroke ................................................................................................. 443
Chapter 7; Paraplegia (ከወገብ በታች ሽባነት) ............................................................................ 460
7.1. Localization of neurologic disorders .......................................................................... 472
7.2. Diseases of the Spinal Cord ...................................................................................... 479
7.2.1. Acute and subacute spinal cord diseases ...................................................... 489
7.2.2. Chronic myelopathies (spinal cord diseases) ................................................. 503
7.2.3. Rehabilitation of spinal cord disorders ............................................................. 506
7.3. GBS (Guillain-Barré syndrome) .................................................................................. 507
7.4. ALS (Amyotrophic Lateral Sclerosis and Other Motor Neuron Diseases) .... 512
Chapter 8; Meningitis (ማጅራት ገትር)........................................................................................ 513

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Chapter 9; CLD/ Chronic liver disease/ (የጉበት በሽታ) ........................................................ 528


9.1 Liver Cirrhosis and Complications of CLD with their Treatment...................... 550
9.1.1 Portal hypertension related cxn.......................................................................... 552
9.1.1.1 Portal Hypertension ........................................................................................ 552
9.1.1.2 Ascites ............................................................................................................... 553
9.1.1.3 Spontaneous bacterial peritonitis (SBP)................................................... 555
9.1.1.4 Esophageal varices and Variceal bleeding ............................................. 557
9.1.2 Hepatic insufficiency related CXN ..................................................................... 559
9.1.2.1 Hepatic Encephalopathy (HE) ..................................................................... 559
9.1.2.2 Hepatorenal Syndrome (HRS) .................................................................... 562
9.1.2.3 Hepatopulmonary syndrome (HPS) ........................................................... 564
9.1.2.4 Synthetic dysfunction ..................................................................................... 565
9.2 Causes of CLD ............................................................................................................... 566
9.2.1 Viral Hepatitis (ሄፓታይቲስ ቫይረስ እና የጉበት ብግነት) ..................................... 566
9.2.2 Alcoholic liver disease........................................................................................... 578
9.2.3 Autoimmune hepatitis ............................................................................................ 580
9.2.4 Genetic, metabolic and infiltrative diseases affecting the liver ................. 584
9.2.4.1 Hereditary Hemochromatosis ....................................................................... 584
9.2.4.2 Wilson’s disease ............................................................................................. 585
9.2.4.3 AAT (α1 ANTITRYPSIN) deficiency ........................................................... 586
9.2.4.4 Nonalcoholic Fatty Liver Diseases (NAFLD) and Nonalcoholic
Steatohepatitis (NASH) ..................................................................................................... 587
9.2.4.5 Other causes of CLD .................................................................................... 589
9.3 Jaundice and hyper bilirubinemia .............................................................................. 589
Chapter 10; DM /Diabetes Mellitus/ (የስኳር በሽታ)................................................................ 595
10.1. ACUTE COMPLICATIONS OF DIABETES ......................................................... 631
10.1.1. DKA and HHS ..................................................................................................... 631
10.1.1.1. Fluid Management of DKA in CHF, CKD, HTN and CLD patients 645
10.1.2. Hypoglycaemia..................................................................................................... 646
10.2. CHRONIC COMPLICATIONS OF DIABETES .................................................... 651
10.2.1. Diabetic nephropathy ......................................................................................... 653
10.2.2. Diabetic Retinopathy .......................................................................................... 654
10.2.3. Diabetic neuropathy ........................................................................................... 654
10.2.4. Diabetic foot ulcer .............................................................................................. 658
10.3. Pediatrics DM and DKA Case Management...................................................... 677

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Chapter 11; AKI/Acute kidney injury/ and CKD/ Chronic kidney disease (የኩላሊት
በሽታ) .................................................................................................................................................. 694
11.1 Acute Kidney Injury (AKI) ........................................................................................ 702
11.2 Chronic Kidney Disease (CKD) .............................................................................. 712
Chapter 12; Glomerular disease (Nephrotic syndrome/NS/ and Nephritic
syndrome/Nts/) ................................................................................................................................. 722
12.1 Nephrotic syndrome (NS)............................................................................................... 729
12.2 Nephritic syndrome .......................................................................................................... 734
Chapter 13; Leishmaniasis (ካላዛር/ጓቋ/ድባ/ እና ቁንጭር) ........................................................ 746
13.1 Leishmaniasis............................................................................................................... 763
13.2 VL; Visceral Leishmaniasis/kala-azar/ (ካላዛር ፣ ጓቋ፣ ድባ) ............................... 767
13.2.1 Management of VL ................................................................................................ 767
13.2.2 Patient Follow-Up in Management of VL ........................................................ 771
13.2.3 VL Relapse............................................................................................................... 773
13.2.4 Treatment of VL by Drug Interruption.............................................................. 776
13.2.5 RVI - VL co infection ............................................................................................ 776
13.2.6 Post kala-azar Dermal Leishmaniasis (PKDL) ............................................... 781
13.2.7 VL Treatment in Special Groups ....................................................................... 783
13.3. Cutaneous Leishmaniasis (CL) /ቁንጭር/ ................................................................... 785
13.4 Diffuse Cutaneous Leishmaniasis (DCL) ................................................................... 789
13.5 Mucocutaneous/Mucosal Leishmaniasis (ML) ........................................................... 790
Chapter 14; Leukaemia (የደም ካንሰር) ....................................................................................... 792
14.1 Acute Leukaemia .............................................................................................................. 803
14.1.1 Acute myelogenous leukemia (AML) ................................................................... 803
14.1.2 Acute lymphoblastic leukemia (ALL).................................................................... 810
14.2 Chronic Leukaemia .......................................................................................................... 814
14.2.1 Chronic Lymphatic Leukemia (CLL) .................................................................... 814
14.2.2 Chronic myelogenous leukemia (CML) ............................................................... 819
CHAPTER 15; Lymphomas (የደም ካንሰር) ................................................................................ 823
15.1 Hodgkin’s lymphoma (HL) .............................................................................................. 832
15,2 Non Hodkins lymphoma ................................................................................................. 839
15.3 Special considerations ..................................................................................................... 844
15.3.1 Tumor lysis syndrome (TLS) ................................................................................. 844
15.3.2 Hyperleukocytosis and leukostasis in hematologic malignancies ................ 848
15.3.3 Neutropenic fever ...................................................................................................... 851

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15.3.4 Neutropenic enterocolitis (typhlitis) ....................................................................... 854


Chapter 16; Case reporting format for bedside, round, exam and case discussion . 857
Part II; Short cases ....................................................................................................................... 869
Chapter 1; Physical examination ............................................................................................... 870
1.1 Respiratory System ............................................................................................................ 870
1.1.1 Physical examination findings .................................................................................. 871
1.1.2 pleural effusion ............................................................................................................. 874
1.1.3 Consolidation................................................................................................................. 875
1.1.4 Pulmonary edema ....................................................................................................... 876
1.1.5 Pneumothorax ............................................................................................................... 877
1.1.6 Pulmonary fibrosis ....................................................................................................... 878
1.1.7 lung collapse (Atelectasis) ........................................................................................ 878
1.1.8 emphysema ................................................................................................................... 879
1.2 Cardiovascular System ...................................................................................................... 880
1.2.1 Physical examination findings .................................................................................. 880
1.2.2. Murmur .......................................................................................................................... 884
1.2.3 Leg edema .................................................................................................................... 889
1.3 Abdominal examination ..................................................................................................... 890
1.3.1 Physical examination findings .................................................................................. 890
1.3.2 Ascites ............................................................................................................................ 892
1.3.3 Splenomegally............................................................................................................... 894
1.3.4 Hepatomegaly, Hepatomegaly with ascites, Hepatosplenomegaly ................ 896
Hepatomegaly ...................................................................................................................... 896
Hepatomegaly with ascites .............................................................................................. 896
1.3.5 Renomegaly .................................................................................................................. 897
1.3.6 Abdominal mass .......................................................................................................... 897
1.4 Nervous system................................................................................................................... 898
1.4.1 Physical examination findings .................................................................................. 898
1.4.2 Paraplegia/paresis ....................................................................................................... 904
1.4.3 Monoplegia/paresis ...................................................................................................... 904
1.4.4 Quadriplegia/paresis .................................................................................................... 905
1.4.5 Coma .............................................................................................................................. 906
1.5 HEENT ................................................................................................................................... 908
1.5.1 physical Examination findings .................................................................................. 908
1.5.2 Icteric sclera ................................................................................................................ 908

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Pale conjunctiva ...................................................................................................................... 908


1.6 LGS......................................................................................................................................... 908
1.6.1 physical Examination findings .................................................................................. 908
1.6.2 LAP .................................................................................................................................. 908
Chapter 2; common medical procedures and result analysis ........................................... 909
2.1 LP (Lumbar puncture) ................................................................................................... 909
2.1.1 CSF analysis............................................................................................................ 911
2.2 Pleural tap (thoracentesis) ........................................................................................... 915
2.2.1 Pleural fluid analysis ............................................................................................. 917
2.3 Peritoneal tap (paracentesis) ...................................................................................... 920
2.3.1 Ascitic fluid analysis .............................................................................................. 921
2.4 BM aspiration................................................................................................................... 922
2.5 Splenic Aspiration ........................................................................................................... 924
2.6 LN aspiration.................................................................................................................... 926
Chapter 3; Shock ........................................................................................................................... 927
3.1. Management of hypovolemic shock ............................................................................. 934
3.2. Cardiogenic shock (pump failure) ................................................................................. 935
3.3. Septic shock........................................................................................................................ 942
3.4. Adrenal Crisis ..................................................................................................................... 944
3.5. Refractory shock ................................................................................................................ 945
3.6. Shock and Pulmonary edema Management when they happen together ....... 945
Chapter 4; Hypoglycaemia .......................................................................................................... 946
Chapter 5; DKA .............................................................................................................................. 946
Chapter 6; Thyroid storm ............................................................................................................. 946
Chapter 7; Nerveous System Related Disorders and Infections ..................................... 946
7.1. CVA (stroke) .................................................................................................................... 946
7.2. Seizure and epilepsy (የሚጥል በሽታ) ........................................................................ 947
7.2.1. Status epilepticus and management of Active seizure in emergency
setup 960
7.2.2. Treatment of Seizures and epilepsy ................................................................. 966
7.3. Bell’s Palsy ....................................................................................................................... 972
7.4. Parkinson’s Disease....................................................................................................... 973
Chapter 8; Respiratory related disorders and infections .................................................... 976
8.1. Pneumonia (የሳንባ ምች) ................................................................................................. 976
8.1.1. Community-Acquired pneumonia (CAP) ........................................................... 980

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8.1.2. Hospital-acquired pneumonia /HAP/ (Nosocomial Pneumonias) ............... 982


8.1.3. Aspiration pneumonia: ........................................................................................... 984
8.1.4. Severe pneumonia ................................................................................................. 987
8.1.5. Empyema and Complicated Parapneumonic Effusions ............................... 989
8.2. Acute tonsillopharyngitis (የቶንሲል በሽታ ፣ የአንቃር እና ጉሮሮ ብግነት) ............... 993
8.3. Asthma (አስም) .................................................................................................................. 1005
8.3.1. Acute asthma exacerbations ................................................................................. 1013
8.3.2. How to use inhalers for asthma management ................................................ 1026
8.3.3. Chronic asthma ....................................................................................................... 1033
Chapter 9; GI related disorders and infections ................................................................... 1043
9.1. Infectious Diarrheal Disease (የተቅማጥ በሽታ/የተቅማጥ ልክፍት/).......................... 1043
9.1.1 Bloody diarrhoea /ደም የቀላቀለ ሰገራ/..................................................................... 1043
9.1.1.1 Bacillary dysentery /በሲላዊ ተቅማጥ፣ በባክቴሪያ ልክፍት የሚመጣ ተቅማጥ/
.............................................................................................................................................. 1043
9.1.1.2 Amoeba (አሜባ) ................................................................................................... 1045
9.1.2. Watery diarrhoea /ውሃ የመሰለ ተቅማጥ/ .............................................................. 1047
9.1.2.1 Giardia (ጃርዲያ) ................................................................................................... 1048
9.1.2.2 Cholera (አተት፣ ኮሌራ)....................................................................................... 1050
Table -Treatment of common Infectious Diarrheal Disease .................................... 1061
9.2. Intestinal Helminthic Infestations (የአንጀት ጥገኛ ተውሳክ ፣የአንጀት ትላትል) and
blood flukes ................................................................................................................................ 1063
9.2.1. Ascariasis/Round worm/ (ወስፋት)......................................................................... 1063
9.2.2. Taeniasis/Tape worm/ (ኮሶ).................................................................................... 1065
9.2.3. Hook worm (መንጠቆ) ............................................................................................... 1068
9.2.4. Schistosomiasis (ቢሊሃርዚያ) .................................................................................. 1070
Table -Treatment of common intestinal helminthic parasitic infestations and blood
flukes ........................................................................................................................................ 1077
9.3. Dyspepsia, PUD and GERD (የጨጓራ ሕመም ፣ ቁስለትና አሲድ መብዛት) ........ 1080
9.3.1. Dyspepsia (የጨጓራ ሕመም፣ የምግብ አለመፈጨት ችግር) .................................. 1080
9.3.2. Peptic ulcer disease (PUD)/የጨጓራ ቁስለት/ ...................................................... 1085
9.3.3. Gastroesophageal reflux disease (GERD) ........................................................ 1087
9.4. GI bleeding ..................................................................................................................... 1089
9.4.1. Upper GI bleeding ................................................................................................... 1089
9.4.2. Lower GI bleeding ................................................................................................... 1094
9.5. IBD (inflammatory Bowel Disease).......................................................................... 1097

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Chapter 10; UTI (የሽንት ቧንቧ ልክፍት/ኢንፌክሽን/) ................................................................ 1109


Chapter 11; Acute febrile illness (AFI) .................................................................................. 1119
11.1. Malaria (ወባ) ............................................................................................................... 1119
11.2. Typhoid fever (ታይፎይድ)........................................................................................ 1147
11.3. Typhus (ታይፈስ) ........................................................................................................ 1153
11.4. Relapsing fever ......................................................................................................... 1157
Chapter 12; MSS Related disorders and infections .......................................................... 1161
12.1. Rheumatologic Disorders............................................................................................. 1161
12.1.1 Gout (ሪህ) ................................................................................................................ 1161
12.1.2. Systemic lupus erythematosus (SLE) (lupus) ................................................ 1171
12.1.3 Rheumatoid arthritis (RA) /ቁርጥማት/................................................................. 1177
12.1.4 Osteoarthritis (የአጥንት እና አንጓ ብግነት)............................................................. 1185
12.2. MSS infections ............................................................................................................... 1189
12.2.1. Pyogenic Osteomyelitis......................................................................................... 1189
12.2.2. Septic Arthritis ......................................................................................................... 1191
Chapter 13; Hematologic Disorders ........................................................................................ 1194
13.1. Anaemia (የደም ማነስ).................................................................................................... 1194
13.1.1. Iron deficiency anemia (IDA) .............................................................................. 1202
13.1.2. Megaloblastic anemia............................................................................................ 1206
13.2. Blood Transfusion.......................................................................................................... 1208
13.3. Thrombocytopenia ......................................................................................................... 1214
13.3.1. Thrombocytopenia in hospitalized patients ..................................................... 1214
13.3.2. Immune/Idiopathic Thrombocytopenic Purpura (ITP) ................................... 1216
13.4. VTE (DVT and PTE) .................................................................................................... 1220
13.4.1. VTE prophylaxis ..................................................................................................... 1230
Chapter 14; Fluid and electrolyte disturbance ..................................................................... 1233
14.1. Fluid, Maintenance Fluid (MF) calculation ............................................................. 1233
14.2. Electrolyte disturbance ................................................................................................. 1237
14.2.1 Hypokalaemia ........................................................................................................... 1237
14.2.2 Hyperkalemia ............................................................................................................ 1240
14.2.3 Hyponatremia ............................................................................................................ 1242
14.2.4 Hypernatremia .......................................................................................................... 1245
14.2.5. Hypocalcemia .......................................................................................................... 1248
14.2.6. Hypercalcemia ......................................................................................................... 1251
14.2.7 Hypomagnesemia .................................................................................................... 1254

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14.2.8 Hypermagnesemia ................................................................................................... 1258


Chapter 15; Dyslipidemia and metabolic syndrome ........................................................... 1261
15.1. Metabolic syndrome ...................................................................................................... 1261
15.2. Dyslipidemia .................................................................................................................... 1261
Chapter 16; STI (የአባላዘር በሽታ) .............................................................................................. 1266
16.1. Vaginal Discharge Syndrome/VDS/ .......................................................................... 1267
16.2. Lower Abdominal Pain/Pelvic inflammatory disease/(PID) ................................ 1269
16.3. Urethral Discharge Syndrome (UDS) ...................................................................... 1271
16.3.1. Persistent/Recurrent Urethral Discharge ........................................................ 1273
16.4. Genital Ulcer Syndrome (GUS)................................................................................. 1275
16.5. Scrotal Swelling ............................................................................................................. 1278
16.4. Inguinal Bubo ................................................................................................................. 1280
16.5. Neonatal conjunctivitis. ................................................................................................ 1282
Syphilis (ቂጥኝ)........................................................................................................................... 1282
Gonorrhea (ጨብጥ)................................................................................................................... 1292
Table; Pharmacologic Treatment of STI............................................................................ 1297
Prevention of STIs ................................................................................................................... 1300
Chapter 17; Sepsis ...................................................................................................................... 1302
Chapter 18; Thyroid Hormone Disorders .............................................................................. 1312
18.1. Thyrotoxicosis and Thyroid storm (የሚረጭ እንቅርት) .......................................... 1312
18.1.1. Thyrotoxicosis .......................................................................................................... 1312
18.1.2. Thyroid storm / thyrotoxic crisis ........................................................................ 1316
18.2. Hypothyroidism ............................................................................................................... 1322
Chapter 19; Poisoning, Drug Overdose, and Envenomation .......................................... 1326
19.1. Poisoning and over dose(መመረዝ) ......................................................................... 1326
General Management for poisoning and overdose ...................................................... 1328
19.2. Specific poisons ............................................................................................................. 1335
19.2.1 Organophosphates and Carbamates poisoning (ጸረ ተባይ፣ ተባይ ማጥፊያ፣
ማላታይን /በተለምዶ/) .............................................................................................................. 1335
19.2.2. Caustics Corrosives (በአሲድ ወይም ቤዝ መመረዝ) .......................................... 1343
19.2.3. Herbicides (ጸረ አረም፣ የአረም ማጥፊያ መርዝ) poisoning .............................. 1345
19.2.3.1 ChlorophenoxyHerbicides ............................................................................... 1345
19.2.3.2 Bipyridyl Herbicides (Paraquat and Diquat) ............................................. 1346
19.2.3.2. Organophosphate herbicides ....................................................................... 1348
19.2.4. Rodenticides Poisoning (የአይጥ መርዝ እና የነቀዝ መድሃኒት) መመረዝ ....... 1348

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19.2.5. Ethanol (ከልክ ያለፈ ስካር፣ በአልኮል መመረዝ) .................................................... 1353


19.2.6. Household Products .............................................................................................. 1355
19.2.6.1. Detergents (መንጽህ) ....................................................................................... 1355
19.2.6.2. Sodium Hypochlorite /Bleach/(በረኪና) ........................................................ 1356
19.2.6.3 Dettol (ዲቶል)..................................................................................................... 1357
19.2.7. Hydrocarbon (ጋዝ፤ቤንዚን፤ኪሮሲን) poisoning .................................................. 1358
19.2.8. Carbon monoxide poisoning (በጭስ መመረዝ) ................................................. 1361
19.3. Snake bite (የእባብ ንክሻ) ............................................................................................... 1363
19.4. Specific Drug Overdoses (እጅግ ከመጠን በላይ የሆነ መድሃኒት በመውሰድ መመረዝ)
...................................................................................................................................................... 1370
19.4.1. Acetaminophen/Paracetamol/ overdose ........................................................... 1370
19.4.2. NSAIDs Overdose .................................................................................................. 1372
19.4.3. Cardiac glycosides (digoxin and digitoxin) overdose .................................. 1373
19.4.4. Opiates and opioids overdose ........................................................................... 1376
19.4.5. Phenothiazines and other antipsychotic drug overdose ............................. 1377
19.4.6. Benzodiazepines (BDZ) Toxicity ........................................................................ 1379
19.4.7. Anticonvulsants poisoning .................................................................................... 1381
19.4.7.1 Phenytoin and fos phenytoin poisoning .................................................... 1381
19.4.7.2 Carbamazepine poisoning ............................................................................. 1383
19.4.7.3 Valproate (valproic acid/VPA/) poisoning .................................................. 1385
19.4.8. Barbiturates (Commonly phenobarbitone/PB/) ............................................... 1386
19.4.9. TCA (Tricyclic antidepressant) Poisoning ....................................................... 1389
Chapter 20; Miscellaneous ........................................................................................................ 1392
20.1. Tetanus (መንጋጋ ቆልፍ)................................................................................................ 1392
20.2. Leprosy (የስጋ ደዌ በሽታ ፣ ቁምጥና) ........................................................................... 1398
20.3. Anthrax (ቁርባ)................................................................................................................. 1409
20.4. Rabies (የእብድ ውሻ በሽታ)............................................................................................ 1413
20.5. Filariasis, Lymphatic (Elephantiasis)/ዝሆኔ/ ............................................................. 1417
20.6. COVID -19 ...................................................................................................................... 1421
Chapter 21; Interpretation of Chest X - Ray (የደረት ራጅ ማንበብ) ................................. 1427
21.1. Step 1. Quality Assessment (Technical Aspects) ................................................ 1428
21.2. Step 2. Assessment of Patient dependent factors ............................................. 1431
21.3. Step 3. Review of important radiographic anatomy ........................................... 1435
21.4. CXR features of common lung pathologies .......................................................... 1461
Chapter 22; Basics of ECG and ECG interpretation ........................................................ 1469

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22.1 ECG.................................................................................................................................... 1469


22.2. ECG Leads and electrodes ........................................................................................ 1470
22.3. ECG GRID ...................................................................................................................... 1474
22.4. ECG COMPLEXES AND INTERVALS.................................................................... 1476
22.5. APPROACH TO ECG INTERPRETATION ............................................................ 1483
22.5.1. Determining the Heart Rate................................................................................ 1483
22.5.2. Rhythm Analysis ..................................................................................................... 1487
22.5.3. Axis determination ................................................................................................. 1492
22.5.4. Intervals..................................................................................................................... 1497
22.5.5. P wave ...................................................................................................................... 1497
22.5.6. QRS complex ........................................................................................................ 1498
22.5.7. ST segment-T wave .............................................................................................. 1500
22.5.8. Overall interpretation ............................................................................................. 1502
22.6. Common Disorders based on Pathologic finding from ECG ........................... 1504
22.6.1 Myocardial Ischemia/infarction ............................................................................. 1504
22.6.2 Pericarditis ................................................................................................................. 1512
22.6.3 Chamber enlargement and hypertrophy ........................................................... 1514
22.6.4 Arrhythmia ................................................................................................................. 1518
22.6.4.1. Atrial and atrioventricular nodal (supraventricular) arrhythmias ........ 1525
22.6.4.1.1 ATRIAL FIBRILLATION AND ATRIAL FLUTTER ........................... 1531
22.6.4.2. Rhythms Produced by Conduction Block ................................................ 1537
22.6.4.3 Ventricular arrhythmias ................................................................................... 1544
22.6.5 Electrolyte abnormalities ........................................................................................ 1556
22.6.6 Drug toxicity .............................................................................................................. 1558
Chapter 23; Basics about rational use of antibiotics ........................................................ 1560
Chapter 24; Symptoms and signs in Amharic (የበሽታ ምልክቶች አማርኛ ትርጉም) ...... 1571
24.1. Amharic translation of Selected Dermatologic disorders (የተወሰኑ የቆዳ
በሽታዎች አማርኛ ትርጉም) ......................................................................................................... 1573
Chapter 25; anatomical body parts in Amharic (የሰውነት አካል ክፍሎች አማርኛ ትርጉም)
.......................................................................................................................................................... 1574
Chapter 26; Common Laboratory Investigations with practical points and procedures
.......................................................................................................................................................... 1577
26.1. Basic Hematology tests ............................................................................................... 1580
26.1.1 BF (Blood film) ........................................................................................................ 1580
26.1.2 Manual hematocrit (M.HCT) ................................................................................. 1585

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26.1.3 Hemoglobin (Hgb) Determination ........................................................................ 1586


26.1.4 PM (Peripheral morphology) ................................................................................ 1588
26.1.5 Blood group and RH (BG & RH) determination, cross match ................. 1589
26.1.6 ESR (Erythrocyte Sedimentation Rate) (Macro and micro /µ/ ESR) ....... 1594
26.2 RBS, FBS, OGTT, and HbA1c .................................................................................. 1596
26.3. U/A (Urine analysis) ..................................................................................................... 1598
26.4. S/E (stool examination) ............................................................................................... 1602
26.5. Serology and Rapid diagnostic tests /RDT/ .......................................................... 1607
26.5.1 Urine HCG ................................................................................................................ 1607
26.5.2 PICT ............................................................................................................................ 1609
26.5.3 Rapid malaria test .................................................................................................. 1610
26.5.4 widal test ................................................................................................................... 1612
26.5.5 Weil-Felix slide agglutination test ....................................................................... 1614
26.5.6 H. Pylori stool antigen and serum Ab test ..................................................... 1616
26.5.7 HBsAg (Hepatitis B virus surface antigen) test ............................................. 1619
26.5.8 HCV Ab (Hepatitis C virus antibody) test ....................................................... 1620
26.5.9 rk- 39 Rapid Diagnostic Test .............................................................................. 1621
26.5.10 RPR (Rapid reagain card test for syphilis) .................................................. 1624
26.5.11 VDRL Slide Qualitative Test.............................................................................. 1625
26.5.12 ASO latex slide agglutination test ................................................................... 1625
26.6. Basic microbiological tests.......................................................................................... 1626
26.6.1 AFB ............................................................................................................................. 1626
26.6.2 Gram stain ................................................................................................................ 1628
26.6.3 Culture & biochemical tests ................................................................................. 1630
Chapter 27; Reference Intervals for Laboratory Tests...................................................... 1640
Reading assignment .................................................................................................................... 1647
References (ዋቢ መጽሐፍት) ....................................................................................................... 1648

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Table of contents

Part I; Long cases

Part I; Long
cases

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Mysteries of best physician's about patient approach

Mysteries of best physician's about patient approach


especially for bedside, round and Oral exam presentation

History → even though, there is interpersonal variations most experts prefer


the following way of history preparation
o Elaborate the chief compliant including aggravating and relieving factors
followed by associated symptoms.
o For chronic patients firstly explain the chronic condition then elaborate
the current condition which leads you what was going on progressively.
Don't forget Adherence and follow up. For example, the precipitant for
DKA may be drug discontinuation and follow up at chronic OPD is one
part of management for chronic diseases.
o Then write positive and negative statements. Pertinent negative
statements have almost equal importance as pertinent positive
statements (e.g. if you say there is no history of Alcohol intake for CLD
patient, you are almost excluding alcoholic liver disease)
o The order of +ve and -ve statements should be risk factor and
precipitants, then complication, last but not the least DDX. But, if there
is pertinent positive, put as top before pertinent negatives regardless of
being RF, CXN or DDX. Always list in the order from most common to
least common and consider geographic area of the patient (for example
for meningitis patient from low land area, you have to consider cerebral
malaria as a DDX)
Put pertinent physical examination findings and don't miss pertinent negatives
Write your diagnosis and make it complete (e.g NYHA class IV, stage C, CHF
2ry to CRMVHD (MR, TR, AR) precipitated by CAP)
o After putting your full DX, write your evidence for the case (You have to
convince by the the order of pt’s smx, sign, other supportive evidence,
RF ± Ix findings. 1st put your +ve evidence then add -ve evidences)
List your differential diagnosis in the order from most common to least
common (and consider what is common in our setup rather than those written
based on western setup).
o While you are listing DDX you have to know what is in favor and
against for that specific DDX. It is better not to list DDX that you don’t
explain well. The examiner will ask you based on what you are telling
him/her.
List IX (better if you list baseline IX, diagnostic IX and common ones first
followed by supportive IX, IX for mgt purpose and drug toxicity, finally follow
up IX. for clinical practice, consider those available in Ethiopia and patients’
affordability)
Last but not list is management principle of your case (Diagnosis).

GOOD LUCK!!!
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Chapter 1; Heart failure (ልብ ድካም) and Other Cardiac Disorders

Chapter 1; Heart failure (ልብ ድካም)


and Other Cardiac Disorders
Dr. Mulualem. G

Clinical features and how to write hx of cardiac patient


History

The cardinal symptoms of heart failure (HF) are fatigue and shortness of
breath.
Fatigue
o Although fatigue traditionally has been ascribed to the low cardiac output
in HF, it is likely that skeletal-muscle abnormalities and other noncardiac
comorbidities (e.g., anemia) also contribute to this symptom.
o Fatigue is a non-specific symptom: if the predominate symptom is
fatigue consider also Hypothyroidism, Adrenal insufficiency, CKD, CLD,
DM and after exclusion of organic causes: chronic fatigue syndrome.
Dyspnea or shortness of breath → Defined as difficult or labored breath
o In the early stages of HF, dyspnea is observed only during exertion;
however, as the disease progresses, dyspnea occurs with less
strenuous activity, and it ultimately may occur even at rest.
o The origin of dyspnea in HF is probably multifactorial.
o The most important mechanism is pulmonary congestion with
accumulation of interstitial or intra-alveolar fluid, which activates juxta
capillary J receptors, which in turn stimulate the rapid, shallow breathing
characteristic of cardiac dyspnea.
o Other factors that contribute to dyspnea on exertion include reductions
in pulmonary compliance, increased airway resistance, respiratory muscle
and/or diaphragm fatigue, and anemia.
o Dyspnea may become less frequent with the onset of right ventricular
(RV) failure and tricuspid regurgitation
Orthopnea
o Defined as dyspnea occurring in the recumbent position
o It is usually a later manifestation of HF than is exertional dyspnea.
o It results from redistribution of fluid from the splanchnic circulation and
lower extremities into the central circulation during recumbency, with a
resultant increase in pulmonary capillary pressure.
o Orthopnea generally is relieved by sitting upright or sleeping with
additional pillows.
o Although orthopnea is a relatively specific symptom of HF, it may occur
in patients with abdominal obesity or ascites and patients with
pulmonary disease whose lung mechanics favor an upright posture
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Chapter 1; Heart failure (ልብ ድካም) and Other Cardiac Disorders

Nocturnal cough
o It is a common manifestation of the process seen in orthopnea and a
frequently overlooked symptom of HF.
o Most Commonly position dependent productive nocturnal cough with
whitish frothy sputum
PND (Paroxysmal nocturnal dyspnea)
o This term refers to acute episodes of severe shortness of breath and
coughing that generally occur at night and awaken the patient from
sleep, usually 1 - 3 h after the patient retires.
o PND may manifest as coughing or wheezing, possibly because of
increased pressure in the bronchial arteries leading to airway
compression, along with interstitial pulmonary edema that leads to
increased airway resistance.
o Whereas orthopnea may be relieved by sitting upright at the side of the
bed with the legs in a dependent position, patients with PND often have
persistent coughing and wheezing even after they have assumed the
upright position.
Palpitations
o An unexpected awareness of the heartbeat.
Cardiac asthma
o It is closely related to PND, is characterized by wheezing secondary to
bronchospasm, and must be differentiated from primary asthma and
pulmonary causes of wheezing.
Ankle swelling if patient develop Congestion (i.e. CHF)
o It is a cardinal manifestation of CHF
o Ankle edema of cardiac origin is usually symmetrical and worst in the
evenings, with improvement during the night. (if the patients spend a lot
of time lying down, we may see sacral edema)
o As failure progresses, edema ascends to involve the legs, thighs,
genitalia and abdomen (i.e. progressive edema to become GBS).
o Also gain in weight of ≥ 3 kg
o Remark: generalized edema is by definition fluid accumulation at
intestinal space (soft tissue) along with third space (plural, peritoneal
and pericardial)
o See Peripheral pitting edema from physical examination in HF below
Weight loss (Cardiac cachexia)
o With severe chronic HF, there may be marked weight loss and
cachexia.
o Significant weight loss when pt loss ≥ 10% of his/her initial body weight
within 6 months
o Although the mechanism of cachexia is not entirely understood, it is
probably multifactorial (may be, due to anorexia from hepatic and
intestinal congestion or mesenteric hypoxia).
o When present, cachexia augurs a poor overall prognosis.
Chest pain
o May be from angina (in MI), Pericarditis or from precipitants like
Pneumonia, PTE etc. 4
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Chapter 1; Heart failure (ልብ ድካም) and Other Cardiac Disorders

Other Symptoms
o Patients with HF also may present with GI symptoms;
▪ Anorexia, nausea, and early satiety associated with abdominal
pain and fullness are common complaints and may be related to
edema of the bowel wall and/or a congested liver.
▪ Congestion of the liver and stretching of its capsule may lead to
right upper quadrant pain.
o Cerebral symptoms such as confusion, disorientation, and sleep and
mood disturbances may be observed in patients with severe HF,
particularly elderly patients with cerebral arteriosclerosis and reduced
cerebral perfusion.
o Nocturia is common in HF and may contribute to insomnia. (Bed rest
will increase renal blood flow as do urine output)
o Syncope, presyncope and dizziness
▪ CNS manifestations due to decreased cardiac output
▪ Syncope: a transient loss of consciousness. There are different
circumstances in which the syncope occurs such as;
• Postural syncope: on standing for prolonged periods or
standing up suddenly
• Micturition syncope: while passing urine
• Tussive syncope: on coughing or
• Vasovagal syncope: with sudden emotional stress
• Remark; cardiac vs vasovagal syncope
o Cardiac syncope has no previous syncopal
episodes. But syncope happens during activity or at
peak activity, there is family Hx of heart disease,
and usually with abnormal ECG. In contrast to
cardiac syncope, vasovagal will have presyncope
episodes, syncope trigger, prolonged standing and
lightheadedness symptom.
▪ Presyncope: a transient sensation of weakness without loss of
consciousness.
▪ Dizziness → feeling of light headedness

Characterization of patient history

Pt’s may present with


o SOB… most common presentation
o GBS
o Bilateral leg swelling
If a known cardiac patient → ask the following on your hx
o For how long he/she was Diagnosed to have cardiac disease
▪ e.g a known cardiac pt for the past 5 years or you can say 5
years back he/she was told to have cardiac disease (you can
ask what was the presentation at that time and how Dx was
made… no need to write on your HPI) 5
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o What medication he/she was taking… e.g he/she was on


Lasix(furosemide), spironolactone, benzathine penicillin ... ask dose
and frequency of each drug
▪ Dietary modification like on salt free diet, recommended to
decrease alcohol intake and to avoid smoking.
o Adherent or not
o Where was the follow up and frequency (every month, every two
months….)
o How was his/her smx’s in between… improving, worsening or no
change at all… if not improving or worsening what was the reason
(non-adherence, wrong diagnoses…)
➢ SOB (dyspnea)
o Insidious in onset
o Progressively worsening (e.g he/she experienced Dyspnea while
doing supra ordinary activities like…. Followed by dyspnea while
doing sub ordinary activities like… and later dyspnoea at rest…
when was the time for each)
➢ Orthopnea… how many pillows he/she use during bed time (e.g orthopnea
of 3 pillows)
➢ PND…. Pt awake from sleep and open windows for Air hunger
➢ Palpitation
➢ Cough
o Most Commonly position dependent productive nocturnal cough with
whitish frothy sputum (even though this is the typical character of
cough in HF, it can be bloody or even Hemoptysis in some cases
like patient with MS, pulmonary edema or PTE)
o It can be dry and persistent then become productive
▪ Position dependent (aggregated when he/she assume supine
position)
▪ Whitish and frothy
▪ Non foul smelling
▪ Non blood tingled
▪ Quantify the amount… e.g 3-4 Arabic coffee cup per day
➢ Leg swelling … ask the following
o Symmetry → bilateral or unilateral (most commonly bilateral.
Unilateral swelling in CHF is less likely)
o Site → pedal, swelling up to the knee, GBS
o Duration
o Progression… e.g goes upwards starting from knee within 2 weeks
duration
o Diurnal variation → disappear in the morning and marked on sitting
position or prolonged standing
o How the pt noticed the swelling N.B body swelling
o Painful or not …. Mostly painless
➢ In cardic pt. →start from leg and goes upward
➢ In renal disease → begin from face (morning
facial puffines) 6
➢ In liver disease → start with abdominal
distension which may progress to GBS
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➢ Weight loss
o E.g. significant weight loss from 53 kg to 45 kg which is 15% of
his/her initial body weight or
o Unquantified but significant weight loss to the extent his/her closes
become loose (if s/he didn’t remember his/her initial body weight but
claim that S/he lose his/her body weight)
o Make sure that the patient is not in diuretics
➢ Chest pain → angina (common in old age → M ≥ 45 years, F ≥ 55 years)
o Retro sternal chest pain
o Squeezing type, heaviness, pressure/burning sensation
o Radiates to left shoulder or medial border of left arm (it can radiate
from jaw to umbilicus)
o Worsened by exertion and relieved by rest or taking nitroglycerine
(nitrates)
o Lasts for 2-5 minutes
o Levine sign +ve… pt make a fist and put his fist on chest to
characterize the smx
o Remark: nitroglycerine alleviate chest pain because of esophageal
spasm
➢ Wheezing…. Diffuse due to cardiac asthma

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Chapter 1; Heart failure (ልብ ድካም) and Other Cardiac Disorders

Preciptant factors

Remember with the mnemonics ‘‘HEART FAILES’’

➢ HTN
➢ Endocarditis (IE)
➢ Arrhythmia (manifest with new onset palpitation and Irregularly irregular
pulse)
➢ Recurrent rheumatic fever and myocarditis
➢ Thyrotoxicosis and pregnancy
➢ Fever (for infection)
➢ Anemia
➢ Infarction
➢ Lung infection (e.g. pneumonia)
➢ Embolism (PE, DVT)
➢ Stress (Dietary i.e. Salt intake, Drug withdrawal, Psychological stress,
physical stress)

Other Risk factors to be assessed in cardiac pt.


➢ Alcohol drinking, chat chewing, cigarette smoking (Smoking, Alcohol, chat
and DM fasten atherosclerotic before the age of 45 which may end up in
IHD and also RF for HTN)
➢ Family hx of sudden cardiac death → associated with HCMP (most
commonly in athletes) and MI
➢ Family hx of similar illness→ DCMP
➢ DM…associated with metabolic sxx (HTN, DM, Hyperlipidaemia, Central
obesity)

Complication of CHF

➢ Severe CHF→ progression of natural course of the diseases resulting in


death
➢ AKI→ resulting from pre renal azotemia (Cardio-renal syndrome)
➢ Cardio embolic stroke
➢ Pulmonary hypertension
➢ Cardiac cirrhosis → which may lead to all complication of cirrhosis like
Hepatic encephalopathy, esophageal varices and others
➢ Cardiac cachexia
➢ Endocarditis and Arrhythmia (atrial Fibrillation)
➢ ? Anemia of chronic illness (NEW NAME: Anemia of inflammation)
➢ Fluid and electrolyte disturbances
o Hypocalcemia, hypomagnesemia, hypokalemia, hyponatremia

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Sample history one

Sample hx of a pt’ from chilga with a DX of NYHA class IV, stage III CHF 2ry to
CRMVHD (MR, TR and AR) precipitated by CAP.

Chief compliant

SOB of three months duration

HPI

This patient was last relatively healthy 3 months back, at which time she started
to experience a gradual onset of dyspnea while doing ordinary activities like going
to church which progressively increase in severity and she began to experience
shortness of breath at rest within one month. Associated with orthopnea of 3
pillows, PND and Palpitation.

One month before admission, she started to experience a gradual onset of dry
cough which later becomes position dependent productive nocturnal cough with
whitish and frothy, non-foul smelling, Non blood tingled, sputum of 3-4 Arabic
coffee cup per day which is aggravated when she assumes supine position but no
chest pain or fever.

Concomitantly she also experienced bilateral, painless leg swelling which starts
from foot and goes upwards to involve the whole leg within 2 weeks duration. The
swelling disappears in the morning and marked on sitting position or prolonged
standing.

She has also significant weight loss from 40 kg to 35 kg within 3 months which is
12.5% of her initial body weight.

Two weeks before admission she experienced chest pain, fever, fast breathing and
worsening of cough for which she visited a local health center at chillga where
she was given augmentin 625 mg, PO,TID for 7 days and azithromycin 500mg,
po, daily for 3 days (hx from referral paper) but no improvement. Later she was
referred to our hospital for better investigation and mgt.

➢ No hx of Fever, reddish discoloration of urine(haematuria), dental


manipulation (tooth extraction), GI/GU manipulation, IV drug abuse or intra
cardiac device (IE)
➢ She doesn’t remember hx of sore throat, migratory joint pain, swelling over
joints, or abnormal body movement (Rheumatic fever)
➢ No hx of Anterior neck swelling, heat intolerance, profuse sweating, sleep
disturbance, palpitation, tremor or irritability (thyrotoxicosis)
➢ No Hx of chest pain or intermittent claudication (Atherosclerosis: MI or PAD)
➢ She was screened for RVI 6 months back and found to be NR (RVI is RF for
DCMP)
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➢ No hx of chronic cough, contact with chronic cougher or a known TB pt, no


hx of previous TB RX (TB is common cause of constrictive pericarditis and chest infection can
precipitate CHF)
➢ No hx of cigarette smoking, chronic alcohol intake or chewing chat (Smoking,
Alcohol, chat and DM fasten atherosclerotic before the age of 45 which may end up in IHD. And also, RF
for HTN)
➢ No hx of Drug intake (Common drugs like NSAID are also a risk factor for MI, Digoxin is risk
factor for Atrial fibrillation, Doxorubicin and Cocaine result in DCMP)
➢ No hx of easy fatigability, blurring of vision, light headedness, tinnitus or
vertigo.
➢ She usually eats injera made of ‘‘teff’’ and ‘‘machilla’’ and ‘’wott’’ made of
‘‘atter’’ and ‘‘dagusa’’ 3-4 times per day. Occasionally he/she eats meat
during holidays (salt is precipitant of CHF, Vitamin B1 deficiency/wet beriberi/ can result in DCMP,
Hemochromatosis also RF for DCMP)
➢ No hx of Flank pain, facial puffiness reduced urine output. (CKD… DDX for GBS,
Cardio renal Sxx)
➢ No hx of RUQ abdominal pain, yellowish discoloration of eyes, pale stool or
dark urine (CLD as DDX)
➢ No self or family hx of HTN, DM or asthma (RF)

Finally, she was admitted to our hospital carried on stretcher by her families

N.B these +ve and -ve statements may not be included in all
causes of CHF. So, modify based on your case

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Sample history two

Sample hx of a pt’ from koladiba with a DX of NYHA class IV stage C


CHF 2ry to RHD Preciptated by drug discontinuation

Chief compliant
Generalized body swelling and exacerbation of SOB of a week duration

HPI
This is a known cardiac pt for the past 5 years on enalapril to be taken 1
tablet twice per day and Lasix (furosemide) to be taken half tablet two times per
day, on salt free diet and recommended to decrease alcohol intake and to avoid
smoking. He was on follow up every month here in our hospital. He discontinued
his medication 4 months back due to financial problem.

A week before admission, he started to experience exacerbation of shortness of


breath at rest associated with orthopnea of 4 pillows, PND, Palpitation, easy
fatigability and generalized body swelling which starts from foot and goes upwards
to involve the leg, abdomen and finally the face within a week. He has also
unquantified but significant weight loss to the extent his closes become loose.

Associated with this he has also position dependent productive nocturnal cough of
whitish and frothy, non-foul smelling, Non blood tingled sputum of 1ACC/day which
is aggregated by lying supine position.

Two months back he developed dyspnea at sub-ordinary activities like going to


toilet, Orthopnea of two pillows, PND and position dependent dry cough. For this
he was admitted at UOGH for two weeks and discharged improved and appointed
with the above medications at cardiac clinic.

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Chapter 1; Heart failure (ልብ ድካም) and Other Cardiac Disorders

Physical examination (pertinent findings)

Readers are recommended to see CVS examination from short case of Nitsbin
(click here → 1.2 Cardiovascular System)

1 GA

✓ Patient may be Acute sick looking, chronic sick looking or acute sick
looking on chronic background depending on the underlying cause and
presence of complication
✓ May be in cardio-pulmonary distress (click and see 1.2 Cardiovascular System
examination)
✓ In mild or moderately severe HF, the patient appears to be in no distress
at rest except for feeling uncomfortable when lying flat for more than a few
minutes.
✓ In more severe HF, the patient must sit upright, may have labored
breathing, and may not be able to finish a sentence because of shortness
of breath.

2 Vital signs

✓ BP
o SBP may be normal or high in early HF, but it generally is reduced
in advanced HF because of severe LV dysfunction.
o The pulse pressure may be diminished, reflecting a reduction in
stroke volume.
o If there is HTN it may be a cause of CHF or 2ry HTN from CHF
o Remark: the presence of left sided S3 gallop may tell us long
standing HTN may be the cause of CHF.
o OHT → from Anemia, diuretics etc.
o Wide pulse pressure → AR, Anemia, thyrotoxicosis, pregnancy,
Aging
o Narrow pulse pressure → AS, Blood loss, cardiac tamponade.
✓ PR
Sinus tachycardia is a nonspecific sign caused by increased
o
adrenergic activity as a compensatory mechanism for low output
failure
o Tachycardia is minor criteria of Framingham criteria
o Week pulse → Shock, AS
o Irregularly irregular pulse → AF (precipitant or 2ry cause of CHF),
multifocal atrial tachycardia.
o Pulses alterans → Rare finding from Advanced CHF
✓ Temperature
o Febrile → Can be from IE, Pneumonia or other infections, Rheumatic
fever (rare in adults to present with rheumatic fever but common in
children)
o Hypothermia → low CO stat (Cardiogenic shock or sepsis)
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Chapter 1; Heart failure (ልብ ድካም) and Other Cardiac Disorders

✓ RR
o Cheyne-Stokes Respiration
▪ Also referred to as periodic respiration or cyclic respiration
▪ Present in 40% of patients with advanced HF and usually is
associated with low cardiac output.
▪ It is caused by an increased sensitivity of the respiratory
center to arterial Pco2 and a lengthy circulatory time.
▪ There is an apneic phase, during which arterial PO2 falls and
arterial PCO2 rises.
▪ These changes in the arterial blood gas content stimulate the
respiratory center, resulting in hyperventilation and hypocapnia,
followed by recurrence of apnea.

3 HEENT

✓ Facial puffiness → part of GBS


✓ Pale conjunctiva and pale buccal mucosa → anemia

4 LGS

✓ Thyroid enlargement → thyrotoxicosis is precipitant factor

5 RS

✓ Pulmonary crackles (rales or crepitations)


o Result from the transudation of fluid from the intravascular space into
the alveoli.
o In patients with pulmonary edema, rales may be heard widely over
both lung fields and may be accompanied by expiratory wheezing
(cardiac asthma).
o When present in patients without concomitant lung disease, rales are
specific for HF.
o Importantly, rales are frequently absent in patients with chronic HF,
even when LV filling pressures are elevated, because of increased
lymphatic drainage of alveolar fluid.
✓ Pleural effusions
o Result from the elevation of pleural capillary pressure and the
resulting transudation of fluid into the pleural cavities.
o Since the pleural veins drain into both the systemic and the
pulmonary veins, pleural effusions occur most commonly with
biventricular failure.
o Although pleural effusions are often bilateral in HF, when they are
unilateral, they occur more frequently in the right pleural space
✓ Consolidation → if there is pneumonia as precipitant (BBS).
✓ Friction rub → Sign of pericarditis (unlike to plural origin not associated with
respiratory cycle).

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Chapter 1; Heart failure (ልብ ድካም) and Other Cardiac Disorders

6 CVS

Arterial examination

✓ Arterial cording from atherosclerosis → best appreciated at radial arteries


✓ Bruit especially over the carotid → rare but high risk for stroke
✓ Pistol shot over femoral artery → AR

Venous examination

✓ Distended neck vein (engorged and pulsatile) → suggest RSHF, TR


✓ Raised JVP → suggest RSHF or biventricular failure
o JVP Normal ≤ 8 cm (3cm above the sternal angle) → by estimating
the height of the venous column of blood above the sternal angle in
centimeters and then adding 5 cm.
✓ +ve hepatojugular reflex
o In the early stages of HF, the venous pressure may be normal at
rest but may become abnormally elevated with sustained (~15s)
pressure on the abdomen (positive abdominojugular reflux).
o Remark: Hepatojugular reflex is important bedside test to differentiate
GBS from cardiac origin vs other causes like CLD.
Precordial examination

✓ Hyper active precordium → suggest cardiac muscle hypertrophy (e.g. LVH)


✓ Silent precordium → IHD, DCMP, morbid obesity, obstructive lung disease
✓ Precordial bulge → rare but it can suggest long standing CHD (N.B. PDA,
ASD… can reach up to adulthood)
✓ Cardiomegaly and ventricular hypertrophy features
o Displaced PMI
▪ PMI usually is displaced below the 5th ICS and/or lateral to
the MCL
▪ Notice; in most causes of Cardiomegaly (e.g. VHD), there is
displaced PMI with active precordium unlike cardiomegaly from
DCMP, which result displaced PMI with silent precordium
o Heave (suggests hypertrophy) and thrill (suggests grade IV murmur)
▪ Patients with RVH may have a sustained and prolonged left
parasternal impulse (heave) extending throughout systole
▪ Heave over the apex suggests LVH
o Sustained diffuse and thrusting PMI, Displaced AI, active precordium
▪ Severe LV hypertrophy leads to a sustained PMI
✓ Murmur of MR and TR frequently present in patients with advanced HF
✓ S3 gallop in some patients and palpable at the apex
o An S3 (or proto diastolic gallop) is most commonly present in
patients with volume overload who have tachycardia and tachypnea,
and it often signifies severe hemodynamic compromise
✓ S4 is not a specific indicator of HF but is usually present in patients with
diastolic dysfunction

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Chapter 1; Heart failure (ልብ ድካም) and Other Cardiac Disorders

7 Abdominal examination

✓ Hepatomegaly
o It is an important sign in patients with HF. which is tender, smooth
and with blunted edge from cardiac congestion of liver
o May pulsate during systole if TR is present.
✓ Ascites → a late sign, occurs as a consequence of increased pressure in
the hepatic veins and the veins draining the peritoneum.
✓ Jaundice → also a late finding in HF, results from impairment of hepatic
function secondary to hepatic congestion and hepatocellular hypoxemia and
is associated with elevations of both direct and indirect bilirubin.
o Remark: severe hemolysis also results in jaundice: severe anemia
may be a cause or precipitant of HF
✓ Rarely tipped splenomegaly from IE

8 GUS

9 MSS

✓ Peripheral pitting edema


o It is a cardinal manifestation of HF, but it is nonspecific and usually
is absent in patients who have been treated adequately with
diuretics.
o It is usually symmetric and dependent in HF and
o Occurs predominantly in the ankles and the pretibial region in
ambulatory patients.
o In bedridden patients, edema may be found in the sacral area
(presacral edema) and the scrotum.
o Long-standing edema may be associated with indurated and
pigmented skin (Stasis dermatitis) .
10 IS

✓ Pallor → Anemia
✓ Cyanosis and cold extremities → suggest decreased CO
o Peripheral vasoconstriction leading to cool peripheral extremities and
cyanosis of the lips and nail beds is caused by excessive adrenergic
activity.
NB: Look for skin manifestation of IE

11 NS

✓ Hemiparesis / hemiplegia 2ry to Cardio embolic stroke

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Chapter 1; Heart failure (ልብ ድካም) and Other Cardiac Disorders

DDX
For Dyspnea (SOB)* For GBS#
1. CHF 2ry to (see table about ‘’etiologies of HF’’ from the 1. CHF → symmetrical and
discussion part below) worsens in the evening and
a. RHD improves early in the
N.B VHD can result from RVHD,
b. HHD morning
IE or DVHD (for old age)
c. VHD 2. Constrictive pericarditis
d. IHD (usually isolated ascites)
e. CMP 3. CKD
f. Constrictive pericarditis (Pericardial disease) 4. Nephrotic syndrome → affects
g. CHD face first
h. Arrhythmia 5. CLD
i. IE 6. Advanced Lymphoma (NHL)
j. Severe anemia 7. Disseminated TB or SLE to
k. Thyrotoxicosis pericardium (result in
2. Pulmonary TB Constrictive pericarditis),
3. Bronchial Asthma (severe persistent Asthma) pleura, Peritoneum…
4. Cor pulmonale 8. Varicose veins and DVT →
a. COPD More of peripheral edema
b. Bronchiectasis 9. Vasodilating drugs (e.g. CCB’s)
c. Lung Abscess 10. ? Protein losing enteropathy
d. ILD
5. Lung ca
* In most patients who present with classic signs and symptoms of HF, the diagnosis is relatively
straightforward. However, even experienced clinicians have difficulty differentiating the dyspnea that
arises from cardiac and pulmonary causes. In this regard, Echo, CXR, biomarkers, pulmonary function
testing, may be useful.
* When HF develops in patients with a preserved EF, it may be difficult to determine the relative
contribution of HF to the dyspnea that occurs in chronic lung disease and/or obesity.

#
Ankle edema may arise secondary to varicose veins, obesity, renal disease, or gravitational effects.
Remark: If all workup for causes of ankle edema are normal consider idiopathic edema.

Ass’t example
NYHA class IV, stage C, CHF 2ry to CRMVHD (MR,
TR, AR) precipitated by CAP

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Chapter 1; Heart failure (ልብ ድካም) and Other Cardiac Disorders

IX

1. Routine Laboratory Testing


o Patients with new-onset HF and those with chronic HF and acute
decompensation should have;
▪ CBC → anemia of Chronic illness or NcNc (Normo cystic
normo chromic) Anemia of IE, leukocytosis suggests infection
such as pneumonia but non-specific, leukocytosis is also minor
criteria of Jones
▪ Electrolytes → Sodium, potassium and calcium: derangement
may lead to arrhythmia. Should be done if diuretics are going
to be started.
▪ BUN and serum creatinine → important for diuretics Mgt, cardio
renal Sxx (elevated BUN/creatinine ratio), complication of
IE(AGN)
▪ Hepatic enzymes → May be elevated: Liver congestion
▪ Urinalysis → hematuria from IE
▪ Urine HCG for all women of child bearing age → pregnancy
may be precipitant, peripartal cardiomyopathy
▪ PICT
o Selected patients should have;
▪ FBS or OGTT → for diabetes mellitus assessment
▪ Lipid profile → for dyslipidemia assessment
▪ TSH, if TSH is abnormal T3 and T4 → done if indicated (e.g
Thyroid enlargement on palpation, if there is Thyrotoxicosis
smx). Elevated T3 & T4 with decreased TSH support
Thyrotoxicosis as precipitant or a cause of high output HF.
▪ Remark: Hypothyroidism may result in pericardial effusion.
2. Echo → can show us
o A semiquantitative assessment of LV size and function
o The presence or absence of valvular and/or regional wall motion
abnormalities (indicative of a prior MI)
o The presence of left atrial dilation and LVH, together with
abnormalities of LV diastolic filling provided by pulse-wave and tissue
Doppler, is useful for the assessment of HFpEF
o Assessing RV size and pulmonary pressures, which are critical in the
evaluation and management of cor pulmonale (click here → Chapter 2;
Chronic lung disorders)
o Vegetation
o Valve abnormality in general (stenotic/regurgitant,thickening/calcification)
o Thrombus → common in left Auricle and mostly Associated with Atrial
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Chapter 1; Heart failure (ልብ ድካም) and Other Cardiac Disorders

o Septal Defect → ASD, VSD, PDA


o Chamber size and wall hypertrophy → e.g. large chamber size in
DCMP, septal and wall Hypertrophy in HCMP
𝑺𝑽
o EF (Ejection Fraction) = 𝑬𝑫𝑽
𝑥 100 % = 50 − 60 %
☛ EF will be low (<30 - 40%) in Heart failure with reduced
ejection fraction (HFrEF) and normal (≥50%) in Heart failure
with preserved ejection fraction (HFpEF)
☛ The most useful index of LV function is the EF.
☛ Because the EF is easy to measure by noninvasive testing
and easy to conceptualize, it has gained wide acceptance
among clinicians.
☛ Unfortunately, the EF has a number of limitations as a true
measure of contractility, since it is influenced by alterations in
afterload and/or preload.
☛ Nonetheless, with the exceptions indicated above, when the
EF is normal (≥50%), systolic function is usually adequate,
and when the EF is significantly depressed (<30 - 40%),
contractility is usually depressed
o Movement (kinesis) of the wall
o Minimal pericardial fluid in acute rheumatic fever
3. CXR → can show us
o Cardiomegaly i.e. Cardiothoracic ratio > 50%
o To assess the state of the pulmonary vasculature, and may identify
noncardiac causes of the patient’s symptoms.
▪ Pulmonary edema → bat wing appearance, cephalization
(Diversion of Blood vessel circulation towards the Apex), Kerl B
lines
▪ Although patients with acute HF have evidence of pulmonary
hypertension, interstitial edema, and/or pulmonary edema, the
majority of patients with chronic HF do not.
o Consolidation → consider Pneumonia as precipitant
o Pleural effusion → obliterated costophrenic angle, meniscus sign +ve
4. ECG → The major importance of the ECG is
▪ To assess cardiac rhythm abnormality such as AF (Atrial
Fibrillation)
▪ To determine the presence of LVH and/or RVH
▪ To assess presence of a prior MI (presence or absence of Q-
waves)
• STEMI/NSTEMI (ST elevation or Non-ST elevation MI)
▪ Prolonged PR interval in RHD
▪ A normal ECG virtually excludes LV systolic dysfunction.
▪ To determine QRS width to ascertain whether the patient may
benefit from resynchronization therapy (not available in our
setup).
5. APR (acute phase reactants) → ESR commonly done in our setup
o Elevated ESR & CRP are also suggestive of infection such as
pneumonia but non-specific
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Chapter 1; Heart failure (ልብ ድካም) and Other Cardiac Disorders

o ESR and CRP elevation are minor criteria of Jones.


6. Cardiac Biomarkers → troponin and CK are available in most private setups
of Ethiopia rather than government hospitals (for normal laboratory reference
values click here → Chapter 27; Reference Intervals for Laboratory Tests)
o Elevated troponin T, I; More specific.
o CKmb also elevated: Important for re-infraction assessment.
o BNP used for prognosis and follow up
▪ Both B-type natriuretic peptide (BNP) and N-terminal pro-BNP
(NT-proBNP), which are released from the failing heart, are
relatively sensitive markers for the presence of HF with
depressed EF
▪ They also are elevated in HF patients with a preserved EF,
albeit to a lesser degree
▪ Moreover, the measurement of BNP or NT-proBNP is useful for
establishing prognosis or disease severity in chronic HF and
can be useful to achieve optimal dosing of medical therapy in
select clinically euvolemic patients
▪ However, it is important to recognize that natriuretic peptide
levels;
• Increase with age and renal impairment
• More elevated in women
• Can be elevated in right HF from any cause.
• Can be falsely low in obese patients.
7. Blood culture → for IE (S.viridans, S. fecalis, S. Aureus, HACEK)
8. ASO titre and DNAse → supportive evidence for ARF (common in children)
9. Cardiac MRI (usually not done in our setup)
o MRI provides a comprehensive analysis of cardiac anatomy and
function and is now the gold standard for assessing LV mass and
volumes.
o MRI also is emerging as a useful and accurate imaging modality for
evaluating patients with HF, both in terms of assessing LV structure
and for determining the cause of HF (e.g., amyloidosis, ischemic
cardiomyopathy, and hemochromatosis).
10. Exercise Testing (not applicable in our setup)
o Treadmill or bicycle exercise testing is not routinely advocated for
patients with HF, but either is useful for assessing the need for
cardiac transplantation in patients with advanced HF.
o A peak oxygen uptake (VO2) <14 mL/kg/min is associated with a
relatively poor prognosis.
▪ Patients with a VO2 <14 mL/kg/min have been shown, in
general, to have better survival when transplanted than when
treated medically.
➢ Remark: For those who have indication for exercise ECG, link to advanced
medical center.

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Discussion

Before going to the details of discussion of HF, you have to know


➢ Framingham diagnostic criteria of HF
➢ NYHA functional classification of HF
➢ Stages of HF
➢ JONES criteria for Acute Rheumatic Fever(ARF) & Rheumatic heart disease
(RHD) and
➢ Modified Dukes criteria for Infective endocarditis (IE).(click the links written in
blue to refer under respective topics below)

1.1 Heart Failure/HF/


HF is a complex clinical syndrome that results from structural or functional
impairment of ventricular filling or ejection of blood, which in turn leads to the
cardinal clinical symptoms of dyspnea and fatigue and signs of HF, namely
edema and rales.
Because many patients present without signs or symptoms of volume overload,
the term “heart failure” is preferred over the older term “congestive heart
failure.”
Heart Failure also defined as an abnormality of cardiac structure or function
leading to failure of the cardiac output to meet the body's metabolic
requirements despite normal filling pressures.
It represents an end stage of a number of different diseases.
Identification of the underlying cause of the Heart Failure is central to diagnosis.
It could result from VHD, IHD, HTN, CMP, thyrotoxicosis, CHD, etc.

Epidemiology
The overall prevalence of HF in the adult population in developed countries is
2%.
HF prevalence follows an exponential pattern, rising with age, and affects 6 -
10% of people aged >65.
Although the relative incidence of HF is lower in women than in men, women
constitute at least one-half the cases of HF because of their longer life
expectancy.
The overall prevalence of HF is thought to be increasing, in part because
current therapies for cardiac disorders, such as MI, VHD, and arrhythmias, are
allowing patients to survive longer.
The prevalence of HF in emerging nations is uncertain because of the lack of
population-based studies in those countries.
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Forms of CHF

➢ HF was once thought to arise primarily in the setting of a depressed left


ventricular (LV) ejection fraction (EF); however, epidemiologic studies have
shown that approximately one-half of patients who develop HF have a normal
or preserved EF (EF ≥ 50%).
➢ Accordingly, the historical terms “systolic” and “diastolic” HF have been
abandoned, and HF patients are now broadly categorized into HF with a
reduced EF (HFrEF; EF < 30 - 40%, formerly systolic failure) or HF with a
preserved EF (HFpEF; EF ≥ 50%, formerly diastolic failure).
➢ Patients with a LVEF between 40 and 50% have been considered as having
a borderline or mid-range EF.

1. HFrEF vs HFpEF
➢ See the notes above and table below (etiologies of heart failure)
2. Right sided versus left sided:

✓left sided failure: dyspnea, ✓right sided failure: peripheral edema,


orthopnea, PND hepatomegaly, ascites
NB.
➢Right sided failure usually results from left sided failure.
➢isolated right sided failure which results from pulmonary hypertension is called
cor pulmonale
3. High output vs low output failure:
high output: thyrotoxicosis, anemia, low output: IHD, DCMP, RCMP
AR
4. Acute vs chronic failure
acute: chronic:
❖ extensive MI, rupture of valves, ❖ DCMP, VHD
myocarditis, massive PE ❖ BP is usually maintained, edema
❖ predominantly systolic abnormality is common
❖ pulmonary edema or hypotension
(cardiogenic shock) without
peripheral edema

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Difference between heart failure (HF) and congestive heart failure (CHF)

HF CHF
✓ Dyspnea, orthopnea, PND, weakness and ✓ Dyspnea, orthopnea and PND together with
decreased exercise tolerance peripheral edema, hepatomegaly, ascites
✓HF symptoms without sign and smx of ✓ HF symptoms together with sign and smx
congestion of congestion
☛ NO Sign of congested heart failure ☛ +ve Signs of congested heart failure
✓There is Murmur of Valvular lesions → refer CVS examination of Nitsbin (click
here → 1.2 Cardiovascular System)
✓ There is Murmur of Valvular lesions

Etiology of heart failure (see table below)

Any condition that leads to an alteration in LV structure or function can


predispose a patient to developing HF.
Although the etiology of HF in patients with a preserved EF differs from that of
patients with depressed EF, there is considerable overlap between the
etiologies of these two conditions.
Rheumatic heart disease remains a major cause of HF in Africa (including our
country Ethiopia) and Asia, especially in the young
Hypertension is an important cause of HF in the African and African-American
populations.
In industrialized countries, coronary artery disease (CAD) has become the
predominant cause in men and women and is responsible for 60 - 75% of
cases of HF.
Hypertension contributes to the development of HF in 75% of patients,
including most patients with CAD.
Both CAD and hypertension interact to augment the risk of HF, as does
diabetes mellitus.
In 20 - 30% of the cases of HF with a depressed EF, the exact etiologic
basis is not known These patients are referred to as having nonischemic,
dilated, or idiopathic cardiomyopathy.

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Table; Etiologies of Heart Failure


Depressed or reduced Ejection Fraction (<30 - Preserved Ejection Fraction (≥ 50%) /HFpEF/
40%)/HFrEF/
➢ Coronary artery disease ➢ Pathologic hypertrophy
o Myocardial infarction a o Primary (HCM)
o Myocardial ischemia a
o Secondary (hypertension)
➢ Chronic pressure overload ➢ Restrictive cardiomyopathy
o Hypertension a o Infiltrative disorders (amyloidosis,
o Obstructive valvular disease (e.g. MS, AS) a
sarcoidosis)
➢ Chronic volume overload o Storage diseases (hemochromatosis)
o Regurgitant valvular disease (e.g. MR. TR) ➢ Aging
o Intracardiac (left-to-right) shunting ➢ Endomyocardial disorders
o Extracardiac shunting ➢ Fibrosis
➢ Chronic lung disease
o Cor pulmonale
o Pulmonary vascular disorders (e.g. Pulmonary High-Output States
arterial HTN) ➢ Metabolic disorders
➢ Nonischemic dilated cardiomyopathy o Thyrotoxicosis
o Familial/genetic disorders ➢ Excessive blood flow requirements
o Infiltrative disorders a o Systemic arteriovenous shunting
➢ Disorders of rate and rhythm o Chronic anemia
o Chronic bradyarrhythmia’s ➢ Nutritional disorders (beriberi)
o Chronic tachyarrhythmias o Selenium or thiamine deficiency
➢ Toxic/drug-induced damage
o Metabolic disorder a
o Viral
➢ Chagas’ disease (only in America)
a
Indicates conditions that can also lead to heart failure with a preserved ejection fraction.

Diagnosis of HF (see IX from the approach section above)

The diagnosis of HF is relatively straightforward when the patient presents


with classic signs and symptoms of HF; however, the signs and symptoms
of HF are neither specific nor sensitive.
Accordingly, the key to making the diagnosis is to have a high index of
suspicion, particularly for high-risk patients.
When these patients present with signs or symptoms of HF, additional
laboratory testing should be performed.
SO, Diagnosis of heart failure is clinical. But investigations are necessary to
identify the underlying cause, precipitating factor, and to guide and monitor
management.

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To identify the underlying cause: Echocardiography, ECG, CXR


To identify precipitating factors based on clinical evaluation (in addition to the above
investigations): CBC, ESR, U/A, blood culture, TFTs, Urine HCG, Cr, BUN, etc..

To guide and monitor management: K+, Na+, Cr, BUN, ALT, AST, serum albumin.

Modified Framingham’s criteria for diagnosis of CHF

❖ Diagnosis requires 2 major or 1 major and 2 minor criteria not attributed to


other medical conditions
Major criteria Minor criteria
1. PND 1) Bilateral leg edema
2. Orthopnea 2) Nocturnal cough
3. Elevated JVP 3) Dyspnea on ordinary exertion
4. S3 gallop 4) Hepatomegaly
5. Pulmonary rales, Pulmonary 5) Pleural effusion
edema on CXR 6) Tachycardia (HR ≥ 120 bpm)
6. Cardiomegaly on CXR 7) Weight loss ≥ 4.5 kg 4.5 kg in
7. Weight loss ≥ 4.5 kg in five days five days
in response to treatment of
presumed CHF

NYHA (New York Heart Association) Classification of Severity


/Functional Capacity
Class I Patients with cardiac disease but without resulting limitation of physical activity.
Ordinary physical activity does not cause undue fatigue, palpitations, dyspnea, or
anginal pain.
Class II Patients with cardiac disease resulting in slight limitation of physical activity. They
are comfortable at rest. Ordinary physical activity results in fatigue, palpitation,
dyspnea, or anginal pain.
Class III Patients with cardiac disease resulting in marked limitation of physical activity. They
are comfortable at rest. Less than ordinary activity causes fatigue, palpitation,
dyspnea, or angina.
Class IV Patients with cardiac disease resulting in inability to carry on any physical activity
without discomfort. Symptoms of heart failure or the anginal syndrome may be
present even at rest. If any physical activity is undertaken, discomfort is increased.
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Stages of Heart Failure (WHO/AHA)


Stage A High risk for HF (like pt with DM, HTN, Dyslipidemia…), without structural
heart disease or symptoms
Stage B Structural Heart disease with asymptomatic left ventricular dysfunction
Stage C Structural heart disease with Prior or current symptoms of HF
Stage D Advanced heart disease and severely symptomatic or refractory HF
requiring intervention (Valvular surgery, cardiac transplant)

Pathogenesis of heart failure

FIGURE 252-1 (Harrison 20th edition) Pathogenesis of heart failure with a depressed ejection
fraction. Heart failure begins after an index event produces an initial decline in the heart’s
pumping capacity. After this initial decline in pumping capacity, a variety of compensatory
mechanisms are activated, including the adrenergic nervous system, the renin-angiotensin-
aldosterone system, and the cytokine system. In the short term, these systems are able to
restore cardiovascular function to a normal homeostatic range with the result that the
patient remains asymptomatic. However, sustained activation of these systems leads to
secondary end-organ damage within the ventricle, with worsening left ventricular remodeling
and subsequent cardiac decompensation.

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FIGURE 252-2 Activation of neurohormonal systems in heart failure. The decreased


cardiac output in heart failure (HF) patients results in an “unloading” of high-pressure
baroreceptors (circles) in the left ventricle, carotid sinus, and aortic arch. This unloading of
the peripheral baroreceptors leads to a loss of inhibitory parasympathetic tone to the
central nervous system (CNS), with a resultant generalized increase in efferent sympathetic
tone, and non-osmotic release of arginine vasopressin (AVP) from the pituitary. AVP (or
antidiuretic hormone [ADH]) is a powerful vasoconstrictor that increases the permeability of
the renal collecting ducts, leading to the reabsorption of free water. These afferent signals
to the CNS also activate efferent sympathetic nervous system pathways that innervate the
heart, kidney, peripheral vasculature, and skeletal muscles. Sympathetic stimulation of the
kidney leads to the release of renin, with a resultant increase in the circulating levels of
angiotensin II and aldosterone. The activation of the renin-angiotensin-aldosterone system
promotes salt and water retention and leads to vasoconstriction of the peripheral
vasculature, myocyte hypertrophy, myocyte cell death, and myocardial fibrosis. Although
these neurohormonal mechanisms facilitate short term adaptation by maintaining blood
pressure, these same neurohormonal mechanisms result in end-organ changes in the heart
and the circulation, as well as to the excessive salt and water retention in advanced HF.

Clinical manifestations of heart failure; see the approach part

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1.1.1 Management of heart failure


Management should be instituted early in parallel with the diagnostic
work up.
Distinctive phenotypes of presentation with diverse management targets
exemplify the extensive syndrome of heart failure. These include;
o Chronic heart failure with reduced ejection fraction (HFrEF)
o Heart failure with preserved ejection fraction (HFpEF),
o Acute decompensated heart failure (ADHF), and
o Advanced heart failure.
Chronic heart failure with reduced ejection fraction (HFrEF)
o Early management evolved from symptom control to disease-
modifying therapy in HFrEF with the advent of;
▪ RAAS directed therapy
▪ Beta receptor antagonists
▪ Mineralocorticoid receptor antagonists
▪ Cardiac resynchronization therapy and
▪ Implantable cardio-defibrillators.
o The treatment of symptomatic heart failure that evolved from a reno
centric (diuretics) and hemodynamic therapy model (digoxin, inotropic
therapy) ushered in the era of disease-modifying therapy with
neurohormonal antagonism.
o In this regard, RAAS blockers and beta blockers form the
cornerstone of pharmacotherapy and lead to attenuation of decline
and improvement in cardiac structure and function with consequent
reduction in symptoms, improvement in Quality of life, decreased
burden of hospitalizations, and a decline in mortality from both pump
failure and arrhythmic deaths
However, similar advances have been elusive in the syndromes of HFpEF
and ADHF, which have remained devoid of convincing therapeutic advances
to alter their natural history.
Heart failure with preserved ejection fraction (HFpEF)
o Therapeutic targets in HFpEF include;
▪ Control of congestion
▪ Stabilization of heart rate and blood pressure and
▪ Efforts at improving exercise tolerance.
o Lowering blood pressure alleviates symptoms more effectively than
targeted therapy with specific agents.
o Addressing surrogate targets, such as regression of ventricular
hypertrophy in HHD, and use of lusitropic agents, such as CCB and
beta receptor antagonists, have been disappointing.
Acute decompensated heart failure (ADHF)
o ADHF is a heterogeneous clinical syndrome most often resulting in
need for hospitalization due to confluence of interrelated
abnormalities of decreased cardiac performance, renal dysfunction,
and alterations in vascular compliance.
o The first principle of management of these patients is to identify and
tackle known precipitants of decompensation.
▪ Identification and management of medication nonadherence
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▪ cold and flu preparations with cardiac stimulants


▪ Active infection and overt or covert pulmonary
thromboembolism should be sought, identified, and treated.
▪ When possible, arrhythmias should be corrected by controlling
heart rate or restoring sinus rhythm in patients with poorly
tolerated rapid atrial fibrillation and by correcting ongoing
ischemia with coronary revascularization or by correcting
offenders such as ongoing bleeding in demand-related
ischemia.
o A parallel step in management involves stabilization of
hemodynamics in those with instability.
o Cardiogenic pulmonary edema is most often a result of acute
decompensated heart failure (ADHF)
o If patient has pulmonary edema or cardiogenic shock, see the respective
sections for initial management approach (click here → Acute HF
(Cardiogenic shock and Pulmonary edema )
In advanced heart failure
o A stage of disease typically encountered in HFrEF, the patient
remains markedly symptomatic with demonstrated refractoriness or
inability to tolerate full-dose neurohormonal antagonism, often
requires escalating doses of diuretics,
and exhibits persistent hyponatremia and renal insufficiency with
frequent episodes of heart failure decompensation requiring recurrent
hospitalizations. Such individuals are at the highest risk of sudden or
progressive pump failure related deaths.
o In contrast, early-stage asymptomatic left ventricular dysfunction is
amenable to preventive care, and its natural history is modifiable by
neurohormonal antagonism.

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Principle of HF management

1. General measures
2. Treating congestion (Diuretics)
3. Correcting the precipitant factor
4. Treatment of underlying cause
5. Increase myocardial contractility
6. Prevent disease progression (Cardiac remodeling)
7. Follow up

1. General measures
• Bed rest
• Elevate bed to Semi-upright position
• Salt restriction (< 2gm or decrease added salt)
• Fluid restriction (< 1.5 - 2 L/day) for hyponatremic patients
• Administer O2 if SaO2 < 90%.
• Activity and life style modifications:
✓ Small and frequent meals
✓ Restrictions on activities within the context of the specific
diagnosis & the patient's ability.
➢ Competitive & strenuous sports activities are usually
contraindicated
➢ Reduce anxiety and emotional stress
✓ Weight loss for obese patients
✓ Cessation of smoking
✓ Avoid other CVD risk factors

2. Treating congestion (Diuretics)

✓ Send sample for Cr, BUN, K+ and Na+ initially and proceed with diuresis.
✓ For diuretic naive patients start furosemide 20 - 40 mg IV (if BP>90/60
mmHg) and double the dose every 2 - 4 hour until the urine output is >1
ml/kg/hr (40-70ml/hr) [max. 400-600mg/day or 200mg per dose].
➢ Response to IV dose occurs 2-4 hours later.
➢ For those already on oral furosemide, start with equal dose of IV
furosemide.
➢ Maintain the dose of furosemide which gave adequate response on
a TID basis.
✓ Start spironolactone 25 - 50 mg/day unless K+ > 5.0 meq/l or Cr > 1.6
mg/dl or GFR<30 ml/min (main reason of adding spironolactone is to
prevent hypokalemia due to furosemide).
➢ Initial dose is 25 mg po per day increased up to 100 mg BID
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➢ Since hyperkalemia is a life-threatening side effect of spironolactone


it is contraindicated in patients with renal failure (k+ >5 mmol/l or
>2.5 mg/dl of CRr)
➢ Remark: In advanced HF spironolactone dose ≥ 50mg have been
found to be necessary to produce natriuresis. Studies shows with the
dose of (50-200mg) there was no significant increase in mean serum
Cr or K+. However close monitoring is warranted.
➢ Spironolactone is aldosterone antagonist (mineralocorticoid receptor
antagonist), potassium sparing diuretics

Goal of diuresis Signs of excess diuresis

➢ Negative fluid balance ➢ Signs of dehydration


➢ Weight loss (0.5-1kg/day) ➢ Hypotension(overt/orthostatic)
➢ Clearance of crepitations in the lungs ➢ Elevated RFTs despite improvement of congestion
➢ Decrement in edema, hepatomegaly, JVP ➢ Severe hypokalemia
➢ Improvement of dyspnea, orthopnea
➢ Improvement in renal function (Cr, BUN)

Patient not responding

✓ Make sure that


o Patient is taking medications as prescribed and is on salt free diet.
o Precipitating factors is managed.
o Patient is not taking drugs like NSAIDS, CCBs, BBs.

NB: Patients with deranged renal function and hypoalbuminemia require higher
doses of diuretics from the outset.

✓ Adjust the diuresis.


o Increase the dose of furosemide (max. 400 - 600mg/day) and
increase spironolactone to 50-100mg/day.
o Increase the frequency of administration of furosemide 4-6 x per day.
Repeated IV bolus doses are recommended than continuous infusion.
o Remark: there is no difference between continuous infusion and
frequent bolus of furosemide for all-cause mortality, length of hospital
stay and electrolyte disturbance, but continuous infusion is superior
with regard to diuretic effect and reduction in BNP.
o For those patients with borderline BP continuous infusion may be
preferred to avoid BP fluctuation with every bolus does of
furosemide.
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o In ICU; furosemide Continuous IV infusion by perfuser: Initial: IV


bolus dose 40 to 100 mg over 1 to 2 minutes, followed by
continuous IV infusion rate of 10 to 40 mg/hour; repeat loading dose
before increasing infusion rate
o Remark: in the absence of perfuser, we can add 200mg of Lasix in
1000ml NS then we can give in a drip with calculated rate.
o If patient not responding with the above approaches, add thiazides:
hydrochlorothiazide, chlorothiazide
➢ Hydrochlorothiazide Initial: 25 mg, PO, daily or BID in the
morning 30 minutes before frusemide administration; maximum
daily dose: 200 mg
➢ Thiazides are weaker diuretic agents useful in mild CHF alone
or used in combination with loop diuretics in CHF which
doesn't respond to high dose lasix
For patients with hypertension and severe Acute MR intravenous nitroglycerin
infusion can be considered in addition to diuretics. (click and see 1.10.2
Pulmonary edema section)
o IV nitroglycerin for Acute decompensated heart failure :Initial: 10 to
20 µg/minute, with subsequent titration (e.g. 10 to 20 µg/minute
every 5 to 15 minutes) up to 200 µg/minute or 0.3 to 0.5
µg/kg/minute with titration (if SBP ≥90 mm Hg) in increments of 20
µg/minute every 1 to 3 minutes up to 400 µg/minute. Patients who
do not respond hemodynamically with doses of ~200 µg/minute
should be considered non-responders.

Remark: Always asses for salt restriction.

Patient improving
❖ Decrease the dose of diuretics every day depending on patient condition.
o Goal is to use the lowest possible dose and frequency to keep
patient dry.
❖ Change IV furosemide to PO and observe the patient with ambulation for a
day or two.
❖ Remark: since PO absorption rate of Lasix is poor, use conversion rate IV
to PO Lasix at 1:2 (20mg IV = 40mg PO).
o Patients requiring higher dose of furosemide may require a double
dose.

3. Correcting the precipitant factor

✓ Manage the identified precipitating factors.

1
4. Treatment of underlying cause 1
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Institute further management for the underlying heart disease (see specific
topic and comorbidities below)

5. Increase myocardial contractility

❖ Digoxin, for class C or D HFrEF, 0.125 - 0.25 mg, PO, daily for positive
inotropy and rate control in patients with atrial fibrillation.
➢ Effects: - Positive inotropic effect (increase myocardial contractility),
increased automaticity (arrythmia), delays AV node conduction
➢ Uses: - In heart failure with reduced EF not responding to diuretic
therapy, particularly when atrial fibrillation co exists with CHF
➢ Toxicity of digoxin:
▪ Early noncardiac: anorexia, nausea, vomiting
▪ Chronic toxicity: weight loss, neuralgia, worsening of CHF,
intractable vomiting
➢ Treatment of toxicity:
▪ Discontinue digoxin
▪ Treat the arrhythmia
▪ Supplement potassium if hypokalemic
▪ Anti-digoxin antibodies

6. Prevent disease progression (Cardiac remodeling)

ACEI, ARBs, Beta-blockers and Aldosterone antagonists have survival


benefits and anti-remodeling
o Remark: Compared to ARBs, ACEI were deemed more effective in
decreasing the incidence of MI and all-cause mortality in patient with
HFrEF.
If patients were already talking ACEIs and BBs (Beta blockers), they can
continue to take them during hospitalization as long as they are not
severely congested, are hemodynamically stable and have normal renal
function.
Temporary discontinuation or dose reduction of BB may be necessary if BP
is low or borderline and patient is severely congested (pulmonary edema).
o Remark: Sudden discontinuation of BBs is deleterious, if patient
admitted for acute decompensated chronic HF while on BBs in the
absence of contraindication (for CLASS II CHF reduce the dose of
BBs by 25%, for CLASS III by 50% and for CLASS IV CHF by
75%).
Temporary discontinuation or dose reduction of ACEIs/ARBs may be
necessary if BP is low or borderline and recent renal function derangement.
For patients in whom previous BB and ACEIs/ARBs have been discontinued
consider reinitiating the drugs as soon as possible sequentially
(ACEIs/ARBs followed by B blockers)
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Note: Initiate Beta blockers, only in stable patients or hospitalized patients


after volume status has been optimized and IV diuretics, vasodilators, and
inotropic agents have all been successfully discontinued. Caution should be
used when initiating in patients who required inotropes during their hospital
course. Increase dose gradually and monitor for congestive signs and
symptoms of HF making every effort to achieve target dose shown to be
effective
Remark: congestion symptoms may worsen within 1-2 weeks of BBs
initiation (surge of counter regulatory hormones / stress hormones).
For HFrEF previously not taking ACEIs/ARBs or BB.
o Start one of the ACEIs/ARBs as soon as BP and RFTs permit and
escalate until discharge
o Start one of the BB following ACEIs/ARBs when BP and PR permit
and escalate until discharge
o Start Spironolactone 25mg/d. (low EF despite maximum dose of the
above two drugs)

Dose of drugs having cardiac anti-remodeling effect

ACEI
o Enalapril 2.5 mg, PO, BID, titrated as tolerated to target dose of 10
mg, PO, BID (maximum: 20 mg/day).
Alternative;
o Lisinopril 2.5 to 5 mg, PO, daily; increase by no more than 10 mg
increments at intervals no less than 2 weeks to the highest tolerated
dose (maximum: 40 mg/day)
ARBs
o Candesartan 4 mg, PO, daily or alternatively 4 to 8 mg, PO, daily;
double the dose at 2-week intervals, as tolerated; target dose: 32
mg once daily
Alternative;
o Valsartan 40 mg, PO BID; titrate dose to 80 mg, and then to 160
mg BID, as tolerated; maximum dose: 320 mg/day.
Beta- blockers
o Metoprolol; Metoprolol tartrate is short acting form, which is
preferred as initial management (especially in pt’s with ACS).
Metoprolol succinate is long acting form
▪ Remark: Metoprolol succinate is superior treatment option
compared to Metoprolol tartrate in treatment of HTN, CHF and
Coronary heart disease.
▪ Metoprolol tartrate (Immediate release): 50 mg, PO, BID;
usual dosage range: 50 to 200 mg, PO, BID; may increase
dose at weekly intervals to desired effect (maximum: 400
mg/day).
▪ Metoprolol succinate (Extended release): 12.5 to 25 mg once
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daily; may double dosage every 2 weeks as tolerated up to


target dose of 200 mg/day.
o Carvedilol
▪ Immediate release; 3.125 mg, PO, BID for 2 weeks; if this
dose is tolerated, may increase to 6.25 mg PO, BID. Double
the dose every 2 weeks to the highest dose tolerated by
patient (maximum 25mg)
▪ Extended release: 10 mg, PO, daily for 2 weeks; if the dose
is tolerated, increase dose to 20 mg, 40 mg, and 80 mg over
successive intervals of at least 2 weeks. Maintain on lower
dose if higher dose is not tolerated (maximum; 80 mg, daily)
o Bisoprolol, 1.25 mg PO, daily; maximum dose: 10 mg, daily
Aldosterone antagonists
o Spironolactone 12.5 to 25 mg, PO, daily; maximum: 50 mg/day. If 25
mg once daily not tolerated, may reduce to 25 mg every other day
▪ NB: 50mg/day patients with high dose furosemide and
hypokalemia

7. Follow up during management of admitted patients

➢ Use the standard heart failure management follow up sheet posted


by the bedside.
➢ V/S including orthostatic hypotension and SPO2 every 1hr until
patient stabilizes and then every 4-6 hrs.
➢ 24 hrs urine output and fluid balance documented every 6hrs
together with V/S.
➢ Weight every 24hrs (morning prior to eating and voiding, same
scale).
o goal is 1kg/day weight loss
➢ Signs of heart failure every 12hrs (JVP, basal crackles, S3 gallop,
hepatomegaly, edema).
➢ Symptoms (dyspnea, orthopnea).
➢ Cr, BUN, K+, Na+ every 24hrs until patient stabilizes and then every
3-5 days and manage accordingly

Table: Sample; heart failure follow up sheet

Date Time BP PR RR T0 Wt SO2 UOP Crepit Hepato JVP Edema Cr Na+ K+ Sign
ation megaly

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Before Discharge
❖ Proper advice: salt consumption, activity, adherence to medications and follow up.
❖ Prescribe adequate medications and give requests for further planned outpatient investigations.
❖ Document medications with dose and further plans clearly on the discharge note.
❖ Early appointment preferably in one-week time to follow up clinic.

Chronic OPD follow up and management

During OPD follow up

Assess Manage:

☛ Symptoms ☛ Escalate dose of ACEIs and BBs if no problem


☛ Functional status ☛ Consider add on therapies like spironolactone, digoxin if
☛ Adherence patient not improving after optimal diuretic, ACEI and
☛ Medication tolerance BB therapy
☛ P/E: V/S, signs of heart failure, ☛ on adherence to treatment and life style modifications
precordial exam
☛ Investigations: Cr, BUN, K+, Na+ as
appropriate

Steps in the management of Heart Failure with Reduced Left Ventricular Systolic
Function (HFrEF)

☛ Step 1: Start low dose ACEIs


☛ Step 2: review after two weeks: Check tolerance and side effects
o BP, symptoms
o Side effects ACEIs
☛ Step 3: Increase dose of ACEIs
o If there is troubling cough related to the ACEIs (not because of
heart failure), switch therapy to ARBs
☛ Step 4: review after one month and assess for Beta blocker therapy
o If a candidate; start low dose Betablocker
☛ Step 5: Review after two weeks for assessment
o If tolerated, increase dose
o Remark: in stable, mildly to moderately symptomatic patients with 35
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systolic HF, initiation of therapy with BBs followed by ACEI has


similarly efficacious to the opposite sequence in terms of combined
mortality and all-cause hospitalization.
☛ Step 6: Review heart failure status (symptom, NYHA class, congestion)
o Optimize therapy as per evidences
☛ Step 7: Monitor therapy at each visit (RFT, Electrolytes, optimize risk
factors)
☛ Step 8: Early referral for refractory cases for cardiologist evaluation

Table; Treatment of chronic heart failure with reduced EF (LVEF<40%) (non-rheumatic*)


Diet, exercise ✓Avoid table salt intake, alcohol and smoking
✓Avoid stimulant caffeine other like khat, marijuana Avoid
excess free water consumption
✓Exercise training in ambulating patients
ACEI Escalate every 1-2 week
☛ Watch for azotemia, increased K+, ✓ Enalapril dose 2.5mg/day - 20mg BID
cough, angioedema Alternative
☛ Contraindicated; pregnancy, renal ✓ Lisinopril dose 10-40mg/day
artery stenosis, hyperkalemia

ARBs (ATII receptor blockers) ✓Candesartan 8-32 mg/day in 1-2 divided doses
☛ Alternative to ACEI (cough, Alternative
angioedema) but not a substitute ✓Valsartan 40 - 80 mg PO BID

ARNI (Angiotensin-Nepro lysin Inhibitors) Sacubitril/Valsartan combination


✓ Starting with 50 mg (24mg/26mg) PO BID to
increase to the most tolerable dose of 200 mg
(97mg/103mg) PO BID
Beta- blockers Preferred: (long releasing and escalate every 2 week)
☛ High dose is more efficacious ✓ Metoprolol dose 6.75 - 200mg per day
☛ Caution: severe COPD/asthma, AV ✓ Carvedilol dose 3.125-25mg BID
block(bradycardia), ✓ Bisoprolol 1.25 mg Po-10 mg Po daily
hypotension(shock) ✓ Nebivolol 1.25 mg PO-10 mg Po daily

Aldosterone antagonist ✓Spironolactone 25mg po per day


☛ Consider in severe HF or post
MI NB: 50mg/day patients with high dose furosemide and
☛ Caution: renal function hypokalemia
derangement, Increased K +

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Diuretics Loop diuretics


☛ Patients with congestion (I.e. Not only ✓Lasix(furosemide) 20mg/day up to 100- 120mg TID/QID
right sided but also orthopnea, PND, (preferred to keep low dose)
nocturnal cough) Thiazide:
☛ Watch electrolyte (Na, K, Cl) and BUN, ✓HCT 12.5-25mg per day (congestion not improved with
Cr high dose Lasix)
Digoxin ✓Dose 0.125-0.25mg per day
☛ Caution: renal failure, hypokalemia,
Rheumatic heart disease (MS)
☛ Use: rate control in AFFVR and added
on therapy
Anticoagulant (OAC) ✓Warfarin 2.5-10mg per day
☛ If indicated

☛ * for Chronic heart failure in rheumatic heart disease patients, click and see

☛ Valvular heart disease (VHD)


☛ ACEI, ARBs, Beta- blockers and Aldosterone antagonists have survival benefits and anti-
remodeling effect
☛ Choice between drugs depends on underlying heart disease
☛ Avoid combination of drugs from same group or ACEI with ARBs and spironolactone

Prognosis
Despite recent advances in the management of HF, the development of
symptomatic HF still carries a poor prognosis.
30 - 40% of patients die within 1 year of diagnosis and 60 - 70% die
within 5 years, mainly from worsening HF or as a sudden event (probably
because of a ventricular arrhythmia).
Although it is difficult to predict prognosis in an individual, patients with
symptoms at rest (NYHA class IV) have a 30 - 70% annual mortality rate,
whereas patients with symptoms with moderate activity (NYHA class II)
have an annual mortality rate of 5 - 10%. Thus, functional status is an
important predictor of patient outcome

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1.2 Acute Rheumatic Fever(ARF) & Rheumatic heart


disease (RHD)

1.2.1. Acute rheumatic Fever (ARF)


❖ Acute rheumatic fever (ARF) is a multisystem disease occurring as a non-
suppurative complication from an autoimmune reaction to infection with
group A streptococcus (GAS).
❖ Most episodes of acute tonsillopharyngitis are caused by viruses.
❖ Up to 30% of sore throats in children and young people are caused
by GABHS
❖ About 0.3% to 3% of young people with an untreated GABHS sore
throat will develop RF
❖ Although many parts of the body may be affected, almost all of the
manifestations resolve completely.
❖ The major exception is cardiac valvular damage (rheumatic heart disease
[RHD]), which may persist after the other features have disappeared.
❖ ARF and RHD are diseases of poverty.
❖ RHD is the most common cause of heart disease in children in
developing countries and is a major cause of mortality and morbidity in
adults as well.
❖ Some 95% of ARF cases and RHD deaths now occur in developing
countries, with particularly high rates in sub-Saharan Africa, Pacific
nations, Australasia, and South and Central Asia.
❖ The pathogenetic pathway from exposure to group A streptococcus
followed by pharyngeal infection and subsequent development of ARF,
ARF recurrences, and development of RHD and its complications is
associated with a range of risk factors and, therefore, potential
interventions at each point.
❖ Crowdedness and poor hygiene lead to increased transmission of the
bacteria

Epidemiology

❖ ARF is mainly a disease of children age 5 - 14 years.


❖ Initial episodes become less common in older adolescents and young
adults and are rare in persons aged >30 years.
❖ By contrast, recurrent episodes of ARF remain relatively common in
adolescents and young adults.
❖ This pattern contrasts with the prevalence of RHD, which peaks between
25 and 40 years.
❖ There is no clear gender association for ARF, but RHD more commonly
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affects females, sometimes up to twice as frequently as males.


❖ The prevalence of rheumatic heart disease in the Ethiopian population
among the asymptomatic school children is 19 per 1000 population.

Pathogenesis

Etiology: infection of the URT with group A, B- hemolytic streptococcus

any strain has the potential to cause it


repeated pharyngitis is required to prime the immune system before the
development of ARF
Basic pathogenesis still unknown, but there are two theories postulated to explain
RF

1st: toxic effect of extra-cellular toxins produced by strep on target organs


such as myocardium, valves, synovium & brain (cytotoxicity theory)
2nd: most popular hypothesis is immunologic damage on target organs as a
result of antigenic similarity b/n strep cellular components & human tissue
(hypothesis of molecular mimicry)
✓ Strep M-protein shares certain amino acid sequence with some
human tissue, this is supposed to lead to cross reactivity b/n the
organism & human host

Clinical features

Incubation period of ~3 weeks (1 - 5 weeks)


 The clinical features of ARF occur
 2 to 3 weeks after sore throat (streptococcal Pharyngitis)
 3 to 6 weeks after skin infection (streptococcal
Pyoderma)
 The exceptions are chorea and indolent carditis, which
may follow prolonged latent periods lasting up to 6 months.
Although many patients report a prior sore throat, the preceding GAS
infection is commonly subclinical; in these cases, it can only
be confirmed using streptococcal antibody testing.
The most common clinical features are Polyarthritis (60 - 75%) and
rheumatic carditis (50 - 60%).
The prevalence of chorea in ARF varies substantially between populations,
ranging from <2 to 30%.
Erythema marginatum and subcutaneous nodules are now rare, being found
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Heart involvement (Rheumatic carditis)


Up to 60% of patients with ARF progress to RHD.
ARF causes pan carditis, affecting the pericardium (pericarditis), epicardium,
myocardium (myocarditis, sometimes manifest as conduction system
disease), and endocardium (valvulitis).
Valvular damage is the hallmark of rheumatic carditis.
o The mitral valve is almost always affected, sometimes together with
the aortic valve
o Isolated aortic valve involvement is rare.
o Damage to the pulmonary or tricuspid valves is usually secondary to
Increased pulmonary pressures resulting from left-sided valvular
disease.
o Early valvular damage leads to regurgitation.
o Over ensuing years, usually as a result of recurrent episodes, leaflet
thickening, scarring, calcification, and valvular stenosis may
develop
o Therefore, the characteristic manifestation of carditis in previously
unaffected individuals is MR, sometimes accompanied by AR.
o MR is the most common early valvular manifestation and may be
accompanied by AR and/or uncommonly by TR; isolated AR is less
common
o Heart failure (HF) and left ventricular (LV) dilation in patients with
ARF are caused chiefly by severe valve disease (mainly MR with or
without AR)
Myocardial inflammation may affect electrical conduction pathways,
leading to P-R interval prolongation (first-degree AV block
or rarely higher-level block) and softening of S1.
People with RHD are often asymptomatic for many years before
their valvular disease progresses to cause cardiac failure.
Moreover, particularly in resource-poor settings, the diagnosis of ARF is
often not made, so children, adolescents, and young adults may have RHD
but not know it.

Joint involvement
The most common form of joint involvement in ARF is arthritis (i.e.,
objective evidence of inflammation, with hot, swollen, red, and/or
tender joints, and involvement of more than one joint (i.e., polyarthritis)).
Polyarthritis is typically migratory, moving from one joint to
another over a period of hours.
ARF almost always affects the large joints, most commonly the knees,
ankles, hips, and elbows, and is asymmetric.
The pain is severe and usually disabling until anti-inflammatory medication
is commenced.
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Less severe joint involvement is also relatively common and has


been recognized as a potential major manifestation in high-risk populations
in the most recent revision of the Jones criteria.
Arthralgia without objective joint inflammation usually affects large joints in
the same migratory pattern as polyarthritis.
In some populations, aseptic mono-arthritis may be a presenting feature of
ARF, which may, in turn, result from early commencement of anti-
inflammatory medication before the typical migratory pattern is established.
The joint manifestations of ARF are highly responsive to salicylates
and other NSAIDs.
o Indeed, joint involvement that persists for more than 1 or 2 days
after starting salicylates is unlikely to be due to ARF.

Chorea
Sydenham’s chorea commonly occurs in the absence of other
manifestations, follows a prolonged latent period after GAS
infection, and is found mainly in females.
The choreiform movements affect particularly the head (causing
characteristic darting movements of the tongue) and the upper limbs.
They may be generalized or restricted to one side of the body (hemi-
chorea).
In mild cases, chorea may be evident only on careful examination, whereas
in the most severe cases, the affected individuals are unable to perform
activities of daily living.
There is often associated emotional lability or obsessive-compulsive traits,
which may last longer than the choreiform movements (which usually
resolve within 6 weeks but sometimes may take up to 6 months).
Clinical maneuvers to elicit features of chorea include:
☛ Milkmaid's grip
☛ Spooning and pronation of the hands during extension
☛ Wormian darting movements of the tongue upon protrusion, and
☛ Examination of handwriting to assess fine motor

Skin manifestations
Erythema marginatum
o The classic rash of ARF is erythema marginatum, which begins
as pink macules that clear centrally, leaving a serpiginous, spreading
edge.
o The rash is evanescent, appearing and disappearing before the
examiner’s eyes.
o It occurs usually on the trunk, sometimes on the limbs, but almost
never on the face.

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Figure; Erythema marginatum

Subcutaneous nodules
o Occur as painless, small (0.5 - 2 cm), mobile lumps beneath the
skin overlying bony prominences, particularly of the hands, feet,
elbows, occiput, and occasionally the vertebrae.
o They are a delayed manifestation, appearing 2 - 3 weeks after the
onset of disease, last for just a few days up to 3 weeks, and are
commonly associated with carditis.

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Figure: Subcutaneous nodules associated with rheumatic fever.

Other features
Fever occurs in most cases of ARF, although rarely in cases of pure
chorea.
o Although high-grade fever (≥39°C) is the rule, lower grade
temperature elevations are not uncommon.
Elevated acute-phase reactants are also present in most cases.

Evidence of a preceding GAS infection

➢ With the exception of chorea and low-grade carditis, both of which may
become manifest many months later, evidence of a preceding GAS infection
is essential in making the diagnosis of ARF.
➢ Because most cases do not have a positive throat swab culture or rapid
antigen test, serologic evidence is usually needed.
o The most common serologic tests are the anti-streptolysin O (ASO)
and anti-DNase B (ADB) titers.

Confirming the diagnosis


Because there is no definitive test, the diagnosis of ARF relies on the
presence of a combination of typical clinical features together with
evidence of the precipitating GAS infection, and the exclusion of other
diagnoses.
This uncertainty led Dr. T. Duckett Jones in 1944 to develop a set of
criteria (subsequently known as the Jones criteria) to aid in the diagnosis.
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The most recent revision of the Jones criteria (see Table Below) require
the clinician to determine if the patient is from a setting or population
known to experience low rates of ARF.
o For this group, there is a set of “low-risk” criteria; for all others,
there is a set of more sensitive criteria.

Table; Jones Criteria


For All Patient Populations with Evidence of Preceding GAS Infection
Diagnosis: initial ARF 2 major manifestations or
1 major plus 2 minor manifestations
PLUS
Evidence of recent strep infection (other
than chorea)
Diagnosis: recurrent ARF 2 major or
1 major and 2 minors or
3 minors
PLUS
Evidence of recent strep infection (other
than chorea)

Low-risk populations a Moderate- and high-risk populations


Major Criteria*
Carditis b Carditis
➢ Clinical and/or subclinical ➢ Clinical and/or subclinical
Arthritis Arthritis
➢ Polyarthritis only ➢ Monoarthritis or polyarthritis
➢ Polyarthralgia c
Chorea Chorea
Erythema marginatum Erythema marginatum
Subcutaneous nodules Subcutaneous nodules
Minor Criteria
Polyarthralgia Monoarthralgia
Fever (≥38.50C) Fever (≥38.50C)
ESR ≥ 60 mm in the first hour and/ ESR ≥30 mm/h and/or CRP
or CRP ≥3.0 mg/dL d ≥3.0 mg/dL d
Prolonged PR interval, after accounting for age Prolonged PR interval, after accounting for age
variability (unless carditis is a major criterion) variability (unless carditis is a major criterion)

a
Low-risk population are those with ARF incidence ≤2 per 100,000 school-age
children or all-age rheumatic heart disease prevalence of ≤1 per 1000 population
per year (Ethiopia is under ‘’high risk populations’’ category).
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b
Subclinical carditis indicates echocardiographic valvulitis.

c
Polyarthralgia should only be considered as a major manifestation in moderate- to high-risk
populations after exclusion of other causes. As in past versions of the criteria, erythema marginatum
and Subcutaneous nodules are rarely “standalone” major criteria. Additionally, joint manifestations can
only be considered in either the major or minor categories but not both in the same patient.

d
CRP value must be greater than upper limit of normal for laboratory. Also, because ESR may evolve
during the course of ARF, peak ESR values should be used.

Abbreviations: ARF, acute rheumatic fever; CRP, C-reactive protein; ESR, erythrocyte sedimentation
rate. GAS, Group A Streptococcal

*Mneumonic for major criteria → JONES

J → Polyarthritis (Migratory Joint pain)


→ Pan Carditis

N → Subcutaneous Nodules

E → Erythema marginatum

S → Sydenham Chorea

Decisions based on Jones criteria

➢ Definite ARF: 2 major, or 1 major plus 2 minor manifestations PLUS


evidence of recent strep infection (other than chorea)

➢ Highly Probable ARF: If an ARF diagnosis is considered highly


probable (but not confirmed due to lack of evidence for recent
streptococcal infection). This group may be more common in Ethiopia
as there is often lack of laboratory tests to confirm recent
streptococcal infections.

➢ Uncertain ARF: in patients from high-risk groups with only one major
manifestation of acute Rheumatic fever or borderline echocardiographic
findings.

Recommended Tests in Cases of Possible ARF 45


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Chapter 1; Heart failure (ልብ ድካም) and Other Cardiac Disorders

➢ Recommended for All Cases


o CBC → leukocytosis
o ESR and CRP → raised
o Blood cultures if febrile
o ECG
▪ If prolonged P-R interval or other rhythm abnormality, repeat
in 2 weeks, and again at 2 months if still abnormal
o Echo
▪ New or worsening regurgitant murmur, minimal pericardial fluid
▪ Consider repeating after 1 month if negative
o Chest x-ray
▪ If clinical or echo evidence of carditis
o Throat swab
▪ Preferably before giving antibiotics
▪ Culture for group A streptococcus
o Antistreptococcal serology:
▪ Both anti-streptolysin O and anti-DNase B titers
▪ If available (repeat 10 - 14 days later if first test not
confirmatory)
➢ Tests for Alternative Diagnoses, Depending on Clinical Features
o Repeated blood cultures if possible, endocarditis
o Joint aspirate (microscopy and culture) for possible septic arthritis
o Copper, ceruloplasmin, antinuclear antibody, drug screen for
choreiform movements
o Serology and autoimmune markers for arboviral, autoimmune, or
reactive arthritis

Management of ARF

➢ There is no treatment for ARF that has been proven to alter the
likelihood of developing, or the severity of RHD. With the exception of
treatment of heart failure, which may be life-saving in cases of severe
carditis, the treatment of ARF is symptomatic.

Non-pharmacologic
✓ Bed rest if the patient has severe rheumatic carditis or arthritis/arthralgia
only.
o Traditional recommendations for long-term bed rest, once the
cornerstone of management, are no longer widely practiced.
Instead, bed rest should be prescribed as needed while arthritis
and arthralgia are present and for patients with heart failure. Once
symptoms are well controlled, gradual mobilization can commence
as tolerated.
✓ Salt restriction if there is associated Heart Failure.
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Pharmacologic
5 approaches
a. Antibiotic therapy
b. Anti-inflammatory therapy (ASA, and NSAID’s)
c. Treat CHF
d. Sydenham chorea treatment if present
e. Prevention

1. Antibiotic therapy
✓ All patients with ARF should receive antibiotics sufficient to treat the
precipitating group A streptococcal infection.
✓ Penicillin is the drug of choice and can be given orally
o Benzathine penicillin G, 1.2 million units (600,000 units for
children ≤30 kg1), IM, stat → drug of choice or
o Amoxicillin, 500mg PO, TID (For children 50/kg/day, TID
[maximum, 1 g], for 10 days or
o Penicillin V, 500 mg [250 mg for children ≤27 kg] PO, BID, for
10 days

o Erythromycin PO for 10 days, if allergic to Penicillin’s.


✓ For more, refer tonsillopharyngitis management (click here → Acute
tonsillopharyngitis (የቶንሲል በሽታ ፣ የአንቃር እና ጉሮሮ ብግነት))

2. Anti-inflammatory therapy (ASA, and NSAID’s)


o These may be used for the treatment of arthritis, arthralgia, and
fever, once the diagnosis is confirmed.
o They are of no proven value in the treatment of carditis or chorea.
▪ Those with carditis without cardiomegaly or CHF may
benefit from aspirin therapy
o Aspirin is the drug of choice2
▪ Migratory polyarthritis, with carditis without cardiomegaly or

1
National NCD management protocol 2021 says 600,000 units for children ≤ 30kg. UpToDate
2018, Says 600,000 units for children ≤ 27kg. we recommend national guideline cut points
(30Kg)
2
Aspirin dose from Harrison 21st edition. (the dose on the text above is from UpToDate
2018, Pediatricians in Ethiopia recommend the UpToDate dose)
50 - 60 mg/kg/day, up to a maximum of 80 - 100 mg/kg per day (4 - 8 g/d in
adults) in 4 - 5 divided doses. When the acute symptoms are substantially
resolved, usually within the first 2 weeks, patients on higher doses can have the
dose reduced to 50 - 60 mg/kg/day for a further 2 - 4 weeks.

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CHF:
• Initial: 100 mg/kg/day, PO, QID for 3 to 5 days,
followed by 75 mg/kg/day, PO, QID for 4 weeks.
▪ Carditis and cardiomegaly or CHF:
• At the beginning of the tapering of the prednisone
dose, aspirin should be started at 75 mg/kg/day, PO,
QID for 6 weeks or
• Ibuprofen 30mg/kg per day 8 hourly.
▪ If Patient is not responding or tolerating ASA or
Ibuprofen Start Prednisolone 2mg/Kg/day for
2 weeks; then aspirin is added at dose 60 mg/Kg/day,
QID for another 2 weeks; then Prednisolone is tapered
& discontinued
▪ Fever, joint manifestations, and elevated acute phase
reactants sometimes recur up to 3 weeks after the
medication is discontinued. This does not indicate a
recurrence and can be managed by recommencing
salicylates for a brief period.
▪ Add a GI prophylaxis - PPI (e.g. Omeprazole 20mg, P.O.,
BID)
o Naproxen is a suitable alternative to aspirin
▪ 10 - 20 mg/kg/day PO, BID

3. Treat CHF (see the respective topic)

➢ Diuretics/fluid restriction for mild or moderate failure


o Furosemide 1-2mg/kg PO/day
➢ ACE inhibitors like enalapril or Lisinopril for more severe failure, particularly
if AR is present
➢ Anti-coagulation medication and digoxin if atrial fibrillation is present
➢ Valve surgery for life-threatening acute carditis (rare)
➢ Prednisolone may be given for severe carditis
➢ Glucocorticoids
o The use of glucocorticoids in ARF remains controversial.
o Many clinicians treat cases of severe carditis (causing heart failure)
with glucocorticoids in the belief that they may reduce the acute
inflammation and result in more rapid resolution of failure. However,
the potential benefits of this treatment should be balanced against
the possible adverse effects.
o Its use was Considered in Patients with carditis and
cardiomegaly or CHF
o If used, prednisone or prednisolone is recommended
▪ 1 - 2 mg/kg/day (maximum, 80 mg), usually for a few
days or up to a maximum of 3 weeks.
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▪ prednisone is 2 mg/kg/day, QID, for 2-3 wk followed by a


tapering of the dose that reduces the dose by 5 mg/24 hr
every 2-3 days.
▪ At the beginning of the tapering of the prednisone dose,
aspirin should be started at 75 mg/kg/day, QID, for 6 wk.
4. Sydenham chorea treatment if present

❖ Medications to control the abnormal movements do not alter the


duration or outcome of chorea.
❖ Milder cases can usually be managed by providing a calm
environment.
❖ In patients with severe chorea
o Carbamazepine at 7–10 mg/kg/day, TID or
o Valproic acid at 15–20 mg/kg/day, TID or
o Phenobarbitone at 3-6 mg/kg/day (particularly in children) can
be given for severe cases.
▪ A response may not be seen for 1 - 2 weeks, and
medication should be continued for 1 - 2 weeks after
symptoms subside.
o Corticosteroids are effective and lead to more rapid symptom
reduction in chorea.
▪ They should be considered in severe or refractory cases.
▪ Prednisone or prednisolone, 0.5 mg/kg, PO, daily, with
weaning as early as possible, preferably after 1 week if
symptoms are reduced, although slower weaning or
temporary dose escalation may be required if symptoms
worsen.

5. Prevention

Primary prevention:
▪ Ideal: eliminating risk factors for GAS infection which are over crowdedness
and poor hygiene (the antibiotics discussed above)
▪ If sore throat is treated within 9 days of commencement ARF will be
prevented

Secondary prevention
 The mainstay of controlling ARF and RHD is secondary prevention.
 When should secondary prophylaxis be considered?
 ARF confirmed by the Revised Jones Criteria
 RHD confirmed on echocardiogram


ARF or RHD not confirmed but considered highly ‘probable’
RHD post-surgery
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 Benefits of Secondary prevention in ARF and RHD


 Prevent further Group A Streptococcal infection
 Prevent recurrence ARF
 Prevent the development of RHD
 Reduce the severity or worsening of RHD. It is associated
with regression of heart disease in approximately 50-70% of
those with good adherence over a decade and reduces
mortality
 Because patients with ARF are at dramatically higher risk than the general
population of developing a further episode of ARF after a group
A streptococcal infection, they should receive long-term penicillin
prophylaxis to prevent recurrences.
 Long term antibiotic prophylaxis is required for those patients who have
sustained an episode of rheumatic fever (see the table below)

o First line
▪ A single IM injection of benzathine penicillin G3 (600,000 IU
for children ≤ 30kg and 1.2 million IU for those >30kg and
adults) every 4 weeks (i.e. monthly)
☛ It can be given every 3 weeks, to persons
considered to be at particularly high risk.
o Alternative
▪ Penicillin V, 250 mg, PO, BID For 10 days, every month or
▪ Amoxicillin 500 mg po TID for 10 days, every month
o For Penicillin-allergic patients
▪ Erythromycin, (250mg, for age < 7 years and 500 mg for
age > 7 years), P.O. BID for 10 days, every month

Table; Duration of secondary prophylaxis


Category of Patient Duration of Prophylaxis
Rheumatic fever without carditis For 5 years after the last attack or
Until age 21 years of age (whichever
is longer)
Rheumatic fever with carditis with no residual For 10 years after the last attack, or
valvular disease Until age 25 years of age (whichever is
longer)
Rheumatic fever with persistent valvular disease, For 10 years after the last attack, or 40
evident clinically or on echocardiography years of age (whichever is longer);
sometimes lifelong prophylaxis

3
NEVER EVER GIVE BPG INTRAVENOUSLY THIS MAY LEAD TO IMMEDIATE DEATH!!
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Follow UP
 Weekly or every 2 weeks follow up of ESR and CRP (normalize within 4-
6 weeks)
 Echo after 1 month to see the progression of carditis

Prognosis of ARF

 Untreated ARF stays for 12 weeks


 60 % of patients with ARF develop RHD
 The arthritis and chorea of acute rheumatic fever resolve completely
without sequelae.
 The long-term sequelae of rheumatic fever are essentially limited to the
heart.
 ≈50-70% of patients with carditis during the initial episode of acute
rheumatic fever recover with no residual heart disease.
 Recurrence risk is ≈ 50% following each GAS pharyngitis after initial ARF.
 The risk of recurrence is highest in the 1st 5 yrs after the initial episode
and decreases with time.
 ≈ 20% of patients who present with “pure” chorea who are not given
secondary prophylaxis develop rheumatic heart disease within 20 yrs

1.2.2. Rheumatic Heart Disease (RHD)

Introduction
 RHD is inflammation of heart valves that follows infection with Group A
beta hemolytic streptococcus, commonly pharyngitis.
 It is thought that 40-60% of patients with ARF will go on to developing
RHD.
 Rheumatic disease (RHD) is the only long-term sequalae of ARF which
can lead to death or disability
 Rheumatic carditis affects mainly the heart valves
 Up to 60% of patients with ARF progress to RHD (i.e. Approximately 50 - 60
% of those with evidence of carditis develop organic valvular damage)
✓ The valvular lesions begin as small verrucae composed of fibrin and
blood cells along the borders of one or more of the heart valves.
✓ With repeated attacks of rheumatic fever, new verrucae form near the
previous ones, and the mural endocardium and chordae tendineae
become involved
 Up to 75% of patients with documented recurrences of RF have some form of
valvular disease after 4 to 5 years of follow-up
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 RHD is the most common cause of heart disease in children in developing


countries and is a major cause of mortality and morbidity in adults as well
 RHD, peaks between 25 and 40 years.
 RHD more commonly affects females, sometimes up to twice as frequently as
males.
 RHD remains a major cause of cardiovascular disease in developing nations
✓ In Africa valvular disease is encountered in the young, not infrequently
in children of school-going age or young females of child-bearing
potential, and with a course that is much more rapid.
 RHD accounts for 12 - 65% of hospital admissions related to cardiovascular
disease and 2 - 10% of hospital discharges in some developing countries.
✓ In Ethiopia, RHD Accounts for 50 % of all Cardiovascular disease
admisions to hospital and common in females

ARC: acute rheumatic carditis; MS: mitral stenosis; MV: mitral valve; MR: mitral regurgitation.

Clinical features

 People with RHD are often asymptomatic for many years before their valvular
disease progresses to cause cardiac failure.
✓ A murmur but no symptoms usually suggests mild-moderate disease
✓ Symptoms usually suggest moderate-severe disease
 Symptoms depend upon the type and severity of disease, and may include
✓ Breathlessness on exertion (dyspnea) or when lying down flat(orthopnea)
✓ Waking at night feeling breathless (paroxysmal nocturnal dsypnoea)
✓ Feeling tired
✓ Generalized weakness
✓ Palpitations
✓ Peripheral edema 52
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✓ left anterior chest pain and syncope in addition to heart failure


symptoms can also occur
P/E
 Patients with RHD may have the following findings if they come with heart
failure or other complications
✓ Tachycardia (Increased heart rate)
✓ Tachypnea (increased respiratory rate)
✓ Raised temperature
✓ Cyanosed lips and tongues
✓ Bluish discoloration)
✓ Chest Crackles
✓ Heart Murmurs
✓ Tender RUQ area (because of liver congestion)
✓ Leg edema
✓ Weak extremities because of stroke.
✓ Chest crackles and cardiac murmurs
 While chronic RHD occurs only as a sequalae of ARF, the majority of patients
with RHD lack a history of past ARF, suggesting that the diagnosis of ARF is
frequently missed with the initial or recurrent insults being subclinical or not
detected.
 RHD generally presents as valve disease, which may or may not be detected
by a murmur.
 Common Murmurs in RHD → MR, AR, MS, AS
 The frequency of symptoms and signs of HF (eg, dyspnea and evidence of
pulmonary edema) and of embolic events (eg, stroke) among patients with
RHD varies depending upon the stage of valve disease at diagnosis.
 In endemic areas presentation with advanced disease is common
 Complications of RHD may happen such as
✓ HF
✓ Atrial fibrillation
✓ IE
✓ Pulmonary hypertension, and
✓ Cardio-embolic stroke (less common)
 Multivalvular disease (varying combinations of stenotic or regurgitant lesions
involving the mitral and aortic valves) is the predominant abnormality in older
adults
✓ The Mitral Valve is involved (MR with or Without MS) in nearly all
cases of RHD, including those with other affected valves.
✓ The aortic valve is involved (AR with or Without AS) in approximately
20 to 30 % of cases.
✓ The tricuspid valve is commonly affected, but tricuspid valve disease is
frequently subclinical until surgery is required.
▪ RHD can cause organic TR and/or tricuspid stenosis.
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▪ Rheumatic tricuspid valve disease is almost invariably associated


with Mitral Valve disease
✓ Pulmonic valve involvement is rare.
 So, the Clinically detectable valvular findings from RHD patients in our setup
are MR and AR with/without TR
 The diagnosis of RHD is generally confirmed by transthoracic
echocardiography, which enables assessment of valve morphology and severity
of valve dysfunction (regurgitation and/or stenosis).
✓ Echocardiography is also used to assess left and right ventricular size
and function and may enable estimation of pulmonary artery systolic
pressure.
 for more, see Rheumatic carditis above and VHD below

World Heart Federation criteria for the echocardiographic diagnosis of RHD

➢ Definite RHD is diagnosed if one or more of the following criteria are


present: (For patients with no history of ARF)
o Pathologic MR and at least two morphologic MV features of RHD
(see table below).
o MS mean gradient ≥4 mmHg (congenital MV anomalies and
nonrheumatic mitral annular calcification must be excluded).
o Pathologic AR and at least two morphologic features of RHD of the
MV.
▪ For individuals ≤20 years old, bicuspid aortic valve, dilated
root, and hypertension must be excluded.
o For individuals ≤20 years old, borderline disease of both the aortic
valve and Mitral Valve.
▪ Combined AR and MR, particularly in high-prevalence regions
and in the absence of CHD, is regarded as rheumatic.
o For individuals <35 years old, pathologic AR, and at least two
morphologic features of RHD of the aortic valve.
▪ Bicuspid aortic valve, dilated aortic root, and hypertension
must be excluded.
➢ Borderline RHD only applies to individuals ≤20 years old and is present if
one of the following criteria is present: (For patients with no history of ARF)
o At least two morphologic features of RHD of the MV without
pathologic MR or MS
o Pathologic MR
o Pathologic AR
➢ For patients with history of ARF
o Consider the diagnosis of RHD definite if there is a typical valvular
abnormality (as defined by one or more morphologic World Heart
Federation criteria of RHD (table below) or
o Evidence of World Heart Federation criteria for pathologic
regurgitation).

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MV: mitral valve; AMVL: anterior mitral valve leaflet; AV: aortic valve; RHD: rheumatic heart disease.
¶: ≥3 mm for individuals aged ≤20 years; ≥4 mm for individuals aged 21 to 40 years; ≥5 mm for
individuals aged >40 years

Screening for RHD


➢ Screening for RHD is recommended for children and young adults in
Ethiopia.
➢ The following sequence is recommended for screening:
o Taking a history for prior ARF
o Echo in all, and then clinical cardiac evaluation of cases with
abnormal echo
➢ Timing and frequency of screening-the evidence on the natural history
of RHD suggests that at least 2 echo-based screening tests are
indicated: one before age 18 and another by 35 years of age.
➢ Cases of probable or possible RHD require a repeat evaluation within
a year to confirm the diagnosis prior to embarking upon long-term
prophylaxis.

Management of RHD
➢ The management of RHD is complex and requires careful co-ordination.
➢ The main goal is to prevent disease progression and to avoid, or at least
delay, valve surgery.
➢ The key principles for effective management of RHD include:
o Effective baseline assessment, education and referral
▪ Establishing the diagnosis of RHD (see above)
▪ Detecting and treating Complications of RHD (see below)
o Treatment of cardiac and other symptoms
o Long-term secondary prophylaxis (to prevent recurrent ARF)
o Regular medical and cardiology review including echocardiography
o Appropriate and timely surgical interventions
o Dental assessment and care
o Advise on Family planning and referral
o Management of RHD in special situations (e.g. pregnancy)
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Medical Management of RHD

➢ It encompasses the identification and management of complications of RHD


and management of patient after cardiac interventions:
o Heart failure
o Atrial fibrillation
o Infective endocarditis
o Stroke
o Post cardiac intervention care

Valve surgery or interventions for RHD

➢ The need for surgery and cardiac interventions in RHD depends on:
o Severity of symptoms
o Evidence that the heart valves are severely damaged
o Left ventricular chamber size and ejection fraction
o Availability of long-term management after surgery (i.e.
anticoagulation)

Indications for interventions

1. Asymptomatic Patients:

➢ Asymptomatic patients with severe valvular lesion (see Echo criteria for
severity) should be closely monitored to decide the appropriate time for
intervention. The following are indications for intervention:
o Severe Pulmonary hypertension.
o For regurgitant lesions (MR and AR), decrease in LV ejection
fraction or Increasing in LV dimensions especially LV end systolic
dimension.
o Severe MS.

2. Symptomatic patients:

➢ Symptomatic patients with severe valve dysfunction should be referred for


intervention.

Type of Interventions in Rheumatic Heart disease

➢ The Heart valves can be repaired or replaced.


➢ Choice of intervention should take into account availability of facilities, future
pregnancy, age and ability to continue to take anticoagulation.
➢ For Patients who wishes to be pregnant and unable to take oral
anticoagulant, valvotomy, valve repair or tissue type of prosthetic valve
should be considered.
➢ For those with atrial fibrillation, younger age, able to take oral
anticoagulation and pregnancy is not an issue mechanical valve
replacement should be considered.
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Cardiac Intervention options

➢ 1- Valve repair
o This is done mainly for MR but needs careful assessment by
Echocardiography to select the suitable candidates.
➢ 2- Percutaneous transvalvular mitral commissurotomy (PTMC):
o Patients with severe MS and suitable valve anatomy should be
considered for PTMC or for closed mitral valvotomy (CMV), if PTMC
is not available.
➢ 3- Valve replacement:
o Prosthetic valve replacement is the option when valve repair or
commissurotomy is not feasible for MV disease and it is the main
procedure for AV disease.
o Valve replacement can be either mechanical valve or bioprosthetic
valve.

Assessment before surgery includes

➢ Echocardiogram to assess severity of heart valve damage


➢ Complete dental assessment and treatment (if required)
➢ Review and management of other health problems (e.g. Kidney disease,
vascular and chronic respiratory disease, cancers, malnutrition or obesity)

Post Valve Surgery Care

➢ Valve surgery is not curative for RHD and many complications can happen
after valve surgery so patients need continuous follow up care. It includes:
o Continue Benzathine Penicillin G monthly injections for life
o In patients with mechanical prosthetic valves:
▪ Warfarin should not be stopped
▪ INR control: target 2.5-3
o Endocarditis prophylaxis before high risk procedures
o Dental hygiene
o Regular medical and echocardiographic review.

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Table; Recommended routine review and management plan for ARF and
RHD

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1.3 Valvular heart disease (VHD)

❖ Majority of VHD are 2ry to CRMVHD (Chronic rheumatic multivalvular heart


disease) for all age groups followed by degenerative VHD in old age.
❖ Rheumatic fever is the dominant cause of VHD in developing and low-
income countries.
❖ The prevalence of VHD increases significantly with age for both men and
women.
o Important left-sided valve disease may affect as many as 12 - 13%
of adults aged >75 years
❖ Infective endocarditis has become a relatively more frequent cause of acute
valvular regurgitation.

1. Aortic Regurgitation (AR)

Also called aortic insufficiency


This condition is due to inadequate closure of the aortic valve leaflets.
For acute aortic regurgitation, mortality is particularly high without surgical
repair.

Causes

✓Acute
o IE
o Aortic dissection
o Trauma (Iatrogenic during a failed replacement surgery)
✓Chronic
o Primary valvular disease:
▪ Rheumatic fever (RHD)
▪ IE
▪ Congenital Bicuspid aortic valve
▪ SLE
▪ Syphilitic aortitis
▪ Ankylosing spondylitis.
▪ Myxomatous (prolapse)
o Aortic root disease: widening of the aortic annulus and separation of the
aortic leaflets are responsible for the AR. causes include;
✓ Aortic dissection
✓ Systemic severe HTN
✓ Cystic medial degeneration of the ascending aorta
✓ Marfan syndrome
✓ Bicuspid aortic valve
✓ Nonsyndromic familial aneurysm
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✓ Aortitis
✓ Idiopathic dilation of the aorta
✓ Annuloaortic ectasia
✓ Osteogenesis imperfecta

Clinical Features

Symptoms

☛ Dyspnea on exertion, PND, orthopnea


☛ Palpitations—worse when lying down
☛ Angina
☛ Cyanosis and shock in acute AR (medical emergency)
☛ Uncomfortable awareness of the heartbeat
☛ Head pounding

Physical examination

☛ Widened pulse pressure—markedly increased systolic BP, with decreased


diastolic BP.
☛ Active precordium with displaced PMI
☛ Murmur of AR
☛ Peripheral signs of AR
✓ deMusset's sign – head bob occurring with each heart beat
✓ Traube's sign – a pistol shot pulse (systolic and diastolic
sounds) heard over the femoral arteries
✓ Duroziez's sign – a systolic and diastolic bruit heard when the
femoral artery is partially compressed
✓ Quincke's pulses – capillary pulsations in the fingertips or lips
✓ Mueller's sign – systolic pulsations of the uvula
✓ Becker's sign – visible pulsations of the retinal arteries &
pupils
✓ Hill's sign – popliteal cuff systolic pressure exceeding brachial
pressure by more than 60 mmHg
✓ Mayne's sign – more than a 15 mmHg decrease in diastolic
blood pressure with arm elevation from the value obtained with
the arm in the standard position
✓ Rosenbach's sign – systolic pulsations of the liver
✓ Gerhard's sign – systolic pulsations of the spleen

Diagnosis

❖ CXR findings: Enlarged cardiac silhouette, dilated aorta


❖ ECG findings: LVH
❖ Echocardiogram
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☛ Assess LV size and function


☛ Look for dilated aortic root and reversal of blood flow in aorta
☛ In acute AR, look for early closure of mitral valve

Serial monitoring

✓ Mild chronic AR- clinical evaluation yearly and routine echo every 2-3 years
✓ Moderate AR - echo every 1-2 years
✓ Severe AR - echo yearly

Treatment

✓ Start enalapril 2.5mg po/day and escalate or amlodipine 5-10mg po/day for
the following patients
☛ Symptomatic severe AR with LV dilation
☛ Asymptomatic severe AR with LVEF <50%
✓ Patients with congestion- refer to pulmonary edema and cardiogenic shock
management
✓ Severe AR with reduced LVEF- refer to the management of HFrEF
☛ N.B. avoid the use of beta blockers in patients with severe AR
✓ Endocarditis prophylaxis- not indicated
✓ Pregnancy – should be avoided in the following patients
➢ NYHA class III to IV symptoms
➢ LVEF <40%
➢ Marfan syndrome
✓ Indications for surgical interventions- patients who can afford and have the
following indications should undergo aortic valve replacement or repair
➢ Symptomatic severe chronic AR
➢ Asymptomatic severe chronic AR and LVEF <50%
➢ Severe chronic AR and severe LV dilatation- LVEDD >75mm or
LVESD >55mm
➢ Severe AR with coronary artery disease requiring bypass graft
surgery

2. TR (Tricuspid Regurgitation)

Causes

Primary (organic)
• Rheumatic fever/RHD
• IE
• Papillary muscle injury (post-MI)
• Myxomatous (tricuspid valve prolapse)
• Leaflet trauma
• Radiation
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• Carcinoid heart disease


• Endomyocardial fibrosis
• Congenital Heart disease in children (Ebstein’s malformation of the
tricuspid valve)
Secondary (functional)
• More than 80% of TR cases encountered in clinical practice are
secondary (functional)
• RV and tricuspid annular dilatation due to multiple causes of RV
enlargement such as
o MI (i.e. remodeling post-RV MI)
o Cardiomyopathy
o Atrial fibrillation (AF)
o Longstanding pulmonary HTN
o Left-sided valve disease

Clinical Features

Symptoms

Mild or moderate degrees of TR are usually well tolerated in the


absence of other hemodynamic disturbances.
Fatigue and exertional dyspnea are early symptoms of isolated, severe TR.
As the disease progresses
• Cervical pulsations
• Abdominal fullness/bloating
• Loss of appetite
• Weight loss
• Painful swelling of the lower extremities.

Signs

Distended neck veins (common finding)


Marked hepatomegaly with systolic pulsations
Ascites
Pleural effusions
Leg edema
Positive hepatojugular reflux sign.
Left parasternal heave
Murmur of TR
• A blowing holosystolic murmur along the lower left sternal margin,
which may be intensified during inspiration (Carvallo’s sign) and
reduced during expiration or the strain phase of the Valsalva
maneuver
AF is usually present in the chronic phase of the disease.

Diagnosis

ECG
• inferior Q-wave MI suggestive of a prior RV MI
• RVH 62
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• RA enlargement
• AF
• a bizarre right bundle branch block-type pattern with preexcitation in
patients with Ebstein’s anomaly
CXR
• RA and RV enlargement, depending on the chronicity and severity of
TR
TTE (Trans thoracic echo) is usually definitive with demonstration of
• Diagnosis and assessment of TR
• RA dilation and RV volume overload
• Prolapsing, flail, scarred, or displaced/tethered tricuspid leaflets with
annular dilatation
• In patients with severe TR, the CO is usually markedly reduced

Treatment

Diuretics can be useful for patients with severe TR and signs of right heart
failure. Loop diuretics like furosemide are typically used
An aldosterone antagonist may be particularly helpful because many
patients have secondary hyperaldosteronism from marked hepatic
congestion.
If heart failure due to left ventricular systolic dysfunction is present,
standard therapy, including beta-blockers and ARB’s are recommended
Correction of pulmonary hypertension can result in improvement in
functional TR, so causes of pulmonary hypertension (such as HF, MS, and
chronic thromboembolic pulmonary disease) should be addressed
Indications for surgical intervention (Tricuspid valve surgery)
• For patients with severe TR who are undergoing left-sided valve
surgery
• For treatment of moderate TR in patients undergoing left-sided valve
surgery who have
o Tricuspid annular dilation (>40 mm)
o A history of right heart failure, or
o Pulmonary arterial hypertension.
• For treatment of severe, primary TR with right heart failure not
responsive to standard medical therapy
• Progressively declining RV systolic function.

3. MR (Mitral Regurgitation)

☛ This condition is due to inadequate closure of the mitral valve.


☛ It could be acute or chronic.
☛ Acute form is associated with much higher mortality

Causes

❖ Acute
o IE (most often S. aureus)
o Papillary muscle rupture (Post MI) or dysfunction (from ischemia)
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o Chordae tendineae rupture


o Blunt trauma
❖ Chronic
o Primary MR - is due to primary abnormality of the valve apparatus. Common
etiologies include
▪ Rheumatic fever/RHD
▪ IE
▪ Mitral valve prolapse (MVP)
▪ Trauma
▪ Congenital (cleft, AV canal)
o Secondary (functional) MR- is due to LV dilatation resulting in annular
dilatation of the mitral valve. Common causes include
▪ IHD
▪ DCMP
▪ HCMP
▪ Chronic Atrial Fibrillation with Left Atrial enlargement and annular dilatation
o Mitral annular calcification
▪ may include elements of both primary and secondary MR as the disease
process may encroach on the leaflets, impair the normal sphincteric
function of the annulus, or both

Clinical Features
Symptoms
✓ Dyspnea on exertion, PND, orthopnea
✓ Palpitations
✓ Later LV failure like Pulmonary edema
Signs
✓ Active precordium with displaced PMI
✓ Apical systolic thrill
✓ S3 gallop
✓ Murmur of MR

Diagnosis
✓ CXR findings: Cardiomegaly, dilated LV, pulmonary edema.
✓ ECG: AFib
✓ Echocardiogram: MR; dilated LA and LV; decreased LV function.
☛ (Doppler and color flow studies) to diagnose the etiology & assess
the severity of MR

Serial monitoring- follow-up echocardiography should be done based on the


severity of MR
✓ Mild MR with no evidence of LV enlargement, LV dysfunction, or pul.
HTN- yearly clinical monitoring is enough. Repeat echocardiography at
these visits is not necessary in the absence of clinical evidence of
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worsening MR
✓ Moderate MR- echo should be done yearly, or sooner if symptoms
occur
✓ Severe MR- echo should be done every 6-12 months, or sooner if
symptoms occur.

Treatment
➢ Depends on the presence or absence of symptoms.
Asymptomatic patients- need only close follow-up.
☛ If patients have associated hypertension, it should be
treated with enalapril or amlodipine
Symptomatic patients- need medical therapy
✓ Lasix 40mg po BID and escalate till the congestion is relieved
✓ Start enalapril 2.5mg po/day and escalate up to 20mg po/day or
maximally tolerated dose
✓ If LVEF < 40%- refer to the protocol for heart failure with reduced
ejection fraction
Atrial fibrillation- refer to AF management protocol
Anticoagulation- similar to patients with mitral stenosis
Endocarditis prophylaxis- not indicated unless prior IE
Prevention of rheumatic recurrence- similar to patients with rheumatic
MR
Indications for surgical intervention- patients who can afford and have
the following indications should be referred early to undergo mitral valve
repair or replacement
✓ Symptomatic severe MR
✓ Asymptomatic severe MR with one of the following factors
o LVEF<60% or LVESD >40mm
o New onset AF
o Pulmonary hypertension

4. Mitral Stenosis (MS)

✓ The disease is more common in women.


✓ Patients are usually asymptomatic until the mitral valve area is reduced to
approximately 1.5 cm2 (normal valve area is 4 - 6 cm2).
✓ Severity- depends on mitral valve area (MVA)
☛ Mild MS → MVA 1.5-2 cm2
☛ Moderate MS → MVA 1.0-1.5 cm2
☛ Severe MS → MVA<1 cm2

Etiology

Rheumatic fever/RHD is the leading cause of MS (>95%)


Other less common etiologies include
o IE with large vegetations
o Congenital (parachute valve, cor triatriatum)
o Severe mitral annular calcification with leaflet involvement
o SLE
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o RA
o Myxoma

Clinical Features

Symptoms

➢ Exertional dyspnea, orthopnea, PND


➢ Palpitations
➢ Hemoptysis
➢ Thromboembolism: often associated with AF
➢ If RV failure occurs, ascites and edema may develop

Signs

➢ Murmur of MS.
➢ Irregularly irregular pulse
➢ With long-standing disease, will find signs of RVF (e.g., right ventricular
heave, raised JVP, hepatomegaly, ascites) and/or pulmonary HTN (loud
P2).
➢ Basal rales on the chest, acute pulmonary edema.
➢ All signs and symptoms will increase with exercise and during
pregnancy.

Diagnosis

➢ CXR: Left atrial enlargement (early)


➢ Echocardiogram—most important test in confirming diagnosis
➢ ECG, CBC, RFT, and electrolytes

Follow-up echocardiography should be done based on the severity of MS

Mild MS- every 3-5 years


Moderate MS- every 1-2 years
Severe MS - yearly

Treatment

HF- Treatment should be instituted for Acute cases (like pulmonary edema and
cardiogenic shock), and symptomatic patients
For patients with symptoms of congestion- pulmonary or peripheral edema
✓ Start Lasix 40mg po BID and escalate every 2wks-1 month till
symptoms subside.
☛ Maximum daily dose of Lasix is 400mg in 3-4 divided doses.
☛ Look for possible side effects of the drug including hypotension
and electrolyte abnormalities
✓ Add spironolactone 25mgs po/day in those patients with Cr < 2.5mg/dl
and serum K+ < 5.5meq/l
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✓ Advise patients to avoid added salt


✓ Once the congestion subsides, reduce Lasix to the lowest possible dose
that can control the symptoms
Patients without congestion but still have exertional symptoms
✓ Start atenolol 25mg po/day and escalate every 2wks-1month till PR
becomes 60-80BPM. Follow for hypotension.
Anticoagulation
✓ Warfarin 5mg po/day with target INR 2.0-3.0
☛ Follow with INR every 2 wks initially till the INR stabilizes and
then every 1-2months.
☛ Indications include
▪ Prior embolic event, left atrial thrombus and presence of
AF
▪ Patients who cannot afford for follow-up INR or have
higher risk of bleeding- start aspirin 81mg po/day
Pregnancy- advise patients to avoid pregnancy and use dual contraception
Benzathine penicillin- 1.2 million IU IM every month lifelong should be given for
all CRHD pt’s
Endocarditis prophylaxis- not indicated unless there is prior IE episode

Indications for surgical intervention- patients who can afford and have the
following indications should be referred as early as possible to undergo PBMV
or valve replacement
✓ Moderate to severe MS with symptoms
✓ Asymptomatic patients with moderate to severe MS and either
pulmonary artery pressure at rest >50mmHg (can be measured with
Doppler echocardiography) or new onset AF

5. Aortic Stenosis (AS)

➢ AS occurs in about one-fourth of all patients with chronic VHD


➢ ~80% of adult patients with symptomatic, valvular AS are male.
➢ It causes obstruction to left ventricular outflow, which results in LVH.
➢ When the aortic valve area falls below 1 cm2, cardiac output fails to
increase with exertion, causing angina (but may be normal at rest).
Causes
Rheumatic fever or RHD.
Congenital (bicuspid, unicuspid)
o Calcification of a congenitally abnormal bicuspid/Unicuspid aortic
valve.
Degenerative calcification
o Calcification of tricuspid aortic valve in elderly.
Radiation

Clinical Features
Symptoms
▪ Patients remain asymptomatic till the valve area is ≤1 cm2. 67
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▪ Classic symptoms include exertional angina, syncope (usually exertional),


dyspnea, and excessive fatigue.
▪ Heart failure symptoms, such as dyspnea on exertion, orthopnea, or
PND
Signs
▪ Active precordium with displaced PMI
▪ Murmur of AS
Diagnosis
✓ CXR findings: Calcific aortic valve, enlarged LV/LA (late)
✓ ECG findings: LVH, LA abnormality
✓ Echocardiography: Valve lesion, degree of stenosis, LVH
✓ Lipid profile
Severity- depends on aortic valve area (AVA)
☛ Mild AS → AVA 1.5-2 cm2
☛ Moderate AS → AVA 1.0-1.5 cm2
☛ Severe AS → AVA ≤ 1 cm2
☛ Aortic valve sclerosis- thickened aortic valve with AVA >2 cm2
Follow-up echocardiography should be done based on the severity of AS
Mild AS- every 3-5 years
Moderate AS- every 2 years
Severe AS - yearly

Treatment
Mainly indicated for symptomatic patients
In patients with severe AS (valve area <1 cm2), strenuous physical activity
and competitive sports should be avoided, even in the asymptomatic stage.
Avoid dehydration and hypovolemia

❖ For asymptomatic patients


✓ Prevention of progression of rheumatic AS- monthly penicillin prophylaxis
✓ Hypertension- should be controlled. Preferably use ACEIs or CCB, like
amlodipine
✓ Concomitant coronary artery disease (CAD) is common, especially in the
elderly. Thus, look for possible evidence of CAD and treat
❖ For symptomatic patients- goals include
✓ Treat concurrent cardiovascular conditions, like coronary artery disease
✓ Prevent or treat superimposed diseases that often exacerbate the effects
of valve obstruction, like HTN
✓ Maintain optimal loading conditions
✓ Treat symptoms
☛ CHF- start Lasix 40mg po BID/TID and escalate till the
congestion improves
☛ Exertional angina and syncope - advice patients to avoid exertion
✓ Patients with depressed EF (LVEF <40%)
✓ Refer to the management of HFrEF guideline and start drugs that have
mortality benefits
❖ Endocarditis prophylaxis- not indicated
❖ Indications for surgical intervention- - patients who can afford and have the
following indications should be referred early to undergo aortic valve
replacement
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✓ Symptomatic severe AS
✓ Severe AS with LVEF <50%
✓ Moderate AS with concomitant coronary artery disease requiring
bypass graft surgery

Reading assignment
Tricuspid stenosis (TS)
Pulmonic stenosis (PS)
Pulmonic Regurgitation (PR)
Multiple and Mixed VHD

1.4 Atherosclerotic cardiovascular diseases

1.4.1 Ischemic heart disease (IHD)


IHD is a condition in which there is an inadequate supply of blood and oxygen
to a portion of the myocardium
Typically occurs when there is imbalance between myocardial oxygen supply
and demand
Commonly caused by atherosclerosis of epicardial coronary arteries
IHD is the leading cause of death and disability in the developed world
The prevalence IHD in developing countries is increasing due to urbanization
and increased adoption of western type diets

Pathophysiology
Determinants of myocardial oxygen demand
✓ Heart rate
✓ Myocardial contractility, and
✓ Myocardial wall tension
Determinants of myocardial oxygen supply
✓ Inspired fraction of oxygen
✓ Pulmonary function
✓ Hemoglobin concentration and function
✓ Adequate level of coronary blood flow
☛ Any mismatch between the above factors could result in myocardial
ischemia/infarction

Causes

❖ Atherosclerosis
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❖ Vasospasm (Prinz metal’s angina)


❖ Arterial thrombi
❖ Coronary emboli
❖ Aortitis
❖ Congenital anomalies- the origin of the left anterior descending coronary artery
from the pulmonary artery
❖ Severe anemia or the presence of carboxyhemoglobin
❖ Increased oxygen demand e.g. - LVH
❖ Two or more causes of ischemia often coexist in a patient e.g. - LVH due to
HTN and atherosclerosis

Coronary atherosclerosis

Atherosclerosis is the narrowing and stiffening of vessels due to


abnormal deposition of atherosclerotic plaque composed of fatty streak,
smooth muscle cells, fibroblasts, and intercellular matrix
When a stenosis reduces the diameter of an epicardial artery by 50%,
there is a limitation of the ability to increase flow to meet the increased
myocardial demand
When the diameter is reduced by ~80%, blood flow at rest may be
reduced and symptoms of angina occur at rest
Clinical manifestations depend on
o Location of obstruction
o Severity of obstruction
o Tempo of onset- acute Vs chronic obstruction

Risk factors for atherosclerosis

Nonmodifiable risk factors


o Male sex
o Age: male > 45 yrs, females > 55
o Family history of premature ischemic heart disease in first
degree relative: male < 55 yrs, females < 65
Modifiable risk factors
o Cigarette smoking
o HTN
o DM
o Dyslipidemia- high LDL and low HDL
o Obesity
o Atherogenic diet: high fat diet
o Alcohol intake
o Physical inactivity

Spectrum of presentation of IHD


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Asymptomatic
o Silent myocardial ischemia
Sudden cardiac death
Ischemic cardiomyopathy
Stable angina pectoris
Acute coronary syndrome (ACS)
o Unstable angina (UA)
o Non-ST segment elevation myocardial infarction (NSTEMI)
o ST-segment elevation myocardial infarction (STEMI)

Stable angina pectoris

Due to transient myocardial ischemia


Characterized by episodes of chest discomfort, usually described as
heaviness, pressure, or squeezing with Levine’s sign
✓ Typically associated with exertion or emotion, and relieved by rest
and nitroglycerin
✓ Usually crescendo-decrescendo in nature
✓ Typically lasts 2-5 minutes
✓ Radiates to either shoulder, both arms, back, interscapular region,
roof of neck, jaw, teeth, and epigastrium
✓ Rarely localized below the umbilicus or above the mandible and
doesn’t radiate to the trapezius muscles
Women, elderly, and diabetic patients can have atypical angina or angina
equivalents such as dyspnea, nausea, fatigue, and faintness

Pain characteristics more typical of nonischemic chest discomfort

Pleuritic pain- sharp or knifelike pain related to respiratory mov’t or cough


Primary or sole location in the mid or lower abdomen
Any discomfort localized with one finger
Reproduced by mov’t or palpation
Constant pain lasting for days
Fleeting pain lasting for seconds or less
Pain radiating into the lower extremities or above the mandible

Differential Diagnosis for chest pain


✓ Heart, pericardium, vascular causes:
❖ Stable angina, variant angina
❖ Acute Coronary Syndrome (ACS)
❖ Pericarditis
❖ Aortic dissection
✓ Pulmonary:
❖ Pulmonary embolism
❖ Pneumothorax
❖ Pleuritis (pleural pain)
❖ Pneumonia
❖ Status asthmaticus
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✓ Gastrointestinal:
❖ Gastroesophageal reflux disease (GERD)
❖ Peptic ulcer disease (PUD)
❖ Diffuse esophageal spasm
❖ Esophageal rupture
✓ Chest wall:
❖ Costochondritis
❖ Muscle strain
❖ Rib fracture
❖ Herpes zoster
✓ Psychiatric:
❖ Panic attacks
❖ Anxiety
❖ Somatization

1.4.1.1 Acute coronary syndrome (ACS)

❖ ACS describes a group of clinical entities that are characterized by severe,


acute myocardial ischemia or infarction resulting from thrombotic occlusion
of coronary artery/arteries as a result atherosclerotic plaque erosion/rupture.
❖ Rarely, the ischemia could be due to coronary artery spasm.

CLASSIFICATION OF ACS

ACS comprises the following 3 clinical entities:

1. Unstable angina:
2. ST-segment elevation myocardial infarction (STEMI):
3. Non-ST-segment elevation myocardial infarction (NSTEMI):

Figure; Acute coronary syndromes. Following disruption of a vulnerable plaque, patients experience
ischemic discomfort resulting from a reduction of flow through the affected epicardial coronary artery.
The flow reduction may be caused by a completely occlusive thrombus ( right) or sub totally occlusive
thrombus (left). Patients with ischemic discomfort may present with or without ST-segment elevation.
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Of patients with ST-segment elevation, the majority (wide red arrow) ultimately develop a Q wave on
the ECG (Qw MI), while a minority (thin red arrow) do not develop Q wave and, in older literature,
were said to have sustained a non-Q-wave MI (NQMI). Patients who present without ST-segment
elevation are suffering from either unstable angina or a non-ST-segment elevation MI (NSTEMI)
(wide green arrows), a distinction that is ultimately made based on the presence or absence of a
serum cardiac biomarker such as CK-MB or a cardiac troponin detected in the blood. The majority of
patients presenting with NSTEMI do not develop a Q wave on the ECG; a minority develop a Qw
MI (thin green arrow).

Definitions of ACS

Combination of symptoms of myocardial ischemia, ECG abnormalities, and


rising or falling pattern of cardiac biomarkers
STEMI- ≥2mm of ST segment elevation in leads V2-V3 and >1mm
elevation in the other two contiguous leads
✓ New or presumably new LBBB pattern
NSTEMI- symptoms of myocardial ischemia and positive cardiac biomarkers

1. Unstable Angina and NSTEMI

Unstable angina is considered to be present in the following


circumstances:
✓ Angina at rest which is >20 minutes in duration
✓ Severe and New onset angina (within the prior 4-6 weeks)
✓ Increasing angina- increasing frequency, longer in duration, or
occurs with less exertion than previous angina (increasing intensity
of chest pain).
Symptoms of myocardial ischemia (typical or atypical) but no elevation in
cardiac enzymes, with or without ECG changes indicative of ischemia.
The distinction between unstable angina and NSTEMI is based entirely on
cardiac enzymes. The latter has elevation of troponin or creatine
kinase-MB (CK-MB). Both unstable angina and NSTEMI lack ST-segment
elevations and pathologic Q waves.
The diagnosis of NSTEMI is established if a patient with clinical features of
UA develops evidence of myocardial necrosis, as reflected in elevated
cardiac biomarkers
Unstable angina has a higher risk of MI and death than stable angina,
and patients with this diagnosis should be hospitalized.

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Table; summary of ACS types


Differentiating features Unstable angina NSTEMI STEMI
ST segment NO ST-segment elevation or Has ST-segment elevations
pathologic Q waves. and/or pathologic Q waves.
Cardiac enzymes No elevation in Has elevation of troponin or creatine kinase-MB
cardiac enzymes (CK-MB)

Pathophysiology

Four pathophysiologic processes may contribute to the development of


UA/NSTEMI
1. Plaque rupture or erosion with a superimposed nonocclusive
thrombus
2. Dynamic obstruction e.g. vasospasm
3. Progressive mechanical obstruction
4. Increased myocardial oxygen demand
More than one of the above processes can be involved
Patients with UA/NSTEMI frequently have multiple plaques at risk of
disruption

Figure; Plaque rupture, thrombosis, and healing

A. Arterial remodelling during atherogenesis


B. Rupture of the plaque's fibrous cap causes thrombosis.
C. When the clot overwhelms the endogenous fibrinolytic mechanisms, it
may propagate and lead to arterial occlusion
D. The subsequent thrombin-induced fibrosis and healing causes a
fibroproliferative response that can lead to a more fibrous lesion that
can produce an eccentric plaque that causes a hemodynamically
significant stenosis.

Diagnosis

The diagnosis of UA is based largely on the clinical presentation


Perform a diagnostic workup to exclude MI in all patients.
Patients with unstable angina have a higher risk of adverse events during
stress testing. These patients should be stabilized with medical
management before referral for stress testing.

❖ ECG
✓ ST-segment depression
✓ Transient ST-segment elevation
✓ T-wave inversion
❖ Cardiac biomarkers- elevated in NSTEMI
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✓ Cardiac troponin- more specific and sensitive marker of myocardial


necrosis
✓ CKMB
❖ Echocardiography
✓ May show regional wall motion abnormalities
❖ Coronary angiography

2. Acute Myocardial Infarction (STEMI and NSTEMI)

MI is due to necrosis of myocardium as a result of an


interruption of blood supply (after a thrombotic occlusion of a
coronary artery previously narrowed by atherosclerosis).
Most cases are due to acute coronary thrombosis: Atheromatous
plaque ruptures into the vessel lumen, and thrombus forms on
top of this lesion, which causes occlusion of the vessel.

A. ST-segment elevation myocardial infarction (STEMI):


✓ Significant ST elevation or new left bundle branch block (LBBB) on
ECG, elevated cardiac enzymes (Troponin and/or CKMB) and
symptoms of myocardial ischemia (typical or atypical).
B. Non-ST-segment elevation myocardial infarction (NSTEMI):
✓ No ST elevation on ECG (other ECG evidence of ischemia
may or may not be present), elevated cardiac enzymes and
symptoms of myocardial ischemia (typical or atypical).

ST-segment elevation myocardial infarction (STEMI)


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Clinical Features

❖ Up to 50% of cases have precipitating factors( e.g. vigorous physical


exercise, emotional stress, or a medical or surgical illness)
❖ The time of onset of STEMI has a pronounced circadian periodicity, with
peak incidence of events between 6 AM and noon
✓ Increase in cathecolamine and cortisol level
✓ Increase in platelet aggregability
❖ Despite advances in the laboratory detection of STEMI, the patient's history
remains crucial to establishing a diagnosis
❖ Chest pain
✓ The pain of STEMI varies in intensity; in most patients it is severe
and, in some instances, intolerable
✓ Patients often describe the pain as heavy, squeezing, and crushing
and “an elephant standing on my chest.” although occasionally it is
described as stabbing or burning
✓ The duration of the pain is prolonged, usually lasting > 30 minutes
and frequently for a number of hours
✓ Typically, the pain involves the central portion of the chest and/or the
epigastrium, and on occasion it radiates to the arms. Less common
sites of radiation include the abdomen, back, lower jaw, and neck,
commonly to the left side.
✓ The pain may commence when the patient is at rest, but when it
begins during a period of exertion, it does not usually subside with
cessation of activity, in contrast to angina pectoris
✓ It is often accompanied by weakness, sweating, nausea, vomiting,
anxiety, and a sense of impending doom
❖ Some patients may have epigastric discomfort.
❖ Atypical presentations of STEMI include the following:
✓ Heart failure (i.e. dyspnea without pain beginning de novo or
worsening of established failure)
✓ Classic angina pectoris without a particularly severe or prolonged
episode
✓ Atypical location of the pain
✓ CNS manifestations, resembling those of stroke, secondary to a sharp
reduction in cardiac output in a patient with cerebral arteriosclerosis
✓ Apprehension and nervousness
✓ Sudden mania or psychosis
✓ Syncope
❖ Silent STEMI: Can be asymptomatic in up to one-third of patients;
painless infarcts or atypical presentations more likely in postoperative
patients, the elderly, diabetic patients, patients without antecedent angina
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❖ The prognoses of patients with silent and symptomatic presentations of


STEMI appear quite similar
❖ Angina equivalents- dyspnea, excessive fatigue, diaphoresis, indigestion
should raise the suspicion of ACS in these patients

P/E

❖ Anxious, restless and may be in cardiopulmonary distress


❖ Heart rate can vary from a marked bradycardia to a rapid regular or
irregular tachycardia
❖ Mostly normotensive
❖ Fever
❖ Bilateral basal rales
❖ Raised JVP
❖ Quiet precordium, and the AI may be difficult to palpate
❖ S3 and S4 gallop
❖ Murmur of MR and friction rub
☛ N.B. Right ventricular infarct will present with inferior ECG changes,
hypotension, elevated jugular venous pressure, hepatomegaly, and clear
lungs.

Killip classification of acute MI

Class I - No evidence of HF
Class II - Findings consistent with mild to moderate HF (S3, lung rales
less than one-half way up the posterior lung fields, or jugular venous
distension)
Class III - Overt pulmonary edema (click and see 1.10.2 Pulmonary edema)
Class IV - 3.2. Cardiogenic shock (pump failure) (click and see the respective
topic)

Diagnosis of STEMI

❖ ECG: Markers for ischemia/infarction include:


o ST-segment elevation: indicates transmural injury and can be
diagnostic of an acute infarct.
o ST-segment depression: Subendocardial injury
o T-wave inversion is sensitive but not specific
o Peaked T waves: Occur very early and may be missed
o Q waves: Evidence for necrosis (specific).
❖ Cardiac enzymes: currently the diagnostic gold standard for myocardial
injury
o Troponins (Troponin I and T): most important enzyme test to order 77
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o CK-MB: less commonly used


o Cardiac enzymes are drawn serially: once on admission and every
6 hours until three samples are obtained. The higher the peak and
the longer enzyme levels remain elevated, the more severe the
myocardial injury and the worse the prognosis.

Other IX

✓ Cardiac imaging: ECHO, Cardiac MRI and angiography, radionuclide imaging


techniques
✓ CBC with platelet count
✓ PT, aPTT and INR
✓ Electrolytes
✓ BUN & Creatinine
✓ RBS
✓ Serum lipid profile
✓ Non specific indices of tissue necrosis and inflammation

COMPLICATIONS OF STEMI
Mechanical
▪ Rupture of the left ventricular free wall
▪ Rupture of IVS
▪ MR
▪ Left ventricular dysfunction
▪ LV aneurysm
▪ Pericarditis
Electrical complications
▪ Arrhythmias
Complications which can be as a result of both mechanical and electrical
disturbances
▪ Heart failure
▪ Cardiogenic shock
▪ Thromboembolism

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Management of ACS

Let’s show you order sheet example for ACS mgt in our set up before going to
detailed management principles → it may be different based on your patient age,
comorbid conditions and complications.

Treatment
New order
❖ Secure double IV line
❖ Put on 100% O2 (if SPO2 is < 95%). E.g. Put on 1L/min of INO2
❖ strict bed rest
❖ Keep NPO and Put on MF
❖ Nitroglycerin, 0.4 mg, Sublingual, Q5min, for 3 doses
❖ Morphine 2mg, IV, every 5min or pethidine 25mg, IV, PRN (if pain refractory to
nitrate therapy alone)
❖ Aspirin, 325 mg, PO, Loading then 81mg (81-100 mg), PO, daily
❖ Clopidogrel, 300 mg, PO, Loading followed by 75 mg, PO, daily
❖ UFH, 5000 IU (60 IU/kg), IV, loading, followed by 17,500 IU (250 IU/kg), SC,
BID, (for 5-7 days until ambulation starts)
❖ Consider Warfarin, 2mg, PO, daily for 2 days based on CHA2DS2- VASc score
❖ Metoprolol tartrate, 50 mg, PO, BID
❖ Atorvastatin 80 mg, PO, daily
❖ Enalapril 2.5 mg, PO, BID
❖ Spironolactone, 12.5mg, PO, daily
❖ Omeprazole, 20mg, PO/via NG tube, BID
❖ Follow Vital sign strictly

Dr. Mulualem. G (GP)

At discharge
→ Give a drug for two weeks to a month then Appoint to Chronic OPD
➢ Metoprolol succinate, 100 mg, PO, daily Life long
➢ Aspirin, 81mg, PO, daily Life long
➢ Clopidogrel, 75 mg, PO, daily for 2 weeks up to 1 year (see below)
➢ Atorvastatin 40 mg, PO, daily for lifelong
➢ Enalapril 2.5 mg, PO, BID, Life long
➢ Spironolactone, 12.5mg, PO, daily, Life long

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Early referral to the high-level facility or urgent specialist consultation is


recommended

Approach to Treating a Patient with Chest Pain

Rule out any life-threatening causes. These include


✓ ACS
✓ Aortic dissection
✓ Pericarditis with cardiac tamponade
✓ Pulmonary embolus
✓ Tension pneumothorax
✓ Esophageal rupture
Assess vital signs
Develop a focused history and P/E
Investigation: focused
✓ ECG in almost all cases
✓ Cardiac enzymes (CK, CK-MB, troponin) depending on clinical
suspicion
✓ CXR in a supportive clinical data
✓ Under appropriate clinical setting, work up the patient for pulmonary
embolism (PE)

Non pharmacologic

Categorize patients based on the above evaluation (see the above table)
✓ Patients with high and intermediate likelihood of ACS should be
admitted to the medical ICU and managed according to ACS
management protocol
✓ Patients with low likelihood of ACS can be discharged from the ED
with advice to come early if they have similar chest pain
☛ Manage the possible cause of the current complaint
Hospital admission and strict bed rest with continuous cardiac monitoring
(ECG monitoring).
❖ Absolute bed rest for 12hrs
❖ Movement only around the bed after 48hrs
❖ Movement to toilet and less than ordinary activities after 72hrs
❖ Avoid strenuous activities for 2 weeks
Establish IV access and obtain blood for troponin, electrolytes, coagulation
profile, RFT.
NPO and fluid diet for the 1st 12hr’s
Give supplemental oxygen if patients are hypoxic (Spo2 <90 %).
UA/NSTEMI requires medical management while STEMI or New LBBB
requires revascularization therapy using PCI or thrombolytics.
o If Primary PCI not available, or is delayed >120 min, use
thrombolytics after ruling out any contraindications
o Streptokinase 1.5 million U in 50 mL of 5% dextrose in water
(D5W) given IV over 60 minutes

Pharmacologic
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Medical Management includes antiplatlets, antischemic, anticoagulants and


cardiac anti-remodeling drugs
o Antiplatelets
▪ Aspirin (ASA)
▪ Clopidogrel
o Anti-ischemics
▪ Nitroglycerin
▪ Morphine
▪ Beta blockers like Metoprolol
▪ Statins
o Anticoagulants
▪ UFH
▪ Warfarin
o Cardiac anti-remodeling
▪ ACE I/ ARB
▪ Spironolactone
o Others
▪ Omeprazole

Glucose and electrolytes


➢ Keep RBS level b/n 140-180 mg/dl (use the protocol for
management of blood glucose in critical patients)
➢ Keep serum K+ level > 4 meq/l
Provide pain control:
o Nitroglycerin: short acting (sublingual or spray):
▪ 3 doses of sublingual nitroglycerine (0.4 mg) for persistent
chest pain every 5 minutes if no hypotension or RV infarction
▪ Patients should be advised to take 1 dose promptly in
response to chest pain. If pain is unrelieved or worsened 3 to
5 minutes after 1 dose, call cardiac emergency team
immediately
▪ Don’t give nitrates for patients who took phosphodiesterase
inhibitors (sildenafil)
o Morphine 2 - 5 mg IV every 5-15 min if pain refractory to nitrate
therapy alone. (C/I: hypotension) then 5mg, IV, QID and PRN
✓ Alternative; pethidine 25-50 mg IV as needed weaker than
morphine
o For patients with continuous or recurrent chest pain despite the above
treatment, IV nitroglycerine infusion should be given in the absence
of contraindications
▪ 5 µg/minute, increase by 5 µg/minute every 3 to 5 minutes to
20 µg/minute. If no response at 20 µg/minute, may increase
by 10 to 20 µg/minute every 3 to 5 minutes (maximum dose:
400 µg/minute) 82
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Dual antiplatelet therapy:


✓ ASA 325 mg loading (Advice to chew the tablet right away)
followed by 81-100 mg (usually 81mg) Po daily lifelong
(commonly used in our setup)
PLUS
✓ Clopidogrel
o UA/NSTEMI:
▪ Initial: 300 mg or 600 mg loading dose, followed by 75
mg once daily for up to 12 months in combination with
aspirin, followed by aspirin indefinitely
o STEMI receiving fibrinolytic therapy (in combination with
aspirin and appropriate anticoagulant)
▪ Age ≤75 years: Loading dose of 300 mg followed by
75 mg once daily for at least 14 days up to 1 year (in
the absence of bleeding).
▪ Age >75 years: 75 mg once daily (no loading dose) for
at least 14 days up to 1 year (in the absence of
bleeding).
β-Blockers:
o Beta-blockers should be initiated within the first 24 hours post
myocardial infarction and continued indefinitely for most patients
✓ Metoprolol; Metoprolol tartrate is short acting form, which is
preferred as initial management for ACS. Metoprolol succinate is long
acting form
☛ Metoprolol tartrate (Immediate release): 50 mg, PO, BID;
usual dosage range: 50 to 200 mg, PO, BID; may increase
dose at weekly intervals to desired effect (maximum: 400
mg/day).
☛ Metoprolol succinate (Extended release): Initial: 100 mg, PO,
daily; may increase dose at weekly intervals to desired effect
(maximum: 400 mg/day).
✓ Alternative; atenolol 25 - 50mg, PO, BID

❖ Beta blockers should be escalated if no heart failure, hypotension,


bradycardia, or active obstructive air way disease
❖ If β-Blockers are C/I due to obstructive airway disease use
Verapamil 80-120 mg, PO, TID
❖ β-Blockers have cardiac remodeling effect

Anticoagulation using Heparin (duration of therapy is for 5-7 days until


ambulation starts)
✓ Enoxaparin
o Patients <75 years of age: Initial: 30 mg IV single bolus plus
1 mg/kg (maximum: 100 mg for the first 2 doses only) SC,
BID.
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▪ The first SC dose should be administered with the IV


bolus. Maintenance: After first 2 doses, administer 1
mg/kg Sc, BID
o Patients ≥75 years of age: Initial: 0.75 mg/kg, SC, BID (Note:
No IV bolus is administered in this population); a maximum
dose of 75 mg is recommended for the first 2 doses.
▪ Maintenance: After first 2 doses, administer 0.75 mg/kg
SC, BID
✓ Alternative: UFH 5000 IU (60 IU/kg), IV loading followed by 250
IU/kg (17,500 IU), SC BID
☛ If infuser is available give maintenance dose 12U/Kg/hr IV
continuous infusion.
Other therapies
a. Statin
❖ High intensity statin therapy; for Age ≤ 75 years
✓ Atorvastatin 80 mg PO daily; if unable to tolerate,
may reduce dose to 40 mg once daily
✓ Alternative; rosuvastatin 20 to 40mg PO, daily
❖ Moderate-intensity statin therapy; for age > 75 years or not
a candidate for high intensity therapy
✓ Atorvastatin 10 to 20 mg PO daily
✓ Alternative;
o Rosuvastatin 20 to 40mg PO, daily or
o Simvastatin 20 to 40mg PO, daily
▪ Low intensity is used to decrease statin induced myopathy in
old age

b. ACEIs in the absence of C/I or ARBs in ACEI intolerant


✓ ACEIs
o Note: In those patients with STEMI in the anterior
location, heart failure, or LV ejection fraction ≤ 40%, an
ACE inhibitor (eg, captopril) should be initiated within
the first 24 hours after MI

o Enalapril 2.5 mg, PO, BID titrated as tolerated to target


dose of 10 mg, PO, BID (maximum: 20 mg/day) or
o Captopril Initial: 6.25 mg; if tolerated, follow with 12.5
mg, PO, TID; then increase to 25 mg, PO, TID during
next several days and then gradually increase over
next several weeks to target dose of 50 mg, PO, TID
▪ some dose schedules are more aggressive to
achieve an increased goal dose within the first
few days of initiation.
✓ ARBs
o Candesartan 4mg BID escalated
o Note: Concurrent therapy with an ACE inhibitor may
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provide additional benefit in patients with HF with


reduced EF who remain symptomatic on standard
therapy and are unable to receive an aldosterone
antagonist
c. Aldosterone antagonists for those with LVEF < 40%, are already on
ACE - I and either HF or DM in absence of hyperkalemia and renal
failure
▪ Spironolactone, 12.5 to 25 mg, PO, daily; maximum: 50 mg/day
▪ Note: withhold treatment if potassium >5.5 mEq/L or renal
function worsens (serum creatinine >4 mg/dL); hold doses until
potassium is <5 mEq/L and consider restarting with a reduced
dose after confirming resolution of hyperkalemia/renal
insufficiency for at least 72 hours
d. Oral anticoagulation(warfarin) for those at high risk of
thromboembolization
☛ Atrial fibrillation with CHA2DS2- VASc > 1, LV thrombus
☛ Considered in patients with poor LV function and apical
hypokinesis
☛ Warfarin; Start 2 to 5 mg, PO, daily for 2 days; lower doses
(e.g. 5 mg once daily)

▪ For CHA2DS2- VASc and HAS-BLED score in patients with


atrial fibrillation, supratherapeutic INR (Management of warfarin-
associated bleeding) click here → Arrhythmia

e. GI prophylaxis and bowel care:


▪ Omeprazole 20 mg po BID routine and
▪ Laxatives for constipation
• Bisacodyl 5 to 15 mg, PO, daily or
• Lactulose, 15 to 30 mL (10 to 20 g or 1 to 2 packets),
PO, daily; may increase to 60 mL (40 g or 2 to 4
packets) daily if necessary

Follow up (Cardiac Monitoring for a Patient with an Acute MI)


➢ BP and PR
➢ Rhythm strip with continuous cardiac monitor: Watch for arrhythmias.
i.e All patients with ACS should be on continuous ECG monitoring
with arrhythmia high priority alarm setup.
➢ Monitor patient’s condition & assess treatment response (pain, ECG,
cardiac enzymes)
o Vital signs: Every 15 minutes until stabilization
o Cardiac markers (troponin levels): every 6 hours if not confirmed
o Manage chest pain: administer nitroglycerine, if no response or
nitroglycerine is contraindicated give morphine
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➢ Auscultate the heart (S3 & S4 gallops, friction rub, and so on) and
lungs (crackles may indicate LV failure, pulmonary edema).
➢Follow for chest pain or angina equivalent symptoms
➢Take ECG every day for at least 3 days→ evolutionary changes (degree of ST
elevation, Q waves)
➢Echocardiography: LV function, wall motion abnormality, LV thrombus
➢Watch for mechanical and electrical complications (the most feared cxn of ACS
is arrythmia)
➢Watch for bleeding in patients at high risk for bleeding
➢Blood sugar should be maintained at 140- 180mg/dl

Preparation for discharge


➢ Ambulation: hemodynamically stable and no chest pain for 12-24
hrs
➢ Discharge after a minimum of 5 days of admission can be
considered if
✓ Pt is hemodynamically stable and no signs of mechanical or
electrical complications
✓ No sign of ongoing ischemia (no chest pain, new ECG
changes and troponin level decreasing)
✓ Pt is able to ambulate without symptoms
Long term medications
➢ ASA, B blockers, ACEIs/ARBs, aldosterone antagonists, and statin
should be continued lifelong
➢ Clopidogrel should be continued for a minimum of 1 month and
ideally up to 1 year
Risk factor modification:
➢ Optimal treatment of HTN, DM, dyslipidemia, smoking cessation
Return to activities
➢ Most patients with uncomplicated course can return to activities after
2 weeks (avoid strenuous activities including coitus for 2 weeks)
➢ Should be advised to slowly increase the level of exertion watching
for symptoms (e.g. Walking distance)
Finally, all patients who can afford, the option of getting referred to a
cardiac hospital in A.A. for risk stratification with stress ECG and diagnostic
and therapeutic coronary intervention should be given. Hemodynamically
stable patients with no ongoing or recurrent ischemia who are on
appropriate medications can fly with reasonable safety after 2 weeks.
NB. Consult the appropriate risk stratification models for prognostication

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1.4.1.2 Chronic coronary syndrome


Chronic Coronary Syndrome is usually due to atherosclerotic lesions that
narrow the major coronary arteries.
Coronary ischemia is due to an imbalance between blood supply and
oxygen demand, leading to inadequate perfusion.
Stable angina occurs when oxygen demand exceeds available blood supply.

Major risk factors

➢ DM — worst risk factor


➢ Hyperlipidemia — elevated LDL
➢ HTN — most common risk factor
➢ Cigarette smoking
➢ Age (men >45 years; women >55 years)
➢ Family history of premature CAD or MI in first-degree relative: Men <55
years; women <65 years
➢ Low levels of HDL

Less common risk factors include:

➢ End-stage renal disease (ESRD) on hemodialysis,


➢ HIV infection,
➢ History of mediastinal radiation.

Minor risk factors (less clear significance) include:

➢ Obesity
➢ Sedentary lifestyle (lack of physical activity)
➢ Stress
➢ Excess alcohol use

Clinical Features

Chest pain or substernal pressure sensation


✓ Lasts less than 10 to 15 minutes (usually 1 to 5 minutes).
✓ Frightening chest discomfort, usually described as heaviness,
pressure. squeezing, tightness; rarely described as sharp or
stabbing pain.
✓ Pain is often gradual in onset.
✓ Brought on by factors that increase myocardial oxygen demand,
such as exertion, stress, or drugs.
✓ Relieved with rest or nitroglycerin

Diagnosis and investigation

❖ Note that physical examination in most patients with CCS is normal.


❖ Resting ECG:
✓ Usually normal in patients with chronic coronary syndrome
✓ Q waves are consistent with a prior MI 87
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✓ If ST-segment or T-wave abnormalities are present during an


episode of chest pain, then treat as unstable angina.
❖ Stress test:
✓ Useful for patients with an intermediate pretest probability of CAD
based upon age, gender, and symptoms.
✓ Stress testing is used in the following situations:
☛ To confirm diagnosis of angina
☛ To evaluate response to therapy in patients with
documented CCS
☛ To identify patients with CCS who may have a high risk of
acute coronary events

Treatment of CCS

❖ Risk factor modification


☛ Smoking cessation
☛ Blood pressure control
☛ Dyslipidemia management:
☛ Obesity: weight loss modifies other risk factors (diabetes, HTN, and
hyperlipidemia) and provides other health benefits.
☛ Exercise: it minimizes emotional stress, promotes weight loss, and
helps reduce other risk factors.
☛ Diet: Reduce intake of saturated fat and cholesterol

Standard of care for patients with CCS

❖ Antiplatelet therapy
✓ ASA 75-100 mg PO daily
✓ Alternative: Clopidogrel 75 mg Po daily
❖ Beta blocker: chest pain, heart rate and blood pressure control
✓ Metoprolol succinate 25-200 mg PO daily
✓ Alternative: Bisoprolol 2.5-10 mg PO daily
❖ Statin: target LDL< 70 mg/dl, dose of statin titrated as per the response
✓ Atorvastatin 20-80 mg PO daily
✓ Alternative: Rosuvastatin 5-20 mg PO daily
❖ Angina management
✓ Betablockers: see above
✓ Calcium channel blockers
☛ Amlodipine 2.5-10 mg PO daily for those with hypertension
✓ Nitrates
☛ Nitroglycerine 0.4 mg sublingual tablets for acute relief
☛ Isosorbide dinitrate 2.5-20 mg PO single dose or divided
doses as needed
☛ Trimetazidine 35 mg Po daily
❖ Review risk factor, symptoms and indication for revascularization
❖ Refractory cases: Need Cardiologist evaluation

Coronary revascularization

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✓ The presence of unstable phases of the disease


✓ Intractable symptoms despite medical therapy
✓ Severe ischemia or high-risk coronary anatomy
✓ Diabetes
✓ Impaired LV function
Revascularization should be employed in conjunction with but not replace
the continuing need to modify risk factors and assess medical therapy
Two options
✓ Percutaneous coronary intervention (PCI)
✓ Coronary artery bypass grafting (CABG)
Indications for early revascularization
✓ Recurrent angina at rest despite medical Rx
✓ Elevated troponin
✓ New ST-segment depression
✓ Recurrent angina/ischemia with CHF symptoms
✓ Positive stress test
✓ EF < 40 %
✓ Decreased BP
✓ Sustained VT
✓ PCI < 6 months, prior CABG
✓ Multiple risk factors
Revascularization should be combined with medical therapy

What is anterior MI, Inferior MI


and posterior MI? →refer under
short case of Nitsbin (click here
→ Chapter 22; Basics of ECG
and ECG interpretation, 22.6.1
Myocardial Ischemia/infarction)

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1.4.2 Peripheral Arterial Disease (Chronic Arterial


Insufficiency)
Peripheral arterial disease (PAD) is an occlusive atherosclerotic disease of the
lower extremities.
➢ Narrowing of arteries other than those supplying heart (CAD) and Brain
(CVA)
➢ It is an arterial ulcer which commonly affect legs
Patients with PAD usually have coexisting CAD (with CHF, history of MI, and
so on) and other chronic medical problems (e.g., diabetes, lung disease)
Sites of occlusion/stenosis:
o Superficial femoral artery (in Hunter canal) is the most common site
o Popliteal artery
o Aortoiliac occlusive disease

Risk factors
➢ Smoking is by far the most important risk factor
➢ Chronic Coronary Syndrome
➢ Dyslipidemia
➢ Hypertension
➢ Diabetes: prevalence is markedly increased in these patients
➢ Age > 65

Clinical Features

Symptoms:

➢ Intermittent claudication: Cramping leg pain that is reliably reproduced by


same walking distance (distance is very constant and reproducible). Pain
is completely relieved by rest.
➢ Rest pain (continuous): Usually felt over the distal metatarsals, where
the arteries are the smallest. Often prominent at night (awakens patient
from sleep). Hanging the foot over side of the bed or standing relieves
pain (extra perfusion to ischemic areas due to gravity)
o Rest pain is always worrisome: suggests severe ischemia (Critical
limb ischemia) such that frank gangrene of involved limb may occur
in the absence of intervention.

Signs:

➢ Diminished or absent pulses, muscular atrophy, decreased hair growth, thick


toenails, and decreased skin temperature
➢ Ischemic ulceration (usually on the toes)
➢ Cold skin
➢ Localized skin necrosis: Secondary to local trauma that does not heal
(due to ischemic limb)
➢ Tissue infarction/gangrene in end-stage disease
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☛ Bluish skin discoloration which complicate with tissue death and


Amputation
➢ Pallor of elevation and rubor of dependency (in advanced disease)
☛ Burger sign +ve → pallor on elevation of limb and redness while
changing to resting position

Femoral or popliteal disease causes calf claudication.


Aortoiliac occlusive disease causes buttock and hip claudication (in
addition to the calves).

Rutherford and Fontaine symptom classification systems

Rutherford

• Stage Zero (0) → Asymptomatic


• Stage 1 → mild claudication, claudication distance > 200 meter
• Stage 2 → moderate claudication, claudication distance < 200 meter
• Stage 3 → severe claudication.
• Stage 4 → rest pain
• Stage 5 → minor tissue loss with ischemic nonhealing ulcer or focal
gangrene with diffuse pedal ischemia
• Stage 6 → major tissue loss, frank gangrene extending above trans
metatarsal level, functional foot no longer salvageable

Fontaine

➢ Stage 1 – No symptoms
➢ Stage 2 – Intermittent claudication subdivided into:
☛ Stage 2a – Without pain on resting, but with claudication at a
distance of greater than 650 feet (200 meters)
☛ Stage 2b – Without pain on resting, but with a claudication distance
of less than 650 feet (200 meters)
➢ Stage 3 – Nocturnal and/or resting pain
➢ Stage 4 – Necrosis (death of tissue) and/or gangrene in the limb

Diagnosis
Clinical suspicion based on symptoms, signs and risk factors
Ankle-to-brachial index (ABI): Ratio of the systolic BP at the ankle to the
systolic BP at the arm.
𝐒𝐁𝐏 𝐨𝐟 𝐚𝐧𝐤𝐥𝐞
☛ Normal 𝐀𝐁𝐈 = 𝐒𝐁𝐏 𝐎𝐅 𝐁𝐫𝐚𝐜𝐤𝐢𝐚𝐥 𝐚𝐫𝐭𝐞𝐫𝐲
= 𝟎. 𝟗 − 𝟏. 𝟑
☛ SBP of ankle measured by Doppler ultrasound guided BP
measurement. But, SBP of arm can be measured by
sphygmomanometer (by any BP cuff available in the ward)
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☛ ABI < 0.9 is evidence for PAD, ABI >1.3 is due to non-
compressible vessels (vessel wall calcification) and indicates
severe disease
☛ Claudication usually when ABI < 0.7
☛ Rest pain usually when ABI < 0.4
Doppler study of the peripheral vessels
Arteriography (contrast in vessels and radiographs)
o Gold standard for diagnosing and locating PAD

Treatment
Non pharmacologic
Conservative management for intermittent claudication.
➢ Smoking cessation (the importance of this cannot be
overemphasized). Smoking is linked to progression of
atherosclerosis and causes vasoconstriction (further decreasing
blood flow).
➢ Graduated exercise program: Walk to point of claudication, rest,
and then continue walking for another cycle.
➢ Foot care (especially important in diabetic patients).
➢ Avoid extremes of temperature (especially extreme cold).

Pharmacologic
➢ Atherosclerotic risk factor reduction (control of hyperlipidemia,
Hypertension, Diabetes):
➢ Antiplatelets
o ASA 81-100 mg Po daily
o Alternative: Clopidogrel 75 mg Po daily
➢ Statin
o Atorvastatin 20 - 80 mg Po daily
o Alternative: Rosuvastatin 5-20 mg Po daily

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1.4.3 Arterial occlusion (acute limb ischemia)

❖ Acute occlusion of an artery, usually caused by embolization.


❖ Common femoral artery is the most common site of occlusion.
❖ Less commonly, in situ thrombosis is the cause.

Sources of emboli:
Heart (85%)
❖ Atrial fibrillation is the most common cause of embolus from the
heart
❖ Post-MI
❖ Post arterial procedure (i.e., coronary angiogram, peripheral
angiogram)
❖ Endocarditis
❖ Myxoma
Aneurysms
Atheromatous plaque

Clinical Features of Acute Limb Ischemia (Remember the 6 Ps)

❖ Pain: acute onset. The patient can tell you precisely when and
where it happened. The pain is very severe, and the patient may
have to sit down or may fall to the ground.
❖ Pallor
❖ Polar (cold)
❖ Paralysis
❖ Paresthesia’s
❖ Pulselessness

Diagnosis

Clinical: high index of suspicion with supportive clinical data.


Doppler study of the vessels.
ECG to look for MI, AFib
Echocardiogram for evaluation of cardiac source of emboli—valves, thrombus,
shunt

Treatment

❖ Main goal: Assess viability of tissues to salvage the limb.


❖ Skeletal muscle can tolerate 6 hours of ischemia; perfusion should be re-
established within this time frame.
❖ Supportive management
✓ Immediately anticoagulate with IV heparin.
✓ Strong analgesic like morphine for pain
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✓ Positioning and psychological support


❖ Definitive mgt
✓ Bypass versus angioplasty in severe ischemia of the leg (BASIL) trial
✓ Percutaneous intervention (angioplasty, stent) is a less invasive
alternative to surgery
✓ Catheter-based intra-arterial thrombolytic therapy is an alternative to
surgery or percutaneous intervention
✓ Urgent referral to the facility where reperfusion is available in
consultation with specialist.

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1.5 Hypertension (የደም ግፊት) and HHD

Hypertension

Hypertension is a serious medical condition that significantly increases the risks


of heart, brain, kidney and other diseases.
According to the WHO STEPS survey the prevalence of hypertension in
Ethiopia is 16%.
In Ethiopia and other low- and middle-income countries, there is a wide gap
between evidence- based recommendations and current practice.
Treatment of major CVD risk factors remains suboptimal, and only a minority
of patients who are treated reach their target levels for blood pressure, blood
sugar and blood cholesterol.

When to measure blood pressure

➢ Measuring blood pressure is the only way to diagnose hypertension, as


most people with raised blood pressure have no symptoms.
➢ Blood pressure measurements should be conducted on all patients during
health facility visits as part of the vital sign.
➢ The Ministry of Health-Ethiopia recommends all adults are advised to
check their blood pressures. But the focus will be screening all adults
aged ≥ 30 years of age as the yield of getting individuals with raised
blood pressure will be higher based on the National WHO Steps
Survey report and pilot program in Ethiopia.
➢ Every patient with elevated blood pressure readings requires immediate
follow-up, according to the protocol.
➢ More frequent blood pressure measurements and control is particularly
important in adults who:
✓ Have had a prior heart attack or stroke
✓ Have diabetes
✓ Have CKD
✓ Are obese
✓ Use tobacco
✓ Have a family history of heart attack or stroke

How to measure blood pressure

❖ Effective treatment algorithms for hypertension are dependent on accurate


blood pressure measurement.
❖ The following advice should be followed for measuring blood pressure: 95
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✓ Use the appropriate cuff size, noting the lines on the cuff to ensure
that it is positioned correctly on the arm. (If the arm circumference is
>32 cm, use large cuff.)
➢ The arm should be supported at heart level, and the bladder of the cuff
should encircle at least 80% of the arm circumference
✓ On initial evaluation it is preferable to measure blood pressure on
both arms and use the arm with the higher reading thereafter
✓ The patient should be sitting with back supported, legs uncrossed,
empty bladder, relaxed for 5 minutes and not talking.
✓ No caffeine during the hour preceding the reading and no smoking
during the preceding 30 minutes
✓ No exogenous adrenergic stimulants, such as phenylephrine in
decongestants or eye drops for pupillary dilatation
✓ Take at least two readings on each visit, separated by as much time
as possible; if readings vary by more than 5 mmHg, take additional
reading until two consecutive readings are close
✓ For the diagnosis of hypertension, take measurement on at least two
visits ≥ one week apart
✓ Check for postural changes by taking readings after five minutes
supine, then immediately and two minutes after standing - this is
particularly important in patients over age 65, diabetics, or those
taking antihypertensive drugs
✓ Blood pressure can be measured either by a conventional
sphygmomanometer (Aneroid or mercury), using a stethoscope, or by
an automated electronic device. The WHO recommended calibrated
electronic device, if available, is preferred because it provides more
reproducible results and is not influenced by variations in technique
or by the bias of the observers.

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Figure: How to measure blood pressure

Diagnosing hypertension

❖ The diagnosis of hypertension should be confirmed at an additional patient


visit, usually 1 to 4 weeks after the first measurement depending on the
measured values and other circumstances.
❖ In general, hypertension is diagnosed if, on two visits, on different days:
✓ Systolic blood pressure on both days is ≥140 mmHg and/or diastolic
blood pressure on both days is ≥90 mmHg.

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Table; Classification of Hypertension and Recommended Management4


Category Systolic (mmHg) Diastolic(mmHg)
Normal <130 And <85
High Normal 130-139 and/or 85-89
Grade 1 140-159 and/or 90-99
Grade 2 160-179 and/or 100-109
Grade 3 ≥180 and/or ≥110
(Severe)
Isolated Systolic >140 and <90
Hypertension
(age >60yr)
Hypertension SBP > 180 mmHg and/or DBP > 110 mmHg in an
Urgency otherwise stable person without clinical or laboratory
evidence of acute target organ damage
Hypertension SBP > 180 mmHg and/or DBP > 110 mmHg
Emergency with the presence of acute target organ damage
➢ Dissecting aortic aneurysm
➢ Acute pulmonary edema
➢ Acute myocardial infarction
➢ Unstable angina pectoris
➢ Acute renal failure
➢ Acute intracranial hemorrhage
➢ Acute ischemic stroke
➢ Hypertensive encephalopathy
➢ Eclampsia or pre-eclampsia

4
NATIONAL NONCOMMUNICABLE DISEASES MANAGEMENT PROTOCOLS, November 2021,
98
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Figure: Initiation of blood pressure-lowering treatment (lifestyle changes and medication)


at different initial office blood pressure levels. BP = blood pressure; CAD = coronary artery
disease; CVD = cardiovascular disease; HMOD= hypertension-mediated organ damage.

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Diagnosis of hypertension

Previously Currently# 5

Stage Value Stage Value

Normal <120/80 mmHg Normal <120/80 mmHg

Pre hypertension 120 − 139 Elevated 120 − 129


80 − 89 < 80

Stage I HTN 140 − 159 Stage I HTN 130 − 139


90 − 99 80 − 89

Stage II HTN 160 − 179 Stage II HTN ≥140/90 mmHg


100 − 109

Hypertensive urgency ≥180/110 mmHg

Hypertensive ≥180/110 mmHg with end organ damage


emergency

Isolated systolic ≥140/ <90


hypertension*

# In our setup we are still using the previous staging system for clinical purpose
* Isolated systolic hypertension is common in old age

Clinical Condition Office Blood Pressure Measurement

< 140/90 140-159/90- 160-179/100- >180/110


99 109

If there is no evidence of end-organ Re-measure Confirm in Confirm as Diagnose HTN and refer to
damages after 1year one Month soon as specialist
possible
within one
week

If there is evidence of end-organ damages Confirm HTN and refer to specialist

Hypertensive Crises (BP> 180/110 mmHg)


with or without target organ damage

5
Reference; UpToDate, © 2018, version 2.0
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Once diagnosis of hypertension is made: Look for end-organ damage based on:

❖ History:
o Symptoms of heart failure (SOB, unusual fatigue and body swelling)
o History of sudden onset body weakness (stroke)
o Intermittent claudication or previous diagnosis of the above problems
on previous evaluation at other health institution
o Severe headache and blurring of vision.
❖ Physical Examination:
o Pulse rate and rhythm
o Signs of heart failure (edema, elevated JVP, crackles on the lungs)
o Focal neurologic deficit, eye signs.
o The physical examination should be done to the maximum capacity of
the health work force including fundoscopic retinal examination if
possible.
❖ Laboratory and other diagnostic tests:
o Waiting for laboratory tests shouldn’t delay the intervention of
hypertension as the disease do much harm than the extra benefit
obtained from the tests.
o The tests are categorized as follows:
✓ Mandatory tests at diagnosis (urine dipstick to check for protein,
Creatinine to check for renal function)
✓ Optional tests at diagnosis (ECG to look for effect of blood pressure
on the heart, Serum electrolytes mainly potassium, TFT to assess a
secondary cause of hypertension)
✓ Indication based tests (Echocardiography for heart failure patients,
brain imaging for suspicion of stroke)
✓ Comorbidity and risk factor assessment tests (Blood sugar and
cholesterol)
❖ Look for risk factors:
o History: Smoking, excess salt intake, sedentary life, low fruit and
vegetable intake, excess alcohol consumption
o Physical Measurement: Weight, height, abdominal circumference,
Calculate BMI:
❖ Cardiovascular Risk assessment; (click here → WHO risk based CVD
(Cardiovascular disease) Management in Ethiopia)
o More than 50% of hypertensive patients have additional CV risk
factors. Most commonly: metabolic syndrome, T2DM, lipid disorders,
high uric acid.
o For all patients found to have raised BP, their future 10-year
cardiovascular risk should be assessed by using WHO CV risk
score.
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o In a setting where serum cholesterol and FBS can be determined


use the laboratory-based risk assessment.
o If laboratory assessment service is not available, the non-laboratory-
based risk chart.

Classification of HTN

1. Essential or primary HTN:

❖ A multi factorial disease where no single etiology is identified


❖ Is the commonest type of HTN accounting for 90 – 95 % of the cases
❖ It results from the interaction between genetic predisposition and
environmental factors

2. Secondary HTN

❖ Occurs secondary to an identifiable cause


❖ Accounts for 5 – 10 % of the cases
✓ Renal paranchymal disease
✓ Renovascular hypertension : renal artery stenosis
✓ Primary aldosteronism
✓ Cushing’s syndrome
✓ Pheochromocytoma

RISK FACTORS FOR ESSENTIAL HYPERTENSION

❖ Non-Modifiable risk factor


o Age. The risk of hypertension increases with age. Through early
middle age, or about age 45
o Sex. hypertension is more common in men. Women are more
likely to suffer the condition after age 55.
o Family histroy of hypertension
o Black race
o Genetic
❖ Modifiable (Behavioral risk factors)
o Physical inactivity
o Increased sodium intake
o Low dietary potassium intake.
o Low dietary vitamin D intake
o Excess alcohol intake
o Cigarette smoking
o Obesity
o Stress.
o Dyslipidemia
o Certain personality traits, such as hostile attitudes and time
urgency/impatience
o Pregnancy
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o Other Chronic medical conditions. such as kidney disease and


sleep apnea.

Indications for Work-up for Secondary Hypertension

1. Severe or resistant hypertension → as defined by the persistence


of high BP despite concurrent use of adequate doses of three
antihypertensive agents from different classes.
2. An acute rise in blood pressure developing in a patient with previously
stable values
3. Age < 30 years in non-obese, non-black patients with a negative family
history of and no other risk factors (e.g., obesity) for hypertension
4. Malignant or accelerated hypertension (eg, patients with severe
hypertension and signs of end-organ damage such as retinal
hemorrhages or papilledema, heart failure, neurologic disturbance,
or acute kidney injury).
5. Proven age of onset before puberty
6. If there are other findings that specifically suggest renovascular or
other forms of secondary hypertension

Hypertension based on ambulatory BP monitoring

✓ A 24 hr mean of ≥ 125/75 mmHg


✓ Day time (awake) mean of ≥ 130/80 mmHg
✓ Night time (asleep) mean of ≥ 110/65 mmHg
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Acute and chronic complications of hypertension


➢ Heart failure:
➢ Coronary artery disease
➢ Stroke
➢ CKD
➢ Peripheral arterial disease and aneurysms
➢ Eye disease (hypertensive retinopathy)
➢ Impaired Cognitive function

Special types of Hypertension

A. Isolated systolic hypertension

➢ Isolated systolic hypertension can be caused by underlying conditions such as


✓ Vascular stiffness
✓ Heart valve problems or
✓ An overactive thyroid (hyperthyroidism).
➢ It is a condition commonly observed in the elderly.
➢ Systolic BP has significant prognostic importance and is also regarded
by some as the most important modifiable cardiovascular risk factor in the
elderly.
➢ Isolated systolic hypertension can lead to serious complications, such as:
stroke, heart disease and CKD.
➢ It should therefore be diagnosed and treated appropriately.
➢ Younger individuals tend to have both systolic and diastolic hypertension but
the level and significance of diastolic blood pressure are higher than elderly
ones.

B. White coat hypertension

➢ Defined as BP that is consistently elevated by office reading only.


➢ In some patients without hypertension, visiting the clinic and measuring BP
may result in a high BP reading (white coat hypertension).
➢ Patients with mildly increased blood pressure (systolic BP 140-160 mmHg
and/or diastolic 90-100 mmHg) at the first visit should have their BP
measurement repeated on at least 2 separate occasions within 2 months to
confirm the diagnosis of hypertension before pharmacological treatment is
considered.
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C. Resistant (to treatment) hypertension → Look at below

Hypertension Treatment
Who should receive hypertension treatment?

➢ Hypertension treatment is indicated for adults diagnosed with hypertension,


as defined above (SBP ≥140 mmHg and/or DBP ≥90 mmHg).
➢ Immediate treatment may be Indicated for adults diagnosed with
hypertension at initial presentation in those with:
o Hypertension mediated organ damage (End-organ damage)
o High WHO CVD risk (Lab based WHO cardiovascular risk
>20% or non-Lab based WHO cardiovascular risk >10%)
o Hypertensive Crises (SBP ≥180 mmHg or DBP ≥110 mmHg)

➢ Lifestyle counseling (healthy diet, physical activity, Cessation of tobacco use


and harmful use of alcohol) is a critical component of good hypertension
management and is often recommended as a first step for patients with
blood pressure of SBP 130–139 mmHg and/or DBP 80–89 mmHg who do
not have other CVD risk factors.
➢ However, in settings where people do not regularly visit the doctor, people
who are recommended only lifestyle modification may not return for re-
evaluation and needed treatment, resulting in uncontrolled hypertension and
associated complications.

Non pharmacologic (Life Style interventions)

All patients diagnosed to have hypertension should be given lifestyle


interventions which include:

o Weight loss: goal BMI 18.5-24.9


o Aerobic exercise: ≥30min exercise/day, ≥5d/week
o Consume healthy diet: Diet rich in fruit and vegetables, low in
saturated and total fat (DASH)
o Reduce salt consumption to less than 1 tea spoonful (5g)/day (i.e. do
not add salt if you are using Ethiopian “berberie” or “Shiro”). No added
salt after food is prepared. Avoid salty foods
o Engage in physical activity
o Avoid smoking and alcohol

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For uncomplicated Grade I hypertension life style intervention can be tried


for 3 months before initiation of medications. If failed to achieve a blood
pressure of less than 140/90 mmHg, then initiation of antihypertensive
medication is recommended.

Pharmacologic (Drug Treatment)


Indications:
❖ Patient who couldn’t achieve target blood pressure with three months
of life style interventions.
❖ At initial presentation in those with:
o Hypertension mediated organ damage (End-organ damage)
o High WHO cardiovascular risk (>10% with non-lab based and
>20% with lab-based WHO risk)
o Hypertensive Crises (SBP ≥180 mmHg or DBP ≥110 mmHg)

➢ Threshold for treatment: all patients including diabetes and CKD


▪ Age <80 years: ≥140/90mmHg
▪ Age >85 years: ≥160/90mmHg
➢ Treatment Goal: all patients including diabetes and CKD
▪ Age <80 years: ≤140/90mmHg
▪ Age >85 years: ≤160/90mmHg
➢ Treatment targets
▪ For most patients, blood pressure is considered controlled when BP
is <140/90 mmHg.

Initial monotherapy in uncomplicated hypertension:


Each class of antihypertensive drugs has been equally effective in
monotherapy trials if the attained blood pressure is similar.
In the absence of a specific indication, the World Hypertension
League and the International Society of Hypertension recommend
three main classes of drugs to be used for initial monotherapy:
o Long acting dihydropyridine calcium channel blockers (such as
amlodipine),
o Thiazide diuretics
o ACE inhibitors or angiotensin II receptor blockers.

Combination therapy

The World Hypertension League and the International Society of


Hypertension recommend the following drugs in a combination
therapy:
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o Long acting dihydropyridine calcium channel blocker plus a


thiazide diuretic,
o Long-acting dihydropyridine calcium channel blocker plus a
long-acting ACE inhibitor/ARB or
o Long-acting ACE inhibitor/ARB plus a thiazide diuretic.
An ACEI and ARB should never be used together in the same patient.
Different antihypertensive medications from the same class should not be
combined.

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Figure: Ethiopia Hypertension Management Algorithm

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1. CCB (Calcium channel blocker)

Long-acting dihydropyridine calcium channel blocker such as amlodipine as


first line drug for the treatment of uncomplicated essential hypertension in
our country.
It is probably effective for all races; reduces need for monitoring of
electrolytes and renal function; avoids need for different treatment for
women of childbearing age who may become pregnant.
☛ Dose: Amlodipine 5 mg daily, escalate to 10 mg if BP is
uncontrolled. Usual dosage range: 5 to 10 mg once daily. Target
dose: 10 mg once daily.
o In general, titrate every 7 to 14 days. Titrate more rapidly,
however, if clinically warranted, provided the patient is
assessed frequently.
Or
☛ Nifedipine (Extended release): Initial: 30 or 60 mg, PO, daily; usual
dosage range: 30 to 90 mg daily; maximum: 90 to 120 mg daily

2. Thiazide diuretics; add on therapy to CCB


Thiazide diuretics such as hydrochlorothiazide to be used as add on when
target BP not achieved on long-acting dihydropyridine calcium channel
blocker such as amlodipine.
It is less expensive than other hypertension medications in our setting and
are probably effective for all races.
Because of the lack of evidence with the readily available thiazide diuretics
such as hydrochlorothiazide as monotherapy with regards to CVD event
reduction, the risk of hypokalemia and the unfavorable effects on lipid and
glucose associated with the drug which necessitates laboratory monitoring,
we suggest to be used as add on.
☛ Dose: Hydrochlorothiazide; Initial: 12.5 to 25 mg, PO, daily; may
increase dose to a target dose range of 25 to 50 mg once daily in
1 to 2 divided doses; usual dosage range: 12.5 to 50 mg daily

3. ACE inhibitors; third agent add on therapy


If a third agent is needed, the alternative class of medication is ACE
inhibitors considering cost of the drug and availability in Ethiopia.
☛ 1st line: Lisinopril, 5 mg, PO, daily (maintained on a diuretic) or 10
mg, PO, daily (not maintained on a diuretic)
o Adjust dose according to blood pressure response. Target
dose; 40 mg, PO, daily; usual dosage range: 10 to 40 mg
daily
o Note: Antihypertensive effect may diminish toward the end of
the dosing interval especially with doses of 10 mg daily. An
increased dose may aid in extending the duration of
antihypertensive effect. Doses up to 80 mg daily have been
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used, but do not appear to give greater effect. If possible,


consider discontinuing diuretics 2 to 3 days prior to initiating
lisinopril; restart diuretic, if needed, after blood pressure is
stable.
☛ 2nd line;
o Enalapril Initial: 5 mg, PO, daily (2.5 mg, PO, daily in patients
taking diuretics); titrate upward, usually at 1- to 2-week
intervals; usual dose range: 10 to 40 mg daily. Target dose:
20 mg daily in 1 or 2 divided doses. Maximum: 40 mg/day.
▪ Note: May add a diuretic if blood pressure cannot be
controlled with enalapril alone.
Or
o Captopril; Initial dose: 25 mg, PO, BID to TID (a lower initial
dose of 12.5 mg, PO, TID may also be considered; may
increase at 1- to 2-week intervals up to 50 mg PO TID;
maximum dose: 450 mg/day
▪ add thiazide diuretic, unless severe renal impairment
coexists then consider loop diuretic, before further
dosage increases or consider other treatment options

4. ARB (Angiotensin II Receptor Blocker;)


Antihypertensive effect usually observed within 2 weeks; maximum
antihypertensive effect seen within 4 to 6 weeks. Dosage must be
individualized. Consider lower initial dosages in volume depleted patients; if
possible, correct volume depletion prior to administration.
➢ Candesartan; Initial: 16 mg, PO, daily; titrate to response; usual range: 8 to
32 mg/day in 1 to 2 divided doses; target dose: 12 to 32 mg daily;
maximum daily dose: 32 mg daily.
Or
➢ Valsartan; Initial: 80 mg or 160 mg, PO, daily (in patients who are not
volume depleted); dose may be increased to achieve desired effect; usual
dosage range : 80 to 320 mg, PO, daily; target dose: 160 to 320 mg, PO,
daily; maximum dose: 320 mg/day.

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Table; Contraindications to antihypertensive medications

Pharmacologic option in Uncomplicated HTN: no end organ damage

First line
✓ Amlodipine/felodipine 2.5-10 mg once daily (escalate 2.5mg every week)
✓ Hydrochlorothiazide 25mg/day
✓ Nifedipine (immediate release) 20-40mg/2-3 times /day
2 line
nd

✓ Enalapril 2.5-40 mg in 2 divided doses


✓ Captopril 12.5-100mg TID
✓ Lisinopril 10-40 mg/day
✓ Candesartan 8-32 mg/day in 1-2 divided doses
Alternative second lines
✓ Beta blockers: selective 𝛽/𝛼 or non-selective e.g. Metoprolol, atenolol,
propranolol, carvedilol
✓ Central acting: methyldopa, clonidine

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Resistant hypertension:

➢ This is defined as BP ≥ 140/90 mmHg despite treatment with at least 3


drugs (including a diuretic) in adequate doses and after exclusion of false
hypertension such as isolated office hypertension and failure to use large
cuffs on large arms.
➢ Causes of resistant hypertension include:
o Poor adherence to therapeutic plan
o Failure to modify life-style including weight gain and heavy alcohol
consumption (binge drinking)
o Continued intake of drugs that raise blood pressure (liquor ice,
glucocorticoids, NSAIDs, etc)
o Obstructive sleep apnoea
o Unsuspected secondary cause
o Irreversible or limited reversibility of organ damage
o Volume overload due to:
▪ Inadequate diuretic therapy
▪ Progressive renal insufficiency
▪ High sodium intake
▪ Hyperaldosteronism

Table: Antihypertensive agents and their common side effects

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Table: Summary of factors other than BP-influencing prognosis


of hypertension;

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1.5.1 MANAGEMENT OF HYPERTENSION IN SPECIAL CLINICAL


CONDITIONS

Background
➢ Hypertensive patients have several comorbidities that can affect
cardiovascular risk and treatment strategies.
➢ The number of comorbidities increases with age, with the prevalence of
hypertension and other diseases.
➢ Common comorbidities include coronary artery disease (CAD), stroke,
CKD, HF, and COPD.
➢ Uncommon comorbidities include rheumatic diseases and psychiatric
diseases.
➢ Common and uncommon comorbidities should be identified and
managed according to available evidence.

Ischemic Cardiovascular Disease and Heart failure


(both ischemic and non-ischemic)

➢ Hypertension is one of the most important risk factors for CAD and
stroke (ischemic or hemorrhagic stroke).
➢ Hypertension is also a risk factor for the development of HF with
reduced ejection fraction (HFrEF), and HF with preserved ejection
fraction (HFpEF).
➢ Clinical outcome is worse, and mortality is increased in hypertensive
patients with HF.
➢ BP should be lowered if ≥140/90 mm Hg and treated to a target of
<130/80 mm Hg (<140/80 in elderly patients).
➢ B-blockers are indicated for all HF patients with >BP 100/60, for HR
>60 beats/minute and with no pulmonary edema.
➢ If LVEF <40 %: ACE inhibitors and spironolactone are prescribed
➢ If there is evidence of Heart failure furosemide should be prescribed
(see heart failure for details)
➢ If BP is still >130/80, non-dihydropyridine CCB’s are prescribed.
➢ Patient with ischemic stroke after acute event: Thiazide diuretic is
preferred initial choice followed by ACEI and CCB’s as third agent.

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Diabetes

➢ BP should be lowered if ≥140/90 mm Hg and treated to a target


<140/90 mm Hg (<130/80 if possible).
➢ Initial antihypertensive choice is similar to non -diabetic patient.
➢ ACEI/ARBs are preferred as second line for all diabetic patients with
HCT as third agent due to concern with raised blood glucose
➢ For proteinuric patient’s initial antihypertensive choice should either be
single agent ACEI/ARB (if BP 130-159/80-99mmHG) or combination of
ACEI/ARB and CCB’s if initial BP is greater than 160/100mmHG.
➢ The treatment should include glucose and lipid lowering as per national
guidelines. (Refer to the national diabetes protocol)

Hypertension and Chronic Kidney Disease (CKD)

➢ Hypertension is a major risk factor for the development and progression


of albuminuria and any form of CKD.
➢ A lower eGFR is associated with resistant hypertension, masked
hypertension, and elevated nighttime BP values.
➢ BP should be lowered if ≥140/90 mm Hg and treated to a target
<140/90 mm Hg (<130/80 if possible).
➢ Furosemide or other loop diuretics are preferred first line agents if
there is volume overload.
➢ If proteinuric and serum creatinine < 2.5mg/dl, ACE inhibitors alone or
in combination with HCT or CCB’s can be used.
➢ If serum creatinine increases by > 30% from baseline stop using the
ACEI/ARB
o Because ACEI and ARB increase serum creatinine level
➢ If Serum creatinine >2.5mg/dl or patient has ESRD CCB’s, loop
diuretics, B blockers or methyldopa can be used.

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ROUTINE CARE FOR HYPERTENSION


Routine monitoring for hypertensive patients

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Table; Considerations for individualizing antihypertensive therapy

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1.5.2 Hypertensive crisis

Definition of Hypertensive urgency and Emergencies and Their Clinical Presentation

❖ Hypertensive urgency: BP ≥ 180/110 mmHg with minimal or no target


organ damage
❖ A hypertensive emergency is the association of substantially elevated BP
with acute Hypertension Mediated Organ Damage (acute HMOD).
✓ Usually BP ≥ 180/110 mmHg, but there is no specific BP threshold
to define a hypertensive emergency.
❖ Target organs include the retina, brain, heart, large arteries, and the
kidneys
o Neurologic damage: encephalopathy, stroke/TIA, papilledema
(fundoscopy)
o Cardiac damage: acute heart failure/pulmonary edema, ACS, aortic
dissection
o Renal damage: acute renal failure/AKI/proteinuria, hematuria, cast
o Microangiopathic hemolytic anemia: preeclampsia/Eclampsia
❖ This situation requires rapid diagnostic workup and immediate BP
reduction to avoid progressive organ failure.
❖ Intravenous therapy is usually required for Hypertensive emergency.
❖ The choice of antihypertensive treatment is predominantly determined by
the type of organ damage.
❖ The 1-year mortality incidence of hypertensive emergencies is more
than 79%, and the median survival is 10.4 months if these persons
are not treated with antihypertensive drug therapy.

Precipitants:
➢ Progression of essential hypertension +/- medical noncompliance
➢ Progression of renovascular disease: AGN, preeclampsia
➢ Endocrine: pheochromocytoma
➢ Cerebral injury (low BP in acute stroke- with treatment)

Specific clinical presentations of hypertensive emergencies include:

❖ Malignant hypertension: Severe BP elevation (commonly >200/120 mm Hg)


associated with advanced bilateral retinopathy (hemorrhages, cotton wool
spots, papilledema).
❖ Hypertensive encephalopathy: Severe BP elevation associated with lethargy,
seizures, cortical blindness and coma in the absence of other explanations.
❖ Hypertensive thrombotic microangiopathy: Severe BP elevation associated with
hemolysis and thrombocytopenia in the absence of other causes and
improvement with BP-lowering therapy.
❖ Other presentations of hypertensive emergencies include severe BP elevation
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associated with cerebral hemorrhage, acute stroke, acute coronary syndrome,


cardio- genic pulmonary edema, aortic aneurysm/dissection, and severe
preeclampsia and eclampsia.

☛ Patients with substantially elevated BP who lack acute HMOD are not
considered a hypertensive emergency and can typically be treated with
oral antihypertensive therapy

Basic investigations:

❖ ECG, BUN, Cr, electrolyte, Urinalysis, CXR (optional)

Clinical Presentation and Diagnostic Workup

❖ The clinical presentation of a hypertensive emergency can vary and is


mainly determined by the organ(s) acutely affected.
❖ There is no specific BP threshold to define a hypertensive emergency.
❖ Symptoms include headaches, visual disturbances, chest pain, dyspnea,
neurologic symptoms, dizziness, and more unspecific presentations.
❖ Medical history: preexisting hypertension, onset and duration of symptoms,
potential causes (nonadherence with prescribed antihypertensive drugs,
lifestyle changes, concomitant use of BP elevating drugs [NSAIDS,
steroids, immunosuppressants, sympathomimetics, cocaine, antiangiogenic
therapy]).

Treatment of hypertensive crisis:

➢ The type of acute HMOD is the main determinant of the preferred


treatment choice.
➢ The timeline and magnitude of BP reduction is strongly dependent on the
clinical context. For example, acute pulmonary edema and aortic dissection
require rapid BP reduction, whereas BP levels not exceeding 220/120 mm
Hg are generally tolerated in acute ischemic stroke for certain periods.
➢ Emergency: decrease MAP by ≈25% in minimum of 2 hours by IV
agents; Goal BP ≤ 160/100 mmHg within 2-6 hours, as tolerated
➢ Urgency: decrease BP in hours/days using PO agents; Goal normal BP in
≈ 1-2 days
➢ Always watch for: UOP, creatinine, mental status; which may indicate
lower BP is not tolerated

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➢ HTN Urgency management

o Nifedipine6 (Immediate release, short acting), 20mg, PO, q 20 to


30min, until target achieved Or
o Captopril7 Oral, sublingual: 12.5 to 25 mg, may repeat as needed;
consider alternative therapy if blood pressure is nonresponsive within
20 to 30 minutes
☛ The trend of using Sublingual nifedipine for HTN Urgency in most setups of
Ethiopia should be avoided because
<<Sublingual nifedipine is contraindicated8 in this setting and should not be
used. Cerebral or myocardial ischemia or infarction can be induced by
aggressive antihypertensive therapy if the blood pressure falls below the
range at which tissue perfusion can be maintained by autoregulation. This
has been most often described with sublingual nifedipine, which may
produce an unpredictable and uncontrolled blood pressure reduction as well
as severe ischemic complications>>
☛ NB: basically, hypertensive emergency should be treated with IV agents but
in shortage of appropriate drugs we can use a hydralazine with short acting
PO drugs (captopril, propranolol, nifedipine) for almost all cases of
emergency
☛ Patients with hypertensive emergencies should be admitted to an ICU

Drug selection9:

✓ Hydralazine: 10-20mg, IV, q20-30 min for maximum of 3-4 doses; fall in BP
begins within 10 to 30 minutes and lasts 2 to 4 hours combined with one
of the following;
➢ Propranolol 20mg Po stat and evaluate: (i.e. if no contraindication for
propranolol/overt heart failure or severe COPD start with hydralazine)
▪ Patients with ACS and aortic dissection (avoid reflex
tachycardia)
▪ Acute renal failure/ATN
➢ Captopril 12.5mg PO stat and evaluate
▪ Caution in patients with acute renal failure and better to use
propranolol, and also use captopril if the patient is not volume
overloaded like Overt heart failure/pulmonary edema
▪ Encephalopathy and stroke (ischemic or hemorrhagic if
indicated)
➢ Nifedipine 20mg Po stat and evaluate (use if propranolol and
captopril are not available or contraindicated)
▪ Acute renal failure
▪ Encephalopathy and stroke

6
In most setups of Ethiopia, Nifedipine; Immediate release, 20mg, PO is the
preferred management principle for hypertensive urgency because of availability ,
may repeat with a 20 mg dose in 20 minutes if needed
7
8
Reference; UpToDate, © 2018, version 2.0
Reference; UpToDate, © 2018, version 2.0
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9
Source; Cardiology handbook, university of Gondar hospital, management guidelines, 2014
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NB:

☛ Caution in combination of hydralazine with nifedipine (reflex tachycardia)


☛ For acute stroke (ischemic, hemorrhagic, SAH) BP should be kept a bit
higher 180-185/100 - 110mmHg until the acute event passed.
☛ In obstetric complication like Preeclampsia with severity features or
Eclampsia;
▪ 1 vial of hydralazine = 1ml = 20mg, so dilute 1ml of
hydralazine with 3ml of NS or Distilled water and give 1ml of
the dilute (i.e. 5mg every 30min until target is achieved)

Hypertensive Emergencies Requiring Immediate BP Lowering


Clinical Presentation Timeline and Target BP First Line Treatment Alternative
Malignant hypertension with or without Several hours, MAP −20% Labetalol, 20mg, over Hydralazine, 10-20mg, IV,
thrombotic microangiopathy or to −25% 2 minutes initially then q20-30 min until target is
acute renal failure 40-80mg, IV, q10min achieved for maximum of 3-
until target is 4 doses
achieved (max total
dose; 300mg)

Hypertensive encephalopathy Immediate, MAP −20% to Labetalol Hydralazine


−25%
Acute ischemic stroke and SBP 1 h, MAP −15% Labetalol Hydralazine
>220 mm Hg or DBP >120 mm
Hg
Acute ischemic stroke with indication 1 h, MAP −15% Labetalol Hydralazine
for thrombolytic therapy and SBP
>185 mm Hg or DBP >110 mm
Hg
Acute hemorrhagic stroke and SBP Immediate, 130<SBP<180 Labetalol Hydralazine
>180 mm Hg mm Hg
Acute coronary event Immediate, SBP <140 Nitroglycerine
mm Hg
Acute cardiogenic pulmonary Immediate, SBP <140 Nitroglycerine (with loop diuretic
edema mm Hg loop diuretic)
Acute aortic disease Immediate, SBP <120 mm nitroglycerine and Labetalol or metoprolol
Hg and heart rate <60 metoprolol
bpm
Eclampsia and severe preeclampsia/ Immediate, SBP <160 mm Labetalol and Hydralazine (5mg, IV, q20-
HELLP Hg and DBP <105 mm magnesium sulphate 30 min until target is achieved
Hg for maximum of 3-4 doses)
or

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short acting nifedipine

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(20mg, po, BID or


sublingual, q30min, until
target achieved)

Follow-Up

➢ Patients who experienced a hypertensive emergency are at increased


risk of cardiovascular and renal disease.
➢ Thorough investigation of potential underlying causes and assessment
of HMOD is mandatory to avoid recurrent presentations with
hypertensive emergencies.
➢ Regular and frequent follow-up (monthly) is recommended until target
BP and ideally regression of HMOD has been achieved.

Notes on specific hypertension medications

❖ Pregnant women and women of childbearing age not on effective contraception


should not be given ACE inhibitors, ARBs, or thiazide/thiazide-like diuretics;
CCBs should be used.

❖ Beta blockers should NOT be used for initial monotherapy in the


absence of a specific indication, as it may have an adverse effect on
some cardiovascular outcomes, particularly in older patients.
a. If a heart attack has been diagnosed within the previous three
years, or there is atrial fibrillation or heart failure, then a beta
blocker should be added to the starting dose of antihypertensive
medication.
b. Patients with angina may also benefit from treatment with a beta
blocker.

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1.5.3 Hypertensive heart disease (HHD)

➢ Heart disease is the most common cause of death in hypertensive patients


☛ LVH, CHF, abnormalities of blood flow due to atherosclerotic
coronary artery disease and microvascular disease, and cardiac
arrhythmias
➢ CHF may be related to systolic dysfunction, diastolic dysfunction, or a
combination of the two
➢ Diastolic dysfunction is an early consequence of hypertension related heart
disease

Image; LVH

➢Hypertension is a risk factor for the development of HF with reduced


ejection fraction (HFrEF), and with preserved ejection fraction (HFpEF).
➢Clinical outcome is worse and mortality is increased in hypertensive patients
with HF.
➢Lifestyle changes are recommended (diet and exercise).
➢Treating hypertension has a major impact on reducing the risk of incident
HF and HF hospitalization, aggressive control of hypertension can regress
or reverse LVH.
➢BP should be lowered if ≥140/90 mm Hg and treated to a target <130/80
mm Hg but >120/70 mm Hg.

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1.6 Infective endocarditis (IE)

❖ IE is defined as an infection of the endocardial surface of the heart, which


may include one or more heart valves, the mural endocardium, or a septal
defect.
❖ Always suspect endocarditis in a patient with a new heart murmur and
unexplained fever or bacteremia.

Risk factors

✓ Structural heart disease (esp. Rheumatic regurgitant valve lesions)


✓ Prosthetic valves
✓ Prior history of IE
✓ Injection drug use
✓ Recent dental manipulation, GI, GU instrumentation

Classifications

❖ Classified into four groups:


✓ Native Valve IE
✓ Prosthetic Valve IE
✓ Intravenous drug abuse (IVDA) IE
✓ Nosocomial IE

Further Classification
Acute endocarditis Subacute endocarditis
✓Most commonly caused by S. aureus ✓Caused by less virulent organisms, such
(highly virulent). as S. viridans and Enterococcus
✓Occurs on a normal heart valve. ✓Occurs on damaged heart valves
✓Rapidly destructive, Metastatic foci ✓Indolent nature
✓If untreated, fatal in less than 6 weeks. ✓If untreated, takes much longer than 6
weeks to cause death

Clinical presentations

❖ History
1. Acute endocarditis is characterized by high grade fever with rapidly
progressive heart failure and metastatic infection. Common etiologies
include S.aureus, pneumococci, and enterococci
2. Subacute endocarditis- evolves during weeks to months with only
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modest toxicity. It is commonly caused by viridians streptococci,


CONS, Enterococci, and HACEK group
❖ Common findings include
✓ Persistent fever
✓ Heart murmurs
✓ Otherwise-unexplained arterial emboli, and
✓ Cutaneous and mucocutaneous lesions, like petechiae, splinter
hemorrhages, janeway lesions, osler’s node, and Roth spots.

Splinter Hemorrhages

Pictures; Splinter Hemorrhages; Nonspecific, non-blanching, Linear reddish-


brown lesions found under the nail bed, usually do NOT extend the entire
length of the nail. Subungual hemorrhages that extend the entire length of the
nail or are primarily located at the proximal end of the nail (near the cuticle)
are like due to trauma.

Janeway lesions

Erythematous, blanching macules, nonpainful, more specific, located on palms


and soles

Osler’s Nodes

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More specific, painful and erythematous nodules, located on pulp of fingers and
toes, more common in subacute IE

Diagnosis

Diagnostic Clues:

Fever, hematuria, night sweating, weight loss, clubbing, changing


murmur, unexplained rapid deterioration of heart failure,
splenomegaly.
Skin manifestations like conjunctival hemorrhage, splinter hemorrhage.
Infective endocarditis is far less common in pure stenotic lesions.
Though history of predisposing procedures are commonly enquired it
is not commonly elicited in most of our patients.

❖ IE should be suspected in any patient with rheumatic VHD (esp.


regurgitant) presenting with fever and/or worsening of heart failure despite
therapy.
❖ Endocarditis most commonly occurs in the mitral or aortic valves

❖ Blood culture
✓ 3 sets of blood culture should be obtained prior to antibiotic therapy.
✓ A minimum of 10ml of blood for each set
✓ Each set of cultures should be taken from separate venipuncture sites
✓ Avoid taking samples from preexisting IV lines
✓ Blood cultures can be taken at any time.
✓ Acutely ill pt
➢ Take 3 blood culture samples over 1hr before beginning empiric
therapy
✓ Subacute endocarditis
➢ Take 3 samples over 12hrs
❖ Echocardiography
✓ Look for vegetations, abscess, new valvular regurgitation, or new partial
dehiscence of prosthetic valve.
✓ Trans esophageal echo (TEE) is better than transthoracic
echocardiography (TTE) in the diagnosis of endocarditis for especially
mitral valve pathology and small aortic vegetations.
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✓ Most patients should get TTE as an initial screening test.


☛ N.B. echocardiographic evidence of vegetations is not necessary to
make the diagnosis as long as sufficient Duke criteria have been
met.
❖ Diagnosis criteria; use modified Dukes clinical criteria: 2 major criteria, 1
major and 3 minor criteria, or 5 minor criteria are required to diagnose
infective endocarditis.
❖ Treatment should be initiated if clinical suspicion is high.

Modified Duke Criteria


Major Criteria
➢ Positive blood culture
– Typical microorganism for infective endocarditis from two separate
blood cultures
– Persistently positive blood culture, defined as recovery of a
microorganism consistent with infective endocarditis from:
• Blood cultures (≥2) drawn more than 12 hr apart, or
• All of three or a majority of four or more separate blood
cultures, with first and last drawn at least 1 hr apart
– Single positive blood culture for Coxiella burnetii or antiphase I
IgG antibody titer >1:800
➢ Evidence of endocardial involvement
– Positive echocardiogram
• Oscillating intracardiac mass, on valve or supporting
structures, or in the path of regurgitant jets, or on
implanted material, in the absence of an alternative
anatomical explanation, or
• Abscess, or
• New partial dehiscence of prosthetic valve, or
– New valvular regurgitation (increase or change in preexisting
murmur not sufficient)

Minor Criteria
1. Predisposing condition (abnormal valve e.g. RHD or abnormal
risk of bacteremia like IV drug abuse, GI/GU manipulation….)
2. Fever ≥38.0°C (100.4°F)
3. Vascular phenomena: Septic arterial or pulmonary emboli, mycotic
aneurysms, intracranial hemorrhage, conjunctival hemorrhages, Janeway
lesions10
4. Immune phenomena: Glomerulonephritis, Osler nodes11, Roth spots12,

10
rheumatoid factor

Janeway lesions are painless erythematous lesions on palms and soles.


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5. Positive blood cultures not meeting major criteria


6. Positive echocardiogram not meeting major criteria

❖ Definite IE
✓ Clinical criteria
➢ 2 major criteria, or
➢ 1 major and 3 minor criteria, or
➢ 5 minor criteria
✓ Pathologic criteria
➢ Microorganism: (via culture or histology) in a
valvular vegetation, embolized vegetation, or
intracardiac abscess
➢ Pathological lesions: vegetation or intracardiac
abscess present, confirmed by histology showing
active endocarditis
❖ Possible IE
✓ 1 major criterion and 1 minor criterion or
✓ 3 minor criteria
❖ Rejected IE
✓ Firm alternative diagnosis for manifestations IE, or
✓ Sustained resolution of manifestations of endocarditis, with
antibiotic therapy for 4 days or less, or
✓ No pathological evidence of infective endocarditis at
surgery or autopsy

Organisms
Native valve endocarditis
➢ S. viridans is the most common organism in native valve
endocarditis.
➢ Other common organisms include:
− Staphylococcus species (S. aureus more commonly than S.
epidermidis) and Enterococci.
− Streptococcus bovis is associated with increased risk of
active colonic malignancy
− HACEK group of organisms: Haemophilus, Actinobacillus,
Cardiobacterium, Eikenella, and Kingella.
Prosthetic valve endocarditis
➢ Staphylococci are the most common causes of early-onset
endocarditis; symptoms appear within 60 days of surgery (S.
epidermidis more commonly than S. aureus).

11

12
Osler nodes are painful, raised lesions of fingers, toes, or feet.
Roth spots are oval, retinal hemorrhages with a clear, pale center.
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➢ Streptococci are the most common cause of late-onset endocarditis;


symptoms appear 60 days after surgery.
Endocarditis in IV drug users
➢ Frequently presents with right-sided endocarditis.
➢ S. aureus is the most common cause.
➢ Other organisms include Enterococci and Streptococci.
➢ Fungi (mostly Candida) and gram-negative rods (mostly
Pseudomonas) are less common causes.

Treatment of IE

❖ PRINCIPLES OF TREATMENT
1) Parentral antibiotics
2) Only bactericidal antibiotics are effective and Bacteriologic result should
direct antibiotic selection
3) High dose & combination of antibiotics designed to give sustained
bactericidal serum concentration to penetrate vegetations!
4) Prolonged treatment to kill dormant bacteria clustered in vegetations! (4-
6 wks)
5) 3 sets of blood cultures should be drawn prior to initiating antibiotic
therapy. start antibiotic treatment immediately after blood culture is
collected over 1 hour in Acute endocarditis or prosthetic valve
endocarditis.

Subacute endocarditis (SBE)- if patient hemodynamically stable wait for 2-3


days till blood culture result is collected

✓ Culture positive
➢ Treat based on the isolated organism and susceptibility pattern
✓ Culture negative endocarditis
➢ SBE- ceftriaxone 2gm/day + gentamycin 3mg/kg for the first
2wks and continue with ceftriaxone only for the remaining wks
of therapy
➢ Acute endocarditis- continue vancomycin + gentamycin for 2
wks and then vancomycin only for the remaining wks of therapy
• Patients with proven or suspected enterococcal
endocarditis should receive combination of vancomycin
and gentamicin for the whole duration of therapy
• If vancomycin is not available or patient cannot afford,
use ceftriaxone 2gm/day with gentamycin
• In our setup we are using ceftriaxone and gentamycin
as 1st line because of availability and cost effectiveness
but not efficacy.

Duration of therapy- Parenteral antibiotics based on culture results for


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extended periods (4 weeks for most patients, sometimes for 6 weeks)

✓ Indications for 6 weeks of antibiotic therapy


▪ Patients with slow clinical response than expected
▪ Presence of cardiac or extracardiac complications
▪ Patients with infections of long duration prior to diagnosis
▪ Infection with highly virulent or resistant organisms

If cultures are negative but there is high clinical suspicion, treat empirically
(See table below) until the organism can be isolated.
Anticoagulants and antiplatelets are not recommended to prevent or treat
embolic complications.

Monitoring during therapy

❖ T0 should be followed at least 4 times a day.


✓ Fever should subside after 5-7 days of antibiotics.
✓ If fever persists beyond 7 days despite appropriate antibiotic therapy,
patients should be evaluated for paravalvular abscess, extracardiac
abscess (spleen, kidney), or complications (embolic events), resistant
organisms like enterococci
❖ Repeating blood culture can be considered in those patients with initial
positive cultures and
✓ Suboptimal clinical response after 1 week of antibiotic therapy
✓ After completing the course of antibiotic therapy
❖ CBC, ESR and RFT should be done at least every week to check for drug
toxicities and response

If patient has intracardiac devices such as pacemaker or ICD, these must


be removed.
Early surgical intervention is warranted for patient with:
o Acute heart failure due to valvular damage.
o Left-sided IE with highly resistant organisms (including MRSA)
o IE complicated by heart block or intracardiac abscess.
o Persistent bacteremia or fevers lasting 5 to 7 days after antibiotic
initiation.
o Recurrent infection in those with prosthetic valves.

Note: Infective endocarditis is almost always fatal if left untreated.

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Empiric antibiotic therapy

Table: Empiric treatment of “community acquired” Native Valve SBE


Antibiotic regimen options Dosage and route Duration Comments
(weeks)
Ceftriaxone 2g, IV, once per day 4-6 If vancomycin is not available or
patient cannot afford
PLUS 3mg/kg, IV, daily 2 Dose should be adjusted to
OR Creatinine clearance.
Gentamicin 1mg/kg/dose, IV, TID Creatinine should be
monitored.

Vancomycin 15mg/kg/dose (1gm), IV, 4 For patients with severe


BID or immediate beta-lactam
allergy.
Do not exceed 2g per day
Adjust dose to creatinine
PLUS clearance.

3mg/kg, IV, daily 2 See above


Gentamicin
OR
1mg/kg/dose, IV, TID

*Treatment should be modified based on culture and sensitivity results as well as clinical
judgement of response, risk factors and expected organisms.
Table: Empiric treatment of health care - associated and IV medicine
users endocarditis
Vancomycin 15mg/kg/dose, IV, BID -Do not exceed 2g per day
-Adjust dose to
4 creatinine clearance.
PLUS
3mg/kg, IV, daily See the table above
OR
1mg/kg/dose, IV, TID 2
Gentamicin
Prophylaxis

❖ Scope of patients who qualify for prophylaxis is much narrower


than in the past.
❖ Must have both a qualifying cardiac indication AND procedure
to warrant antibiotic prophylaxis.
❖ Qualifying cardiac indications
✓ Prosthetic heart valves (including mechanical, bioprosthetic, and
transcatheter valves).
✓ History of infective endocarditis
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✓ Congenital heart disease


− Unrepaired cyanotic congenital heart disease.
− Repaired congenital heart disease, with prosthetic material,
during first 6 months after procedure
✓ Cardiac transplant with valvopathy.
❖ Qualifying procedures
✓ Dental procedures involving manipulation of gingival mucosa or
periapical region of teeth (extractions, implants, periodontal
surgery, cleaning when bleeding expected).
✓ Procedures involving biopsy or incision of respiratory mucosa
✓ Procedures involving infected skin or musculoskeletal tissue

Indications for surgery in IE

Significant embolic events


Persistent infection, and
Progressive cardiac failure

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1.7 Arrhythmia
Readers are recommended to click here and read → Chapter 22; Basics of
ECG and ECG interpretation before reading arrythmia.

Arrhythmias are disorders of cardiac rate, rhythm and conduction.


Arrhythmias are classified as bradyarrhythmia’s and tachyarrhythmias
Bradyarrhythmia’s include
o Sinus bradycardia
o Sinus pauses and
o Atrioventricular blocks.
The tachyarrhythmias can further be classified into supraventricular and
ventricular arrhythmias, based on their site of origin.
o Supraventricular tachyarrhythmias includes
☛ Atrial fibrillation
☛ Atrial flutter
☛ Paroxysmal supraventricular tachycardia and
☛ Multifocal atrial tachycardia.
o Ventricular tachyarrhythmias include
☛ Ventricular tachycardia and
☛ Ventricular fibrillation.
The etiologies for arrhythmias are:
o Structural heart disease (VHD, CMP, CAD)
o Thyrotoxicosis
o Electrolyte abnormalities
o Ingestion of stimulants
o Side effects of some medicines (digoxin, antiarrhythmic medicines)
Clinical features of arrythmias in general include:
o Palpitation
o Shortness of breath
o Dizziness/syncope
o Sensation of a pause in the heart beat
o Chest discomfort that mimics symptoms of myocardial
ischemia(angina)
o Development of Heart Failure or decompensation of previously existing
Heart Failure
o Sudden death
ECG is the main stay of diagnosis.
o Other investigations like Echo, CXR, TFT, CBC, electrolytes should
be guided by clinical data.
o Prior to treatment of any suspected arrhythmia the diagnosis should
be confirmed with ECG.
☛ It is dangerous to give any antiarrhythmic medicine without
doing ECG!
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SVT = Supraventricular tachycardia, PVCs = premature ventricular contractions, AVNRT =


Atrioventricular node reentry tachycardia, AVRT = Atrioventricular reentrant tachycardia.
BBB = Bundle Branch Block, VT = Ventricular tachycardia

Figure; Clinical approach to arrhythmias

1. Tachyarrhythmias

1.1 Supraventricular tachyarrhythmias

1.1.1 Paroxysmal supraventricular tachycardia

❖ Paroxysmal supra-ventricular tachycardia (PSVT) is an intermittent narrow


complex tachyarrhythmia other than Atrial Fibrillation, atrial flutter, and MAT
(Multifocal Atrial Tachycardia).
❖ PSVT usually occurs in individuals without underlying structural heart disease.
❖ ECG shows regular narrow QRS tachycardia. P wave may be seen
preceding or following or superimposed on QRS complex or may not be
seen.

Treatment

Non pharmacologic
❖ Vagal maneuvers: maneuvers which increase vagal activity can terminate
episodes of PSVT. ECG and blood pressure monitoring is required during
the procedure.
☛ Carotid sinus massage: supine position with the neck extended. The
carotid sinus is located inferior to the angle of the jaw at the level
of the thyroid cartilage. Steady pressure is applied to one carotid
sinus for 5 to 10 seconds. If no response, repeat it in the
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Note: Carotid massage should not be attempted in patients with carotid


bruit/stenosis or ischemic stroke. Both carotid sinuses should never be
massaged simultaneously.
☛ Valsalva maneuver: while in the supine position the patient is
instructed to exhale forcefully against a closed glottis with closed
mouth and nose for 10 seconds. Adequacy indicated by neck vein
distension, and increased tone in the abdominal wall muscles.
❖ Synchronized electrical Cardioversion: required rarely for hemodynamically
unstable patients. The energy needed is 150 to 200 joules for monophasic
defibrillators.

Pharmacologic

Termination of acute episode


First line

✓ Adenosine, I.V, very rapidly (over 1-2 seconds): Initial: 6mg; if not effective
within 1-2 minutes, 12mg may be given; may repeat 12mg bolus if needed.
Follow each dose with 20ml very rapid NS flush.
Alternatives

✓ Metoprolol, IV, 2.5-5mg every 2-5 minutes (maximum total dose: 15mg over
a 10-15minute period). OR
✓ Verapamil, I.V, 2.5-5mg over 2 minutes; second dose of 5-10mg may be
given after 15-30 minutes; maximum total dose: 20-30mg OR
✓ Digoxin, 0.5 to 1mg IV over a period of 10 to 15 min followed by 0.25mg
every 2-4 hours with a total dose less than 1.5mg with in 24-hour period

Prevention of recurrence (chronic therapy)


First line: beta blockers

✓ Metoprolol succinate (Extended release): 25-200mg/day, P.O. OR


✓ Atenolol, 25-100mg/day, P.O. OR
✓ Propranolol 10-40mg P.O. 3-4 times daily
Alternatives

✓ Verapamil, immediate release 40-120mg, P.O.TID or extended release 180-


360mg/day

1.1.2 Atrial fibrillation and flutter

Atrial fibrillation

Atrial fibrillation is marked by disorganized, rapid, and irregular atrial


activation which results in irregular ventricular response.
The ventricular rate is usually rapid.
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The ECG in Atrial Fibrillation is characterized by the lack of P-waves,


irregularly irregular ventricular response and narrow QRS.

Atrial flutter

Atrial flutter is characterized by regular rapid atrial rate of 260 - 300 beats
per minute, which usually results in a regular ventricular response in a 2:1
ratio resulting in a heart rate of 130 - 150 beats per minute.
The ventricular response can sometimes be in 3:1, 4:1, irregular or rarely
1:1 ratio.
The typical ECG finding is of saw-tooth appearance of the baseline mainly
on inferior leads (II, III, AVF) with rapid, regular and narrow QRS.

Treatment
Note: The management of atrial fibrillation and atrial flutter are the same.

Non pharmacologic

❖ Avoid stimulants (e.g. Caffeine, Khat) and alcohol intake.


❖ Immediate electrical cardio-version-associated with hemodynamic instability
(cardiogenic shock) due to a rapid ventricular rate.
❖ If hypotension occurs at ventricular rate <130 beats/min, other causes of
hypotension should be investigated.
❖ The energy requirement is usually 100 to 200 joules; it should be
synchronized.

Pharmacologic

1. ventricular rate control

Acute ventricular rate control

First line

✓ Metoprolol, 2.5 - 5mg, IV, over 3–5 min, to maximum total dose 15mg
over 10-15 minutes
Alternative

✓ Digoxin, 0.25mg, IV, q2h until 1 mg total (digoxin is the first line medicine
if atrial fibrillation is associated with severe left Ventricular dysfunction)

Chronic ventricular rate control (Maintenance)

First line: Beta blockers


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✓ Metoprolol, preferred beta blocker in patients with Heart Failure with


depressed LV (left ventricle) systolic function. OR
☛ Immediate release (Metoprolol tartrate): 25-100 mg twice daily
☛ Extended release (Metoprolol succinate): 25 - 200 mg/day
✓ Atenolol, 25-100mg P.O., daily
Alternatives

✓ Digoxin, 0.125 - 0.25mg P.O., daily.


☛ Digoxin can be added to beta blocker when the ventricular rate
control is suboptimal.
☛ It is the preferred agent when Heart Failure due to LV systolic
dysfunction is not well controlled.
OR
✓ Verapamil, 40-80mg P.O., 2-3 times daily.

2. Anticoagulation to prevent cardioembolic cerebrovascular accident (CVA)

❖ Risk stratify patients for thrombotic complications with the CHA2DS2-VASc


score.
❖ This is a scoring calculator used to estimate annual stroke risk in a patient
with AFib or atrial flutter.

Scoring systems for assessing the risk of stroke (CHA 2DS2-


VASc) and bleeding (HAS-BLED) in patients with atrial fibrillation

CHA2DS2-VASc Score HAS-BLED* Score

CHF 1 Hypertension (systolic blood 1


pressure >160 mm Hg)
Hypertension 1 Abnormal renal and liver function 1 or 2
(1 point each)
Age ≥ 75 years old 2 Stroke 1
DM 1 Bleeding tendency/predisposition 1
Stroke/TIA/Thromboembolism 2 Labile INRs (if on warfarin) 1
Vascular disease (prior MI, PAD, or 1 Elderly (e.g. age >65 years old) 1
aortic plaque)
Age 65 - 74 years old 1 Drugs or alcohol (1 point each) 1 or 2
Sex category (i.e. female sex) 1
Maximum score 9 Maximum score 9

* The HAS-BLED bleeding risk score has only been validated in patients with
atrial fibrillation
❖ Hypertension is defined as SBP >160 mmHg.
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❖ Abnormal renal function is defined as the presence of chronic dialysis,


renal transplantation, or serum creatinine ≥ 2.2 mg/dl or ≥ 200 µmol/L.
❖ Abnormal liver function is defined as CLD (e.g. cirrhosis) or biochemical
evidence of significant hepatic derangement (e.g. bilirubin > 2 X the upper
limit of normal, plus one or more of ALT, AST, and/or ALP > 3 X the
upper limit normal).
❖ Bleeding predisposition includes chronic bleeding disorder or previous
bleeding requiring hospitalization or transfusion.
❖ Labile INRs for a patient on warfarin includes unstable INRs, excessively
high INRs, or <60 % time in therapeutic range.

CHA2DS2VASc score Interpretation

❖ The higher the score, the higher the annual stroke risk.
❖ For patients with CHA2DS2VASc score >1, anticoagulation is generally
indicated unless high bleeding risk
o Score 0 → No antithrombotic
o Score 1 → Anti-platelet or anticoagulation
o Score ≥ 2 → anticoagulation.
❖ Commonly used Antiplatelets include Aspirin (1st line) & clopidogrel (2nd
line). Commonly used anticoagulants include warfarin, UFH, LMWH

HAS-BLED Score Interpretation


0 points: 1.13 bleeds per 100 patient-years
1 point: 1.02 bleeds per 100 patient-years
2 points: 1.88 bleeds per 100 patient-years
3 points: 3.74 bleeds per 100 patient-years
4 points: 8.70 bleeds per 100 patient-years
5 to 9 points: Insufficient data

Choice of anticoagulant: depends on etiology of AFib or atrial flutter.


For patients with mechanical valves, mitral valvular disease, or ventricular
assist devices, warfarin is the only oral anticoagulant available. For other
patients, direct oral anticoagulants (DOACs) can be used.
DOACs approved for AFib include factor Xa inhibitors (apixaban,
rivaroxaban, edoxaban) and direct thrombin inhibitors (dabigatran). These
agents do not require lab monitoring. Cost is the limiting factor for wider
use in resource limited settings like Ethiopia.
Rivaroxaban is the available direct oral anticoagulant in Ethiopia.
o The dose is Rivaroxaban 20 mg Po daily.
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o Dose adjustment is required for patients with renal failure, elderly,


low body weight and those with high risk of bleeding.

Warfarin:

✓ Widely available and affordable anticoagulant


✓ Warfarin has a narrow therapeutic range and during therapy monitoring
using INR is mandatory.
✓ An INR of 2 to 3 is the anticoagulation goal range (therapeutic range) for
warfarin.
✓ Warfarin, starting dose, 2.5 - 5mg/day, dose titrated to achieve INR of 2.0-
3.0.
✓ The goal is to maintain time in therapeutic (TTR) range above 70 %.

Warfarin dosing and monitoring


Suggested dose changes for maintaining INR within a target range of 2–3

INR Dose change


<1.5 Increase by 20%
1.6–1.9 Increase by 10%
2-3 Therapeutic range
3.1–3.4 Decrease by 10%, adjustment may not be necessary
3.5–3.9 Decrease by 20%, consider holding one dose
4.0–4.9 Hold dose until INR returns to range then decrease by 20–30%

Management of supratherapeutic INR values


INR Patient situation Action
3.1–5.0 No bleeding or need for rapid Omit next few warfarin doses and/or restart at lower
reversal dose when INR approaches desired range. If INR is
(i.e., no need for surgery) only minimally above range, no dose reduction may
be needed.
5.1–9.0 No bleeding or need for rapid Omit next 1–2 doses, monitor INR more frequently,
reversal and restart at lower dose when INR approaches
target range or omit dose and give 1 - 2.5 mg
vitamin K orally (use this if patient has risk factor for
bleeding).
No bleeding but reversal Vitamin K1 2–4 mg orally (expected reversal within
needed for surgery or dental
extraction within 24 hours
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24 hours); give additional 1–2 mg if INR remains
high at 24 hours.

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9.1–20.0 No bleeding Stop warfarin; give vitamin K1 3–5 mg orally; follow


INR closely; repeat vitamin K1 if needed. Reassess
need and dose of warfarin when INR approaches
desirable range.
Rapid Serious bleeding or major Stop warfarin; give vitamin K1 10 mg by slow IV
reversal warfarin overdose infusion. May repeat vitamin K1 every 12 hours and
required give fresh plasma transfusion or prothrombin
(>20.0) complex concentrate as needed. When appropriate,
heparin can be given until the patient becomes
responsive to warfarin.
Life Replace with prothrombin complex concentrate and
Threatening give 10 mg of vitamin K1 by infusion. May repeat if
Bleeding needed. Give fresh frozen plasma if prothrombin
complex concentrates not available.

1.2 Ventricular tachycardia

❖ Ventricular tachycardias are wide QRS tachyarrhythmias that originate in the


myocardium.
❖ They are commonly associated with some form of structural heart disease.
❖ Based on their clinical significance, they can be divided in to two:
1) Malignant (potentially lethal) arrhythmias → sustained ventricular
tachycardia (VT) and Ventricular fibrillation.
2) Non sustained (hemodynamically tolerated) arrhythmias → premature
ventricular contractions (PVCs), non-sustained ventricular tachycardia
(NSVT), and accelerated idioventricular rhythm (AIVR).
❖ Ventricular tachycardia which stays for more than 30 seconds is labeled
sustained.
❖ All Wide QRS (> 120 ms) tachycardias are considered and treated as
ventricular tachyarrhythmias until proved otherwise.

Treatment

Non pharmacologic
CPR should be provided to patients with sustained VT with cardiac arrest
(the victim is unresponsive, pulseless and not breathing).
O2 via face mask or nasal catheter.
Continuous ECG monitor.
Suction device and endotracheal intubation set should be ready.
Correct electrolyte disorders.
Reassure patients with non-sustained ventricular tachycardia.
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Defibrillation:
➢ Sustained polymorphic VT, ventricular flutter, or ventricular fibrillation
Emergency defibrillation (without synchronization), with >200 Joules
(monophasic), increase the energy to the maximum if arrhythmia persists.
➢ Sustained monomorphic VT: synchronized with >200 Joules (monophasic).

Note:

☛ If the hemodynamic status allows conscious sedation should be provided.


☛ DC cardioversion is first line therapy for sustained wide QRS tachycardias.
☛ Pharmacologic treatment may be an acceptable option in hemodynamically
stable monomorphic VT with no Heart Failure.

Pharmacologic
First line:

✓ Amiodarone, IV
➢ Stable VT regimen:
☛ Step 1: 150mg over first 10 minutes (dilute in 100ml D5W)
☛ Step 2: 360mg over next 6 hours (dilute in 500ml D5W): 1
mg/minute
☛ Step 3: 540mg (dilute in 500 to 1000ml D5W) over next 18 hours:
0.5mg/minute
➢ Pulseless VT (cardiac arrest) regimen:
☛ If unresponsive to defibrillation attempts and CPR; Amiodarone, I.V
push, 300mg (undiluted)
☛ If VT or VF recurs, administer supplemental dose of 150mg and
continue CPR.
Alternative:

✓ lidocaine, IV
➢ Both stable VT and Pulseless VT (cardiac arrest) regimen:
☛ Lidocaine, I.V, 1 - 1.5mg/kg; repeat with 0.5 - 0.75mg/kg every 5-10
minutes if no response. (maximum cumulative dose: 3mg/kg).
☛ Follow with continuous infusion of 1 - 4mg/minute
☛ Preparation for continuous infusion: 2g of lidocaine/250ml D5W
☛ Rate of infusion: 1mg/min = 7.5ml/hour, 2mg/min =15ml/hour, 3mg/min=
22.5ml/hr, 4mg/min= 30ml/min

Prevention of recurrence
Non-pharmacologic
➢ Standard treatment of the underlying cause is the main stay of treatment for
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➢ Correct precipitating causes (e.g. hypoxia, hypo/hyperkalemia, acidosis,


pulmonary embolism).
➢ Discontinue arrhythmogenic medicines-digoxin, antiarrhythmic medicines.
Pharmacologic
First line

✓ Amiodarone, 400-800mg, PO, BID, for 1-3 weeks


▪ when adequate arrhythmia control is achieved, decrease to 300-400mg,
PO, BID to daily for 1 month. Maintenance: 400mg/day
Alternative or additional to Amiodarone → Beta blockers:

✓ Metoprolol succinate, extended release: P.O., 25-200mg/day or


✓ Atenolol, 25-100mg daily

1.3 Adult tachycardia

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2. Bradycardia (Bradyarrhythmia)

AV block describes a delay/block of atrial impulses at the atrioventricular node of


varying severity.
When severe it results in symptomatic bradycardia which can manifest as easy
fatigability, Heart Failure, syncope, seizures and bradycardia associated
ventricular tachycardias.
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It is caused by structural heart diseases (mainly IHD, CMP’s, CHD), medicines


(beta blockers, verapamil, digoxin), electrolyte abnormalities, hypothyroidism and
cardiac surgery.
☛ ECG is the diagnostic Ix modality of AV block.

Treatment
❖ Look for reversible causes and act accordingly

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Cardiac arrest (የልብ ምት መቋረጥ)

[Sudden] cardiac arrest is the sudden cessation of cardiac activity so that the
victim becomes unresponsive, with no normal breathing and no signs of
circulation.
If corrective measures are not taken rapidly, this condition progresses to
sudden death.
Cardiac arrest should be used to signify an event as described above, that is
reversed, usually by CPR and/or defibrillation or cardioversion, or cardiac
pacing.
Sudden cardiac death (SCD) should not be used to describe events that are
not fatal."
These events mostly occur in patients with structural heart disease (that may
not have been previously diagnosed), particularly coronary heart disease or
sustained ventricular tachycardia/ventricular fibrillation.

Management of cardiac arrest

Look at the algorism below

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Sodium bicarbonate May be considered in the setting of prolonged cardiac


arrest only after adequate alveolar ventilation has been established and
effective cardiac compressions.

o
Dose: Initial: 1 mEq/kg/dose, IV; repeat doses should be guided by
arterial blood gases
Routine use of NaHCO 3 is not recommended.
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o Note: In some cardiac arrest situations (e.g. metabolic acidosis,


hyperkalemia, or tricyclic antidepressant overdose), sodium
bicarbonate may be beneficial.

Cardioversion and defibrillation

Cardioversion and Defibrillation

Attach ECG monitor and pulse oximeter


Prepare
o Oxygen with preferably a facemask or nasal prong
o Endotracheal tube
o Laryngoscope
o Suction machine
o Airway adjuncts (bag-valve mask, oral and nasal airways)
o Resuscitation medications (epinephrine, atropine, amiodarone)
o A defibrillator with hand held paddle electrodes
Establish IV line
Monitoring and preoxygenation
o BP, PR, and RR should be measured at frequent, regular intervals;
o oxygen saturation (SpO2), and cardiac rhythm should be
monitored continuously
o Patient's level of alertness, depth of respiration, and response to
painful stimuli
o 100% oxygen should be administered for 5 to 15 minutes by nasal
cannula or face mask before the procedure and continued throughout
the procedure
Perform procedural sedation
o Discuss the risks, benefits, and alternatives of the procedure and the
planned sedation with the patient or caretaker and answer any
questions
o Propofol, initial loading dose of 0.5 to 1 mg/kg IV, followed by doses
of 0.5 mg/kg IV every 3-5 minutes as necessary
o Midazolam, 0.5 or 1 mg at a time and titrated to effect. No single
dose should exceed 2.5 mg
o Ketamine, 1 to 2 mg/kg is given IV over one to two minutes. Doses
of 0.25 to 0.5 mg/kg may be repeated every 5 to 10 minutes
thereafter

o *Procedural sedation may be skipped in a patient who is unstable


Electrode positioning → Pad placement
o Sternal-apical (anterolateral) position, with the right pad placed on
the right superior-anterior chest below the clavicle, and the left pad
placed on the inferior-lateral left chest, lateral to the left breast
o Apply pads at least 2.5 cm away from any implantable devices
o Apply a wet gauze at the site of electrode placement 149
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Energy selection
o Select the appropriate energy for the specific arrhythmia
o Press the sync button if synchronization is required
Clear you and your team and deliver the shock
o Say “I am going to shock on three. One, two, three, shocking”
o Perform a visual check to make sure you have no contact with the
patient, the stretcher or other equipment

Click on the link below and watch the video

Manual defibrillation

https://youtu.be/Dubih8EzBJQ

How to perform cardioversion and defibrillation

https://youtu.be/T7Zv9vLdWtE

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1.8 Pericarditis

Classification of pericarditis

A. Classification based on duration of illness

➢ Acute pericarditis (<6 weeks)


✓ Fibrinous
✓ Effusive (serous or sanguineous)
➢ Subacute pericarditis (6 weeks to 6 months)
✓ Effusive-constrictive
✓ Constrictive
➢ Chronic pericarditis (>6 months)
✓ Effusive
✓ Constrictive
✓ Adhesive (nonconstructive)

B. Etiologic Classification of pericarditis

I. Infectious II. Non infectious


A. Acute idiopathic
A. Viral (coxsackievirus A and B, B. Renal failure
echovirus, herpesviruses, mumps, C. Neoplasia
adenovirus, hepatitis, HIV) 1. Primary tumors (benign or
B. Pyogenic (pneumococcus, malignant, mesothelioma)
Streptococcus, Staphylococcus, 2. Tumors metastatic to
Neisseria, Legionella, Chlamydia) pericardium (lung and breast
C. Tuberculous cancer, lymphoma, leukemia)
D. Fungal (histoplasmosis, D. Trauma (penetrating chest wall,
coccidioidomycosis, Candida, nonpenetrating)
blastomycosis) E. Aortic dissection (with leakage into
E. Other infections (syphilitic, protozoal, pericardial sac)
parasitic) F. Acute myocardial infarction
G. Post irradiation
H. Familial Mediterranean fever
I. Familial pericarditis
1.Mulibrey nanism
J. Metabolic (myxedema, cholesterol)

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III. Pericarditis presumably related to hypersensitivity or autoimmunity

A. Rheumatic fever
B. Collagen vascular disease (SLE, RA, ankylosing spondylitis, scleroderma,
granulomatosis with polyangiitis [Wegener’s])
C. Drug-induced (e.g., procainamide, hydralazine, phenytoin, isoniazid, minoxidil,
anticoagulants, methysergide)
D. Postcardiac injury
1. Post pericardiotomy
2. Posttraumatic
3. Post myocardial infarction (Dressler’s syndrome)

ACUTE PERICARDITIS

➢ Pericardial inflammation of < 6wks


➢ Acute pericarditis, by far the most common pathologic process involving the
pericardium
➢ Can occur in a wide variety of diseases, but the majority of cases are
idiopathic
➢ Most cases of acute idiopathic pericarditis are presumed to be viral in
etiology

CLINICAL MANIFESTATIONS OF ACUTE PERICARDITIS:

Acute pericarditis has four principal diagnostic features


1. Chest pain
2. Pericardial friction rub
3. ECG features
4. Pericardial effusion
➢ Chest pain present in >95%
✓ The pain of pericarditis is often severe
✓ Often sharp pleuritic, but can be constricting
✓ It is most commonly retrosternal, but can also be centered in the left
anterior chest or epigastrium
▪ referred to neck arms and shoulder
✓ The most characteristic radiation is the trapezius ridge, which is
highly specific for pericarditis
✓ Characteristically, pericardial pain intensified by lying supine, and
relieved by sitting up and leaning forward
✓ Associated symptoms can include dyspnea, cough, and occasionally
hiccups
➢ Hx of an antecedent fever and URTI may suggest viral causes of
pericarditis
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➢ The differentiation of Acute MI from acute pericarditis may be challenging


when, with the latter, serum biomarkers of myocardial damage such as
troponin and creatine kinase-MB rise, presumably because of concomitant
involvement of the epicardium in the inflammatory process (an epi-
myocarditis) with resulting myocyte necrosis. However, these elevations, if
they occur, are quite modest compared to those in Acute MI, given the
extensive ST-segment elevation in pericarditis.
P/E
➢ Uncomfortable and anxious
➢ Low-grade fever
➢ Sinus tachycardia
➢ Pericardial friction rub

DIFFERENTIAL DIAGNOSIS

Pneumonia or pneumonitis with pleurisy (which may coexist with pericarditis)


Pulmonary embolus/infarction
Costochondritis,
GERD
MI
Other considerations include
o Aortic dissection
o Intraabdominal processes
o Pneumothorax, and
o Herpes zoster pain before skin lesions appear

Initial Approach to the Patient with Definite or Suspected Acute Pericarditis

1. If diagnosis is suspected but not certain → check frequently for pericardial


friction rub and do ECG frequently
2. If diagnosis is certain → do the following to determine etiology, associated
condition and CXN
✓ CXR
✓ ECHO
✓ CK with MB fraction, Troponin I
✓ Serum ANA for young females
✓ Initiate therapy with NSAID

ECG FINDINGS IN ACUTE PERICARDITIS

✓ Stage 1: There is widespread elevation of the ST segments, often with


upward concavity, involving two or three standard limb leads and V2 to V6,
with reciprocal depressions only in aVR and sometimes V1, as well as PR-
segment depression. Usually there are no significant changes in QRS
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complexes.
✓ Stage 2: after several days, the ST segments return to normal
✓ Stage 3 :T waves become inverted
✓ Stage 4: ultimately, weeks or months after the onset of acute pericarditis,
the ECG returns to normal

For more read from chapter 22 of short cases (click here → Chapter 22; Basics of
ECG and ECG interpretation)

Echo
• Presence of pericardial effusion and its hemodynamic effect

MANAGEMENT OF ACUTE PERICARDITIS

Acute idiopathic pericarditis is a self-limited disease without significant


complications or recurrence in 70 to 90%
✓ If lab data support acute idiopathic pericarditis symptomatic treatment with
NSAID’s should be initiated
Anti-inflammatory agents
o NSAIDS: ibuprofen, ASA
o Steroids → Steroids are used if there is no response after 48hr of taking
NSAID
▪ Prednisone, 1-2 mg/kg/day, PO, daily or BID, for 4-6 wks, followed
by gradual tapering.
▪ use concurrent NSAID
o Colchicine
▪ Chronic +/- NSAID
▪ Useful in recurrent pericarditis
Rx depending on the etiology
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➢ Antibiotics → Purulent pericarditis


➢ Anti TB → TB pericarditis

Complications of acute pericarditis

1. Pericardial Effusion
2. Cardiac Tamponade
3. Constrictive Pericarditis (1%)
4. Recurrence (15-30% in idiopathic)

1. PERICARDIAL EFFUSION AND TAMPONADE

Accumulation of fluid in the pericardial space in a quantity sufficient to cause


serious obstruction to the inflow of blood to the ventricles results in cardiac
tamponade
It is not only the amount but the rate of fluid accumulation determines the
development of cardiac tamponade
o The quantity of fluid necessary to produce this critical state may be as
small as 200 mL when the fluid develops rapidly or >2000 mL in slowly
developing effusions when the pericardium has had the opportunity to
stretch and adapt to an increasing volume
This complication may be fatal if it is not recognized and treated promptly
Any of cause of acute pericarditis can cause pericardial effusion and
tamponade
Those causes of effusion with a high incidence of progression to tamponade
are bacterial (including mycobacteria), fungal, uremic and neoplastic
involvement
The frequency of the different causes of pericardial effusion varies in published
reports

CLINICAL FEATURES
Occasionally, large, asymptomatic chronic effusions are discovered when
CXR is obtained for an unrelated reason
Pericardial pain
Dyspnea (in tamponade)
Tachycardia is the rule unless heart rate lowering drugs have been
administered, conduction system disease coexists, or a preterminal
bradycardic reflex has supervened
Apical impulse may not be palpable
ed cardiac dullness
Friction rub may disappear
Ewart’s sign (the base of the left lung may be compressed by pericardial
fluid and produce an area dullness and increased fremitus (and egophony)
beneath the angle of the left scapula)
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Beck's triad → severe tamponade


• Hypotension
• Muffled heart sounds
• Elevated JVP
uncomfortable patient, with signs reflecting varying degrees of reduced
cardiac output and shock including tachypnea; diaphoresis; cool extremities;
peripheral cyanosis; depressed sensorium
Hypotension is usually present, although in early stages compensatory
mechanisms maintain the blood pressure
A paradoxical pulse

DIAGNOSTIC APPROACH

1. ECG: low QRS voltage and electrical alternans.


2. CXR:
❑ The cardiac silhouette remains normal until pericardial effusions are at
least moderate in size.
❑ With moderate and larger effusions, the anteroposterior cardiac silhouette
assumes a rounded, flask like appearance.
❑ The lungs characteristically appear oligemic

CXR in pericardial effusion

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3. ECHO; Assess the hemodynamic impact:


4. Establish the cause: laboratory tests and pericadiocentesis and biopsy

MANAGEMENT
❖ Treatement of the underlying disease
❖ Management of cardiac tamponade
➢ Fluid resucitation
➢ Fluid drainage: the choice between open drainage and
pericardiocentesis is based upon local preference and experience,
and upon individual patient considerations

2. CONSTRICTIVE PERICARDITIS

❖ It is the end stage of an inflammatory process involving the pericardium


❖ The result of scarring and consequent loss of elasticity of the pericardial
sac
❖ The pathological changes are chronic inflammation, sometimes with
calcification.
❖ Pericardium is thicker than normal in approximately 80 % of cases
❖ In the developed world the cause is most commonly idiopathic, postsurgical,
or radiation injury
❖ TB was the most common cause in in developing countries
❖ Although constriction can follow an initial insult by as little as several
months, it usually takes years to develop
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PATHOPHYSIOLOGY
Inability of the ventricles to fill because of the limitations imposed by the rigid,
thickened pericardium
Ventricular filling is unimpeded during early diastole but is reduced abruptly
when the elastic limit of the pericardium is reached, whereas in cardiac
tamponade, ventricular filling is impeded throughout diastole
Despite these hemodynamic changes, myocardial function may be normal or
only slightly impaired

CLINICAL MANIFESTATION

✓ Weakness, fatigue, weight gain, ascites and edema are common


✓ Chronically sick looking
✓ In advanced cases there are anasarca, skeletal muscle wasting, and cachexia
✓ Exertional dyspnea is common, and orthopnea may occur, although it is usually
not severe
✓ Distended neck veins
✓ venous pressure may fail to decline during inspiration (Kussmaul's sign)
✓ The pulse pressure is normal or reduced
✓ In 1/3 of the cases, a paradoxical pulse can be detected
✓ Congestive hepatomegaly
✓ Ascites is common and is usually more prominent than dependent edema
✓ The apical pulse is reduced and may retract in systole (Broadbent's sign)
✓ The heart sounds may be distant; an early 3rd heart sound, i.e., a pericardial
knock, at the cardiac apex, it occurs with the abrupt cessation of ventricular
filling
✓ Murmur of TR

DIFFERENTIAL DIAGNOSIS
Restrictive cardiomyopathy
Cardiac tamponade
Core pulmonale
Tricuspid stenosis

INVESTIGATIONS
❖ ECG:
➢ Low voltage of the QRS complexes
➢ Diffuse flattening or inversion of the T waves.
➢ Atrial fibrillation (in about 1/3 of patients)
❖ CXR: shows a normal or slightly enlarged heart; pericardial calcification is
most common in tuberculous pericarditis

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Picture; CXR showing marked pericardial calcifications in a patient with constrictive


pericarditis

❖ ECHO
❖ CT/MRI scan
❖ Cardiac catheterization

MANAGEMENT OF CONSTFICTIVE PERICARDITIS

Pericardial resection is the only definitive treatment,


✓ Dietary sodium restriction and diuretics are useful during preoperative
preparation
✓ Digoxin is usefull postoperatively
Treatement of the underlying cause like tuberculosis is equally important

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1.9 Cardiomyopathy (CMP) and myocarditis

A. Cardiomyopathy (CMP)

A heterogeneous group of diseases of the myocardium associated with


mechanical and/or electrical dysfunction that usually exhibit inappropriate
ventricular hypertrophy or dilatation and are due to a variety of causes that
frequently are genetic
CMP’s Are diseases of heart muscle that result from a myriad of insults such
as genetic defects, cardiac myocyte injury, or infiltration of myocardial tissues
The term was previously reserved for primary diseases of the heart muscles,
not including processes affecting valvular structures, coronary vasculature, or
pericardium
Because of the recognition of the final common pathway phenomenon, the use
of the term cardiomyopathy to denote specific cardiomyopathies such as
ischemic cardiomyopathy or valvular cardiomyopathy has entered into common
use

Classification
A. Etiologic classification
❖ Primary cardiomyopathies→ Predominantly involving the heart; Are further
subdivided in to
✓ Genetic
✓ Acquired
✓ Mixed
❖ Secondary cardiomyopathies → Accompanied by other organ system
involvement

B. Morphologic classification
✓ Based on echocardiographic and autopsy findings
➢ Dilated cardiomyopathy (DCMP)
➢ Restrictive cardiomyopathy (RCMP) and
➢ Hypertrophic cardiomyopathy (HCMP)

General presentation
Early symptoms often relate to exertional intolerance with SOB or fatigue
Progressive SOB
Nocturnal cough
Chest pain
Peripheral oedema and ascites
Arrhythmias
Embolic events

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 ECG
 CXR
 ECHO (two-dimensional and Doppler)
 Chemistry:
✓ Na, K, Ca, Mg, RBS/FBS, U/A, Creatinine and BUN, Albumin, total
protein, LFT, Lipid profile, TSH, Creatine kinase, Serum iron,
transferrin saturation,
 Hematology:
✓ Hgb, CBC, ESR

Initial Evaluation Only in Patients Selected for Possible Specific Diagnosis

❖ Titers for infection in presence of clinical suspicion:


➢ Acute viral (coxsackie virus, echovirus, influenza virus)
➢ HIV
➢ Chagas' disease
➢ Lyme disease
➢ Toxoplasmosis
❖ Catheterization with coronary angiography in patients with angina who are
candidates for intervention
❖ Serologies for active rheumatologic disease
❖ Endomyocardial biopsy including sample for electron microscopy when
suspecting specific diagnosis with therapeutic implications
❖ Screening for sleep-disordered breathing

Table; Presentation with Symptomatic Cardiomyopathy

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Table; Investigation finding with Cardiomyopathy

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1. Dilated cardiomyopathy (DCMP)

It is the most common cardiomyopathic phenotype


DCMP may occur at any age, it most commonly becomes apparent
clinically in the 3rd or 4th decades of age
DCMP phenotype is often viewed as a “final common pathway” of
numerous types of cardiac injuries
LV and/or RV systolic pump function is impaired, leading to progressive
cardiac dilatation (remodeling)
1/3rd of cases are familial
Characterized by an enlarged left ventricle with decreased systolic function
Systolic failure is more marked than diastolic dysfunction
MR commonly develops as the valvular apparatus is distorted and is
usually substantial by the time heart failure is severe
Dilation and decreased function of the right ventricle may result from
 Initial injury
 Mechanical interaction with the failing left ventricle
 Elevated afterload presented by secondary pulmonary hypertension

Etiology
1. Idiopathic(primary)- 2/3rd of cases
2. Secondary:
❖ Post infectious (viral myocarditis/ coxsackie, adenovirus, HIV, hepatitis C/,
parasitic/ T. cruzi—Chagas’ disease, trypanosomiasis, toxoplasmosis/,
bacterial/ diphtheria/, spirochetal/ Borrelia burgdorferi—Lyme disease)/,
Rickettsial /Q fever/, Fungal /with systemic infection/)
❖ Toxic (alcohol, chemotherapeutics, heavy metals)
❖ Metabolic (nutritional deficiency, endocrinopathies/ Thyroid disease,
Pheochromocytoma, Diabetes/, electrolyte deficiencies/ Ca, Mg,
Phosphate/, obesity, hemochromatosis)
❖ Peripartum cardiomyopathy
❖ A reversible form of DCM may be found with alcohol abuse, pregnancy,
thyroid disease, cocaine use, and chronic uncontrolled tachycardia

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1.1 Peripartum cardiomyopathy (PPCMP)

❖ Develops within the 3rd trimester or within the first 6 months after delivery
❖ Risk factors
✓ Increased maternal age
✓ Increased parity
✓ Twin pregnancy
✓ Malnutrition
✓ Use of tocolytic therapy for premature labor
✓ Preeclampsia

❖ Exact cause unknown


✓ Cross-reactivity of anti-uterine antibodies against cardiac muscle
✓ Abnormal prolactin cleavage fragments triggering myocardial necrosis
✓ Increased antiangiogenic signaling

1.2 Alcoholic cardiomyopathy

❖ Alcohol is the most common toxin implicated in chronic DCMP


❖ Excess consumption may contribute to > 10% of cases of heart failure
❖ The alcohol consumption necessary to produce cardiomyopathy in an
otherwise normal heart has been estimated to be 5-6 drinks daily for 5-10
years
 Frequent binge drinking may also be sufficient

Treatment
✓ Abstinence from alcohol
✓ Diuretics and neurohormonal antagonists

CLINICAL FEATURES OF DCMP

Symptoms of left- and right-sided CHF usually develop gradually


Some patients have LV dilatation for months or even years before
becoming symptomatic
Although vague chest pain may be present, typical angina pectoris is
unusual and suggests the presence of IHD
Syncope due to arrhythmias and systemic embolism (often emanating from
a ventricular thrombus)
Cardiomegaly and CHF findings
Narrow pulse pressure and raised JVP (In advanced disease)
S3 & S4 gallop
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INVESTIGATIONS

❖ CXR:
✓ Enlargement of the cardiac silhouette due to LV dilatation
✓ The lung fields may demonstrate pulmonary vascular redistribution
and interstitial or, in advanced cases, alveolar edema

CXR; demonstrates marked enlargement of the cardiac silhouette compatible with a DCMP.
Cardiomegaly is nonspecific and can be seen with any etiology of cardiomyopathy.
❖ ECG:
✓ Sinus tachycardia or atrial fibrillation, ventricular arrhythmias, left
atrial abnormality, low voltage, diffuse nonspecific ST-T-wave
abnormalities, and sometimes intraventricular and/or AV conduction
defects
❖ Echo, CT, & CMRI
✓ Show LV dilatation, with normal, minimally thickened, or thinned
walls, and systolic dysfunction
❖ BNP level is usually elevated
❖ Cardiac catheterization and coronary angiography are often performed to
exclude IHD

TREATEMENT OF DCMP

Chronic anticoagulation → for the concern of Systemic embolization


Standard therapy of HF is indicated
Treatement of the underlying etiology whenever possible

Prognosis of DCMP

Most patients pursue an inexorably downhill course, and the majority,


particularly those >55 years, die within 4 years of the onset of symptoms
Spontaneous improvement or stabilization occurs in about 1/4th of patients
Patients of African ancestry are more likely to suffer more rapidly
progressive CHF and death than Caucasians
Death is due to either progressive HF or ventricular tachy- or
bradyarrhythmia; SCD is a constant threat
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2. HYPERTROPHIC CARDIOMYOPATHY(HCMP)

❖ HCM is characterized by a thickened but nondilated left ventricle in the


absence of another cardiac or systemic condition capable of producing the
magnitude of hypertrophy such as: HTN, AS
❖ LVH is asymmetric, often with preferential hypertrophy of the interventricular
septum
 Septal hypertrophy > LV free wall hypertrophy
❖ The most common of the genetic cardiovascular diseases

Variants of HCM

8 - 10% 15 - 20%

65 - 70%

PATHOPHYSIOLOGY OF HCM

Left ventricular outflow obstruction


☛ LV outflow tract is narrowed in classic obstructive HCM by septal
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hypertrophy and, in some patients, by anterior displacement of the


mitral valve (systolic anterior movement)
✓ Increased LV contractility
✓ Decreased ventricular preload
✓ Decreased aortic impedance and pressure (afterload)
Myocardial ischemia
Diastolic dysfunction
Arrythmia

CLINICAL MANIFESTATIONS OF HCM

➢ The clinical course of HCM is highly variable


➢ Many patients are asymptomatic or mildly symptomatic and may be
relatives of patients with known disease
➢ Usually presents between the ages of 20 and 40 years
➢ The first clinical manifestation may be SCD, frequently occurring during or
after physical exertion
➢ HCM is the most common cause of SCD in young competitive athletes
➢ In symptomatic patients, the most common complaint is dyspnea
➢ Other symptoms include syncope, angina pectoris, and fatigue.
➢ Symptoms are not closely related to the presence or severity of an outflow
pressure gradient
➢ Most patients demonstrate a double or triple apical precordial impulse and
S4 gallop
➢ Those with intraventricular pressure gradients may have a rapidly rising
arterial pulse
➢ The hallmark of obstructive HCM is systolic murmur (MR, TR)

INVESTIGATION

ECG: LVH and widespread deep broad Q wave, tachyarrhythmias


CXR: may be normal, mild to moderate increase in the cardiac silhouette
ECHO:
 Demonstrates LV hypertrophy, often with the septum 1.3x the
thickness of the posterior LV free wall. The septum may demonstrate
an unusual "ground-glass" appearance, probably related to its
myocardial fibrosis.
 SAM of MV, often accompanied by MR, is found in patients with
pressure gradients.
 The LV cavity typically is small in HCM, with vigorous motion of the
posterior wall but with reduced septal excursion

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TREATEMENT OF HCM

❖ Since SCD often occurs during or just after physical exertion, competitive
sports and very strenuous activities should be proscribed
❖ Dehydration should be avoided, and diuretics used with caution in
congested patients
❖ Beta- blockers drugs and verapamil
✓ Decrease HR and increase the length of time for diastolic filling, as
well as to decrease the inotropic state
 Amiodarone reduces frequency of arrythmias
❖ Diuretics, nitrates, dihydropyridine calcium blockers, vasodilators, and -
adrenergic agonists are best avoided, particularly in patients with known LV
outflow tract pressure gradients
❖ Alcohol ingestion may produce sufficient vasodilatation to exacerbate an
outflow pressure gradient
❖ Atrial fibrillation is poorly tolerated, and a strong effort should be made to
restore and then maintain sinus rhythm and slow rate
✓ Beta blockers
✓ Amiodarone
✓ Non-dihydropyridine calcium channel blockers
✓ Electrical cardioversion
❖ Surgical myotomy/myectomy and alcohol septal ablation can also reduce
obstruction and improve symptoms
❖ The insertion of an ICD should be considered in patients with a high-risk
profile for SCD
✓ Two or more risk factors for SCD

Risk factors for SCD in HCMP

History of cardiac arrest or spontaneous sustained ventricular tachycardia


Syncope
Family history of sudden cardiac death
Spontaneous non-sustained ventricular tachycardia
LV thickness >30 mm
Abnormal blood pressure response to exercise

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3. RESTRICTIVE CARDIOMYOPATHY (RCMP)

The hallmark of RCMP is abnormal diastolic function; the ventricular walls


are excessively rigid and impede ventricular filling
The least common of the three cardiomyopathies
Partial obliteration of the ventricular cavity by fibrous tissue and thrombus
contributes to the abnormally increased resistance to ventricular filling
In late stages systolic function is also impaired
Myocardial fibrosis, hypertrophy, or infiltration due to a variety of causes is
responsible

Causes

❖ Infiltrative disorders
✓ Amyloidosis
✓ Storage disorders
✓ Hemochromatosis
✓ Inherited metabolic defects
➢ Fabry’s disease
➢ Glycogen storage disease
❖ Fibrotic
✓ Radiation
✓ Scleroderma
✓ Endomyocardial
✓ Tropical endomyocardial fibrosis (EMF)
✓ Hyper eosinophilic syndrome (Loffler’s endocarditis)
✓ Carcinoid syndrome

CLINICAL FEATURES

Exercise intolerance and dyspnea are usually prominent


✓ Thromboembolic complications are common
Commonly have dependent edema, ascites, and an enlarged, tender, and
often pulsatile liver
✓ More right sided symptoms
Kussmaul’s sign is positive
Distant heart sounds
S4 and S3 gallop (S4 is more common than S3)

☛ Unlike constrictive pericarditis the apex impulse is usually easily palpable,


and MR is more common

Investigations
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✓ ECG often shows Low-voltage, nonspecific ST-T-wave abnormalities and


various arrhythmias
✓ Echo, CTI, and CMRI typically reveal
 Symmetrically thickened LV walls and normal or slightly reduced
ventricular volumes and systolic function;
 The atria are usually dilated
 Intramural thrombus

☛ Differentiation of RCMP from constrictive pericarditis is of importance


because the latter is often curable by surgery

Treatment of RCMP

Treatment of heart failure


➢ Diuretics
➢ Neurohormonal antagonists
➢ Cautious use of digoxin
Treatment of underlying causes
➢ Management is usually disappointing, except for hemochromatosis
and Fabry's disease
Chronic anticoagulation is often recommended to reduce the risk of
embolization from the heart
Prognosis depends on the underlying cause

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B. Myocarditis

❖ Myocarditis (inflammation of the heart) can result from multiple causes but is
most commonly attributed infective agents that can injure the myocardium
through direct invasion, production of cardiotoxic substances, or chronic
inflammation with or without persistent infection.
❖ Classified as
➢ Infectious and non-infectious myocarditis (The paradigm of noninfective
inflammatory myocarditis is cardiac transplant rejection)
➢ Acute, subacute and chronic myocarditis
❖ Infectious myocarditis has been reported with almost all types of infective
agents but is most commonly associated with viruses and the protozoan
trypanosoma cruzi → T.cruzi infection is not ever seen yet in Ethiopia
❖ Myocarditis is often associated with systemic inflammatory diseases, such as
polymyositis and dermatomyositis, which affect skeletal and cardiac muscle.

Clinical presentation of viral myocarditis

The typical patient with presumed viral myocarditis is young to middle-aged


adult who develops progressive dyspnea and weakness within a few days
to weeks after a viral syndrome
Typical signs of CHF occur and may progress rapidly to shock, atrial or
ventricular arrhythmias, and sudden death.
Fulminant presentation with fever, respiratory distress, tachycardia,
hypotension, gallop rhythm, and murmur (HSM at apex = MR)
Cardiac findings include overactive precordial impulse, gallop rhythm,
murmur of MR.
Chest pain- due to pericardial involvement
o Myopericarditis
o Arrhythmias
Pulmonary or systemic emboli

Investigation

➢ ECG
➢ Echo
➢ Cardiac troponins
➢ Creatine phosphokinase
➢ Cardiac MRI
➢ Endomyocardial biopsy
o Indications
▪ Presentation with ventricular tachyarrhythmias
▪ Suspicion of alternative diagnosis such as sarcoidosis and giant
cell myocarditis
➢ Circulating viral titers between acute and convalescent blood samples
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Management

There is currently no specific therapy recommended during any stage of viral


myocarditis.
During acute infection, therapy with anti-inflammatory or immunosuppressive
medications is avoided, as their use has been shown to increase viral
replication and myocardial injury
Benznidazole and nifurtimox which for chronic T. cruzi infection.
Treatment of other infectious causes of myocarditis
Supportive care
Inotropic agents, preferably milrinone, should be entertained but used with
caution because of their proarrhythmic potential.
Diuretics, ACE inhibitors, and ARB’s are of use in patients with compensated
CHF but may be contraindicated in those presenting with fulminant heart failure
and cardiovascular collapse
If significant atrial or ventricular arrhythmias, specific antiarrhythmic agents
(amiodarone) and anticoagulants should be administered and ICD placement
considered.

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1.10 Acute HF (Cardiogenic


shock and Pulmonary
edema)
➢ Cardiogenic shock (CS) and pulmonary edema (PE) are life-threatening
high acuity conditions that require treatment as medical emergencies,
usually in an ICU or cardiac ICU (CICU).
➢ The most common joint etiology is severe left ventricular (LV) dysfunction
from myocardial infarction (MI) that leads to pulmonary congestion and/or
systemic hypoperfusion.
These are classified based on the relative absence and/or presence of
congestion and hemodynamic compromise.
Key Questions
✓ Does the patient have heart failure?
✓ If so which syndrome among the acute heart failure syndromes?
✓ Is it a new onset or worsening of a previously known cardiac
disease?
✓ Is there a treatable precipitating factor?
✓ Does the patient require admission to the ICU or a general
medical ward?

Acute heart failure sydromes

Two-minute hemodynamic profile


assessment: Patients presentation can be
fitted in either of these syndromes.

Warm=good systemic perfusion

Cold=hypoperfusion (Cardiogenic shock


No PE or CS (only Predominant PE CS=Cardiogenic shock
worsened congestion)
Dry=No lung congestion

Wet= Lung congestion (Pulmonary Edema)

PE=Pulmonary Edema
Predominant CS Both PE and CS

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Factors leading to less rapid deterioration Factors leading to rapid deterioration


✓ Non adherence to drugs/diet or under dosage ✓ Tachy/brady arrhythmia
✓ Infections (pneumonia, IE) ✓ Acute Coronary Syndrome (ACS)
✓ Anemia ✓ Acute pulmonary embolism
✓ Thyroid disorders ✓ Hypertensive crisis
✓ Pregnancy ✓ Cardiac tamponade
✓ Renal failure ✓ Aortic dissection
✓ Drugs (BB, CCB, NSAIDS)

Indications for admission


Indications for admission to the ICU Indications for admission to General ward
• Cardiogenic shock • Worsened congestion
• Dyspnea at rest (SO2 < 90% which • Dyspnea at rest (tachypnea or SO2< 90%)
doesn’t improve with intranasal O2) which improves with intranasal O2
• Hemodynamically significant arrhythmia
• Acute Coronary Syndrome (ACS)
• Hypertensive emergency
• Altered mental status

1.10. 1 Cardiogenic shock

➔ Refer from Shock under short case of Nitsbin (click here →


3.2. Cardiogenic shock (pump failure))

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1.10.2 Pulmonary edema

➢ Pulmonary edema is a term that is used to describe a particularly dramatic


form of cardiogenic alveolar pulmonary edema
➢ It is often difficult to distinguish between cardiogenic and noncardiogenic
causes of acute pulmonary edema.

Table; suggestive features to distinguish Cardiogenic from Noncardiogenic Pulmonary Edema


Cardiogenic Pulmonary Edema Noncardiogenic Pulmonary Edema
On P/E there is evidence of increased Dominated by the findings of the
intracardiac pressures (S3 gallop, elevated precipitating condition; pulmonary findings
JVP, peripheral edema), and rales and/or may be relatively normal in the early stages.
wheezes on auscultation of the chest. On CXR heart size is normal, alveolar
CXR → radiographic abnormalities typically infiltrates are distributed more uniformly
show Kerley B lines, cardiomegaly (an throughout the lungs, and pleural effusions
enlarged cardiac silhouette), vascular are uncommon.
redistribution, interstitial thickening, and hypoxemia is due primarily to intrapulmonary
perihilar alveolar infiltrates; pleural effusions shunting and typically persists despite high
are common. concentrations of inhaled O2.
hypoxemia is due largely to ventilation- The major causes of noncardiogenic pulmonary
perfusion mismatch and responds to the edema are the ARDS and, less often, high
administration of supplemental oxygen. altitude and neurogenic pulmonary edema. Other
It is most often a result of acute less common causes include;
decompensated heart failure (ADHF) → usually o Pulmonary embolism
due to left ventricular systolic or diastolic o Eclampsia
dysfunction, but may also be due to fluid o Transfusion-related acute lung injury
overload, severe hypertension, renal artery (TRALI).
stenosis, or severe renal disease. o Opioid overdose
o DKA

Cardiogenic pulmonary edema is a common and potentially fatal cause of


acute respiratory distress.
o It is most often a result of acute decompensated heart failure (ADHF)
o ADHF is most commonly due to left ventricular systolic or diastolic
dysfunction, with or without additional cardiac pathology, such as CAD
or valve abnormalities.
o However, a variety of conditions or events can cause cardiogenic
pulmonary edema in the absence of heart disease, including primary
fluid overload (e.g. due to blood transfusion), severe hypertension, renal
artery stenosis, and severe renal disease.
Noncardiogenic pulmonary edema is a distinct clinical syndrome associated with
diffuse filling of the alveolar spaces in the absence of elevated pulmonary
capillary wedge pressure
o Noncardiogenic pulmonary edema is identified clinically by the presence
of radiographic evidence of alveolar fluid accumulation without
hemodynamic evidence to suggest a cardiogenic etiology (i.e. pulmonary
artery wedge pressure ≤18 mmHg).
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o The accumulation of fluid and protein in the alveolar space leads to


decreased diffusing capacity, hypoxemia, and shortness of breath.
o The major causes of noncardiogenic pulmonary edema are the acute
respiratory distress syndrome (ARDS) and, less often, high altitude and
neurogenic pulmonary edema. Other less common causes include;
▪ Opioid overdose
▪ Pulmonary embolism
▪ Eclampsia
▪ Transfusion-related acute lung injury (TRALI).
o Hypoalbuminemia alone is not a cause of pulmonary edema.
o Neurogenic pulmonary edema (NPE) is one form of noncardiogenic
pulmonary edema with an increase in pulmonary interstitial and alveolar
fluid that is due to an acute central nervous system injury and usually
develops rapidly after the injury. It is sometimes classified as a form of
ARDS, but its pathophysiology and prognosis are different.

Pathophysiology
❖ Pulmonary edema is due to the movement of excess fluid into the alveoli
as a result of an alteration in one or more of Starling's forces.
❖ In cardiogenic pulmonary edema, a high pulmonary capillary pressure (as
estimated clinically from the pulmonary artery wedge pressure) is
responsible for the abnormal fluid movement. In contrast, noncardiogenic
pulmonary edema is caused by various disorders in which factors other
than elevated pulmonary capillary pressure are responsible for protein and
fluid accumulation in the alveoli
❖ Cardiogenic pulmonary edema is characterized by increased transudation of
protein-poor fluid into the pulmonary interstitium and alveolar spaces.
❖ The primary etiologic factor is a rapid and acute increase in left ventricular
filling pressures and left atrial pressure, usually associated with a reduction
in cardiac output.

Clinical features
▪ Acute pulmonary edema usually presents with the
o Rapid onset of dyspnea at rest
o Tachypnea
o Tachycardia, and
o Severe hypoxemia (SO2< 90%).
▪ Other features include;
o Cardiorespiratory distress
o High/normal BP
▪ Hypertension is due to release of endogenous catecholamines.
o Relative dullness
o Decreased air entry
o Fine crepitations (Bilateral basal rales) and wheeze in the lung
▪ Crackles and wheezing due to alveolar flooding and airway
compression from peribronchial cuffing may be audible.
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o Raised JVP
o S3 gallop

Diagnosis
➢ Chest X-ray → CXR finding of pulmonary edema
o Vascular redistribution: cephalization of the vessels (Diversion of
Blood vessel circulation towards the Apex)
o Interstitial edema, peribronchial cuffing, and Kerley B and A lines.
▪ Kerley B lines: seen at the peripheral lung; due to thickened
interlobular septa.
▪ Kerley A lines radiate outward from the hila and may
represent dilation of lymphatic channels.
o Alveolar edema
▪ Bilateral perihilar opacifications
▪ Bat wing/butterfly appearance when severe
▪ Pleural effusions and cardiomegaly are often present.

Note: pulmonary edema is usually symmetric and dependent

Picture; A) Kerley B lines (black arrow); Tiny horizontal lines seen at the periphery of the
basal lung area, perpendicular to the pleura…represent fluid in the interlobular septa. B) PA
CXR: typical batwing distribution of air space disease

➢ Echo → may identify systolic and diastolic ventricular dysfunction and valvular
lesions.
➢ ECG → ST elevation and evolving Q waves are usually diagnostic of acute MI
and should prompt immediate institution of MI protocols and coronary artery
revascularization therapy.
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➢ BNP → when substantially elevated, support heart failure as the etiology of


acute dyspnea with pulmonary edema.

Treatment of pulmonary edema


The treatment of pulmonary edema depends on the specific etiology.
As an acute, life-threatening condition, a number of measures must
be applied immediately to support the circulation, gas exchange, and lung
mechanics.
Simultaneously, conditions that frequently complicate pulmonary edema
must be corrected such as
o Infection
o Acidemia
o Anemia
o AKI
Treatable precipitating causes (e.g. hypertensive crisis, ACS, arrhythmia
like AF) should be looked for and managed promptly

❖ Physical Methods
o In no hypotensive patients, venous return can be reduced by use
of the sitting position with the legs dangling along the side of the
bed.
❖ Oxygen Therapy
o Early oxygenation and ventilation support are lifesaving
o Generally, the goal is O2 saturation of ≥92%, but very high saturation
(>98%) may be detrimental.
o Oxygen should be given in Sitting position
o If SO2< 90%, administer O2 by nasal canula at 4-6 l/min.
o If SO2 doesn’t improve in 10 min, administer high flow O2(10-12 l/min)
by face mask.
o If SO2 is still low, give ventilator support by CPAP in conscious
cooperative patients or intubate if patient cannot protect his /her
airways and put on MV with low PEEP.
o If SO2 is persistently higher than 90% and cardiorespiratory distress
improves with treatment, revert O2 administration to nasal canula and
progressively decrease O2 flow and discontinue
❖ Administer morphine 2-4 mg IV bolus every 2-4 hr.
❖ Furosemide 40mg IV for naïve (intravenous dose which is equal to their
previous oral dose for those already taking oral furosemide) and double
the dose every 1hr until adequate urine output AND crackles in the chest
start to decrease and maintain the dose of furosemide that gave
adequate response every 4hrs for the first 24 hr and decrease frequency
in subsequent days.
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☛ Follow up of response and other management principles are similar to


management of other heart failure syndromes (click here → Management of
heart failure)
For patients not responding adequately to diuretics with systolic BP >110mmHg,
the following vasodilator therapies can be used:
o Sublingual nitroglycerin (0.4 mg × 3 every 5 min) is first-line therapy for
acute cardiogenic pulmonary edema.
o If pulmonary edema persists in the absence of hypotension, sublingual
may be followed by IV nitroglycerin.
o IV nitroglycerine infusion
▪ 10 to 20 µg/minute, with subsequent titration (eg, 10 to 20
µg/minute every 5 to 15 minutes) up to 200 µg/minute or
▪ 0.3 to 0.5 µg/kg/minute with titration (if SBP ≥90 mm Hg) in
increments of 20 µg/minute every 1 to 3 minutes up to 400
µg/minute.
▪ Patients who do not respond hemodynamically with doses of ~200
µg/minute should be considered non-responders
o If nitroglycerine not available, either of the following can be tried.
✓ Isosorbide dinitrate 10mg, PO, TID (8AM, 1PM and 6PM) escalated
to 40mg PO TID or
✓ Captopril 6.25mg to 12.5 mg, PO, TID (target dose; 50mg TID) or
✓ enalapril 2.5 mg, PO, BID, titrated every 6hrs as tolerated to target
dose of 10 mg, PO, BID (maximum: 20 mg/day).
✓ Notice; ACE inhibitors reduce both afterload and preload and are
recommended for hypertensive patients.

For Shock and Pulmonary edema Management when they happen together,
refer chapter 3 from Short case of Nitsbin (click here → 3.6. Shock and
Pulmonary edema Management when they happen together )

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1.10.2.1 ARDS (Acute respiratory distress syndrome)


Acute respiratory distress syndrome (ARDS) is a clinical syndrome of severe
dyspnea of rapid onset, hypoxemia, and diffuse pulmonary infiltrates leading to
respiratory failure.
ARDS is caused by diffuse lung injury from many underlying medical and
surgical disorders.
The lung injury may be direct, as occurs in toxic inhalation, or indirect, as
occurs in sepsis.
ARDS is defined by three categories based on the degrees of hypoxemia.
These stages of mild, moderate, and severe ARDS are associated with
mortality risk and with the duration of mechanical ventilation in survivors.
Previously it was called shock lung, adult respiratory distress syndrome.
Subsequent recognition that individuals of any age could be afflicted led to the
current term, acute respiratory distress syndrome (ARDS).
Clinical hallmarks of ARDS are hypoxemia and bilateral radiographic opacities,
while the pathological hallmark is diffuse alveolar damage (i.e. alveolar edema
with or without focal hemorrhage, acute inflammation of the alveolar walls, and
hyaline membranes).
ARDS is associated with a variety of risk factors and etiologies. These
conditions are grouped together under the term ARDS because the clinical,
physiological features, pathological features, and management are similar
regardless of the inciting event.

Etiologies and predisposing factors

More than 60 possible causes of ARDS have been identified and other potential
causes continue to emerge as adverse pulmonary reactions to new therapies are
observed

Table; list of conditions associated with ARDS

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1. Sepsis → the most common 14. Leucoagglutinin reactions


cause of ARDS 15. Acute Pancreatitis
2. Aspiration 16. Near drowning
3. Infectious pneumonia 17. Smoke inhalation
4. Severe trauma 18. Cardiopulmonary bypass
5. Pulmonary contusion 19. Following bone marrow
6. Multiple fractures transplantation
7. Amniotic fluid embolism 20. Acute eosinophilic pneumonia*
8. Neurogenic pulmonary edema 21. Bronchiolitis obliterans organizing
9. Surface burns pneumonia (BOOP)*
10. Multiple blood transfusions → 22. Miliary tuberculosis*
Transfusion-related acute lung 23. Other risk factors
injury (TRALI) o Cigarette smoking
11. Following upper airway o Cardiopulmonary bypass
obstruction o Thoracic surgery
12. Venous air embolism o Pneumonectomy
13. Drugs and alcohol → Drug o Obesity
overdose and drug reactions o Blood type A

*Specific treatment required

CLINICAL FEATURES

✓ The clinical features of ARDS usually appear within 6 to 72 hours of an


inciting event and worsen rapidly.
✓ Patients typically present with;
o Dyspnea
o Cyanosis (i.e. hypoxemia)
o Diffuse crackles.
✓ The bilateral alveolar infiltrates and diffuse crackles are
persistent
o Respiratory distress is usually evident, including tachypnea,
tachycardia, diaphoresis, and use of accessory muscles of
respiration.
o A cough and chest pain may also exist.
✓ Clinical findings related to the precipitant may also exist at presentation.
As an example, in patients with ARDS due to sepsis, there may be fever,
hypotension, leukocytosis, lactic acidosis, and DIC.

Investigations

➢ Sepsis work up based on septic focus → CBC, ESR and CRP, U/A, S/E,
Culture, CXR
➢ CXR → The initial chest radiograph typically has bilateral alveolar infiltrates

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➢ Chest CT → usually reveals widespread patchy or coalescent airspace


opacities that are usually more apparent in the dependent lung zones. The
infiltrates do not have to be diffuse or severe, as bilateral infiltrates of any
severity are sufficient.

➢ ABG analysis → Arterial blood gases reveal hypoxemia, which is often


accompanied by acute respiratory alkalosis and an elevated alveolar-arterial
oxygen gradient. High concentrations of supplemental oxygen are generally
required to maintain adequate oxygenation.
➢ Microscopic (pathologic) evaluation → lower respiratory samples can be taken
by
o Flexible bronchoscopy
o Lung biopsy → it should be reserved for carefully selected patients
whose acute hypoxemic respiratory failure remains of uncertain etiology
after nondiagnostic flexible bronchoscopy if one or more of the diagnostic
possibilities under consideration might warrant targeted therapy or would
substantially change the prognosis. Examples include cryptogenic
organizing pneumonia, an acute fungal lung infection, an acute
exacerbation of a chronic interstitial lung disease, vasculitis, or
disseminated cancer.

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Clinical course and pathologic stages

Diffuse alveolar damage (DAD) is the most common pathologic finding seen in
patients with ARDS.
1. “acute/exudative phase → Common findings during the first week include
eosinophilic hyaline membranes, intra-alveolar edema, congestion of the
capillaries, widening of the interstitium, and extensive thrombi caused by
localized coagulation abnormalities
2. Proliferative phase → Later findings include expansion of the interstitium
with loose, myxoid fibroblastic tissue, type 2 pneumocyte hyperplasia,
squamous metaplasia, thrombi, and vascular remodeling. Some patients
progress to a fibrotic stage, characterized by obliteration of normal lung
architecture, diffuse fibrosis, and cyst formation.

DIAGNOSTIC EVALUATION

➢ The diagnostic evaluation is aimed at identifying specific causes of ARDS that


are amenable to treatment and excluding other conditions that also present
with acute hypoxemia, bilateral alveolar infiltrates, and respiratory distress.
➢ Because the current international consensus definition of ARDS (see
'Diagnostic criteria' below) specifies no criteria relating to the underlying
etiology of acute bilateral inflammatory lung injury, some uncertainty remains
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with respect to which conditions should or should not be included under the
ARDS diagnostic umbrella.
➢ Generally included are disorders that are known to cause diffuse alveolar
damage and have the potential to resolve over time.
➢ Thus, viral or diffuse bacterial pneumonia and acute inhalational injuries are
included, whereas eosinophilic pneumonia and diffuse alveolar hemorrhage
associated with collagen vascular diseases are not.
➢ R/o Cardiogenic pulmonary edema
o It is the primary alternative that needs to be excluded because it is
common and can be clinically indistinguishable from ARDS.
o See clinical features from the table above (Distinguishing features of
Cardiogenic from Noncardiogenic Pulmonary Edema) → Absence of these
features helps distinguish ARDS from cardiogenic pulmonary edema
o Distinguishing cardiogenic pulmonary edema from ARDS can be aided by
measurement of a brain natriuretic peptide (BNP) level, echocardiography,
and, less often, right heart catheterization.
➢ Excluding other causes of hypoxemic respiratory failure

DIAGNOSTIC CRITERIA (Berlin definition)

ARDS can be diagnosed once cardiogenic pulmonary edema and alternative


causes of acute hypoxemic respiratory failure and bilateral infiltrates have been
excluded.
The Berlin Definition of ARDS requires that all of the following criteria be
present to diagnose ARDS:
o Respiratory symptoms must have begun within one week of a known
clinical insult, or the patient must have new or worsening symptoms
during the past week.
o Bilateral opacities consistent with pulmonary edema must be present
on a CXR or CT. These opacities must not be fully explained by
pleural effusions, lobar collapse, lung collapse, or pulmonary nodules.
o The patient’s respiratory failure must not be fully explained by cardiac
failure or fluid overload. An objective assessment (eg,
echocardiography) to exclude hydrostatic pulmonary edema is required
if no risk factors for ARDS are present.
o A moderate to severe impairment of oxygenation must be present, as
defined by the ratio of arterial oxygen tension to fraction of inspired
oxygen (PaO2/FiO2). The severity of the hypoxemia defines the severity
of the ARDS based on ABG analysis:
▪ Mild ARDS – The PaO2/FiO2 is >200 mmHg, but ≤300 mmHg,
on ventilator settings that include positive end-expiratory pressure
(PEEP) or continuous positive airway pressure (CPAP) ≥5 cm
H2O.
▪ Moderate ARDS – The PaO2/FiO2 is >100 mmHg, but ≤200
mmHg, on ventilator settings that include PEEP ≥5 cm H2O.
▪ Severe ARDS – The PaO2/FiO2 is ≤100 mmHg on ventilators
setting that include PEEP ≥5 cm H2O.
The Berlin Definition of ARDS replaces the American-European Consensus
Conference’s definition of ARDS.
o The major changes to the Berlin Definition are that the term “acute
lung injury” has been eliminated, the pulmonary capillary wedge
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pressure (ie, pulmonary artery occlusion pressure) criterion has been


removed, and minimal ventilator settings have been added.
o Despite these definitions, studies suggest that ARDS, in particular mild
ARDS, remains under recognized by clinicians.

Table; Diagnostic Criteria for ARDS


Severity; Mild: 200 mmHg < Pao2/Fio2 ≤ 300 mmHg
oxygenation* Moderate: 100 mmHg < Pao2/Fio2 ≤ 200 mmHg
Severe: Pao2/Fio2 ≤ 100 mmHg
Onset Acute: Within 1 week of a clinical insult or new or worsening
respiratory symptoms.
CXR Bilateral opacities consistent with pulmonary edema not fully
explained by effusions, lobar/lung collapse, or nodules
Absence of left atrial Hydrostatic edema is not the primary cause of respiratory
hypertension failure. If no ARDS risk factor is present, then some
objective evaluation is required (e.g., echocardiography) to
rule out hydrostatic edema
*As assessed on at least 5 cm H2O of positive end expiratory pressure (PEEP).
Abbreviations: ARDS, acute respiratory distress syndrome; Fio2, inspired O2 percentage;
Pao2, arterial partial pressure of O2; PCWP, pulmonary capillary wedge pressure.

Kigali‘s modification of Berlin criteria to diagnose ARDS


➢ New onset/worsening respiratory symptom
➢ Spo2/FIo2 ≤ 315
➢ Bilateral opacities not explained by effusion, lobar/lung collapse or
nodules by CXR or ultrasound
➢ Respiratory failure not fully explained by cardiac failure or fluid overload
(may need objective assessment, such as echocardiography, to exclude
hydrostatic edema if no risk factor present)
o If SpO2 unavailable: suspect ARDS in any patient with worsening
respiratory failure despite receiving supplemental oxygen via nasal
cannula at 5 l/min

DIFFERENTIAL DIAGNOSIS

1. Cardiogenic pulmonary edema


2. An acute exacerbation of idiopathic pulmonary fibrosis or other chronic
ILD
3. Diffuse alveolar hemorrhage
4. Idiopathic acute eosinophilic pneumonia (IAEP)
5. Cryptogenic organizing pneumonia (COP)
6. Acute interstitial pneumonia (Hamman-Rich syndrome)
7. Metastatic Cancer to lung
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Management

ABC of life and Supportive management


o Prone Positioning
o A minority of patients with ARDS die from respiratory failure alone.
More commonly, such patients succumb to their primary illness or to
secondary complications such as sepsis or multiorgan system failure
o Management of hypoxia → By definition, patients with ARDS are
severely hypoxemic. Options available for improving arterial oxygen
saturation (SaO2) include:
✓ Oxygen supplementation
✓ Intubation and mechanical ventilation
o Patients with ARDS require meticulous supportive care, including;
✓ ICU admission for severe cases
✓ Prone positioning (bed elevation)→ improves oxygenation in
the majority of patients with ARDS
✓ Nursing care and positioning for critically ill patients
✓ Intelligent use of sedatives and neuromuscular blockade
▪ Patients with severe ARDS may require sedation for
several days or longer
▪ choice of agent should be driven by the patient’s
specific needs. For example, narcotics may be used for
pain and suppression of the respiratory drive;
benzodiazepines may be used for anxiety; and
antipsychotic agents may be helpful for agitated
delirium
▪ All these agents have potential side effects which
needs evaluation with specialist (if available,
pneumonologist intervention is required)
✓ Analgesics → Morphine
✓ Hemodynamic management
✓ Nutritional support
✓ Control of blood glucose levels
✓ Expeditious evaluation and treatment of nosocomial
pneumonia
✓ Prophylaxis against deep DVT and GI bleeding.
▪ These patients often have multiple risk factors for
venous thrombosis, including prolonged immobility,
trauma, activation of the coagulation pathway, and
predisposing illnesses, such as sepsis, obesity, and
malignancy. Thus, all patients admitted to intensive
care units require some form of thromboprophylaxis
▪ Stress ulcer prophylaxis → Oral PPI (like omeprazole,
pantoprazole) for critically ill patients who are able to
receive enteral medications, Oral PPI or H2 blockers
(like cimetidine) for critically ill patients who cannot
receive enteral medications
Pharmacologic management
o Lasix for pulmonary edema → look at above
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✓ Conservative strategy of fluid management in patients with


ARDS, as long as hypotension and organ hypoperfusion can
be avoided
o Macrolides like azithromycin, erythromycin have a beneficial effect in
ARDS
o Aspirin has been studied as a preventative agent in patients with
ARDS. However, no role for it in the treatment of ARDS
o Systemic glucocorticoids should be administered to patients when
ARDS has been precipitated by a steroid-responsive process (eg,
acute eosinophilic pneumonia) or in patients in whom steroids have a
proven role (eg, community acquired pneumonia). However, their
administration to patients with ARDS from other causes is controversial
✓ N.B Patients who received glucocorticoids prior to the onset
of ARDS associated with higher mortality
Early detection and treatment of complications

Figure; Algorithm for the initial management of ARDS. Clinical trials have provided
evidence-based therapeutic goals for a stepwise approach to the early mechanical
ventilation, oxygenation, and correction of acidosis and diuresis of critically ill patients with
ARDS.
FiO2, inspired O2 percentage; MAP, mean arterial pressure; PBW, predicted body weight;
RR, respiratory rate; SPO2, arterial oxyhemoglobin saturation measured by pulse oximetry.

Complications
Complications related to mechanical ventilation
o Pulmonary barotrauma
o Nosocomial (Hospital acquired) pneumonia → it is an important
complication among patients with ARDS and can contribute to
increased morbidity, including prolonged mechanical ventilation
Complications related to critical illness and being in the ICU
o Delirium
o DVT
o GI bleeding due to stress ulceration
o Catheter-related infections.
o Poor nutrition 188
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Prognosis and outcomes

ARDS is associated with appreciable mortality, with estimates ranging from 26


to 58%. Mortality increases with disease severity.
The underlying cause of the ARDS is the most common cause of death
among patients who die early. In contrast, nosocomial pneumonia and sepsis
are the most common causes of death among patients who die later in their
clinical course. Patients uncommonly die from respiratory failure
Predictors of death
o Patient-related → The mortality rate increased progressively with age,
ranging from 24% among patients 15 to 19 years of age to 60%
among patients 85 years of age or older. obesity may impact the
mortality
o Disease-related predictors of mortality include severe hypoxemia,
failure of oxygenation to improve, pulmonary vascular dysfunction,
increased dead space, infection, a high severity of illness score, a
non-traumatic cause of the ARDS, and certain biomarkers and gene
polymorphisms.
o Treatment-related predictors of mortality which may be associated with
higher mortality include;
✓ Positive fluid balance
✓ Patients who received glucocorticoids prior to the onset of
ARDS
✓ Patients who receive packed red blood cell transfusions
✓ Patients who are intubated late in the course of the disease

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1.11 WHO risk based CVD (Cardiovascular disease)


Management in Ethiopia

INTRODUCTION TO CV RISK ASSESSMENT

➢ CVDs are number one cause of death globally with estimated 17.9 million
people dying from CVDs in 2016, representing 31% of all global deaths.
➢ Of CVD deaths, 85% are due to heart attack and stroke and about 80% occur
in low- and middle-income countries, often in people less than 60 years of
age.
➢ CVDs are rising alarmingly in Ethiopia on top of already existing CVDs like
RHD, CMP and cor-pulmonale.

1.11.1 CARDIOVASCULAR RISK ESTIMATION

➢ The first WHO risk prediction chart was developed in 2007 and recent
update was made in 2019 where the world was divided into 21 GBD
regions and Ethiopia is represented by the Eastern Sub-Saharan African
Region.
➢ It is with this basis that the national CV working group developed this
risk.

WHO CVD Risk Charts


Definitions of terms

➢ It is worth to define the following terms before using WHO risk charts.
o CV risk: in the WHO risk assessment CV risk refers to the chance
of having fatal or nonfatal heart attack or stroke in the next 10
years with the current risk profile of the patient.
o CV risk factors are any biologic or environmental conditions known
to increase the inherent risk/chance of having CV event. They are
classified into modifiable and nonmodifiable risk factors.
o The following are known modifiable cardiovascular risk factors:
▪ HTN
▪ DM
▪ Dyslipidemia (raised total cholesterol, low HDL, high LDL or
raised TGs)
▪ Overweight/Obesity/Metabolic Syndrome
▪ Low physical exercise
▪ Unhealthy diet (Low fruit intake, excess salt intake,
consumption of high saturated or trans-fat diet)
▪ Smoking
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▪ Excess alcohol intake


▪ Psychosocial Stress
o The non-modifiable risk factors include
▪ Age
▪ Gender
▪ Family history
▪ Race and
▪ Other genetic factors

➢ Cardiovascular disease (CVD): is manifested cardiovascular event


(stroke, heart attack, peripheral arterial, or aortic disease).
➢ Risk chart: is collection of tables of risk estimates with different types
and levels of risk factors.
➢ Primary Prevention: This is control of risk factors before cardiovascular
disease develops.
➢ Secondary Prevention: Prevention of further occurrence or progression of
previous cardiovascular disease.

TYPES OF WHO RISK CHARTS


➢ WHO risk charts were developed for estimation of the chance of future
cardiovascular event in those individuals who never had cardiovascular
diseases.
➢ It does not apply for patients who have already developed
cardiovascular diseases.
➢ There are two types of WHO risk charts based on availability of
laboratory facility to measure blood glucose and cholesterol levels

A. Laboratory-based WHO CVD risk charts

➢ These are CVD risk charts that include measurements of total


cholesterol and information on diabetes mellitus.
➢ The variables needed for using this chart are as follows:
o History:
▪ Age: specific numbers between 40 to 74 years. The risk
prediction doesn’t apply for age category out of the specified
range.
▪ Smoking: current or past history of smoking
▪ Sex: Male OR Female
▪ Diabetes: Yes OR No. If history of diabetes is not known OR
there is no blood sugar determination facility; then risk
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assessment should be done using the other


risk prediction chart (the non-laboratory-based charts)
o Physical Examination
▪ BP: measured value of the systolic blood pressure
o Laboratory
▪ Blood sugar: to diagnose diabetes
▪ Total cholesterol: Measured values of total cholesterol in
mmol/L.
➢ In most of the Ethiopian Laboratories, total cholesterol is in mg/dl units;
but the risk prediction score applies values in mmol/l units.
➢ The cholesterol value in mg/dl should be multiplied by 0.02586 before
applying the value for risk prediction.

B.Non-laboratory-based WHO risk charts

➢ WHO CVD risk (non-laboratory-based) charts can be used to predict


total CVD risk without information on total cholesterol and diabetes.
➢ The non-laboratory-based WHO CVD risk charts are aimed at
stratification in low-resource communities where Cholesterol determination
is not available and office settings and can be used for decisions
regarding referral.
➢ Patients diagnosed to have diabetes and non-diabetic patients with
non-lab-based risk level of > 10% should be considered high risk and
managed accordingly in areas where serum cholesterol cannot be
determined.
➢ To use the non-lab-based chart, the following variables should be
available:
o History:
▪ Age: specific numbers between 40 to 74 years. The risk
prediction doesn’t apply for age category out of the specified
range
▪ Smoking: current smoking
▪ Sex: Male OR Female
o Physical Examination
▪ BP: measured value of the SBP
▪ BMI

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Figure: Steps in selecting appropriate Chart for WHO CV Risk Assessment

INSTRUCTIONS FOR USING THE WHO CVD RISK CHARTS


A. Laboratory- based Risk Chart
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➢ These charts are to be used only for individuals whose status regarding
diabetes and total cholesterol is available

Table: Instructions for using laboratory-based WHO risk Chart

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Figure: Step by Step Instructions for using laboratory based WHO risk
Chart

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Table: Laboratory based WHO risk Chart

B. Non laboratory-based WHO CV Risk Charts

➢ These charts are for the use in settings where blood glucose and
cholesterol cannot be measured

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Table: Instructions for using Non laboratory-based WHO risk Chart

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Figure: Step by Step Instructions for using Non-laboratory based WHO risk
Chart

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Table: Non-Laboratory based WHO risk Chart


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APPLICATIONS OF WHO RISK ASSESSMENT CHARTS

➢ As stated above the WHO risk chart applies for patients who haven’t
been diagnosed to have CVD like stroke, heart attack, peripheral
arterial, or aortic diseases.
➢ For patients with CVD, management should include specific disease
management and more intense risk factor management with lifestyle
interventions and pharmacologic agents.

1. Hypertension (See HTN treatment protocol for details)

➢ Target blood pressure should be < 140/90mmHg in all risk groups


➢ For patients with high WHO risk (>10% with non-lab based and >20%
with lab-based WHO risk), antihypertensive drug should be started to
lower BP below 140/90 on top of life style interventions.
➢ For patients with BP of 140-159/90-99 mmHG and no end-organ
damage or CVD, antihypertensive drug can be started after 3 months
trial of life style interventions to keep BP <140/90mmHG.
➢ For any WHO risk level and BP >160/100mmHG drug should be started
to lower BP below 140/90 on top of life style intervention

2. Dyslipidemia

➢ All patients with WHO risk level > 20% should receive statin as part of
primary prevention.
➢ All patients with TC of 324mg/dl or serum LDL of > 190 if available
should be given statin regardless of risk level.
➢ All diabetic patients older than 40 years should receive statin regardless
of WHO risk level or serum cholesterol level.

3. Lifestyle interventions

➢ All individuals should be encouraged to engage in healthy lifestyle at


any risk level.
➢ If CVD risk is < 10% and no CVD risk factors, reassess CVD risk after
5 years.
➢ Patients with any behavioral (unhealthy diet, smoking, excess alcohol
intake, sedentary life) and physiologic risk factors (obese or patients with
metabolic syndrome) should be routinely evaluated for control of these
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4. Patients with high CVD risks (>20% with lab-based and >10 %
with non-lab based WHO risk Charts)

➢ Are managed like patients with established CVDs.


➢ Statin should be started and preferably referred to specialist center for
better evaluation and initiation of treatments.
➢ Dose: Atorvastatin 20-40mg/day if not available Simvastatin 40mg/day for
primary prevention of CV events.
➢ For patients with previous cardiovascular events or for patients with very
high cholesterol levels (Total cholesterol >320mg and/or LDL cholesterol
>190mg/dl) double the above doses.

Table. Management guidance for total CVD risk


For more about CVD risk assessment refer from Short case of Nitsbin
Under Dyslipidemia (click here → 15.2. Dyslipidemia)
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Chapter 1; Heart failure (ልብ ድካም) and Other Cardiac Disorders

1.12. DM and Hypertension Follow Up Form

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Chapter 2; Chronic lung disorders and Cor pulmonale

Chapter 2; Chronic lung disorders


and Cor pulmonale
Dr. Mulualem. G, Dr. Asmare.W

➢ N.B the approach (Hx, P/E, IX, DDX…) we discussed here is considering Cor
pulmonale 2ry to COPD. If you have a patient with different diagnosis (e.g.
COPD only, Cor pulmonale 2ry to Post TB fibrosis…), you can modify this
approach.

COPD (Chronic obstructive lung disease)

Clinical features and how to write hx of COPD patient


History

➢ COPD patients may present with


o Exacerbation of SOB
o Chronic cough
➢ The three most common symptoms in COPD are cough, sputum production,
and exertional dyspnea.
o Many patients have such symptoms for months or years before
seeking medical attention and may present with exacerbations
o From the three, the most common early symptom is exertional
dyspnea. Less common symptoms include wheezing and chest
tightness.
➢ Chronic cough → a.k.a smoker’s cough
o The cough is intermittent early in the morning at the beginning which
progressively become persistent throughout the day, but is seldom
entirely nocturnal.
o Aggravated by dust and increase in intensity and frequency at night
➢ Sputum production
o Sputum initially occurs in the morning but later will be present all
day long.
o It is usually tenacious and mucoid and in small quantities. Clear,
whitish, yellow or greenish (change in sputum color usually to
purulent suggest infectious exacerbation)
o Usually tenacious and mucoid
o Massive in amount which increase progressively in amount
o Usually abnormal → a mix of saliva and mucus in the airway
➢ SOB (dyspnea, breathlessness) → daily activities can become very difficult
as the condition gradually worsens
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o Insidious in onset
o Progressively worsening (e.g he/she experienced Dyspnea while
doing supra ordinary activities like…. Followed by dyspnea while
doing sub ordinary activities like… and later dyspnoea at rest…
when was the time for each)
o Aggravated by excessive cigarette smoking, adverse atmospheric
condition, infection…
o Activities involving significant arm work, particularly at or above
shoulder level, are particularly difficult for many patients with COPD.
Conversely, activities that allow the patient to brace the arms and
use accessory muscles of respiration are better tolerated. Examples
of such activities include pushing a shopping cart or walking on a
treadmill.
o As COPD advances, the principal feature is worsening dyspnea on
exertion with increasing intrusion on the ability to perform vocational
or avocational activities.
o In the most advanced stages, patients are breathless doing simple
activities of daily living.
o Patients may also develop resting hypoxemia and require institution
of supplemental oxygen.
N.B Common variants of COPD

Chronic bronchitis Emphysema


✓ Cough and sputum production ✓ Permanent Dilatation of the
for at least 3 months in at least Airway below terminal bronchiole
2 consecutive years with alveolar wall destruction.
✓ Predominant productive cough ✓ Predominant SOB
✓ Clinical definition and Dx of ✓ Pathologic definition
exclusion

➢ Wheezing
➢ Chest tightness (squeezing chest pain or chest discomfort which
exacerbated by exertion but no radiation)
➢ Recurrent respiratory infections (cough, runny nose, sore throat, fever…) →
risk factor for exacerbation
➢ GBS if they develop Cor pulmonale.

Cor pulmonale
➢ The symptoms in chronic Cor pulmonale generally are related to the underlying
pulmonary disorder.
➢ In our set up, Cor pulmonale patients usually have longstanding COPD or TB
(e.g. Post TB fibrosis…) then they develop Cor pulmonale (isolated RSHF) smx
➢ They may present with
o Dyspnea or Exacerbation of SOB → the most common symptom
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o Lower-extremity edema and even increased abdominal girth due to


ascites, even may progress to GBS (Generalized body swelling)

For example
➢ SOB Of 2 years duration associated with productive cough with sputum
production. The Patient was diagnosed to have TB 06 years back, Treated and
improved. Currently presented with exacerbation of SOB of two weeks duration
and GBS of one-week duration (characterize GBS in detail) but no orthopnea,
PND or palpitation (absence of these symptoms suggests isolated RSHF) (refer
CHF of Nitsbin for GBS characterization)

Risk factors for COPD

A. Exposure
➢ Cigarette smoking or Environmental tobacco smoke (ETS)
✓ At least 10-20 pack year
❖ 𝑝𝑎𝑐𝑘 𝑦𝑒𝑎𝑟 =
(𝑛𝑢𝑚𝑏𝑒𝑟 𝑜𝑓 𝑐𝑖𝑔𝑎𝑟𝑒𝑡𝑡𝑒 𝑠𝑚𝑜𝑘𝑒𝑑 𝑝𝑒𝑟 𝑑𝑎𝑦) 𝑥 (𝑛𝑢𝑚𝑏𝑒𝑟 𝑜𝑓 𝑦𝑒𝑎𝑟𝑠 ℎ𝑒 𝑜𝑟 𝑠ℎ𝑒 𝑠𝑚𝑜𝑘𝑒𝑑)
20
❖ One pack of cigarette contain 20 cigarettes
✓ Accounts for 85-90% of all cases of COPD → 10-20 % of smokers will
develop COPD & from COPD patients 80-90% are smokers which is
related to genetic and environmental factors
✓ The most common risk factor in westerns for both emphysema and
chronic bronchitis
➢ Air pollution→ indoor or outdoor air pollution
✓ Indoor air pollution
o Common risk factor in our setup (Ethiopia)
o In our setup the most common cause is poor ventilation of
house and indoor smoke produced by biomass fuel
combustion and dust exposure during house cleaning in rural
areas (especially in women)
o 90% of rural household use biomass fuel as a source of
energy (wood, charcoal, vegetable and plant matter, animal
dung)
o In developing countries 50% of COPD death is from biomass
smoke and 75 % are female
✓ Outdoor air pollution → also contributes to the lungs total burden of
inhaled particles, although it appears to have a relatively small effect
in causing COPD.
➢ Occupational exposure → High risk groups include factory workers, coal
mining, cotton textile industry…
o Exposure to organic and inorganic dusts, chemicals agents and
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Chapter 2; Chronic lung disorders and Cor pulmonale

o Inhaled irritants (direct chemical inhalation) such as cadmium,


isocyanates, and fumes result in sudden airway constriction
➢ Respiratory infection → they are the cause of acute exacerbation. E.g.
acute bronchitis
➢ Low socioeconomic status
o Its association with Risk of COPD is not clear. However, this pattern
may be related to indoor and outdoor air pollution, crowding, poor
nutrition, infections or other factors related to low socioeconomic
status.

B. Host Factors

➢ Genetic factors → alpha1 antitrypsin (AAT) deficiency especially for


emphysema. N.B AAT act against lung parenchyma destructive enzymes
(protease/elastase/ and trypsin)
➢ Asthma and airway hyper responsiveness
➢ Old age (Age > 65)
o Over all, aging increase COPD risk. In our set up COPD can
happen in < 65 years old (we didn’t get data about age and COPD
association in Ethiopia)
➢ Gender → common in females, may be associated with high risk of
exposure from indoor pollution
➢ Lung Growth and development
o Any factor that affect lung growth during pregnancy and childhood
(E.g. Low birth weight, neonatal meconium aspiration syndrome,
respiratory infections) has the potential to increase an individual’s risk
of developing COPD during adult hood

Complication of COPD

➢ Cxn related to emphysema


✓ Respiratory insufficiency
✓ Respiratory failure (N.B type I respiratory failure related with hypoxia.
But type II respiratory failure related with hypoxia and hypercapnia)
✓ Pneumonia
✓ Pneumothorax
✓ Pulmonary HTN
➢ Respiratory infection
✓ Common cold
✓ Flue
✓ Pneumonia
✓ Acute bronchitis
➢ Corpulmonale (Isolated RSHF) and Pulmonary HTN
➢ Secondary polycythemia
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➢ MI
➢ Lung ca
➢ Depression→ dyspnea prevent patient from doing enjoy full activities which
lead to depression

Sample history
Sample history of a patient from sanja woreda with the DX of cor pulmonale 2ry to
COPD

Chief compliant
Exacerbation of SOB of 01-week duration

HPI

For the past 20 years, this patient had a progressively increasing intermittent productive
cough with non-foul-smelling, non-blood tinged, sputum of 3-4 Arabic coffee cup per day
which later became increased up-to 10 Arabic coffee cup/day which is aggravated by
dust and increase in intensity and frequency at night.

Four years back she was having insidious onset of progressively increasing shortness of
breath. For this she visited sanja primary hospital where she was admitted and told to
have lung disease (unspecified) after CXR and blood examination was done and she
was on intra nasal oxygen and discharged after 2 weeks of hospital stay. For the same
compliant she had a total of 4 admissions.

Two weeks prior to her admission, she started to experience generalized body swelling
which starts from foot and goes upwards to involve the leg, abdomen and finally the face
associated with stabbing type of RUQ abdominal pain, loss of appetite and Unquantified
but significant weight loss to the extent her closes become loose but no Orthopnea,
PND, chest pain or palpitation.

Currently presented with exacerbation of shortness of breath while doing supra ordinary
activities like fetching water from long distance which later worsen to the extent of
dyspnea at rest.
➢ She cooks 3x/day in muddy kitchen which has no windows. And she has dust
exposure throughout her life while cleaning the house and excreta of cattle’s.
She lives in a family size of 6. all are alive and healthy, they live in iron
corrugated house having 2 rooms, one windows and one door (all are
functional.), they have separate kitchen and toilet room (indoor air pollution)
➢ Her husband is a farmer, she is house wife, Claimed that, their income is
enough to support the family/if possible, quantify/ (socioeconomic status is RF, to assess
Work place dust exposure, such as factory workers, coal mining, cotton textile industry)
➢ She experienced cough, rhinorrhea, fever and sore throat repeatedly where she
was treated at a local health center multiple time. (URTI are RF for exacerbation of
COPD or may happen as a complication of COPD)
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Chapter 2; Chronic lung disorders and Cor pulmonale

➢ No hx of cigarette smoking or hemoptysis (smoking is RF for both COPD, Emphysema


and Lung ca → the last is DDX or CXN)
➢ No family hx of similar illness (genetic→ AAT deficiency)
➢ She usually eats injera made of ‘‘teff’’ and ‘‘machilla’’ and ‘’wott’’ made of
‘‘atter’’ and ‘‘dagusa’’ 3-4 times per day. Occasionally she eats meat during
holidays (nutrition)
➢ No hx of contact with a known TB patient or previous TB treatment (post TB
fibrosis as DDX)
➢ No self or family hx of DM, HTN or Asthma (RF and DDX)
➢ Screened for RVI 6 months back and found to be NR (RF)
➢ No hx of bone pain, herbicide exposure, epistaxis or bleeding from other body
sites (mediastinal lymphoma → DDX)
➢ No hx of drug intake other than those mentioned above (drugs as a cause of cough
e.g. ACE-I like Enalapril, amiodarone, methotrexate, hydralazine)

Finally, she was admitted to our hospital supported physically by his families

Physical examination (pertinent findings)

1. GA
Respiratory distress signs (e.g. use of accessory muscle of Respiration)
“Tripod” position

Picture; “tripod position”; child is sitting up and leaning forward on outstretched


hands, to facilitate the actions of the sternocleidomastoid, scalene, and
intercostal muscles which helps to decrease respiratory distress (RD). This is a
patient with epiglottitis who developed RD, we put here to have Knowhow of tripod position

Picture; Left) ‘’Tripod position’’ in patient with emphysema, Right) Patient with
Chronic bronchitis sitting comfortably. But this is not necessarily the Stereotype
(the opposite form may be seen).

Low BMI, with significant weight loss → Due to inadequate oral intake
Previously the consideration was; Pink puffers (emphysema) tilt forward,
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Chapter 2; Chronic lung disorders and Cor pulmonale

o Nowadays, classifying patients as Pink puffers and blue bloaters


is obsolete, because most patients have features of both chronic
bronchitis and emphysema
2. Vital signs
✓ Febrile → if there is acute respiratory infection
✓ Desaturated patient (decreased O2 saturation)
3. HEENT
✓ Plethora (injected and hyperemic conjunctiva) → 2ry to polycythemia
✓ Anemia features → pale conjunctiva
✓ Central cyanosis
4. LGS

5. RS
✓ Inspection
Use of accessory muscles of respiration → predominantly in
emphysema
Pursing of lips → close lips tightly during expiration (in emphysema)
Reduced tracheal length above the sternal notch
Tracheal tug → trachea descend during inspiration
Subcostal and intercostal retraction
Jugular vein distension during expiration
Barrel shaped chest → AP diameter of chest > lateral diameter due
to hyperinflation → common in emphysema
Central cyanosis → predominantly in chronic bronchitis
Hoover’s sign +ve → paradoxical inward movement of ribcage with
inspiration
✓ Palpation
Decreased chest expansion bilaterally → like restrictive lung disease
Tracheal tug
✓ Percussion
Hyper resonant → common in emphysema
Loss of cardiac and liver dullness → flattening of diaphragm
Poor diaphragmatic excursion → enlarged liver volume
✓ Auscultation
Decreased Air entry bilaterally
Vesicular breath sound with prolonged expiration
Coarse crepitation (crackles) and wheeze at lung bases throughout
the respiratory cycle
Ronchi at expiration

N.B type II respiratory failure features

➢ Central cyanosis
➢ Flapping tremor
➢ Bounding pulse
➢ CHF features (raised JVP, right ventricular heave, loud P2, hepatomegaly,
pedal edema)
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6. CVS
✓ Distended neck vein from RSHF → N.B. Neck vein distension, liver
enlargement and peripheral oedema could be due to cor pulmonale or due
to severe hyperinflation.
✓ Parasternal heave from RV hypertrophy in pulmonary HTN
✓ Split of S2 which suggests corpulmonale
✓ Murmur of TR and PR
✓ Distant heart sound
7. Abdominal examination
✓ Easily palpable liver due to severe hyperinflation or due to congestion from
RSHF.
In the case of RSHF it is tender hepatomegaly. In severe
hyperinflation, liver may palpable due to pushing down effect from
diaphragm but, it doesn’t mean hepatomegaly. SO, Hepatomegaly
is after measuring TVLS.

8 GUS

9 MSS

✓ Peripheral edema from cor pulmonale


✓ Loss of muscle mass and peripheral muscle weakness are consistent with
malnutrition and /or skeletal muscle dysfunction.
10 IS

✓ cyanosis
11 NS

Signs of COPD can be summarized as the follows (Source → Harrison 21st


edition)

➢ In the early stages of COPD, patients usually have an entirely normal physical
examination.
➢ Current smokers may have signs of active smoking, including;
 An odor of smoke or
 Nicotine staining of fingernails.
➢ Expiratory wheezing → In patients with more severe disease
➢ A barrel chest and enlarged lung volumes with poor diaphragmatic excursion
→ signs of hyperinflation
➢ Patients with severe airflow obstruction may also exhibit;
 Use of accessory muscles of respiration
 Sitting in the characteristic “tripod” position → to facilitate the actions of
the sternocleidomastoid, scalene, and intercostal muscles.
➢ Cyanosis, visible in the lips and nail beds.
➢ Cachexia, with significant weight loss, bitemporal wasting, and diffuse loss of
subcutaneous adipose tissue → may happen in Advanced disease
 Associated with both inadequate oral intake and elevated levels of
inflammatory cytokines (TNF-α).
 An independent poor prognostic factor in COPD.
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➢ Hoover’s sign (Paradoxical inward movement of the rib cage with inspiration)
 Seen In advanced disease
 The result of alteration of the vector of diaphragmatic contraction on the
rib cage as a result of chronic hyperinflation.
➢ Signs of overt right heart failure, termed Cor pulmonale, are relatively
infrequent since the advent of supplemental oxygen therapy.
➢ Clubbing of the digits is not a sign of COPD
 Its presence should alert the clinician to initiate an investigation for
causes of clubbing (the development of lung cancer is the most likely
explanation for newly developed clubbing).
➢ Although traditional teaching is that patients with predominant
emphysema, termed “pink puffers,” are thin and noncyanotic at rest
and have prominent use of accessory muscles, and patients with
chronic bronchitis are more likely to be heavy and cyanotic (“blue
bloaters”), current evidence demonstrates that most patients have elements of
both chronic bronchitis and emphysema and that the physical examination does
not reliably differentiate the two entities.

Signs of Cor pulmonale can be summarized as the follows (Source →


Harrison 21st edition)

Physical examination findings of Cor pulmonale include;


➢ Findings of pulmonary hypertension such as
 Accentuated P2 component of S2
 A right-sided S3 or S4, and TR.
➢ Auscultation of the lungs can highlight the underlying parenchymal lung
disorder
➢ In chronic cor pulmonale, the murmur of TR, an S3 gallop and a RV heave
palpable along the left sternal border
➢ The most blatant findings are reflective of high right-sided filling pressures and
hypervolemia such as
 Elevated JVP
 Hepatomegaly
 Pulsatile liver
 Ascites, and especially lower-extremity edema.
➢ Cyanosis is a late finding in cor pulmonale

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Chapter 2; Chronic lung disorders and Cor pulmonale

DDX

Differential diagnosis of COPD


➢ Suggestive Features for differentiation, we put here, tend to be characteristic of
the respective diseases, but do not occur in every case.
 For example, a person who has never smoked may develop COPD
(especially in the developing world, where other risk factors may be more
important than cigarette smoking); asthma may develop in adult and even
elderly patients.

COPD
 Onset in mid-life; onset in early adulthood should prompt suspicion
for alpha-1 antitrypsin deficiency
 Symptoms slowly progressive
 Long smoking history, although can occur in nonsmokers
 Dyspnea during exercise
 Largely irreversible airflow limitation
Asthma
 Severe and severe persistent form of asthma are DDX for COPD
 It may be one of the variants of COPD
 seasonal and there may be triggering agents
 Symptoms vary from day to day, more at night/early morning
 wheezing is predominant
 Onset early in life (common in childhood, peak at 3 years)
 Allergy, rhinitis, and/or eczema also present
 +ve Family history of asthma
 Largely reversible airflow limitation
Bronchiectasis
 Cough and large volume of mucopurulent, tenacious, position dependent,
sputum last for months to years
 There may be hemoptysis
 Commonly associated with recurrent or persistent bacterial infection
 Coarse crackles on auscultation, clubbing of digits
 Chest radiograph/HRCT shows bronchial dilation, bronchial wall thickening
 ‘’Trump truck sign’’ and ‘’signet ring sign’’ in high resolution CT (HRCT)
→ continuous non-tapering airway with bronchial dilatation and bronchial
wall thickening
▪ N.B HRCT is gold standard Ix for bronchiectasis
 Obstructive spirometry finding
 Bronchiectasis is 2ry to
▪ Acquired → TB (Post TB fibrosis is the commonest cause in our
setup), pneumonia, obstruction of the bronchial tree
▪ Congenital → Cystic Fibrosis (common in westerns)
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Tuberculosis
 Typical features of TB (Cough more than 2 weeks associated with Fever
weight loss, night seat)
 Maye have contact history
 Onset all ages
 Chest radiograph shows upper lung zone scarring and/or calcified
granulomata
 High local prevalence of tuberculosis especially in developing countries
Heart failure
 Fine basilar crackles on auscultation
 Dyspnea associated with Orthopnea, PND and Signs of Congestion if
there is CHF
 Chest radiograph shows dilated heart, pulmonary edema
Lung ca
 Primary lung ca or metastasis from breast, bowel, bladder, brain….
 Present with bloody sputum and chronic cough
 Patients have family hx of lung ca and cmn in smokers
 N.B. the pneumonic ‘’S’’ with smoking in lung ca
Smoking and central Non-smokers and peripheral
❖ SCC ❖ Adenocarcinoma
❖ Small cell carcinoma ❖ Large cell carcinoma
❖ SOB and cough are ❖ Hemoptysis and chest pain
common presentation are common presentations

Central airway obstruction (e.g. Bronchogenic or metastatic cancer,


lymphadenopathy, Mediastinal mass, scarring from endotracheal tube)
 Monophonic wheeze or stridor
 Chest radiograph often normal
 Airway narrowing on three-dimensional reconstruction of HRCT scan
 Variable inspiratory or fixed slowing on flow volume loop
 May end up with superior vanacava sxx
N.B 4T’s of mediastinal mass

 Terrible lymphoma (NHL is cmn)


 Thyroid mass (retrosternal extension of thyroid mass)
 Teratoma
 Thymoma
Drugs
E.g. amiodarone, methotrexate, hydralazine, ACE-I…
Result in pulmonary fibrosis
Smx resolve if the drug is discontinued
End up with irreversible sxx, if there is chronic exposure
Porto systemic schistosomiasis
OSA (Obstructive sleep apnea)/ untreated/
Snoring at night, daytime somnolence
Common in obese and DM pt’s
Obliterative bronchiolitis
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 Rare
 Onset in younger age, nonsmokers
 May have history of rheumatoid arthritis or fume exposure
 HRCT on expiration shows hypodense areas, mosaic pattern
Diffuse pan bronchiolitis
 Extremely rare to consider in our setup, Highest prevalence in East Asia
 Most patients are male and nonsmokers
 Almost all have chronic sinusitis
 Chest radiograph and HRCT show diffuse small centrilobular nodular
opacities and hyperinflation

DDX for COPD exacerbations


➢ Pneumonia
➢ Pneumothorax
➢ Pulmonary embolus (PE) → should also be considered, as the incidence of PE
is increased in COPD exacerbations.
➢ Pulmonary edema (Cardiogenic)
➢ Pleural effusion
➢ Cardiac Arrythmias (Atrial fibrillation/flutter)

DDX for Cor pulmonale

➢ CHF
➢ Constrictive pericarditis
➢ RCMP (Restrictive cardiomyopathy)
➢ Right ventricular infarction
➢ Atrial myxoma
➢ VSD (Ventricular septal defect)

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Chapter 2; Chronic lung disorders and Cor pulmonale

Table; Aetiology of Chronic Cor Pulmonale (i.e Cor pulmonale 2ry to;)

1. Diseases of the Lung Parenchyma


COPD
 Although COPD is responsible for ~50% of the cases of Cor pulmonale (western data), any
disease that affects the pulmonary vasculature or parenchyma can lead to Cor pulmonale.
 Common Variants of COPD include
☛ Chronic bronchitis
☛ Emphysema
Bronchiectasis
Post TB fibrosis
 Common in developing countries (common cause of Cor pulmonale in our setup. No specific
data in Ethiopia to compare with COPD, but it is known that, Post TB fibrosis is the
commonest cause of Bronchiectasis in Ethiopia)
 Most patients have hx of TB treatment with cure and relapse multiple times
ILD
 Pt’s present with prolonged unexplained SOB, dry cough
 Classified as
▪ Known/idiopathic
▪ Acute/subacute/chronic
▪ Granulomatous/inflammatory
 There are so many disorders (>200) which classified under ILD because they have similar
C/F, radiologic feature and mgt. such as;
▪ Idiopathic interstitial pneumonias (idiopathic pulmonary fibrosis/IPF/)
o IPF is the commonest form of ILD
▪ Secondary interstitial diseases
▪ Sarcoidosis
Combined pulmonary fibrosis and emphysema
Others including Developmental lung disorders (e.g. Bronchopulmonary dysplasia in infants)
2. Disorders of Chronic (Alveolar) Hypoxia
Chest wall disorders
 Kyphoscoliosis
Chronic exposure to high altitude
Neuromuscular respiratory failure
Alveolar hypoventilation syndromes
Central hypoventilation syndrome
3. Diseases of the Pulmonary Vasculature
Pulmonary arterial hypertension (PAH)
Chronic thromboembolic pulmonary hypertension (e.g. Massive PTE in acute cases or Chronic
PTE)
Mediastinal disorders affecting central pulmonary vasculature
Pulmonary tumour thrombotic microangiopathy

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IX

Baseline IX
❖ CXR

Radiographic features suggestive of COPD (usually seen in advanced disease)


include:

✓ Signs of hyper inflation

A flat diaphragmatic contour and an increased retrosternal


airspace on a lateral radiograph i.e. Increased A-P Diameter
(increased lung volume) which is evidenced by more horizontal
alignment of ribs (image 2).
Tear drop appearance of heart (narrow vertical heart)
Loss of peripheral vascular marking

✓ Rapidly tapering vascular shadows, increased radiolucency of the lung, a


flat diaphragm, and a long, narrow heart shadow on a frontal radiograph
(image 1).
✓ Bullae, defined as radiolucent areas > 1cm in diameter and surrounded
by arcuate hairline shadows.
o They are due to locally severe disease, and may or may not be
accompanied by widespread emphysema (image 3).
✓ When advanced COPD leads to pulmonary hypertension and Cor
pulmonale;
o Prominent hilar vascular shadows and encroachment of the heart
shadow on the retrosternal space may be seen.
o The cardiac enlargement may become evident only by comparison
with previous chest radiographs
o RV hypertrophy, right atrial dilatation, prominent pulmonary artery
✓ CXR also done to r/o pneumonia, lung ca, CHF, pleural effusion from
RSHF, and pneumothorax

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Chapter 2; Chronic lung disorders and Cor pulmonale

image 1 image 2

image 3 image 4

CXR features of Pulmonary hypertension include;


 Enlargement of the central pulmonary arteries, “vascular pruning,” and
cardiomegaly
▪ The term “vascular pruning,” is used to indicate attenuated
peripheral pulmonary arteries that looks like a ‘’pruned tree’’

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❖ ECG → in Cor pulmonale and Pulmonary hypertension; can show as


In severe pulmonary hypertension shows
o P pulmonale (characteristic peaked P wave)
o Right axis deviation, and
o RV hypertrophy (R/S ratio > 1)
Supraventricular hypertrophy
Dysrhythmia such as Atrial flutter
❖ Echo
 Used for the diagnosis of isolated RSHF (Cor pulmonale), Pulmonary HTN
and helps to r/o LSHF
 In Cor pulmonale
▪ Echo Used to measure RV wall thickness and chamber dimensions
▪ The interventricular septum may move paradoxically during systole
in the presence of RV pressure overload, highlighting a deleterious
interaction between the RV and the LV.

▪ N.B. MRI is also useful for assessing RV structure and function,


particularly in patients who are difficult to image with 2-D
echocardiography because of severe lung disease

 Pulmonary hypertension (PH)


▪ All forms of PH may demonstrate a hypertrophied and dilated right
ventricle with elevated estimated pulmonary artery systolic pressure
▪ Doppler echocardiography can be used to assess pulmonary artery
pressures
o PH can be diagnosed when Pulmonary artery pressure greater
than 25mmhg (after Right heart catheterization)
o Cardiac catheterization (in western setups, not applicable in
our setup) → confirms the diagnosis of pulmonary
hypertension and can exclude elevated left-sided pressures as
a cause for right-sided HF
▪ Echo is also important to identify etiologies of PH, such as;
o Valvular disease
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o Left ventricular systolic and diastolic dysfunction


o Intracardiac shunts, and other cardiac diseases.
▪ TR (functional murmur) can be detected either by physical
examination or Echo
❖ CBC → what do you expect from CBC
✓ Polycythemia commonly
✓ Anemia
✓ Leukocytosis as evidence of infection
✓ 2ry erythrocytosis
❖ Sputum examination (BAL)→ In acute exacerbation it reveals TB,
pneumonia
❖ PICT, RBS, LFT and RFT (OFT is based on indication) → to asses
comorbidity

Other Ix to be done if available


❖ Diagnostic investigations for COPD
PFT /Pulmonary function test/(Spirometry)
✓ Spirometry is “the gold standard”, most reproducible, standardized,
objective way of measuring airflow limitation
✓ Expiratory airflow limitation is the hallmark physiologic change of
COPD → FEV1, FVC, FEV1/FVC all decreased
✓ A postbronchodilator FEV1/FVC ratio < 70% i.e. < 0.7, in
combination with an FEV1 < 80% predicted (obstructive pattern)
✓ In an individual with cough, sputum production or dyspnea
and exposure to risk factors confirms the diagnosis
✓ Bronchodilator reversibility should be performed at least once to
exclude asthma and to establish the best lung function for the
individual patient, and, to a lesser degree, to estimate the prognosis.
✓ N.B. in COPD, obstruction not improved with short acting
bronchodilator administration but in bronchial asthma there will
be > 12 % improvement of FEV1 after 15 min administration
of short acting bronchodilator (like salbutamol)
✓ Other diagnostic tests
✓ Sample of sputum
✓ Chest X-ray
✓ High resolution CT (HRCT)
✓ Arterial blood gases
✓ Pulse Oximeter → it is part of physical examination but very
necessary for diagnosis
✓ Look at GOLD staging of COPD based on Spirometry and clinical
parameters under discussion part of COPD below

How can we differentiate obstructive lung disease (e.g. COPD, Asthma) from
Restrictive lung disease (e.g. ILD) based on spirometry?
✓ In obstructive lung disease, FEV1 decreased but FVC is normal so
FEV1/FVC ratio decreased. In restrictive lung disease, FEV1 and
FVC decreased simultaneously so the FEV1/FVC ratio is normal.

❖ HRCT (High resolution CT)


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CT scanning is not needed for the routine diagnosis of COPD.


Usually, it is performed when;
o A change in symptoms suggests a complication of COPD (eg,
pneumonia, pneumothorax, giant bullae)
o An alternate diagnosis (eg, thromboembolic disease), or
o A patient is being considered for lung volume reduction
surgery or lung transplantation
CT Assist in classification of COPD. It has high sensitivity and
specificity than CXR for emphysema
o Certain CT scan features can determine whether the
emphysema is centriacinar (centrilobular), panacinar, or
paraseptal, although this is usually not necessary for clinical
management
Classic findings of Pulmonary Hypertension on CT include;
o Those found on chest radiograph
o Enlarged pulmonary arteries, peripheral pruning of the small
vessels, and enlarged right ventricle and atrium.
o However, high-resolution CT may also reveal signs of venous
congestion, including centrilobular ground glass infiltrate and
thickened septal lines.
o In the absence of left heart disease, these findings suggest
pulmonary venous disease, a rare cause of PAH that can be
quite challenging to diagnose.
o CT is also critical for distinguishing co-morbid interstitial lung
disease or emphysema.

N.B. HRCT is important Ix modality for bronchiectasis, ILD, lung ca,


massive PTE, lung abscess

❖ ABG/Arterial blood gas/ analysis in Cor pulmonale 2ry to chronic lung


disorders, typically reveal hypoxemia with or without hypercapnia (decreased
PaO2 and increased PaCO2).
❖ Serum AAT level → normal range is 100 - 200 mg/dL, low or deficient in
emphysema.
❖ Thrombophilia screen → to detect chronic venous thromboembolism
(proteins C and S, ant thrombin III, homocysteine levels)
❖ ANA → SLE Blood culture → for severe pneumonia in RVI pt, has 10 %
sensitivity
❖ ADF → Pleural marker
❖ BNP → Elevated in patients with Cor pulmonale secondary to RV
myocardial stretch
❖ Lung Biopsy
✓ Last option
✓ Biopsy shows emphysema subtypes (centri-acinar, pan-acinar, para-
septal, irregular)

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Discussion

2.1 Obstructive Lung diseases

2.1.1 COPD (Chronic obstructive pulmonary disease)


COPD is defined as a disease state characterized by persistent respiratory
symptoms and airflow limitation that is not fully reversible.
The classic definition of COPD requires the presence of chronic airflow
obstruction, determined by spirometry, that usually occurs in the setting of
noxious environmental exposures—most commonly cigarette smoking. (indoor air
pollution in our setup)

➢ GOLD13 (Global Initiative for Chronic Obstructive Lung Disease), defines COPD
as:
"COPD is a common, preventable, and treatable disease that is characterized
by persistent respiratory symptoms and airflow limitation that is due to
airway and/or alveolar abnormalities usually caused by significant exposure to
noxious particles or gases.’’

COPD includes;
 Emphysema → an anatomically defined condition characterized by
destruction of the lung alveoli with air space enlargement
 Chronic bronchitis → a clinically defined condition with chronic cough and
phlegm; and
 Small airway disease → a condition in which small bronchioles are
narrowed and reduced in number.
Emphysema, chronic bronchitis, and small airway disease are present in
varying degrees in different COPD patients.
Patients with a history of cigarette smoking without chronic airflow obstruction
may have chronic bronchitis, emphysema, and dyspnea. Although these
patients are not included within the classic definition of COPD, they may have
similar disease processes.
The chronic airflow limitation that characterizes COPD is caused by a mixture
of small airways disease (e.g. obstructive bronchiolitis) and parenchymal
destruction (emphysema), the relative contributions of which vary from person
to person.
It is a chronic disease that is showing progressive upward trend in both
mortality and morbidity

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COPD is the 3rd leading cause of death in the United States. And also,
almost 90% of COPD deaths occur in low- and middle-income countries, where
effective strategies for prevention and control are not always implemented or
accessible.
Different guidelines use other forms of terminology for COPD (chronic
obstructive pulmonary disease). All of them are the same entities, these are;
 COLD (chronic obstructive lung disease)
 COAD (chronic obstructive airway disease)
 CORD (chronic obstructive Respiratory disease)
Although COPD affects the lungs, it also produces significant systemic
consequences.
Some patients can have manifestations of both COPD and asthma and, hence,
told to have Asthma COPD overlap syndrome (ACOS).

Asthma-COPD overlap syndrome (ACOS)


➢ Although asthma and COPD are distinct syndromes with different
clinical presentations and underlying inflammatory mechanisms, some
patients with asthma have features of COPD (for example, asthmatics
who smoke and severe asthmatics with irreversible airflow limitation)
and some patients with COPD have features of asthma with more
reversibility and increased airway and blood eosinophils.
➢ This may represent the coincidence of two common diseases, or these may be
distinct phenotypes.
➢ ACOS patients tend to have more symptoms and exacerbations. They may
benefit from triple therapy with ICS (Inhalational corticosteroids), LABA (long
acting 𝛽2 agonists), and LAMA (long acting muscarinic antagonists e.g.
theophylline)

Difference between Obstructive lung disease (e.g. COPD, Asthma) from


Restrictive lung disease (e.g. ILD)
Obstructive lung disease (e.g. COPD, Asthma) Restrictive lung disease (e.g. ILD)

✓ Spirometry reveals Obstructive pattern ✓ Spirometry reveals a restrictive pattern


 FEV1 decreased but FVC is normal  FEV1 and FVC decreased simultaneously
so FEV1/FVC* ratio decreased so the FEV1/FVC ratio is normal.

𝑭𝑬𝑽𝟏 𝒅𝒆𝒄𝒓𝒆𝒂𝒔𝒆𝒅 𝑭𝑬𝑽𝟏 𝒅𝒆𝒄𝒓𝒆𝒂𝒔𝒆𝒅


𝒊. 𝒆. 𝑭𝑽𝑪 𝒏𝒐𝒓𝒎𝒂𝒍
= decreased ratio 𝒊. 𝒆. 𝑭𝑽𝑪 𝒅𝒆𝒄𝒓𝒆𝒂𝒔𝒆𝒅
= Normal ratio

 Lung volume measurements reveal a  Lung volume measurements reveal a


normal to increased value of both RV normal to decreased TLC, and an
and TLC, so there is an increase in increase in RV/TLC. This increased
RV/TLC# ratio. RV/TLC ratio may reflect the relative
✓ As the name implies there is airway decrease in TLC or a real increase in RV
obstruction and patients present with SOB, (true hyperinflation)
Chronic productive cough (in asthma ✓ Patients usually present with prolonged
patients, even though there is obstruction,
there may not have cough at all)
unexplained SOB, dry cough
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* FEV1 = Forced expiratory volume in 1 sec, FVC = Forced vital capacity


#
TLC = total lung capacity, RV = residual volume

Difference between COPD and Asthma

COPD ACOS Asthma*


❖ Obstruction not improved with ❖ There will be > 12 % improvement (a
short acting bronchodilator ➔ Some patients >12% and 200-mL increase in FEV1),
administration (it may be with asthma 15 min after administration of short
partially reversible) cannot be acting bronchodilator (like salbutamol),
❖ symptoms show less distinguished from or in some patients by a 2-4 week
variability, never completely COPD with the trial of oral corticosteroids (OCS) like
remit, and show much less current diagnostic prednisone or prednisolone 30 - 40
(or no) reversibility to tests. The mg daily (may be fully reversible)
bronchodilators management of ❖ symptoms show variability, seasonal
❖ COPD is more likely in this patients and depends on triggering factors
elderly patients and may should be similar ❖ Occur at any age. Especially common
coexist with asthma. And to that of asthma in children, peak at 3 years, 50%
usually have hx of smoking, ➔ Look at the develop before the age of 10 and
in our set up indoor smoking above notes another 35% before 40
(i.e. indoor air pollution from ❖ Episodic course
biomass fuel) ❖ Airway remodelling but no lung
❖ Slowly progressive obstruction
❖ Airway remodeling and lung  If there is obstruction, the so
obstruction called Chronic obstructive asthma
❖ Inflammatory cells is subset of COPD
 Neutrophilic bronchitis ❖ Inflammatory cells
 Eosinophilic during  Eosinophilic bronchitis
exacerbations  Neutrophils in severe disease

* For details of asthma, refer respiratory section from short case on Nitsbin (click here → 8.3. Asthma
(አስም) )

Spectrum of Disease in COPD

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COPD Phenotypes include;

Chronic bronchitis
Emphysema:
Chronic obstructive asthma (Chronic asthma with airway remodeling and fixed
obstruction).

Table; difference between Chronic bronchitis and emphysema*


Chronic bronchitis# Emphysema
☛ Chronic bronchitis is defined as a chronic ☛ An abnormal permanent enlargement of the
productive cough for 3 months in each of 2 distal air spaces, distal to the terminal
successive years in a patient in whom other bronchioles, accompanied by destruction of their
causes of chronic cough (eg, bronchiectasis) walls and without obvious (macroscopic)
have been excluded. fibrosis.
➢ Clinical definition and Dx of exclusion ➢ Pathologic definition
☛ Predominant productive cough ☛ Predominant SOB with little/no cough or
➢ Expectoration is due to goblet cell hyperplasia expectoration
and inflammation ➢ SOB is due to destruction of gas exchange air
☛ Rhonchi, wheeze and coarse crackles may be spaces which intern forms non-functioning wide
heard Air sac
☛ It may precede or follow development of airflow ➢ Production of protease from smoking leads to
limitation. destruction of basement membrane and
☛ Symptoms of chronic bronchitis may develop in connective tissue which will cause emphysema
cigarette smokers as early as 36 years of age ☛ Use of accessory muscles of respiration and
and have been associated with a higher Pursing of lips are predominant in emphysema
frequency of exacerbation events, even in the ☛ Barrel shaped chest with hyperinflated lung that
absence of airflow obstruction. push the diaphragm down (flattening of
diaphragm) is common in emphysema
* The old classification of Chronic bronchitis as ‘’blue bloaters’’ and emphysema as ‘’pink puffers’’ is
obsolete nowadays.
#
Acute bronchitis patients present with sore throat, fatigue, fever, runny nose, vomiting and diarrhoea,
cough, SOB. While, Chronic bronchitis patients present with cough, sputum, cyanosis, hypercapnia,
pulmonary hypertension, Right ventricular failure, peripheral edema

Emphysema classification
Emphysema is classified into distinct pathologic types (Figure below), which
include;
 Centrilobular emphysema
 Pan lobular emphysema and
 Para septal emphysema.
Centrilobular emphysema
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 The type which is most frequently associated with cigarette smoking,


and characterized by enlarged air spaces found (initially) in association
with respiratory bronchioles.
 It is usually most prominent in the upper lobes and superior segments of
lower lobes and is often quite focal.
Pan lobular emphysema
 refers to abnormally large air spaces evenly distributed within and across
acinar units.
 It is commonly observed in patients with α1AT deficiency, which has a
predilection for the lower lobes.
Para septal emphysema
 occurs in 10 -15% of cases and is distributed along the pleural margins
with relative sparing of the lung core or central regions.
 It is commonly associated with significant airway inflammation and with
centrilobular emphysema.

FIGURE; CT patterns of emphysema.

A. Centrilobular emphysema with severe upper lobe involvement in a


68-year-old man with a 70 pack-year smoking history but forced expiratory volume
(FEV1) 81% predicted (GOLD spirometry grade 1)
B. Pan lobular emphysema with diffuse loss of lung parenchymal detail predominantly in
the lower lobes in a 64-year-old man with severe α1AT deficiency; and
C. Para septal emphysema with marked airway inflammation in a 52-year-old woman with
a 37 pack-year smoking history and FEV1 40% predicted

Pathophysiology

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Causes of Airflow Limitation

Irreversible
➢ Fibrosis and narrowing of the airways
➢ Loss of elastic recoil due to alveolar destruction
➢ Destruction of alveolar support that maintains patency of small airways

Reversible
➢ Accumulation of inflammatory cells, mucus, and plasma exudate in bronchi
➢ Smooth muscle contraction in peripheral and central airways
➢ Dynamic hyperinflation during exercise

Natural history

An accelerated decline in lung function is the single most important feature of


COPD.
COPD is generally a progressive disease, especially if the patient’s exposure to
noxious substances, most often tobacco smoking, continues.
If exposure is stopped, the disease may still progress, mainly due to the
decline in lung function that normally occurs with ageing.
Nevertheless, stopping exposure to noxious agents, even after significant
airflow limitation is present, can result in some improvement in function and will
slow or even hold the progression of the disease.

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Diagnosis of COPD

Presumptive Diagnosis

COPD should be considered in any patient who has:


 A smoking history of at least 10-20 pack/yrs and/or a history of exposure
to other risk factors
 Chronic cough with or without sputum production
 Dyspnea
 Onset of respiratory symptoms in 40s
 Respiratory infection that persists or recurs

For details of Clinical features and Investigation → look at the approach part
above

Classification of Severity of Airflow Limitation in COPD


Table; GOLD* Criteria for Severity of Airflow Obstruction in COPD
GOLD stage Severity FEV1 (In patients with FEV1/FVC ratio < 0.7)
I Mild ≥ 80% predicted
II Moderate FEV1 ≥50% but <80% predicted [50 - 80%)
III Severe FEV1 ≥30% but <50% predicted [30 - 50%)
IV Very severe FEV1 < 30% predicted
* GOLD stands for Global Initiative for chronic obstructive lung disease; GOLD
guidelines (http://www.goldcopd.org ). This table taken from Harrison 21st
edition
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How can we asses symptom severity of GOLD classification?

Symptom severity is assessed using the CAT score or mMRC grade (CAT =
COPD Assessment Tool, mMRC = Modified Medical Research Council)
Lung function, in addition to the number of exacerbations and hospitalizations
for exacerbations in the previous 12 months, can be used to predict future
risk.
 A history of 0 or 1 exacerbation in the past 12 months and GOLD I or II
spirometry level suggests a low future risk of exacerbations
 ≥ 2 exacerbations or a hospitalized exacerbation or GOLD III or IV
spirometry level suggest a high future risk.
These components are combined into four groups as shown the table:

Table; GOLD: COPD severity assessment


Annual frequency of COPD Respiratory symptoms (based on the mMRC* or CAT#
exacerbations/hospitalizations scales)
mMRC grade 0 to 1; CAT mMRC grade ≥2; CAT
score <10 sore ≥10
(less symptoms) (High symptoms)
0 or 1 exacerbations per year Group A Group B
without hospitalization (low risk)
≥2 exacerbations per year or Group C Group D
≥1 hospitalization (high risk)

*mMRC: modified Medical Research Council dyspnea scale → Provides a single number for
degree of breathlessness:

0 → Only with strenuous activity


1 → Hurrying on level ground or walking up a slight hill
2 → Walk slower than peers or stop walking at their own pace
3 → Walking about 100 yards or after a few minutes on level ground
4 → Too breathless to leave the house or when dressing

CAT: COPD Assessment Test → http://www.catestonline.org , http://www.goldcopd.org


#

➢ An 8-item COPD health status measure with Likert scale responses for questions about
cough, phlegm, chest tightness, dyspnea on one flight of stairs, limitation in home
activities, confidence in leaving the home, sleep and energy.
➢ Range of total score is 0 - 40.

Management of stable COPD

The two main goals of therapy are;


✓ To provide symptomatic relief → reduce respiratory symptoms,
improve exercise tolerance, improve health status and
✓ To reduce future risk → prevent disease progression, prevent and
treat exacerbations, and reduce mortality.
The overall approach to managing stable COPD should be characterized by a
stepwise increase in the treatment, depending on the severity of the disease.
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Management principles of COPD include;


 Assessing and monitoring of the disease
 Avoidance of modifiable risk factors and vaccinations
 Oxygen therapy
 Pulmonary rehabilitation.
 Pharmacologic therapies
 Identify and treat complications
▪ Cor pulmonale and RSHF mgt
▪ Polycythemia mgt (e.g. phlebotomy)
 Surgical management for selected patients
▪ Lung Volume Reduction Surgery
▪ Lung Transplantation

A. Assessing and monitoring of the disease

Factors Determining Severity of Chronic COPD


 Severity of symptoms
 Severity of airflow limitation
 Frequency and severity of exacerbations
 Presence of complications of COPD, respiratory insufficiency or
Comorbidity
 General health status
 Number of medications needed to manage the disease.

B. Avoidance of modifiable risk factors and vaccinations

Smoking cessation is the single most effective - and cost effective -


intervention to reduce the risk of developing COPD and stop its progression.
 Brief tobacco dependence treatment (e.g. nicotine replacement) &
counseling are effective.
Reduction of indoor air pollution through introduction of non-smoking cooking
devices or alternative fuels should be encouraged.
Vaccination
 Influenza vaccination reduces serious illness and death. All Patients with
COPD should receive the influenza vaccine annually.
 Pneumococcal vaccination (PCV13 and PPSV23): recommended for all
patients ≥65. The PPSV23 is also recommended in younger patients with
significant comorbidity including chronic lung or heart diseases.

C. Oxygen therapy:

All patients with desaturation should be put on intranasal O2 during hospital


stay.
In our setup, most patients need home O2 (so, discharge with O2, if they can
afford, communicate and link to oxygen supply companies)
Long-term oxygen therapy (LTOT) i.e. long-term administration of oxygen
≥15hrs/day, to patients with severe resting hypoxemia in COPD, increases
survival and improves the quality of life.
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➢ Indications for continuous long-term oxygen therapy (LTOT) for patients with
COPD → i.e. indication for home oxygen
 Saturation of oxygen (SaO2) ≤ 88 % or PaO2 ≤ 55 mmHg (7.32 kPa)
confirmed twice over 3 weeks period
 In the presence of Cor pulmonale; one of the following
▪ SaO2 ≤ 89 % or PaO2 ≤ 59 mmHg (7.85 kPa)
▪ Evidence of pulmonary hypertension (ECG evidence of P pulmonale)
▪ Polycythemia (Hematocrit > 55 %) or
▪ Clinical evidence of right heart failure (peripheral edema suggesting
CHF)
 Specific situations
▪ SaO2 ≥ 90 % or PaO2 ≥60 mmHg (7.98 kPa) with lung disease and
other clinical needs such as sleep apnea with nocturnal desaturation
not corrected by CPAP.
▪ If the patient meets criteria at rest, O2 should also be prescribed
during sleep and exercise, and appropriately titrated.
▪ If the patient is normoxemic at rest but desaturates during exercise
(PaO2 ≤55 mmHg [7.32 kPa]), O2 is generally prescribed for use
during exercise. For patients who desaturate (PaO2 ≤55 mmHg [7.32
kPa]) during sleep, further evaluation with polysomnography may be
indicated to assess for sleep-disordered breathing.

N.B.
The Only three interventions have been demonstrated to improve survival of
patients with COPD are;
☛ Smoking cessation
☛ Oxygen therapy in chronically hypoxemic patients, and
☛ Lung volume reduction surgery (LVRS) in selected patients with
emphysema.
Oxygen is a drug that should be given with correct dosing and based on
indication
 Order example; ‘’ Put on 2L/min of INO2 OR put on Intranasal oxygen at
a rate of 2 L/minute''

Relation between oxygen flow rate and the fraction of inspired oxygen(FiO2)

100%
90%
90% 86%
82%
78%
80% 74%
70%
70% 64% 66%
60%
60% 56%
52%
48%
50% 44%
40%
40% 36%
32%
28%
30% 24%
20%
10%
0%
1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18
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Chart; Relation between oxygen flow rate in L/min (X-axis) and the fraction of
inspired oxygen (FiO2)/y-axis/. Each additional L/min in oxygen flow increases the
FiO2 by about 4 % (i.e. 24%, 28%, 32%... the difference in between is 4%). For
example, if you put the patient in 2L/min, S/he will get 28% additional oxygen
from the baseline SaO2(On the other way, if the initial SaO2 is 62 %, in order to
make 90%, this patient will require additional 28 % oxygen which is 2L/min). If ≥
10L/min is required, use face mask instead of Intra nasal cannula.

D. Pulmonary rehabilitation:

➢ Exercise should be encouraged at all stages and patients reassured that


breathlessness, while distressing, is not dangerous.
➢ Physical training, disease education and nutritional counseling reduce
symptoms, improve health status and enhance confidence.

E. Pharmacologic therapies;

These are used to reduced symptoms, reduce the frequency and severity of
exacerbations, and improve exercise tolerance and health status.
But, none of the existing medications for COPD has been shown to modify the
long-term decline in lung function that is the hallmark of this disease.
Therefore, pharmacotherapy for COPD is used to decrease symptoms and/or
complications.
Pharmacologic therapy options for COPD include;
 Bronchodilators
 Steroids (ICS or OCS)
 Combined ICS and bronchodilators
 Antibiotics

A. Bronchodilators → central to the symptomatic management of COPD. They


are given on an as-needed basis or on a regular basis to prevent or reduce
symptoms. Bronchodilators include;
 beta2 /𝛽2/ agonists
▪ 𝛽2 agonists classified as
o Short acting 𝛽2 agonists (SABA) → e.g. Salbutamol
o Long acting 𝛽2 agonists (LABA) → e.g. Salmeterol, Formoterol
▪ The effect of SABAs usually wears off in 4 - 6 hours whereas
those LABAs have duration of action up to 12 hours.
▪ SABA like Salbutamol may be used for patients with mild disease
but LABA like Salmeterol and Formoterol inhalers are usually more
appropriate for those with moderate to severe disease.
▪ Regular and as needed SABAs or SAMAs improves symptoms and
FEV1.
▪ SABAs can also be used as needed (in between doses of LABAs).
 Antimuscarinic (Anticholinergic) drugs:
▪ Short Acting Muscarinic Antagonist (SAMA) like Ipratropium
▪ Long Acting Muscarinic Antagonist (LAMA) like Tiotropium
▪ Ipratropium has a duration of action that is between 6 - 8 hours
whereas Tiotropium lasts for up to 24 hours.
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▪ LAMAs generally improve symptoms and health status, and reduce


exacerbations and related hospitalizations.
 Oral bronchodilator therapy:
▪ Methylxanthines (e.g. Theophylline/theophedrine 120/11mg tablets)
may be contemplated in patients who cannot use inhaled devices
efficiently.

B. Steroids (ICS or OCS)


 Inhaled glucocorticosteroids (ICS) → e.g. Beclomethasone, Fluticasone
 Oral corticosteroids (OCS) → e.g. prednisolone 5mg tabs
▪ Useful during exacerbations but maintenance therapy contributes to
osteoporosis and impaired skeletal muscle function, and should be
avoided.
▪ Oral glucocorticoid trials assist in the diagnosis of asthma but do
not predict response to inhaled glucocorticoids in COPD.

C. Combined ICS and bronchodilators → The FDC of an ICS and a LABA (e.g.
fluticasone with salmeterol, budesonide with formoterol)
 Because there is no loose preparation of LABAs in the market, we
generally tend to use combination of LABA/ICS.
 This combination improves lung function, reduces the frequency and
severity of exacerbations and improves quality of life especially in patients
with moderate to very severe COPD and exacerbations. These
advantages may be accompanied by an increased risk of pneumonia,
particularly in the elderly.
 Use this combination especially when there is;
▪ History of hospitalization for exacerbation
▪ ≥ 2 exacerbations per year
▪ Blood eosinophils >300/µl or
▪ History of (concomitant) asthma.
D. Antibiotics
 There are strong data implicating bacterial infection as a precipitant of a
substantial portion of exacerbations.
 Azithromycin, chosen for both its anti-inflammatory and antimicrobial
properties
▪ Azithromycin, 250mg, po daily or 500mg, 3x per week for
prevention of exacerbations of COPD
▪ Duration of prophylaxis in clinical studies was 01 year.

Step-up Therapy based on GOLD staging

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Inhaled medication therapy based on grouping patients by severity of symptoms


and risk of exacerbations.

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FIGURE 292-6 (Harrison 21st edition); Medication therapy for stable COPD.
Initial pharmacological therapy (Panel A) is based on both COPD exacerbations and respiratory symptoms
(assessed through the modified Medical Research Council (mMRC) dyspnea questionnaire or the COPD
Assessment Test (CAT)). Follow-up pharmacological therapy (Panel B) is based on response to treatment
initiation and reassessment of symptoms and exacerbations. Global Strategy for the Diagnosis, Management and
Prevention of COPD, Global Initiative for Chronic Obstructive Lung Disease (GOLD), 2021.
*For Panel B: consider if eos ≥300 or eos ≥100 AND ≥2 moderate exacerbations/1 hospitalization.
**Consider de-escalation of ICS or switch if pneumonia, inappropriate original indication or lack of response to
ICS. CATTM, COPD Assessment TestTM; Eos, blood eosinophil count in cells per microliter; FEV1, forced
expiratory volume in 1 second; ICS, inhaled corticosteroid; LABA, longacting beta agonist; LAMA, long-acting
muscarinic antagonist; mMRC, modified Medical Research Council dyspnea questionnaire. (Reproduced with
permission from the Global Strategy for Diagnosis, Management and Prevention of COPD 2021, ©.) 236
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Surgical management for carefully selected patients

➢ Lung Volume Reduction Surgery (LVRS) For patients with emphysema


 Surgery, to remove the most emphysematous portions of lung, improves
exercise, lung function, and survival.
 Patients with upper lobe-predominant emphysema and a low post-
rehabilitation exercise capacity are most likely to benefit from LVRS
 Patients with an FEV1 <20% of predicted and diffusely distributed
emphysema on CT scan have increased mortality after the procedure, and
thus are not candidates for LVRS.

➢ Lung Transplantation
 COPD is currently the second leading indication for lung transplantation.
 Candidates for lung transplantation should have;
▪ Very severe airflow limitation
▪ Severe disability despite maximal medical therapy, and
▪ Be free of significant comorbid conditions such as liver, renal, or
cardiac disease.

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2.1.1.1 Exacerbations of COPD


Exacerbations are a prominent feature of the natural history of COPD.
Exacerbations are episodic acute worsening of respiratory symptoms, including
increased dyspnea, cough, wheezing, and/ or change in the amount and
character of sputum.
They may or may not be accompanied by other signs of illness, including
fever, myalgias, and sore throat.
The strongest single predictor of exacerbations is a history of a previous
exacerbation.
The frequency of exacerbations increases as airflow obstruction worsens;
patients with severe (FEV1 <50% predicted) or very severe airflow obstruction
(FEV1 <30% predicted) on average have 1 - 3 episodes per year.
However, some individuals with very severe airflow obstruction do not have
frequent exacerbations.
Other factors, such as an elevated ratio of the diameter of the pulmonary
artery to aorta on chest CT, and gastroesophageal reflux, are also associated
with increased risk of COPD exacerbations.

Precipitating Causes

➢ A variety of stimuli may result in the final common pathway of airway


inflammation and increased respiratory symptoms that are characteristic of
COPD exacerbations.
➢ Infection of tracheobronchial tree and air pollution are most common causes of
COPD exacerbation
 Bacterial infection/superinfection is involved in >50% of exacerbations.
 Viral respiratory infections are present in approximately 1/3rd of COPD
exacerbations.
➢ No specific precipitant can be identified, In a significant minority of instances
(20 - 35%). This figure increases up to 1/3rd of cases in our setup

Patient Approach

Establish the severity of the exacerbation as well as the severity of preexisting


COPD. The more severe either of these two components, the more likely that
the patient will require hospital admission.
The history should include;
 Quantification of the degree and change in dyspnea
 Fever
 Change in character of sputum
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 Associated symptoms such as wheezing, nausea, vomiting, diarrhea,


myalgias, and chills.
 Frequency and severity of prior exacerbation.
 The single greatest risk factor for hospitalization with an exacerbation is a
history of previous hospitalization.
Physical examination;
 An assessment of the degree of distress of the patient.
▪ Tachycardia
▪ Tachypnea
▪ Use of accessory muscles
▪ Signs of perioral or peripheral cyanosis
▪ The ability to speak in complete sentences, and
▪ The patient’s mental status.
 Chest examination
▪ Focal findings
▪ Degree of air movement
▪ Wheezing
▪ Asymmetry in the chest examination (suggesting large airway
obstruction or pneumothorax mimicking an exacerbation), and
▪ Paradoxical motion of the abdominal wall.

DDX for COPD exacerbations → see Approach part of this chapter above

Investigation
 Chest x-ray or chest CT scan.
▪ For patients with severe underlying COPD, who are in moderate
or severe distress, or those with focal findings
▪ Approximately 25% of x-rays in this clinical situation will be
abnormal, with the most frequent findings being pneumonia and
CHF.
 Arterial blood-gas analysis
▪ For patients with advanced COPD, a history of hypercarbia, mental
status changes (confusion, sleepiness), or those in significant
distress.
▪ The presence of hypercarbia, defined as a PCO2 >45 mmHg, has
important implications for treatment (discussed below).
 Pulmonary function test is not recommended

Management of exacerbations of COPD

Indication for admission


 New or worsening hypoxemia
 Severe underlying disease 239
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 Those whose living situation is not conducive to careful observation and


the delivery of prescribed treatment. (this is the commonest reason in our
setup, and almost all patients need admission) and
 Respiratory acidosis and hypercarbia

Most COPD patients in our country are undiagnosed, a few of them are told
they have ‘’bronchitis’’ without confirmatory spirometry and still fewer have
confirmed COPD.
 Therefore, as discussed in patient approach part, COPD with acute
exacerbation should be considered in every patient presenting with a
recent worsening of his/her longstanding cough or dyspnea or sputum
color change (purulence).

Non-pharmacologic management principles are the same as stable COPD


management (see above). These include;
 Assessing and monitoring of the disease
 Avoidance of modifiable risk factors/precipitant causes and vaccinations
 Pulmonary rehabilitation.

Pharmacologic management

COPD exacerbations can be classified into 4 categories based on severity


(look at GOLD severity classification above)
☛ Mild: can be managed at home with SABAs only.
☛ Moderate: can be managed as outpatient with SABAs + antibiotics+
steroids
☛ Severe without respiratory failure: can be treated in the wards with
SABAs + antibiotics+ steroids.
☛ Severe with respiratory failure: Needs ICU admission for Respiratory
support (Noninvasive or invasive ventilation).
✓ Noninvasive intermittent positive pressure ventilation (NIPPV)
in exacerbations improves blood gases and pH, reduces in-
hospital mortality, decreases the need for invasive mechanical
ventilation and intubation, and decreases the length of hospital
stay.
Pharmacologic management Principles include;
 Oxygen therapy
 Bronchodilators → Inhaled bronchodilators (beta2-agonists and/or
anticholinergics)
 Corticosteroids
 Antibiotics → if there is features of airway infection (like increased
volume/change of color of sputum, fever). Identify and treat precipitant
causes

 ? Mucolytic Agents: a few patients with viscous sputum may benefit but
the widespread use cannot be recommended
 ? Antitussives: Cough, a troublesome symptom in COPD, has a protective
role. Regular use of antitussives contraindicated

1. Oxygen therapy
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☛ Deliver a flow rate of <15 L/min.


☛ Source of oxygen can be a cylinder (>99% pure oxygen) or oxygen
concentrator (90% oxygen,10% nitrogen).
☛ Titrated to achieve a SaO2 of 88-90% to avoid oxygen induced
hypercapnia.
☛ See the details from stable COPD management above
2. Bronchodilators
☛ Short acting bronchodilators:
o Metered dose inhaler (MDI)= Salbutamol inhaler (200
mcg/actuation): 2-3 puffs every hour and then tapered to 2 puffs
every 4hrs.
▪ To read and watch video on how to use MDI, (click here
→ 8.3.2. How to use inhalers for asthma management )
o Nebulization of salbutamol or combined salbutamol/ipratropium
bromide solution.
☛ Long-acting bronchodilators + ICS → should be continued if patient was
using them and should be started at discharge if they were not being
used.

3. Corticosteroids
☛ Only used when having a significant exacerbation (moderate or severe
disease), as they may lead to development of pneumonia and sepsis
☛ Can be given orally (prednisolone 40mg) or IV (hydrocortisone or
methylprednisolone). Oral and IV routes are equally effective
☛ Recommended for 5-7 days only

4. Antibiotics
☛ Recommended for moderate to severe illness or when the sputum is
purulent.
☛ Patients experiencing COPD exacerbations with clinical signs of airway
infection (e.g., increased volume and change of color of sputum, and/or
fever) may benefit from antibiotic treatment.
☛ Antibiotics are usually given for 5-7days
☛ The specific antibiotic given should depend on the sensitivity pattern of
the hospital.
o Commonly Augmentin (Amoxicillin/clavulanic acid), cephalosporins,
quinolones or macrolides can be used.
☛ Sputum culture is generally not helpful except in few conditions which
may be associated with Gram negative infections like pseudomonas
aeruginosa. Such as
o Patient has recurrent exacerbation.
o Patient is on invasive mechanical ventilation.

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2.1.2 Asthma
→ Refer under short case of Nitsbin (click here → 8.3. Asthma (አስም))

2.2 Restrictive lung disease

2.2.1 ILD (Interstitial Lung disease)


Dr. Mulualem. G, Dr. Asmare. W

ILDs (a.k.a Diffuse Parenchymal Lung Diseases/ DPLDs/) are a


heterogeneous group of disorders that are classified together because of
similar clinical, radiographic, physiologic, or pathologic manifestations
Include a large number (>200) of heterogeneous conditions that affect
the lung parenchyma with varying degrees of inflammation and fibrosis
“interstitial”- indicates the abnormality begins in the interstitium
o It’s a misleading term as most of these disorders are also
associated with extensive alteration of alveolar and airway
architecture
Are associated with considerable rates of morbidity and mortality, and
there is little consensus regarding the best management of most of
them.

Classification

>200 diseases are known to be associated with diffuse parenchymal


lung involvement making classification of ILDs very difficult
o Primary conditions, or
o Part of multiorgan process
There are various classification schemes

5. Based on the major underlying histopathology


✓ Those associated with predominant inflammation and fibrosis
✓ Those with predominantly granulomatous reactions in interstitial or
vascular areas
6. Based on the cause
✓ ILDs of known cause or association
✓ Idiopathic
☛ Idiopathic interstitial pneumonias
☛ Granulomatous DPLDs
☛ Other forms of DPLDs
The treatment choices and prognosis depend mainly on the causes and
types of ILD, so ascertaining the correct diagnosis is important
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A variety of infections can cause interstitial opacities on CXR, including


fungal, atypical bacterial, and viral pneumonias, especially in
immunosuppressed individuals. R/O these conditions before considering
ILD.

FIGURE 293-1(Harrison 21st edition) Classification of interstitial lung disease. This algorithm represents a common
approach to subclassifying the interstitial lung diseases. It is typical to divide the interstitial lung diseases into
those of known and unknown causes (although it is important to note that genetic studies demonstrate that a
significant portion of familial and idiopathic pulmonary fibrosis [classically described as diseases of unknown

cause] may be explained, in part, by genetic factors)

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Diffuse parenchymal lung diseases consist of disorders of known causes (rheumatic disease, environmental or
drug related) as well as disorders of unknown cause. The latter include idiopathic interstitial pneumonias,
granulomatous lung disorders (eg, sarcoidosis), and other forms of interstitial lung disease including
lymphangioleiomyomatosis, pulmonary Langerhans cell histiocytosis/histiocytosis X, and eosinophilic pneumonia.

The interstitial pneumonias are further categorized as chronic fibrosing, acute or subacute fibrosing, or smoking

related. Lymphoid interstitial pneumonia is typically associated with other disease processes, such as rheumatic
disease or immunosuppression; idiopathic lymphoid interstitial pneumonia is rare.

DPLD: diffuse parenchymal lung disease; IIP: idiopathic interstitial pneumonia; LAM: lymphangioleiomyomatosis;
PLCH: pulmonary Langerhans cell histiocytosis/histiocytosis X.

➢ The most common identifiable causes of ILD are exposure to


occupational and environmental agents, especially the inhalation of
inorganic dusts, organic dusts, and various fumes or gases
➢ Sarcoidosis, and idiopathic pulmonary fibrosis (IPF) are the most
common ILDs of unknown etiology.
➢ ILD can also complicate the course of most of the connective tissue
diseases like polymyositis/dermatomyositis, rheumatoid arthritis, and
SLE

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Pathogenesis

Diagram; Proposed mechanism for the pathogenesis of pulmonary fibrosis. The lung is naturally exposed to

repetitive injury from a variety of exogenous and endogenous stimuli. Several local and systemic factors (e.g.,
fibroblasts, circulating fibrocytes, chemokines, growth factors, and clotting factors) contribute to tissue healing and

functional recovery. Dysregulation of this intricate network through genetic predisposition, autoimmune conditions,

or superimposed diseases can lead to aberrant wound healing, with the result of pulmonary fibrosis. Alternatively,

excessive injury to the lung may overwhelm even intact reparative mechanisms and lead to pulmonary fibrosis 245
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➢ ILDs are nonmalignant disorders and are not caused by identified


infectious agents
➢ The precise mechanism leading from injury to fibrosis is not known
➢ Although there are multiple initiating agents, the mechanisms of repair
have common features leading to common clinical findings

Clinical approach

Patients with ILD commonly present with


☛ Symptoms of progressive dyspnea
☛ Persistent dry cough
☛ Symptoms associated with the underlying disease, such as
CTDs
☛ History of occupational smoking
☛ Abnormal chest radiograph
☛ Restrictive pattern on spirometry
Certain peculiar features of presentations help to differentiate the
different types of ILDs
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History

➢ Age – some of the ILDs are more common in certain age groups
o Sarcoidosis, CTDs-associated ILDs, LAM, inherited forms of ILD,
and PLCH commonly present b/n ages of 20-40 yrs
o Most patients with IPF are over the age of 50yrs
(LAM: lymphangioleiomyomatosis; PLCH: pulmonary Langerhans cell histiocytosis/histiocytosis X.)

o
➢ Gender
o Female
▪ LAM and tuberous sclerosis
▪ LIP, CTDs associated ILDs except RA
(LIP = Lymphoid interstitial pneumonia)

o Male
▪ IPF
▪ ILD associated with RA
▪ Pneumoconiosis

➢ Onset of symptoms
o Acute presentation- unusual, days to weeks
▪ Acute interstitial pneumonia
▪ Eosinophilic pneumonia
▪ Hypersensitivity pneumonitis
▪ Cryptogenic organizing pneumonia
▪ NB- infectious causes of interstitial infiltrates should be ruled
out
o Subacute- weeks to months 247
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Can occur in all ILDs



Sarcoidosis, drug induced ILDs, alveolar hemorrhage sxxs,

SLE associated pneumonitis
o Chronic presentations- months to years
▪ Most ILDs present with longstanding sxs
▪ IPF
▪ Sarcoidosis
▪ Pneumoconiosis
▪ PLCH and CTDs
▪ Important ddxs are COPD and chronic HF
o Episodic presentations- unusual, but can occur in
▪ Eosinophilic pneumonia, hypersensitivity pneumonitis, COP,
and pulm hemorrhage sxx
o Hypersensitivity pneumonitis and sarcoidosis can have acute,
subacute, or chronic presentations
➢ Past medical history
o CTDs, IBD, or malignancy
o Medications and prior irradiation
o Immunosuppression
o Hx of allergy and asthma
➢ Smoking history
o Some ILDs occur largely among current or former smokers
▪ PLCH
▪ DIP
▪ RB-ILD
▪ IPF
(PLCH: pulmonary Langerhans cell histiocytosis/histiocytosis X, DIP; Desquamative Interstitial
Pneumonia, RB-ILD; Respiratory Bronchiolitis – ILD, IPF; Idiopathic pulmonary fibrosis)

o Active smoking can contribute to complications in pts with


Goodpasture’s sxx
➢ Family history
o Autosomal dominant pattern of inheritance has been reported for
familial IPF, tuberous sclerosis, and neurofibromatosis
o Autosomal recessive pattern of inheritance has been identified
for Niemann-Pick disease, Gaucher’s disease, and Hermansky-
pudlak sxx
➢ Occupational and environmental exposures
o Review of home and work environment
o A strict chronologic listing of the pt’s lifelong employment
o The degree of exposure, duration, latency of exposure, and the
use of protective devices
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Symptoms- most are nonspecific, but some will help to narrow


differential
☛ Dyspnea- sarcoidosis, silicosis, and PLCH may have extensive
parenchymal lung disease on CXR without significant dyspnea
☛ Cough-particularly bothersome in conditions that involve the
airways like sarcoidosis, PLCH, hypersensitivity pneumonitis
☛ Hemoptysis- diffuse alveolar hemorrhage sxx, PLCH,
granulomatous vasculitidis
☛ Wheezing – lymphangitic carcinomtosis, chronic eosilophilic
pneumonia, respiratory bronchiolitis 250
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☛ Chest pain- CTDs, sarcoidosis, or pneumthorax


☛ Extrapulmonary symptoms

Physical examination

➢ Findings are nonspecific, except the extrapulm ones suggesting the


underlying sytemic disorder
➢ Tachypnea
➢ Bibasilar end inspiratory crackles
➢ Accentuated P2, evidence of right side heart failure
➢ Clubbing- common in IPF and asbestosis, but rare in sarcoidosis and
hypersensitivity pneumonitis
➢ Extrapulmonary findings of systemic disease

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Diagnostic testing

➢ Lab tests
o CBC with differential
o U/A, BUN, cr
o RVI screening
o ANA, RF
o ANCA, anti-BM antibodies
o
o
CRP, ESR
ACEs
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➢ ECG
➢ Echocardiography
➢ Chest X-ray
o Reticular pattern is the most common finding
o Nodular and reticulonodular pattern can also be seen
o The correlation b/n CXR abnormalities and clinical or
histopathologic stage of the disease is generally poor.
o The presence of honeycombing portends poor prognosis
o Evaluate all previous chest films to assess the rate of change in
disease activity
o Could be normal in 10% of pts with ILD, esp hypersensitivity
pneumonitis

Picture; Honeycombing- clustered cystic airspaces

➢ Certain radiologic patterns give important clues to specific etiologies


➢ Other clues include changes in lung volumes, disease distribution,
and associated findings, including pleural and LN inv’t
➢ The main radiologic patterns seen in ILDS include
o Reticular
o Nodular-including micronodular and miliary
o Linear- septal or kerley’s
o Reticulonodular
o Destructive
o Alveolar
o Bronchial
o Arterial patterns
➢ Reticular pattern
o Acute diseases
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▪ Acute pneumonia in CTDs


▪ Allergic pneumonitis
o Chronic diseases
▪ All idiopathic interstitial pneumonias
▪ CTDs
▪ Asbestosis
▪ Radiation pneumonia
▪ Drug reactions
▪ LAM

Micronodular patterns – seen infrequently


☛ Early stages of pneumoconiosis
☛ Alveolar microlithiasis

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Nodular pattern
☛ Usually seen in granulomatous lesions
☛ Sarcoidosis
☛ Pneumoconiosis
☛ Pulm hemosiderosis
☛ Neoplasms
☛ Infectious causes- tbc, fungal infections

Linear opacities- kerley lines


☛ Due to thickening of the interlobular septa
☛ Frequently seen in LV failure
☛ Can be seen in lymphangitic carcinomatosis, asbestosis,
RBILD and viral infections
Lung volumes
☛ Loss of lung volume is a frequent feature of all ILDs
☛ Some ILDs are associated with normal or large lung volumes
due to airflow obstruction or cystic changes
☛ PLCH
☛ Sarcoidosis
☛ LAM
☛ Low lung volumes can also represent the first manifestation of
ILD

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CXR; shows coarse reticular and reticulonodular opacities involving both lungs diffusely. The lung volumes are
preserved. Enlarged central pulmonary arteries suggest pulmonary arterial hypertension

➢ Disease distribution
o The anatomic distribution of lung disease can greatly facilitate
the approach to ddx
o Upper zone lung disease
▪ Sarcoidosis
▪ Pneumoconiosis except asbestosis
▪ PLCH
▪ Radiation fibrosis
▪ Infectious causes- tbc and fungal disease
▪ Ankylosing spondylitis

Chest radiograph shows a destructive pattern Chest radiograph shows multiple larger
with marked loss of volume in both upper nodules, 3-5 mm in diameter, with a bias
lobes, retraction of both hilar regions
cephalad, distortion, and hyperexpansion of
the lung bases. Bilateral upper lobe cavities
containing mycetomas are present.
for the upper lobes. Note calcification in
some of the pulmonary nodules and the
hilar lymph nodes.
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➢ Basal lung disease


o DIP
o NIP and fibrosis
o IPF/UIP
o Asbestosis
o Scleroderma
o Rheumatoid arthritis
o Drug reactions
➢ Central, perihilar disease
o Sarcoidosis
o Lymphoma
o Kaposi sarcoma
➢ Peripheral lung disease
o IIPs
o Asbestosis
o Eosinophilic lung disease
o Graft-vs-host disease
➢ NB- advanced stages of any infiltrative lung process can involve both
lungs diffusely

Associated findings
Pleural disease
✓ Pneumothorax
☛ PLCH
☛ LAM
✓ Pleural effusions
☛ Metastatic malignancies
☛ CVDs esp RA and SLE
☛ LAM
✓ Pleural plaques- accompany 30-50% of pts with longstanding
asbestos exposure

HRCT

➢ For early detection and confirmation of ILD


➢ Better assessment of the extent and distribution of disease
➢ Avoids the need for biopsy in those pts with IPF
➢ Certain features suggest specific diagnosis 257
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o LAP with upper lobe inv’t- sarcoidosis and other granulomatous


lesions
o Pleural plaques with linear calcification- asbestosis
o Subpleural and bibasilar reticular opacities associated with
honeycomb changes and traction bronchiectasis- IPF, RA
associated ILD, or chronic hypersensitivity pneumonitis

Idiopathic pulmonary fibrosis. High-resolution CT image shows bibasal, peripheral predominant reticular abnormality
with traction bronchiectasis and honeycombing. The lung biopsy showed the typical features of usual interstitial

pneumonia. Stage II sarcoidosis according to Siltzbach's classification. Multiple miliary peribronchiolar nodules are
scattered diffusely throughout both lungs. In addition, both hilar regions are enlarged due to lymph node

enlargement.

Pulmonary function testing


➢ Spirometry
o Assess the extent of pulmonary involvement
o Most ILDs have a restrictive pattern
▪ Reduced TLC, FRC, and RV
▪ FEV1 and FVC- reduced
▪ FEV1/FVC ratio- normal or increased
o Some ILDs can have obstructive pattern
▪ Sarcoidosis
▪ LAM
▪ Hypersensitivity pneumonitis
▪ PLCH
▪ Tuberous sclerosis
▪ Combined COPD with ILD
o Have prognostic value in pts with IIPs, esp IPF and NSIP
➢ Diffusing capacity (DLCO)
o Reduced DLCO is a common finding 258
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o The severity of DLCO doesn’t correlate well with disease


prognosis
➢ Gas exchange at rest and during exercise
o Resting arterial blood gases may be normal in early ILD
o Normal PaO2 at rest doesn’t rule out significant hypoxemia
during exercise or sleep
o Exercise testing- 6MWT
▪ To follow ILD activity and responsiveness to Rx
➢ Bronchoalveolar lavage (BAL)
o Pts with hemoptysis
o Acute onset ILD
o Certain causes of ILD
▪ Sarcoidosis
▪ Hypersensitivity pneumonitis
▪ PLCH
o Suspicion of infectious causes
o No role in IPF
o No role in the assessment of ILD progression or response to
therapy
➢ Lung biopsy
o The most effective method for confirming the diagnosis and
assessing disease activity
o Done if less invasive evaluations are not sufficient to make the
correct dx
o Atypical or progressive sns and sxs
▪ Age <50yrs
▪ Fever, wt loss, hemoptysis
o Atypical radiographic features
o Rapid clinical deterioration
o Sudden change in radiographic appearance
o Relative C/Is
▪ Serious CVDs
▪ Honeycombing and other radiologic evidence of diffuse end-
stage disease
▪ Severe pulm dysfunction and elderly

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Image; ILD diagnostic algorithm

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Treatment of ILDs
➢ Goal
o Reduce further lung damage
▪ Permanent removal of the offending agent
▪ Early identification and aggressive suppression of the acute
and chronic inflammatory process
o Therapy doesn’t reverse fibrosis
➢ Identify and Rx treatable causes
➢ Hypoxemia- supplemental O2
➢ Management of cor pulmonale
➢ Pulmonary rehabilitation
➢ Drug therapy
o Glucocorticoids
▪ For symptomatic ILD pts
▪ Start prednisone, 0.5 - 1 mg/kg, PO, daily for 4–12 weeks, at
which time the patient is reevaluated and taper slowly
• If the patient is stable or improved, the dose is tapered to
0.25– 0.5 mg/kg and is maintained at this level for an
additional 4–12 weeks, depending on the course.
▪Rapid tapering or a shortened course can result in
recurrence
o Cyclophosphamide and azathioprine
▪ (1 - 2 mg/kg/day), and mycophenolate mofetil, with or without
glucocorticoids for 8–12 weeks
▪ If no response to steroids
▪ IPF, vasculitis, progressive systemic sclerosis
o Methotrexate, colchicine, penicillamine and cyclosporine
▪ If the above measures fail or not tolerated
➢ Lung transplantation

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2.3 Suppurative lung diseases

Suppurative Lung Diseases are group of pulmonary disorders that characterized


by presence of pus within the lung parenchyma. These include;
❖ Bronchiectasis
❖ Lung abscess and
❖ Empyema

Here, we will discuss about Bronchiectasis and lung abscess. For Empyema,
refer respiratory section from short case of Nitsbin (click here → Empyema and
Complicated Parapneumonic Effusions)

2.3.1 Bronchiectasis

Bronchiectasis refers to an irreversible airway dilation that involves the lung in


either a focal or a diffuse manner
Classically, it has been categorized as
❖ Cylindrical or tubular (the most common form)
❖ Varicose
❖ Cystic
It shares many clinical features with COPD, including inflamed and easily
collapsible airways, obstruction to airflow, impaired clearance of secretions and
frequent office visits and hospitalizations.

Etiology

➢ Bronchiectasis can arise from infectious or noninfectious causes


➢ Clues to the underlying etiology are often provided by the pattern of lung
involvement.
➢ Focal bronchiectasis refers to bronchiectatic changes in a localized area of the
lung and can be a consequence of obstruction of the airway. The cause may
be;
 Extrinsic (e.g., due to compression by adjacent lymphadenopathy or
parenchymal tumor mass) or
 Intrinsic (e.g., due to an airway tumor or aspirated foreign body, Mucus
Plugging (e.g. postoperative mucoid impaction, a scarred/ stenotic airway,
or bronchial atresia from congenital underdevelopment of the airway).
➢ Diffuse bronchiectasis is characterized by widespread bronchiectatic changes
throughout the lung and often arises from an underlying systemic or infectious
disease process (i.e. acquired or congenital causes).

✓ Acquired (~74%)
▪ Infectious → A variety of infections can cause bronchiectasis by
destroying and damaging the bronchial walls and interfering with
ciliary action.
o Influenza, Adenovirus, Pertussis, Mycobacterium (M. TB, MAC)
o Post TB fibrosis is the commonest cause in Ethiopia
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o Recurrent infections (airway obstruction, immunodeficiency,


allergic bronchopulmonary aspergillosis, mycobacterium)
o RVI (cause abnormal lung defense),
▪ Inflammatory;
o Gastric Aspiration
o Autoimmune disease (RA, SLE, Crohn disease, Sjogren’s
Syndrome, etc.)
o Ammonia
o Neoplasm (not common)
✓ Naturally will have faster course but Slower in carcinoids

✓ Congenital:
▪ Cystic fibrosis, Primary ciliary dyskinesia (e.g., Kartagener
syndrome), Immunoglobulin deficiency (IgG, IgA...)
o Cystic fibrosis (CF) is the most common cause of
bronchiectasis (accounts for half of all cases) world wide
o Have diffuse pattern commonly occur in upper lobes.
➢ In many cases (25 - 50%), the etiology of bronchiectasis is not determined
(idiopathic).

Pathophysiology

Induction of bronchiectasis requires two factors:


o An infectious insult
o Impaired drainage, airway obstruction, or a defect in host defense
The most widely cited mechanism of infectious bronchiectasis is the “vicious
cycle hypothesis,” in which susceptibility to infection and poor mucociliary
clearance result in microbial colonization of the bronchial tree.
o The presence of the microbes incites continued chronic inflammation,
with consequent damage to the airway wall, continued impairment of
secretions and microbial clearance, and ongoing propagation of the
infectious/inflammatory cycle.
o Significant small-airway wall inflammation and larger-airway wall
destruction as well as dilation, with loss of elastin, smooth muscle,
and cartilage.
Proposed mechanisms for noninfectious bronchiectasis include immune-
mediated reactions that damage the bronchial wall (e.g., those associated with
systemic autoimmune conditions such as SLE, RA…)
Traction bronchiectasis refers to dilated airways arising from parenchymal
distortion as a result of lung fibrosis (e.g., post radiation fibrosis or idiopathic
pulmonary fibrosis).
Site:
o Left lung involved more than Right lung (Left to Right ratio = 9 : 7 )
o Left Lower lobe most frequently involved, Followed by Right middle
lobe........Left upper lobe

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Clinical Presentation:

Most cases, onset is in childhood but, symptoms generally appear in 2nd - 3rd
Decades
Relatively common in females (F:M = 2.5 : 1.5)
The most common clinical presentation is a persistent productive cough with
ongoing production of thick, tenacious sputum which may/may not be foul-
smelling.
Dyspnea
Hemoptysis → due to rupture of blood vessels near bronchial wall surfaces;
usually mild and self-limited, but sometimes can be brisk and presents as an
emergency
Crackles and wheezing on lung auscultation
Clubbing of the digits in some patients
Acute exacerbations of bronchiectasis are usually characterized by changes in
the nature of sputum production, with increased volume and purulence.
However, typical signs and symptoms of lung infection, such as fever and new
infiltrates, may not be present.
Evaluation of focal bronchiectasis almost always requires bronchoscopy to
exclude airway obstruction by an underlying mass or foreign body

Diagnosis and Investigations

The diagnosis is usually clinically (a persistent chronic cough and sputum


production) accompanied by consistent radiographic features.

B. CXR
 Although chest radiographs lack sensitivity, the presence of “tram tracks”
indicating dilated airways is consistent with bronchiectasis.
 CXR is abnormal in most cases, but findings are nonspecific. Suspicious,
but non diagnostic radiographic findings include linear atelectasis, dilated
and thickened airways and irregular peripheral opacities that may
represent mucopurulent plugs.

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C. High-resolution Chest CT → is Gold Standard diagnostic imaging (i.e. more


specific for bronchiectasis and is the imaging modality of choice for confirming
the diagnosis.). CT findings include;
 Airway dilation (detected as parallel “tram tracks” or as the “signet-ring
sign”—a cross-sectional area of the airway with a diameter at least 1.5
times that of the adjacent vessel)
 Lack of bronchial tapering (including the presence of tubular structures
within 1 cm from the pleural surface)
 Bronchial wall thickening in dilated airways
 Inspissated secretions (e.g., the “tree-in-bud” pattern)
 Cysts emanating from the bronchial wall (especially pronounced in cystic
bronchiectasis)

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D. PFTs (if available) reveal an obstructive pattern


 Mild to moderate airflow obstruction is often detected on pulmonary
function tests, overlapping with that seen at presentation with other
conditions, such as COPD
E. Laboratory tests;
 CBC with differential → supportive, if infectious cause is suspected, but
may be normal
 Sputum smear and culture for bacteria, mycobacteria, and fungi
▪ AFB or other TB diagnostic tests should be done, for a patient
suspected with bronchiectasis, considering epidemiology of TB in
Ethiopia
 Rheumatoid factor

F. Other laboratory tests (not available in our set up)


 Immunoglobulin quantitation to measure the levels of the immunoglobulins
IgG, IgM, and IgA and
 Testing for cystic fibrosis: including Alpha-1 antitrypsin
level and/or genotype
 Specific aspergillus IgE and IgG antibodies, total serum IgE level
 IgG subclass levels
 Antibody titers to pneumococcal serotypes before and four weeks after
vaccination with polysaccharide pneumococcal vaccine

Management of Bronchiectasis

Conservative medical therapy


 Mainstay of treatment for bronchiectasis is conservative medical therapy
 Treatment of infectious bronchiectasis is directed at the control of
active infection and improvements in secretion clearance and bronchial
hygiene so as to decrease the microbial load within the airways and
minimize the risk of repeated infections.
Surgical management
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1) Medical therapy includes

➢ Stop smoking (Tobacco Use) for smokers


➢ Control Infection → Antibiotics for acute exacerbations and superimposed
infections
 Superimposed infections are signaled by change in quality/quantity of
sputum, fever, chest pain, etc.
 Antibiotics targeting the causative or presumptive pathogen (with
Haemophilus influenzae and P. aeruginosa isolated commonly) should be
administered in acute exacerbations
 Duration is usually for a minimum of 7 - 10 days and perhaps for as
long as 14 days.
 For severe cases; 2-3 weeks of IV followed by Oral (decreases morbidity,
controversial)
➢ Eliminate reversible underlying cause
 TB → Anti TB
 Foreign bodies → Remove
 Endobronchial Tumors → Remove (surgical)
 Hypogammaglobinemia → Life Time IV supplementation
➢ Improve bronchial secretion clearance
 Chest physiotherapy (postural drainage, chest percussion) to help remove
the mucus
 Mucolytic (N-acetyl cysteine, Recombinant DNase)
➢ Reverse air flow limitation by Inhaled Bronchodilators (e.g. salbutamol)
➢ Consider oral/ systemic glucocorticosteroids (e.g. Prednisolone/prednisone,
hydrocortisone) as anti-inflammatory agents

2) Surgical management

Indication →refractory significant symptoms despite a prolonged medical trial


In select cases, surgery can be considered with;
▪ Resection of a focal area of suppuration.
▪ Lung transplantation → can be considered in advanced cases,
Principles;
 Seldom performed on children ≤ 2 yrs. Because of likelihood of
improvement on medical therapy as the child grows
 Priorities given to preservation of lung parenchyma
 Exclude uncorrectable causes: Ciliary dyskinesia, multimodality
 Use dual-lumen endotracheal tube may minimize spillage to contralateral
lung
 Segmentectomy or lobectomy, as indicated by anatomic involvement
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 For bilateral disease, side with greater involvement is resected first


(symptoms may sufficiently improve to preclude resection of opposite side)
 For those ultimately requiring bilateral resection, an interval 6 -12 months
is generally recommended to allow adequate recovery and evaluation of
symptoms

2.3.2 Lung Abscess


Dr. Mulualem. G

Lung abscess (a.k.a necrotizing pneumonia) represents necrosis and cavitation


of the lung following microbial infection.
Lung abscesses can be single or multiple but usually are marked by a single
dominant cavity >2 cm in diameter (> 6 cm is poor prognostic sign).
Most cases of lung abscess may be due to complications of aspiration
pneumonia by anaerobic microorganisms present in the gingival cervices.
In general, middle-aged men are more commonly affected than middle-aged
women (age > 60 is poor prognostic sign)

Risk factors for primary lung abscess

Aspiration → The major risk factor for primary lung abscesses. Patients at
particular risk for aspiration include;
o Those with altered mental status
o Prior cerebrovascular or cardiovascular events
o Seizures
o Esophageal dysmotility or esophageal lesions (strictures or tumors)
o Gastric distention and/or GERD, especially those who spend substantial
time in the recumbent position
o Alcoholism
o Drug overdose
o Bulbar dysfunction
o Neuromuscular disease.

Etiology and pathogenesis

Lung abscesses are usually characterized as either primary (~80% of cases)


or secondary.
Primary lung abscesses usually arise from aspiration, are often caused
principally by anaerobic bacteria, and occur in the absence of an underlying
pulmonary or systemic condition.
o The development of primary lung abscesses is thought to originate
when chiefly anaerobic bacteria in the gingival crevices are aspirated
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into the lung parenchyma in a susceptible host


o Pneumonitis develops initially (exacerbated in part by tissue damage
caused by gastric acid); then, over a period of 7 - 14 days, the
anaerobic bacteria produce parenchymal necrosis and cavitation
Secondary lung abscesses arise in the setting of an underlying condition,
such as; A post obstructive process (e.g., a bronchial foreign body or tumor)
or A systemic process (e.g., HIV infection or another immunocompromising
condition).
o The pathogenesis of secondary abscesses depends on the
predisposing factor. For example, in cases of bronchial obstruction from
malignancy or a foreign body, the obstructing lesion prevents clearance
of oropharyngeal secretions, leading to abscess development.
o With underlying systemic conditions (e.g., immunosuppression), impaired
host defense mechanisms lead to increased susceptibility to the
development of lung abscesses caused by a broad range of
pathogens, including opportunistic organisms
o Lung abscesses also arise from septic emboli
Lung abscesses can also be characterized as acute (< 4 - 6 weeks in
duration) or chronic (~40% of cases).
o Symptom duration of > 8 weeks is poor prognostic sign
Examples of Microbial Pathogens That Can Cause Lung Abscesses include;
o Primary lung abscess (usually with risk factors for aspiration)
▪ Often polymicrobial, primarily including Anaerobes (e.g., Pepto
streptococcus spp, Bacteroides spp) as well as microaerophilic
streptococci
o Secondary lung abscess (often with underlying immunocompromise)
▪ Staphylococcus aureus → can arise from Embolic lesions (often
from endocarditis)
▪ Pseudomonas aeruginosa → most common
▪ Enterobacteriaceae)
▪ Nocardia spp., Aspergillus spp., Cryptococcus spp, Legionella
spp.
▪ PCP (Pneumocystis jirovecii)
o Endemic infections (with or without underlying immunocompromise)
▪ M. tuberculosis (as well as MAC)
▪ Histoplasma capsulatum, Coccidioides, Blastomyces spp.,
▪ parasites (e.g., Entamoeba histolytica, Strongyloides stercoralis)

Clinical features
− Clinical manifestations may initially be similar to those of pneumonia, with
fevers, cough, sputum production, and chest pain
− Copious putrid or malodorous sputum is typical for anaerobic infection and
common in lung abscess.
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or ward where the sputum is collected.


− Absence of chills or rigors. But Patients with lung abscesses due to non-
anaerobic organisms, such as S. aureus, may present with a more fulminant
course characterized by high fevers and rapid progression.
− Hemoptysis or pleurisy
− A more chronic and indolent systemic presentation that includes night sweats,
fatigue, and anemia is often observed with anaerobic lung abscesses.
− Findings on physical examination may include;
o Fevers
o Poor dentition, and/or gingival disease
o Amphoric and/or cavernous breath sounds on lung auscultation.
o Digital clubbing and the absence of a gag reflex.

Differential diagnosis

Noninfectious processes that result in cavitary lung lesions, include;


➢ Lung infarction
➢ Malignancy
➢ Sequestration
➢ Cryptogenic organizing pneumonia
➢ Sarcoidosis
➢ Vasculitides and other autoimmune diseases (e.g., granulomatosis with
polyangiitis)
➢ Lung cysts or bullae containing fluid
➢ Septic emboli (e.g., from tricuspid valve endocarditis)

Complications of lung abscess

Larger cavity size on presentation may correlate with the development of


persistent cystic changes (pneumatoceles) or bronchiectasis.
Additional possible complications include
o Recurrence of abscesses despite appropriate therapy
o Extension to the pleural space with development of empyema
o Life-threatening hemoptysis, and
o Massive aspiration of lung abscess contents.

Investigations and diagnosis

1. CXR
➢ a thick-walled cavity with an air-fluid level
➢ pulmonary infiltrates with cavity confirm diagnosis in majority of patients.

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Image 1, Lung abscess; PA (A) and lateral (B) CXR show areas of consolidation and several air-fluid levels
within the right lower lobe. Less extensive consolidation is evident in the right middle lobe.

2. CT scan
➢ CT permits better anatomic definition than CXR and may provide earlier
evidence of cavitation.
➢ CT may also yield additional information regarding a possible underlying
cause of lung abscess, such as malignancy
➢ May help to distinguish a peripheral lung abscess from a pleural infection.
o This distinction has important implications for treatment because a
pleural space infection, such as an empyema, may require urgent
drainage.
➢ But in our setup CT is too costly for most patients and it is better to
diagnose clinically and with CXR findings

Image 2, Lung abscess; CT image of the above pt confirms the CXR findings and also demonstrates a few
centrilobular nodules in the right middle lobe (black arrow). The patient was a 50-year-old man with
pneumonia due to anaerobic organisms.

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Figure; Representative chest CT scans demonstrating development of lung abscesses. This patient was
immunocompromised by underlying lymphoma and developed severe Pseudomonas aeruginosa pneumonia, as
represented by a left lung infiltrate with concern for central regions of necrosis (panel A, black arrow). Two
weeks later, areas of cavitation with air-fluid levels were visible in this region and were consistent with the
development of lung abscesses (panel B, white arrow).

3. Gram stain and culture of expectorated sputum → contaminations is likely,


may indicate upper airway pathogens than the lower, may be negative if
antibiotic already started
4. AFB and KOH examination of sputum → if TB or fungal causes are
considered.
5. Pleural fluid analysis → click here → Pleural fluid analysis
6. Blood cultures → When a secondary lung abscess is present or empirical
therapy fails to elicit a response, sputum and blood cultures are advised

NB: the isolation of anaerobic microorganisms from lung infections is usually


challenging (rarely grow from blood samples and mostly contaminated from
sputum and aspirates), except for empyema patients.

Treatment of lung abscess

Principles of management include;


− Chest physiotherapy and postural drainage
− Empiric antibiotic therapy
− Surgery in selected cases

Empiric antibiotic therapy for lung abscess

Anaerobic coverage is imperative regardless of culture (both strict and


facultative anaerobes) Since Mixed infection (anaerobes and facultative
anaerobes like oral streptococci) is common in lung abscess.
If non oral floral pathogen is detected from microbiologic reports, tailor
treatment to the specific microorganism.

First line

✓ Ampicillin-sulbactam 1.5 - 3 g IV QID.


o Once the patient’s condition is stable, change to oral Augmentin
(amoxicillin-clavulanate)
o This therapy should be continued until imaging demonstrates that the
lung abscess has cleared or regressed to a small scar.
o Treatment duration may range from 3 - 4 weeks to as long as 14
weeks (usually 4-8 weeks)

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✓ Ceftriaxone (1g IV BID or 2 g IV daily) or


✓ Penicillin G 1 - 2 million units IV QID or
✓ Cefotaxime 1 or 2 g IV TID
plus
✓ Metronidazole 500 mg PO TID
o N.B Notably, metronidazole is not effective as a single agent: it
covers anaerobic organisms but not the microaerophilic streptococci.
So, combination with penicillin’s is mandatory
☛ For penicillin-allergic patients
o Clindamycin, 600 mg, IV, TID then, with the disappearance of fever
and clinical improvement, 300 mg PO QID

Or one of the following

✓ Piperacilin/tazobactam 4.5 gm IV QID


✓ Meropenem 1 g IV TID

Parenteral-to-Oral Switch of antibiotics:

➢ After treatment with intravenous antibiotics for the first 2-3 weeks or
until significant resolution of symptoms, patients can be treated with oral
antibiotics until the end of treatment.
➢ Augmentin (Amoxicillin + clavulanic acid), 625mg P.O TID is the preferred
agent.
➢ Clindamycin, 300mg P.O, QID14 is an alternative otherwise the choice may
be guided by the susceptibility data available.

Follow up

Do weekly or 2 times per week CXR in patients showing clinical


improvement, with discontinuation of therapy when the radiograph is clear or
there is a small, stable, residual lesion

Surgical management

Indication;
Patients who do not respond to antibiotics and whose additional diagnostic
studies fail to identify an additional pathogen that can be treated
Treatment Options include;
Surgical resection and
Percutaneous drainage of the abscess → especially when the patient is a poor
surgical candidate.

14
This dose if from Harrison 21 st edition. 2021 national STG guideline for General hospitals of Ethiopia
recommend ‘’Clindamycin 450 - 600mg, PO, TID’’
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Timing of surgical intervention can be challenging;


The goal is to balance the morbidity/mortality risk of a procedure with the need
for definitively clearing the abscess in the setting of persistent infection that is
not responsive to nonsurgical approaches.

Possible complications of percutaneous drainage include


Bacterial contamination of the pleural space
Pneumothorax
Hemothorax.

Prognosis

Mortality rates for secondary abscesses are generally higher—as high as 75%,
while rates for primary abscesses have been as low as 2%
Other poor prognostic factors include;
o Age of > 60 years
o The presence of aerobic bacteria
o Sepsis at presentation
o Symptom duration of >8 weeks, and
o Abscess size of >6 cm.

Prevention

➢ Mitigation of underlying risk factors may be the best approach to prevention


of lung abscesses, with attention directed toward;
o Airway protection
o Oral hygiene, and
o Minimized sedation with elevation of the head of the bed for patients
at risk for aspiration.
➢ Prophylaxis against certain pathogens in at-risk patients (e.g., recipients of
bone marrow or solid organ transplants or patients whose immune systems
are significantly compromised by HIV infection) may be undertaken.

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2.4. Cor pulmonale and Pulmonary Hypertension

➢ Cor pulmonale is a Latin word meaning ‘’Pulmonary heart’’


➢ Cor pulmonale is an isolated right sided failure which results from pulmonary
hypertension
➢ Cor pulmonale, also referred to as pulmonary heart disease, is broadly defined
by altered RV/right ventricle/ structure and/or function in the context of chronic
lung disease and is triggered by the presence of pulmonary hypertension.
➢ On the other way, cor pulmonale can be defined as the enlargement and
failure of the right ventricle of the heart as a response to increased vascular
resistance (such as from pulmonary stenosis) or high blood pressure in the
lungs.
➢ Although Right Ventricular dysfunction is an important sequela of HFpEF and
HFrEF, this is not considered as cor pulmonale. So, to be classified as
pulmonary heart disease, the cause must originate from the lung (i.e. in the
pulmonary circulation system)
➢ Right ventricular Hypertrophy due to a systemic defect is not classified as
pulmonary heart disease. The heart and lungs are intricately related; whenever
the heart is affected by a disease, the lungs risk following and vice versa.

Etiology and epidemiology

➢ Chronic cor pulmonale develops in response to chronic pulmonary hypertension


resulting from parenchymal lung disorders, primary pulmonary vascular
diseases, or conditions leading to alveolar hypoxia (see table above).
➢ The true prevalence of cor pulmonale is difficult to ascertain.
 First, not all patients with chronic lung disease will develop cor pulmonale,
which may be subclinical in compensated individuals.
 Second, the ability to detect pulmonary hypertension and cor pulmonale
by routine physical examination and laboratory testing is relatively
insensitive
➢ Once susceptible patients develop cor pulmonale, their prognosis worsens,
regardless of the underlying etiology.
➢ Although COPD is responsible for ~50% of the cases of cor pulmonale
(western data), any disease that affects the pulmonary vasculature or
parenchyma can lead to cor pulmonale.
➢ Primary pulmonary vascular disorders, such as pulmonary arterial hypertension
or chronic thromboembolic pulmonary hypertension, are relatively rare causes
of cor pulmonale, but cor pulmonale is extremely common with these
conditions, given the magnitude of elevated pulmonary artery pressures and
pulmonary vascular resistance.
➢ Look at the table from DDX part of patient approach above

Pathophysiology

➢ Although many conditions can lead to cor pulmonale, the common


pathophysiologic mechanism is pulmonary hypertension and increased RV
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afterload sufficient to alter RV structure (i.e., dilation with or without


hypertrophy) and function.
 Normally, mean pulmonary artery pressure is only ~15 mmHg (does not
increase significantly even with increasing multiples of cardiac output
because of pulmonary vasodilation and blood vessel recruitment in the
pulmonary circulatory bed)
➢ In the setting of parenchymal lung diseases, primary pulmonary vascular
disorders, or chronic (alveolar) hypoxia, the circulatory bed undergoes vascular
remodeling, vasoconstriction, and destruction. As a result, pulmonary artery
pressures and RV afterload increases, setting the stage for cor pulmonale
➢ The systemic consequences of cor pulmonale relate to alterations in cardiac
output as well as salt and water homeostasis.
➢ Anatomically, the RV is a thin-walled, compliant chamber better suited to
handle volume overload than pressure overload. Thus, the sustained pressure
overload eventually leads to RV dysfunction and failure.
➢ The response of the RV to pulmonary hypertension depends on the acuteness
and severity of the pressure overload.
 Acute cor pulmonale occurs after a sudden and severe stimulus (e.g.,
massive pulmonary embolus), with RV dilatation and failure but no RV
hypertrophy.
 Chronic cor pulmonale, however, evolves slowly and in conjunction with
modest, compensatory RV hypertrophy that lowers wall tension and
preserves RV function. Over time, RV dilation ensues leading to an
increase in RV wall tension and overt dysfunction.
 Acute decompensation of compensated chronic cor pulmonale is a
common clinical occurrence.
➢ Triggers include;
 Worsening hypoxia from any cause (e.g. pneumonia)
 Acidemia (e.g., exacerbation of COPD)
 Acute pulmonary embolus
 Atrial tachyarrhythmia
 Hypervolemia, and
 Mechanical ventilation that compresses blood vessels associated with
alveoli and further increasing RV afterload.

Clinical features and Investigation → look at the approach section above

Treatment

➢ Identification and treatment of the underlying cause is the mainstay of


treatment
➢ The treatment for cor pulmonale may include the following;
 Oxygen therapy
▪ Oxygen is often required to resolve the shortness of breath.
Additionally, oxygen to the lungs also helps relax the blood vessels
and eases right heart failure.
▪ Look at below, indications for home oxygen, under COPD
management
 Antibiotics → if there is acute exacerbation or sign of infection
 Diuretics → to decrease strain on the heart;
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▪ Diuretics should be used with caution.


▪ In RSHF Hypervolemia is preload dependent, minimal and moderate
dose of diuretics may end up with cardiogenic shock. So, slow and
cautious escalation is needed
▪ ACE-inhibitors [with diuretics] used for cardiac remodeling effect
▪ But, in LSHF Diuretics can be escalated up easily unless there is
low BP from the onset. (e.g. furosemide 20-40 mg IV, double the
dose every 2-4hours, max. 400-600mg/day)
 Phlebotomy (Venesection)→ is used in severe secondary polycythemia
(because of hypoxia), which improves symptoms though survival rate has
not been proven to increase.
 Expectorants
 Digitalis
 Bronchodilators → When wheezing is present, the majority of individuals
require a bronchodilator.
 Anticoagulants → are used when venous thromboembolism is present.
 Transplantation → Finally, transplantation of single/double lung in extreme
cases of cor pulmonale is also an option.

Pulmonary hypertension (PH)


➢ Pulmonary hypertension (PH) is a spectrum of diseases involving the
pulmonary vasculature, and defined as an elevation in pulmonary arterial
pressures (mean pulmonary artery pressure [PAP] >22 mmHg
or an estimated systolic PAP >36 mmHg).
➢ Pulmonary arterial hypertension (PAH) is a relatively rare form of PH and is
characterized by symptoms of dyspnea, chest pain, and syncope.
➢ If left untreated, the disease carries a high mortality rate, with the most
common cause of death being decompensated right heart failure.

Clinical features

➢ The diagnosis of PH can be missed without a reasonable high index of


suspicion.
➢ PH symptoms are nonspecific, insidious, and overlap considerably with many
common conditions, including asthma and other lung disease, and cardiac
disease.
➢ Most patients will present with dyspnea and/or fatigue, whereas edema, chest
pain, presyncope, and syncope are less common and associated with more
advanced disease.
➢ In early phases of PAH, the physical examination is often unrevealing.
➢ As the disease progresses there may be evidence of RSHF with elevated JVP,
lower extremity edema, and ascites.
➢ Additionally, the CVS examination may reveal an accentuated P2 component of
the S2 (typical sign for PH) a right-sided S3 or S4, and TR.
➢ Clubbing may be seen in some chronic lung diseases
➢ Crackles on examination of the lungs and systemic hypertension may be clues
to left-sided systolic or diastolic heart failure.
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Investigations → see the approach section above

PFT (Pulmonary function tests)


 Results of PFT may suggest restrictive or obstructive lung diseases as
the cause of dyspnea or PH
 N.B an isolated reduction in diffusing capacity of the lungs for carbon
monoxide (DLCO) is the classic finding in PAH,
LFT, HBsAg → to screen for underlying liver disease
BNP → Important in diagnosis and management of PH
RHC (Right heart catheterization) with pulmonary vasodilator testing
 Remains the gold standard both to establish the diagnosis of PH and to
guide selection of Appropriate medical therapy.
 The definition of precapillary PH or PAH requires;
▪ An increased mean pulmonary arterial pressure (mPAP >25 mmHg)
▪ A pulmonary capillary wedge pressure (PCWP), left atrial pressure,
or left ventricular end-diastolic pressure (LVEDP) ≤15 mmHg; and
▪ Total pulmonary vascular resistance (PVR) >3 Wood units.

Classification system of Pulmonary hypertension


➢ WHO classifies patients with PH into five groups based upon etiology.
➢ WHO functional classification for pulmonary hypertension (Class I to Class IV)
is the same as NYHA functional classification of Heart failure.
 The only difference is, Patients with pulmonary hypertension in WHO but
Patients with cardiac disease in NYHA (click here → Chapter 1; Heart
failure (ልብ ድካም))

Group I; PAH (pulmonary arterial Hypertension)


Relatively rare cause of PH and diagnosis of exclusion
PAH includes a group of diseases and defined as a sustained elevation in
resting mPAP ≥25 mmHg based on Right heart catheterization
It can be further classified as
 Idiopathic PAH
 Heritable
 Drug- and toxin-induced
 Associated with Connective tissue diseases, HIV infection, Portal
hypertension, Congenital heart diseases, Schistosomiasis

Group II; PH due to left heart disease


The commonest cause of PH
WHO Group II PH includes;
❖ Left heart systolic dysfunction
❖ Aortic and mitral valve disease, and
❖ Heart failure with preserved ejection fraction (HFpEF)
The hallmark of Group II PH is elevated left atrial pressure with resulting
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Increased pulmonary venous pressure indirectly leads to a rise in pulmonary


arterial pressure.
The presence of PH portends a poor prognosis in all forms of heart failure

Group III; PH due to chronic lung disease


Intrinsic lung disease is the second most common cause of PH
PH has been observed in both COPD and ILD (from ILD, Commonly in
idiopathic pulmonary fibrosis)
It can also be seen in diseases with mixed obstructive/restrictive physiology:
bronchiectasis, cystic fibrosis, emphysema predominantly in the upper lung
zones and mixed obstructive restrictive disease marked by fibrosis in the lower
lung zones

Group IV; PH associated with chronic thromboembolism

Group V; PH with unclear multifactorial mechanisms


A group of miscellaneous diseases that only rarely cause PH, Examples
include PH caused by;
 Hematologic disorders (eg, chronic hemolytic anemia, myeloproliferative
disorders, splenectomy)
 Systemic disorders (eg, sarcoidosis)
 Metabolic disorders (eg, glycogen storage disease, Gaucher disease,
thyroid disorders)
 Others (e.g. chronic renal failure, tumoral obstruction, fibrosing
mediastinitis, segmental pulmonary hypertension)

Management of Pulmonary Hypertension (PH)

➢ The baseline severity of PH should be determined prior to the initiation of


therapy
 Functional impairment and hemodynamic derangement are the key
determinants of disease severity
 The next step is classifying the patient condition based on WHO etiology
classification (Group I to V) and WHO functional classification (Class I to
IV)
➢ Several therapies should be considered in patients with All groups of PH
including diuretic, oxygen, anticoagulant, and digoxin therapy, as well as
exercise.
 These therapies should be administered taking into consideration the
underlying cause as well as the risks and benefits associated with each
therapy.
➢ Once the severity of the patient's pulmonary hypertension has been
determined, Treatment of the underlying cause is the mainstay of treatment of
PH

Group I → There are no effective primary therapies for most types of group I
PAH. As a result, advanced therapy is often needed
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Chapter 2; Chronic lung disorders and Cor pulmonale

 Without treatment PAH is invariably fatal.


 While there is no cure for PAH, current pharmacologic therapies improve
morbidity, and in some cases, mortality.
 Management options include;
▪ Prostacyclin and prostacyclin analogues and agonists
▪ NO (Nitric oxide) pathway enhancers
▪ Endothelin receptor antagonists (ERAs) and
▪ Combination of those agents
Group II → treatment of the underlying heart disease
Group III → treatment of the underlying cause of hypoxemia and correction of
the hypoxemia with supplemental oxygen.
 Oxygen is the only modality with proven mortality benefit in some patients
with group III PH
Group IV → Anticoagulation is primary medical therapy for patients with group
IV PH
 Surgical thromboendarterectomy is primary surgical therapy for selected
patients with thromboembolic obstruction of the proximal pulmonary
arteries
Group V → treatment of the underlying cause

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Chapter 3; TB/Tuberculosis/ (የሳንባ ነቀርሳ ፣ ቲቢ)

Chapter 3; TB/Tuberculosis/ (የሳንባ


ነቀርሳ ፣ ቲቢ)
Dr. Mulualem. G, Dr. Asmare.W

Clinical features and how to write hx of TB patient


History

➢ TB Pt’s may present with


Pulmonary TB symptoms
o Persistent cough for ≥ 2 weeks, (cough of any duration for
HIV positives)
o Fever for ≥ 2 weeks
o Night sweats
o Unexplained weight loss
Extra pulmonary manifestations → Look at discussion section below
Both pulmonary and extrapulmonary
➢ The most common symptom of pulmonary TB is a productive cough of ≥ 2
weeks, which may be accompanied by other respiratory symptoms (SOB, chest
pains, and hemoptysis) and/or constitutional symptoms (loss of appetite, weight
loss, fever, night sweats, and fatigue).
➢ However, cough might not be the predominant presentation for certain
population group, particularly in people living with HIV, young children, and
severely malnourished. Hence, high index of suspicion is required to diagnose
TB among these groups.
➢ A history of contact with infectious TB case, and presence of documented
recent weight loss may indicate the presence of TB in such patients to warrant
investigation.
➢ Some patients may present with;
▪ Chest pains → due to pleurisy, muscle strain
▪ SOB (breathlessness) → due to extensive lung disease or concomitant
pleural effusion
▪ Localized wheeze → due to local Tuberculous bronchitis, or because of
external pressure on the bronchus by an enlarged lymph node.

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Characterization of patient history

➢ Cough (82%)
Gradual in onset → chronic (≥ 2 weeks)
Comes day and night without aggravating and relieving factor
or worsen at night
Initially patients may present with dry cough
➢ Sputum
As said above Initially TB patients may present with dry cough,
later becomes productive cough with
✓ Mucoid (purulent) sputum
✓ Non-position dependent
✓ Non blood tingled (sometimes blood streaked in cavitary
lesions or haemoptysis /30%/)
✓ Non foul smelling
✓ ‘’X’’ Arabic coffee cup per day
✓ Increase in frequency and amount gradually
➢ B smx’s
✓ Fever (75%) → low grade, intermittent with/without chills and
rigor
✓ Night sweet (65%)
✓ Weight loss (73%) → Significant weight loss (>5% of his/her
initial body weight or significant but unquantified weight loss to
the extent his/her cloth becomes loose)
➢ Appetite loss (61%)
➢ Easy fatigability

➢ SOB
✓ Progressive in onset
✓ Common if there is pleural effusion from disseminated TB
➢ Chest pain (pleuritic chest pain) /54%/ → also from pleural effusion and
characterized by
✓ Sudden, sharp, stabbing, localized pain
✓ Aggravated by deep breathing, coughing, sneezing, laughing
etc
✓ Relieved by assuming to the same side of the effusion
o N.B pain relieved by leaning forward in pericarditis
✓ May radiate to shoulder or back
✓ Associated with rapid and shallow breathing, SOB, dry cough

☛ Manifestations of HIV-infected patients → Refer under RVI section of


Nitsbin (click here →RIV - TB) 282
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Risk factors

Determinants of transmission
▪ Duration of contact with TB pt
▪ Shared environment of contact (e.g poorly ventilated house)
▪ Similar illness in the family, living in the same house or
dormitory, camp, refuge place
▪ Geographical location → TB is common in 3rd world countries
RF for developing disease after infection
▪ Cigarette smoking
▪ Comorbidities → RVI (RVI increase risk of acquiring TB, 20-37
times greater lifetime risk than HIV negative), DM, CKD…
o Currently DM highly Increases Risk of Acquiring TB Like
RVI (but we didn’t get actual data of Association)
▪ Recent infection (< 1 year)
▪ Fibrotic lung disease
▪ Malnutrition and immunocompromisation
LOC → increase risk of Aspiration
Industrial chemical exposure

Complication of TB

➢ Pulmonary complications of TB include


▪ Hemoptysis
▪ Pneumothorax, bronchiectasis
• TB is the commonest acquired cause of bronchiectasis in our
set up (N.B Cystic fibrosis is the commonest cause of
bronchiectasis in western set up)
▪ Extensive pulmonary destruction
• Post TB fibrosis which result in COPD
▪ Malignancy and
▪ Chronic pulmonary aspergillosis.
• Aspergilloma formation in TB cavitary lesions → infection of
cavity by aspergillus flavus
➢ Extra pulmonary TB
✓ TB lymphadenitis
✓ Genito urinary TB
✓ Skeletal TB
✓ Pleural TB which may complicate with Empyema formation
✓ TB pericarditis
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✓ TB peritonitis
✓ Intestinal TB
✓ TB meningitis and Tuberculoma
✓ Miliary TB

Sample history

Chief compliant

Cough of 3 weeks duration

HPI
This patient was last relatively healthy 03 weeks back at which time she
started to experience a gradual onset of initially dry cough which Comes day
and night without aggravating and relieving factor. Later becomes non position
dependent productive cough with Mucoid, non-position dependent, Non blood
tingled, non-foul-smelling sputum of half to 1 Arabic coffee cup per day which
Increase in frequency and amount progressively. Associated with this she also
experienced low grade, intermittent fever, profuse night sweat to the extent her
under wear becomes soaked and unquantified but significant weight loss to the
extent her clothes become loose but no SOB or chest pain.
10 years back, her husband was diagnosed with Pulmonary TB. Diagnosis was
made with sputum examination and CXR at addis zemen primary hospital. He
discontinued the medication due to unknown reason and died (contact hx is strong
RF)
Currently she is not married and lives in family size of 4. She has 3 boys and
one daughter. All are above 5 years old, alive and healthy. (family screening,
especially those under five years old, is one of principle of management)
Lives in well ventilated iron corrugated house having 2 windows and
one door, all are functional, with separate kitchen. (poorly ventilated house
accelerates TB transmission and RF for COPD → DDX)
She was screened for RVI 04 months back and found to be NR (RVI
increase risk of acquiring TB 20 to 37x than seronegative persons)
No hx of Cigarette smoking, or hemoptysis (cigarette is RF for developing disease after
TB infection, and RF for Lung ca → DDX)
No hx of abnormal body movement, LOC or tracheal intubation (aspiration →
RF)
No hx of DM, HTN or Asthma (comorbidities → RF)
No hx of swelling over the neck, axilla or groin (LN TB or scrofula → CXN)
No hx of Flank pain, dysuria, urgency, frequency or hematuria (Genito urinary
TB /stricture, pyelonephritis, sterile pyuria…. Infertility and menstrual abnormality in females/ → cxn)
No hx of bone pain, joint pain or swelling (bone TB → CXN)
No hx of tinnitus, blurring of vision, light headedness or easy fatigability
(anaemia 2ry to bone marrow suppression _ bone TB → CXN)
No hx of headache, fever or neck stiffness (TB meningitis → CXN)
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No hx of back pain, body weakness or back bone deformity (gibbus formation

which result in paraplegia → CXN)


No hx of bone pain, herbicide exposure, epistaxis or bleeding from other body
sites (mediastinal lymphoma → DDX)
No hx of dyspnea, leg swelling or RUQ abdominal pain (COPD and Cor pulmonale →
DDX. N.B considering COPD as DDX with this short duration of cough in this case, makes very unlikely)
No hx of tooth extraction, lower facial pain or nasal discharge (RF for lung
abscess → DDX)
No hx of drug intake (DDX for coughing; e.g. ACE - I’s Like Enalapril)
No hx of contact with animal abortus material (even though extremely rare, brucellosis can
present as TB → DDX)

Finally, she was admitted to our hospital supported physically by her


families

Physical examination (pertinent findings)

1 GA → Chronically sick looking

2 Vital signs

➢ Febrile → TB is one of the causes of FUO (fever of unknown origin)


➢ Tachycardia and tachypnoea → especially in miliary TB
➢ Low BMI → emaciated (Cachexia)

3 HEENT

➢ Pale conjunctiva → Anaemia from skeletal TB with bone marrow


involvement

4 LGS

➢ Cervical or supraclavicular LAP → TB lymphadenitis

5 RS

➢ Clubbing
➢ Signs of pleural effusion
➢ Rales, rhonchi, amphoric breath sound
➢ Apical consolidation signs
➢ Localized wheeze → TB bronchitis, LAP obstructing the bronchus

6 CVS

➢ Pericardial friction rub → TB pericarditis

7 Abdominal examination

➢ Tiped splenomegaly with/without hepatomegaly → Miliary TB


➢ Palpable mass and intestinal obstruction → intestinal TB 285
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➢ Huge Ascites → TB peritonitis


➢ GOO (Gastric outlet obstruction) → TB LAP obstructing the pylorus

8 GUS → CVAT from genitourinary TB

9 MSS

➢ Back bone tenderness and deformity → gibbus (TB spondylitis)


➢ Knee or other major joint swelling (bone and joint TB)

10 IS

➢ Palmar pallor → Anaemia from skeletal TB with bone marrow involvement


➢ Erythema nodosum commonly in shins and rarely in thigh → primary TB

11 NS

➢ Meningeal irritation signs → TB meningitis


➢ Paraplegia → pott’s disease

DDX for patients presenting with chronic cough


1) Pulmonary TB
2) Lymphoma
Present with B smx’s as the same as TB (fever, night sweat, weight
loss)
Mediastinal lymphoma (NHL)
✓ Misdiagnosed as TB
☛ Case scenario; One Patient with mediastinal lymphoma at UOG Hospital,
was misdiagnosed as pulmonary TB and she was on anti TB for a long
period of time but no improvement. Finally, mediastinal lymphoma was
diagnosed after chest CT scan was done (ward c, @2012 e.c.)
3) Cor pulmonale
4) COPD
5) Bronchiectasis
6) Lung abscess → very offensive foul-smelling sputum and fever is typical
for lung abscess
7) ILD
Pt’s present with prolonged unexplained SOB, dry cough
Misdiagnosed as TB

For Cor pulmonale, COPD, Bronchiectasis, Lung abscess and ILD refer
chapter 2 (click here → Chapter 2; Chronic lung disorders)
8) Lung ca
Usually have +ve family hx of lung ca, common in smokers and
present with bloody sputum.
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Refer under long case of Nitsbin (click here → Chapter 4; Lung


cancer (የሳንባ ካንሰር))
9) Drug’s (E.g. ACE -I’s Like Enalapril)
Common side effect of ACE -I’s Like Enalapril is unexplained dry
cough
If other causes of cough are ruled out in a patient taking ACE -I’s
→ discontinue the drug and change with other alternatives like
ARB’s or CCB’s based on the case. If the cough is due to the drug
side effect, Cough will stop after 2-3 days of discontinuation of ACE
-I’s.
10) SLE
F: M ratio is 9:1
Involves lung, pleura (pleural effusion), pericardium (leg edema)
refer under short case of Nitsbin (click here →12.1.2. Systemic lupus
erythematosus (SLE) (lupus))

11) MAC (mycobacterium avium complex)


12) FUNGAL infections
13) GERD
14) VL
15) Brucellosis
✓ Extremely rare
✓ Associated with animal abortus exposure
✓ Caused by brucella abortus
✓ Have similar clinical picture as TB and difficult to differentiate

For RVI - TB DDX refer under RVI Section of Nitsbin (click


here →

Pneumonia with parapneumonic effusion)

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IX

A. Diagnosis For active TB

1. CXR → what do you expect from CXR?


There is no pathognomonic sign
Upper lobe lesion with or without cavity (reactivation TB)
Apical consolidation
Lower lobe opacity, hilar, peritracheal or mediastinal
lymphadenopathy (primary TB)
Hilar LAP (post primary TB)
Milliary pattern may be helpful in diagnosing some forms of
extrapulmonary TB
Normal in 30% of HIV pts. With TB
Pleural effusion → request PA and lateral decubitus view CXR if you
suspect pleural effusion
✓ Obliterated costophrenic angle
✓ +ve meniscus sign
✓ Haziness over the dependent lung field
Old granuloma
Infiltration

Picture; CXR showing a right-upper-lobe infiltrate and a cavity with


an air-fluid level in a patient with active tuberculosis

2. Sputum examination
Sputum examination includes
o AFB microscopy
o Culture → gold standard, minimum of 10-100 bacilli per ml
are required for growth, unlike AFB microscopy which needs
approximately 10,000 bacilli per ml for detection of bacteria
o Gene expert → TB dx, RMP sensitivity
o Gram stain → to screen bacterial superinfection
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o PCR if available
AFB microscopy
o The detection of acid-fast bacilli (AFB) on microscopic
examination of stained sputum smears is the most rapid and
inexpensive TB diagnostic tool.
o A serious of at least 3 single specimens should be collected
in 8 to 24 hours interval (with at least one specimen obtained
early in the morning) which should be submitted to the
laboratory for AFB smear and mycobacterial culture, although
the diagnosis often can be made with 2 specimens
▪ Spot - morning - spot examination (currently we are
using spot - spot examination only)
o If pt present with dry cough, use induced sputum with BAL or
hypertonic saline method
o Sputum AFB smears are relatively less sensitive (45 - 80%)
than nucleic acid amplification (NAA) or culture; approximately
10,000 bacilli per mL are needed for detection of bacteria in
AFB smear using light microscopy.

MYCOBACTERIAL CULTURE
o +ve in 80% of active TB
o Gold standard, minimum of 10-100 bacilli per ml are required
for growth
o 6 - 8 weeks may be required before growth is detected for
conventional media and 1-3wks for Liquid media
o 1-2 wks more for sensitivity test
Gene x-pert (Nucleic acid amplification technology)
o Useful in the diagnosis of AFB-negative pulmonary and
extrapulmonary TB.
o Detects Rifampicin resistance
o Have Sensitivity of 98% among AFB-positive cases and ~70%
among AFB-negative specimens
o Results available in 4-6 hours

N.B

❖ Smear +ve TB
2 +ve sputum examination or
1 +ve sputum examination and one of the following
o 1 culture +ve examination or
o Typical CXR finding or
o RVI pt
❖ Smear -ve TB
Culture +ve but doesn’t fulfil the above criteria and unresponsive
to broad spectrum antibiotics
✓ For smear -ve patients
▪ Repeat smear and request CXR 289
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▪ If all IX including CXR do not suggest TB, prescribe


antibiotics for two weeks
❖ Follow up sputum examination (Look at management part below)
➢ Sputum examination for all new smear +ve pt’s should be repeated at
2nd, 5th, and 6th months
➢ Sputum examination for previously treated patient should be done at 3rd,
5th and 8th months

3. Pleural fluid analysis → for pleural involvement; refer under short cases of
Nitsbin (click here → Pleural fluid analysis)
Determinations of ADA and IFN-γ levels in pleural fluid may be
useful adjunctive tests in the diagnosis of pleural TB (Tuberculous
pleural effusion is ADA value of >40 U/L).
4. Urine LF-LAM assay
➢ The urine LF-LAM assay is an immunocapture assay based on the
detection of the mycobacterial LAM antigen in urine, and is a potential
point-of-care test for certain populations being evaluated for TB.
➢ Although the assay lacks sensitivity, it can be used as a fast, bedside,
rule-in test for HIV-positive individuals, especially in urgent cases where
a rapid TB diagnosis is critical for the patient’s survival.
➢ The detection of mycobacterial LAM antigen in urine does not provide
any information on drug resistance.

B. DIAGNOSIS OF LATENT M. TUBERCULOSIS INFECTION (LTBI)

5. TST/Tuberculin skin test/ (Mantoux test) → PPD (purified protein derivative)


a.k.a Tuberculin
The Mantoux TST is the intradermal injection of 0.1 ml purified
protein derivative (PPD). For Indurations, measure after 48-72hrs
Tuberculin sensitivity develops 3 weeks to 3 months (most often in
4-8 weeks) after inhalation of organisms

Picture; TST induration

A TST should be regarded as positive in the following circumstances:

PPD ≥ 5mm within 48-72hrs suggest +ve test in the following


conditions
o For immunocompromised patients (like RVI &organ
transplant pts) because they have less reactive immunity
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o Recent contact of TB patient


o Fibrotic changes on CXR suggestive of old TB
o Patients on treatment with TNF-alpha blockers
PPD ≥ 10mm induration
o Recent arrivals from high prevalence countries
o Injection Drug Users
o Nursing Homes, Prisons
o Mycobacterial Lab. Workers
PPD ≥ 15mm is a +ve test even if the is no risk factor for TB
Extremely important for children (for those not vaccinated with
BCG) and latent TB in adult
False negative PPD test
o Overwhelming TB
o Wrong techniques
o Immunocompromised patients
▪ HIV
▪ Steroids
▪ Cancer
▪ Measles and
▪ Severe PEM (Protein energy malnutrition) i.e. SAM
in children
False positive PPD test
o Atypical mycobacterial infections
o Hypersensitivity to constituents
o BCG vaccination
6. IGRA (interferon-gamma release assay)

➢ Both TST and IGRA are recommended for immunocompromised adults


(although intended to increase sensitivity in this high-risk group, there is
no specific evidence to support this practice); LTBI treatment is
warranted if either test is positive. Immunocompromised children should
be referred to a specialist.
➢ TST is recommended for new entrants from high-incidence countries who
present to health care services; an IGRA can be offered if TST not
available.
➢ IGRA alone may be used for outbreak situations and other circumstances
in which follow-up for TST interpretation may be difficult.

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C. Baseline investigation

7. CBC
NcNc anaemia
Thrombocytopenia 2ry to Rifampicin treatment
8. ESR → elevated (supportive for diagnosis)
9. U/A → U/A done as baseline, urine culture may be done for dx
Sterile pyuria (i.e. culture -ve pus in urine)
Urine culture may be +ve for genitourinary TB
10. RFT → as a Pre-treatment Evaluation
BUN and creatinine to start ant TB treatment, since anti TB drugs
have nephrotoxic effect (e.g. streptomycin is nephrotoxic)
11. Live Enzymes (SGPT, SGOT) → as a Pre-treatment Evaluation, anti TB drugs
have hepatotoxic effect (especially pyrazinamide)
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12. PICT → RVI -TB coinfection is very common


13. Urine HCG → for all women of child bearing age, as a Pre-treatment
Evaluation

D. Additional investigations to be done based on indication

For patients with suspected, any form of, extrapulmonary TB.


o BAL (Bronchoalveolar lavage), Fiberoptic bronchoscopy
▪ Invasive diagnostic procedures
▪ Then, AFB, Gene expert, culture, gram stain can be done from the
sample
For extra pulmonary TB involving the pleura
o Pleural fluid analysis
Common investigation in our set up
o CXR
o Chest U/S
▪ Can differentiate
• Loculated effusion from tumour
• Pleural effusion from thickening of pleura
▪ Guide thoracentesis
o Chest CT scan and MRI
o Pleural biopsy
▪ Diagnostic for pleural TB
▪ Granuloma formation is expected
▪ Culture +ve in 80% Of Cases

TB lymphadenitis
▪ FNAC, LN Biopsy, AFB, Tissue culture (50%+ve)
▪ From enlarged LN
▪ N.B Biopsy also can be taken from pleura and solid lesions
TB peritonitis
▪ Abdominal U/S
▪ Peritoneal TAP
Musculo skeletal tuberculosis (TB)
▪ X-ray of the involved part
▪ Synovial fluid aspiration or synovial biopsy and analysis if there is
Joint swelling
• findings of Synovial fluid analysis are usually nonspecific
▪ Microscopy and culture of infected material
• Tissue may be obtained by needle aspiration and/or biopsy;
CT guidance is useful in regions where available.
▪ CT or MRI reveals the characteristic lesion.
• But, consider if other IX failed to suggest DX (this is for cost
effectiveness)
TB Pericarditis
o Echo, CT, or MRI → shows effusion and thickness across the
pericardial space.
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o Pericardiocentesis under echo guidance


▪ exudative fluid, with a high count of predominantly lymphocytes and
monocytes
▪ hemorrhagic effusion is common.
o Direct smear examination → is very rarely positive.
o Culture → +ve in up to 2/3rd of cases
▪ pericardial biopsy has a higher yield.
Intracranial TB
o MRI is useful in the diagnosis of intracranial TB
▪ Tuberculous meningitis
✓ LP (CSF analysis)
▪ Tuberculoma
✓ Brain MRI/CT
✓ For intracranial TB like tuberculoma (biopsy is
necessary to dx tuberculoma)
For Genito urinary TB
o Diagnosis requires biopsy or culture of specimens obtained by dilation
and curettage.
▪ Culture -yields a definitive diagnosis in nearly 90% of cases.
▪ Culture-negative pyuria in acidic urine should raise the suspicion of
TB (i.e. Pyuria in U/A but culture -ve, which is known as sterile
pyuria)
Hydronephrosis
▪ IV pyelography
▪ Abdominal U/S
▪ Abdominal CT/MRI
Stricture secondary to Genito urinary TB
▪ Cystourethrography can show;
o Deformities and obstructions, calcifications and ureteral stricture
▪ CT and MRI are more sensitive if Cystourethrography fails to detect

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Discussion

3.1 Pulmonary TB

Definition of terminologies in TB infection

Pulmonary TB (PTB) → M. Tuberculosis infection localized to lung parenchyma


or the tracheobronchial tree
Extra pulmonary TB → lymphohematogenous spread or local extension of M.
Tuberculosis to different organ systems. It includes disseminated and miliary
patterns of dissemination. E.g. TB lymphadenitis, TB meningitis, Pott’s
Disease…..
Disseminated TB → a mycobacterial infection in which mycobacteria have
spread from the lungs to other parts of the body through the blood or lymph
system. E.g. Disseminated TB to the lungs, pleura and peritoneum
Miliary tuberculosis → used to denote all forms of progressive, widely
disseminated hematogenous TB which spreads to various organs. some
authors use disseminated TB interchangeably with miliary TB. however, miliary
TB in fact refers more specifically to disseminated TB which presents with a
millet-seed-like appearance on a chest x ray, when the disease is spread by
blood throughout the lungs. Miliary TB is classified as PTB because there are
lesions in the lungs (look at miliary TB section below)

EPIDEMIOLOGY

➢ Mycobacterium tuberculosis is the second most common infectious cause


of death in adults worldwide (second to HIV, which is the most common
infectious cause of death).
➢ The human host serves as a natural reservoir for M. tuberculosis
➢ More than two billion people (about 30 percent of the world population)
are estimated to be infected with M. tuberculosis. The global incidence of
tuberculosis (TB) peaked around 2003 and appears to be declining
slowly.
➢ The epidemiology of TB varies substantially around the world. The
highest rates are observed in sub-Saharan Africa, India, and the islands
of Southeast Asia and Micronesia.

Tuberculosis situations in Ethiopia

Tuberculosis is a major public health problem posing significant deleterious


health impacts by affecting the productive segment of the population and
resulting serious burden to the health system and exploiting the
individuals/household economy.
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Ethiopia remains to be among the 30 countries reported with high burden of


TB, TB/HIV and DR-TB for 2015 to 2020.
TB related mortality is highlighted in the top 10 reported causes of death
among hospital admissions, with annual estimated death rate of 26 per
100,000 populations in 2015

II. Microbiology, Natural history, and pathogenesis

MICROBIOLOGY

M. tuberculosis belongs to the genus Mycobacterium, which includes more than


50 other species, often collectively referred to as nontuberculous mycobacteria.
Tuberculosis (TB) is defined as a disease caused by members of the M.
tuberculosis complex, which include the tubercle bacillus (M. tuberculosis), M.
bovis, M. africanum, M. microti, M. canetti, M. caprae, M. pinnipedii, and M. orygis

Transmission of M. tuberculosis

From inhalation of droplet nuclei (1-5 um in diameter) produced when patient


with pulmonary or laryngeal TB coughs. Rarely from ingestion of raw milk from
cows affected by bovine TB, congenital
Transmission facilitated by prolonged exposure to infectious environment; small
enclosed spaces with inadequate ventilation
The probability of transmission depends on the dynamics of four major factor
A. The susceptibility of the host
B. Degree of infectiousness of the person with TB disease
C. Environmental factors and
D. Level of exposure (proximity, frequency and duration).

The risk of infection of a susceptible individual is therefore higher with close,


prolonged, indoor exposure to a person with infectious pulmonary TB.
Patients with cough who are AFB smear +ve are considered most infectious
The most infectious patients have cavitary pulmonary disease or laryngeal TB
or endobronchial TB.
Sputum smear-negative/culture positive TB patients are less infectious,
responsible for < 20% of transmission.
Culture negative pulmonary TB and Extrapulmonary TB pts are generally non-
infectious.
Persons with both HIV infection and TB are less likely to have cavitation’s,
they may be less infectious than persons without HIV co-infection.
Population groups with conditions that compromise the immune system,
including People living with HIV, Diabetics, young age groups and
malnourished, are at higher risk of developing Active TB as they fail to contain
the latent TB infection from progressing to active disease.
Besides, congregated settings like prisons, refugee camps, homeless shelters
and urban slums are usually overcrowded and poorly ventilated. The
inhabitants usually are very poor, neglected and marginalized contributing to
higher transmission risk and susceptibility to TB.
Consumption of raw milk containing M.bovis is also a possible way of getting
infected by TB, though it is much less frequent.
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Natural History of M. tuberculosis Infection

➢ Inhalation of aerosol droplets containing M. tuberculosis with subsequent


deposition in the lungs leads to one of four possible outcomes:
✓ Immediate clearance of the organism
✓ Primary disease: immediate onset of active disease (common among
children, not associated with high-level transmissibility, middle and lower
lung zones)
✓ Latent infection
✓ Reactivation disease: onset of active disease many years following a
period of latent infection (frequently cavitary and more often infectious
than primary disease, usually localized to the apical and posterior
segments of the upper lobes)
➢ In the great majority (90-95%) of persons infected with M. Tuberculosis, the
immune system either kills the bacilli or perhaps more often, keeps them
suppressed (silent focus) resulting in a latent TB infection (LTBI).
➢ In immunocompetent individuals, only 5-10% of infected persons develop active
disease in their lifetime.
➢ Individuals with latent TB infection do not have symptoms as there is no tissue
destruction by the bacilli and are not infectious.
➢ Active TB disease may arise from progression of the primary lesion after
infection, or from endogenous reactivation of latent foci, which remained
dormant since the initial infection, or from exogenous re-infection.
➢ The progression from LTBI to TB disease may occur at any time, from soon
to many years later.
➢ Post primary TB usually affects the lungs though any body part can be
affected after haematogenous and/or lymphatic spread of the bacilli.
➢ Persons who have Active TB are usually infectious
➢ Natural history of confirmed TB disease (without HIV) if left untreated
o 50% die in 5 year
o 25% cured
o 25 % chronically positive (infectious)

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CLINICAL MANIFESTATION

Presumptive Tuberculosis case;


Any person who presents with symptoms and/or signs suggestive of
tuberculosis, in particular cough of ≥ 2 weeks duration, which may
be accompanied by other respiratory symptoms (shortness of breath, chest
pains, and hemoptysis) and/or constitutional symptoms (loss of appetite, weight
loss, fever, night sweats, and fatigue).
Presumptive TB case also includes any person with CXR abnormality
suggestive of TB with or without other symptoms/signs suggestive of TB.

Case of tuberculosis:
Refers to a patient in whom TB has been bacteriologically Confirmed or
diagnosed by a clinician decision.

A bacteriologically confirmed TB case:


Refers to a patient from whom at least one biological specimen is positive
mycobacterium TB by either smear microscopy, Xpert MTB/RIF, culture or other
WHO approved bacteriologic detection tests.

A clinically diagnosed TB case:


A patient who does not fulfil the criteria for a bacteriological confirmed case
but, has been diagnosed with active TB by an experienced clinician and is
decided to be given, a full course of TB treatment.
This definition includes cases diagnosed on the basis of X-ray abnormalities or
suggestive histology and extra-pulmonary cases diagnosed without confirmation
of mycobacterium TB.

3.2 Extra Pulmonary TB

CLASSIFICATIONS → pulmonary, Extrapulmonary or both.

o Extrapulmonary TB may occur in 10-40% of patients.


o Patients may present with non-specific symptoms such as unintentional weight
loss, night sweats and fever for more than 2 weeks. Other symptoms depend
on the site or organ affected.
o Commonly involved sites are the lymph nodes, pleura, genitourinary tract,
bones and joints, meninges, peritoneum, and pericardium.
o Extra pulmonary TB is seen commonly due to HIV
 Up to 2/3rd of HIV infected patients with TB may have both pulmonary
and extrapulmonary or extrapulmonary TB alone.

✓ TB LYMPHADENITIS
The most common presentation of extra pulmonary TB
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Common in children and in person with advanced stages of HIV infection.


Cervical Lymph nodes is the commonest sites of involvement, though axillary
and intraabdominal lymph nodes may also be affected. Most commonly at
posterior cervical and supraclavicular sites.
Slowly developing painless swelling on the sides of the neck is the
commonest complaint.
Initially cervical lymph nodes are firm and discrete, and may later be matted
together and become fluctuant
The overlying skin may breakdown with the formation of abscesses and chronic
discharging sinuses /scrofula/, which heal with scarring.
In HIV infected patients, lymphadenopathies can be acute and resemble acute
pyogenic lymphadenitis.
50% of cases have pulmonary involvement, systemic symptoms are uncommon
except in HIV-infected patients.
DX → FNAC, Biopsy, AFB, Tissue culture (50%+ve)

Pictures; TB lymphadenitis with a draining sinus tract /scrofula/

2. Tuberculous pleural effusion

o TB is the commonest cause of a unilateral pleural effusion. It is also the


commonest form of HIV-related extra-pulmonary disease
o Most often present as non-productive cough of acute onset, chest pain, SOB
and Fever.
o Isolated pleural effusion usually reflects recent primary infection, and the
collection due to hypersensitivity response to mycobacterial antigens or
Contiguous parenchymal spread.
o The effusion may be small, remain unnoticed, and resolve spontaneously or
may be sufficiently large to cause symptoms such as fever, pleuritic chest
pain, and dyspnea.
o Physical findings are those of pleural effusion: dullness to percussion and
absence of breath sounds.
o DX;
➢ CXR- effusion, may show parenchymal lesion
➢ Thoracentesis- straw colored and at times hemorrhagic fluid, Exudative →
refer short case of Nitsbin (click here → Pleural fluid analysis) 299
➢ AFB smear, and cultures often negative
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➢ Pleural concentration of adenosine deaminase (ADA > 40 U/L) and IFN-γ


➢ Xpert MTB/RIF- 75% +ve
➢ Pleural Biopsy: granulomas and/or yields a positive culture in 80%.

3. Tuberculous empyema
It is a less common complication of pulmonary TB; from rupture of a cavity or
a bronchopleural fistula.
CXR shows hydro pneumothorax with an air-fluid level.
The pleural fluid is purulent and thick and contains large numbers of
lymphocytes.
Acid-fast smears and mycobacterial cultures are often positive.
Surgical drainage is usually required as an adjunct to chemotherapy.
Tuberculous empyema may result in severe pleural fibrosis and restrictive lung
disease.
Removal of the thickened visceral pleura (decortication) is occasionally
necessary to improve lung function.

4. TB of CNS

o TB meningitis and intracranial tuberculoma are the two most common forms.

4.1 TB MENINGITIS
~5% of extrapulmonary cases
Results from the hematogenous spread of primary or post primary pulmonary
TB or from the rupture of a subependymal tubercle into the subarachnoid
space.
TB Meningitis is mainly a disease of childhood and young adults in developing
countries.
Develops in adults, especially those infected with HIV.
It usually evolves over 2 to 6 weeks.
Clinical manifestation includes;
✓ Focal neurological deficits
✓ Features of raised ICP
✓ Signs of meningeal irritation
✓ Focal or generalized seizures and
✓ Cranial nerve palsies, the sixth nerve involvement being the most
common.
Presents subtly as headache and slight mental changes after a prodrome of
weeks of low-grade fever, malaise, anorexia, and irritability.
If not recognized, tuberculous meningitis may evolve acutely with severe
headache, confusion, lethargy, altered sensorium, and neck rigidity
Typically, the disease evolves over 1 - 2 weeks.
TB meningitis have 3 stages
i. Stage I: prodromal phase → non-specific symptoms (fever, headache,
confusion), no meningeal signs
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ii. Stage II: meningitis phase → typical disease with meningeal signs
iii. Stage III: comatose phase

Diagnosis

Lumbar puncture is the cornerstone of diagnosis


 Examination of CSF → refer short case of Nitsbin (click here → CSF
analysis)
 Repeated lumbar punctures increase the yield
 Culture of CSF is diagnostic in up to 80% of cases and remains the
gold standard
 Xpert MTB/RIF has a sensitivity of up to 80% and is the preferred
initial diagnostic option.

Imaging studies (CT and MRI) → hydrocephalus and abnormal enhancement of


basal cisterns or ependyma.
If unrecognized, tuberculous meningitis is uniformly fatal.
Neurologic sequelae are documented in 25% of treated cases, in most of
which the diagnosis has been delayed.

4.2 TUBERCULOMA
o Tuberculoma is an uncommon manifestation of CNS TB, presents as one or
more space-occupying lesions.
o Intracranial tuberculoma can be asymptomatic or produce headache, seizure or
some type of neurological impairment.
o On brain imaging, solitary tuberculoma (size: few mm to 3-4 cm) are
more frequent than multiple lesions.
CT or MRI reveals contrast-enhanced ring lesions, but biopsy is necessary to
establish the diagnosis.

5. GI TB
Mechanisms are involved: swallowing of sputum, hematogenous spread, or
(largely in developing areas) ingestion of raw milk from cows affected by
bovine TB
The terminal ileum and the cecum are the sites most commonly involved
Abdominal pain (at times similar to that associated with appendicitis) and
swelling, obstruction, hematochezia, and a palpable mass in the abdomen are
common findings at presentation.
Fever, weight loss, anorexia, and night sweats are also common.
Tuberculous peritonitis follows either the direct spread of tubercle bacilli from
ruptured lymph nodes and intraabdominal organs (e.g. genital TB in women) or
hematogenous seeding.
Nonspecific abdominal pain, fever, and ascites should raise the suspicion of
tuberculous peritonitis.
Tuberculous peritonitis- paracentesis reveals an exudative fluid with a high
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The yield of direct smear and culture is relatively low; culture of a large
volume of ascitic fluid can increase the yield, but peritoneal biopsy (with a
specimen best obtained by laparoscopy) is often needed to establish the
diagnosis.

6. TB of the Upper Airways


o Nearly always a complication of advanced cavitary pulmonary TB.
o TB of the upper air ways may involve the larynx, pharynx, and epiglottis.
o Symptoms include hoarseness, dysphonia, and dysphagia in addition to chronic
productive cough
o Acid-fast smear of the sputum is often positive
o Carcinoma of the larynx may have similar features but is usually painless.

7. Genitourinary TB
o Accounts for ~10–15%of all extrapulmonary cases.
o Involve any portion of the genitourinary tract.
o Local symptoms predominate
➢ Up to 75% of patients have chest radiographic abnormalities
➢ Urinary frequency, dysuria, nocturia, hematuria, and flank or Abdominal pain
are common presentations.
➢ Asymptomatic and their disease discovered only after severe destructive
lesions of the kidneys have developed.
➢ Urinalysis - in 90% of cases pyuria and hematuria.
Culture-negative pyuria (Sterile pyuria) in acidic urine should raise the
suspicion of TB
o CT, MRI show; deformities and obstructions, calcifications and ureteral stricture
o Culture -yields a definitive diagnosis in nearly 90% of cases.
o In female patients, it affects the fallopian tubes and the endometrium and may
cause infertility, pelvic pain, and menstrual abnormalities.
o Diagnosis requires biopsy or culture of specimens obtained by dilation and
curettage.
o In male patients, genital TB preferentially affects the epididymis, producing a
slightly tender mass that may drain externally through a fistulous tract; orchitis
and prostatitis may also develop.
o In almost half of cases of genitourinary TB, urinary tract disease is also
present.
o Genitourinary TB responds well to chemotherapy

8. SKELETAL TB
~10% of extrapulmonary cases
Reactivation of hematogenous foci or to spread from adjacent paravertebral
lymph nodes
TB can affect any bone but most commonly affects the vertebral column.
Weight-bearing joints (the spine in 40% of cases, the hips in 13%, and the
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Active tuberculosis (TB) disease can develop immediately or after decades of


latent infection.
In highly endemic regions, musculoskeletal TB usually manifests clinically in the
year following primary lung infection and therefore occurs most frequently in
relatively young patients.
Outside endemic areas, musculoskeletal TB is more commonly associated with
late reactivation of infection and occurs mainly in adults.
Two types of bone and joint involvement associated with TB infection have
been described:
o The caseous exudative type → characterized by bone destruction, local
swelling, abscess formation, sinus formation, and constitutional
symptoms; it occurs most often in children.
o The granular type → more insidious and less destructive than the
caseous exudative type, and abscess formation is less common; it
occurs most often in adults. However, host-parasite interactions in
tuberculosis are dynamic, often with mixed patterns and transitions along
a continuum.
Forms of skeletal tuberculosis (TB) include spondylitis (Pott’s disease), arthritis,
and osteomyelitis.

Tuberculous spondylitis (Pott’s disease)

o Most commonly affects the lower thoracic and upper lumbar region; disease
involving the cervical and upper thoracic region is less common.
o Infection generally begins with inflammation of the anterior aspect of the
intervertebral joints; typically, it spreads behind the anterior ligament to involve
the adjacent vertebral body. Once two adjacent vertebrae are involved,
infection enters the adjoining intervertebral disc space.
o This tends to occur later in Pott's disease than in bacterial vertebral
osteomyelitis and may have the radiographic appearance of relative disc
sparing.
o Eventually, the avascular disc tissue dies; there is vertebral narrowing and
subsequent vertebral collapse. Gibbus deformity, a form of structural kyphosis,
distorts spinal canal anatomy. The spinal cord is then at risk of compression,
resulting in paraplegia.

Picture; Gibbus deformity in an infant


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o Spread may occur into the soft paravertebral tissue to form a so-called “cold
abscess” (soft tissue mass). It’s formation of at the site is common.
o Noncontiguous spinal disease (eg, disease at more than one level) is
uncommon, although in one South African series it was described in 16 of 98
cases.
o The most common symptom is local pain, which increases in severity over
weeks to months, sometimes in association with muscle spasm and rigidity.
The muscle spasm can extend beyond the diseased area. In some cases, a
characteristic erect posture and "aldermanic" gait may be observed in which
the patient walks with short, deliberate steps to avoid jarring of the spine.
Constitutional symptoms such as fever and weight loss are present in less
than 40 percent of cases.
o The diagnosis of musculoskeletal TB is established by microscopy and culture
of infected material. Tissue may be obtained by needle aspiration and/or biopsy;
CT guidance is useful in regions where available.
o CT or MRI reveals the characteristic lesion
o The diagnosis of tuberculous arthritis can be established by synovial biopsy.
Synovial fluid may be examined, but findings are usually nonspecific; the white
cell count can be high or low, with preponderance of either neutrophils or
lymphocytes.
o Treatment of musculoskeletal tuberculosis consists of antimicrobial therapy. In
some cases, surgical intervention is also warranted.
o Surgical intervention is warranted for patients in the following circumstances:
✓ Patients with spinal disease and advanced neurological deficits
✓ Patients with spinal disease and worsening neurological deficits
progressing while on appropriate therapy
✓ Patients with spinal disease and kyphosis >40 degrees at the time of
presentation
✓ Patients with chest wall cold abscess

9. TB PERICARDITIS
o Tuberculous pericarditis occurs in approximately 1 to 2 % of patients with
pulmonary tuberculosis (TB).
o Develops frequently in HIV-infected patients
o Case fatality rates are as high as 40%
o Direct extension from adjacent mediastinal or hilar lymph nodes, hematogenous
spread.
o Four pathological stages of tuberculous pericarditis have been described:
✓ Fibrinous exudation with polymorphonuclear leukocytosis, abundant
mycobacteria, and early granuloma formation with loose organization of
macrophages and T cells
✓ Serosanguineous effusion with lymphocytic exudate and high protein
concentration; tubercle bacilli present in low concentrations
✓ Absorption of effusion with granulomatous caseation and pericardial
thickening with subsequent fibrosis
✓ Constrictive scarring; fibrosing visceral and parietal pericardium contracts
on the cardiac chambers and may become calcified, leading to
constrictive pericarditis, which impedes diastolic filling.
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Clinical features
o The onset may be subacute, although an acute presentation
o Dyspnea, fever, dull retrosternal pain, and a pericardial friction rub, is possible.
(Cough -94%, Dyspnea - 88%, Chest pain (often pleuritic) - 76%, Night sweats
- 56%, Orthopnea - 53%, Weight loss - 48%)
o An effusion eventually develops in many cases; cardiovascular symptoms and
signs of cardiac tamponade may ultimately appear.

Investigation
o Echo, CT, or MRI shows effusion and thickness across the pericardial space.
o Pericardiocentesis under echocardiographic guidance; exudative fluid, with a
high count of predominantly lymphocytes and monocytes; hemorrhagic effusion
is common.
o Direct smear examination is very rarely positive.
o Culture - +ve in up to 2/3rd of cases, pericardial biopsy has a higher yield.

Complications:
o Chronic constrictive pericarditis, tamponade calcification, which may be visible
on a chest radiograph.
o The approach to antituberculosis therapy for treatment of tuberculous
pericarditis is generally the same as that for pulmonary tuberculosis.

10. Miliary tuberculosis


The term miliary TB was originally a pathologic and then a radiographic
description; it is now used to denote all forms of progressive, widely
disseminated hematogenous TB.
The term also may be used more broadly (and incorrectly) by some to denote
involvement at multiple sites, whether or not disease presents with the classic
radiographic or pathologic nodular appearance characteristic of hematogenous
spread.
Miliary TB is a severe manifestation of tuberculosis.
Risk factors include;
o Extremes of ages (very young and elderly)
o Malnourished
o Altered cell mediated immunity such as HIV, CKD, and solid organ
transplant recipients.
The most frequently affected organs are liver, spleen, lung, lymph nodes,
meninges, bone marrow and the adrenal glands.
The clinical presentation ranges from severe acute forms involving septic
shock, multiple organ dysfunction syndrome and ARDS to a more frequent
subacute presentation with insidious symptoms such as trivial physical
examination.
Miliary TB can arise as a result of progressive primary infection or via
reactivation of a latent focus with subsequent spread via the bloodstream
Physical findings include;
o Hepatomegaly, splenomegaly, and lymphadenopathy.
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o Eye examination may reveal choroidal tubercles, which are


pathognomonic of miliary TB, in up to 30% of cases.
o Meningismus occurs in fewer than 10% of cases

Investigation and diagnosis

o Chest radiography → can show;


✓ Micronodular infiltrates (miliary pattern) in 2/3rd of patients that assist in
the diagnosis of miliary TB.
✓ No radiographic abnormality
✓ Large infiltrates, interstitial infiltrates
o Sputum-smear microscopy is negative in most cases.
o Anemia with leukopenia, lymphopenia, neutrophilic leukocytosis and Leukemoid
reactions, and polycythemia.
o Elevation of alkaline phosphatase
o Bronchoalveolar lavage and transbronchial biopsy are more likely to provide
bacteriologic confirmation, and granulomas are evident in liver or bone-marrow
biopsy specimens from many patients.

o If it goes unrecognized, miliary TB is lethal

NB; The term "miliary" was coined in 1700 by John Jacobus Manget, who likened
the appearance of the involved lung to millet seeds, with its surface covered with
small, firm white nodules. some authors use disseminated TB interchangeably with
miliary TB. however, miliary TB in fact refers more specifically to disseminated TB
which presents with a millet-seed-like appearance on a chest x ray, when the
disease is spead by blood throughout the lungs.

Picture; miliary TB

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3.3 RVI-TB Coinfection

☛ Refer under RVI section of Nitsbin (click here → RIV - TB coinfection)

3.4 Management of TB
Principles of TB Treatment

1. Chemotherapy → Anti TB drugs


2. Adjuvant therapy
o Include steroid therapy and pyridoxine
o Indication for steroid
▪ CNS TB (TB meningitis, tuberculoma)
▪ TB Pericarditis
▪ TB adrenalitis
▪ Miliary TB with acute air blocking syndrome
o Supplement with Pyridoxine (Vit B6), 25 to 50 mg, PO daily to prevent
peripheral neuropathy from Isoniazid side effect
3. Nutritional therapy
4. Family screening; should be done for
o Those under five children
o Pregnant ladies
o Elders, age >65 yrs
o All HIV /AIDS pts at home
5. Follow up

The aims of treatment of Tuberculosis are:

o To cure the patient from TB


o To prevent death from TB disease and its late effects
o To prevent relapse of TB
o To prevent the development of acquired drug resistance, and
o To decrease TB transmission

Pre-treatment Evaluation and preparation for treatment

o Before you put patients on anti-TB drugs, gather baseline information on: how
diagnosis of TB has been made, check for confirmatory Bacteriologic
information, determine the site of involvement, offer HIV test, assess risk for
drug resistance and co-morbid conditions like pregnancy, renal or liver disease
...

First line drugs;

Rifampicin(R) → The most bactericidal and potent sterilizing agent.


Isoniazid (H) → Highly bactericidal especially in the first few days
Pyrazinamide (Z) → Bacteriostatic and Only active in acidic environment and
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Ethambutol (E) - Bacteriostatic and effective to prevent drug resistance when


administered with other potent drugs.

In order to achieve the designed aim of treatment, anti-TB treatment regimen


should not only be designed considering effectiveness and safety of the drugs
but also the treatment needs to be administered;
o In appropriate combination of drugs
o In the correct dosage
o Regularly taken by the patient, and
o For a sufficient period of time.
Dose→ HRZE - 5,10,25,15 mg/kg for adults…. HRZE -10,15,35,20 mg/kg for
pediatrics. Children weighing ≥ 25kg can be treated using recommendation for
adults.

Table: First line TB treatment adult and pediatric dosing chart using body weight bands
Adult and pediatric ≥25 kg weight Pediatrics
Patient Regimen and dose in two phases Daily dose Regimen and dose in two phases
weight Intensive: 2(RHZE); Continuation: (mg/kg weight) Intensive: 2(RHZ) (E) Continuation: 4(RH)
band (kg) 4(RH);
RHZ; 75/50/150 E; 100 RH; 75/50 mg
RHZE RH; 150/75 mg mg
;150/75/400/275 mg
mg
20-29 1 ½ 1 ½ 4-7kg 1 1 1

30-39 2 2 8-11kg 2 2 2
40-54 3 3 12-15kg 3 3 3
≥55 4 4 16-24kg 4 4 4
25+kg Adult dosages recommended
Note: all TB patients on treatment need daily Pyridoxine 50mg tablet supplement.

Second line drugs; drugs (including injectable fluoroquinolones and


aminoglycosides) which are used for the treatment of Drug resistant TB

o Amikacin (Am)
o Capreomycin (Cm)
o Cycloserine (Cs)
o Ethionamide (Eto)
o Kanamycin (Km)
o Levofloxacin (Lfx)
o para-Aminosalicylic acid (PAS)
Streptomycin (S) → 1st line in some clinical conditions
o
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TB treatment is administered in two phases:

Intensive (initial) phase: aims to render the patient non-infectious by rapidly


reducing the bacillary load in the sputum and brings clinical improvement in
most patients receiving effective treatment.
Continuation phase: aims to sterilize the remaining semi-dormant bacilli and is
important to ensure cure/ completion of treatment and prevent relapse after
completion of treatment.

Dosing frequency and regimens of Anti TB drugs:

o Daily administration of all doses of the 6 months.


o All New TB patients are presumed to have drug-susceptible TB unless they
have developed active TB after known contact with a patient documented to
have drug-resistant TB.
o The preferred regimens (unless there is special consideration) are 2RHZE/4RH
o TB treatment should be implemented under DOT (directly observed treatment)
in Ethiopia considering the high TB/HIV and MDR-TB prevalence.
o For patients who have developed active TB after known contact with a patient
documented to have drug-resistant TB; treatment should be decided based on
rapid DST (Drug Susceptibility Test) result. While awaiting DST result, the
patient may be initiated treatment with the regimen based on the DST of the
presumed source case as they are likely to have a similar drug resistance
pattern.
o In all previously treated TB patients who require re-treatment, specimen for
rapid molecular-based DST for first line TB drugs should be obtained at or
before the start of treatment to inform the choice of appropriate treatment
regimen.
o While awaiting the DST result, the standard first line treatment regimen
2(RHZE)/4(RH) is recommended for previously treated TB patients
o Note that, re-treatment regimen for 08 months with addition of streptomycin
should no longer be prescribed for patients coming to receive treatment for
repeated TB episode.

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Diagram; explanation of terminologies in anti TB prescription

Treatment of Extra-pulmonary TB (EPTB)

o Extra-pulmonary tuberculosis (EPTB) is generally treated with the same


regimen as pulmonary tuberculosis.
o The guiding principles for patient registration, regimen designing, monitoring of
treatment and outcome definitions are similar to patients with pulmonary TB.
o Additional considerations in EPTB Treatment:
✓ Treat patient with extra-pulmonary TB involving any site for 6 months with
standardized first-line regimen with the exception of CNS TB (meningitis,
tuberculoma) and Osteoarticular TB (including vertebral bones, joint and
osteomyelitis), which require prolongation of the continuation phase for 10
months and for a total of 12 months: 2RHZE/10RH
✓ An initial adjuvant corticosteroid therapy with dexamethasone or
prednisolone tapered over 6-8weeks should be used for patients with
Tuberculosis meningitis and/or pericarditis to improve outcome and reduce
complications.
i. Adults and children >14 years should start treatment with
֎ Dexamethasone 0.4 mg/kg/day with a tapering course over 6 to 8
weeks.
ii. Children (<14 years) should be given
 Prednisolone 4mg/kg/day (or equivalent dose dexamethasone: 0.6
mg/kg/day) for 4 weeks, followed by a tapering course over 4 weeks.

Precautions during treatment with 1st line anti-TB medicines

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Treatment of patients with renal failure:


Consult expert.
If not possible to consult, then avoid Streptomycin & Ethambutol; therefore, the
recommended regimen is 2RHZ/4RH.

Treatment of patients with (previously known) liver disorder (e.g.


hepatitis, cirrhosis):
o Most anti-TB medicines can cause liver damage.
o Do not give Pyrazinamide because this is the most hepatotoxic anti-TB
medicine.
o Hence, for TB patients with liver disease, recommended regimens are:
2RHES/6RH or 9RHE.
o If the patient has severe liver damage (e.g. In the case of jaundice), the
treatment regimen should be changed to 2HES /10 EH.
o The dose of Rifampicin for these patients should not exceed 8mg/kg and
Isoniazid dose should not exceed 4 mg/kg.

Pericardial tuberculosis
For patients with pericardial tuberculosis, the same regimen (as pulmonary) of
anti-TB treatment is recommended (need expert opinion in diagnosis and
treatment).
Corticosteroids are recommended as adjunctive therapy for 11 weeks during
the first period of anti-tuberculosis therapy with tapering as shown in the table
below.

Table; Prednisone dose for adult TB patients with TB pericarditis


Weeks of Prednisolone dosage
treatment
1-4 60mg/day
5-8 30mg/day
9-10 15mg/day
11th week 5mg/day (then discontinue at end of 11th
week)

Tuberculous meningitis

o Patients presenting with more severe brain impairment such as drowsiness,


neurological signs, or coma have a greater risk of neurological sequelae and
higher mortality.
o Chemotherapy should be initiated with 2RHZS/7RH or 2RHZS/10RH
o Adjunctive corticosteroid therapy is recommended for all patients.
First line
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o Dexamethasone, 12 mg/day (8 mg/day for children < 25 kg) for 3


weeks and then decreased gradually during the subsequent 3 weeks.
Alternative
o Prednisolone, 60mg/day (2-4mg/kg/day for children), for 3 weeks, then
tapered off gradually over the following 3 weeks

Treatment during pregnancy and breast-feeding

o Avoid Streptomycin because of the risk of toxic effects on the fetus.


o Chemotherapy should not be discontinued during breast-feeding.
o When a breast-feeding mother has Pulmonary TB, the infant should, regardless
of prior vaccination with BCG, be given chemo-prophylaxis and then be
vaccinated with BCG if not previously vaccinated.

3.5 Baby of a mother with Active tuberculosis


If the mother has active lung tuberculosis (sputum smear positive TB) and was
treated for less than two months before birth or was diagnosed with
tuberculosis after birth:
o Reassure the mother that it is safe for her to breastfeed her baby;
o Do not give the tuberculosis vaccine (BCG) at birth
o Give prophylactic isoniazid 5 mg/kg, PO, daily

Follow up and management of baby of mother with active TB


At the age of 6 weeks, the baby should be re evaluated
o If there are any findings suggestive of active disease, start full anti TB
treatment according to national guidelines.
o If the baby is doing well and tests are negative, continue prophylactic
isoniazid to complete 6 months
Delay BCG vaccine until two weeks after treatment is completed.
If BCG was already given, repeat BCG 2 weeks after the end of the isoniazid
treatment.

Refer updated NICU guideline for more

Follow up and monitoring treatment responses of adult patients


During treatment follow-up, monitoring of patient’s progress involves:
o Clinical assessment (including signs and symptoms, weight
measurement)
o Follow-up AFB sputum examination, and
o Detection and treatment of adverse drug reaction

i. Clinical Monitoring of TB patients:

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✓ Health worker or a community TB treatment supporter must observe and


ensure each patient swallows every single dose of the medicines; this is
called directly observed treatment or DOT
✓ Persistence or reappearance of clinical feature of TB, including weight
monitoring
Weight is a useful indicator of clinical improvement especially in children and
should be monitored monthly.
✓ Treatment adherence by reviewing the “treatment supporter card” or UNIT
TB register Risk for developing acquired drug resistance, and need for
DST (Drug Susceptibility Test) screening, Occurrence of Adverse drug
reaction, and Development of TB complications.
✓ Unsatisfactory response to treatment beyond two months of treatment
should alarm the possibility of drug resistance or alternative diagnoses.

ii. Bacteriologic monitoring of bacteriologically confirmed pulmonary TB patients:

❖ Besides the clinical monitoring, bacteriologically confirmed pulmonary TB


patients (i.e. those diagnosed by identification of bacilli by smear
microscopy, culture or Xpert MTB/RIF assay) need their sputum to be
checked using AFB microscopy.
❖ Molecular technique like Xpert MTB/RIF assay cannot be used to monitor
treatment response as the technique may give false positive result as it
identifies dead bacilli.
❖ Follow-up sputum examination is done for all new smears +ve TB cases at
the 2nd, 5th and 6th month.
✓ If smear result is +ve at 2nd month, a repeat sputum smear
examination is done at the 3rd month and if it is still positive, the
sample must be sent for DST.
✓ If smear result is +ve at 5th month or later, it is declared that
treatment has failed and patient will be started on re-treatment
regimen and sputum is examined for DST.
✓ If smear is -ve at 5th and 6th month of follow-up, patient is declared
cured.
❖ Follow-up sputum examination is done for all previously treated smear
positive TB cases at 3rd, 5th and 8th month.
✓ If smear result is +ve at the 3rd month, sample must be sent for
DST.
✓ If smear result is +ve at the 5th month or later, it is declared that
treatment has failed and patient must be started on 2nd line
treatment regimen pending the DST result.
✓ If smear is -ve at 5th and 8th month of follow-up, patient is declared
cured.

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Figure: Sputum AFB Follow-up for Bacteriologically Confirmed PTB Patients

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Fig. Flow Chart for Sputum AFB Follow-up for bacteriologically confirmed
previously treated PTB Patients

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Table; Common side effects of Anti-TB drugs


Drug Side effects
o all are hepatotoxic but Pyrazinamide is most common
hepatotoxic anti TB drug
R/RMP/ o Body fluid discoloration
(Rifampicin) o Drug-Drug interaction with Nevirapine in RVI pt’s
o Hepatitis, Thrombocytopenia, fever
H /INH/ o Peripheral neuropathy → can be prevented by prescribing
(Isoniazid) INH together with Pyridoxine (Vit.B6)
o Hepatitis, hypersensitivity Reaction
Z (pyrazinamide) o Hepatitis, Hyperuricemia, Teratogenic
E (Ethambutol) Mnemonic → E for eye
o Reversible optic neuritis
o Color blindness (especially for red and green colors)
o Scotoma
o Hypersensitivity reaction, rash
S (Streptomycin) o Nephrotoxicity (all aminoglycosides are Nephrotoxic)
o Congenital deafness (CN VIII damage)

N.B

❖ Drug susceptibility testing (DST) on all TB isolates.


❖ HIV testing on all cases.
❖ Begin initial therapy before DST results are back.
❖ Never add a single drug to a failing regime
❖ Adherence to therapy is major issue--DOT for all.

Table: Management of New Pulmonary TB Treatment


Interruptersa

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3.6 Drug resistant TB


❖ TB is considered drug-resistant (DR) when the TB causative agent
(mycobacterium tuberculosis) is not killed by one or more of the available
anti-TB medicines.
❖ Medicine resistant TB can be primary or secondary (acquired).
✓ Primary resistance → it is medicine resistance among new cases; it
is resistance to one or more anti-TB medicines in a person who has
never been previously treated for TB.
✓ Secondary resistance → it is medicine resistance among previously
treated cases; in people diagnosed with TB who start anti-TB
treatment and subsequently acquire resistance to one or more of the
medicines used during the treatment.
❖ Both medicines susceptible and resistant MTB spread in the same manner.
❖ There are five different types of drug resistance: Cases are classified in
categories based on drug susceptibility testing (DST) of clinical isolates
confirmed to be M. tuberculosis:
✓ Rifampicin resistant TB: resistance to Rifampicin detected using
phenotypic or genotypic methods, with or without resistance to other
anti-TB drugs.
✓ Multidrug-resistance (MDR): Resistance to at least Isoniazid and
Rifampicin.
✓ Multidrug- or rifampicin-resistant TB (MDR/RR-TB): is the term used
to group MDR-TB and RRTB cases together as MDR/RR-TB; both
MDR-TB and RR-TB cases are eligible for treatment with MDRTB
regimens. MDR/RR-TB usually refers to all patients affected by either
MDR-TB or RR-TB.
✓ Isoniazid-resistant TB (Hr-TB): TB caused by Mycobacterium
tuberculosis strains resistant to isoniazid and susceptible to rifampicin
✓ Pre-XDR-TB: TB caused by Mycobacterium tuberculosis strains that
fulfil the definition of MDR/RRTB and that are also resistant to any
fluoroquinolone.
✓ Extensively drug-resistant TB (XDR-TB): TB caused by
Mycobacterium tuberculosis strains that fulfil the definition of
MDR/RR-TB and that are also resistant to any fluoroquinolone and
at least one additional Group A drug (Bedaquiline or Linezolid).
Since XDR-TB progresses from MDR-TB in two steps, the term “pre–XDR-TB”
was introduced to recognize MDR-TB with additional resistance to either one
but not both of these classes of medicines.
❖ The clinical features of drug susceptible and drug resistant TB are the
same
❖ Investigations
✓ Direct smear microscopy
✓ Line Probe Assay (LPA) directly from the sputum specimen or
cultured sample
✓ Culture and DST
✓ Gene Xpert MTB/RIF test
✓ CXR
✓ HIV test
✓ Other tests: CBC, U/A, FBS, LFT, RFT, Serum electrolyte, TSH,
HCG, Audiometric test
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❖ Definitive diagnosis of Drug-resistant TB depends on laboratory diagnosis


through Medicine Susceptibility testing (DST); it requires that M.tuberculosis
is isolated and drug susceptibility test is completed.

MDR - TB treatment in Ethiopia


o Duration of treatment
✓ Intensive phase → the injectable agents is used for a minimum of 8
months and at least 4 months after culture conversion
✓ Continuation phase →The total treatment is for a minimum of 18 months
beyond culture conversion
o Patients with laboratory confirmed Rifampicin-/Multi drug resistant TB (RR/MDR-
TB) require treatment with second-line TB regimens.
o MDR-TB Patients with strains resistant to at least rifampicin and Isoniazid are
treated with standardized second line treatment regimen for at least 18–21
months.

❖ If you suspect Drug resistant TB refer to a specialized hospital having TB


Treatment center
❖ Detailed management of Drug resistance TB is beyond the scope of this
text book. Readers are advised to read;

✓ Guidelines for Clinical and Programmatic Management of TB,


TB/HIV, DR-TB and Leprosy in Ethiopia, 7th edition, 2021
✓ National Programmatic management of Drug resistant TB in Ethiopia,
FMOH, December 2019 and
✓ Standard treatment guideline for general hospitals in Ethiopia, 4th
edition, 2021

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Chapter 4; Lung cancer (የሳንባ ካንሰር)

Chapter 4; Lung cancer (የሳንባ


ካንሰር)
Dr. Asmare.W

Epidemiology

o Incidence peaks 55 - 65 years


o leading cause of cancer-related death in North America and Europe, killing
over three times as many men as prostate cancer and nearly twice as many
women as breast cancer.
o Most preventable b/c 90 % associated with smoking
o Adenocarcinoma. highest (32%), squamous (28%) after 25 years age

Etiology and Risk factors

❖ A number of environmental and lifestyle factors have been associated with


the subsequent development of lung cancer, of which cigarette smoking is
the most important.
❖ Smoking
✓ The primary risk factor for the development of lung cancer is
cigarette smoking, which is estimated to account for approximately
90 % of all lung cancers.
✓ The risk of developing lung cancer for a current smoker of one pack
per day for 40 years is approximately 20 times that of someone who
has never smoked.
✓ Factors that increase the risk of developing lung cancer in smokers
include the extent of smoking and exposure to other carcinogenic
factors, such as asbestos.
✓ Carcinogens and tumor promoters in
a. Pack year=dose X length, (RR-13X,1.5X)
b. Sex - women more susceptible
c. Quitting/prevent starting
✓ Decreases with cessation of smoking but may never return to the
nonsmoker level.
❖ Genetic factors
✓ Genetic factors can affect both the risk for and prognosis from lung
cancer.
✓ Although the genetic basis of lung cancer is still being elucidated,
there is a clearly established familial risk (most patients have +ve
family hx of lung ca).
❖ Radiation therapy (RT)
✓ can increase the risk of a second primary lung cancer in patients
who have been treated for other malignancies.
❖ Environmental toxins
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✓ These include exposure to second-hand smoke, asbestos, radon,


metals (arsenic, chromium, and nickel), ionizing radiation, and
polycyclic aromatic hydrocarbons.
❖ Pulmonary fibrosis
✓ The risk for lung cancer is increased approximately sevenfold in
patients with pulmonary fibrosis. This increased risk appears to be
independent of smoking.
❖ HIV infection
✓ The incidence of lung cancer among individuals infected with HIV is
increased compared with that seen in uninfected controls.
❖ Alcohol
❖ Dietary factors
✓ various dietary factors (antioxidants, cruciferous vegetables, and
phytoestrogens) may reduce the risk of lung cancer, but the role of
these factors is not well established.
✓ As an example, the Alpha-Tocopherol, Beta-Carotene Cancer
Prevention Study actually showed an increase in lung cancer among
smokers with dietary supplementation of beta-carotene.

Pathology

❖ Lung ca arising from respiratory epithelium: bronchi, bronchiole, alveoli


❖ Predominant types include:
Non-small cell lung cancer (NSCLC)
o NSCLC is the most common form of lung cancer and is divided into the
following types:
▪ Squamous cell carcinoma (SCC)
▪ Adenocarcinoma
▪ Large cell carcinoma
▪ Carcinoid tumors
Small cell lung cancer (SCLC)
☛ Primary pulmonary lymphoma
o 88% primary lung ca are 4 cell types
▪ Squamous(epidermoid)ca
▪ Small cell ca (oat cell)
▪ Adenocarcinoma (Broncho alveolar)
▪ Large cell (anaplastic)ca
o 11% undifferentiated
▪ Carcinoids
▪ Gland tumors
Mesothelioma, lymphoma, sarcomas are not lung ca

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Table; Comparison b/n SCLC & NSCLC


Small cell lung ca NSCLC
Type Oat cell Squamous, adeno, large cell,
bronchoalveolar, mixed
Histology Scanty cytoplasm, Abundant cytoplasm
Small hyperchromatic nuclei, Pleomorphic nuclei
indistinct nucleoli, diffuse Coarse chromatin
sheet of cells Prominent nucleoli
Glandular/squamous
Molecular Neuroendocrine property Absent
Oncogenes/tumor RB mutation Different
suppressors
Metastasis at Early Localized
presentation
Treatment Chemo + radio Surgery + radio
response

1. Squamous Cell carcinoma (SCC)

Characterized by keratinization and/or intercellular bridges on histopathology.


SCC was the most frequent histologic type of lung tumor in nearly all studies
done prior to the mid-1980s.
Now, adenocarcinoma is more common than squamous cell carcinoma,
particularly in women
95% are smokers and males
Lower rate with metastatic disease
Associated with HPO (clubbing) and hypercalcemia
Two thirds of cases occur centrally, with involvement of the main stem, lobar,
or segmental bronchi.
It is more commonly associated with HPO (clubbing), cavitation, Pancoast
syndrome, and hypercalcemia.

2. Adenocarcinoma

o Adenocarcinoma is the most common type of lung cancer in contemporary


series, accounting for approximately one-half of lung cancer cases.
o The increased incidence of adenocarcinoma is thought to be due to the
introduction of low-tar filter cigarettes in the 1960s, although such causality is
unproven.
o It is the most common subtype in women and nonsmokers.
o Most tumors occur in the periphery.
o Subtypes: Bronchi alveolar carcinoma (BAC), now known as adenocarcinoma
in situ: Characterized by slow lepidic growth.

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3. Large Cell Carcinoma

Undifferentiated malignant epithelial tumors that lack features of small cell


carcinoma and glandular or squamous differentiation.
They are characterized by large nuclei, prominent nucleoli, and a moderate
amount of cytoplasm.

4. Carcinoid Tumor

o Pulmonary carcinoid tumors represent about 1 - 5% of all lung malignancies.


o They are mainly of two types, typical and atypical:
Typical carcinoid: < 2 mitoses per 10 high-power fields and absence of
necrosis.
Atypical carcinoid: > 2 mitoses per 10 high-power fields or presence of
necrosis.
o Usually occur in those who have never smoked.
o About 70% of carcinoids develop in the proximal airways and may be
associated with chronic cough, hemoptysis, and bronchial obstruction.
o Peripheral carcinoids are generally asymptomatic.
o Fewer than 2% of cases are associated with carcinoid syndrome(a combination
of symptoms and lesions mostly produced by the release of serotonin from
carcinoid tumors of the gastrointestinal tract that have metastasized to the
liver; consists of irregular mottled blushing, flat angiomas of the skin, acquired
tricuspid and pulmonary stenosis often with regurgitation, occasionally with
some minor involvement of valves on the left side of the heart, diarrhea,
bronchial spasm, mental aberration, and excretion of large quantities of 5-
hydroxyindoleacetic acid.)
o Treatment of carcinoid tumors is different from that of other types of NSCLC:
Typical carcinoid: Limited resection with segmentectomy and regional lymph
node dissection
Atypical carcinoid: Lobectomy and mediastinal lymph node dissection.
Metastasis: No known benefit to chemotherapy or radiation therapy. Local
treatment of metastases may lead to prolonged remission.

SMALL CELL LUNG CANCER (SCLC)

o SCLC is characterized by proliferation of small cells with scant cytoplasm, ill-


defined borders, salt and pepper chromatin, frequent nuclear molding, and a
high mitotic count.
o Up to 98% of patients with SCLC have a history of smoking.
o The natural history of SCLC is early metastasis and death. Vast majority
present with metastatic disease (early)
o Unlike NSCLC, SCLC is always considered a systemic disease at diagnosis.
o Liver, bone, bone marrow, and the central nervous system are the most
commonly affected extrapulmonary organs.
o Usually centrally located.
o Paraneoplastic syndromes related common
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o SCLC shows an excellent response to chemotherapy, but almost always recurs.


o Median survival for disease confined to the chest is 4 - 6 months without
treatment.
o For metastatic disease, median survival is 5 - 9 weeks without treatment.

Summary on pathology
o Adenocarcinoma + nonsmoker → consider another primary site
o Central mass and endobronchial smx → squamous/small cell ca
o Peripheral nodule/mass with pleural → adenocarcinoma/large cell ca
o Squamous and large cell → cavitate 10-20%
o Bronchoalveolar ca → from peripheral airways-radiologically single mass,
diffuse, multinodular, fluffy infiltrates

Clinical manifestations

o Local sign and symptoms


➢ Asymptomatic 5-15% routine CXR
➢ Cough, hemoptysis, wheezing, stridor, dyspnea, post obstructive pneumonitis
(fever) → central / endobronchial primary tumor
➢ Pain-pleursy, chest wall +/-cough, dyspnea → peripheral growth primary tumo
➢ features of lung abscess → (cavitation’s/obstruction)

o Invasion or obstruction of adjacent structures


➢ Tracheal obstruction
➢ Esophageal compression/dysphagia
➢ Hoarseness→ recurrent laryngeal nerve paralysis
➢ Increased hemidiaphragm/dyspnea→ phrenic nerve paralysis
➢ Horner’s syndrome (sympathetic n. paralysis, enophthalmos, ptosis, miosis,
anhidrosis)
o Growth in regional lymph nodes
o Distant metastasis (Hematogeneous)
➢ At autopsy >95% of SCLC, 80% adenocarcinoma and large cell,50%
squamous metastasis.
➢ To any organ;
Brain→ neurologic deficit (ICSOL)
Bone→ pain/pathologic fracture
Bone marrow→ cytopenia
Liver→ liver dysfunction, obstructive, pain
Lymph node→ supraclavicular/axilla/groin
Spinal cord→ compression syndrome, epidural, bone fracture
Adrenal gland → Adrenal insufficiency rare but high rate of metastasis (40%).
o Paraneoplastic syndromes. 5-10%
Common/may be presenting smx
May mimic metastasis-inappropriate palliation therapy
Relieved by successful treatment of tumor
Systemic disease-anorexia, wt loss, cachexia, fever
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Endocrine syndrome: hypercalcemia, hyponatremia (SIADH), hypokalemia


(increased ACTH), Cushing’s syndrome
Skeletal / connective tissue SXX: clubbing/ HPOA (hypertrophic pulmonary
osteoarthropathy)
Neurologic /myopathic syndromes → Myasthenia, peripheral neuropathy,
cortical/cerebellar degeneration

Staging

o Determine patient’s prognosis and type of treatment.


o Staging differ for SCLC and NSCLC.

✓ Staging of NSCLC (TNM staging)

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✓ Staging for SCLC

Simple two-stage system


Limited-stage disease (30%SCLC)
o disease confined to one hemithorax and regional lymph node (including
mediastinal, contralateral hilar, and usually ipsilateral supraclavicular
nodes)
Extensive-stage disease (70%)
o disease exceeding those boundaries cardiac tamponade, malignant
pleural effusion, and bilateral pulmonary parenchymal

Diagnosis

Goals — The major goals of the initial evaluation of a patient with suspected
lung cancer are to assess the following:
o Clinical extent and stage of disease
o Optimal target site and modality for the first tissue biopsy
o Specific histological subtype
o Presence of comorbidities, secondary complications, and paraneoplastic
syndromes that influence treatment options and outcome
o Patient values and preferences that influence diagnostic and therapeutic
choice
The preferred approach uses imaging as a road map and invasive biopsy as a
tool to confirm both the histopathological diagnosis and the stage of disease.
When feasible, diagnosis and staging should be established concurrently by
targeting for invasive biopsy the abnormality that would yield the most
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advanced stage. However, some patients will require multiple imaging


studies and/or invasive procedures for tissue sampling.
No single diagnostic algorithm sufficiently addresses the complexity and
variation in disease patterns of lung cancer.

Clinical suspicion;
o The majority of patients who present with clinical signs or symptoms
due to lung cancer have advanced disease.
o The most common presenting manifestations are the following:
▪ Cough (50 to 75%)
▪ Hemoptysis (25 to 50%)
▪ Dyspnea (25 %)
▪ Chest pain (20 %)
o Lung cancer should always be suspected in a current or former smoker
with new onset of cough or hemoptysis.
o Both non-small cell lung cancer (NSCLC) and small cell lung cancer
(SCLC) can present with similar symptoms, and few clinical features
reliably distinguish them from each other.
o Features that suggest SCLC include rapidly progressive symptoms and
the presence of paraneoplastic syndromes (eg, syndrome of
inappropriate antidiuretic hormone), bulky multi-station mediastinal
metastasis, superior vena cava syndrome, and bone and brain
metastases.
o In contrast, Pancoast's syndrome and hypercalcemia are more frequently
encountered in patients with NSCLC.
CXR → demonstrating the following
o new or enlarging focal lesion
o pleural effusion
o pleural nodularity
o enlarged hilar or paratracheal nodes
o endobronchial lesion
o post-obstructive pneumonia or segmental or lobar atelectasis.
CT scan of the chest
o Every patient with suspected lung cancer should undergo CT scan of
the chest.
o IV contrast enhancement is preferable as it may distinguish mediastinal
invasion of the primary tumor or metastatic lymph nodes from vascular
structures.
o Images of the liver and adrenal glands should also be included.
o In most patients, CT scan assesses;
▪ the anatomic location and size of the tumor (T)
▪ nodal (N), and
▪ metastatic disease of the pleura, liver, and adrenal glands (M).
o CT findings suggestive of malignancy in a patient with a solitary
pulmonary nodule include
▪ large lesion size (eg, >15 mm)
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▪ upper lobe location


▪ thick-walled cavitation
▪ presence or development of a solid component within a ground
glass lesion, and
▪ detection of growth by follow-up imaging.
o The finding of multiple nodules in a patient with a known or suspected
extra thoracic malignancy strongly suggests pulmonary metastasis.

Whole body PET (positron emission tomography) scan.


Imaging metastatic disease → Indications include;
o Patients with focal symptoms, signs, or laboratory tests suggestive of
metastatic disease. The modality used depends on the site of suspected
metastases
o Patients with clinical stage III or IV disease have an increased risk of
occult intracranial metastasis and may benefit from routine imaging of
the brain with magnetic resonance imaging (MRI) or CT if MRI is not
available. The rationale for routine brain imaging is the high risk of
distant disease in this population, especially metastases to the brain. In
this setting, an MRI of the brain may be performed for the early
detection of brain metastases so that early treatment can be
administered before development of neurologic deficits or seizures
o In patients with clinical stage I/II disease who are candidates for curative
resection, there is consensus that routine brain imaging with MRI
is not indicated.
lab investigations; perform the following laboratory studies when chest imaging
is suspicious for lung cancer:
o CBC
o Electrolytes
o Liver enzymes
o LFT
o RFT
pathology;
o A diagnosis of lung cancer should not be made without definitive
pathology.
o At a minimum, this involves selecting a biopsy site and obtaining an
adequate sample for microscopic examination.
o Cytologic specimens can be obtained from the following sites;
▪ Lung → Sputum, transthoracic needle aspirates, and bronchoscopic
washings, brushings, or needle aspirates
▪ Lymph node → Transthoracic, transbronchial, and transesophageal
aspirates
▪ Distant metastasis → Pleural fluid, needle aspirates of metastatic
tissue.
o Core or biopsy tissue can be obtained from the following:
▪ Lung → Endobronchial biopsy (forceps), transbronchial biopsy
(forceps or needle), transthoracic (needle) biopsy, surgical biopsy
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▪ Lymph node → Bronchoscopic and transthoracic needle core


biopsy, surgical biopsy.
▪ Distant metastasis – Core needle aspirates of metastatic tissue
(eg liver, bone, adrenal).

Management of Lung ca

1. NSCLC

Stage I and II:


o Surgery is first-line treatment.
o Adjuvant chemotherapy may be useful in selected cases of stage IB
disease, especially if the tumor is > 4 cm.
Stage II disease
o surgery followed by adjuvant chemotherapy.
Stage IIIA:
o Most cases are unresectable.
o Chemotherapy and/or radiation therapy may be used.
Stage IIIB:
o Combined chemotherapy and radiation therapy is used.
Stage IV:
o Chemotherapy. Radiation therapy for palliation only.
Special considerations
o Superior sulcus tumor with Pancoast syndrome:
▪ It is a constellation of symptoms and signs that include shoulder
and arm pain along the distribution of the C8, T1, and T2;
Horner’s syndrome; and weakness and atrophy of the hand.
▪ It is seen in one third of patients with superior sulcus tumors.
o Superior vena cava syndrome:
▪ is usually the result of direct obstruction of the superior vena cava
by malignancies.
▪ Bronchogenic carcinoma is the most common cause.

2. SCLC;
Chemotherapy;
o LIMITED DISEASE
▪ response rate of 70 - 80% to chemotherapy and thoracic radiation
therapy, with a complete clinical response rate of 50–60%.
o EXTENSIVE DISEASE
▪ response rate of 60–80% to chemotherapy, with only 20% of
patients achieving complete clinical remission.
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Chapter 4; Lung cancer (የሳንባ ካንሰር)

PROGNOSTIC FACTORS
Strongest predictors of survival:
o Good performance status (Karnofsky scale)
o Lesser extent of disease
o Younger age
o Absence of weight loss
Other predictors of better survival:
o Smoking cessation
o Standard uptake value of the primary tumor on positron emission
tomography (PET) scan.
Histologic subtype not considered a predictor of survival.

BENIGN LUNG NEOPLASM


Most present as asymptomatic solitary pulmonary nodules, incidentally
discovered radiographically.
About 50% of benign lung neoplasms are hamartomas.
Broadly divided into epithelial and nonepithelial tumors.
EPITHELIAL NEOPLASMS
o Types include: Papilloma; Micro nodular pneumocyte hyperplasia,
o Papilloma’s
▪ SQUAMOUS PAPILLOMA, most often associated with cigarette
smoking and human papilloma virus. Most occur in central large
airways.
NONEPITHELIAL NEOPLASMS
o Types include: Solitary fibrous tumors, Hamartomas
o Hamartomas
▪ Most common benign lung neoplasm in adults
▪ More common in men
▪ Generally discovered incidentally in the sixth or seventh decade
▪ Parenchymal or endobronchial (10%) nodules with characteristic
popcorn calcification.
▪ Can present as solitary pulmonary nodules.

Management of benign lung tumors


Most benign lung tumors don’t require management.
It requires only yearly follow up with imaging.

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Chapter 5; RVI (ኤችአይቪ ኤዲስ)


Dr. Mulualem. G

Clinical features and how to write hx of RVI patient


History

Pt’s may present with common OI syndromes like TB, Anaemia, cryptococcal
meningitis, esophagial candidiasis etc.
If a known RVI patient → ask the following on your hx
o For how long he/she was Diagnosed to have RVI in his/her blood
▪ E.g a known RVI pt for the past 10 years or you can say 10
years back he/she was told to have RVI (you have to ask
what was the presentation at that time and how Dx was
made… you may not need to write on your HPI)
o What is the regimen he/she is taking and for how long s/he was on
HAART?
▪ If there is gap between RVI Dx and initiation of regimen ask
the reason for delay of initiation of ART
o What was the baseline and current CD4 count and viral load?
▪ E.g. a known RVI pt for the past 10 years on TDF + 3TC+
DTG/EFV with baseline and current CD4 count of 250 and
500 cells/mm3 respectively. and current viral load of 50
copies/ml
o If regimen was changed in between ask the reason of shifting to
other regimens (drug side effect, treatment failure...)
o Adherent or not
o Where was the follow up and frequency of follow up
Clinical features are Variable depending on the degree of immunodeficiency
(clinical stage of disease).
The first few weeks after initial infection, individuals may be asymptomatic or
an influenza-like illness including fever, headache, rash or sore throat.
Acute HIV syndrome → 50 - 70% of persons with HIV infection experience an
acute clinical syndrome approximately 3 - 6 weeks after primary infection.
Usually persists for 1 to several weeks
General symptoms → Fever, Pharyngitis, Lymphadenopathy (70% of cases),
Headache/retro-orbital pain, Arthralgias/myalgia, Lethargy/malaise/,
Anorexia/Weight loss/Nausea/Vomiting/Diarrhea
At advanced immunodeficiency, patients are at a very high risk of being
infected with OI. So, write hx of opportunistic infection….
For this section let us see hx of oesophageal candidiasis. (for Cryptococcal
meningitis & TB, look at under respective topic in long cases of Nitsibin)

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Chapter 5; RVI (ኤችአይቪ ኤዲስ)

Oesophageal candidiasis hx
➢ Odynophagia or dysphagia
Scraping type of retrosternal pain during swallowing solid foods
and/or fluid diet
Relieving and aggravating factors
Radiation
➢ Loss of appetite
➢ Nausea, Vomiting (characterize vomiting)
Non bilious/bilious
Non projectile/ projectile
Non blood tingled/ blood mixed
Non foul smelling / foul smelling
Vomiting of ingested matter
Frequency of vomiting (x-y days per day)
➢ Hematemesis and/or melena
➢ Diarrhoea (characterize diarrhoea)
Large volume
Watery
Associated abdominal pain
➢ Easy fatigability
➢ Fever (characterize fever)
o Low/ high grade
o Intermittent/ continuous
o Associated with chilis rigor or not

Risk factors For RVI exposure

➢ MSP
➢ Blood transfusion
➢ IV drug abuse (sharing of needle)
➢ Sharing of needle, blade and other sharp materials
➢ Occupation → prostitute
➢ MTCT (mother to child transmission)

Complication

➢ OI
✓ TB → Pulmonary/extra pulmonary TB
✓ PCP
✓ Cryptococcal meningitis
Toxoplasmosis

➢ Every
➢ IRIS
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Chapter 5; RVI (ኤችአይቪ ኤዲስ)

Sample history

Sample hx of a patient with the dx of Stage IV RVI + Disseminated TB to the


lung and pleura + anemia of chronic illness

Chief compliant

Cough of one-month duration.

HPI

This is a known RVI patient for the past 04 years initially on TDF + 3TC + EFV for
03 years later the regimen changed to TDF + 3TC+ DTG when DTG was introduced
to the market, with unknown baseline CD4 count and current CD4 count of 50
cells/mm3 with current viral load of 150 copies/ml. He discontinued his follow up from
UOG hospital and his medications 07 months back, because of the current pandemic
(covid -19), financial and transport problem, since he lives in very remote area from
gondar town.

Currently presented with cough of a month duration which is non position dependent
productive cough with Mucoid, non-position dependent, Non blood tingled, non-foul-
smelling sputum of 2 - 3 Arabic coffee cup per day that increase in frequency and
amount progressively. Associated with this he also experienced low grade intermittent
fever, Night sweet and significant weight loss from 61 kg to 53 kg which is 13% of
his initial body weight.

Two weeks before admission, he also developed a gradual onset of dyspnea while
doing ordinary activities like going to church which progressively increase in severity
and he began to experience shortness of breath at rest within 01 week duration
associated with Sudden, sharp, stabbing and localized Chest pain which is aggravated
by deep breathing, coughing, sneezing, laughing and relieved by lying down on right
lateral decubitus position.

➢ He has blurring of vision, easy fatigability and light headedness but


no Tinnitus or vertigo (anaemia in RVI from AZT toxicity, OI/B19, TB/, opportunistic
malignancy with bone marrow suppression like lymphoma, anaemia of chronic illness and RVI by itself)
➢ No hx of contact with a known TB patient or previous TB treatment
(RVI-TB association is very cmn OI)
➢ There is no swelling over the neck, axilla or groin area (PGL/Persistent
generalized LAP/, lymphoma especially NHL)
➢ He has dyspnoea but no orthopnoea, PND or palpitation (HIV
cardiomyopathy, constrictive pericarditis)
➢ No hx of Flank pain, dysuria, haematuria, frequency or urgency (TDF
toxicity, HIVAN/HIV associated nephropathy/)
➢ No hx of rash over the body, skin ulceration, joint pain, muscle pain
or itching sensation (skin rash of RVI /PPE, VZV…/)
➢ No hx of Eye pain or discharge (uveitis, retinitis)
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Chapter 5; RVI (ኤችአይቪ ኤዲስ)

➢ No hx of Diarrhoea, abdominal pain, weight loss or fever (unexplained


chronic Diarrhoea > 1 month, weight loss and fever are stage III features of RVI)
➢ No hx of headache, forgetfulness, visual disturbance, sleep
disturbance, or Abnormal body movement (ADC/AIDS dementia complex/, CNS
toxoplasmosis, primary CNS lymphoma, HIV encephalopathy, aseptic meningitis, PMLE/progressive
multifocal leukoencephalopathy/)
➢ No hx of smoking or chronic alcohol intake (increased risk for respiratory disease
like PCP)
➢ No self or family hx of DM, HTN or Asthma

Finally, he was admitted to our hospital walking by himself

Physical examination (pertinent findings)

1 GA → CSL

2 Vital signs

➢ OHT (orthostatic hypotension) from autonomic dysregulation


➢ Tachycardia, febrile
➢ emaciated

3 HEENT

➢ Whitish plaque on tongue, buccal mucosa or Vertical folds on lateral lingual


margin → OHL (Oral hairy leucoplakia), oropharyngeal candidiasis
N.B
OHL Oropharyngeal candidiasis
➢ Can’t be scraped by scapula ➢ Can be scraped by scapula
➢ Vertical folds on lateral ➢ Flat, painless, white cheesy
lingual margin plaques on the medial
➢ Caused by EBV tongue surface
➢ Caused by C. albicans

Pictures; left) Pseudomembranous thrush, right) Atrophic thrush

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Chapter 5; RVI (ኤችአይቪ ኤዲስ)

Picture; Oral hairy leucoplakia

➢ KS (Kaposi sarcoma in oral cavity)


Pictures; KS in Eye, oral mucosa and skin over the hands

➢ Aphthous ulcer

Picture; Aphthous stomatitis/ aphthous ulcer

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Chapter 5; RVI (ኤችአይቪ ኤዲስ)

➢ Necrotizing Gingivitis

Picture; Necrotizing Gingivitis

➢ Periorbital edema due to HIVAN (HIV associated nephropathy)


➢ Eye discharge → uveitis, retinitis from CMV infection
➢ Retinal cotton wool spot on fundoscopy
➢ Herpes labialis
o Shallow, clustered ulcers (Usually painful) around oral and peri oral
area are characteristic
o May be solitary and deep in the severely immunocompromised
patient

Image; herpes labialis


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Chapter 5; RVI (ኤችአይቪ ኤዲስ)

➢ Seborrheic dermatitis; Itchy scaly skin condition, especially affecting scalp,


face, upper trunk (also common in non-HIV)

Picture; Seborrheic dermatitis

4 LGS

➢ PGL (persistent generalized lymphadenopathy)


➢ LAP from hematologic manifestation of HIV (thrombocytopenia)

5.RS

➢ Consolidation → pneumonia (PCP, S. pneumonia, K. pneumonia)


➢ Pleural effusion → Disseminated TB to pleura, NHL (primary effusive
lymphoma), Pneumonia with parapneumonic effusion

6. CVS
➢ CHF 2ry to DCMP (ZDV, RVI by itself)
7. Abdominal examination
➢ HSM (hepatosplenomegaly) → hematologic malignancy like NHL, ARS
(acute retroviral sxx) Phase of RVI
8. GUS
➢ Genital ulcer (genital herpes)

Picture; Chronic extensive genital HSV

➢ Renal failure → HIVAN


➢ Hypogonadism
9. MSS
➢ Leg edema → HIV cardiomyopathy resulting CHF, renal failure due to
HIVAN

10. IS

➢ Varicella (Chicken pox) rash 336


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Chapter 5; RVI (ኤችአይቪ ኤዲስ)

➢ Herpes zoster(shingles) rash


o Painful vesicular rash in a dermatomal distribution of a nerve
supply that does not cross the midline.
o Most common areas: trunk, particularly the flanks, and forehead.
Can involve the eye and cause corneal scarring and blindness.
o The rash is generally limited to one dermatome, but can
occasionally affect two or three neighboring dermatomes.
o Some patients can also have a few scattered vesicles located at
some distance away from the involved dermatome.
o Pain sometimes comes before the appearance of the rash.
o Vesicles form in groups and progress to crusted lesions after a
few days.

Pictures; herpes zoster infection which follows dermatomes over the chest

Picture;left) Herpes zoster over the left posterior chest. Right) left lateral side of the
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Chapter 5; RVI (ኤችአይቪ ኤዲስ)

➢ Mucocutaneous ulcer
➢ Erythematous maculopapular rash of PPE (Pruritic papular eruption)
o Intensely pruritic, discrete, firm papules with variable stages of
development and predilection for extremities, though it can
involve trunk and face.
o Excoriation results in pigmentation, scarring and nodules

Picture; PPE, Always exlcude scabies, insect bites

Look at cutaneous OI section at discussion part below for more about


varicella, zoster and PPE (click here → Cutaneous disorders related to
RVI infection)

11. NS

➢ GCS & MMSE


Altered mentation 2ry to ADC
➢ CN → CN palsy like visual disturbance
C. meningitis
Rarely toxoplasmosis
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Chapter 5; RVI (ኤችአይቪ ኤዲስ)

➢ Motor
FND (e.g. hemiplegia) → space occupying lesions like primary
CNS lymphoma
Multiple lesions from CNS toxo, tuberculoma
➢ Sensory
TM (Transverse myelitis with distinct sensory level)
Paresthesia
➢ Coordination, gait and drift
Impaired rapid alternation movement
Ataxia
Seizure→ encephalopathy, CNS toxoplasmosis, C. Meningitis and
other etiologies of meningitis, primary CNS lymphoma, PMLE
➢ Meningeal irritation sign +ve in
C. meningitis
Aseptic meningitis
Syphilitic meningitis
Lymphomatous meningitis
HIV meningoencephalopathy
PMLE (progressive multifocal leukoencephalopathy)

DDX

RVI - TB DDX for pulmonary effusion

1) Pneumonia with parapneumonic effusion


✓ If infected it will form empyema
2) Primary effusive lymphoma
✓ a.k.a body cavity lymphoma
✓ Caused by KSV, EBV
3) Kaposi sarcoma of respiratory tract
Manifest with fever, cough, hemoptysis, SOB, chest pain
4) Bronchiectasis
Cough and mucopurulent, tenacious, position dependent, massive
sputum last for months to years, hemoptysis
Crepitation and rhonchi
2ry to
o Acquired → TB (common in our setup), pneumonia,
obstruction of the bronchial tree
o Congenital → Cystic Fibrosis (common in westerns)
5) Fungal infections
✓ Disseminated candidiasis to the respiratory tract
✓ Cryptococcus
✓ Histoplasmosis 339
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Chapter 5; RVI (ኤችአይቪ ኤዲስ)

✓ Aspergilloma
6) Bronchogenic ca → Family hx, Smoking hx, Bloody sputum (Hemoptysis)
7) Lung Abscess
✓ Offensive foul-smelling sputum which is copious in amount
✓ Fever
✓ If rupture → Bronchopleural fistula → effusion

RVI - esophageal candidiasis DDX

1) Esophageal candidiasis
AIDS Defining disease
Occur when CD4 count is < 200
N.B. AIDS defining Diseases include
▪ Kaposi Sarcoma
▪ Cervical ca
▪ OHL
▪ Cerebral toxo
▪ Esophageal ca
▪ ADC
2) Infectious esophagitis
CMV → Fever, odynophagia, substernal chest pain, nausea
HSV → odynophagia and/or dysphagia, fever, retrosternal chest pain,
coexisting herpes labialis
3) Drug induced esophagitis
Characterized by severe dysphagia to the extent difficulty of
swallowing saliva
4) Lymphoma to esophagus
Lymphoma
MALToma
5) Esophageal ca
6) Esophageal stricture

IX

General Ix for all RVI pt


1. CD4 and Viral load
Normal CD4 count = 700 - 1200 cells/µl
Viral Load target with HAART = Less than 50 copies/mm3
Diagnosis of RVI include
o Direct detection of the virus
▪ Viral load → commonly done in our set up
▪ P24 antigen
o Antibody detection
▪ Rapid Antibody test → commonly done in our set up
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o Currently One step → 1st Response → unigold


(previously it was KHB → stat pack → unigold
Then Updated to Stat pack → Abon → SD bioline)

▪ ELISA
▪ Western blot
2. CBC→ Megaloblastic anemia from AZT toxicity, pancytopenia
3. RBS
4. U/A → proteinuria in HIVAN
5. CXR
r/o TB, pneumonia
PCP → perihilar infiltrate, ground glass appearance
6. Sputum examination (gene x-pert for TB screening)
Gram stain from BAL, induced sputum, Transbronchial biopsy→ definitive
dx for PCP
AFB
Culture
Gene x-pert
PCR
7. RFT → for drug toxicity, HIVAN
8. LFT → for drug toxicity
9. Lipid profile (Triglyceride, Cholestrol, HDL and LDL)
10. Hepatitis screening → before initiation of ART since HBV also treated with
TDF
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RVI TB Ix → the above baseline IX plus

11. CXR
TB features on CXR
o Early typical adult features
☛ Upper lobe infiltration/cavitation
☛ No significant LAP/ pleural effusion
✓ Late atypical features
o Lower/middle lobe opacity
o Little/no cavitation
o Miliary/interstitial pattern
o Hilar/paratracheal LAP
o Pleural/pericardial effusion
o May be normal finding
12. Pleural fluid analysis → refer under short cases of Nitsbin (click here →
Pleural fluid analysis)
13. Chest U/S → can differentiate
✓ Loculated effusion from tumor
✓ Pleural effusion from pleural thickening
14. Chest CT → also differentiate pleural effusion from pleural thickening
15. Culture → gold standard Ix in RVI-TB
16. RFT and LFT for Anti TB toxicity

N.B
If you suspect esophageal candidiasis in RVI patient there is no
specific investigation modality. Rather, treat with systemic
antifungals and if odynophagia improves within 3-4 days, the
cause of odynophagia is highly likely esophageal candidiasis

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Other Ix based on indication


17. Brain CT and MRI → can show us ring enhancing lesion in CNS
toxoplasmosis
18. Abdominal U/S → CKD from HIVAN

Laboratory monitoring for toxicity of ART


❖ Baseline
✓ CBC
✓ Liver enzymes
✓ RFT
✓ RBS
✓ Pregnancy test
✓ Lipid profile

❖ Follow up
✓ Baseline Ix Repeated monthly (particularly at the initiation of ART)
then every 3 months once stabilized. Then at any time if indicated

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Discussion

5.1. HIV/AIDS
➢ HIV (Human Immuno-deficiency Virus) is an infectious disease caused by HIV,
a human retrovirus
➢ It is essentially a disease of the immune system, which results in progressive
immunodeficiency state leaving the individual susceptible to various types of
infections and the development of malignancies.
➢ HIV disease should be viewed as a spectrum ranging from primary infection,
with or without the acute syndrome, to an asymptomatic stage, to advanced
disease characterized by profound immunodeficiency and susceptibility to
opportunistic infections (OI).
➢ The most advanced stage of HIV infection is called AIDS
➢ AIDS (Acquired Immunodeficiency Syndrome) is the late /most advanced/ stage
of HIV infection
➢ Current case definition for AIDS;
✓ Any HIV-infected person with a CD4+ T-cell count <200/μl
✓ Development of an AIDS-defining clinical condition (see staging below)

Etiology
➢ Human retroviruses; HIV-1 and HIV-2
✓ Family of human retroviruses (Retroviridae), Subfamily of lentiviruses
✓ RNA viruses whose hallmark is the reverse transcription of its genomic
RNA to DNA by the enzyme reverse transcriptase
➢ HIV-1 is the most common cause of AIDS worldwide.
➢ HIV-2 has been identified predominantly in western Africa but Small numbers
of cases have also been reported in Europe, South America, Canada, and the
U.S. Has ~40% sequence homology with HIV-1 and More closely related to
simian immunodeficiency viruses

Transmission
❖ Sexual contact (unsafe): heterosexual and homosexual. It is major
means of transmission.
❖ Contact with blood, blood products, or other bodily fluids (as in drug
abusers who share contaminated intravenous needles)
o Potentially infectious fluids
▪ Blood, Seminal fluid, Vaginal secretion
▪ Body fluids: CSF, synovial fluid, pleural fluid, peritoneal
fluid, pericardial fluid, and amniotic fluid.
▪ Breast milk
▪ Pus

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o BUT, Saliva, Tear, Sweat, Vomitus, Sputum, Nasal secretion,


Stool & Urine are not considered potentially infectious unless
they are visibly bloody.
❖ MTCT/Mother to child transmission/; Intrapartum or perinatally from
mother to infant or via breast milk
❖ Contact with HIV-infected specimens (a definite but small occupational
risk of infection for health care workers and laboratory personnel)
❖ STIs- play a role in HIV disease transmission and progression

Diagnostic Approach
➢ Diagnosis of HIV infection → Diagnosis depends on demonstration of
antibodies to HIV and/or direct detection of HIV or one of its components.
Antibodies to HIV appear 2 - 12 weeks after infection
➢ Diagnosis of AIDS → CD4+ T-cell count <200/μL or AIDS-defining clinical
condition

Effects of HIV

➢ Direct effects:
✓ Nervous (encephalopathy and peripheral neuropathy)
✓ Kidney (HIVAN = HIV-associated nephropathy)
✓ Cardiac (HIV cardiomyopathy)
✓ Endocrine (hypogonadism in both sexes)
✓ GI tract (dysmotility and malabsorption/ ?HIV enteropathy)
➢ Indirect effects:
✓ Opportunistic infections and tumors as a consequence of
immunosuppression

Natural history of HIV infection

1. Phase 1: Transmission
2. Phase 2: Acute retroviral syndrome
✓ IP - 2-6 weeks post exposure
✓ Present with Fever, Sore throat, Nausea /Vomiting/diarrhea, Weight loss
/myalgia /arthralgia, Maculopapular rash (face, trunk, extremities),
Hepatosplenomegaly, Neurologic abnormalities (Aseptic meningitis,
Encephalitis, Peripheral neuropathy, GBS, Facial Palsy, Brachial neuritis,
Psychosis
✓ HIV Ab test negative
✓ CD+4 T cells number and function decline; But high viremia, high HIV RNA
levels and P24 antigenemia (high viral load) …
✓ Period of extreme infectiousness
✓ Be aware of false negatives
✓ Using rapid tests >95% of patients will test positive within 6 months

3. Phase 3: HIV Sero-conversion (Window Period)


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✓ Window period is a time period between acquisition of HIV infection and


antibody production
✓ Sero-conversion usually occurs within 6 weeks (80% antibody +ve) to 3
months (100% antibody +ve) after transmission. Rare cases will take
longer
4. Phase 4: Latent infection (Clinical latency)
✓ Asymptomatic stage
✓ No virologic latency → i.e. Period of continued viral replication and
gradual decline in CD4 + cells
✓ Viral set point:
• The level of HIV viremia early in the course of HIV where
the viral load plateaus
• predicts the likelihood of progression to AIDS in the next 5
years (The higher the viral set point: The more rapid disease
progression to AIDS and the more rapid the fall in CD4
count)
✓ In contrast to viral load, baseline CD4 is not a good predictor of time to
progression to AIDS. However, as the CD4 count declines over time (50-
100/year), patients will develop opportunistic infections

5. Phase 5: AIDS

CDC classification system of HIV-infected persons

CD 4 cell count A B C
(asymptomatic, PGL, (symptoms not in A (AIDS indicators)
acute retro viral or C)
syndrome)
> 500 cells/µl A1 B1 C1
200 - 499 cells/µl A2 B2 C2
< 200 cells/µl A3 B3 C3

A3, B3 and C (C1 - C3) defines AIDS

N.B for clinical practice, WHO classification is used commonly and CDC
classification is not used most of the time.

Patterns of HIV Disease Progression from primary HIV infection

Typical Progressors (90%) → 7 - 10 years


Rapid Progressors (< 5%) → <3 years
✓ High viral load, faster CD+4 decline
Long-term Non-progressors (< 10%) → >15-20 years
✓ Normal /stable CD4, without ART

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Clinical Stages of HIV Disease as per WHO Classification

Stage Features Performance


Status
1 ≥1 of the conditions listed below in an adolescent or adult (>13 years) with asymptomatic,
documented HIV infection; normal activity
➢ Asymptomatic HIV infection
➢ Persistent generalized lymphadenopathy (Enlarged lymph nodes > 1cm, in
2 or more non-contiguous extra-inguinal sites, in absence of known cause;
lasting more than 3 month)
➢ ARS (Acute Retroviral /HIV/Syndrome) → Acute (primary) HIV infection
with accompanying illness or history of acute HIV infection
2 ➢ Unexplained Weight loss <10% of presumed body weight symptoms, but
➢ Minor mucocutaneous manifestations: Picture; Seborrhoeic nearly fully
✓ Papular pruritic eruptions (PPE) dermatitis; Itchy scaly ambulatory
✓ Seborrhoeic dermatitis skin condition, especially
affecting scalp, face,
✓ Angular chelitis upper trunk (also
✓ Fungal nail infections of fingers common in non-HIV)
✓ Recurrent oral ulcerations (≥ 2 times/6months)
➢ Herpes zoster (current or in last 5 years)
➢ Recurrent upper respiratory tract infections (sinusitis, otitis media,
bronchitis, pharyngitis)
3 ➢ Oral candidiasis In bed more than
➢ Unexplained Weight loss >10% normal but <
➢ Unexplained chronic diarrhoea > 1 month 50% of normal
➢ Unexplained prolonged fever (intermittent or constant for >1 month) daytime during
➢ Recurrent vaginal candidiasis the previous
➢ Oral hairy leucoplakia (OHL) month
➢ Pulmonary tuberculosis currently or within the previous 2 years
➢ Severe presumed bacterial infections (e.g. pneumonia, empyema,
pyomyositis, bone or joint infection, meningitis, bacteraemia)
➢ Acute necrotizing ulcerative stomatitis, gingivitis or periodontitis
➢ Unexplained:
✓ Anaemia (<8g/dl) or
✓ Neutropenia (<500/mm³) or for > 1 month
✓ Thrombocytopenia (<50,000/mm³)
4 ➢ Recurrent severe bacterial pneumonia In bed > 50% of
➢ Chronic HSV infection- orolabial, genital, or anorectal of > 1 month normal daytime
duration during previous
➢ CMV infection (other than liver, spleen, LN) month
➢ CNS toxoplasmosis
➢ Cryptococcal meningitis (or other extra pulmonary crypto)
➢ Extrapulmonary tuberculosis
➢ HIV encephalopathy
➢ Progressive multifocal leukoencephalopathy (PML)
➢ HIV wasting syndrome 347
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✓ Weight loss > 10% PLUS


✓ Unexplained chronic diarrhoea > 1 month OR
✓ Unexplained prolonged fever > 1 month
➢ Pneumocystis pneumonia (PCP)
➢ Candidiasis of esophagus, trachea, bronchi, or lungs
➢ Any disseminated endemic mycosis (Histoplasmosis, Coccidiomycosis,
Penicilliosis )
➢ Kaposi's sarcoma
➢ Invasive cervical carcinoma
➢ Cryptosporidiosis, Isosporiasis
➢ Disseminated Mycobacterial diseases other than tuberculosis
➢ Recurrent non-typhoidal salmonella septicaemia (≥ 2 episodes in 1 year)
➢ Lymphoma (cerebral or B-cell NHL)
➢ VL
➢ Visceral Herpes simplex
➢ HIVAN (HIV - associated nephropathy)
➢ HIV - associated cardiomyopathy
➢ HIV Enteropathy

T- staging
➢ T-staging refers to clinical staging while on ART for at least 6 months
➢ Based on T-staging WHO stage 1 corresponds to stage T1, Stage 2 to T2,
stage 3 to T3 and Stage 4 to T3
➢ Used as an indicator of treatment outcome
➢ Prompts consideration to switch therapy
➢ Clinical events before the first six months of therapy are excluded from this
definition

5.2. Treatment of RVI

Objective
➢ Suppress viral replication to undetectable levels durably;
➢ Restore and preserve immunologic function;
➢ Prevent HIV transmission;
➢ Prevent opportunistic infections;
➢ Rehabilitate the patient and allow full function and survival.
Non pharmacologic
➢ Counseling and psychological support
➢ Nutritional support
➢ Socio-economic support

Pharmacologic
➢ Management of HIV disease includes prevention and treatment of OI and
controlling viral replication with HAART.
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Goal of HAART

❖ Virological → to decrease viral load


❖ Immunological → to increase CD4 Cell count (Immunity) Healthy life style
❖ Clinical → to decrease occurrence of OI

Indications for initiation of ART


General Considerations for ART:
➢ Effectiveness of ART is assessed by clinical observations, CD4 cell count
and viral load.
➢ ART should be initiated ASAP and not delayed until the immune system is
irreversibly damaged.
➢ For ART naïve patients, treatment is initiated with a combination of 3
medicines (Triple Therapy); consisting of 2 NRTIs and a 3rd medicine from the
NNRTI, Integrase Inhibitor (II) or Protease Inhibitors (PI).

Table: Anti-retroviral medicines for adults and adolescents


Medicine class/Medicine Dose (most of the time found in FDC form) Common side effects*
Nucleoside & Nucleotide RTl's (NRTI)
Tenofovir (TDF) 300 mg daily Nephrotoxicity
Lamivudine (3TC) 150 mg BID or 300 mg daily Safe drug among ART
Zidovudine (ZDV, AZT) 250−300 mg BID Megaloblastic anemia
Abacavir (ABC) 300 mg BID or 600 mg daily Hypersensitivity
reaction
Emtricitabine (FTC) 200 mg daily Safe, may cause
Headache, diarrhoea,
rash
Stavudine (D4T) Peripheral neuropathy,
lipoatrophy
Didanosine (ddI) Pancreatitis
Non-Nucleoside RTl's (NNRTI)
Efavirenz (EFV) 400-600mg daily CNS toxicity, rarely
severe skin reaction
Nevirapine (NVP) 200 mg daily for 14 days, then 200mg BID Drug-Drug interaction
with Rifampicin,
Hepatitis,
Hypersensitivity
reaction
Etravirine (ETV) 200 mg BID
Protease inhibitors (PI)
Atazanavir/ritonavir (ATV/r) 300mg/100mg daily Headache,
diarrhoea,rash
Darunavir + ritonavir (DRV/r) 800 mg + 100 mg daily (for individuals with
no previous PI) or 600 mg + 100 mg BID
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(for individuals with previous PI use)


Lopinavir/ritonavir (LPV/r) ➢ 400mg/100mg BID (533mg/133mg B I D ➢ Lopinavir →
when combined with EFV or NVP Paresthesia,
➢ Considerations for individuals receiving TB hyperlipidemia
therapy ➢ Ritonavir →
➢ In the presence of rifabutin, no dose Hyperglycemia,
adjustment required. asthenia
➢ In the presence of rifampicin, adjusted
dose of LPV/r: LPV 800 mg + RTV 200
mg BID or LPV 400 mg + RTV 400 mg
BID). OR, SQV/r (SQV 400 mg + RTV
400 mg twice daily), with close
monitoring.
Integrase inhibitors / Integrase strand transfer inhibitors (II / INSTIs)
Dolutegravir (DTG) ➢ 50 mg, PO, daily
➢ If TB coinfection, 50mg, PO, BID
Raltegravir (RAL) ➢ Treatment- naïve patients: Film-coated tablet:
400 mg, PO, BID or 1,200 mg, PO, daily
➢ Treatment- experienced patients: Film-coated
tablet: 400 mg, PO, BID.
*The major causes of drug discontinuation in the first 3-6 months after initiating ART are due to drug
toxicities
*Toxicities of NNRTIs (NVP and EFV) occur in the first few weeks, and may be life-threatening
*ABC hypersensitivity reaction starting from first week following initiation
*Anaemia and neutropenia due to ZDV occur in the first 3 months

When to start treatment


❖ Unlike the previous recommendations, it is critical to initiate ART ASAP
(same day to within 7 days of HIV diagnosis); this reduces HIV related
morbidity and mortality, and reducing forward transmission of HIV including
MTCT.
❖ All HIV positive people are eligible for ART irrespective of their WHO
clinical staging and/or CD4 count following a confirmed HIV diagnosis,
clinical assessment and assessment of client readiness.
❖ As a priority, ART should be initiated ASAP in all adolescents and adults
with advanced disease (WHO stage 3 to 4, CD4 count ≤350 cells/mm3)
and all children regardless of WHO staging and CD4 count/percentage
❖ For women identified at labor and delivery, provide ART with in the same
hour of HIV diagnosis with brief counseling and provide detailed counseling
on ARV and adherence after delivery.
❖ Requirements for initiation of ART
✓ HIV positive test result with written documentation
✓ Start only patients with medical eligibility for ART
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✓ Ensure readiness of patient for ARV therapy


❖ Infections may cause transient decrease in CD4 count & be careful with
interpretation of the CD4 count. Therefore, treat and stabilize any OIs
before starting ART.

Medicine Regimens
First-line regimens for adults and adolescents In Ethiopia: for treatment naive patient
for the first time.
➢ TDF + 3TC + DTG/EFV as a once-daily dose.
✓ FDC (Fixed-dose combinations) and once-daily regimens are preferred.
✓ For HIV/TB co-infected adults and adolescents, the recommended dose of
DTG is 50 mg, PO, BID.

Table Summary of first-line ART regimens for adults, pregnant & breastfeeding women, adolescents and
children.
Population Preferred first-line regimens Alternative first-line regimens a
Adults (including those with TB/ ➢ TDF + 3TC + DTG (FDC)* ➢ AZT + 3TC + EFV/NVP OR
HIV b-coinfection) OR ➢ TDF + 3TC + NVP
➢ TDF + 3TC + EFV (FDC)**
Pregnant and breastfeeding ➢ TDF + 3TC + EFV (FDC)
women
Adolescents (10 to 19 years) ➢ TDF + 3TC + DTG (FDC)* ➢ AZT + 3TC + EFV/NVP OR
weight ≥35 kg (Including those OR ➢ TDF + 3TC + NVP OR
with TB/HIV -coinfection.)
b
➢ TDF + 3TC + EFV (FDC)** ➢ ABC + 3TC + EFV
Children 3 years to <10 years ➢ AZT/ABC + 3TC + EFV ➢ AZT + 3TC + NVP OR
and adolescents’ weight <35 kg ➢ TDF + 3TC + EFV OR
➢ TDF + 3TC + NVP OR
➢ ABC + 3TC + NVP***
Children <3 years ➢ ABC/AZT + 3TC + LPV/r ➢ ABC/AZT+ 3TC + NVP
a
ABC or boosted PIs (ATV/r, LPV/r) can be used in special circumstances
b
In case of TB-HIV coinfection, the dose of DTG should be 50mg BID.
*If available as triple FDC, TDF+3TC+DTG is the preferred regimen for HIV positive adult and
adolescent patients.
**TDF+3TC+EFV400 (FDC) will replace the TDF+3TC+EFV600 (FDC) for adults and adolescents
(except for pregnant mothers and TB/HIV co-infected patients as there is no adequate data for this
groups) up on availability.
*** Caution: co-administration of ABC with NVP in pediatric patients will increase the risk of
hypersensitivity reaction and requires extreme precaution.

Management of advanced HIV disease


➢ For adults and adolescents, and children >5 years, advanced HIV disease is
defined as CD4 cell count <200cells/mm3 or WHO stage 3 or 4 event.
➢ All children <5 years old with HIV are considered as having advanced HIV
disease.
➢ A package of interventions including screening, treatment and/or prophylaxis for
major OIs, rapid ART initiation and intensified adherence support should be
offered to everyone presenting with advanced HIV disease including those who
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are reengaging with care after a period of interruption.

First line for advanced HIV disease treatment


✓ TDF + 3TC + DTG/EFV as a once-daily dose.
Alternatives first line
✓ AZT + 3TC + EFV

Second line drugs are used if there is treatment failure or if there is serious side
effect develops from 1st line drugs.

5.2.1. Antiretroviral treatment failure

➢ Routine viral load testing is a more sensitive and earlier indicator of treatment
failure.
➢ To detect treatment failure proactively, routine viral load testing should be done
at 6 and 12 months of initiating ART and then every 12 months thereafter and
plus whenever there is clinical or immunologic suspicion of treatment failure.

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Table: Definitions of clinical, immunological and virologic failure for the decision to switch ART regimens
Failure Definition Remark
Clinical Adults and adolescents ➢ The condition must be
failure ➢ New or recurrent clinical event indicating severe differentiated from IRIS
immunodeficiency (WHO clinical stage 4 condition and occurring after initiating ART.
certain WHO clinical stage 3 conditions (pulmonary TB
and severe bacterial infections) may also indicate
treatment failure) after 6 months of effective treatment.

Adults and adolescents ➢ Without concomitant or recent


Immunologic ➢ CD4 count ≤ 250 cells/mm3 following clinical failure or infection to cause a transient
failure decline in the CD4 cell
Persistent CD4 levels below 100 cells/mm3.
count.
➢ Persistent is to mean at least
Children
2 CD4 measurements below
➢ Younger than 5 years:
the threshold.
✓ Persistent CD4 level < 200 cells/mm3 or <10%;
➢ Current WHO clinical and
➢ Older than 5 years:
immunological criteria have
✓ Persistent CD4 levels < 100 cells/mm3. low sensitivity and positive
predictive value for identifying
individuals with virologic
failure.
Virologic ➢ Viral load > 1000 copies/ml based on 2 consecutive viral ➢ An individual must be taking
failure load measurements in 3 months, with enhanced ART for at least 6 months
adherence support following the first viral load test. before it can be determined
that a regimen has failed.
➢ Viral Load testing should not
be done when there is an
acute infection/fever.

Causes of Treatment Failure


➢ Viral Factors:
✓ drug-resistant virus, either transmitted or acquired
✓ Aggressive virus: a “rapid progressor”, “syncytial forming.”
✓ Patient Factors
➢ Patient factors (Poor adherence)
✓ Poor absorption
✓ Rapid elimination
✓ comorbidities e.g., active substance abuse, depression
➢ Drug Factors
✓ Low potency regimen
✓ Antagonist combination
✓ Drug-drug interaction
✓ Drug-food interactions
✓ Inappropriate dosing
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✓ Drug side effects and toxicities

Re-engaging with care after ART interruption


➢ Re-evaluate for possible adherence barriers and advanced clinical conditions.
➢ Then resume the same (previous) ART regimen used before interruption.
However, people interrupting NNRTI - containing regimen (high risk of drug
resistance) should restart using a DTG - containing regimen (has high genetic
barrier to resistance and can bring rapid viral suppression)
➢ Then, ongoing Enhanced Adherence Counseling (EAC), frequent follow-up,
close viral load monitoring/determining at 3 and 6 months after resuming ART
is required.
➢ If there is confirmed failure of the current treatment regimen, the client needs
to be switched to appropriate second-line or third line regimen.

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Figure. Algorithm for routine clinical and viral load monitoring. * For those patients
with identified significant adherence barriers, it is advisable to extend the provision of
Enhanced adherence counseling for 6 months before doing the second Viral load testing
in order to properly address the barriers and give optimal time for viral suppression to
happen

➢ Using a boosted PI + two NRTI combinations is recommended as the preferred


for second-line ART for adults, adolescents and also for children when NNRTI-
containing regimens were used in first-line ART.
➢ In children using a PI-based regimen for first-line ART, switching to NNRTI or
maintaining the PI regimen is recommended according to their age.

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Table: preferred second-line ART regimens for adults and adolescents


Target population Preferred second-line regimen
Adults and If TDF+3TC+DTG#used in first-line AZT + 3TC + ATV/r or LPV/r
adolescents If AZT was used in first-line ART TDF + 3TC + LPV/r or ATV/r
(≥10 years)* If TDF was used in first-line ART AZT + 3TC + LPV/r or ATV/r
HIV and TB co- If rifabutin is not available Same NRTI backbones as
infection recommended for adults and
adolescents plus double-dose LPV/r
(that is, LPV/r 800 mg/200 mg twice
daily) or standard LPV dose with an
adjusted dose of RTV (that is, LPV/r
400 mg/400 mg twice daily).
HIV and HBV co- DTG + TDF/3TC + ATV/r OR ➢ If switching an ARV regimen in
infection AZT + TDF + 3TC + (ATV/r or HBV/HIV coinfected patients,
LPV/r) HBV active ARV drugs
(TDF/3TC) should be continued
in the new regimen.
➢ Discontinuation of HBV active
ARV drugs may lead to
reactivation of HBV and result in
serious hepatocellular damage.
➢ The DTG regimen may be
preferred if the loose AZT is
unavailable.
➢ If DTG regimen used, watch
increased hepatotoxicity of DTG
and HBV
*Adult clients taking ABC can be shifted to AZT. For pregnant women same regimens recommended
as for adults and adolescents, but cautious counseling or alternative suggestions (if available) is
required before DTG use (low NTD risk of 0.3% vs 0.1 % in non DTG regimens).15 If TDF and ABC
have been used in the first-line regimen, patients may be referred to experienced physicians for
selection of the second-line medicines.

#
For HIV/ TB co-infected adults and adolescents, the recommended dose of DTG is 50 mg
twice daily. Children weighing more than 20 kg can take adult 50mg film-coated tablets,RAL can be
used in neonates and children less than 20 kg body weight.

Identification and management of second-line treatment failure


15
‘’Start ART for HIV positive mothers who are breastfeeding even if it was not started
before (currently recommended regimen TDF/3TC/ DTG)’’ MANAGEMENT PROTOCOL ON
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➢ Patients who are on 2nd line regimen and have high viral load level (>1000
copies/ml) after 6 months of treatment need to go through the algorithm as
described for first line treatment failure with enhanced adherence support and
repeat test after 3 months to decide second line treatment failure.
➢ If confirmed to have 2nd line failure, consult (or refer to) experienced physicians
for initiation of 3rd line regimens.
➢ Before switching to 3rd line regimen, ensure the following.
✓ Two consecutive viral load measurements > 1000 copies/ml at least 3
months apart.
✓ First viral load measurement done at least 6 months after switching to 2nd
line regimen.
✓ The repeat viral load test should be done after 3 months of enhanced
adherence support.
✓ The approach in switching to 3rd line should follow the guiding principles
listed out for switching to 2nd line drugs.

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5.2.2. Monitoring ARV Treatment

➢ Start from the day of initiation.


➢ The first six months of therapy are especially critical for monitoring.

What to expect in the first months of ART and how to manage them?
➢ ART initiation may be associated with IRIS as well as early adverse drug
events, such as drug hypersensitivity, in the first three months of ART
➢ Be alert to OIs and/or IRIS as well as adverse drug events, in the early phase
of ART initiation.
➢ Especially a high mortality seen in the first three to six months of ART
initiation among people who started ART with advanced HIV disease with
existing co-infections and/or co- morbidities, severely low hemoglobin, low body
mass index (severe malnutrition) and/or very low CD4 counts.
➢ Failure to achieve CD4 recovery or presence of CD4 decline after treatment
initiation particularly after one year (common in those with very low CD4 cell
on ART initiation) should alert to potential adherence problems or primary non-
response to ART, and consideration should be given to continue prophylaxis
for OI such as CPT till patients recovers immunologically.

5.3. IRIS (Immune reconstitution inflammatory syndrome)

➢ IRIS is a spectrum of clinical signs and symptoms thought to be associated


with immune recovery brought about by a response to ART.
➢ It occurs among 10 - 30% of the people initiating ART, usually within the first
4 - 8 weeks after initiating therapy.
➢ It may present in two different ways:
✓ Paradoxical IRIS
• An OI or tumor diagnosed before ART initially responds to
treatment but then deteriorates after ART starts
• The most serious and life-threatening forms of paradoxical
IRIS are for TB, Cryptococcus’s, Kaposi’s sarcoma and
hepatitis.
• BCG vaccine - associated IRIS (localized and systemic) may
occur in some HIV infected infants.
✓ Unmasking IRIS → initiating ART triggers disease that is not clinically
apparent before ART.
➢ It is diagnosis of exclusion. i.e. It should be considered only when the
presentation cannot be explained by a new infection, expected course of a
known infection or drug toxicity
➢ Before initiating ARV, providers need to give due consideration for patients with
low CD4 cell count (<50 cells/mm3) at ART initiation, disseminated OIs or
tumors and a shorter duration of therapy for OIs before ART starts as they are
the main risk factors for IRIS.
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➢ IRIS is not indicative of treatment failure or drug side effect and doesn’t need
discontinuation or change of ARVs.
➢ It is generally self-limiting, and interruption of ART is rarely indicated, but
people may need to be reassured in the face of protracted symptoms to
prevent discontinuation of or poor adherence to ART.
➢ (NB: Actively watch for IRIS in patients starting with first-line regimens
containing integrase-inhibitors such as DTG)
➢ The most important steps to reduce the development of IRIS include:
✓ Earlier HIV diagnosis and initiation of ART before a decline to < 200 CD4
cells/mm3
✓ Improved screening for OIs before ART, especially TB and Cryptococcus;
and
✓ Optimal management of OIs before initiating ART.
➢ Timing of ART in people with OIs requires; balancing a greater risk of IRIS
after early initiation against continuing high mortality if ART is delayed.

Investigation and diagnosis of IRIS


➢ Most or all of the following features should be present in order to make the
diagnosis of IRIS:
✓ A low pretreatment CD4 count (often < 100 cells/µL) except in
tuberculosis. IRIS secondary to preexisting TB infection may occur in
individuals with CD4 counts >200;
✓ A positive immunological response to ART;
✓ The absence of evidence of drug-resistant infection, bacterial super
infection, drug allergy or other adverse drug reactions, patient
noncompliance, or reduced drug levels due to drug-drug interactions or
mal-absorption after appropriate evaluation for the clinical presentation;
✓ The presence of clinical manifestations consistent with an inflammatory
condition; and
✓ A temporal association between HAART initiation and the onset of clinical
features of illness- usually within the first 6 months.
➢ Commonly seen when ART is started at very low CD4 count.
➢ Atypical presentations are common
✓ localized lymphadenitis, prolonged fever, pulmonary infiltrates, hepatitis,
increased intracranial pressure, uveitis, sarcoidosis, and Graves’ disease.
✓ The clinical course can be protracted, and severe cases can be fatal
✓ Steroids may be indicated for some conditions
➢ Conditions that can present as IRIS: TB, cryptococcal meningitis, PCP, CNS
toxo, herpes virus, CMV, PMLE, kaposi sarcoma, Grave’s disease…

Management of IRIS
➢ Patients should generally be treated for the underlying OI ASAP.
➢ Continuation of ART when IRIS occurs.

Anti-inflammatory agents’ vs IRIS:


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➢ Particularly helpful in settings of obstructive mass lesions (e.g. expanding


cervical lymph node).
➢ Their use, particularly corticosteroids, must be weighed against potential
risks/side effects.
➢ If corticosteroids, initiate therapy with prednisone 1 mg/kg/day (maximal dose
60 - 80 mg) followed by a rapid taper over a 10 to 14-day period.
➢ IRIS in closed spaces (e.g. CNS OI) should be managed promptly to avert
significant morbidity and mortality.

Follow up

➢ Standardized clinical assessment of patients and, when available baseline CD4


count, are important to determine the severity of immunosuppression and
decide on initiation of prophylactic therapies.
➢ Before initiating ART, patients shall be thoroughly evaluated at baseline and
periodically for the rest of their lives to monitor toxicity, intolerance, poor
response or failure to treatment, OIs, other co-morbidities are always need to
be looked for and managed.
➢ Once on ART:
☛ 1st follow-up visit will be every 1 week for the first 2 consecutive visits
and a gradual extension.
☛ Then, appointed every 2 weeks during the 1st month of treatment and
☛ Every 4 weeks (every month) then after until 24 weeks of treatment.
☛ After the 24th weeks of initiation of antiretroviral therapy patients will be
scheduled to return every 12 weeks.
➢ During each visit, patient should be evaluated for new symptoms that may be
related to medicine side effects, the disease progression, and clinical
improvements/deterioration, and adherence, development of OIs or recurrent
problems that may exist
➢ Patients should be encouraged to come at any time if they have concerns and
can be seen out of the above schedule whenever necessary.
➢ When a woman in reproductive age is taking DTG containing regimen,
occurrence of pregnancy shall be prevented and monitored. If pregnancy
happens while on DTG containing regimen, DTG shall be replaced with EFV.
➢ For ART, a high level of sustained adherence is extremely necessary.

Monitoring for toxicity of ART

Guiding principles
✓ Establish whether the clinical condition is due to ARV toxicities, other
drugs, or other illness including new OI’s
✓ Try to identify the responsible ARV drug.
✓ Assess the severity using toxicity grading matrix.
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Clinical monitoring for toxicity of ART

➢ The major causes of drug discontinuation in the first 3-6 months after initiating
ART are due to drug toxicities; and hence, they must be closely monitored.
They occur from few weeks to months.
➢ All patients require clinical evaluation at least every month in the first 6
months for ARV related toxicity. Subsequent follow-up can be done by
months.
➢ The most frequent drug adverse reactions include:
✓ Toxicities of NNRTIs (NVP and EFV) occurring in the first few weeks, and
may be life- threatening.
✓ ABC hypersensitivity reaction starting from first week following initiation.
✓ Anemia and neutropenia due to AZT occur in the first 3 months.
✓ Intolerance to certain drugs, in particular AZT induced gastrointestinal
problems, are important barriers to adherence unless appropriate
measures are taken.
➢ The clinical manifestations due to hypersensitivity reactions (ABC and NVP)
may be confused with IRIS.
➢ Laboratory monitoring for toxicity of ART: look at IX section Above

5.4. Post-exposure prophylaxis (PEP) and Pre-exposure


prophylaxis /PrEP/

Steps to manage potential HIV exposed person

1. Treat the exposure site /immediate measures


➢ Percutaneous injury or injury to non-intact skin:
✓ Wash exposed site with soap & water ASAP, without scrubbing
✓ Avoid using antiseptics.
✓ Allow free bleeding but do not squeeze the wound.
➢ Exposed mucous membranes:
✓ Irrigate copiously with clean water or saline.
2. Report the exposure: To PEP focal person or ART physician or nurse in the
facility immediately to handle the case based on the national programmatic
recommendations
3. Start PEP; PEP is a medical emergency - If possible, administer the first dose
within 2 hours of exposure.

PEP recommendations based on risk assessment (Look at the table below)


➢ PEP is indicated for occupational exposures with a percutaneous, mucous
membrane and non-intact skin exposure with potentially infectious body fluids.
➢ If the HIV status is unknown, starting empiric PEP and confirming the source
patient HIV status is very critical to weight the benefit against the cost of
treatment continuation.
➢ If the source patient is inaccessible for HIV testing for any reason, empiric
PEP is recommended regardless of the knowledge of HIV status particularly for
high-risk exposure settings or high-risk source patients. For instance, if the
source is at high risk for HIV infection (eg, injection drug users) or has
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symptoms suggesting HIV infection or risky exposure setting (e.g., needle stick
from a sharps container in an HIV clinic).

Table: Recommended PEP based on risk assessment


Source HIV status Recommendations to potential infectious body fluid occupational exposure*
Source patient is HIV 3 drug PEP (preferred regimen: TDF +3TC+DTG) **
positive (symptomatic or
asymptomatic)
Source patient HIV status is Give 3 drug PEP while awaiting HIV testing
unknown
Source patient is HIV No PEP warranted
negative
➢ Extended PEP (3-Drug Regimen or Triple FDC):
✓ TDF+ 3TC + DTG, Once daily for 28 days (Triple FDC; TDF 300mg, 3TC 300mg, DTG 50mg)
• Raltegravir (400 mg BID) or boosted PI based regimen may be used in pregnant
mothers
Or
✓ TDF + AZT + 3TC + LPV/r, PO, BID for 28 days (AZT 300mg, 3TC 150mg, LPV/r 400mg/100mg)
Or
✓ TDF + AZT + 3TC + ATV/r, PO, daily for 28 days (ATV/r 300mg/100mg)
*Infectious body fluids include blood, semen, vaginal secretions, any body fluids contaminated with visible
blood, as well as cerebrospinal, synovial, pleural, peritoneal, pericardial, and amniotic fluids are potentially
infectious. On the other hand, feces, nasal secretions, saliva, gastric secretions, sputum, sweat, tears,
urine, and/or vomitus are not considered infectious unless they contain blood;
**3 drug PEP preferred over two drug regimen and should be given within 72 hours for 28 days.

Timing and duration of initiation of prophylaxis:

☛ PEP is a medical emergency.


☛ To be effective, PEP should commence ASAP (within 1 - 2 hours). The
maximum delay for initiation of treatment which would prevent infection
is not known in humans.
☛ Do not consider PEP beyond 72 hours post exposure.
☛ Prophylaxis is to be given for 28 days.

Testing and monitoring after occupational exposure:

➢ Testing source:
✓ If the source is negative no need for further assessment of the exposed
victim is needed. If the source is positive, tasting the exposed person is
needed.
➢ HIV serology test of the exposed person:
✓ Immediately after exposure.
✓ If the result is positive no need for PEP, but if negative administer PEP
ASAP as outlined above and then repeat serology at 6 weeks, 3 months,
and 6 months.
✓ HBV Testing (screening) is also recommended.
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➢ NB: initiate PEP immediately after exposure until test result confirms the HIV
status of the victim. Stop PEP if the health worker is positive for HIV
antibodies.
➢ Following HIV exposure there is a need for psychosocial support.

Prevention of Transmission of HIV after Sexual Assault

➢ Need counseling about potential risk of HIV infection


➢ Know the victim’s HIV status prior to PEP
➢ Encourage patient to be tested ASAP with a delay not > 72 hours
➢ Inform possibility of transmitting infection during sero-conversion
➢ Instruct to return at 6 weeks and 3 months post sexual assault for PICT.
➢ Post-rape prophylaxis should be monitored & evaluated for:
✓ Emergency contraceptives
✓ Psychosocial and legal support
✓ Screening for conventional STIs and follow-up management
✓ Drug side effects
✓ Sero-conversion
➢ Recommended PEP for post sexual Assault HIV exposure
✓ AZT/TDF + 3TC + DTG for 28 days. Alternatively, Kaletra or boosted
Atazanavir can substitute DTG

Follow-up of client exposed to HIV

➢ Post exposure testing


✓ A client who is taking PEP should be followed in adult ART clinic
✓ Instruct to return at 6 weeks, 3 months and 6 months post sexual assault
for PICT.
➢ Monitoring and management of PEP toxicity
✓ Reassessed within 3-5 days for medication tolerability and toxicity.
✓ A further risk assessment re-evaluation may also be appropriate as
necessary
✓ Drug toxicity should be tested at baseline and again 2 weeks after
starting PEP.
✓ The scope of testing is based on medical conditions of candidate and
toxicity of drugs included in PEP regimen.
✓ Minimal, lab monitoring for toxicity includes CBC and LFT.
✓ If toxicity is noted, modification of regimen should be considered.

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Pre-Exposure prophylaxis (PrEP)

➢ Oral PrEP of HIV is the use of ARV drugs by people who are not infected
with HIV but at a substantial risk.
➢ Substantial risk of HIV infection is defined as incidence of HIV higher than 3
per 100 person-years in the absence of PrEP.
✓ HIV-positive sexual partner, recent bacterial STI, high number of sex
partners, history of inconsistent or no condom use and commercial sex
work; In high HIV prevalence area or network; HIV-positive injecting
partner sharing injection equipment.
➢ PrEP is aimed to block the acquisition of HIV.
➢ Eligibility for PrEP
✓ Negative HIV test result before prescribing PrEP
✓ No signs/symptoms of acute HIV infection
✓ Normal renal function; no contraindicated medications
✓ Known hepatitis B virus infection and vaccination status
➢ Prescriptions for PrEP and follow-up
✓ Daily, continuing, oral doses of TDF+3TC or FTC, ≤ 90-day supply
✓ Follow-up visits at least every 3 months to provide the following:
• HIV test, medication adherence counseling, behavioral risk
reduction support, side effect assessment, STI symptom
assessment
• At 3 months and every 6 months thereafter, assess renal
function
• Every 3-6 months, test for bacterial STIs

16
5.5. PMTCT and treatment of RVI exposed infant
➢ PMTCT (Prevention of mother to child transmission) of HIV have four prongs
✓ Prong 1: Primary prevention of HIV infection
✓ Prong 2: Prevention of unintended pregnancies in HIV-positive women →
emphasizes reducing the number of unplanned or unwanted pregnancies
and effective family planning counseling service
✓ Prong 3: Prevention of HIV transmission from women living with HIV to
their infants → addresses care for HIV-positive women during pregnancy,
labor and childbirth, and breastfeeding and care for their infants.
✓ Prong 4: Provision of treatment, care, and support to women living with
HIV, and their infants, partner, and families → including on-going, chronic
care and treatment for HIV-positive pregnant/postpartum women and their
HIV-exposed and HIV-positive children both during and beyond the
PMTCT intervention period.
➢ All HIV positive pregnant, laboring and lactating mothers will be initiated on
HAART for life (TDF, 3TC and DTG).

16
Details of PMTCT are beyond the scope of this text book. Here is a highlight to have knowhow only. It is
better to link mothers, to PMTCT clinic, special ANC follow up and labor management is mandatory. 364
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➢ HIV positive woman already on ART at time of pregnancy should continue and
stay on the same regimen.

Post-partum and Neonatal care


➢ Continue initial ART for those who are initiated earlier.
➢ Start ART for HIV positive mothers who are breastfeeding even if it was not
started before (currently recommended regimen TDF + 3TC + DTG)
➢ For mothers who fulfill Acceptable, Feasible, Affordable, Sustainable and Safe
(AFASS) feeding, formula feeding should be considered after thorough
discussion with the family.
➢ For those who do not fulfill AFASS, breastfeeding must be exclusive for 6
months and complementary feeding should start at 6th month. Breastfeeding
should be continued until the first year of life but not more than two years.

RVI exposed infant


➢ Give Nevirapine plus zidovudine syrup for the first 6 weeks and continue NVP
syrup only for the next 6 weeks for all HIV exposed infants (see table below
for dosing).
➢ Zidovudine and nevirapine should be given during the first week of life.
Start treatment ASAP after birth (within 48 hours)
➢ CPT should be started early
✓ Cotrimoxazole syrup (240mg/5ml), 48mg/kg/day, PO, BID

Table; Enhanced Post-natal Prophylaxis (e-PNP) for HIV Exposed Infants17


Infant age and Weight Dose
duration of treatment
0-6 weeks < 2500g ☛ Nevirapine syrup (50mg/5ml i.e.10mg/ml), 8
mg/kg/dose, PO, daily plus
☛ Zidovudine syrup (50mg/5ml), 2 mg/kg/dose, PO,
BID
> 2500g ☛ Nevirapine syrup (50mg/5ml), 12 mg/kg/dose,
PO, daily plus
☛ Zidovudine syrup (50mg/5ml), 4 mg/kg/dose, PO,
BID
6-12 week Nevirapine syrup (50mg/5ml), 12 mg/kg/dose, PO, daily
17
The note above is from UpToDate 2018. We recommend to use these one per Kg dose.
Below is a table taken from <<Management protocol on selected obstetrics topics for hospitals, FMOH,
Ethiopia, December 2020>> for comparison.

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DNA/PCR should be done at 6 weeks of life and HIV negatives should


be followed as HIV Exposed Infant (HEIs).
✓ DNA/PCR positive babies should be linked to pediatric ART for
chronic HIV/AIDS follow up
✓ Do confirmatory rapid HIV antibodies test for DNA/PCR
negative HEIs 6 weeks after the cessation of breastfeeding
Discharge negative babies for follow up after rapid HIV antibody test
and link the positive babies to chronic pediatric HIV care, treatment and
follow up.
Give postpartum family planning counseling and provide mothers with
family planning method of their choice as per the PMTCT guideline and
post-partum care section of the protocol.
Immunization and growth monitoring for the baby should be done the
same way as non-HIV exposed babies
The mother and infant should do their follow up at the MNCH clinic,
where they can get integrated MNCH and HIV care.
After discharge link the mother with ART clinic in the following
scenarios:
✓ If the baby is DNA/PCR positive
✓ If the baby is rapid HIV AB test positive
✓ If the baby is dead.
✓ If the mother develops any HIV/AIDS related complications of
the disease or its treatment

Further reading
➢ MANAGEMENT PROTOCOL ON SELECTED OBSTETRICS TOPICS FOR HOSPITALS,
December 2020, FMOH, Ethiopia
➢ WHO PMTCT guideline; ANTIRETROVIRAL DRUGS FOR TREATING PREGNANT WOMEN AND
PREVENTING HIV INFECTION IN INFANTS: TOWARDS UNIVERSAL ACCESS

5.6. Opportunistic infections (OI’s)


➢ OIs are new or pre-existing conditions that occur when the immune system is
impaired.
➢ They are the major cause of morbidity & mortality in HIV patients.
➢ Diseases directly caused by the HIV are not considered opportunistic diseases.
E.g. HIV encephalopathy, HIVAN
➢ As the CD4 level declines, the risk of opportunistic infections increases. The
level of immunity determines the occurrence and type of OIs.
➢ Most common OIs are both preventable & treatable.
➢ Screening and management of OIs is critical at any time of HIV care.
➢ Frequently affected organ systems are the nervous, gastro-intestinal and
respiratory systems, and the skin.
➢ In general, milder infections such as herpes zoster and other skin infections
occur early whereas serious life-threatening infections such as CNS
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toxoplasmosis and Cryptococcal meningitis occur later with severe immune-


suppression.
➢ Some life-threatening infections, such as pneumonia and TB, may occur early
as well as later. When TB occurs later it is atypical, more disseminated and
more extra pulmonary

General strategies to prevent OIs are:


➢ Reduction of exposure
➢ Chemoprophylaxis (primary/secondary)
✓ The 3 Chemoprophylaxis therapies practiced in Ethiopia;
• CPT (cotrimoxazole preventive therapy)
• IPT (INH preventive therapy)
• Fluconazole
➢ Immunization and
➢ Starting HAART

Co-trimoxazole preventive therapy (CPT)

➢ An effective prophylaxis against:


✓ Various bacterial infections: Streptococcus pneumoniae, Salmonella
species, Shigella species, E. Coli, S. Aureus, H. Influenzae and Nocardia
✓ PCP (Pneumocystis jirovecii)
✓ Toxoplasmosis
✓ Diarrhea caused by Isospora belli or Cyclospora
✓ Malaria
➢ Dose; cotrimoxazole 960 mg, PO, daily
✓ for pediatrics; cotrimoxazole syrup (240mg/5ml), 48mg/kg/day, PO, daily.

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Table: CPT indication for primary prophylaxis


Age Criteria for initiation Criteria for discontinuation* Monitoring
approach
HIV In all, starting at 4 - Until risk of HIV transmission ends or HIV infection
exposed 6 weeks after birth is excluded clinical at 3-
infants month
<5 years In all Discontinue for those older than 5 years of age who Intervals
are clinically stable, with evidence of immune
recovery (CD4 cell count >350 cells/mm3) and/or
viral suppression on ART
≥5 years, Any WHO stage and Discontinue in clinically stable patients (individuals on
including CD4 count ≤350 ART for at least one year without any new WHO
adults cells/mm3 Or WHO clinical stage 2, 3 or 4 events) with;
stage 3 or 4, ✓ Evidence of immune recovery and/or viral
irrespective of CD4 suppression (CD4 count >350 cells/mm3,
level with viral load suppression) or
✓ Two consecutive CD4 count > 350
cells/mm3 if no viral load result
➢ *Discontinue also if the person has SJS (Stevens-Johnson syndrome), severe liver disease, severe
anemia, severe pancytopenia or negative HIV status.
➢ Contraindications to CPT: severe allergy to sulfa drugs; severe liver disease, severe renal disease
and G6PD deficiency.

Isoniazid Prophylaxis Therapy (IPT)

Look at under RVI TB below

Fluconazole prophylaxis

➢ Indication
✓ After completing treatment for Cryptococcal meningitis
➢ Dose: 200mg Po daily

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5.6.1. Respiratory system OI’s

➢ Both URTIs & LRTIs are common


➢ Leading causes of death
✓ Bacterial – Strept. pneumonia, H. influenza, legionaries, nocardia,
Rhodococcus equi, S.aureus, G-ves (klebsella), Mycobacteria (TB, MAC)
✓ Viruses – CMV, EBV
✓ Fungal – PCP, Cryptococcus, histoplasmosis, candida, mucoromycosis
✓ Protozoal – toxoplasmosis
✓ Neoplastic – Kaposi sarcoma, lymphoma
✓ Idiopathic – lymphoid and idiopathic interstitial pneumonia

5.6.1.1. RIV - TB coinfection

➢ TB is the most frequent life-threatening OI and a leading cause of death


among HIV infected people.
➢ TB increases HIV replication through immune activation, thus high viral load
and rapid progression of HIV disease.
➢ On the other hand, HIV increases susceptibility to M. tuberculosis infection (20-
37 times greater lifetime risk than HIV negative), progression to TB disease
and the incidence and prevalence of TB. This necessitates collaboration among
the two programs.

Impact of HIV on TB

➢ Increases rate of TB re-activation, progression and active TB


➢ Increases TB morbidity and mortality (5 - 14-fold)
➢ Alters clinical manifestations of TB
☛ The clinical manifestations of TB in HIV-infected patients are influenced
by the degree of immunosuppression.
☛ Early in the course of HIV disease, the clinical presentation of TB is
similar to that of HIV-uninfected patients; symptoms include fever, cough,
weight loss, fatigue, loss of appetite, night sweats, and hemoptysis.
☛ As immunity declines, the frequency of pulmonary cavitation and
hemoptysis also declines.
☛ HIV-infected patients with advanced immunosuppression are at increased
risk of extrapulmonary TB and disseminated TB. Virtually any site can
be involved; the most common presentations are lymphadenitis and
pleural involvement.
☛ Septicemic-like illness with hypotension can occur, with high mortality
rate unless diagnosed and treated rapidly. In contrast, active tuberculosis
may be subclinical in some patients with advanced immunosuppression,
with no symptoms and a normal chest radiograph.
➢ Creates diagnostic challenges → TB diagnosis in HIV infected patients is
difficult
✓ Clinical manifestations become more atypical as immune function
deteriorates
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• Sputum-smear negativity (up to 40% in culture proven


pulmonary cases), atypical CXR finding, lack of classic
granuloma formation in the late stages, and a negative TST
✓ Negative AFB smear or Gene Xpert do not rule out PTB
✓ Extra pulmonary manifestations are common than pulmonary TB
✓ Empiric anti-TB may be warranted in many circumstance
✓ Complicates treatment

Impact of TB on HIV

➢ TB infection activates T-cells, indirectly supporting HIV replication


➢ Accelerates HIV disease progression → Active TB is associated with increased
HIV-1 viral load, progression to AIDS, high mortality

Table; Timing of ART for adults and children with TB


Patients with tuberculosis found to be HIV positive HIV positive patients taking ART diagnosed
with TB
➢ Start ART in all TB patients, including with drug-resistant TB, ➢ Start anti-TB
irrespective of the CD4 count. ➢ Modify ART regimen to avoid drug-drug
➢ Start anti-TB treatment first, followed by ART ASAP within the interaction (e.g. change NVP with EFV)
first 8 weeks. ➢ If patients develop TB while on ART for
➢ It is recommended that ART be initiated as soon as TB 3-6 months, continue ART throughout TB
therapy is tolerated. Ideally, this may be as early as 2 treatment and patients with NVP based
weeks and not later than 8 weeks. treatment should be shifted to EFV. The
➢ If profound immune-suppression (such as CD4 count < 50 cells/ recommended regimen is: TDF/3TC/ EFV
mm3), ART should be started immediately within the first 2 weeks of or DTG
initiating TB treatment. ➢ Evaluate for treatment failure
➢ Patients who present with TB before initiation of ART the
preferred regimen are EFV containing first line regimen
➢ TDF+3TC+ EFV is preferred regimen for TB/HIV co-infected
adult regardless of pregnancy status.
➢ Efavirenz is a preferred drug in patients starting ART while on
Anti-TB treatment. When second line is initiated LPV/r is
preferable.

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The 3 I’s intervention for RVI - TB

A) Intensify TB case finding and ensure quality TB treatment


B) IPT
C) Infection control

I. Intensify TB case finding and ensure quality TB treatment

➢ All HIV positive clients should be informed about risk of developing active TB
and the advantages of being screened for TB.
➢ Asses sign and symptoms of active TB (may have atypical presentation) and
contact history with TB case
➢ If the evaluation shows no TB, children should be offered IPT, if no
contraindications, regardless of their age.
➢ Diagnosis of TB is challenging in HIV positive individuals, especially when the
stage of the disease is advanced.
➢ Thorough clinical evaluation, including exclusion of other OI, should be done.
Acute bacterial pneumonia or PCP may occur in patients with underlying
tuberculosis and patients should therefore be reevaluated for tuberculosis,
particularly if respiratory symptoms persist after treatment.

Clinical manifestations:
➢ Variable, depending on CD4 count
➢ In early HIV - TB presents in a typical manner
➢ In late stages of HIV, when CD4 is <200, a primary TB - like pattern with
atypical clinical & CXR findings are common
✓ Extra-pulmonary and disseminated disease is more likely (70%)
✓ Common extrapulmonary sites are: LNs, Pleura, Pericardium, CNS, GI,
Kidney, Bone.
➢ TB IRIS: Paradoxical or Unmasking type

Diagnosis and IX

➢ “TB suspect” is defined by one or more of following:


✓ Cough > 2 weeks
✓ Constitutional symptoms (fever, weight loss, night sweats, contact history)
✓ CXR suggestive of pulmonary TB
➢ GeneXpert Test (XPert MTB/RIF Test) is the preferred initial diagnostic test
✓ Recommended as an initial diagnostic test for all presumptive TB cases
(individuals wih TB symptoms) among HIV infected people.
✓ One sputum sample for the facility which have Xpert test and two
samples for sample referring facilities
✓ Should be used rather than conventional microscopy, culture and drug
susceptibility testing (DST) as the initial diagnostic test in adults and
children suspected of having HIV-associated TB or multidrug resistant TB.
✓ It is also a preferred initial test for CSF specimens if TB meningitis
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✓ May be used as a replacement test for usual practice (including


conventional microscopy, culture or histopathology) for testing specific non-
respiratory specimens (lymph nodes and other tissues) from patients
suspected of having extra pulmonary TB.
➢ AFB microscopy (2 spot tests with in 1 hour): if access to XPert MTB/RIF test
is limited.
➢ CXR
✓ Early HIV
• typical adult TB features (with upper-lobe infiltrates/cavitation,
no significant LAP or pleural effusion)
✓ Late HIV → Atypical clinical & CXR findings are common
• Lower/middle lobe opacity, little or no cavitation, interstitial /
milliary pattern, adenopathy (hilar, paratracheal), Pleural/
Pericardial effusion
• CXR MAY BE NORMAL
➢ Sputum culture: In patients with XPert negative results, sputum culture may be
indicated. Culture is the gold standard

Diagnosis of extra-pulmonary tuberculosis in HIV positive

➢ Extra-pulmonary tuberculosis is more HIV-related than pulmonary TB.


➢ The accurate diagnosis of extra-pulmonary tuberculosis is complex and difficult,
particularly with limited diagnostic capacity. Therefore, it is important to have
high-index of suspicion and critically evaluate through clinical algorithms.
➢ If available, do organ specific investigations.

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Algorism for Diagnosis of RVI - TB;


1
Presumptive TB is defined as having symptom and signs consistent with TB;
mainly persistent cough of two or more weeks (or cough of any duration if HIV
positive).
2
For patients in whom “HIV test is not done” at time of TB evaluation, Xpert test
may be the initial test if the clinician has strong clinical suspicion of HIV
infection or if the patient possesses risk behavior to acquire HIV infection.
3
Liquid specimens from EPTB site (in particular CSF) may be subjected to Xpert
test without additional processing.
4
Xpert test is preferred test to examine presumptive TB patients identified at
facility where the machine is available.
5
Broad spectrum antimicrobials, excluding fluoroquinolone or anti-TB drugs is to
be given for 10-14days.
6
RR-TB result in patients considered to be low risk for MDR-TB warrants DR-TB
risk re-assessment and a repeat Xpert test on fresh specimen, and if result
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shows RR-TB again; link the patient to TIC for Second line TB treatment; but
if the repeat test result identifies TB but not RR-TB, initiate first line TB
regimen as bacteriologically confirmed susceptible TB at TB clinic.

☛ Antibiotic trial: has a role to treat concomitant bacterial infection for


people living with HIV having cough or serious illness, but not helpful in
the diagnosis of TB in HIV positives.

Table: Extra pulmonary TB diagnostic approaches in HIV positive patients


Type of TB Evidences Strongly Suggestive of EPTB Investigations and recommendations
Lymph Node TB ➢ ≥ 2cm in size ➢ LN Aspirate for AFB has 85% yield
➢ Asymmetrical / localized ➢ If not possible to do FNAC of LN,
➢ Painless swelling start anti-TB.
➢ Firm/ fluctuated
➢ Cervical location
➢ patient with weight loss, night sweats,
fever
Pleural effusion ➢ Unilateral effusion Start anti-TB ASAP.
➢ Pleural fluid analysis shows;
✓ Clear and straw colored
✓ Clots on standing in a tube without
anti- coagulants
✓ Protein >30g/L & >50% lymphocytes
➢ Patients with weight loss, night sweats,
fever, or evidence of TB elsewhere
Tuberculosis ➢ Patients with weight loss, night sweats, ➢ Admit patient, start anti-TB with
Meningitis fever steroids ASAP.
➢ CSF is clear with high protein, low ➢ Start treatment for cryptococcal
glucose and lymphocytes meningitis based on clinical or lab
➢ Cryptococcal antigen (or Indian Ink and evidences.
fungal culture) negative in CSF Evidence ➢ Note: GeneXpert test has to be
of TB elsewhere conducted on CSF specimen as an
initial diagnostic test as much as
possible.
Pericardial Effusion ➢ Hemodynamically significant pericardial ➢ CXR, Echo or chest ultrasound;
effusion, often with pleural effusions, Lung pericardiocentesis, and pericardial
fields clear and intra-thoracic biopsy; routine TB Workup.
lymphadenopathy. ➢ Start anti-TB ASAP
➢ Usually patients with weight loss, night
sweats, fever.
➢ N.B. 90% of Pericardial Effusions in HIV
positive patients in high-TB burden areas

Disseminated TB
is due to TB.
➢ Patients with weight loss, night sweats,
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fever and cough critically ill)


➢ Abnormal CXR (which can include miliary
pattern)
➢ Large spleen/liver, Anemia
TB of the Spine Pain over localized area, children/ adolescents ➢ Spinal imaging (e.g. X-Ray, MRI)
- often thoracic vertebrae. Adults: frequently ➢ FNA of vertebral lesions and/or
lumbar vertebrae. paraspinous abscesses when feasible.

II. TB prevention with IPT (isoniazid preventive therapy)

➢ IPT is the use of Isoniazid to sterilize (prevent reactivation) latent TB infection.


➢ Screening for exclusion of active TB in HIV infected persons is the single most
important step that should precede the decision to initiate IPT.
➢ The dose of INH is 300mg/day for adults and 10mg/kg for children for 6
months.
➢ It is also desirable to provide pyridoxine (vitamin B6), 25mg/day, to prevent
INH-induced peripheral neuropathy.

TB Preventive Therapy (TPT):

➢ TPT is recommended for the following priority populations in Ethiopia:


✓ Adolescents and adults living with HIV who are unlikely to have
active TB based on symptom and/or chest radiography screening.
✓ Children 12 months or older who are living with HIV and are
considered unlikely to have active TB on an appropriate clinical
and/or chest x-ray evaluation.
✓ Infants younger than 12 months who are living with HIV and who
have been exposed to an index PTB case and are unlikely to have
active TB on an appropriate clinical and/or radiologic evaluation.
✓ HIV negative children and adolescents (< 15 years of age) who are
household contacts of a bacteriologically confirmed pulmonary TB
case after active TB is ruled out based on appropriate clinical
and/or radiologic evaluation.
✓ Patients initiating anti-TNF therapy, receiving dialysis, preparing for
organ or hematologic transplant and patients with silicosis after
excluding active TB disease.

Contraindications of IPT;
➢ Individuals with any one or more of the following conditions should not receive
IPT:
✓ Symptoms compatible with tuberculosis even if the diagnosis isn’t yet
confirmed.
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✓ Active hepatitis (chronic or acute)


✓ Regular and heavy alcohol consumptions
✓ Prior allergy or intolerance to isoniazid
✓ Symptoms of peripheral neuropathy

NB: Past history of TB and current pregnancy should not be contraindications


for starting IPT.

National policy:
☛ IPT should be administered at enrolment to HIV care after ruling out
active TB.
☛ IPT is to be administered once and should not be repeated unless there
is strong indication on its benefits which is to be decided by senior
physician.
☛ IPT should be administered only for 6 months.
☛ IPT should not be administered right after completing full course of TB
treatment
☛ IPT can be administered for patients who had history of TB treatment
before 3 years.

Follow-up of patients on IPT


➢ Patients should be given monthly supply of Isoniazid for the first 3 months and
3 months’ supply for the remaining months.
➢ At each follow-up visit assess;
✓ Adherence to treatment and educate client
✓ Drug toxicity.
✓ Signs and symptoms of active tuberculosis or other OI.
✓ Stop IPT if active TB is diagnosed and to immediately start anti-TB.

Treatment interruption management


➢ IPT is said to be completed if a patient completed the full course of therapy
within 9 months period (i.e. the six months doses should be finished in nine
months’ time).
➢ If the client discontinues treatment for a period of < 3 months: Resume the
same course by adding for the missed doses at the end.
➢ If the client discontinues treatment for a period of > 3 months: Re-initiate new
course of IPT for 6 months.

Repetition and prolongation of IPT:


➢ Repeating IPT after the first cycle of IPT or the provision of IPT after
completion of full course of TB therapy is not recommended in Ethiopia.

Provide HIV testing and counseling to presumptive and


confirmed TB patients
➢ Among TB-HIV co-infected patients, other OIs are significant causes of
morbidity and mortality even with a successful treatment of TB, necessitating
routine HIV testing and counseling to all TB patients.
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Presumptive treatment of TB for people living with HIV


➢ To prevent the death of people with HIV in situations where expedited
diagnosis of TB is not possible or feasible due to the clinical condition of the
patient or limited access to TB diagnostic services.
➢ No case definition for presumptive TB.
➢ WHO algorithms include initiation of TB treatment for people with HIV in
peripheral facilities based exclusively on clinical suspicion (without TB
investigations) for seriously sick patients (with respiratory distress) based on the
judgment of the clinician.
➢ However, every effort should be made to confirm the diagnosis of TB after
initiation of presumptive treatment and that treatment should be stopped only if
there is bacteriological, histological or strong clinical evidence of an alternative
diagnosis.

Introduce HIV prevention interventions for presumptive and


confirmed TB patients
➢ All clients attending TB clinics should be screened for STI using a set of
simple questions.
➢ Those with symptoms of STI should be treated or referred to the treatment
providers.
➢ Condoms should be made available in TB clinics.

Infection control

➢ People living with HIV are at high risk of acquiring TB in health care facilities
and congregate settings.
➢ Each health care facility should have a TB infection control plan for the facility
that includes administrative, environmental and personal protection measures to
reduce the transmission of TB in health care and congregate settings and
surveillance of TB disease among workers.

Summary of recommendations for key actions of infection control


☛ Taking Administrative, Health worker and care provider, Environmental
and personal level protective measures
☛ Provide HIV testing and counseling to presumptive and confirmed TB
patient
☛ Presumptive treatment of TB for people living with HIV
☛ Introduce HIV and other STI prevention interventions for presumptive
and confirmed TB patients
☛ Provide CPT for HIV positive TB patients
☛ Ensure HIV prevention, treatment and care for HIV positive TB patients

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MDR (Multidrug-resistant) TB and HIV


➢ Xpert MTB/RIF is the preferred test where possible, since this it is more
sensitive for detecting TB among people with HIV and rapidly detects rifampicin
resistance, thus greatly shortening the time to diagnose and treat MDR-TB.
➢ The burden of MDR-TB can be reduced by strengthening HIV prevention,
improving infection control and collaboration between HIV and TB control
activities, with special attention to the groups at the highest risk of MDR-TB
and HIV infection, such as people who inject drugs and those exposed in
congregate settings.

5.6.1.2. Pneumonia in RVI patient

1. Bacterial pneumonia

➢ Bacterial pneumonia tends to be more severe and recurrent as the CD4 counts
drops significantly.
➢ Pneumonia can also concomitantly present with sinusitis and/or bacteremia.
➢ If not treated promptly, extra pulmonary complications like empyema,
meningitis, pericarditis, hepatitis and arthritis can follow.
➢ Management is the same as non-RVI patients (for more click here →
Pneumonia (የሳንባ ምች))

2. Pneumocystis pneumonia (PCP)

➢ Caused by Pneumocystis jiroveci, formerly known as pneumocystis carini


pneumonia, classified as a fungus but also have characteristics of protozoa.
➢ It frequently causes pneumonia among immuno-compromised individuals.
➢ It commonly occurs when patients have significant immune suppression (CD4 <
200cells/mm3 or CD4 percentage < 14%).

Clinical manifestation
➢ Typical have an insidious (sub-acute onset over 2 to 4 weeks) onset of low-
grade fever, dry cough, fatigue and progressive dyspnea exacerbated by
exertion.
➢ Patients will have an increasing tachypnea, tachycardia and cyanosis as the
disease progresses.
➢ Physical examination reveals fever, tachypnea, tachycardia and scattered rales
in the lungs but examination of the lungs can appear normal in some patients.
➢ In children highest incidence is seen between 2-6 months of age and is
characterized by abrupt onset of fever, tachypnea, dyspnea and cyanosis.
➢ Due to non-specific presentation, PCP should always be considered in those
patients with evidence of moderate to severe immunosuppression who come up
with cough, progressive dyspnea or fatigue.

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➢ Clinical Dx; presumptive diagnosis of PCP is based on clinical judgment


➢ Chest X-ray: a perihilar interstitial infiltration with tendency to spread outwards
is Typical finding. Can be normal in 20% of patients.

Picture; Bilateral interstitial infiltrates beginning in the perihilar regions (ground


glass appearance)

➢ Culture: definitive diagnosis of PCP. Induced sputum sample using special


stains like Giemsa or methylamine silver stains, but these tests are not
routinely done in Ethiopia.

Treatment
➢ Oxygen should be given in moderate and severe cases.

First line:
➢ Cotrimoxazole, 960mg (15-20mg/kg/day), P.O/IV, TID/QID for 3 weeks
✓ Give the same medicine IV if the patient is not able to swallow the
medicine and shift orally when tolerable.
✓ Close monitoring is necessary during the initial 5 days of treatment and if
patient grows sicker, administration of oxygen is useful.
✓ In severely ill patients with marked respiratory distress and extensive
chest X-ray findings prednisolone has to be given simultaneously
✓ Toxicity of co-trimoxazole, like skin rash, bone marrow suppression,
hepatitis and renal failure can be troublesome in some patients with
advanced HIV disease and requires close monitoring. SJS (Steven
Johnson syndrome) may occur if the patient is allowed to take the
medicine after the development of rash.
✓ Secondary prophylaxis after completion of the course of treatment with
CPT should be continued.
Alternative:
➢ Clindamycin+ Primaquine or Dapsone for 3 weeks
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✓ Clindamycin, 600 mg BID (300-450mg P.O., TID) for 3 weeks PLUS


✓ Primaquine, 30mg base P.O, daily (15 mg BID) for 3 weeks.
OR
✓ Clindamycin 600 mg QID, for 3 weeks plus
✓ Dapsone 100 mg daily for 3 weeks.
OR
✓ Trimethoprim, 20mg/kg/day, P.O, QID for 3 weeks PLUS
✓ Dapsone, 100mg P.O., daily for 3 weeks
OR
✓ Pentamidine Isethionate, 4mg/kg I.V. daily for 3 weeks. It should be given
to those who fail to tolerate the above regimen.

N.B.
☛ Typically, a mild rash with fever develops 7 to 10 days after initiation of
therapy.
☛ Bone marrow suppression may occur, and CBC monitoring is useful.
☛ Possible hepatotoxicity and nephrotoxicity may also be evaluated at the
3rd week of therapy.
☛ Consider spontaneous pneumothorax in patients with sudden
deterioration in clinical condition.

Adjuvant treatment
➢ Corticosteroids → Indicated if SPO2 <90%, In the absence of pulse oximetry,
clinical judgment should be used to select moderately to severely sick patients
who benefit from corticosteroids.
✓ Prednisolone 40mg BID (i.e. 80 mg) for 5 days, then 20mg BID for 5
days, then 20mg daily until completion of intensive co-trimoxazole therapy
(for 11 days). No tapering from the 20 mg dose is necessary.
✓ For severe PCP in children: prednisolone 2mg/kg per day for the first 7 -
10 days followed by a tapering regimen for the next 10 - 14 days.

Pregnancy considerations
➢ The management and the prophylaxis for pregnant is similar to non-pregnant
mothers.
➢ TMP-SMX is the preferred drug in pregnant. However, be aware of the
theoretical risk of teratogenicity in the first trimester with the use of TMP-SMX.
➢ Aerosolized pentamidine or oral atovaquone can be used as alternative than
discontinuing chemoprophylaxis in the first trimester

3. Lymphoid interstitial pneumonitis (LIP)

➢ One of the most common chronic lower respiratory conditions occurring in up


to 25% of children with HIV/AIDS

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➢ Ranges from asymptomatic disease with isolated radiographic findings to


bullous lung disease with pulmonary insufficiency.
➢ Symptomatic children present with insidious onset of tachypnea, cough, and
mild to moderate hypoxemia with normal auscultatory findings or minimal rales
or wheezing.
➢ Progressive disease is accompanied by digital clubbing and symptomatic
hypoxemia.
➢ Associated physical findings include generalized, hepatosplenomegaly and
parotid enlargement.

Diagnosis
➢ Usually based on clinical examination findings, diffuse bilateral reticulonodular
infiltrate on X-ray with mediastinal lymphadenopathy.
➢ It is important to exclude tuberculosis and other infectious etiology.

Treatment
➢ Symptomatic treatment (hydration, oxygen).
➢ Antibiotics: if there is a superimposed bacterial infection.
➢ Bronchodilators: may be helpful in mild to moderate disease.
➢ Corticosteroids: reserved for children with significant hypoxemia and symptoms
of pulmonary insufficiency. Give prednisolone 1- 2 mg/kg/day for 6 - 8 weeks
and then taper as tolerated.

5.6.2. Gastrointestinal (GI) opportunistic diseases

➢ GI OIs commonly manifest with diarrhea, nausea and vomiting, dysphagia and
odynophagia among others.
➢ Most common causes among HIV infected are Isospora belli, cryptosporidium,
shigella and salmonella, CMV etc.
➢ A scenario of multiple concurrent GI infections is fairly common.
➢ A number of drugs with similar effects can pose challenges in differential
diagnosis.
➢ Infectious OI
✓ Candida
✓ Bacterial
✓ HSV
✓ EBV
✓ CMV
➢ Non- Infectious
✓ Angular chelitis
✓ Malignancies (kaposi’s sarcoma/KS/, lymphoma)
✓ Aphthous ulcers
➢ Oral – candidiasis, aphthus ulcer, kaposi’s sarcoma, gingivitis, periodontitis,
oral hairy leukoplakia
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➢ Esophagus – esophagitis due to candida, CMV, HSV, KS

The general principle of managing GI OIs


✓ Identifying and treating the specific offending agent and
✓ Providing supportive care to monitor situations such as fluid loss.

5.6.2.1. Candida infection

Dysphagia and odynophagia

➢ Dysphagia (difficulty in swallowing) and odynophagia (painful swallowing) are


symptoms of esophagitis occurring at advanced stages of AIDS.
➢ They are usually caused by candida, HSV, CMV, and aphthous ulcers.
➢ As well as a sign of severe immunodeficiency, esophagitis also seriously
impairs the patient’s nutritional status. Therefore, prompt diagnosis and
treatment are mandatory to avert nutritional complications and inability to
swallow prescribed medications.
➢ Children will present with reluctance to eat, excessive salivation, or crying while
feeding.
➢ If thrush is associated with dysphagia, odynophagia, and/or retrosternal pain,
consider esophageal candidiasis but this can also occur in the absence of oral
thrush.

Table: Candida Infection management


First line Alternative Duration
Oropharyngeal ➢ Fluconazole 100-200 mg ➢ Posaconazole 400 mg PO BID on 7 - 14 days
candidiasis PO, daily (3mg/k/day in day 1, then daily or
children) or ➢ Miconazole buccal tablets 50 mg PO
(oral trush ➢ Itraconazole 200 mg PO daily or
may occur in daily or ➢ Clotrimazole troches 10 mg PO five
> 90% of ➢ ketoconazole 200 mg BID times daily or
HIV/AIDS (3-6mg/kg/day daily in ➢ Nystatin 5 mL (100,000 units/mL)-
patients in children) swish and swallow 4 or 5 times daily
any time)
Esophageal ➢ Fluconazole 100 - 400 mg ➢ Voriconazole 200 mg PO or IV twice daily or 14 - 21 days
candidiasis PO/IV daily or ➢ Posaconazole 400 mg PO BID on
➢ Itraconazole 200 mg PO day 1, then daily or
(majorly an daily ➢ Other azoles or
extension of ➢ Caspofungins or
oral trash but ➢ amphotericin B
not always)
Vulvovaginal ➢ Fluconazole 150 mg PO, ➢ Itraconazole 200 mg orally daily for 3 3 - 7 days
candidiasis stat or
➢ Topical azoles (e.g.
- 7 days
➢ Boric acid 600 mg vaginal
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miconazole vaginal pessary) suppository once daily for 14 days


for 3 - 7 days for azole refractory candidiasis
➢ Severe or recurrent vaginitis: oral
fluconazole (100–200 mg) or topical
antifungals for ≥7 days

☛ Risk of recurrence after completing treatment may be high.


☛ If the patient is on ART, s/he should be investigated for treatment
failure.
☛ Take necessary precautions regarding drug interactions especially with
ketoconazole.
☛ Patients may need hospital admission for supportive care till the
oesophageal symptoms improve and necessary long-term treatments are
started.
☛ If diagnosis suggests HSV esophagitis use acyclovir 400mg po 5 times
daily for 14 to 21 days.

Prevention
➢ Administration of ART and immune restoration is an effective means to prevent
disease.
➢ ART failure should be investigated if there is recurrent infection.
➢ Routine primary prophylaxis is not recommended.
➢ Secondary prophylaxis or chronic suppressive therapy is not also recommended
unless frequent or sever recurrence, if used (Fluconazole 100 mg PO once
daily for oral/esophageal and 150 weekly for VVC), discontinue therapy if CD4
count >200 cells/mm3.

Pregnancy
➢ Pregnancy upsurges the risk of vaginal colonization with Candida species.
➢ Topical therapy is preferable for treatment of oral candidiasis in pregnancy, but
is essential for vulvovaginal candidiasis, especially during the first trimester.
➢ Chemoprophylaxis using systemically absorbed azoles against oropharyngeal,
esophageal, or vaginal candidiasis should not be initiated during pregnancy or
should be discontinued in women who become pregnant.

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5.6.2.2. Aphthous stomatitis/ aphthous ulcer

➢ Unknown etiology
➢ Usually painful & self-limiting
➢ May interfere with swallowing.
➢ Look at image under physical examination (patient approach in RVI) section of
this chapter.
➢ Rx:
✓ General measures
• Oral hygiene
• Avoidance of exacerbating factors – Where possible, reduce
traumatic factors inside the mouth (eg, sharp/rough dental
restorations, braces). Avoid habits that cause trauma (eg,
biting cheeks or lips) and foods that seem to exacerbate the
process (Avoid spicy foods).
• Pain control – Topical anesthetics provide immediate
symptomatic relief of short duration;
o 2% lidocaine, may be applied directly to surface of
ulcers or used as a swish and spit
o Diphenhydramine liquid: 12.5 mg/5 mL; 5 mL swish
and spit
o Aluminum hydroxide, magnesium hydroxide, and
simethicone suspension: 5 to 10 mL swish and spit
• Control of secondary infection; Nystatin suspension (400,000
to 600,000 units) swish and swallow four times daily or
Clotrimazole troches (10 mg) four to five times daily
✓ Topical steroids (Triamcinolone oral paste)
• Triamcinolone oral paste; Press a small amount (about 1/4
inch) to the lesion at bedtime; a larger quantity may be
required for coverage of some lesions. For severe lesions,
may be used 2 or 3 times daily after meals.
✓ A short course of oral corticosteroids may be beneficial in patients with
severe Recurrent aphthous stomatitis that is not controlled with topical
therapies
• Prednisone, 20 to 40 mg, PO, daily for 4-7 days.

5.6.2.3. Necrotizing Gingivitis

➢ Inflammation of the gums


➢ Extensive and necrotic
➢ Tooth loss
➢ Anaerobic infection
➢ Treatment
✓ Amoxycillin 500mg PO TID for 10 to 14 days Plus
✓ Metronidazole 500mg PO TID for 10 to 14 days
✓ Debridement for severe cases

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5.6.2.4. Herpes simplex (HSV1)/Herpes Labialis/

➢ Shallow, clustered ulcers around oral and peri oral area are characteristic
➢ May be solitary and deep in the severely immunocompromised patient
➢ Usually painful
➢ DDx: aphthous ulcers
➢ NOTE: Vesicles are rarely seen in the mouth!
➢ Rx:
✓ Local antiseptics to avoid superinfection
✓ Acyclovir, 400 mg, PO, TID, for 1 week

5.6.2.5. Diarrhea in HIV patients

➢ Diarrhea is defined, as passing of > 3 loose or watery stools per day.


➢ It may be acute or chronic, persistent or intermittent.
➢ Diarrhea is among the most frequent symptoms of HIV disease.
➢ Delay in treatment can result in fluid loss and hemodynamic instability. Chronic
diarrhea may also lead to nutritional deficiencies and wasting.
➢ Risk of a bacterial enteric infections (including bacteremia risk) increases as
CD4 count declines, with the greatest risk in patients with CD4 counts <200
cells/mm3.

Causes of Diarrhoea in HIV patients

➢ Protozoal infection:
✓ Cryptosporidium species, Isospora belli, Microsporidium species,
Entamoeba histolytica, G. lamblia,
➢ Bacterial infection:
✓ Campylobacter, Shigella, and Salmonella species
➢ Toxin induced:
✓ E. Coli and Clostridium difficile
➢ Mycobacterial infection:
✓ M. avium complex, M. TB
➢ Helminthic infection:
✓ Strongyloides stercoralis
➢ Viral infection:
✓ CMV, HSV
➢ Fungal infection:
✓ Histoplasmosis, coccidioidomycosis, and penicilliosis, Candida species
(seldom a cause of diarrhoea)
➢ Non-infectious disorders:
✓ Kaposi’s sarcoma, lymphoma
➢ AIDS enteropathy:
✓ Direct cytopathic effect of HIV disease
➢ Drug Side effects:
✓ Antibiotics, ART

Laboratory evaluation
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➢ Stool microscopy for ova or parasite, inflammatory cells at least 3 times


➢ Modified AFB staining for cryptosporidium, isospora belli
➢ Stool culture when indicated (optional).

Management

➢ Fluid and electrolyte replacement, nutritional support → The most important first
step is correction of fluid loss. Depending on the severity of dehydration, ORS
or IV fluid therapy can be given. Patients with severe dehydration need to be
admitted for IV fluid administration.
➢ In children zinc 20mg per day for 10-14 days (10mg per day for infants <
6months of age) should be added
➢ If specific enteric pathogen is identified or strongly suspected on clinical
grounds, it should be treated accordingly

Empiric treatment of bacterial enteric infections


➢ Pending Diagnostic Studies: For patients with advanced HIV (CD4 count <200
cells/mm3 or concomitant AIDS-defining illnesses) and clinically severe diarrhea
(≥6 liquid stools/day or bloody stool and/or accompanying fever or chills);
and/or patients with bloody diarrhea but repeatedly negative stool results
especially with constitutional symptoms such as fever.

First line
✓ Ciprofloxacin 500–750 mg PO (or 400 mg IV), BID
Alternative
✓ Ceftriaxone,1 g, IV, daily or
✓ Cefotaxime, 1 g, IV, TID.

NB: Diagnostic fecal specimens should be obtained prior to empiric antimicrobial


therapy initiation; and antibiotic susceptibilities should be performed in settings
where microbiologic facilities are available to confirm and inform antibiotic choice
given increased reports of antibiotic resistance.

➢ The treatment duration depends on the expected pathogen and may generally
extend from 7–14 days for uncomplicated cases and 2 to 3 weeks for
complicated (bacteremia, recurrent infection and/or advanced AIDS)
➢ Hospitalize and use IV antibiotic therapy if marked nauseas, vomiting, diarrhea,
electrolyte abnormalities, acidosis, blood pressure instability, and/or when there
is a clinical judgment for severity of disease
➢ For patients with persistent diarrhea (>14 days) but no other severe clinical
signs (e.g., dehydration, blood in stool), antibiotic therapy can be withheld until
a diagnosis is confirmed.
➢ Prophylactic antimicrobial to prevent bacterial enteric illness is not usually
recommended, including for travelers.

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Table: Treatment of specific enteric pathogens


Agent CD4 Symptom Diagnosis Rx
E. hystolytica Any Bloody stool, Stool Metronidazole
colitis microscopy
Giardia
Cryptosporidium <150 Watery diarrhoea Modified AFB ART*
Isospora belli <100 TMP-SMX
Microsporidium < 50 Giemsa stain Albendazole
CMV <50 Watery/bloody Tissue biopsy Ganciclovir
diarrhoea,
colitis
*No specific treatment for Cryptosporidium but it will improve with immune restoration
following ART.

Symptomatic treatment
➢ In adults use anti-diarrhoeal agents Loperamide 4mg stat then 2mg after each
bowel motion or Diphenoxylate 5mg QID.
➢ Necessary caution should be taken to avoid anti- diarrhoeal agents in bacterial
or parasitic infectious colitis or enteritis, since toxic mega colon may occur.
➢ Patients with chronic diarrhoea will develop nutritional deficiencies of variable
severity; therefore, proper nutritional assessment and support are helpful.

Persistent Diarrhoea Management

➢ Empiric antibiotic Rx if 3 stool tests are negative and no blood in stool


✓ Cotrimoxazole or ciprofloxacin + metronidazole
✓ Consider albendazole for 2 wks
✓ Treatment of lymphoma, Tb, MAC, ….
➢ If no response consider ART to boost immunity (for HIV enteropathy and non
treatable OIs like Cryptosporidium)

5.6.2.6. Peri-anal problems

➢ A number of chronic or acute peri-anal problems commonly occur among


Patient’s living with HIV disease, particularly in advanced immunodeficiency.
These include recurrent peri-anal abscesses, chronic peri-anal fistula, peri-anal
herpes (severe, persistent and extensive), and peri-anal warts (sometimes large
with obstructive problems).
➢ Patients with peri-anal problems frequently go to local healers and come with
complicated situations.

Treatment of peri-anal abscess in adolescents and adults

➢ Can be easily diagnosed with DRE


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➢ Early treatment is mandatory to avoid extension to peri-anal abscess depending


on immunological status of patient and thus more serious morbidity.
➢ If surgical incision is required, it should be done promptly on first visit.
Otherwise, broad spectrum antibiotics such as Augmentin or alternatively
amoxicillin or ampicillin must be administered in sufficient dose for at least 10
days.
➢ Palliative care including Sithz baths and analgesics are also important.

Peri-anal and/or genital herpes

➢ Latent or active infection with HSV I and II are common in the general
population, and is usually mild in immune-competent persons.
➢ Severe cutaneous disease or visceral involvement is usually restricted to
patients with advanced immunosuppression with a CD4 count <100 cell/mm3.
➢ The lesions become extensive, persistent, severe and sometimes with bleeding.
➢ Unless thorough evaluation with regular inspection of genital and peri-anal
areas is done, patients very often don’t complain about genital lesions.
➢ The response to Acyclovir is gratifying if it is done in sufficient dose (400mg 4-
5 time/day) and sufficient duration (10 days to 2 weeks in moderately severe
or severe cases).
➢ There is risk of recurrence with severe immunodeficiency. In such cases repeat
treatment and put patient on chronic HIV care including ART.
➢ Herpetic oro-labial infection is treated the same way as ano-genital herpes
➢ The treatment of anal and genital warts is particularly frustrating when
they are large.
➢ Unlike other OIs, the response to ART is not satisfactory.
➢ Patients who have very well responded immunologically with ART continue to
suffer from the warts.
➢ Depending on the size, cauterization, podophyllin treatment and surgical
debulking, etc. may be tried.

5.6.3. CNS opportunistic diseases

➢ Neurological manifestations of HIV can occur at any time from viral acquisition
to the late stages of AIDS.
➢ They are varied and may affect any part of the nervous system including the
brain, spinal cord, ANS and the peripheral nerves.
➢ HIV affects the nervous system in 70-80% of infected patients.
➢ The effect may be due to direct effect of the virus, OIs and/or malignancies.
➢ For certain neurological manifestations, a single aetiology is responsible while
in others it is due to multiple causes.
➢ Most life-threatening neurological complications of HIV occur during the severe
immunodeficiency state and specific aetiological diagnosis in the Ethiopian
setting is often a major challenge.
➢ Diagnosis of neurological disorders in HIV in our setting depends on the
history and standard neurological examinations.
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Neurological complications in HIV patients may be due to:


➢ HIV (HIV encephalopathy)
➢ OIs (toxoplasmosis, crypotococcal meningitis)
➢ Neurosyphilis
➢ Malignancies (primary CNS lymphoma); and
➢ Drugs (e.g. EFV, etc.)

☛ Early in the course of HIV


✓ Aseptic meningitis
✓ GBS, CIDP
✓ Transvers myelitis
✓ Peripheral neuropathy
☛ Late stage HIV
✓ Diffuse processes (meningitis, meningoencephalitis)
• Cryptococcal, Tb, syphilitic, listeria, lymphomatous, aseptic
(HIV 1) meningitis
• AIDS dementia complex
✓ Metabolic encephalopathies

Focal Neurological Deficit in HIV infected people


✓ Toxoplasmosis
✓ Tuberculoma
✓ Brain abscess
✓ Progressive Multifocal Leukoencephalopathy (PML)
✓ Syphilis
✓ Cryptococcoma
✓ Primary CNS Lymphoma
✓ Stroke/ vasculitis
✓ Viral encephalitis (HSV, VZ)

5.6.3.1. CNS Toxoplasmosis

➢ Toxoplasmic encephalitis (TE) is caused by the protozoan Toxoplasma gondii


➢ Disease appears to occur almost exclusively because of reactivation of latent
tissue cysts in individuals with underlying immunodeficiency.
➢ Primary infection occasionally is associated with acute cerebral or disseminated
disease.
➢ Sero-prevalence varies substantially in different communities; in Ethiopia,
general prevalence is about 80%.

Clinical Manifestations
➢ Focal encephalitis with headache, confusion, fever and/or signs of FND (motor
weakness) → The most common clinical presentation of T. gondii infection
among patients with AIDS
✓ Focal neurological abnormalities may be present on physical examination,
and in the absence of treatment, disease progression results in seizures,
stupor, and coma.
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➢ may also present with non-specific headache and psychiatric symptoms.

Investigations and diagnosis


➢ Serologic test
✓ IgG antibodies → almost uniformly seropositive
✓ The absence of IgG antibody makes a diagnosis of toxoplasmosis unlikely
but not impossible.
✓ On the other hand, positive test or high titer for Ig-M would suggest a
more recent infection. IgM antibodies usually are absent.
✓ Quantitative antibody titers are not useful for diagnosis.

➢ Neuro-imaging (CT scan or MRI of the brain)


✓ Definitive diagnosis of CNS toxoplasmosis requires a compatible clinical
syndrome; identification of one or more mass lesions by CT, MRI, or
other radiographic testing; and detection of the organism in a clinical
sample.
✓ In the absence of imaging support, empirical treatment is justified when
patients present with FND and the CD4 count is < 200 cells μl.
✓ Failure to respond to conventional therapy, based on presumptive clinical
diagnosis within a week or two of initiation of therapy, suggests the
diagnosis to be unlikely.
✓ With empirical treatment for toxoplasmosis, nearly 90% of patients will
demonstrate clinical improvement within days of starting therapy.
✓ Radiological evidence of improvement is usual after 14 days of treatment.

Figure; CNS toxoplasmosis. A coronal postcontrast T1-weighted MRI scan demonstrates


a peripheral enhancing lesion in the left frontal lobe, associated with an eccentric
nodular area of enhancement (arrow); this is so-called ‘’eccentric target sign’’ which is
typical of toxoplasmosis.

Treatment

First line regimen in the Ethiopian context is:


✓ Cotrimoxazole (Trimethoprim/sulfamethoxazole) 80/400, 4 tablets, PO, BID,
for 28 days, followed by 2 tablets BID for 3 months.

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• In children 10mg of trimethoprim + 50mg of


sulfamethoxazole/kg/dose, BID for 28 days followed by
maintenance therapy at 50% reduced dosage for 3 months.
✓ Maintenance treatment (Secondary prophylaxis): use co-trimoxazole 960mg
daily for adults’ and in children.

Alternative regimen
I.
✓ Sulfadiazine, 1-2 gm PO QID for 6 weeks or 3 weeks after resolution of
lesion PLUS
✓ Pyrimethamine: loading dose of 200 mg stat, followed by 50-75 mg/day
for 6 weeks. PLUS
✓ Folinic acid (Leucovorin): 10-20 mg/d for six weeks

OR
II.
✓ Pyrimethamine and Folinic Acid (Leucovorin): (standard dose) PLUS
✓ Clindamycin: initially 200-400mg I.V. then 600 mg QID (300-900mg)

OR
III.
✓ Sulfadoxin Pyrimethamine, 1000mg/50mg, P.O., BID for 2 days, and then
one tablet/day for 6 weeks. PLUS
✓ Folinic Acid (Leucovorin): (standard dose) for 6 weeks
✓ Followed by Maintenance treatment with Pyrimethamine, 25mg/day PO,
daily

Chronic maintenance treatment (Secondary prophylaxis) for TE:


➢ Co-trimoxazole 960mg daily for adults.
➢ Discontinuing chronic maintenance therapy if: successfully completed initial
therapy, remain asymptomatic of signs and symptoms of TE, and CD4 count
>200 cells/mm3 for >6 months in response to ART.
➢ Reinitiate prophylaxis if CD4 count <200 cells/mm3

Other supportive measures


➢ Adjunctive corticosteroids should be used for patients with radiographic
evidence of midline shift, signs of critically elevated ICP and altered sensorium
or clinical deterioration within the first 48 hours of therapy.
✓ Dexamethasone 4 mg (0.15mg/kg/dose for children) QID is usually chosen
and is generally tapered over several days and discontinued ASAP.
➢ Anticonvulsants should be administered to patients with a history of seizures,
but should not be given routinely for prophylaxis to all patients with the
presumed diagnosis of TE. Careful attention needs to be paid to any potential
drug interactions.

Primary prophylaxis
✓ Cotrimoxazole, 960mg PO, daily
✓ Indications for Initiating Primary Prophylaxis: 391
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• Toxoplasma IgG positive patients with CD4 count <100


cells/mm3
✓ When to discontinuing primary prophylaxis:
• CD4 count >200 cells/mm3 for >3 months in response to
ART
✓ Indication for restarting primary prophylaxis:
• CD4 count <100 to 200 cells/mm3 (AIII)

Pregnancy considerations
➢ Pyrimethamine and sulfadiazine are considered safe in pregnancy.
➢ Pyrimethamine should better be avoided during the first trimester and sulfa
drugs (including Sulphamethoxazole, sulfadiazine) have a potential risk of
neonatal kernicterus upon exposures in late pregnancy though no clearly
convincing data yet.
➢ The use of TMP (TMP-SMX) in the first trimester should also be evaluated
against the potential risk

5.6.3.2. Cryptococcal meningitis

➢ Cryptococcal meningitis is particularly common in advanced immunodeficiency


(CD4 count generally <100/mm3).
➢ It is a major contributor to high mortality before and after ART is initiated
because of delayed presentation, together with poor availability and high cost
of its treatment.
➢ Most HIV-associated cryptococcal infections are caused by Cryptococcus
neoformans.
➢ Long-term steroid therapy, as well as other immunosuppressive medicines, is
also risks for cryptococal infection.
➢ Typically, infection is acquired by inhalation of the fungus into the lungs.
➢ Cryptococcus is found in most warm climate, and is not restricted to the
tropics.

Prevention of cryptococcal disease in people living with HIV


➢ The use of routine serum or Plasma cryptococcal antigen screening in ART-
naive adults followed by pre-emptive antifungal therapy if screening is positive
to reduce the development of cryptococcal disease, should be considered prior
to ART initiation:
✓ Where patients with a CD4 count less than 100 cells/mm3; and
✓ Where this population also has a high prevalence (>3%) of cryptococcal
antigenemia.

✓ The following algorithm or decision-making guide shows how to decide


whether a patient needs prophylactic fluconazole treatment to CrAg
screening positive and asymptomatic patients with CD4 count less than
100cells/ml.
✓ If the prevalence of cryptococcal disease is high in the locality (most
likely in our setups), testing at CD4 count less than 200cells/ml may be
preferred.
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✓ If the CrAg test is not available, prophylaxis might be warranted for


patients with low CD4 count (<100 to 200cells/ml) in high-risk areas (>3%
of cryptococcal antigenemia).

Fig; Decision-making guide for Cryptococcus screening

Clinical features
Sub-acute meningitis, with high mortality:

➢ In HIV-infected patients, cryptococcosis commonly presents as a sub-acute


meningitis or meningoencephalitis with fever, malaise, and headache.
➢ Headache increasing over days to weeks, nausea, seizures, confusion,
irritability, blurred vision, sixth cranial nerve palsy, papilloedema on retinal
exam are common.
➢ Classic meningeal symptoms and signs, such as neck stiffness and
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photophobia, occur in only 1/4th to 1/3rd of patients.


➢ Some patients experience encephalopathic symptoms, such as lethargy,
altered mentation, personality changes, and memory loss that are usually a
result of increased intracranial pressure, thought to result from impaired CSF
absorption, or yeast infection of the brain.
➢ Coma or a reduced level of consciousness is associated with a poor
prognosis.

Non- meningeal presentations of cryptococcosis include:


➢ Lung infections: pneumonia or chest pain and cough in a minority of patients,
but often no fever.
➢ Skin lesions and lymphadenitis: Disseminated disease is associated with
papular lesions with an umbilicated, centrally depressed area (similar
appearance to molluscum contagiosum), which can become ulcerated.

Complications
➢ Chronic extensive genital HSV
➢ Raised ICP (increasing headache, vomiting, and cranial nerve palsy)
➢ Hydrocephalus, blindness, dementia, and personality change can occur as
permanent sequelae.
➢ Cryptococcomas can develop in the brain, more commonly in patients who
are not immunocompromised.
➢ Coma, cerebral oedema, and death follow if it is untreated, usually due to
elevated ICP.

Investigations and diagnosis


➢ LP and CSF analysis
➢ Serology for cryptococcal antigens: If it is not possible or contraindicated to do
LP, serum cryptococcal antigen can be used for diagnosis.
➢ CXR to demonstrate the organism

Management

➢ Requires hospitalization and evaluation by physician.


➢ The treatment is aimed at suppressing fungal growth and preventing squeal
related to increased ICP.

Non-Pharmacologic
➢ Control of raised ICP: daily LP with withdrawal of 20-30ml of CSF
➢ Coma care (including NG tube feeding) if the patient is unconscious

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Pharmacologic
Phases of management: Induction for 2 weeks followed by consolidation for 8
weeks

Options Induction (2 weeks) Consolidation (8 weeks) Maintenance (or


secondary prophylaxis)
Option A ➢ (High dose) Fluconazole 600 mg Fluconazole 800 mg/day Fluconazole 200 mg
BID (In children 12mg/kg/dose (children 12mg/kg/day) daily (children
BID) 6mg/kg/day)
Plus
➢ Flucytosine, 25 mg/kg, PO, QID
Option B* ➢ Amphotericin, 0.7 - 1 mg/kg/day Fluconazole 400 - 800
Plus mg/day
➢ fluconazole 800 mg/day OR
➢ Flucytosine, 100mg/kg
☛ * If amphotericin used laboratory monitoring and pre-hydration is recommended.
☛ * If the patient has meningitis or pneumonia, treatment with a regimen containing
amphotericin is preferred provided that facilities allow appropriate monitoring (kidney
function and electrolytes).

➢ Minimize acute infusion reactions when amphotericin is given (e.g. Fever, chills,
headache, hypotension) by the following ways;
✓ Infuse the initial dose slowly over 3 - 6 hours.
✓ Prophylactic antipyretics or hydrocortisone should only be used in patients
who have previously experienced acute infusion reactions (and in whom
continued treatment with amphotericin is essential).

➢ Discontinuation of maintenance treatment (secondary prophylaxis): when


patients are stable and adherent to ART and anti-fungal maintenance treatment
for at least one year and have a CD4 cell count maintained at ≥ 200 cells/
mm3 (2 measurements 6 months apart).
➢ Restarting Maintenance Therapy:
o If CD4 count declines to ≤100 cells/µL

Management of elevated ICP:

➢ >90% of death s in the 1st 2 weeks and 40% of deaths in 3rd to 10th weeks
are due to increased ICP. Thus, it is a must to manage.
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➢ Daily serial LP should be done by drawing 20-30 ml of CSF based on


patient’s clinical response.
➢ Signs of ICP (headache, altered mental status, meningismus and changing in
hearing or vision) should be closely monitored, if possible opening pressure
should be measured.
➢ There is no role for acetazolamide, mannitol, or corticosteroids to reduce ICP.

Timing of ART initiation: Delay initiation of ART

➢ ART initiation should be deferred until there is evidence of a sustained clinical


response to anti-fungal therapy due to life-threatening IRIS risk and
➢ After 2-4 weeks of induction and consolidation treatment with amphotericin B-
containing regimens combined with fluconazole, or
➢ After 4-6 weeks of induction and consolidation treatment with high-dose oral
fluconazole regimen (four weeks with non-meningeal disease).
➢ NB: Corticosteroids should not be routinely used during induction therapy
unless it is used for management of IRIS

Poor prognostic signs

➢ Extra CNS manifestation (especially pulmonary)


➢ Altered mental status
➢ Low CSF WBC count less than 20cells/µL
➢ High CSF cryptococcal antigen titer

5.6.3.3. Peripheral neuropathies

➢ Among the most common causes of painful legs in HIV infection (due to
complication of HIV infection itself, of drug therapy, or of other metabolic or
organ dysfunction or nutritional deficiencies).
➢ Distal symmetrical sensory polyneuropathy is the most common presentation
but mono-neuropathies can also occur.
➢ The neuropathies associated with HIV can be classified as:
✓ Primary → HIV-associated.
✓ Secondary → causes related to medications (INH), OIs or organ
dysfunctions.

Diagnosis

➢ Diagnosis is almost always clinical → pain, tingling sensations, paresthesia or


numbness, depressed or absent ankle reflex, decreased sensitivity to different
modalities of sensation and in severe cases, difficulty in walking. The feet and
sometimes the hands are involved in symmetrical distribution.
➢ The diagnosis can be supported by electro diagnostic studies including
electromyography (EMG) and nerve conduction studies (NCS) when available.
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Treatment

➢ Avoid the offending agent if identified.


➢ Remove other drugs associated with peripheral neuropathy.
➢ Supplemental vitamin intake for all patients including concomitant administration
of pyridoxine with INH.
➢ Adjuvants for pain management (such as Amitriptyline, carbamazepine)
indicated for patients with pain and paresthesia.

Monitoring of events

➢ Recognize presence of peripheral neuropathy.


➢ Assess severity at each clinical visit.
➢ Avoid drugs causing neuropathy.

5.6.4. Cutaneous disorders related to RVI infection

➢ Early OIs manifestations of HIV infection frequently occur in the skin.


➢ Adverse drug reactions (e.g., Nevirapine reactions may be life-threatening) and
noninfectious conditions (e.g., neoplasm) or unknown causes also lead to the
skin disorders in HIV patients.
➢ Nevertheless, infections are commonly seen in clinical practice;

Clinical features
➢ Pruritus is the most common dermatologic symptom in HIV infected patients.
✓ It can be localized indicating primary skin lesion, or generalized that may
or may not indicate primary skin lesions.
✓ In many patient’s pruritus may be severe and may not be amenable to
available therapy.
✓ The most common skin conditions associated with pruritus in patients with
HIV include the following:
• Excessive dryness of the skin (Xerosis cutis)
• Eczemas like seborrheic dermatitis or contact dermatitis
• Folliculitis (may include S. aureus infection or hypersensitivity
to insects)
• Drug eruptions
• Scabies
• Intertrigo (Candida, tinea, herpes simplex)

Diagnosis
➢ In most patients, diagnosis of skin disorders with HIV disease can be
established by examining the lesions, clinically.
➢ However, as immune deficiency advances it may be useful to use
investigations such as biopsy to diagnose specific dermatosis or use staining
and culture to diagnose specific infections.
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Skin disorders in HIV disease

➢ Skin disorders in HIV patients can be due to infections, neoplasm, and


hypersensitivity to foreign agents including drugs, or to unknown causes.
Nevertheless, infections are commonly seen in clinical practice; refer to the
following table:

Table: Common skin infections in HIV disease


Infections Disease Clinical Presentations Treatment Remark
Bacterial Cellulitis Poorly defined Erythema. ➢ Amoxicillin 500 mg Mostly encountered
Pus and crust at the site TID for 14 days lower extremities and
plus signs of inflammation. or often unilateral.
➢ Erythromycin 500
mg QID if allergic
to penicillin.
Impetigo Erythematous small papules ➢ Topical antibiotics Usually a superficial
usually limited to few lesions ➢ Amoxicillin for lesion.
coalescing in to crusted extensive disease.
plaques.
Carbuncle Nodular Lesion with ➢ Cloxacillin 500mg Involves the trunk as
extensions to the deeper QID for 10 days. well as extremities.
Structure. Signs of
Inflammation present.
Viral HSV ➢ Painful vesicular lesion ➢ Acyclovir 400mg, If Chronic (> one
around mouth or PO, TID, for 10 month) patient will
genitalia. days. (In children benefit from immediate
➢ Recurrent and extensive, 20 mg/kg/dose ART initiation if not on
difficult to eradicate QID) ART
during advanced immune
deficiency.
HZV Painful and vesicular Acyclovir 800mg 5X ➢ When it involves
eruptions with dermatomal per day for 7 days. the eyes, it is a
distribution. When healed, (Monitor RFT). medical emergency.
scar will remain. ➢ Do not give
Acyclovir* if
duration is >72
hours.
Warts / Painless flat to raised warts Podophyllin, Premalignant and risk
verrucae over fingers or genitalia in Imiquimod, for cervical cancer.
advanced immune deficiency, Cryotherapy and
they tend to be multiple and Consult experts
exophytic.
Molluscum Umbilicated and raised facial May not require Contagious
Contagiosum lesions that tend to be very
big during immunodeficiency
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state.
Parasitic Scabies Pruritic lesions ranging from First line
infestation pinpointed erythematous ➢ Permethrin 5%, Thin films of cream applied
papules involving interdigital, to all areas of body from the neck down
axillae and groin areas to and is washed off after 8-14 hours. Repeat
varying degrees of the same dose after a week
hyperkeratotic plaques Alternative
associated with significant ➢ BBL (Benzyl benzoate Lotion), applied to
skin thickening and crusting. the entire body, neck to toe for 3 to 5
consecutive evenings. Bath should be taken
before the first and after the last
application.
Systemic:
➢ Ivermectin, 200µg/kg stat, for Norwegian
(crusted scabies) and resistant forms of
scabies. And it is ideal for institutional
outbreaks.
➢ Antihistamines (such as cetirizine 5 - 10
mg daily) are given for pruritus
➢ antibiotics such as cloxacillin are given for
bacterial superinfections
➢ Burrows are visible in mild infestations but
in crust scabies may not be evident leading
to misdiagnosis.
Fungus Dermatophyt Superficial causing ringworm ➢ Topical antifungal (such as ketoconazole
osis or athlete’s foot cream) for limited skin affected.
➢ Fluconazole for extensive lesion 100mg
daily for 10 days.
Oral Thrush White plaques on the buccal ➢ Miconazole gel 2% apply BID
mucosa including the ➢ Fluconazole 100 mg daily for 10 for
tongues that can be scraped recurrent or oropharyngeal thrush.
off leaving red base. Can be
associated with candida
paronychia or intertrigo.
Deep Fungal Presentation varies from ➢ Disseminated Cryptococcus can be
infection fungating nodules and confused for Molluscum contagiosum.
tumors to ulcers and diffuse ➢ Treat with amphotericin induction and/ or
papulonodular disease fluconazole maintenance.

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5.6.4.1. varicella-zoster (Chicken Pox) /ጉድፍ/

➢ Varicella virus causes two distinct syndromes in humans:


1. Chicken pox → a primary illness, which most often occurs in children and is
relatively benign
2. Herpes zoster → a second distinct syndrome, which occurs in older adults
or immunocompromised hosts and is due to reactivation of the dormant virus
in the nerves. Herpes zoster causes significantly intense and sometimes long-
standing pain. Herpes zoster in a young person is highly predictive of HIV
infection and is a WHO clinical stage 2 conditions.

Clinical features of chicken pox


➢ Prodrome of fever, malaise, nausea, “flu-like” illness. 2 - 5 days later a
generalized, itchy rash appears.
➢ Rash → Crops of papules-vesicles, then crusted lesions appear all over,
sparing the palms and soles.
➢ Lesions co-exist in different stages of progression; i.e. new papules appear
when older lesions are already crusted. Intense itching occurs.

Complications
➢ Complications are more often if HIV acquire as adults, and particularly in
pregnant.
➢ After the introduction of vaccine, the number of complications in children
dramatically declined, although the most common complication has remained
bacterial superinfections;
➢ complications included
✓ Pneumonia
✓ Skin and soft tissue infections (42 %)
✓ Dehydration (11 %), and
✓ Neurologic complications (9 %) → Encephalitis, Reye syndrome
hepatitis or haemorrhagic syndromes
➢ Varicella complications acquired during pregnancy before 28 weeks’ gestation,
will cause congenital abnormalities in the child (also called congenital varicella
syndrome). If acquired around the time of birth, it can cause neonatal varicella,
which carries a high rate of pneumonia and other complications.

Treatment
➢ Start treatment ASAP ideally in < 24 hours after symptom onset.
➢ For oral treatment, the value of starting after 24 hours is not well established

Anti-viral therapy
➢ Acyclovir and its analogues (valacyclovir, famciclovir) are effective for the
treatment of primary varicella in both healthy and immunocompromised hosts
➢ It is recommended for all HIV-positive adults.
➢ D u r a t i o n o f t r e a t m e n t i s f o r 7 - 1 0 d a y s . Consider longer
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Drug options
✓ Acyclovir
• In adults including pregnant women:
o Acyclovir, 800mg, PO, 5 times daily for 7 - 10 days.
• In immunocompromised adults or those with disseminated
disease:
o Acyclovir, 10mg/kg, IV, TID for 7 - 10 days (high-
dose oral acyclovir, if no IV available).
Or
✓ Valacyclovir, 1 g, PO, TID for 7 to 10 days o r
✓ Famciclovir, 500 mg, PO, TID for 7 to 10 days
N.B.
☛ For Extensive cutaneous lesions or visceral involvement:
✓ Acyclovir, 10 to 15 mg/kg/dose, IV, TID, until clinical improvement
✓ Switch to oral famciclovir or valacyclovir (preferred) or acyclovir
(alternative) to complete a 10 to 14 days course when formation of new
lesions has ceased and signs/symptoms of visceral infection are
improving

Supportive care
➢ The following general measures can be used for the symptomatic management
of rash and fever, and can also help reduce the risk of developing certain
complications:
✓ Antihistamines or calamine lotion are helpful for the symptomatic
treatment of pruritus.
✓ Paracetamol should be used to treat fever, particularly in children.
• Non aspirin NSAID’s can also be used. However, some
providers discourage NSAIDS because of the uncertain
association with streptococcal superinfection.
• Salicylates should be avoided since aspirin has been
associated with the onset of Reye syndrome in the setting of
a viral infection
✓ Fingernails should be closely cropped to avoid significant excoriation and
secondary bacterial infection.
✓ Secondary bacterial infections may require antibiotics.

5.6.4.2. Herpes zoster (shingles) /አልማዝ ባለጭራ

Clinical features
➢ Painful vesicular rash in a dermatomal distribution of a nerve supply that
does not cross the midline. Pain sometimes comes before the appearance of
the rash. Vesicles form in groups and progress to crusted lesions after a few
days.
➢ The rash is generally limited to one dermatome, but can occasionally affect
two or three neighboring dermatomes.
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➢ Some patients can also have a few scattered vesicles located at some
distance away from the involved dermatome.
➢ Most common areas: trunk, particularly the flanks, and forehead. Can involve
the eye and cause corneal scarring and blindness.
➢ HIV patients have more frequent multidermal involvement, involvement of the
trigeminal nerve, presence of systemic symptoms, and have a higher risk of
disseminated disease.
➢ Myelitis, meningitis, and encephalitis with headache, fever, neck stiffness,
altered motor and sensory function.
➢ Guillain-Barre syndrome.
➢ See pictures from physical examination section of Approach part of this
chapter above.

Complications
➢ Blindness due to corneal involvement.
➢ Post-herpetic neuralgia: chronic pain in the area where the lesions occurred
that can last for months to years after the acute episode.

Treatment

➢ The management of herpes zoster includes:


✓ Antiviral therapy → to hasten healing of cutaneous lesions and to
decrease the duration and severity of acute neuritis. Whether antiviral
therapy decreases the risk of post-herpetic neuralgia is unclear.
✓ Analgesia for patients with moderate to severe acute neuritis.
✓ Local lesion care with daily bathing with soap and water.
✓ Antihistamines or calamine lotion may be used to reduce itching

Choice of Antiviral agent


✓ Acyclovir: 800 mg 5 times daily for 7 days or
✓ Valacyclovir: 1g, PO, TID for 7 days or
✓ Famciclovir: 500 mg, PO, TID for 7 days

N.B
➢ Acyclovir is available in most setups of Ethiopia. Valacyclovir and Famciclovir
are preferred over acyclovir because of dosage frequency to increase
adherence but there is no clear difference in efficacy.
➢ Acyclovir and its analogues (Valacyclovir, Famciclovir) are dependent upon
renal function for clearance. So, follow up with RFT and dose adjustment is
needed in moderate to severe renal insufficiency.

Recommendations about antiviral therapy timing


1. ≤ 72 hours after onset

➢ Antiviral therapy should be initiated within 72 hours of clinical symptoms of


uncomplicated herpes zoster to maximize the potential benefits of treatment. 402
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➢ The benefit of antiviral therapy appears to be greatest in patients older than 50


years of age, in whom the pain of zoster generally persists longer. Although
the efficacy of antiviral therapy in patients less than 50 years of age has not
been as well studied, the risk of adverse events secondary to antiviral therapy
is very low.

2. >72 hours after onset

➢ Administer antiviral therapy after 72 hours if new lesions are appearing at the
time of presentation, as this indicates ongoing viral replication.
➢ However, the clinical utility of initiating antiviral therapy more than 72 hours
after the onset of lesions in immunocompetent persons is unknown.
➢ There is likely minimal benefit of antiviral therapy in the patient who has
lesions that have encrusted.

3. Immunocompromised hosts

➢ Antiviral therapy should be initiated in all immunocompromised patients with


herpes zoster, even if they present after 72 hours.
➢ Rapid initiation of therapy is particularly critical in the severely
immunocompromised patient, such as the organ transplant recipient.
➢ Immunocompromised hosts with disseminated zoster should be hospitalized for
IV acyclovir therapy.

Analgesia for acute neuritis


➢ Although antiviral therapy reduces pain associated with acute neuritis, pain
syndromes associated with herpes zoster can still be severe.
➢ Use the following agents for the treatment of acute neuritis.
✓ for mild pain → NSAID’s or paracetamol, either alone, or in combination
with a weak opioid analgesic (e.g. codeine or tramadol).
✓ For moderate to severe pain that disturbs sleep → stronger opioid
analgesics (e.g. oxycodone or morphine) may be necessary.

For Secondary bacterial infection


➢ Appropriate staphylococcal and streptococcal antibiotic coverage in addition to
antiviral therapy.
➢ Patients should also be counseled to contact their clinician if they observe
increased erythema, warmth, or purulence surrounding any lesions, which could
suggest secondary bacterial skin infection.

Adjuvant therapies
➢ Unless there is neuropathic pain or post herpetic neuralgia, For patients with
uncomplicated zoster, there is no role for adjuvant agents, such as gabapentin,
TCA (like amitriptyline), or glucocorticoids, in the acute setting.

Patient monitoring 403


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➢ Serial patient monitoring should include standardized pain measures and


frequent follow-up to assess efficacy in relief of symptoms

Recurrent zoster
➢ Patients with recurrent zoster should be treated with antiviral therapy using
similar a dose and duration as treatment of their initial episode.
➢ However, episodes of recurrent zoster are uncommon. Thus, viral cultures or
other detection assays (eg, antigen or DNA detection) if available, should be
performed since some patients (eg, those who present with recurrent herpes
simplex outside of the mouth or genital area) may be misdiagnosed as having
recurrent zoster.
➢ There are no data regarding the potential benefit of zoster vaccine in this
scenario.

Complicated zoster
➢ Certain immunocompetent patients with herpes zoster will present with ocular,
otic, or neurologic manifestations.
➢ Such patients may require IV and/or prolonged therapy.
➢ In addition, there may be a role for adjunctive glucocorticoids in certain
conditions.

A) Herpes zoster ophthalmicus


➢ a serious sight-threatening condition, has been linked to varicella zoster virus
(VZV) reactivation within the trigeminal ganglion.
➢ Patients can develop conjunctivitis, episcleritis, keratitis, and/or iritis.
➢ Early diagnosis and treatment is critical to prevent progressive corneal
involvement and potential loss of vision.
➢ For mild ophthalmic involvement, topical acyclovir, 3% eye ointment
applied into the eye every 4 hours should be given.
➢ The standard approach to herpes zoster ophthalmicus includes
✓ Oral antiviral therapy (acyclovir, valacyclovir, or famciclovir) to limit VZV
replication plus
✓ Adjunctive topical steroid drops to reduce the inflammatory response and
control immune-associated keratitis and iritis.
✓ Parenteral acyclovir (10 mg/kg, IV,TID for 7 days) should be administered
if the patient is immunocompromised or requires hospitalization for sight-
threatening disease.

B. Acute retinal necrosis


➢ For immunocompetent patients
✓ Acyclovir, 10 mg/kg, IV, TID, for 10 to 14 days followed by valacyclovir,
1g, PO, TID, for approximately 6 weeks.
➢ Such patients should be managed in conjunction with an ophthalmologist to
evaluate the need for intraocular therapy and/or vitrectomy.
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➢ In addition, empiric systemic glucocorticoids may be considered, especially if


there is decreased visual acuity secondary to inflammation or optic nerve
involvement.
✓ prednisolone, 1 mg/kg/day, PO and taper by 10 mg every 5 days.

C. Ramsay Hunt syndrome

➢ The major otologic complication of VZV reactivation, which typically includes


the triad of;
✓ Ipsilateral facial paralysis
✓ Ear pain, and
✓ Vesicles in the auditory canal and auricle.
➢ Management
✓ Valacyclovir 1g, PO, TID for 7 to 10 days (if not available use acyclovir)
PLUS
✓ Prednisone, 1 mg/kg for 5 days, without a tapering.
✓ In severe cases (eg, vertigo, tinnitus, or hearing loss), IV therapy can be
initiated, and the patient can then be transitioned to an oral antiviral agent
when the lesions begin to crust.

D. Neurologic complications

➢ Neurologic complications where viral replication likely plays an important role


(eg, symptomatic meningitis, encephalitis, and myelitis).
➢ Treatment
✓ Acyclovir, 10 mg/kg, IV, TID, for 10 to 14 days

E. Postherpetic neuralgia
➢ The diagnosis is typically made when pain persists beyond four months in the
same distribution as a preceding documented episode of acute herpes zoster
➢ Additional factors supporting the diagnosis are:
✓ Advanced age
✓ Severe prodromal pain with acute herpes zoster
✓ Severe preceding rash
✓ Distribution in trigeminal or brachial plexus dermatomes
✓ The presence of allodynia
➢ Management
✓ Tricyclic antidepressants (e.g. Amitriptyline), gabapentin, and
pregabalin are generally the drugs of first choice.
✓ Amitriptyline 25 - 50mg before bed for neuropathic pain and post-
herpetic neuralgia

Preventing transmission to others

➢ Varicella and zoster are vaccine preventable diseases caused by VZV (MMRV
vaccine) 405
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➢ VZV is transmitted from person to person by direct contact or by aerosolization


of virus from skin lesions.
➢ In general, VZV is much less transmissible from a person presenting with
herpes zoster than from a person presenting with varicella.
➢ Patients with localized zoster are not infectious before vesicles appear and are
no longer infectious when the lesions have re-epithelized.
➢ For those with active lesions, there are no specific precautions within the
community setting. However, patients should be counseled about the risk of
viral transmission to others. In addition, until the rash has crusted, patients
should be advised to:
✓ Keep the rash covered, if feasible, and to wash their hands often to
prevent the spread of virus to others.
✓ Isolation of the patient to avoid spreading the virus. Contact
should be avoided until all lesions are crusted over → Avoid
contact with pregnant women who have never had chickenpox or the
varicella vaccine, premature or low birth weight infants, and
immunocompromised individuals.

5.6.4.3. Pruritic papular eruption (PPE)

➢ Its prevalence ranges from 12 - 46% and it is uncommon in HIV negatives


(PPV of 82 - 87%, and may play role in diagnosing HIV).

Clinical presentation and diagnosis:

➢ Intensely pruritic, discrete, firm papules with variable stages of development


and predilection for extremities, though it can involve trunk and face.
➢ Excoriation results in pigmentation, scarring and nodules.
➢ In extreme form, eosinophilia and eosinophilic infiltrates of the skin are present.
➢ Severity of rash often correlates with CD4 count.
➢ Look at pictures under physical examination section from approach part of this
chapter above

Treatment:
➢ Topical steroid and oral antihistamines.
➢ If refractory (often), short course prednisolone may be used.
➢ ART is often effective.

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5.6.5. Kaposi sarcoma (KS)

➢ A multicentric neoplasm consisting of multiple vascular nodules appearing in


the skin, mucous membranes, and viscera
➢ AIDS defining malignancy. Can occur at any CD4 count
➢ Variants:
✓ AIDS related/ epidemic KS
✓ Endemic/ African
✓ Organ transplant related
✓ Classic
☛ Aetiology → HHV-8 or KS associated HSV
☛ Manifestation
✓ Pink /brown/ purple cutaneous and or mucosal papule or plaque.
✓ It can appear anywhere in the body and often is symmetric (skin/ mucous
membrane, GI, chest)
➢ Can occur as IRIS
➢ DDx
✓ Purpura, hematomas, angiomas, dermatofibromas, or nevi
✓ Bacillary angiomatosis, skin lymphoma, sarcoidosis, …
➢ Dx → biopsy
➢ Staging:

Good risk (stage 0) Poor risk (stage 1)


➢ Skin, LN, minimal mucosa ➢ Extensive lesions, associate
involvement edema or ulcer
➢ CD4 > 200, ➢ CD4 < 200
➢ No B symptoms ➢ B symptoms present
➢ No OI’s ➢ Presence of other OI
➢ Good performance status ➢ Poor performance status.
(Karnofsky >70)

Treatment

➢ ART
➢ Local therapy → cryotherapy, laser, intralesional vinblastin, local radiation
➢ Systemic chemotherapy → indicated for rapidly progressive, severe
lymphedema, pulmonary and other visceral involvement
✓ Regimen → adriamycin, beomycin, vincristin every 2-3 weeks for 6 cycle.
✓ Liposomal daunorubicin/doxorubicin, paclitaxel have better response rate

5.6.6. RVI - VL co infection


Refer from Leishmaniasis (click here → RVI - VL co infection)

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Chapter 6; Stroke (የጭንቅላት ደም ስር በሽታ፣ እስትሮክ)

Chapter 6; Stroke (የጭንቅላት ደም ስር


በሽታ፣ እስትሮክ)
Dr. Mulualem. G

Clinical features and how to write hx of stroke patient


History

Pt’s may present with


o Right or left sided body weakness
o Failure to communicate
o LOC
If a known Hypertensive patient → ask the following on your hx
o For how long he/she was Diagnosed to have hypertension
▪ e.g a known hypertensive pt for the past 3 years or you can
say 5 years back he/she was told to have hypertension (you
can ask what was the presentation at that time and how Dx
was made… no need to write on your HPI)
o What medication he/she was taking… e.g he/she was on Amlodipine,
HCT, Enalapril... ask dose and frequency of each drug, advised to
stop alcohol and on salt restriction
o Adherent or not
o Where was the follow up and frequency (every month, every two
months….)
o How was his/her smx’s in between… improving, worsening or no
change at all… if not improving or worsening what was the reason
(non-adherence, wrong diagnoses…)
Ask handedness of the pt (Right or left-handed)
Speech area is in the dominant hemisphere. If there is derangement
of speech, the dominant hemisphere is high likely to be the affected
one.
90% of right-handed persons are left dominance and 50% of left-
handed persons are left dominant
Right or left sided body weakness (i.e. both upper and lower extremity
weakness of one side of the body)
It can be expressed as failure to use right/left upper and lower
extremities.
Sudden onset (maximal at onset) or progressive onset which worsen
until limb becomes flaccid/rigid based on the type of stroke
Happens while pt is awake and working his/her daily activities in
hemorrhagic stroke (e.g. failed to hold meal while trying to eat, failed
suddenly during farming etc.). Noticed while he/she awake from
sleep or happen on his/her bed time in ischemic stroke 408
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Starts from UL to LL or the reverse. Or may involve both upper and


lower extremities at a time to the extent s/he failed to stand or can’t
raise, flex, extend by him/herself
Speech disturbance → Broca’s or Wernicke’s aphasia which indicate MCA
involvement
Aphasia
Difficult to communicate or difficulty of understanding/ may
understand only gesture
There may be associated failure to swallow
If there is blurring of vision, decreased hearing ability in one or both
sides → PCA is involved
LOC, confusion
Vomiting → may precede LOC and it is a sign of increased ICP
Projectile, nonbilious, nonblood tingled, non-foul-smelling vomiting of
ingested matter/other, X-Y times per day
Face deviation to the opposite side or to the same side of weakness
To the opposite side of weakness → uncrossed hemiparesis/plegia
To the same side of weakness → crossed hemiparesis/plegia
Headache and neck stiffness
Globalized type of headache, relieving and aggravating factors
May be sudden and severe → ‘’the worst headache ever’’ in SAH
Abnormal body movement → indicates cerebellar involvement
Starts abruptly
With or without warning manifestations
Generalized/partial
With up rolling of the eyes and drooling of saliva
Followed by excessive salivation, bleeding from tongue (tongue bite),
urinary or fecal incontinence (observed by one of family members)
Finally, LOC → ask duration of LOC which is mostly less than 5
minutes
Remark; Previous history of seizure helps to rule out stroke mimics
Fecal or urine incontinence → indicates ACA involvement

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N.B
Hemorrhagic stroke Ischemic stroke
Gradual in onset→ progressive Maximal at onset → severe FND at the
worsening of smx’s onset
o Remark; except SAH in which No change in mentation
symptoms present begin No features of increased ICP
abruptly ICH present with Happens at rest or during sleep time → i.e.
gradual onset usually noticed in the morning
Associated with decreased level of RF that favors ischemic stroke include
consciousness (LOC) ✓ DM
+ve features of increased ICP → ✓ CHF (atrial fibrillation) resulting in
projectile vomiting, headache, cardioembolic stroke
papilledema on P/E ✓ Previous MI and PAD
Stroke happening at stressful
conditions and pt is awake like Embolic strokes occur often when patients
farming, sexual activity etc. are awake; the weakness is often maximal
HTN, High alcohol intake and smoking at onset and hardly progress thereafter; the
favors hemorrhagic stroke but can be neurologic deficits are often severe as the
RF for Ischemic stroke also. infarcts are very large; often follows TIA.
ICH are characterized by premonitory Thrombotic strokes start suddenly but
symptoms like headache; nausea and neurologic deficits are stuttering and
vomiting; onset is sudden with rapid progresses relatively slowly; often stroke
progression of neurologic features over occur during night while patients are asleep.
hours; often associated with loss of
consciousness; often occur during
strenuous activities

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Risk factors for stroke

Modifiable RF Non modifiable RF


HTN Old age
DM ✓ An increasing age is the most
Dyslipidaemia powerful risk factor for stroke.
Obesity and physical inactivity ✓ The incidence of stroke doubles
Alcohol intake each decade past 55 years of age:
Cigarette smoking Half of all strokes occur in people
✓ A major risk factor for CAD, stroke, older than 75 years.
and PAD
✓ It is an independent risk factor for Gender (M>F)
ischemic stroke in men and women of ✓ Men age 45 - 75 develop ischemic
all ages, and a leading risk factor of strokes at higher rates than women;
carotid atherosclerosis in men: 2-3 thereafter, stroke rates are higher in
times than non-smokers women
✓ Women has higher case fatality
TIA rates than men
Prior stroke
CHF (especially atrial fibrillation, VHD, Race → common in African Americans
DCMP and IE which predispose to cardio Previous vascular event like MI,
embolic stroke) embolism
✓ Atrial fibrillation, is the most common Genetic disorders like EDS and marfan
cause for cardio-embolic stroke, and it syndrome → increased risk of vascular
is a risk factor for future dissection to result SAH.
cardiovascular disease. Family hx
CAD, PAD
OCP use N.B ABCD2 score
Hyperlipidemia (atherosclerosis)
Anticoagulant therapy ABCD2 Score

Hypercoagulable states (SCA, PCV, A → Age > 60 1

protein S &C deficiency, antithrombin III B → BP ≥ 140/90 1

deficiency, SLE) C → Clinical smx like


Substance abuse like cocaine, ☛ Unilateral weakness------- 2

amphetamine ☛ Speech disturbance------- 1

Trauma → carotid or vertebral artery D → duration


dissection ☛ Lasting ≥ 60 minutes ---- 2
Spinal manipulation → vertebral artery 1
☛ < 60 minutes --------------
dissection
D → DM 1

Total 9

ABCD2 scores of ≥ 4 indicate a moderate to high


stroke risk and justify prompt hospital admission

➢ It is designed to identify risk of ischemic stroke in the first


seven days after TI
3 month rate of stroke can be calculated from the score

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Complication of stroke
Early complications

✓ Cxn due to immobility


▪ Infection like pneumonia
▪ Aspiration from LOC
▪ Pressure sore
▪ Painful shoulder
▪ Venous TE like DVT and PE
▪ UTI/constipation
✓ Cxn due to cortical brain injury
▪ Cerebral edema and hemorrhage
▪ Seizure
✓ Fall down injury during the attack

Late complications

✓ Contracture or spasticity
✓ Neurologic disability or paralysis like wheelchair dependent
✓ Epilepsy
✓ Aphasia
✓ Sleep disturbance
✓ Socioeconomic factor related to difficulty in involvement of daily activity and
permanent need of help from family members
✓ Depression/anxiety from prolonged immobility

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Sample history
Sample history of a patient from debark with Emergency ward DX of Right sided,
crossed, flaccid hemiplegia 2ry to ischemic stroke 2ry to uncontrolled HTN r/o
hemorrhagic stroke

Chief compliant
Failure to use right upper and lower extremities of 4 hr’s duration

HPI

This is a Right-handed, known hypertensive patient for the past 3 years on amlodipine to
be taken 10 mg po daily and Hydrochlorothiazide to be taken 25 mg po daily, advised to
stop alcohol and on salt restriction. He was Adherent for his medication with regular
follow up at debark general hospital every two to three months.
Currently presented with Sudden onset right sided body weakness of both upper and
lower extremities of 04 hours duration. The weakness happens on his bed time in which
he noticed while he awakes from sleep. It was maximal at onset involving both upper
and lower extremities at a time to the extent he failed to stand from sleeping position
and can’t raise, flex or extend his right-side extremities by himself.

Two hours before admission he experienced failure to communicate but he was able to
understand only gesture associated with face deviation towards the right side but no
LOC, vomiting or headache

While they were coming to our hospital by ambulance (approximately 30 minutes before
admission), he experienced single episode of sudden onset, generalized Abnormal body
movement together with up rolling of the eyes and drooling of saliva followed by
excessive salivation, bleeding from tongue and urinary incontinence (observed by one of
family members in the ambulance), Finally he loses his consciousness and awakes
approximately 3-4 minutes later.

For this, he visited debark general hospital where he was catheterized, glucose level
measured, put on intranasal oxygen, resuscitated with half bag of NS and referred to our
hospital for better investigation and management.
➢ No hx of DM (RF)
➢ No hx of Dyspnoea, orthopnoea, PND, palpitation (cardioembolic stroke from cardiac
causes)
➢ No hx of head trauma (RF, or DDX in SDH)
➢ No hx of Smoking or chronic alcohol intake (RF)
➢ No hx chat chewing or other drug use (cocaine, amphetamine… for females consider
OCP as hypercoagulable state)
➢ No hx of malar rash, photophobia or joint pain (SLE as RF)
➢ No hx of gum bleeding, epistaxis or bleeding from other sites (bleeding
disorder may be the cause for haemorrhagic stroke, don’t give heparin in bleeding disorders)
➢ No hx of intermittent claudication or leg swelling (DVT as
➢ No hx of chest pain cough or fever (pneumonia, PE as cxn)
cxn)
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➢ No hx of constipation (cxn)
➢ No hx of Ear discharge, tooth extraction, or sinusitis (brain abscess as DDX)
➢ No Similar hx of illness in the family, previous hx of similar illness or

transient weakness of extremities (TIA, Hemiplegic migraine)

Finally, he was admitted to our hospital ED carried by his families from


ambulance.

Physical examination (pertinent findings)

1 GA
➢ Face deviation
➢ LOC (decreased level of consciousness)
➢ Limb position → Externally rotated limb (in flaccid hemiparesis/plegia), internally
rotated limb (in spastic hemiparesis/plegia)
➢ Speech disturbance
➢ Cardio respiratory distress

2 Vital signs
➢ Irregularly irregular pulse → Atrial fibrillation
➢ HTN as RF, may be hypotensive
o Hypotension is associated with worsening of stroke; can be
associated with serious concomitant conditions like MI, aortic
dissection or sepsis.
o Hypertension is a normal response to stroke but malignant HTN
should be treated.
o Very high HTN may suggest ICH.
➢ Tachypnoea and tachycardia
➢ Febrile

3 HEENT
➢ Eye changes
o Retina → hollen horst plaque from amaurosis fugax (mono ocular
blindness due to occlusion of ophthalmic branch of carotid artery),
diabetic changes, Retinal emboli, hypertensive changes, arcus senilis
4 LGS
5 RS
➢ Chyne stocke breathing (deep and labored tachypnoea followed by
apnoea)→ due to hemispheric cerebral oedema
➢ Pulmonary edema
➢ Pneumonia features (from aspiration pneumonia or infection)

6 CVS
➢ Bruit over the carotid artery and other major arteries
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➢ Arrythmia (Abnormal pulse rhythm like irregularly irregular pulse from atrial
fibrillation)
➢ CHF Features or Murmur (like MR, TR AR)
➢ Cardiomegaly signs from longstanding HTN
7 Abdominal examination
8 GUS
➢ Bladder distension from urinary retention
9 MSS
➢ DVT (peripheral emboli) → limb ischemia
➢ Injuries sustained during collapse with stroke
10 IS
➢ Skin and mucous membrane bleeding features → bleeding disorders as a
cause of ICH
➢ Xanthelasma, rash → arteritis, splinter haemorrhage, livido reticularis
11 NS
➢ Level of consciousness
❖ May be comatose
➢ CN
❖ CN palsy
✓ CN VII damage → Facial deviation
▪ Infra nuclear if both upper and lower face area
involved
▪ Supranuclear if only lower face part involved
❖ Dilated pupil, decerebrate rigidity → visual field examination is
very important if posterior fossa haemorrhage is suspected
❖ Homonymous visual field defects
➢ Motor examination
Inspection → decreased muscle bulk of the affected limb,
fasciculation
Palpation
✓ Hyper/hypotonic→ i.e. spastic or flaccid weakness
respectively
✓ Decreased power
✓ Hyperreflexia in spastic hemiparesis and hyporeflexia in
flaccid hemiparesis
➢ Sensory examination
Sensory loss on the affected side → difficult to assess if
comatose
➢ Meningeal irritation signs are usually -ve but there may be +ve
➢ Coordination
Construction apraxia (inability to perform learned activity e.g.
writing)
Cortical sensory loss
✓ Absent stereognosis
✓ Agraphtesia
✓ Absent two-point discrimination
✓ Absent simultaneous extinction. 415
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N.B
Very critical tests: swallow test; ocular muscles and gaze tests; mental status
assessment and sensori-motor assessment

❖ ACA damage
❖ MCA damage
✓ aphasia
❖ PCA damage
✓ Dysarthria and facial numbness
✓ Ataxia and hornor sxx
✓ Facial weakness
✓ Hemiparesis
✓ Hemisensory loss
✓ Hemianopia
✓ comatose
❖ Thalamic hemorrhage
✓ Down and inward deviation of eye
✓ Unequal pupil with absent pupillary reflex
✓ Ipsilateral horner sxx
✓ Absent convergence
❖ Pontine hemorrhage
✓ Deep coma with quadriplegia
✓ Decerebrate rigidity with pinpoint pupil that react to light
✓ Doll’s head/oculocephalic manoeuvre

NIHSS (The National Institutes of Health Stroke Scale) score

➢ The NIHSS is a highly reliable and valid screening assessment for the
rapid evaluation of a patient with acute stroke: Although it’s not a substitute
for comprehensive neurologic examination.
➢ The 11-item scale measures consciousness, orientation, visual fields, gaze,
language fluency and comprehension, speech, sensory loss and neglect,
motor strength, and limb ataxia.
➢ The scale can easily be completed in less than 10 minutes and serves as
an initial measure of stroke severity ranging from 0 (no deficits) to 42
(maximum score)
➢ Minor stroke considered when NIHSS score is <5
➢ NIHSS score emphasizes much on dominant hemispheric function than non-
dominant functions
➢ Additionally, the NIHSS may underestimate posterior circulation stroke
deficits compared to anterior circulation stroke deficits

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Components of NIHSS score


For clinical practice only, you are not obliged to rehearse it (you can use
this text or UpToDate 2018 during scoring)
1. A. Level of consciousness
Alert (0 points)
Not alert, but arousable with minimal stimulation (1 point)
Not alert, requires repeated stimulation to attend (2 points)
Responds only with reflex motor or autonomic effects or totally
unresponsive, flaccid, and areflexic (3 points)
B. Patient knows month and own age
Answers both correctly (0 points)
Answers one correctly (1 point)
Both incorrect (2 points)
C. Patient opens and closes eyes and grips and releases the nonparetic
hand on command
Obeys both correctly (0 points)
Obeys one correctly (1 point)
Both incorrect (2 points)
2. Best gaze (only horizontal eye movement)
Normal (0 points)
Partial gaze palsy (1 point)
Forced deviation (2 points)
3. Visual field testing
No visual loss (0 points)
Partial hemianopia (1 point)
Complete hemianopia (2 points)
Bilateral hemianopia (blind including cortical blindness) (3 points)
4. Facial Palsy /paresis/ (ask patient to show teeth or raise eyebrows and
close eye)
Normal symmetrical movement (0 points)
Minor paralysis (flattened nasolabial fold, asymmetry on smiling)
(1 point)
Partial paralysis (total or near total paralysis of lower face) (2
points)
Complete paralysis of one or both sides (3 points)
5. Motor function of arm
A. right arm
No drift (0 points)
Drift (1 point)
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Some effort against gravity (2 points)


No effort against gravity (3 points)
No movement (4 points)
Untestable (amputation or joint fusion at the shoulder) (0 points)
B. Motor function of left arm
No drift (0 points)
Drift (1 point)
Some effort against gravity (2 points)
No effort against gravity (3 points)
No movement (4 points)
Untestable (amputation or joint fusion at the shoulder) (0 points)
6. Motor function of leg
A. right leg
No drift (0 points)
Drift (1 point)
Some effort against gravity (2 points)
No effort against gravity (3 points)
No movement (4 points)
Untestable (amputation or joint fusion at the hip) (0 points)
B. left leg
No drift (0 points)
Drift (1 point)
Some effort against gravity (2 points)
No effort against gravity (3 points)
No movement (4 points)
Untestable (amputation or joint fusion at the hip) (0 points)
7. Limb ataxia
Absent (0 points)
Present in one limb (1 point)
Present in two limbs (2 points)
Untestable (amputation or joint fusion) (0 points)
8. Sensory to pinprick or withdrawal from noxious stimulus
Normal (0 points)
Mild-to-moderate sensory loss (1 point)
Severe-to-total sensory loss (2 points)
9. Language
✓ No aphasia (0 points) 418
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Mild-to-moderate aphasia (1 point)


Severe aphasia (2 points)
Mute, global aphasia (3 points)
10. Dysarthria
None (0 points)
Mild-to-moderate dysarthria (1 point)
Severe dysarthria (2 points)
Intubated or other physical barrier to producing speech (0 points)
11. Extinction and inattention
No abnormality (0 points)
Visual, tactile, auditory, spatial, or personal inattention or
extinction to bilateral simultaneous stimulation in one of the
sensory modalities (1 point)
Profound hemi-inattention or extinction to more than one
modality (2 points)

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DDX
1) Stroke
Hemorrhagic stroke
✓ ICH
✓ SAH
Ischaemic stroke
✓ Embolic
✓ Thrombotic
2) Vasculitis
✓ TB
✓ Syphilis
✓ SLE
3) Bleeding to brain tumour→ characterized by seizure, hydrocephalus, acute
neurologic features like FND
✓ Glioblastoma multiforme
✓ Metastasis tumour to brain from melanoma, Bronchogenic ca, RCC
4) Acute SDH
5) Neurosyphilis
✓ Vasculitis
✓ Syphilitic guma
6) Todd’s paralysis → a.k.a post ictal paralysis. paralysis which occurs
following seizure
7) Hemiplegic migraine
8) Encephalopathy
✓ Metabolic → hepatic encephalopathy, ureamic encephalopathy
✓ Toxic → alcohol, illicit drugs
✓ Infectious → meningoencephalopathy, sepsis
9) Brain abscess
Triads of brain abscess include fever, headache, FND
10) Neurocysticercosis
✓ Rare in Ethiopia since pork is not usual food due to cultural and
religious values
11) Space occupying lesions
✓ Take long time course unlike stroke

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Stroke mimics

STROKE is considered when focal deficits occurs abruptly and follow vascular
territory

Final Ass’t example

Right/left sided, Crossed/uncrossed, spastic/flaccid, hemiparesis/plegia, 2ry to


ischaemic/hemorrhagic stroke 2ry to cardio embolism/HTN/DM….

N.B.

Face deviation to the opposite side of weakness → uncrossed


hemiparesis/plegia
Face deviation towards the same side of weakness → crossed
hemiparesis/plegia
Spastic → limb rotated inward and hypertonic
Flaccid → limb rotated outward and hypotonic

Then localize the lesion as supra/infranuclear (i.e cortical or subcortical) → refer


paraplegia of Nitsbin (click hre → Localization of neurologic disorders )

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IX

N.B for stroke pt’s, before going to the list of Ix modalities Do RBS, manage life
threatening conditions, stabilize the patient, then do emergency CT. After that, you
will go to other IX and mgt concomitantly.

‘Time is brain’
1. Perform RBS
If suspected bleeding risk; CBC, PT, PTT
2. Perform CT
3. Start rTPA if indicated

1. RBS & FBS


✓ To r/o hypoglycemia
✓ DM is RF for stroke
✓ FBS Should be between 140 and 180
▪ If FBS is < 50 or > 400, thrombolytic (t-PA) is contraindicated
2. CBC & ESR
✓ PCV, hypercoagulable state from SLE
✓ Leukocytosis from infection
3. Lipid profile
✓ Hyperlipidemia (dyslipidemia is RF for stroke)
4. PT & PTT
✓ For mgt purpose → to give heparin based on bleeding tendency
✓ Hypercoagulable states (thromboembolism)
✓ Hemorrhagic stroke from bleeding tendency
5. PICT
6. OFT → like LFT, RFT to prevent 2ry brain injury
7. Serum electrolyte level
✓ Hyponatremia (cerebral salt wasting sxx) in SAH
✓ Cerebral edema in hyponatremia
✓ Hypernatremia in metabolic encephalopathy → DDX
8. Syphilis serology (VDRL in our set up)
9. Blood culture→ if IE is suspected
10. ANA → for SLE

Imaging

11. CT scan

✓ Goal of CT scan is to
o Exclude hemorrhage
o Asses the degree of brain injury
o Identify vascular lesion
o Identify other pathologies (stroke mimics)
✓ CT is preferred than MRI in first cases of stroke 422
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✓ Mandatory initial Ix which should be done immediately on patient


arrival. Time took from initial evaluation to door of CT scan should
not exceed 30 minutes (but difficult to do immediately in our setup)

✓ Haemorrhagic stroke appears hyperdense since blood have iron


content
✓ Ischaemic stroke appears hypodense
✓ More sensitive than MRI for hemorrhage
✓ Infarcts may not appear with in 48 hr’s
o DWI is more sensitive than noncontrast CT scan for detection
of "acute" ischemic stroke
✓ After differentiating the type of stroke by emergency CT scan search
for the cause based on available Ix’s (Doppler carotid scan,
MRA/CTA, cerebral arteriography, PET/SPECT scan)

ISCHEMIC STROKE HEMORRHAGIC STROKE

Watch for early signs of ischemia in CT scan

o Obscuration of the lentiform nucleus


o Loss of insular ribbon or obscuration sylvian fissure
o Cortical hypoattenuation and sulcal effacement
o Hyperattenuation of a large vessel, hyperdense MCA sign

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CT IS important for
1. Large-artery atherosclerotic disease resulting in stenosis or occlusion,
2. Small-vessel or penetrating artery disease (lacunes)
3. Cardiogenic or artery-to-artery embolism,
4. Non-atherosclerotic vasculopathies,
5. Hyper-coagulable disorders
6. Infarcts of undetermined causes

Remark; CT is highly sensitive for hyper acute hemorrhage

12. MRI

✓ Useful to delineate ischemic strokes, especially involving the brainstem or


cerebellum, or lacunar strokes,
✓ Diffusion, perfusion, and gradient echo MR sequences can rapidly detect
early ischemic and hemorrhagic lesions
✓ Describe the amount of at-risk tissue (the “ischemic penumbra”)

13. ECG & ECHO


✓ Arrythmia
✓ Recent MI


IE (vegetation), thrombus, cardiac shunt (paradoxical embolism)
For mgt purpose → don’t elevate BP if there is MI and stroke
together
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14. Carotid and Aortic doppler U/S


✓ Describe the nature of the vessel and assess the presence of
atheroma or thrombi
✓ Better with carotid angiography

15. CXR → cardiomegaly from longstanding HTN


16. MRI based angiography (MRA) → can detect stenosis of the artery, giant
aneurysm, arterial dissection

Discussion

Look at neurolocalization before the discussion of stroke for better understanding


(click here → Localization of neurologic disorders)

Stroke
Cerebro-vascular diseases include some of the most common and
devastating disorders collectively called as Stroke
A stroke, or cerebrovascular accident, is defined as an abrupt onset of a
neurologic deficit that is attributable to a focal vascular cause.
Stroke is defined by the WHO as a clinical syndrome consisting of 'rapidly
developing clinical signs of focal (at times global) disturbance of cerebral
function, lasting more than 24 hours or leading to death with no apparent
cause other than that of vascular origin'.
Include Ischemic stroke, Hemorrhagic stroke, and Cerebro-vascular
anomalies such as intracranial aneurysms and AVMs (Arteriovenous
malformations).
All of which manifest with an abrupt onset of neurologic features that are
often focal in nature: Often follow vascular distributions.
Focal ischemia or infarction is usually caused by thrombosis of the cerebral
vessels themselves or by emboli from a proximal arterial source or the
heart.
A generalized reduction in cerebral blood flow due to systemic hypotension
(e.g., cardiac arrhythmia, MI or hemorrhagic shock) produces Syncope.
If low cerebral blood flow persists for a longer duration, then infarction in
the border zones between the major cerebral artery distributions may
develop: Watershed ischemia
Intracranial hemorrhage (ICH) is caused by bleeding directly into or around
the brain; it produces neurologic deficit by mass effect, blood toxic effect or
increased ICP

Stroke: Classification

1. Ischemic Stroke 425


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Acute occlusion of an intracranial vessel causes reduction in blood flow to


the brain region it supplies because of either an in-situ thrombosis
formation or an embolus showered from the heart or proximal arteries

1.1 Embolic: Cardio embolic or arterio-arterial emboli; Paradoxical embolism


1.2 Thrombotic: Thrombosis formation in intra cranial vessels themselves

2. Hemorrhagic Stroke

Acute bleeding into intra cranial structures generally called intra-cranial


hemorrhage.
Based on the location of bleeding: Intra-paranchymal; SAH; SDH; EDH; IVH

6.1 Ischemic stroke

Epidemiology
✓ Stroke is the second leading cause of death worldwide
✓ Every 40 seconds there is an occurrence of stroke in USA.
✓ Some 88% of these strokes are ischemic. Around 18-20% of stroke is due
to ICH
✓ In developing areas, the Incidence rate of ICH is relatively higher
✓ In UOG Hospital; among stroke patients admitted to the Hospital, 60-70%
are due to Ischemic stroke commonest cause being arterio-arterial embolic
stroke
✓ Steep decreases in stroke incidence and mortality have occurred in
industrialized nations.
• This is attributed to a declining stroke incidence, and lower case-
fatality rates, with suggestive evidence favoring a trend in declining
stroke severity.
• However, the declining stroke incidence has been reversing with the
aging of the population, greater awareness of stroke symptoms, and
better diagnostic tools
✓ Stroke mortality and incidence are increasing in developing nations.
✓ Socioeconomic factors, dietary and lifestyle behaviors, different patterns of
risk factors, and environmental conditions may explain the different
incidences of stroke observed in different parts of the world
✓ Increased life expectancy; improved awareness and improved diagnostic
facilities contribute to increase in incidence rate

Pathophysiology of ischemic stroke


❖ Acute occlusion of an intracranial vessel causes reduction in blood flow
to the brain region it supplies.
❖ The magnitude of flow reduction is a function of collateral blood flow, and
this depends on; 426
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✓ Individual vascular anatomy (which may be altered by disease) i.e.


Collateral supply
✓ The site and extent of occlusion
✓ Systemic blood pressure.
✓ The duration of ischemia
▪ A decrease in cerebral blood flow to zero causes death of
brain tissue within 4 - 10 min
❖ Certain conditions like fever; low BP; hyper or hypoglycemia; electrolyte
disturbances; MI…. Can fasten the progression of ischemia to infarction
❖ If blood flow is restored to ischemic tissue before significant infarction
develops, the patient may experience only transient symptoms, and the
clinical syndrome is called a transient ischemic attack (TIA).
❖ Another important concept is the ischemic penumbra, defined as the
ischemic but reversibly dysfunctional tissue surrounding a core area of
infarction.
o The penumbra can be imaged by perfusion imaging using MRI or
CT (see below and (see figure below)
o The ischemic penumbra will eventually progress to infarction
if no change in flow occurs, and hence saving the ischemic
penumbra is the goal of revascularization therapies.
o The factors that determine the progression of ischemic penumbra
▪ Collateral circulation; systemic BP; duration and extent of
occlusion
▪ Systemic conditions like fever, electrolytes, MI

Figure; Acute left middle cerebral artery (MCA) stroke with right hemiplegia but preserved
language. B) Predicted region of infarct (red) and penumbra (green) based on CT
perfusion data. E) CT scan of the brain 2 days later; note infarction in the region
predicted in B but preservation of the penumbral region by successful revascularization.

Etiologies of ischemic stroke


➢ Thrombosis
o Lacunar stroke (small vessel)
o Large vessel thrombosis
o Dehydration
➢ Embolic occlusion
o Artery-to-artery: Atherosclerosis; Arterial dissection 427
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Cardio-embolic: Atrial fibrillation; Mural thrombus; MI; Dilated CMP;


o
MS; IE
➢ Uncommon causes
o Hypercoagulable disorders: Protein C deficiency; Protein S def.
o Antithrombin III deficiency
o Antiphospholipid syndrome.
o Vasculopathies: Vasculitis; CADASIL; Fibromuscular dysplasia

Large artery Atherothrombotic Infarctions


❖ Almost always occur in patients who already have significant risk factors for
cerebro-vascular atherosclerosis: Commonest cause of large artery stroke
❖ The mechanism of large-artery athero-thrombotic infarction are:
☛ Often artery-to-artery embolization.
☛ Thrombosis in the pre-existing arterial disease
❖ Atherosclerosis often affects large vessel commonly:
☛ Bifurcation of common carotid artery;
☛ proximal ICA;
☛ carotid siphon;
☛ MCA;
☛ vertebrobasilar arteries

Small vessel or penetrating artery disease


❖ Small vessel stroke is affection of smaller and penetrating end arteries
❖ Atherosclerosis or Lipo-hyalinosis
❖ Lacunae usually occur in older patients with long-standing arterial
hypertension, current cigarette smoking, and DM.
❖ The most frequent sites of involvement are the putamen, basis pontis,
thalamus, posterior limb of the internal capsule, and caudate nucleus.
❖ About 20-30% of ischemic stroke

Cardiogenic embolism
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❖ Cardio-embolic strokes are associated with substantial morbidity and


mortality.
❖ Embolism of cardiac origin accounts for approximately 15% to 20% of all
ischemic strokes.
❖ These cardiac emboli may be composed of platelet, fibrin, platelet-fibrin,
calcium, micro-organisms, or neoplastic fragments.
❖ Common causes are AF; MI; IE; rheumatic MS; Prosthetic valves; CMP;
atrial myxoma

Cardio-embolic stroke: AF

❖ AF if is the commonest cause of cardio-embolic stroke: 2/3rd of cardio-


embolic stroke

Table, CHA2DS2-VASc risk stratification score for estimation of stroke risk for
nonvalvular atrial fibrillation in adults

CHA2DS2-VASc Score

1. CHF 1
2. HTN 1
3. Age
☛ ≤ 64 ---------------------------- 0
☛ 65 - 74 ------------------------- 1
☛ ≥ 75 ---------------------------- 2
4. DM 1
5. Prior Stroke or TIA or 2
thromboembolism (doubled)
6. Vascular disease (MI, PAD, 1
Arterial plaque)
7. Sex category
☛ Female ------------------------- 1
☛ Male ---------------------------- 0
Maximum score 10

CHA2DS2-VASc score Adjusted stroke rate (% Recommendation


per year)
0 0 No antithrombotic
1 1.3 Anti-platelet or
anticoagulation
2 2.2
3 3.2
4 4.0
5 6.7
6 9.8 anticoagulation
7 11.2
8 10.8
9 12.2
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CHA2DS2-VASc score Interpretation

❖ The higher the score, the higher the annual stroke risk.
❖ For patients with CHA2DS2-VASc score >1, anticoagulation is generally
indicated unless high bleeding risk/based on HASBLED score/
o Score 0→ No antithrombotic
o Score 1→ Anti-platelet or anticoagulation
o Score ≥ 2 → anticoagulation.
❖ Commonly used Antiplatelets include Aspirin (1st line) & clopidogrel (2nd
line). Commonly used anticoagulants include warfarin, UFH, LMWH

Selected Non atherosclerotic vasculopathies


➢ Cervico-cephalic arterial dissection
➢ Traumatic cerebro-vascular disease
➢ Radiation-induced vasculopathy
➢ Moyamoya disease
➢ Fibro-muscular dysplasia
➢ Vasculitis
➢ Migraine's infarction

Cervico-cephalic arterial dissections


One of the most frequent non-atherosclerotic vasculopathies causing
ischemic in stroke in youngs
Most dissections involve the extra-cranial segment of the internal carotid
artery or extra-cranial vertebral arteries.
Intracranial carotid and vertebro-basilar dissections are less common: Cause
ICH/SAH
Trauma; Fibro-muscular dysplasia; Marfan syndrome; Syphilis…. are
common risk factors

Stroke syndromes: Based on the arterial distribution and clinical profile

➢ TIA (Transient ischemic attacks)


➢ Large vessel stroke syndromes
✓ Carotid artery system syndromes
☛ MCA syndrome; ACA syndrome
✓ Vertebro-basillar artery syndrome
✓ PCA (Posterior cerebral artery) syndrome
➢ Small vessel artery (Lacunar) syndrome
➢ Watershed infarction syndrome

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Transient ischemic attacks (TIA)


➢ A TIA is a transient focal neurologic feature which completely resolve within
24 hours without evidence of infarction on neuro-imaging; attributed to focal
vascular even
➢ Time based definition
o A TIA is a temporary and “non-marching” neurological deficit of
sudden onset; attributed to focal ischemia of the brain, retina, or
cochlea; and lasting < 24hr’s (i.e. Completely resolve within < 24
hours with normal imaging finding)
o Yet most TIAs last only a few minutes.
o Episodes that last longer than 1h are usually due to small infarctions
➢ Tissue based definition
o Any transient episode, regardless of duration, associated with NO
clinically appropriate lesion by neuroimaging be defined as a TIA.
o Prolonged events (>1–6 hours in duration) be defined as stroke
rather than TIA when otherwise clinically appropriate
➢ The blood flow is restored and the focal deficits improved
➢ Vasculitis of any cause results both bleeding and infarction
▪ Vascular disorder – cerebral ischemia – if restored rapidly – TIA
▪ Vascular disorder – cerebral ischemia – if persisted – infarction –
Stroke

TIA: Epidemiology and prognosis

➢ TIA is a strong predictor of stroke


➢ One-third of untreated TIA patients having a stroke within 5 years.
➢ About 1 in 10 patients with TIA experience a stroke in the next 3 months.
➢ The interval from the last TIA is an important predictor of stroke risk; of all
patients who subsequently experience stroke, 21% do so within 1 month
and 51% do so within 1 year of the last TIA and 50% of strokes occur
within 48 hours of TIA
➢ Cardiac events are the principal cause of death in patients who have had a
TIA.
➢ 5-6% of annual mortality is by MI

TIA: Etiologies and Risk factors


TIAs may result from:

➢ Athero-thrombo-embolism that originates from ulcerated extra-cranial arteries


➢ Emboli of cardiac origin
➢ Occlusion of small penetrating arteries that arise from the large surface
arteries of the circle of Willis
➢ Altered local blood flow (perfusion failure) due to severe arterial stenosis,
non-atherosclerotic vasculopathies, or hyper-coagulable states

TIA: Clinical features

❖ The onset of TIA symptoms is sudden, reaching maximum intensity almost


immediately.
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❖ To qualify as a TIA, therefore, an episode should also be followed by


complete clinical recovery.
❖ The clinical symptoms related with the affected vessel

Lacunar infarct syndromes

❖ Ischemic strokes resulting from small-vessel or penetrating artery disease


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❖ Lacunar infarcts are small ischemic infarctions in the deep regions of the
brain or brainstem
❖ The most common risk factors are Age; DM; HTN and smoking
❖ These infarctions result from occlusion of the penetrating arteries branches
from: The anterior choroidal, middle cerebral, posterior cerebral, and basilar
arteries.
❖ Pathologic changes include Lipohyalinotic changes; microemboli or
atherosclerosis.

Pure motor hemiparesis: internal capsule; basis pontis; corona radiata;


cerebral peduncle
Pure sensory stroke: thalamus
Sensori-motor stroke: internal capsule and thalamus
Homo-lateral ataxia and crural paresis (ataxic hemiparesis): basis pontis or
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Dysarthria - clumsy hand syndrome: Basis pontis

Small Vessel Stroke Syndromes

Watershed infarction syndromes


Watershed Ischemia and Infarction

❖ Occur in the border zone between adjacent arterial perfusion beds of the
major circulations:
– During or after cardiac surgery
– After an episode of sustained and severe arterial hypotension that
can happen after cardiac arrest, prolonged hypoxemia, or bilateral
severe carotid artery disease
❖ May be caused by micro-embolism or hyper-viscosity states.
❖ Often bilateral but can be unilateral if there is severe arterial stenosis on
one side only
❖ Ischemia in the border zone or junctional territory of the ACA, MCA, and
PCA may result in bilateral parieto-occipital infarcts.
❖ There can be a variety of visual manifestations, including bilateral lower
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❖ Ischemia between the territories of the ACA and MCA bilaterally may result
in bilateral fronto-parietal infarctions:
❖ Bi-brachial cortical sensori-motor impairment (“person in a barrel”) and
impaired saccadic eye movements
❖ Ischemia in the border zone between the MCA and PCA may cause
bilateral parieto-temporal infarctions.
❖ Defects such as dyslexia, dyscalculia, dysgraphia, and memory defects for
verbal and nonverbal material may be seen

6.2 Hemorrhagic stroke (Intracranial hemorrhage)


➢ Intracranial hemorrhage consists of various spectrum of bleeding in the cranial
fossa and grossly divided into:
– Traumatic intracranial bleeding
– Non-traumatic intracranial bleeding
➢ Based on the location of bleeding:
– Intra-cerebral hemorrhage (ICH)
– Subarachnoid hemorrhage (SAH)
– Epidural and subdural hematoma (EDH & SDH)
– Intra-ventricular hemorrhage (IVH)

➢ Intra-cerebral hemorrhage (ICH) is a common neurologic event with significant


morbidity and mortality.
➢ ICH accounts for approximately 10% to 15% of new strokes that occur every
year. These numbers are expected to increase with the increased longevity of
the population
➢ The overall morbidity and mortality of ICH has not significantly declined over
the past several decades.
➢ Thirty-day mortality ranges between 30% and 50% and only about 20% will
regain independence at 6 months.
➢ Despite these statistics, most patients have survivable hemorrhages with
aggressive medical care

Changing in Epidemiology

➢ Traditionally, chronic hypertension accounted for approximately 80% to 90% of


documented ICHs
➢ More recent epidemiologic studies report that chronic hypertension now
accounts for only about half (50%) of all ICHs.
➢ This change in etiologies largely has to do with improved control of
hypertension, the aging of the population, and increased use of anticoagulation.
➢ Improvements in radiologic techniques also have led to detection of smaller
and more subtle hemorrhages
➢ In the developing countries: HTN is still the most common and significant
cause of ICH

Hypertensive hemorrhage:

➢ Bleeding is on deep penetrating arteries: deep brain tissue bleeding


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Figure; Hypertensive hemorrhage. Trans axial non-contrast CT scan through the


region of the basal ganglia reveals a hematoma involving the left putamen in a
patient with rapidly progressive onset of right hemiparesis.

Non hypertensive hemorrhage:

➢ Bleeding occurs anywhere in the brain depending on the cause: Often lobar
and multiple hemorrhage

Etiologies of ICH: Non-Traumatic causes

• Hypertension
• Vascular malformations
• Intracranial tumors


Bleeding Disorders, Anticoagulants, and Fibrinolytic Treatment
Cerebral Amyloid Angiopathy
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• Granulomatous Angiitis of the CNS and Other Vasculitides


• Sympathomimetic Agents
• Hemorrhagic Infarction

Hypertensive ICH
➢ The main cause of ICH is hypertension.
➢ The primary role of HTN in ICH is supported by a high frequency (72% -
81%) of hx of HTN, significantly higher BP measurements at admission in
comparison with patients with other stroke subtypes, high frequency of LVH,
and over-representation of common genetic variants associated with
hypertension.
➢ Excluding patients with hemorrhage associated with ruptured AVMs, tumor,
anticoagulant and thrombolytic therapy, and cocaine ingestion; it was
determined that the cause was hypertension in 72% of patients. Although
the prevalence of HTN in ICH cases is dropping to 50% in recent years
➢ Patients with severe acute hypertension may have a similar risk as those
patients with chronic low-grade hypertension: the issue is uncontrolled HTN
➢ The vascular lesion produced by chronic hypertension that leads to arterial
rupture and ICH is probably lipohyalinosis of small intra-parenchymal
arteries: Ultimately formation of micro aneurysm
➢ The most related risk factors for development of theses vascular changes
with HTN are duration of HTN and older age.
➢ Common sites of bleeding are: Putamen > Lobar > Thalamus > Cerebellum
> Pons……

Bleeding into a tumor


➢ Relatively rare (<10% of ICH cases).
➢ The tumor types most likely to lead to this rare complication are
Glioblastoma multiforme or metastases from melanoma, bronchogenic
carcinoma, choriocarcinoma, or renal cell carcinoma
➢ Different from HTN related ICH:
➢ Papilledema at presentation and headache long before bleeding
➢ Location of bleeding: Corpus callosum, Multiple bleeds
➢ CT signs of ring forming bleed; nodular enhancement and huge surrounding
edema

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Use of anticoagulation
Patients on long-term anti-coagulation have a risk of ICH of approximately
1% per year, although the highest risk is within the first year.
Risk factors include:
✓ Older age
✓ Hypertension
✓ Previous ischemic stroke, and leukoariosis.
ICH risk is significantly increased when the INR is > 3.5 and add on use
of anti-platelets.

Signs of micro-bleeds in imaging

These hemorrhages have certain distinctive clinical characteristics when


compared to HTN induced ICH:
They tend to present with a slowly progressive course, at times over
periods as long as 48 to 72 hours.
The bleeding expands with relatively larger size before clinical features:
Often multiple Bleeding from other areas

Cerebral amyloid angiopathy (CAA)


CAA is characterized by selective deposition of ß-amyloid in the walls of
cerebral vessels, primarily small and medium sized arteries of the cortex
and leptomeninges.
CAA increases steadily with age, reaching 60% in individuals > 90 years.
It characteristically causes ICH in the elderly and is rarely documented
before the age of 55 years
The superficial location of the affected vessels in the cortex and lepto-
meninges is responsible for a predominantly lobar location of ICH.
Multiple and recurrent lobar bleeding
30% of cases have dementia: ADs
Focal deficits or seizure may occur before major bleeding

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Difference between ICH and Hemorrhagic infarction


Hemorrhagic infarction characteristically occurs
✓ In the setting of cerebral embolism
✓ Rarely following restoration of cerebral perfusion to border zone
infarcts that had resulted from global hypo-perfusion
✓ Following cerebral venous thrombosis

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Pathophysiology of hematoma formation


✓ The exact means by which ICH occurs is not completely understood: The
mechanism of ICH depends on the cause of bleeding
✓ ICH secondary to hypertension occurs in areas of the brain that are
perfused by the lenticulo-striate arteries arising directly from the large basal
cerebral arteries.

SUSEPTIBLE VESSEL
These vessels are branched from large arteries proximal to arterioles where cerebral
auto -regulation occurs

CHRONIC INJURY
Atherosclerosis and HTN will result a series of injuries to these vessels ultimately
result in thickening and fragile

ICH
The exact mechanism how these vessels bleed is not known but:
Micro anurysm formation; sudden high BP and inability for the vessels to maintain
RBCs in the vessels

Pathophysiology of hematoma expansion


CT studies reveal that approximately 40% of ICHs will expand from the
initial size of the hemorrhage.
In those patients in whom hematoma expansion is detected, 75% will have
hematoma expansion within the first 6 hours, and almost all of the rest will
have expansion within 24 hours
How expansion occurs is similarly unknown.
Traditionally, hemorrhages were believed to expand because of local mass
effect leading to progressive tearing of small vessels and damage of
neurologic tissue.
It is now believed that much of the hemorrhage expands along white matter
tissue planes that surround intact neurologic tissue

Factors related with hematoma expansion

Poorly controlled DM and SBP > 200 mm Hg


The role of anti-platelet use and hematoma expansion is unclear
The finding of contrast extra-vasation during CTA has been used to identify
patients at risk for hematoma expansion: SPOT SIGN

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Secondary brain injury after bleeding


If and how secondary damage occurs is also a matter of debate.
1. MRI volumetric analysis reveals a decrease in hemispheric volume
ipsilateral to an ICH: Compression effect.
2. Similarly, apoptotic markers are increased in patients with ICH, suggesting
that much of ICH-related damage may be secondary: Apoptosis induced.
3. Red blood cell lysis occurs approximately 6 to 8 days after the initial
hemorrhage: Complement induced inflammation.
4. A subsequent release of hemoglobin and its byproducts (primarily thrombin)
is believed to be involved in both direct and indirect neural toxicity: Free
Iron toxicity
5. Damage to the BBB result in brain edema and subsequent complications.

Clinical presentation
The clinical presentation of ICH has two main elements:
1. Symptoms that reflect the effects of intracranial hypertension
2. Those smx’s that are specific for the location of the hematoma

A characteristic of ICH at presentation is the frequent progression of focal


neurological deficits over periods of hours.
This early course reflects progressive enlargement of the hematoma
The general clinical manifestations of ICH related to increased ICP
(headache, vomiting, and depressed level of consciousness) vary in their
frequency at onset of ICH.
The correlation of these symptoms (especially abnormal level of
consciousness) with hematoma size applies to all anatomical varieties of
ICH, which in turn relates directly to mortality.

Putaminal hemorrhage

➢ The most common variety of ICH, 35% of cases.


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➢ Dense hemiplegia; dysarthria; contra-lateral gaze palsy and progress to


coma.
➢ Commonest cause is HTN
➢ Ventricular extension seen as a poor prognostic factor with higher mortality

Lobar hemorrhage

➢ Lobar hemorrhage is second to putaminal hemorrhage in frequency, 25% of


ICH cases.
➢ Non-hypertensive mechanisms including AVMs, sympathomimetic agents (in
young patients), and CAA (in elderly patients) are frequent causes.
➢ The peripheral location of these hematomas explains the lower frequency of
coma at onset.
➢ Seizure occurs in many cases

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6.3. Management of Stroke

Evaluation of Acute Stroke


➢ Time is Brain: Early fibrinolytic treatment
✓ ‘‘Be quick, but don’t hurry.’’
✓ Time took from initial evaluation to door of CT scan should not
exceed 30 minutes
➢ The main goals of evaluation of acute stroke is:
2. To diagnosis of acute stroke or other stroke mimics
3. To differentiate ischemic from hemorrhagic stroke and analyze the
subtype of stroke
4. Identify prompt risk factors
5. Assess the severity of the disease and indications of rTPA
➢ The most important and initial evaluation was the onset of the symptoms
with the exact clock: Example 2:00 AM rather than using hours or minutes
like 2 hours ago.
o Remark; symptom onset is defined as the time the patient was last
known to be normal. If awaken with weakness to take stroke onset
as time he/she went to bed
➢ The mode of onset and chronology of symptoms: helps to identify stroke
syndromes

Management principles
1. Differentiate Ischemic from hemorrhagic stroke ASAP (Clinically, Emergency
CT in best setups)
2. ABC of life
✓ Treat and prevent aspiration (target is saturation ≥ 94%)
✓ Treat hypotension and shock (may be cause of stroke)
3. RBS → if low manage as hypoglycemia
4. Emergency CT
✓ Non contrast CT
✓ Can detect ischemia as early as 1hr and hemorrhage within 10 min
(i.e used to r/o hemorrhagic stroke)
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N.B MRI is very sensitive and specific, but it needs time for Dx
5. Identify the cause
6. Specific and supportive management based on type of stroke
7. Follow with Neurosign chart if patient is not concious

Neuro sign chart


BP PR RR T0 GCS Vomiting Abnormal Pupillary Power Tone Reflex Input Out Fluid sign
body mov’t reflex put balance

A. Management of ischemic stroke

Let’s show you order sheet example for Ischemic stroke mgt in our set up
before going to detailed management principles → it may be different based
on your patient comorbid conditions and complications.

Treatment
New order
❖ Secure double IV line
❖ Put on 100% O2 (if SPO2 is < 95%). E.g. Put on 1L/min of INO2
❖ Atorvastatin 80 mg, PO, daily (for at least 3 months, then 40 mg daily for life
long which should be continued with chronic OPD follow up)
❖ Aspirin, 325 mg, PO, Loading then 81mg (81-100 mg), PO, daily
❖ UFH, 5,000 IU, Sc, BID (Consider Warfarin if there is CHADVASC score
indication)
❖ Omeprazole, 20mg, PO/via NG tube, BID
❖ NG Tube feeding with 300ml of semisolid food every 3 hours and Monitor swallow
test daily (this order is, if swallow test is -ve)
❖ Catheterize and follow input and output strictly (i.e. Maintain fluid balance)
❖ Do RBS QID (control of glucose to be between 140 mg/dL and 180 mg/dL)
❖ Position every 1hr (for critical pt) or every 2hr (for noncritical pt)
❖ Follow Vital sign strictly

Dr. Mulualem. G (GP)

Added order
If BP > 220/110 mmHg
❖ Lasix or HCT Plus 444
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❖ ACE-I (Captopril/enalapril) or CCB (amlodipine)


If Hyperglycemia (>180 mg/dL) give insulin → see dose below
If febrile → antipyretics and cooling cloths (cold compression)
If GCS < 8, insert NG tube and Intubate. Routine NG tube, airway, and catheter care
with eye and mouth care.
If there is DVT and PE
❖ UFH, 5,000 IU, IV, loading then 250 IU/kg/dose, Sc, BID
❖ Add warfarin 2-5mg, PO/IV, on day 1 or 2 of UFH, daily for 2 days, check INR
after 2 days and adjust based on the result
❖ Overlap warfarin and UFH for at least 5 days until desired INR/INR=2-3/
maintained for 24hr then discontinue UFH.
If there is cerebral edema (increased ICP)
❖ Head position between 30 and 450
❖ Mannitol Loading dose 1g/kg over 30-60min, followed by a maintenance dose of
0.5g/kg every 4-6hrs (if measuring weight is difficult, mannitol 300ml loading
over 30 min then a maintenance dose of 100ml QID then deescalate)
❖ Maintenance of euvolemia with NS, avoid dextrose solutions
Treat causes and comorbidities → Atrial fibrillation, MI, UTI, Pneumonia….
Treat electrolyte disturbance
❖ Link to physiotherapy (when patient is stable and before discharge)

rTPA is not available in most setups of Ethiopia


For hemorrhagic stroke, all managements above are the same except; avoid UFH,
warfarin, aspirin, and atorvastatin. Consider indication for surgical removal. It
needs strictly control of BP (see Hemorrhagic stroke mgt below)

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Elements of stroke management


– ABC of life
– Treatment of acute ischemic stroke
– Treatment and prevention of causes and risk factors
– Comprehensive functional rehabilitation
– Comprehensive nursing care and prevention of complications

Three basic principles of Acute stroke care include;


1. Acute reperfusion therapy (Achieve timely re-canalization of the
occluded artery and reperfusion of the ischemic tissue)
1.1 IV thrombolysis with rTPA (recombinant tissue plasminogen
activator = Alteplase)
1.2 mechanical thrombectomy
2. Optimize collateral flow
3. Avoid secondary brain injury
➢ All Should be performed at the same time
➢ All are directed for Salvaging ischemic penumbra

1. Acute reperfusion therapy

There is incontrovertible evidence that IV thrombolysis with rTPA and


endovascular thrombectomy with a retrievable stent improve neurologic
outcomes in patients with acute ischemic stroke.
Both treatments should be administered as quickly as possible after stroke
onset, can be combined, and are safe in appropriately selected candidates.
IV thrombolysis and mechanical thrombectomy can produce reperfusion injury
after re-canalization.
Reperfusion injury can manifest with hemorrhage and edema.
✓ It is more severe when the area of established infarction is large
✓ Good patient selection and prompt treatment are crucial to avoid this
complication.

1.1 IV Thrombolysis

✓ IV thrombolysis with rTPA is proven to be effective in improving functional


outcomes after an ischemic stroke up to 4.5 hours after symptom onset.
✓ The first step of evaluation of acute stroke is to decide eligibility for rTPA.
• Time of onset
• Age > 18 yrs
• RBS; BP
• NIHSS score and CT findings
• Other Contraindications

Indication for r-TPA

Clinical diagnosis of Ischemic stroke


Onset of symptoms to time of drug administration ≤4.5 h; Best in the first 3
hours
CT scan showing no hemorrhage or edema of >1/3 of the MCA territory
Age 18 ≥ years
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ABSOLUTE CONTRAINDICATIONS

Sustained BP >185/110 mmHg despite treatment


RBS < 50 mg/dl or > 400 mg/dl
Bleeding diathesis; INR > 1.7, on anticoagulants or Platelets < 100,000/mm;
Recent head injury or intracerebral hemorrhage; History of head injury in
the last 3 months
Major surgery in preceding 14 days
GI bleeding in preceding 21 days
Recent myocardial infarction
Arterial puncture at non-compressible site within 7days;
Previous ICH recently or suspected SAH; brain tumor; AVM
BP > 185/110;

OTHER CONSIDERATIONS
Minor stroke (Typically NIHSS score <5) and rapidly improving deficits
Pregnancy
Seizure at onset with post-ictal residual deficits
Major extra cranial injuries and surgery in the last 15 days

Administration of rtPA

➢ IV access with two peripheral IV lines (avoid arterial or central line placement)
➢ Review eligibility for rtPA
➢ Administer 0.9 mg/kg IV (maximum 90 mg) IV as 10% of total dose by bolus,
followed by remainder of total dose over 1 hour
➢ Frequent cuff blood pressure monitoring
➢ No other antithrombotic treatment for 24 h
➢ For decline in neurologic status or uncontrolled blood pressure, stop infusion,
give cryoprecipitate, and reimage brain emergently
➢ Avoid urethral catheterization for ≥2 h

CXN of rTPA

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✓ is a rare but potentially serious complication of rtPA administration:


especially in those with ACE-I:
✓ Rx with anti-histamines and steroids
ICH: 1.9 % - 6.4%.
✓ Treatment includes;
➢ Control of hypertension (systolic target 140 mmHg to 160 mm
Hg)
➢ Reversal of the fibrinolytic effect with cryoprecipitate (10 units)
or an antifibrinolytic agent (tranexamic acid 10 mg/kg to 15
mg/kg IV over 20 minutes or έ-aminocaproic acid 5 g IV
followed by an infusion of 1 g/h if necessary

1.2 Mechanical thrombectomy

Clinical indications

Age ≥ 18 years
NIHSS score ≥ 6
Time from Symptom onset to groin puncture < 6 hours
Good prestrike functional status
Presence of proximal intracranial artery occlusion
ASPECTS score ≥ 6 on baseline CT scan (ASPECTS = Alberta stroke
program early CT score)

Other indications for mechanical thrombectomy

✓ Failed rTPA
✓ Large thrombus on imaging

Standard Post reperfusion care

➢ Admission to a step-down or ICU


➢ Maintenance of NPO status until dysphagia screening is performed to avoid
aspiration pneumonia
➢ Administration of isotonic IV fluids (not dextrose containing because of risk
of hyperglycaemia)
➢ BP and neurologic monitoring every 15 minutes for 2 hours, then every 30
minutes for 6 hours, then every hour for 16 hours after treatment
➢ Aggressive blood pressure treatment if SBP is > 180 mm Hg or DBP is
>105 mm Hg
➢ Emergent CT scan of the brain if neurologic decline, acute increase in
blood pressure, nausea, vomiting, or new headache is present to rule out
haemorrhagic transformation
➢ Repeat brain imaging at 24 hours to assess for asymptomatic haemorrhage
and to allow initiation of anti-platelet therapy

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2. Optimize collateral circulation

➢ BP and Stroke
✓ Higher BP at the onset of stroke is required; part of physiologic
response to perfuse collateral vessels
✓ BP should be lowered if above 220/110 mmHg if rTPA is not used;
reduce by 15% in the first 24 hours: if rTPA to be used keep the
BP below 180/90.
✓ Diuretics and ACE-I are preferred but any treatment choice
✓ BP should be improved if its low; Using IV fluids and vasopressors

➢ Hyperglycemia / hypoglycemia

✓ Hyperglycemia (>180 mg/dL) and Hypoglycemia during the first 24


hours after stroke are poor prognostic indicator.
✓ Keep RBS level between 70 and 180 mg/dl in the acute setting:
Dextrose/insulin
✓ If there is hyperglycemia give insulin with sliding scale principle*
RBS value (mg/dl) Insulin dose (IU) to be given
181 – 200 2 i.e.
201 – 250 3 increase
251 – 300 4 by 1 IU
301 – 350 5 for every
351- 400 6 rise of
> 400 50 mg/dl
✓ Check Urine ketone
and glucose
✓ Consider DKA if S/he
has DM
* Look at DM management for more

3. Prevent secondary brain injury

❖ Conditions that exacerbate neurologic injury and ischemic penumbra include:


✓ Fever and dehydration
✓ Aspiration and nutritional deficiency
✓ Airway obstruction and hypoxia
✓ Electrolyte disturbances and organ dysfunction
✓ Presence of complications including: infections, DVT, cerebral edema,
Neuro-protective treatments: Hypothermia; Fluoxetine

3.1 Airway protection and oxygenation

✓ Stroke patient should be positioned appropriately: flat or 30o up depending


on the condition of the patient
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✓ Oral secretions should be removed; oral airway if necessary; intubation if


GCS < 8
✓ Saturation of oxygen should be above 95% in acute state; if low assess
airway and reasons for lower oxygenation and put on them with 100%
oxygen.
✓ Assess the respiratory pattern and rate and assess sign of aspiration

3.2 Nutrition and Feeding

➢ Assess for dysphagia; and aspiration using swallow test and GCS
➢ NG tube feeding and intravenous fluid in early states of stroke
❖ NG tube for
✓ Feeding
✓ Prevention of aspiration
✓ Dysphagia

N.B

✓ Oral or oropharyngeal dysphagia is common Because of CN palsy


(pseudo bulbar palsy)
✓ Check swallow test
➢ Give 30ml of water to swallow with one breath
➢ S/he should complete with in 10 sec
➢ If there is chocking episode and remnant in mouth swallow
test is -ve → insert NG tube for feeding. If not, swallow test
is +ve and s/he can take PO
➢ Absent gag reflex doesn’t mean -ve swallow test
✓ Feeding in NG tube
➢ Calculate metabolic demand (md)
➢ Metabolic demand of adult is 2000 - 2500 ml per day
➢ md coefficient = md x 1.5
➢ Divide the total amount of metabolic demand for 8 to give
over 3hr. e.g. if the md is 2400ml, then 2400/8 = 300ml, so
give 300ml every 3hr (the trend in our setup is, NG Tube
feeding 300ml every 3hr)
➢ add insensible loss
➢ The food for feeding should be semisolid
➢ If there is concomitant DM, avoid high sugar containing food

3.3 Fever, electrolyte and organ function

➢ Assess for fever; if occurred assess for site of infection and treat; use
antipyretics and cooling cloths (cold compression) to reduce fever
➢ Monitor electrolyte frequently and treat: commonest abnormality is
hyponatremia
➢ Monitor LFT and RFT as well as cardiac evaluation frequently and treat

3.4 Standard nursing care


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Bed side care for the clothing and intermittent positioning to prevent
pressure sore
Routine NG tube; airway; and catheter care with eye and mouth care
Monitor swallow daily and act accordingly

3.5 Treatment of stroke complications

3.5.1 Infections

Fever after a stroke should prompt evaluation for common sources,


including pneumonia and UTI.
Pneumonia is the commonest cause of fever in the first 48 hours of stroke
with risk factors including aspiration; atelectasis; intubation…
Early mobilization, airway care and dysphagia assessment prevent
pneumonia
UTI occur in 11% to 15% of patients with stroke, and are often seen
during the first 5 days of the hospitalization. Prolonged catheter use and
poor catheter care are risk factors

3.5.2 DVT

The development of DVT may take place as early as day 2 after stroke
onset, with a peak incidence between days 2 and 7.
PTE occurs in 1-3% of stroke with mortality rate of 13-25%
Severe disability; old age and dehydration are risk factors

DVT and PE treatment


➢ Initiate warfarin 2-5mg, PO/IV, on day 1 or 2 of parenteral
anticoagulation therapy (e.g LMWH or UFH)
➢ Overlap warfarin and parenteral anticoagulant for at least 5 days
until desired INR (therapeutic INR = 2-3) maintained for 24hr then
discontinue parenteral therapy
N.B

Heparin dose
Prophylaxis Therapeutic
UFH 5,000 IU, Sc, BID 5,000 IU, IV, loading then 250
IU/kg/dose, sc, BID or 80 IU/kg/hr
maintenance dose
LMWH (e.g. 1mg/kg/day (40mg, sc, 1mg/kg/dose, sc, BID
enoxaparin) daily)

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3.5.3 Cerebral edema

Neurologic deterioration is often observed within 72 to 96 hours from onset


of the stroke.
Decreased level of arousal may be the earliest clinical change indicating
symptomatic cerebral edema.
Other early signs are: increased sleepiness; headache, N/V; worsening of
motor deficit and pupillary signs
In general, sign and smx of cerebral edema include
▪ Decreased alertness
▪ Projectile vomiting
▪ Cushing triad → HTN, bradycardia, irregular breathing pattern
▪ Papilledema
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Treatment includes:
✓ Head position between 30 and 45o
✓ Start osmotic therapy with Hypertonic saline or IV mannitol
✓ Mechanical ventilation: Hyperventilation
✓ Steroid (like dexamethasone, 6mg, IM) → for meningitis, brain tumor,
brain abscess
✓ Consider decompressive surgery
Patients at the highest risk for developing malignant cerebral edema are:
▪ Internal carotid artery or proximal middle cerebral artery with a large
infarction volume;
▪ CT with frank hypodensity within 6 hours; more than 1/3rd of
hemisphere infarction; midline shift > 5 mm in the first two days of
stroke
Clinical factors associated with cerebral edema:
– An NIHSS score > 20 in dominant hemispheric strokes or > 15 in
non-dominant hemispheric strokes has been associated with
malignant infarction.
– Other clinical factors associated with edema are early nausea and
vomiting, female sex, congestive heart failure, and leukocytosis at
presentation.
General managements of cerebral edema include
✓ Frequent neurologic examinations to monitor for neurologic
deterioration
✓ Maintenance of normothermia
✓ Avoidance of hypercarbia
✓ Maintenance of euvolemia while avoiding hypotonic solutions
✓ Control of glucose to between 140 mg/dL and 180 mg/dL
✓ Correction of hyponatremia
✓ Prevention of aggravating factors

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Management of increased ICP in the setting of acute


ischemic stroke
Correction of factors exacerbating increased ICP

➢ Hypercarbia
➢ Hypoxia
➢ Hyperthermia
➢ Acidosis
➢ Hypotension
➢ Hypovolemia

Positional

 Initial management of elevated ICP includes elevating the head of the bed to
30 degrees (avoidance of flat supine position) and appropriate sedation and
pain control.
 Avoidance of head and neck positions compressing jugular veins

Medical management

Endotracheal intubation and mechanical ventilation if GCS < 8


Hyperventilation to a Pco2 of 35 ± 3 mmHg (if herniating)
Mannitol
✓ Loading dose 1g/kg/dose over 30-60min, followed by a maintenance
dose of 0.25 to 5 g/kg/dose (usually 0.5g/kg) TID or QID (depending on
clinical status, serum osmolality, volume status and ICP measurement)
☛ It should not be given over a long period (as continuous infusion)
☛ 20g of mannitol = 100ml (i.e. mannitol 20g/100ml, 1g=5ml) (for
e.g. for 60kg adult pt loading dose 1g x 60kg = 60g = 300ml,
maintenance 0.5g x 60kg =30g = 150ml)
☛ The usual trend in our setup is 300ml loading over 30 min then
a maintenance dose of 100ml QID then deescalate → 50ml,
25ml…
☛ Inspect for crystals prior to administration. If crystals are present,
re dissolve by warming solution
✓ The goal is dehydrating the brain not the patient and maintenance of
serum osmolality 300-320mOsm/L.
Consider hypertonic saline (23.4%)
✓ Loading dose 30ml over 10-20min followed by maintenance dose of 3%
hypertonic saline, 1ml/kg/hr titrated to a serum sodium of 150-155meq/l

Fluid management

 Maintenance of euvolemia with Isotonic solution using NS


 Avoidance of glucose containing solutions because hyperglycemia is
associated with worse prognosis for stroke
 Replacement of urinary losses with NS in patients receiving mannitol.
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4. Management of risk factors and prevention of recurrent stroke

GENERAL MEASURES

Control of associated risk factors such as hypertension, dyslipidemia,


cigarette smoking and alcohol intake; dietary treatment and exercise
General measures include
o Anti-thrombotic agents
o Modifying risk factors
o Antihypertensive agents
o Statin treatment
o Diet and physical activity
The prevention strategy depends on the mechanism of Ischemic stroke

4.1 Platelet anti-aggregates

Platelet anti-aggregates: include Aspirin; Clopidogrel and Ticlopidine as well


as Phospho-di esterase inhibitors like Dipyridamole.
first line of therapy in patients at high risk for stroke

Aspirin
✓ Loading dose of 325 mg then 81-100 mg maintenance should be
given as early as possible and ideally within 48 hours of stroke
onset.

o Alternative: Clopidogrel 75 mg Po daily

4.2 Anticoagulants and statins

Lipid lowering agents


✓ High dose statins;
• Atorvastatin (80 mg) for at least 3 months, then half the dose (40
mg) for life is recommended in arterial causes of stroke
o Age ≤75 years: High-intensity therapy: 80 mg once daily; if
unable to tolerate, may reduce dose to 40 mg once daily
o Age >75 years or not a candidate for high intensity therapy:
Moderate-intensity therapy: 10 to 20 mg once daily
o For Type 1 or 2 diabetes and age 40 to 75 years: Moderate-
intensity therapy: 10 to 20 mg once daily
• Alternative: Rosuvastatin 40 mg Po daily

Warfarin

✓ Inhibits the synthesis of factors II, VII, IX, and X, as well as proteins C and
S: follow up with PT; PTT and INR
✓ Indicated for primary and secondary prevention of stroke in patients with
NVAF: depends on CHA2DS2Vas score
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✓ Other Indication for secondary prevention includes: cardio-embolic stroke


following structural diseases of the heart like RHD; MI; DCMP…. Or
following large vessel stroke with AF.
✓ Initial dose; 2-5mg, PO/IV, daily for 2 days, check INR after 2days and
adjust based on the result

N.B

Indication for dual anticoagulant

➢ Recurrent Stroke
➢ Resistance to Single anticoagulant
➢ Intracranial atherosclerosis
➢ Large vessel stroke (e.g. MCA stroke)
➢ MI + Stroke

4.3 Prophylactic anticoagulants

Unfractionated Heparin 5000 IU SC TID


Alternative: Enoxaparin (LMWH) 40 mg SC daily

4.4 BP management

Lower levels of BP from pre-stroke level is associated with reduction of


stroke risk in the future if the stroke is due to atherosclerosis.
BP treatment should be started after the acute stroke is stabilized (4-5
days after stroke)
In general, do not give antihypertensive agents in the first 24 hours
unless one of the following three conditions is present:
o The patient’s BP is very high (systolic >220, diastolic >120, or
mean arterial pressure >130 mm Hg).
o The patient has a significant medical indication for antihypertensive
therapy. Examples include: Acute MI, Aortic dissection, Severe
heart failure, Hypertensive encephalopathy.
Better anti-hypertensives after stroke are diuretics; ACE-I or CCB.
Advice on how to reduce salt intake, limit alcohol intake, avoid licorice and
decongestants.
Smoking: Counseling, liberal nicotine replacement therapy, varenicline or
bupropion
Obesity: Counseling on caloric restriction, referral to dietitian, bariatric
surgery in refractory patients with severe obesity and diabetes mellitus or
insulin resistance:
Exercise counseling and high adherence Mediterranean diet

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Supportive management for Ischemic stroke

❖ Administer O2
❖ GI prophylaxis for Cushing ulcer
❖ DVT prophylaxis after 24hrs → early physiotherapy
❖ Bladder care
❖ NG tube
❖ Prevent bedsore
✓ Positioning every 1hr for critical pt and every 2hr for non-critical pt
❖ Treat comorbidities → MI, UTI, Pneumonia…. which increase metabolic
demand of brain and increase 2ry brain injury
❖ Treat electrolyte disturbance
❖ Anti-hypertensive
✓ If s/he was on antihypertensive mgt, resume previous dose after
24hr
✓ For new case treat after 7day
✓ For hypertensive urgency use hydralazine, labetalol (beta blocker)
✓ For chronic HTN → ACE-I/ARB or ACE-I/diuretics
❖ Physiotherapy
✓ Speech therapy
✓ Physical therapy
✓ Neuro rehabilitation
❖ Treat the underlying cause
✓ Cardioembolic stroke → anticoagulant based on CHA2DVASC2 score
✓ AF
✓ IE → emergency antibiotic then definitive surgery based on indication

B. Management of hemorrhagic stroke

Basic and supportive cares are the same as ischemic stroke


Issues related to treatment of ICH have been dominated by two main
considerations:
1. The type and intensity of medical interventions required to improve
the functional and vital prognosis and
2. The choice between medical and surgical therapy.

Treatment can be broadly categorized into:


1. Acute medical interventions designed to decrease hematoma
expansion
2. Methods to decrease secondary injury

Basic medical care

Patients with a GCS < 8 should be intubated to decrease the risk of


aspiration.
Mechanical ventilation should ensure adequate oxygenation and normal
levels of carbon dioxide:
Airway care and prevention of aspiration if GCS is > 8
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Hyperventilation for acute management of increased ICP. Osmotic therapy


should be initiated with mannitol or hypertonic saline.
Isotonic IV fluids are started and adjusted to correct for any electrolyte
abnormalities with the goal of obtaining and maintaining euvolemia.
Feeding should be initiated as soon as swallow test is performed
EVD (external ventricular drainage) should be considered in hydrocephalus;
IVH; and if CBF (cerebral blood flow) is < 60
Cardiopulmonary complications are common after ICH and can worsen
outcome.
ECG changes and troponin leaks may be found during ICH but do not
appear to affect short-term prognosis: needs to be followed repeatedly.
Pneumonia and pulmonary edema are the most common pulmonary
complications that should be looked for and treated promptly: Fever should
be treated
Pneumatic compression devices and elastic stockings have been shown to
be effective preventive treatment for DVT and PTE: Prophylactic Heparin is
an alternative
Continuous EEG should be considered in patients after an intra-cranial
hemorrhage that has a disproportionate effect on their level of
consciousness: AEDs

1. Attempts to reduce hematoma expansion

✓ Most cerebral hemorrhages stopped bleeding within 6 hours.


✓ Rapidly reducing the BP to < 140/80 mmHg has been associated with
reduced hematoma size. Particularly in the 1st 6hrs
✓ BP reduction
o Elevated BP increases ICP and can cause further bleeding.
However, hypotension can lower cerebral blood flow, worsening the
neurologic deficits. Therefore, BP reduction must be gradual.
o Treatment is indicated if systolic BP is >180 or the MAP is >130.
▪ Labetalol: Intravenous boluses
❖ Initial dose: 10 to 20 mg IV push over 2 minutes
❖ Until target is achieved give double the initial dose in 15
minutes (maximum dose: 80 mg/dose)
❖ A total maximum dose: 300 mg.
OR
▪ Labetalol Continuous IV infusion: Initial: 0.5 to 2 mg/minute.
Titrate the dose to a maximum of 10 mg/minute. A total
maximum dose: 300mg
▪ Hydralazine; 5mg, IV every 20-30 minutes until target BP
achieved
✓ If there is hemorrhagic transformation give cryoprecipitate
✓ Serum glucose level should be kept between 100 and 180 mg/dl:
Correction doses with insulin

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2. Methods to Decrease Secondary Injury

✓ A significant amount of the neurologic damage that occurs after ICH can be
attributed to secondary processes.
✓ A rationale for surgical removal of ICH is to remove the offending
substances before secondary damage can develop: Unfortunately, only a
few ICHs are candidates for surgical removal.
▪ Cerebellar hemorrhages > 3 cm in diameter should have surgical
evacuation.
The Minimally Invasive Surgery Plus T-PA for ICH Evacuation
The Intra-operative CT-Guided Endoscopic Surgery for ICH

❖ Look other methods of decreasing 2ry brain injury in ischemic stroke mgt

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Chapter 7; Paraplegia (ከወገብ በታች ሽባነት)

Chapter 7; Paraplegia (ከወገብ


በታች ሽባነት)
Dr. Mulualem. G

Clinical features and how to write hx of paraplegia


patient
History

➢ Pt’s may present with


Failure to use both (R&L) lower extremity (i.e. bilateral lower
extremity weakness)
Back pain or neck pain
➢ Weakness
1st let us remember the terminologies
✓ Monoplegia → weakness of one extremity
✓ Paraplegia → weakness of two extremities (commonly bilateral
lower extremities)
✓ Triplegia → weakness of three extremities
✓ Quadriplegia → weakness of four extremities
Ask the symmetry → i.e. bilateral in paraplegia
From where to where is the progression of weakness
✓ Proximal to distal → weakness starts with
▪ Difficulty of raising hand/combing hair
▪ Difficulty of standing from sitting position/walking up
hails
✓ Distal to proximal → weakness starts with
o Difficulty of unbuttoning, scissoring
Onset → from start of weakness to complete loss of function but not
upto hospital arrival
✓ Abrupt (maximal at onset)
✓ Progressive → worsen gradually then complete immobilization
o Long duration of smx favours benign process eg
intradural tumor usualy benign
Associated with
✓ Numbness → starts in the feet and progress upwards
✓ Burning sensation
✓ Paraesthesia
✓ Cold sensation
✓ Anhidrosis → below the lesion
✓ heaviness
➢ Back pain
1st smx mostly
Onset → rapid/slow
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Localized over the spine (in non-compressive lesions) or radiate to


root distribution like to buttock or LL i.e. radicular pain (in
compressive lesions)
Characterize the pain
✓ Sharp, lancinating, radicular pain, aggravated by coughing,
sneezing, or straining → compressive lesions
✓ Dull aching or burning, bund like, localized pain → non
compressive
Persistent or intermittent
Associated with low grade intermittent fever, chills and rigor (e.g. in
post viral TM/transverse myelitis/)
o N.B if fever is associated with chills and rigor mostly it is high
grade fever
➢ Preceding infection smx → URTI, GI infections, UTI
➢ Hx of trauma
➢ Autonomic dysfunction like incontinence
Faces/flatus, urinary incontinence
Urgency, hesitancy
Constipation, urinary retention
➢ Fever
➢ Ulceration → with foul smelling discharge
➢ Neck stiffness

Risk factors

➢ Infection
Syphilis → Tabes dorsalis
TB → TM (transverse myelitis), TB spondylitis
Viral → TM
Schistosomiasis
▪ TM, granulomatous disease
▪ S. mansoni and S. hematobium typically infect the spinal cord
causing rapidelly progressive TM, affect lower thoracic spinal
cord followed by lumbosacral spinal cord
Brucellosis
➢ IV drug use, impaired immunity, infection → for epidural abscess
➢ Vaccination → GBS from acute rabies vaccine
➢ Diet → guaya → neuro-laterization
➢ Malnutrition
Vitamin B12 deficiency which result in SCDC (severe combined
degeneration of the cord), common in vegetarians
Vitamin B12 deficiency also occurs in post illeal resection
Copper deficiency → Myeloneuropathy
➢ Trauma → Disc prolapse (common in heavy weight lifters), SDH over the
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Chapter 7; Paraplegia (ከወገብ በታች ሽባነት)

➢ Occlusion of anterior spinal artery → anterior cord sxx


Caused by atherosclerosis, embolism, vasculitis…
Other cause of anterior cord sxx is abdominal surgery (rupture of the
aorta) → spinal cord infarction
➢ Malignancy
primary or metastasis to spinal cord
hematologic malignancy involving vertebral bones
other malignancies which metastasize to the back bone like prostate,
breast, bronchogenic ca,RCC, GI malignancy (retroperitoneal
neoplasm though the vertebral foramen)
➢ Family history → ALS (amyotropic lateral sclerosis), hereditary spastic
paraplegia
➢ AF, IE, DCMP, CHF → result in cardiac emboli to anterior spinal artery
➢ DM → Posterior cord sxx, DSPN (Distal symmetric pyelonephropathy)
➢ RVI → vascular myelopathy, SCDC

Complication of paraplegia

➢ DVT
➢ Aspiration pneumonia
➢ Bed sore
➢ Neurogenic Bladder (Urinary stasis)

Sample history

Sample history of a patient from Metema with the DX of paraplegia 2ry to non-
compressive myelopathy 2ry to acute transverse myelitis.

Chief compliant
Bilateral lower extremity weakness of 10 hrs duration

HPI
This patient was last relatively healthy 10 hours back, at which time he started to
experience sudden onset of bilateral lower extremity weakness while he was
sitting with families in a holiday gathering. The weakness was maximal at onset
to the extent he failed to stand from sitting position and he was unable to raise,
flex or extend the legs by himself. Associated with this he also feels numbness
which starts in the feet and progress upwards, burning sensation, Paresthesia,
Cold sensation heaviness of the legs, Fecal and urinary incontinence.

Three days prior to the onset of weakness, he experienced persistent, dull


aching, bund like type of back pain which is localized over the spine area without
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any aggravating and relieving factors associated with low grade intermittent fever
without chills or rigor. For this he visited a local clinic at metema where he was
given unspecified antipain, and red oval tablets to be taken 3 times per day. He
got improvement for the pain and he visited metema primary hospital when he
sustained weakness and after catheterization he was referred immediately to our
hospital for better investigation and management.
➢ He is unmarried daily laboror and has hx of unsafe sexual practice with
multiple sexual partners but no genital ulcer or penile discharge (tabes
dorsalis/tertiary syphilis/ i.e. posterior cord sxx, post viral TM, RF for herepes zoster)
➢ NO hx of chronic cough, contact with chronic cougher or a known TB
patient (TM /transverse myelitis/, TB spondylitis]
➢ No hx of vaccination (GBS from acute rabies vaccine)

➢ He/she usually eats injera made of ‘‘teff’’ and ‘‘machilla’’ and ‘’wott’’
made of ‘‘atter’’ and ‘‘dagusa’’ 3-4 times per day. Occasionally he/she
eats meat during holidays (guaya → neurolateralization, vitamin B12 deficiency → SCDC,
copper deficiency → myeloneuropathy)
➢ No hx of smoking or chronic alcohol intake
➢ No hx of river water contact (RWC) or post RWC itching (schistosomiasis)
➢ No hx of abdominal surgery (rupture of the aorta → spinal cord infarction)
➢ No hx of pesticide or herbicide exposure, radiotherapy to the back
(Lymphoma is the commonest cause of compressive myelopathy, radiation myelopathy)
➢ No hx of Bone pain, epistaxis, swelling over the neck, axilla or groin
(hematologic malignancy involving vertebral bones, also r/o other malignancies which metastasize to the back
bone like prostate, breast, bronchogenic ca, RCC, GI malignancy)
➢ No hx of trauma to the back (SDH over the spinal cord)
➢ No family hx of similar illness (ALS, hereditary spastic paraplegia)
➢ No hx of dspnea, orthopnea, PND or palpitation (cardiac emboli resulting in anterior
spinal cord sxx)
➢ No hx of tinnitus, blurring of vision or light headedness (Vitamin B12 deficiency
→ SCDC)
➢ NO hx of DM, HTN or asthma (DM cause posterior cord sxx without weakness)
➢ Screened for RVI and found to be NR (GBS, TM, Vascular myelopathy, SCDC)

Finally, S/he was admitted to our hospital supported physically by his


families

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Physical examination (pertinent findings)

1 GA

2 Vital signs
❖ GBS or other causes of autonomic dysfunction
➢ OHT ❖ In compressive myelopathy autonomic dysfunction happens late in the disease
➢ Tachycardia progression since autonomic pathway is in the center of spinal cord which will
be affected later when the mass is huge enough
➢ BP, for autonomic dysfunction
➢ Fever → in case of infection, epidural abscess
➢ Tachypnea
Pulmonary embolism from DVT which intern result from prolonged
immobilization due to paraplegia
Diaphragmatic paralysis (characterized by paradoxical respiratory
movement)
➢ Arrythmia → AF is RF for embolism which results in anterior cord sxx

3 HEENT → anaemia 2ry to vitamin B12 deficiency

4 LGS

Breast ca features
Cervical LAP from lymphoma which result in compressive myelopathy
Anhidrosis and sweat level

5 RS

TB features → check TB findings in all systems


Consolidation from aspiration pneumonia
Dullness and decreased air entry for lung ca

6 CVS

CHF features, IE, DCMP → cardiac emboli → anterior cord sxx

7 Abdominal examination

Abdominal distension from fecal or urinary retension


Constipation
DRE → Poor rectal tone, features of prostatic ca which metastasize to back
bone

8 GUS

Urinary retention
Sexual dysfunction

9 MSS

Spinal tenderness especially point tenderness in disc prolapse


Gibbus with deformity in TB
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Bed sore, DVT → CXN


11 IS → pallor from vitamin B12 deficiency
12 NS
Atrophy (wasting)
Hypo/hypertonic
Hypo/hyperreflexia, areflexia
Power
➢ 0/5 & 1/5 → plegia
➢ 2/5 - 4/5 → paresis
➢ 5/5 → normal
Sensory and sweat level
Position and vibration sensation loss in posterior cord disorders
Pain and temperature sensation loss in anterior cord disorders
Autonomic dysfunction (like incontinence) in central cord involvement
Absent superficial reflexes especially abdominal and cremasteric reflex
Stiff neck → cervical spondylosis

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DDX

DDX of Paraplegia
UMNL LMNL
Brain Spinal cord Plexopathy
Parasagittal Compressive non-compressive Radiculopathy
sinus o Bilateral
thrombosis Primary spinal cord tumours Infectious poliomyelitis
Mass over the o Intramedullary o TM (transverse Neuropathy
parasagittal ▪ Ependymoma myelitis) NMJ disorders
area ▪ Astrocytoma o Neurosyphilis o Myasthenia
ACA stroke o Extramedullary (tabes dorsalis) gravis
Hydrocephalus ▪ Neurofibroma o Rabies vaccine Myopathy
▪ Meningioma o HSV2, CMV, GBS
▪ schwannoma EBV, HIV, HTLV Cauda equina sxx
2ry spinal cord tumours o Lyme disease Conus medullaris
(metastasis to spinal cord) Metabolic MND (motor neuron
o Bronchogenic ca o Vitamin B12 disease)
o Breast ca deficiency →
o Prostatic ca SCDC
o Lymphoma Vascular (Spinal cord
o Multiple myeloma syndromes)
o GI cancers o Anterior spinal
o RCC cord sxx (Spinal
Granulomatous infections cord infarction)
o TB o Posterior cord
o Schistosomiasis SXX
o CTD (connective tissue o Central cord sxx
disease) o BSS
o Brucellosis o Complete cord
Disc prolapse (herniation) transaction
Syringomyelia o Cauda equina sxx
Epidural abscess in spinal cord and conus
Sarcoidosis medullaris →
Early stage of foramen LMNL
magnum sxx
Spinal stenosis
Mixed
Have mixed features of UMNL and LMNL
ALS
MS
Spinal shock
SCDC

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DDX of paraplegia based on onset of illness


Acute causes Chronic causes
TM ALS
GBS Peripheral neuropathy
Disc prolapse Granulomatous infections
Spinal cord infarction Metastatic tumours
Epidural abscess Primary spinal cord tumours
Cervical spondylosis

❖ UMNL (upper motor neuron lesion)


✓ Brain
Parasagittal sinus thrombosis
Mas over the parasagittal area
Hydrocephalus
ACA stroke
✓ Spinal cord

N.B

Spinal cord lesions can be compressive or non-compressive. Let us see their


difference with the characteristic presentation.

Compressive non-compressive
➢ Back pain ➢ Back pain
radicular pain radiates to root distribution. Localized over the spine
For example, to buttock or LL Dull aching or burning, bund like,
Sharp, lancinating, radicular pain, localized pain
aggravated by coughing, sneezing, or ➢ After back pain all other manifestations
straining like weakness, sensory loss and
➢ 1 pt present with back pain then progress
st
autonomic dysfunction may happen at the
sequentially to weakness → sensory loss → same time especially in complete cord
autonomic dysfunction (like urinary incontinence involvement. Typical example is TM.
and sexual dysfunction). This is due to horizontal ➢ Separate sensory loss is cmn in non-
localization in spinal cord. compressive lesions. For example
autonomic area Pain and temperature loss →
sensory area anterior cord sxx
motor area Position and vibration loss →
posterior cord sxx

Image. Spinal cord horizontal localization

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Compressive
▪ Primary spinal cord tumours
➢ Intramedullary → sphincter abnormality is the earliest manifestation
o Ependymoma
o Astrocytoma
➢ extramedullary
o neurofibroma
o meningioma
o schwannoma
▪ secondary spinal cord tumours (metastasis to spinal cord)
➢ Bronchogenic ca
➢ Breast ca
➢ Prostatic ca
o Commonly involve lumbosacral area
o Osteoblastic tumour unlike all other malignancies (osteolytic)
➢ Lymphoma
➢ Multiple myeloma
➢ GI cancers
➢ RCC
▪ Granulomatous infections
➢ TB → can cause of TM
o TB spondylitis a.k.a pott’s disease
o Gibbus (wedge shaped fusion of two vertebrae) deformity is
typical feature
o Usually occur in the absence of extra spinal TB
o Cmn in lower thoracic and upper lumbar area
➢ Schistosomiasis
➢ CTD (connective tissue disease)
➢ brucellosis
▪ Disc prolapse (herniation)
➢ Heavy weight lifters and overweight are at risk
➢ C/F → chronic low back pain and prolonged weakness
▪ Syringomyelia
➢ Cavity formation within the cord
➢ Chronic and progressive
➢ Caused by Acquired or congenital factors (acquired causes can be
from post infectious, trauma/from hyperextended neck during caring
objects by head/)
➢ Spare the posterior column
➢ Sensory loss (pain and temperature loss) involved
➢ There is wasting of small hand muscles
▪ Sarcoidosis
▪ Epidural abscess in spinal cord
➢ Triads include fever, back pain and FND (Paraplegia)
➢ Tender over the involved area
➢ There may be Sensory level
➢ Cmn in immunocompromised pt’s
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➢ Staphylococcus is the cmn etiologic agent


▪ Early stage of foramen magnum sxx → Clock wise rotation of weakness
▪ Spinal stenosis

Non compressive
▪ infectious
➢ TM (transverse myelitis)
o Sudden, rapid weakness which manifest with in hrs to days
o Present with fever, back/limb pain followed by sensory level, bladder
disturbance within hrs
o Usually happens following infection with MMRV (measles, mumps,
rubella, varicella), EBV, CMV, influenza virus
o Having sharp sensory level differentiate it from GBS
o DX criteria
• Bilateral motor, sensory and autonomic dysfunction occurring
simultaneously
• Sensory level
• Progression to nadir of clinical deficit between 4hrs and 21 days
of onset
• Exclusion of compressive, post radiation, neoplastic and vascular
causes
➢ Neurosyphilis → tabes dorsalis
o Cause posterior cord sxx
• No weakness
• Pain and temperature preserved
• Only position and vibration sensation lost
o Happen after 2-3 decades of syphilis infection unless congenital
syphilis
➢ Rabies vaccine
➢ HSV2, CMV, EBV, HIV, HTLV
➢ Lyme disease
▪ Metabolic
➢ Vitamin B12 deficiency → SCDC
▪ Vascular (Spinal cord syndromes)
➢ Anterior spinal cord sxx (Spinal cord infarction)
o Rare, if it occurs commonly occur in mid thoracic spinal cord (water
shed area)
o Common in anterior spinal cord because anterior spinal artery is
single artery unlike posterior spinal cord arteries
o Spare position and vibration sensation
o More sudden in onset than TM
o RF include cardiogenic emboli, thrombus, vasculitis, hypotension,
atherosclerosis, aortic dissection
➢ Posterior cord SXX
➢ Central cord sxx
➢ BSS
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➢ Complete cord transaction


➢ Cauda equina sxx and conus medullaris → LMNL
❖ LMNL (lower motor neuron lesion)
✓ Plexopathy
✓ Radiculopathy
Bilateral poliomyelitis
▪ Typically affect anterior horn
▪ Acute in onset
✓ Neuropathy
✓ NMJ disorders
Myasthenia gravis
✓ Myopathy
✓ GBS
Variants of GBS include
▪ AMAN (acute motor axonal neuropathy)
▪ ASMAN (acute sensorimotor axonal neuropathy)
▪ AIDP (acute inflammatory demyelinating polyradiculoneuropathy)
▪ MFS (Miller Fisher syndrome)
Nowadays CIDP (chronic inflammatory demyelinating
polyradiculoneuropathy) is out of GBS variant
8 A’s of GBS
o Autoimmune
o Areflexia
o Ascending paralysis
o Acute
o Afebrile
o Absence of sensory level
o Autonomic involvement → OHT, arrythmia
o Acellular CSF (albumin cytogenic dissociation → decreased
number
of cells but, increased protein/albumin of CSF)
✓ Cauda equina sxx
✓ Conus medullaris
✓ MND (motor neuron disease)
Spare sensory system
Idiopathic
Cmn in old age pt’s (>55)
Chronic in onset
Initially Unilateral which progress to the other side
e.g. bulbar palsy, ALS (corticospinal + anterior horn cell
degeneration), primary lateral sclerosis (only cortico spinal tract
degeneration)
❖ Mixed
✓ ALS
✓ MS
✓ Spinal shock
✓ SCDC
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If the lesion is in thoracic area it cause paraplrgia, if it is in cervical


area it cause quadriplegia
Present with
▪ ascending parasthesia (tingling, numbness)
▪ glove and stocking pattern

IX

1. Spinal X-ray
Request to the target level depending on the site of lesion (for
example if lesion is at T8 with sensory level at T10 the request
should be ‘’thoracic veretebral X-ray centered at T8’’)
Important for
✓ Gibbus in TB (TB spondylitis) → wedge shaped fusion of
lower part of the upper vertebrae and upper part of the lower
vertebrae (if you suspect TB spondylitis do Spinal x-ray, CBC,
ESR, CXR and other TB work up)
✓ Herniated inter vertebral disc
✓ 2ry deposit of malignancy
▪ Osteblastic in prostatic ca but osteolytic in other
malignancies
✓ Fracture or dislocation of vertebrae, bone density
✓ Cervical spondylosis
2. Spinal MRI
Ix of choice which confirm the site of lesion
✓ Have excellent anatomic resolution and extent of tumour
Distinguish between malignancy and other lesions like epidural
abscess, tuberculoma, epidural haemorrhage
If MRI is not available do CT myelography
✓ Permit CSF analysis
3. ESR and blood culture → for epidural abscess
4. CBC
Megaloblastic Anaemia in vitamin B12 deficiency (low hemoglobin
with MCV > 100)
Leucocytosis in epidural abscess and malignancy
Multiple myeloma → plasmacytosis
5. CSF analysis
Low opening pressure
Acellular CSF (albumin cytogenic dissociation → No cell/decreased
number of cells but, increased protein/albumin of CSF) in GBS
Xanthochrome
Important for epidural abscess

6. PICT → SCDC, TM
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7. RBS → DSPN (distal symmetric polyneuropathy) characterized by glove and


stocking pattern
8. Nerve conduction test (NCT) → neuropathy
9. Muscle biopsy → from largest muscle involved for myopathy dx
10. S/E → TM, GI source of infection like campylobacter in GBS
11. U/A and urine culture → TM
12. BUN & creatinine
13. Tumour markers

Discussion

7.1. Localization of neurologic disorders


➢ Neuro-localization is Identification of what site of the nervous system has been
affected:
➢ Two Pillars for the Diagnosis of neurologic disorders
Where is the lesion? → Anatomic diagnosis
✓ CNS
▪ Cortex
▪ Subcortical areas
▪ Brainstem
▪ Spinal cord
✓ PNS
▪ Nerve Root lesion (radiculopathy)
▪ Plexus lesion (plexopathy)
▪ Peripheral nerve lesion
▪ Multifocal or diffuse Peripheral Neuropathy
▪ NMJ and Muscles
What is the lesion? → Pathologic diagnosis
✓ Vascular lesions
✓ Infectious lesions
✓ Inflammatory lesions
✓ Neoplastic disorders
✓ Demyelinating lesions
✓ Degenerative disorders
✓ Hereditary abnormalities
✓ Deficiency and Metabolic
✓ Toxin and Drug related

Distinction between CNS and PNS lesions


Signs and CNS lesions (UMNL) PNS lesions (LMNL)
symptoms
Pain Headache; Neuropathic pain are not Neuropathic pain; Distorted
common; Central pain sensation like allodynia
Pattern of CST distribution weakness; Hemi body Symmetric weakness; Very focal
weakness
Pattern of
distribution;
Hemi distribution sensory loss;
weakness; Myotomal weakness
Stocking-glove; Fiber type
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sensory loss Dissociated sensory Sx, Sensory Dermatome distribution


Reflexes Hyperreflexia, pathologic reflex and loss Areflexia; Hyporeflexia or normal
of coetaneous reflex coetaneous reflex are spared
Tone Spastic, rigidity; paratonia Normal or flaccid; Myotonia
Cranial nerve Incomplete lesions Complete; often bilateral
Mental Can occur depending on the area of Very rare
affection affection
Others Cortical signs; Cerebellar signs… Atrophy; Fasciculation; Spasms….

Regional localization

If UMNL
✓ The cortex; hemispheres
✓ Subcortical white matter
✓ Diencephalon; basal ganglia, thalamus
✓ Brain stem
✓ Spinal cord
If LMNL
✓ Spinal nerves
✓ Plexus
✓ Peripheral nerve
✓ NMJ
✓ Muscle
Interpret the characteristic motor, Gait and sensory abnormality to locate
regional neurologic disease.
Use the specific function of region for best localization.
For example: Cortical functions like speech, cortical sensory function

Regional Motor localization

CST (corticospinal tract) and CBT (corticobulbar tract) originates from


pre-central frontal gyrus called motor nucleus

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The motor fibers are somatotopically organized in patterns that reflect


their functional importance: Motor homunculus
✓ Medial to lateral: Bladder function – legs – arms – face – oro-
buchal

Picture; Motor homunculus

Differential weakness (difference in grade of weakness between UL and


LL): CST disorder
Transverse Localization: Signs and symptoms of cortical lesion like
aphasia; seizure; cognition

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Picture; Motor function localization

CST and CBT progress down wards via corona-radiata as the fibers
dispersed widely before reaching the internal capsule: Differential
hemiparesis (arm > face > leg, or vice versa)
In the internal capsule, the CST and CBT converge independently to
rest at the posterior limb and genu of internal Capsule: Dense
hemiparesis
In the brainstem: CST and CBT join together to pass through cerebral
peduncle and basis pontis: Dense hemiparesis and bulbar palsy
Transverse localization: CBT are crossed in the brainstem before
supplying CN nuclei.

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Picture; Motor function localization

At the medulla: CST cross the midline to the opposite side to run to the
respective level of the spinal cord
At the point of decussation, crossed and uncrossed fibers are found
near each other which can result various types of weaknesses: Crural
paresis, diplegia, hemiplegia, quadriplegia depending on the specific
location.
At the spinal cord CST ends to excite the alpha motor N: Paraplegia;
quadriplegia
Transverse Localization: The lower four CN lesions cause crossed
paralysis with body weakness

Extra-pyramidal control of motor function

➢ CST and CBT projections to the basal ganglia and cerebellum have an active
role in the planning and execution of movements.
➢ The cerebellum and basal ganglia are critically important for coordinated and
organized finely tuned motor functions
➢ The cerebellum has a major role in the coordination of movements and control
of equilibrium and muscle tone. The cerebellum controls the ipsilateral limbs
through connections with the SC and BS; but opposite to the cortex → Ataxia
➢ The basal ganglia play a major role in the control of posture and movt.
Participate in motor planning through reciprocal connections. The cortico-striate
pathway includes direct and indirect projections from the cerebral cortex to the
striatum → movement disorders

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Table; Summary Of UMNL


Location of the injury Pattern and distribution of motor weakness
Cortex Signs and symptoms of cortical lesion like aphasia; seizure;
cognition
Corona radiata Differential hemiparesis
Internal capsule Dense hemiparesis
Brainstem Dense hemiparesis and bulbar palsy
Spinal cord Paraplegia (lower thoracic and lumbosacral cord injury);
quadriplegia (mainly cervical and rarely higher thoracic cord
injury)

Table; Summary Of LMNL


Location of the injury Pattern and distribution of motor weakness
Spinal nerves Myotomal muscle weakness often not recognized
Plexus Monoparesis affecting only one limb
Single nerve Weakness of the muscles that are supplied by the affected
nerve
Diffuse affection of Distal symmetric; Proximal symmetric muscles of the limbs
many nerve fibers are involved.

Regional localization of the Sensory system

Figure; left) The main somatosensory pathways. The spinothalamic tract (pain, thermal sense) and
the posterior column–lemniscal system (touch, pressure, joint position) are shown. Offshoots from
the ascending anterolateral fasciculus (spinothalamic tract) to nuclei in themedulla, pons, and
mesencephalon and nuclear terminations of the tract are indicated.

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Table; Regional localization of the Sensory system


Location in the NS Characteristics sensory loss distribution
Peripheral nerve Sensory loss generally confined to the area supplied by the
lesions nerve; sensory loss of the whole limb; dermatomal pattern or
symmetric distal sensory distribution
Spinal cord lesions Distinct sensory level with all modalities; isloated loss of pain and
temperature; isolated vibration and position loss; cape in shoulder
distribution; hemicord pattern
Brainstem lesions Contralateral pain and temperature loss to the CN palsy and
sensation of the face; Contralateral vibration and position loss to
the CN palsy
Thalamus Contral-lateral hemi sensory loss of all modalities which includes
the face; complex hemi-sensation loss; Central pain
Cortex Hemisensory loss with differential sensory loss; cortical sensory
loss; complex sensory loss…

Table; Transverse localization


Location Motor Sensory Specific
in the NS
Spinal Distal weakness ➢ Sensory level with all Bladder and
cord predominates modalities; tingling; bowel involved
Paraparesis, numbness; parasthesisa; Lhermitt’s sign
quadriparesis, back pain sweat level
syringomyelic pattern, ➢ Pattern specific: Brown- sensory level
hemiparesis or sequard, posterior cord… vertebral
monoparesis. tenderness
Weakness is spastic with
pathologic reflexes and
loss of cutaneous
reflexes
Segmental LMNL pattern
at the site of the lesion
Brainstem Contra-lateral hemi- ➢ Lateral: Contra-lateral pain Crossed deficit
weakness; may or may and temp. sense loss with Gaze palsy
not involve the face crossed pain and temp loss Loss of
Medullary and bilateral on the face consciousness if
brainstem lesions could ➢ Medial: Contra-lateral RF affected
have various forms of vibration and position loss Vertigo
weakness. Bulbar affection
Spastic type of Nausea
weakness; weakness Vomiting…
often dense
Depending on the
location of the lesion
crossed cranial nerve
palsy. M2; P4; MD;4
Thalamus
and
Weakness is solely
because of Internal
➢ Sensory dysfunction is
solely a result of thalamic
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internal Capsule affection lesion aphasia


capsule Weakness is often dense ➢ Contra-lateral sensation loss emotional facial
with affection of CN and in all modalities and involve palsy
the face on the same the face; sensory hemiataxia cognitive decline
side of the body ➢ Complex sensory affection; sleep
weakness; spastic type hemi-inattention disturbance
of weakness coma
Thalamic pain
syndrome
movement
disorders

Cortex Weakness is hemi ➢ Hemisensory loss; Higher cortical


distribution; differential differential sensory loss function
weakness: arm > face > ➢ Complex sensory function Apraxia
leg, or vice versa are affected: extinction; Aphasia
Spastic weakness stereognosis; neglect; visual field
Complex motor function defects
are affected; planned anosmia
motor activity; motor seizure…. CN
memory… I&II

7.2. Diseases of the Spinal Cord


Diseases of the spinal cord produce quadriplegia, paraplegia, and
sensory deficits far beyond the damage they would inflict elsewhere in
the nervous system. Because the spinal cord contains, in a small cross-
sectional area, almost the entire motor output and sensory input of the
trunk and limbs.
Many spinal cord diseases are reversible if recognized and treated at an
early stage; thus, they are among the most critical of neurologic
emergencies.
The efficient use of diagnostic procedures, guided by knowledge of the
anatomy and the clinical features of spinal cord diseases, is required to
maximize the likelihood of a successful outcome.

Treatable Spinal Cord Disorders

Compressive
✓ Epidural, intradural, or intramedullary neoplasm
✓ Epidural abscess
✓ Epidural hemorrhage
✓ Cervical spondylosis
✓ Herniated disk
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✓ Posttraumatic compression by fractured or displaced vertebra or


hemorrhage
Vascular
✓ Arteriovenous malformation and dural fistula
✓ Antiphospholipid syndrome and other hypercoagulable states
Inflammatory
✓ Multiple sclerosis
✓ Neuromyelitis optica
✓ Transverse myelitis
✓ Sarcoidosis
✓ Sjögren-related myelopathy
✓ SLE-related myelopathy
✓ Vasculitis
Infectious
✓ Viral: VZV, HSV-1 and 2, CMV, HIV, HTLV-1, others
✓ Bacterial and mycobacterial: Borrelia, Listeria, syphilis, others
✓ Mycoplasma pneumoniae
✓ Parasitic: schistosomiasis, toxoplasmosis, cystercercosis
Developmental
✓ Syringomyelia
✓ Meningomyelocele
✓ Tethered cord syndrome
Metabolic
✓ Vitamin B12 deficiency (subacute combined degeneration)
✓ Copper deficiency

Spinal cord Anatomy relevant to clinical signs

➢ The spinal cord has 31 segments, each defined by an exciting ventral motor
root and entering dorsal sensory root.
➢ The mature spinal cord ends at approximately the first lumbar vertebral body.
➢ The lower spinal nerves take an increasingly downward course to exit via
intervertebral foramina.
➢ The first seven pairs of cervical spinal nerves exit above the same-numbered
vertebral bodies, whereas all the subsequent nerves exit below the same-
numbered vertebral bodies because of the presence of eight cervical spinal
cord segments but only seven cervical vertebrae (see table below).
➢ These relationships assume particular importance for localization of lesions that
cause spinal cord compression.
➢ Sensory loss below the circumferential level of the umbilicus, for example,
corresponds to the T10 cord segment but indicates involvement of the cord
adjacent to the 7th or 8th thoracic vertebral body.
➢ In addition, at every level, the main ascending and descending tracts are
somatotopically organized with a laminated distribution that reflects the origin or
destination of nerve fibers.

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Spinal Cord Levels Relative to the Vertebral Bodies


Spinal Cord Level Corresponding vertebral body
Upper cervical Same as cord level
Lower cervical 1 level higher
Upper thoracic 2 levels higher
Lower thoracic 2 - 3 levels higher
Lumbar T10-T12
Sacral T12-L1

Determining the Level of the Lesion

The presence of a horizontally defined level (sensory level) below


which sensory, motor, and autonomic function is impaired is a hallmark
of a lesion of the spinal cord.
Sensory loss below this level is the result of damage to the
spinothalamic tract
on the opposite side, 1 to 2 segments higher in the case of a unilateral
spinal cord lesion, and at the level of a bilateral lesion.
✓ The discrepancy in the level of a unilateral lesion is the result of
the course of the second-order sensory fibers, which originate in
the dorsal horn, and ascend for one or two levels as they cross
anterior to the central canal to join the opposite spinothalamic tract.
Lesions that transect the descending corticospinal and other motor tracts
cause paraplegia or quadriplegia with heightened deep tendon reflexes,
Babinski signs, and eventual spasticity (the upper motor neuron
syndrome).
Transverse damage to the cord also produces autonomic disturbances
consisting of absent sweating below the implicated cord level and
bladder, bowel, and sexual dysfunction.
The uppermost level of a spinal cord lesion can also be localized by
attention to the segmental signs corresponding to disturbed motor or
sensory innervation by an individual cord segment.
✓ A band of altered sensation (hyperalgesia or hyperpathia) at the
upper end of the sensory disturbance, fasciculations or atrophy in
muscles innervated by one or several segments, or a muted or
absent deep tendon reflex may be noted at this level.
✓ These signs also can occur with focal root or peripheral nerve
disorders; thus, they are most useful when they occur together with
signs of long tract damage.
With severe and acute transverse lesions, the limbs initially may be
flaccid
rather than spastic.
✓ This state of “spinal shock” lasts for several days,
rarely for weeks, and may be mistaken for extensive damage to
the
anterior horn cells over many segments of the cord or for an acute
polyneuropathy.
The main features of transverse damage at each level of the spinal
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Cervical Cord
➢ Upper cervical cord lesions produce quadriplegia and weakness of the
diaphragm.
➢ The uppermost level of weakness and reflex loss with lesions at C5-C6 is in
the biceps; at C7, in finger and wrist extensors and triceps; and at C8, finger,
and wrist flexion.
➢ Horner’s syndrome (miosis, ptosis, and facial hypohidrosis) may accompany a
cervical cord lesion at any level.

Thoracic Cord
Lesions here are localized by the sensory level on the trunk and, if
present, by the site of midline back pain.
Useful markers of the sensory level on the trunk are the nipples (T4)
and
umbilicus (T10).
Leg weakness and disturbances of bladder and bowel function
accompany the paralysis.
Lesions at T9-T10 paralyze the lower—but not the upper—abdominal
muscles, resulting in upward movement of the umbilicus when the
abdominal wall contracts (Beevor’s sign).

Lumbar Cord
➢ Lesions at the L2-L4 spinal cord levels paralyze flexion and adduction of the
thigh, weaken leg extension at the knee, and abolish the patellar reflex.
➢ Lesions at L5-S1 paralyze only movements of the foot and ankle, flexion at the
knee, and extension of the thigh, and abolish the ankle jerks (S1).

Sacral Cord/Conus Medullaris syndrome


The conus medullaris is the tapered caudal termination of the spinal
cord, comprising the sacral and single coccygeal segments.
The distinctive conus syndrome consists of;
✓ Bilateral saddle anesthesia (S3-S5)
✓ Prominent bladder and bowel dysfunction (urinary retention and
incontinence with lax anal tone), and
✓ Impotence.
The bulbocavernosus (S2-S4) and anal (S4-S5) reflexes are absent.
Muscle strength is largely preserved. By contrast, lesions of the cauda
equina, the nerve roots derived from the lower cord, are characterized
by low back and radicular pain, asymmetric leg weakness and sensory
loss, variable areflexia in the lower extremities, and relative sparing of
bowel and bladder function.
Mass lesions in the lower spinal canal often produce a mixed clinical
picture with elements of both cauda equina and conus medullaris
syndromes.

Cauda equina syndrome (CES)


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➢ signifies an injury of multiple lumbosacral nerve roots within the spinal canal
distal to the termination of the spinal cord at L1-L2.
➢ Lower back pain, weakness and areflexia in the legs, saddle anesthesia, or
loss of bladder function may occur.
➢ The problem must be distinguished from conus medullaris syndrome, acute
transverse myelitis, and Guillain-Barré syndrome.
➢ Combined involvement of the conus medullaris and cauda equina can occur.
➢ CES is most commonly due to a large ruptured lumbosacral intervertebral disk,
but other causes include lumbosacral spine fracture, hematoma within the
spinal canal (sometimes following lumbar puncture in patients with
coagulopathy), and tumor or other compressive mass lesions.
➢ Treatment is surgical decompression, sometimes on an urgent basis in an
attempt to restore or preserve motor or sphincter function, or radiotherapy for
metastatic tumors

Special Patterns of Spinal Cord Disease

Figure; Transverse section through the spinal cord, composite representation, illustrating the principal
ascending (left) and descending (right) pathways. The lateral and ventral spinothalamic tracts ascend
contralateral to the side of the body that is innervated.
C, cervical; D, distal; E, extensors; F, flexors; L, lumbar; P, proximal; S, sacral; T, thoracic.

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Picture; Common spinal cord syndromes

➢ Most fiber tracts—including the posterior columns and the spinocerebellar and
pyramidal tracts—are situated on the side of the body they innervate. However,
afferent fibers mediating pain and temperature sensation ascend in the
spinothalamic tract contralateral to the side they supply.
➢ The anatomic configurations of these tracts produce characteristic syndromes
that provide clues to the underlying disease process.
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Brown-Sequard [Hemicord] Syndrome

This consists of ipsilateral weakness (corticospinal tract) and loss of joint


position and vibratory sense (posterior column), with contralateral loss of
pain and temperature sense (spinothalamic tract) one or two levels
below the lesion.
Segmental signs, such as radicular pain, muscle atrophy, or loss of a
deep tendon reflex, are unilateral.
Partial forms are more common than the fully developed syndrome.

Central Cord Syndrome

➢ This syndrome results from selective damage to the gray matter nerve cells
and crossing spinothalamic tracts surrounding the central canal.
➢ In the cervical cord, the central cord syndrome produces arm weakness out of
proportion to leg weakness and a “dissociated” sensory loss, meaning loss of
pain and temperature sensations over the shoulders, lower neck, and upper
trunk (cape distribution), in contrast to preservation of light touch, joint position,
and vibration sense in these regions.
➢ Spinal trauma, syringomyelia, and intrinsic cord tumors are the main causes.

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Infarction of the cord is generally the result of occlusion or diminished


flow in this artery.
The result is bilateral tissue destruction at several contiguous levels that
spares
the posterior columns.
All spinal cord functions—motor, sensory, and autonomic—are lost below
the level of the lesion, with the striking exception of retained vibration
and position sensation.

Figure; Anterior Spinal Artery Syndrome

Foramen Magnum Syndrome

Lesions in this area interrupt decussating pyramidal tract fibers destined


for the legs, which cross caudal to those of the arms, resulting in
weakness of the legs (crural paresis).
Compressive lesions near the foramen magnum may produce weakness
of the ipsilateral shoulder and arm followed by weakness of the
ipsilateral leg, then the contralateral leg, and finally the contralateral
arm, an “around the clock” pattern that may begin in any of the four
limbs.
There is typically suboccipital pain spreading to the neck and shoulders.

Intramedullary and Extramedullary Syndromes

➢ It is useful to differentiate intramedullary processes, arising within the substance


of the cord, from extramedullary ones that lie outside the cord and compress
the spinal cord or its vascular supply.
➢ The differentiating features are only relative and serve as clinical guides.
➢ With extramedullary lesions, radicular pain is often prominent, and there is
early sacral sensory loss and spastic weakness in the legs with incontinence
due to the superficial location of the corresponding sensory and motor fibers in
the spinothalamic and corticospinal tracts.
➢ Regarding extramedullary lesions, a further distinction is made between
extradural and intradural masses, as the former are generally malignant and
the latter benign (neurofibroma being a common cause). Consequently, a long
duration of symptoms favors an intradural origin.
➢ Intramedullary lesions tend to produce poorly localized burning pain rather than
radicular pain and to spare sensation in the perineal and sacral areas (“sacral
sparing”), reflecting the laminated configuration of the spinothalamic tract with
sacral fibers outermost; corticospinal tract signs appear later.
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Complete cord transection

Causes
✓ Trauma
✓ Metastatic carcinoma
✓ Multiple sclerosis
✓ Spinal epidural haematoma
✓ Autoimmune disorders
✓ Post vaccinial syndromes
✓ Infectious and postinfectious disorders
All ascending tracts from below and descending tracts from above are
interrupted
Affects motor, sensory, and autonomic functions
✓ Sensory
▪ all sensations are affected
▪ Pin prick test is very valuable
▪ Segmental paresthesia occurs at the level of lesion
✓ Motor
▪ Paraplegia due to corticospinal tract
▪ First spinal shock-followed by hypertonic hyper reflexic
paraplegia
▪ Loss of abdominal and cremasteric reflexes
▪ At the level of lesion LMN signs occur
✓ Autonomic-
▪ Urinary retention and constipation
▪ Anhidrosis, trophic skin changes, vasomotor instability below
the level of lesion
▪ Sexual dysfunction can occur

Posterior column syndrome

➢ Occurs due to neurosyphilis, diabetes mellitus


➢ Usually occurs 10 to 20 yrs after infection
➢ Sensory
✓ Impaired position and vibration sense in LL
✓ Tactile and postural hallucinations can occur
✓ Numbness or paresthesia are frequent complaints
✓ Sensory ataxia
✓ Positive rhomberg sign
➢ Corticospinal tracts are spared
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Figure; Posterior column syndrome

Posterolateral column disease

Causes;
✓ Vit B12 deficiency
✓ AIDS
✓ HTLV Associated myelopathy
✓ Cervical spondylosis
Affects both the dorsal column and the lateral corticospinal tracts
Paresthesia in feet
Loss of proprioception and vibration in legs
Sensory ataxia
positive rhomberg sign
Bladder atony
Corticospinal tract involvement
✓ Spasticity
✓ Hyperreflexia
✓ Bilateral Babinski sign
AIDS associated dementia and spastic bladder is present
HTLV associated myelopathy
✓ slowly progressive paraparesis
✓ increase in csf igG antibodies to HTLV1

Figure; Posterolateral column disease

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7.2.1. Acute and subacute spinal cord diseases


Symptoms of the cord diseases that evolve over days or weeks are
focal
neck or back pain, followed by various combinations of paresthesia’s,
sensory loss, motor weakness, and sphincter disturbance.
There may be mild sensory symptoms only or a devastating functional
transection of the cord.
When paresthesia’s begin in the feet and then ascend a polyneuropathy
is often considered, and in such cases the presence of bladder
disturbances and a sharply demarcated spinal cord level provide
important clues to the spinal cord origin of the disease.
In severe and abrupt cases, areflexia reflecting spinal shock may be
present, but hyperreflexia supervenes over days or weeks; persistent
areflexic paralysis with a sensory level usually indicates necrosis over
multiple segments of the spinal cord.

Distinguishing Compressive from No compressive Myelopathy

➢ The first priority is to exclude treatable compression of the cord by a mass


lesion.
➢ The common causes are
✓ Tumor
✓ Epidural abscess or hematoma
✓ Herniated disk, and
✓ Spondylitic vertebral pathology.
➢ Epidural compression due to malignancy or abscess often causes warning
signs of neck or back pain, bladder disturbances, and sensory symptoms that
precede the development of paralysis.
➢ Spinal subluxation, hemorrhage, and non-compressive etiologies such as
infarction are more likely to produce myelopathy without antecedent symptoms
➢ MRI with gadolinium, centered on the clinically suspected level, is the initial
diagnostic procedure if it is available; it is often appropriate to image the entire
spine (cervical through sacral regions) to search for additional clinically silent
lesions.
➢ Once compressive lesions have been excluded, non-compressive causes of
acute myelopathy that are intrinsic to the cord are considered, primarily
vascular, inflammatory, and infectious etiologies.

Compressive myelopathies

A. Neoplastic Spinal Cord Compression

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In adults, most neoplasms are epidural in origin, resulting from


metastases to the adjacent vertebral column.
Almost any malignant tumor can metastasize to the spinal column, with
breast, lung, prostate, kidney, lymphoma, and myeloma being particularly
frequent.
The thoracic spinal column is most commonly involved
✓ Exceptions are metastases from prostate and ovarian cancer, which
occur disproportionately in the sacral and lumbar vertebrae,
probably from spread through Batson’s plexus, a network of veins
along the anterior epidural space.
Retroperitoneal neoplasms (especially lymphomas or sarcomas) enter the
spinal canal laterally through the intervertebral foramina and produce
radicular pain with signs of weakness that corresponds to the level of
involved nerve roots.
Pain is usually the initial symptom of spinal metastasis
✓ It may be aching and localized or sharp and radiating in quality
and typically worsens with movement, coughing, or sneezing and
characteristically awakens patients at night.
✓ A recent onset of persistent back pain, particularly if in the thoracic
spine (which is uncommonly involved by spondylosis), should
prompt consideration of vertebral metastasis.
✓ Rarely, pain is mild or absent.
Plain radiographs of the spine and radionuclide bone scans have a
limited role in diagnosis because they do not identify 15 - 20% of
metastatic vertebral lesions and fail to detect paravertebral masses that
reach the epidural space through the intervertebral foramina.
MRI provides excellent anatomic resolution of the extent of spinal
tumors and is able to distinguish between malignant lesions and other
masses—epidural abscess, tuberculoma, lipoma, or epidural hemorrhage,
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✓ Vertebral metastases are usually hypointense relative to a normal


bone marrow signal on T1-weighted MRI; after the administration of
gadolinium, contrast enhancement may deceptively “normalize” the
appearance of the tumor by increasing its intensity to that of
normal bone marrow.

Figure; Epidural spinal cord compression due to breast carcinoma. Sagittal T1-weighted (A) and T2-
weighted (B) magnetic resonance imaging scans through the cervicothoracic junction reveal an
infiltrated and collapsed second thoracic vertebral body with posterior displacement and compression
of the upper thoracic spinal cord. The low-intensity bone marrow signal in A signifies replacement by
tumor.

Infections of the spinal column (osteomyelitis and related disorders) are


distinctive in that, unlike tumor, they often cross the disk space to
involve the adjacent vertebral body.
If there are radicular symptoms but no evidence of myelopathy, it may
be safe to defer imaging for 24 - 48 h.
Up to 40% of patients who present with cord compression at one level
are found to have asymptomatic epidural metastases elsewhere; thus,
imaging of the entire length of the spine is important to define the
extent of disease.

Treatment of Neoplastic Spinal Cord Compression

Management of cord compression includes


✓ Glucocorticoids to reduce cord edema
✓ Local radiotherapy (initiated as early as possible) to the
symptomatic lesion, and
✓ Specific therapy for the underlying tumor type.
Glucocorticoids
✓ Glucocorticoids (typically dexamethasone, 10 mg IV, stat) can be
administered before an imaging study if there is clinical suspicion
of cord compression and continued at a lower dose (4 mg, PO,
QID) until definitive treatment with radiotherapy and/or surgical
decompression is completed.
Radiotherapy
✓ Radiotherapy alone may be effective even for some typically
radioresistant metastases.
✓ A good response to therapy can be expected in individuals who
are ambulatory at presentation.
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✓ Treatment usually prevents new weakness, and some recovery of


motor function occurs in up to one-third of patients.
✓ Motor deficits (paraplegia or quadriplegia), once established for >12
h, do not usually improve, and beyond 48 h the prognosis for
substantial motor recovery is poor.
✓ Although most patients do not experience recurrences in the
months following radiotherapy, with survival beyond 2 years
recurrence becomes increasingly likely and can be managed with
additional radiotherapy.
✓ Biopsy of the epidural mass is unnecessary in patients with known
primary cancer, but it is indicated if a history of underlying cancer
is
lacking.
Surgery
✓ Either decompression by laminectomy or vertebral
body resection
✓ Indicated when
▪ signs of cord compression worsen despite radiotherapy
▪ the maximum-tolerated dose of radiotherapy has been
delivered previously to the site, or
▪ a vertebral compression fracture or spinal instability contributes
to
cord compression.

Intradural mass

In contrast to tumors of the epidural space, most intradural mass


lesions are slow-growing and benign.
Meningiomas and neurofibromas account for most of these, with
occasional cases caused by chordoma, lipoma, dermoid, or sarcoma.
Meningiomas are often located posterior to the thoracic cord or near the
foramen magnum, although they can arise from the meninges anywhere
along
the spinal canal.

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Figure; MRI of a thoracic meningioma. Coronal T1-weighted postcontrast image through the
thoracic spinal cord demonstrates intense and uniform enhancement of a well-circumscribed
extramedullary mass (arrows) that displaces the spinal cord to the left.

Neurofibromas are benign tumors of the nerve sheath that typically arise
from the posterior root; when multiple, neurofibromatosis is the likely
etiology.
Symptoms usually begin with radicular sensory symptoms followed by an
asymmetric, progressive spinal cord syndrome.
Therapy is surgical resection.

Primary intramedullary tumors of the spinal cord

➢ They are uncommon.


➢ They present as central cord or hemicord syndromes, often in the
cervical region.
➢ There may be poorly localized burning pain in the extremities and sparing of
sacral sensation.
➢ In adults, these lesions are ependymomas, hemangioblastomas, or low-grade
astrocytomas.

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Figure; MRI of an intramedullary astrocytoma. Sagittal T1-weighted postcontrast image through


the cervical spine demonstrates expansion of the upper cervical spine by a mass lesion
emanating from within the spinal cord at the corticomedullary junction. Irregular peripheral
enhancement occurs within the mass (arrows).

➢ Complete resection of an intramedullary ependymoma is often possible with


microsurgical techniques.
➢ Debulking of an intramedullary astrocytoma can also be helpful, as these are
often slowly growing lesions; the value of adjunctive radiotherapy and
chemotherapy is uncertain.
➢ Secondary (metastatic) intramedullary tumors also occur, especially in patients
with advanced metastatic disease, although these are not nearly as frequent as
brain metastases.

Spinal Epidural Abscess

Spinal epidural abscess presents with


✓ Midline back or neck pain
✓ Fever, and
✓ Progressive limb weakness.
Aching pain is almost always present, either over the spine or in a
radicular pattern.
The duration of pain prior to presentation is generally ≤ 2 weeks but
may on occasion be several months or longer.
Fever is typically but not invariably present, accompanied by elevated
WBC count, raised ESR and CRP.
As the abscess expands, further spinal cord damage results from
venous
congestion and thrombosis.
Once weakness and other signs of myelopathy appear, progression may
be rapid and irreversible.
A more chronic sterile granulomatous form of abscess is also known,
usually
after treatment of an acute epidural infection.
Risk factors include an
✓ Impaired immune status (HIV, diabetes mellitus, renal failure,
alcoholism, malignancy)
✓ IV drug abuse, and
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✓ Infections of the skin or other tissues.


▪ 2/3rd of epidural infections results from hematogenous spread
of bacteria from the skin (furunculosis), soft tissue (pharyngeal
or dental abscesses; sinusitis), or deep viscera (bacterial
endocarditis). The remainder arises from direct extension of a
local infection to the subdural space
▪ Examples of local predisposing conditions are
• vertebral osteomyelitis
• decubitus ulcers
• lumbar puncture
• epidural anesthesia, or
• spinal surgery.
Etiology
✓ S. aureus
▪ MRSA is an important consideration, and therapy should be
tailored to this possibility.
✓ gram-negative bacilli
✓ Streptococcus, anaerobes, and fungi can also cause epidural
abscesses.
✓ Tuberculosis from an adjacent vertebral source (Pott’s disease)
remains an important cause in the developing world.

Investigations

➢ MRI localizes the abscess and excludes other causes of


myelopathy.

Figure; MRI of a spinal epidural abscess due to tuberculosis. A. Sagittal T2-weighted free
spin-echo MR sequence. A hypointense mass replaces the posterior elements of C3 and
extends epidurally to compress the spinal cord (arrows). B. Sagittal T1-weighted image after
contrast administration reveals a diffuse enhancement of the epidural process ( arrows) with
extension into the epidural space.

➢ Blood cultures
✓ Are positive in > 50% of cases, but direct aspiration of the abscess at
surgery is often required for a microbiologic diagnosis.
➢ Lumbar puncture
✓ It Is only required if encephalopathy or other clinical signs raise the
question of associated meningitis, a feature that is found in <25% of
cases.
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✓ The level of the puncture should be planned to minimize the risk of


meningitis due to passage of the needle through infected tissue.
✓ A high cervical tap is sometimes the safest approach.
✓ CSF abnormalities in epidural and subdural abscess consist of
▪ pleocytosis with a preponderance of polymorphonuclear cells
▪ an elevated protein level, and
▪ a reduced glucose levels
✓ the responsible organism is not cultured unless there is associated
meningitis.

Treatment of Spinal Epidural Abscess

➢ Treatment is by decompressive laminectomy with debridement


combined with long-term antibiotic treatment.
➢ Surgical evacuation prevents development of paralysis and may improve or
reverse paralysis in evolution, but it is unlikely to improve deficits of more
than several days in duration.
➢ Broad-spectrum antibiotics should be started empirically before surgery and
then modified on the basis of culture results
✓ vancomycin 15 - 20 mg/kg, IV, BID Plus
✓ ceftriaxone, 1gm, IV, BID Plus
✓ (if indicated for anaerobes) metronidazole 7.5 mg/kg IV, QID
➢ Medication is generally continued for 6 - 8 weeks.
➢ If surgery is contraindicated or if there is a fixed paraplegia or quadriplegia
that is unlikely to improve following surgery, long-term administration of
systemic and oral antibiotics can be used; in such cases, the choice of
antibiotics may be guided by results of blood cultures.
➢ Surgical management remains the treatment of choice unless the abscess is
limited in size and causes few or no neurologic signs.
➢ With prompt diagnosis and treatment of spinal epidural abscess, up to 2/3rd of
patients experiences significant recovery.

Spinal Epidural Hematoma

➢ Hemorrhage into the epidural (or subdural) space causes acute focal or
radicular pain followed by variable signs of a spinal cord or conus medullaris
disorder.
➢ Therapeutic anticoagulation, trauma, tumor, or blood dyscrasias are
predisposing conditions.
➢ Rare cases complicate lumbar puncture or epidural anesthesia.
➢ MRI and CT confirm the clinical suspicion and can delineate the extent of the
bleeding.
➢ Treatment consists of prompt reversal of any underlying clotting disorder and
surgical decompression.
➢ Surgery may be followed by substantial recovery, especially in patients with
some preservation of motor function preoperatively.
➢ Because of the risk of hemorrhage, lumbar puncture should be avoided
whenever possible in patients with severe thrombocytopenia or other
coagulopathies.
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Hematomyelia

➢ Hemorrhage into the substance of the spinal cord is a rare result of trauma,
intraparenchymal vascular malformation, vasculitis due to polyarteritis nodosa or
SLE, bleeding disorders, or a spinal cord neoplasm.
➢ Hematomyelia presents as an acute painful transverse myelopathy.
➢ With large lesions, extension into the subarachnoid space results in
subarachnoid hemorrhage.
➢ Diagnosis is by MRI or CT.
➢ Therapy is supportive, and surgical intervention is generally not useful.
✓ An exception is hematomyelia due to an underlying vascular
malformation, for which spinal angiography and endovascular occlusion
may be indicated, or surgery to evacuate the clot and remove the
underlying vascular lesion.

Non-Compressive myelopathies
The most frequent causes of non-compressive acute transverse
myelopathy are;
✓ spinal cord infarction
✓ infectious (primarily viral) causes.
✓ postinfectious or idiopathic transverse myelitis
▪ which is presumed to be an immune condition related to
acute disseminated encephalomyelitis
✓ systemic inflammatory disorders, including SLE and sarcoidosis
✓ demyelinating diseases, including multiple sclerosis (MS)
✓ neuromyelitis optica (NMO)
After spinal cord compression is excluded, the evaluation generally
requires a lumbar puncture and a search for underlying systemic
disease
Acute transverse myelopathies
✓ Rapidly progressive
✓ Maximum deficit in hrs to days
✓ The inflammation is generally restricted to one or two segments,
usually in the thoracic cord
✓ Symptoms develop rapidly over hrs; occasionally over several
weeks
✓ Typically, the inflammation is bilateral, producing weakness and
multimodality sensory disturbance below the level of the lesion
✓ Unilateral syndromes have been described as well
✓ Almost all patients develop Leg weakness of varying severity, arm
weakness if the lesion is in the cervical cord
✓ Bowel and bladder dysfunction also occur
✓ Rapid onset complete paraplegia & spinal shock are associated
with poorer outcomes

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Image; transverse myelopathy

☛ Spinal Cord Infarction

➢ The cord is supplied by three arteries that course vertically over its surface:
✓ a single anterior spinal artery and
✓ paired posterior spinal arteries.

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➢ The anterior spinal artery originates in paired branches of the vertebral arteries
at the cranciocervical junction and is fed by additional radicular vessels that
arise at C6, at an upper thoracic level, and, most consistently, at T11-L2
(artery of Adamkiewicz).
➢ At each spinal cord segment, paired penetrating vessels branch from the
anterior spinal artery to supply the anterior two-thirds of the cord; the posterior
spinal arteries, which often become less distinct below the midthoracic level,
supply the posterior columns.
➢ Spinal cord ischemia can occur at any level; however, the presence of the
artery of Adamkiewicz below, and the anterior spinal artery circulation above,
creates a region of marginal blood flow in the upper thoracic segments.
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➢ With hypotension or cross-clamping of the aorta, cord infarction typically occurs


at the level of T3-T4, and also at boundary zones between the anterior and
posterior spinal artery territories. The latter may result in a rapidly progressive
syndrome over hours of weakness and spasticity with little sensory change.
➢ Acute infarction in the territory of the anterior spinal artery produces “anterior
cord syndrome”.
✓ Paraplegia or quadriplegia
✓ Dissociated sensory loss affecting pain and temperature sense but sparing
vibration and position sense, and
✓ Loss of sphincter control
➢ Onset may be sudden but more typically is progressive over minutes or a few
hours, unlike stroke in the cerebral hemispheres.
➢ Sharp midline or radiating back pain localized to the area of ischemia is
frequent.
➢ Areflexia due to spinal shock is often present initially; with time, hyperreflexia
and spasticity appear.
➢ Less common is infarction in the territory of the posterior spinal arteries,
resulting in loss of posterior column function either on one side or bilaterally.
➢ Causes of spinal cord infarction include;
✓ Aortic atherosclerosis
✓ Dissecting aortic aneurysm
✓ Vertebral artery occlusion or dissection in the neck
✓ Aortic surgery
✓ Profound hypotension from any cause.
✓ A surfer’s myelopathy
✓ Cardiogenic emboli
✓ Vasculitis
✓ collagen vascular disease (particularly SLE, Sjögren’s syndrome, and the
antiphospholipid antibody syndrome).
✓ In a substantial number of cases, no cause can be found, and
thromboembolism in arterial feeders is suspected.
➢ MRI may fail to demonstrate infarctions of the cord, especially in the first day,
but often the imaging becomes abnormal at the affected level.
➢ In cord infarction due to presumed thromboembolism, acute anticoagulation is
not indicated, with the possible exception of the unusual transient ischemic
attack or incomplete infarction with a stuttering or progressive course.
➢ Prognosis following spinal cord infarction is influenced by the severity of the
deficits at presentation; patients with severe motor weakness and those with
persistent areflexia usually do poorly

2. Acute infectious myelitis (a.k.a Acute transverse myelitis)

Many viruses have been associated with an acute myelitis that is


infectious in nature rather than postinfectious.
Nonetheless, the two processes are often difficult to distinguish.
Etiologies
✓ Viral → most common
▪ Herpes zoster
▪ HSV types 1 and 2
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▪ HSV-2 (and less commonly HSV-1) produces a distinctive


syndrome of recurrent sacral cauda equina neuritis in
association with outbreaks of genital herpes (Elsberg’s
syndrome).
▪ EBV
▪ CMV
▪ rabies virus
▪ Zika virus
▪ Poliomyelitis → it is the prototypic viral myelitis, but it is more
or less restricted to the anterior gray matter of the cord
containing the spinal motoneurons.
▪ Enteroviruses (including enterovirus 71 and coxsackie)
▪ Japanese encephalitis and other flaviviruses such as West
Nile virus.
▪ Chronic viral myelitic infections, such as those due to HIV or
HTLV-1
✓ Bacterial and mycobacterial myelitis (most are essentially
abscesses)
are less common than viral causes and much less frequent than
cerebral bacterial abscess.
▪ Almost any pathogenic species may be responsible,
including
• Borrelia burgdorferi (Lyme disease)
• Listeria monocytogenes
• Mycobacterium tuberculosis, and
• Treponema pallidum (syphilis).
▪ Mycoplasma pneumoniae may be a cause of myelitis, but its
status is uncertain because many cases are more properly
classified as postinfectious.
✓ Parasitic
▪ Schistosomiasis is an important cause of parasitic myelitis in
endemic areas.
• The process is intensely inflammatory and granulomatous,
caused by a local response to tissue-digesting enzymes
from the ova of the parasite, typically Schistosoma
hematobium or Schistosoma mansoni.
▪ Toxoplasmosis can occasionally cause a focal myelopathy,
and this diagnosis should especially be considered in patients
with AIDS.
▪ Cysticercosis is another consideration in pork meet users,
although myelitis from this helminth is far less common than
parenchymal brain or meningeal involvement.

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* Clinical events that are consistent with transverse myelitis but that are not associated
with cerebrospinal fluid abnormalities or abnormalities detected on
MRI and that have no identifiable underlying cause are categorized as possible
idiopathic transverse myelitis.
† The IgG index is a measure of intrathecal synthesis of immunoglobulin and is
calculated with the use of the following formula: (CSF IgG ÷ serum IgG) ÷ (CSF
albumin ÷ serum albumin), where CSF denotes cerebrospinal fluid.

Management
➢ In cases of suspected viral myelitis, it may be appropriate to begin specific
therapy pending laboratory confirmation.
➢ Herpes zoster, HSV, and EBV myelitis are treated with
✓ Acyclovir,10 mg/kg, IV, TID for 10 - 14 days or
✓ valacyclovir 2 g PO, TID for 10 - 14 days
➢ CMV is treated with
✓ Ganciclovir, 5 mg/kg IV BID) for 2 weeks
plus
✓ Foscarnet, 60 mg/kg IV TID) for 2 weeks or
✓ Cidofovir, 5 mg/kg per week for 2 weeks.

3. Postinfectious myelitis

Many cases of myelitis, termed postinfectious or postvaccinal, follow an


infection or vaccination.
Numerous organisms have been implicated, including
✓ EBV
✓ CMV
✓ Mycoplasma
✓ Influenza
✓ Measles
✓ Varicella
✓ mumps, and
✓ yellow fever.
As in the related disorder acute disseminated encephalomyelitis,
postinfectious myelitis often begins as the patient appears to be
recovering from an acute febrile infection, or in the subsequent days or
weeks, but an infectious agent cannot be isolated from the nervous
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The presumption is that the myelitis represents an autoimmune disorder


triggered by infection and is not due to direct infection of the spinal
cord.
Treatment is usually with glucocorticoids or, in fulminant cases, plasma
exchange.

4. Multiple sclerosis (MS)


➢ MS may present with acute myelitis
➢ MS attacks rarely cause a transverse myelopathy (i.e., attacks of bilateral
sensory disturbances, unilateral or bilateral weakness, and bladder or bowel
symptoms), but it is among the most common causes of a partial cord
syndrome.
➢ MRI findings in MS-associated myelitis typically consist of mild swelling of the
cord and diffuse or multifocal “shoddy” areas of abnormal signal on T2-
weighted sequences.
➢ Contrast enhancement, indicating disruption in the blood-brain barrier associated
with inflammation, is present in many acute cases.
➢ Treatment of acute episodes of MS-associated myelitis consists of
methylprednisolone (500 mg, IV daily for 3 days) followed by oral prednisone
(1 mg/kg/d for several weeks, then gradual taper).
➢ A course of plasma exchange may be indicated for severe cases if
glucocorticoids are ineffective.

7.2.2. Chronic myelopathies (spinal cord diseases)

Syringomyelia

➢ Syringomyelia is a developmental cavity of the cervical cord that may


enlarge and produce progressive myelopathy or may remain asymptomatic.
➢ Symptoms begin insidiously in adolescence or early adulthood, progress
irregularly, and may undergo spontaneous arrest for several years.
➢ Many young patients acquire a cervical-thoracic scoliosis.
➢ More than half of all cases are associated with Chiari type 1 malformations in
which the cerebellar tonsils protrude through the foramen magnum and into the
cervical spinal canal.
➢ The presentation is a central cord syndrome consisting of a regional
dissociated sensory loss (loss of pain and temperature sensation with sparing
of touch and vibration) and areflexic weakness in the upper limbs.
➢ The sensory deficit has a distribution that is “suspended” over the nape of the
neck, shoulders, and upper arms (cape distribution) or in the hands.
➢ Most cases begin asymmetrically with unilateral sensory loss in the hands that
leads to injuries and burns that are not appreciated by the patient.
➢ Muscle wasting in the lower neck, shoulders, arms, and hands with asymmetric
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➢ As the cavity enlarges and compresses the long tracts, spasticity and
weakness of the legs, bladder and bowel dysfunction, and a Horner’s
syndrome appear.
➢ Some patients develop facial numbness and sensory loss from damage to the
descending tract of the trigeminal nerve (C2 level or above).
➢ In cases with Chiari malformations, cough-induced headache and neck,
arm, or facial pain may be reported.
➢ Extension of the syrinx into the medulla, syringobulbia, causes palatal or vocal
cord paralysis, dysarthria, horizontal or vertical nystagmus, episodic dizziness or
vertigo, and tongue weakness with atrophy.
➢ MRI accurately identifies developmental and acquired syrinx cavities and their
associated spinal cord enlargement.
➢ Images of the brain and the entire spinal cord should be obtained to delineate
the full longitudinal extent of the syrinx, assess posterior fossa structures
for the Chiari malformation, and determine whether hydrocephalus is present.

Treatment of syringomyelia

Treatment of syringomyelia is generally unsatisfactory.


The Chiari tonsillar herniation may be decompressed, generally by
suboccipital
craniectomy, upper cervical laminectomy, and placement of a dural
graft.
With Chiari malformations, shunting of hydrocephalus generally precedes
any attempt to correct the syrinx.
Surgery may stabilize the neurologic deficit, and some patients improve.
Patients with few symptoms and signs from the syrinx do not require
surgery and are followed by serial clinical and imaging examinations.
Syrinx cavities secondary to trauma or infection, if symptomatic, are
treated with a decompression and drainage procedure in which a small
shunt is inserted between the cavity and subarachnoid space;
alternatively, the cavity can be fenestrated.
Cases due to intramedullary spinal cord tumor are generally managed
by resection of the tumor.

2) Subacute combined degeneration (Vit B12 deficiency)

➢ This treatable myelopathy presents with subacute paresthesias in the hands


and feet, loss of vibration and position sensation, and a progressive spastic
and ataxic weakness.
➢ Loss of reflexes due to an associated peripheral neuropathy in a patient who
also has Babinski signs is an important diagnostic clue.
➢ Optic atrophy and irritability or other cognitive changes may be prominent in
advanced cases and are occasionally the presenting symptoms.
➢ The myelopathy of subacute combined degeneration tends to be diffuse rather
than focal; signs are generally symmetric and reflect predominant involvement
of the posterior and lateral tracts, including Romberg’s sign.
➢ Causes include dietary deficiency, especially in vegans, and gastric
malabsorption syndromes including pernicious anemia.
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➢ The diagnosis is confirmed by the finding of macrocytic red blood cells, a low
serum B12 concentration, and elevated serum levels of homocysteine and
methylmalonic acid.
➢ Treatment is by replacement therapy, beginning with 1000 μg of intramuscular
vitamin B12 repeated at regular intervals or by subsequent oral treatment.

3) Tabes dorsalis

The classic syphilitic syndromes of tabes dorsalis and meningovascular


inflammation of the spinal cord are now less frequent than in the past
but must be considered in the differential diagnosis of spinal cord
disorders.
The characteristic symptoms of tabes are fleeting and repetitive
lancinating pains, primarily in the legs or less often in the back, thorax,
abdomen, arms, and face.
Ataxia of the legs and gait due to loss of position sense occurs in half
of patients.
Paresthesias, bladder disturbances, and acute abdominal pain with
vomiting (visceral crisis) occur in 15 - 30% of patients.
The cardinal signs of tabes are
✓ loss of reflexes in the legs
✓ impaired position and vibratory sense
✓ Romberg sign; and
✓ in almost all cases, bilateral Argyll Robertson pupils, which fail to
constrict to light but accommodate.
Diabetic polyradiculopathy may simulate this condition.
Treatment of tabes dorsalis and other forms of neurosyphilis consists of
penicillin G, IV/IM in combination with oral probenecid

Reading Assignment

4) Chronic myelopathy of Multiple sclerosis


5) Spondylotic myelopathy
6) Vascular malformation of the cord and dura
7) Hereditary spastic paraplegia
8) Adeno myeloneuropathy
9) Hypocupric myelopathy

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7.2.3. Rehabilitation of spinal cord disorders


The prospects for recovery from an acute destructive spinal cord lesion
fade after ~6 months.
The disability associated with irreversible spinal cord damage is
determined primarily by the level of the lesion and by whether the
disturbance in function is complete or incomplete
Unexplained fever, worsening of spasticity, or deterioration in neurologic
function should prompt a search for infection, thrombophlebitis, or an
intraabdominal pathology.
✓ The loss of normal thermoregulation and inability to maintain
normal
body temperature can produce recurrent fever (quadriplegic fever),
although most episodes of fever are due to infection of the urinary
tract, lung, skin, or bone.
Bladder dysfunction generally results from loss of supraspinal
innervation of the detrusor muscle of the bladder wall and the sphincter
musculature.
✓ Detrusor spasticity is treated with anticholinergic drugs (oxybutynin,
2.5 - 5 mg qid) or TCA with anticholinergic properties (imipramine,
25 - 200 mg/d).
✓ Failure of the sphincter muscle to relax during bladder emptying
(urinary dyssynergia) may be managed with the α-adrenergic
blocking agent terazosin (1 - 2 mg TID or QID) Or Tamsulosin
0.4mg, PO, daily, with intermittent catheterization, or, if that is not
feasible, by use of a condom catheter in men or a permanent
indwelling catheter.
✓ Surgical options include the creation of an artificial bladder by
isolating a segment of intestine that can be catheterized
intermittently (enterocystoplasty) or can drain continuously to an
external appliance (urinary conduit).
✓ Bladder areflexia due to acute spinal shock or conus lesions is
best treated by catheterization.
Bowel regimens and disimpaction are necessary in most patients to
ensure at
least biweekly evacuation and avoid colonic distention or obstruction.
Patients with acute cord injury are at risk for venous thrombosis and
pulmonary embolism.
✓ Use of calf-compression devices and anticoagulation with LMWH is
recommended.
✓ In cases of persistent paralysis, anticoagulation should probably be
continued for 3 months.
Prophylaxis against decubitus ulcers should involve
✓ Frequent changes in position in a chair or bed
✓ the use of special mattresses, and
✓ cushioning of areas where pressure sores often develop, such as
the sacral prominence and heels.
Early treatment of ulcers with careful cleansing, surgical or enzyme
debridement of necrotic tissue, and appropriate dressing and drainage
may prevent infection of adjacent soft tissue or bone
Spasticity is aided by stretching exercises to maintain mobility of joints.
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Diazepam is useful for leg spasms that interrupt sleep (2 - 4 mg at


bedtime).
Management of chronic pain
✓ Despite the loss of sensory function, many patients with spinal cord
injury experience chronic pain sufficient to diminish their quality of
life
A paroxysmal autonomic hyperreflexia may occur following lesions above
the major splanchnic sympathetic outflow at T6.
✓ Headache, flushing, and diaphoresis above the level of the lesion,
as well as hypertension with bradycardia or tachycardia, are the
major symptoms.
✓ The trigger is typically a noxious stimulus—for example, bladder or
bowel
distention, a urinary tract infection, or a decubitus ulcer—below the
level of the cord lesion.
✓ Treatment consists of removal of offending
stimuli or short-acting antihypertensive drugs are useful in some
patients.
Attention to these details allows longevity and a productive life for
patients with complete transverse myelopathies.

7.3. GBS (Guillain-Barré syndrome)

➢ Guillain-Barré syndrome (GBS) is an acute, frequently severe, and


fulminant polyradiculoneuropathy that is autoimmune in nature.
➢ Males are at slightly higher risk for GBS than females, and in Western
countries, adults are more frequently affected than children.

Clinical Manifestations

8 A’s of GBS
✓ Autoimmune
✓ Areflexia
✓ Ascending paralysis
✓ Acute
✓ Afebrile
✓ Absence of sensory level
✓ Autonomic involvement → OHT, arrythmia
✓ Acellular CSF (albumin cytogenic dissociation → decreased number
of cells but, increased protein/albumin of CSF)
GBS manifests as a rapidly evolving areflexic motor paralysis with or
without sensory disturbance.
The usual pattern is an ascending paralysis that may be first noticed as
rubbery legs.
Weakness typically Acute evolving over hours to a few days and is
frequently accompanied by tingling dysesthesias in the extremities.
The legs are usually more affected than the arms, and facial diparesis
is
present in 50% of affected individuals.
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The lower cranial nerves are also frequently involved, causing bulbar
weakness with difficulty handling secretions and maintaining an airway;
the diagnosis in these patients may initially be mistaken for brainstem
ischemia.
Pain in the neck, shoulder, back, or diffusely over the spine is also
common in the early stages of GBS, occurring in ~50% of patients.
Most patients require hospitalization, and in different series, up to 30%
require ventilatory assistance at some time during the illness.
The need for mechanical ventilation is associated with more severe
weakness on admission, a rapid tempo of progression, and the
presence of facial and/or bulbar weakness during the first week of
symptoms.
Fever and constitutional symptoms are absent at the onset and, if
present, cast doubt on the diagnosis.
Deep tendon reflexes attenuate or disappear within the first few days of
onset.
Cutaneous sensory deficits (e.g., loss of pain and temperature
sensation) are usually relatively mild, but functions subserved by large
sensory fibers, such as deep tendon reflexes and proprioception, are
more severely affected.
Bladder dysfunction may occur in severe cases but is usually transient.
If bladder dysfunction is a prominent feature and comes early in the
course or there is a sensory level on examination, diagnostic
possibilities other than GBS should be considered, particularly spinal
cord disease.
Once clinical worsening stops and the patient reaches a plateau (almost
always within 4 weeks of onset), further progression is unlikely.
Autonomic involvement is common and may occur even in patients
whose GBS is otherwise mild.
✓ The usual manifestations are loss of vasomotor control with wide
fluctuations in blood pressure, postural hypotension, and cardiac
dysrhythmias.
✓ These features require close monitoring, and management and can
be fatal.
Pain is another common feature of GBS
✓ in addition to the acute pain described above, a deep aching pain
may be present in weakened muscles that patients liken to having
over exercised the previous day.
✓ Other pains in GBS include dysesthetic pain in the extremities as a
manifestation of sensory nerve fiber involvement.
✓ These pains are self-limited and often respond to standard
analgesics.

Subtypes of GBS

➢ Several subtypes of GBS are recognized, as determined primarily by


electrodiagnostic (Edx) and pathologic distinctions (see table below).
✓ Acute inflammatory demyelinating polyneuropathy (AIDP) → The most
common variant
✓ Acute motor axonal neuropathy (AMAN)
✓ Acute motor sensory axonal neuropathy (AMSAN). often clinically severe
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✓ Miller Fisher syndrome (MFS)


▪ regional variant which presents as rapidly evolving ataxia and
areflexia of limbs without weakness, and ophthalmoplegia, often
with pupillary paralysis.
▪ The MFS variant accounts for ~5% of all cases
✓ Other regional variants of GBS include
▪ Pure sensory forms
▪ Ophthalmoplegia as part of severe motor-sensory GBS
▪ GBS with severe bulbar and facial paralysis, sometimes
associated with antecedent CMV infection and
▪ Acute pandysautonomia

Antecedent Events

Approximately 70% of cases of GBS occur 1 - 3 weeks after an acute


infectious process, usually respiratory or GI.
20 - 30% of all cases are preceded by infection or reinfection with
Campylobacter jejuni.
A similar proportion is preceded by CMV or EBV.
Other viruses (e.g., HIV, hepatitis E, Zika) and also Mycoplasma
pneumoniae have been identified as agents involved in antecedent
infections, as have recent immunizations.
Post vaccine association → influenza vaccine, Older-type rabies vaccine
GBS also occurs more frequently in patients with lymphoma (including
Hodgkin’s disease), in HIV-seropositive individuals, and in patients with
SLE.

Laboratory Features

➢ CSF findings are distinctive, consisting of an elevated CSF protein level (100 -
1000 mg/dL]) without accompanying pleocytosis.
➢ The CSF is often normal when symptoms have been present for ≤48 h; by the
end of the first week, the level of protein is usually elevated.
➢ A transient increase in the CSF white cell count (10 - 100/μL) occurs on
occasion in otherwise typical GBS; however, a sustained CSF pleocytosis
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suggests an alternative diagnosis (viral myelitis) or a concurrent diagnosis such


as unrecognized HIV infection, leukemia or lymphoma with infiltration of nerves,
or neurosarcoidosis.
➢ Electrodiagnostic studies

Treatment of GBS

➢ In the vast majority of patients with GBS, treatment should be


initiated as soon after diagnosis as possible.
➢ Each day counts; ~2 weeks after the first motor symptoms, it is not known
whether immunotherapy is still effective.
➢ If the patient has already reached the plateau stage, then treatment probably is
no longer indicated, unless the patient has severe motor weakness and one
cannot exclude the possibility that an immunologic attack is still ongoing.
➢ Either high-dose intravenous immune globulin (IVIg) or plasmapheresis can be
initiated, as they are equally effective for typical GBS.
➢ A combination of the two therapies is not significantly better than either alone.
➢ IVIg is often the initial therapy chosen because of its ease of administration
and good safety record.
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➢ IVIg may be preferable to plasma exchange (PE) for the AMAN and MFS
variants of GBS.
➢ IVIg is administered as five daily infusions for a total dose of 2 g/kg.
➢ A course of plasmapheresis usually consists of ~40–50 mL/kg PE 4 - 5 times
over 7 - 10 days.
➢ treatment reduces the need for mechanical ventilation by nearly half (from 27
to 14% with PE) and increases the likelihood of full recovery at 1 year (from
55 to 68%).
➢ Functionally significant improvement may occur toward the end of the first
week of treatment or may be delayed for several weeks.
➢ The lack of noticeable improvement following a course of IVIg or PE is not an
indication to treat with the alternate treatment.
➢ However, there are occasional patients who are treated early in the course of
GBS and improve, who then relapse within a month.
➢ Brief retreatment with the original therapy is usually effective in such cases.
➢ Glucocorticoids have not been found to be effective in GBS.
➢ Occasional patients with very mild forms of GBS, especially those who appear
to have already reached a plateau when initially seen, may be managed
conservatively without IVIg or PE.
➢ In the worsening phase of GBS, most patients require monitoring in a critical
care setting, with particular attention to vital capacity, heart rhythm, blood
pressure, nutrition, deep-vein thrombosis prophylaxis, cardiovascular status,
early consideration (after 2 weeks of intubation) of tracheotomy, and chest
physiotherapy.
➢ As noted, ~30% of patients with GBS require ventilatory assistance, sometimes
for prolonged periods of time (several weeks or longer).
➢ Frequent turning and assiduous skin care are important, as are daily range-of
motion exercises to avoid joint contractures and daily reassurance as to the
generally good outlook for recovery.

Prognosis and Recovery


Approximately 85% of patients with GBS achieve a full functional
recovery within several months to a year, although minor findings on
examination (such as areflexia) may persist and patients often complain
of continued symptoms, including fatigue.
The mortality rate is <5% in optimal settings; death usually results from
secondary pulmonary complications.
Poor prognosis features
✓ patients with severe proximal motor and sensory axonal damage.
✓ advanced age
✓ a fulminant or severe attack, and
✓ a delay in the onset of treatment.
Between 5 and 10% of patients with typical GBS have one or more late
relapses; many of these cases are then classified as chronic
inflammatory demyelinating polyneuropathy (CIDP).

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Chronic inflammatory demyelinating polyneuropathy


(CIDP)
CIDP is distinguished from GBS by its chronic course.
Onset is usually gradual over a few months or longer, but in a few
cases, the initial attack is indistinguishable from that of GBS.
In other respects, this neuropathy shares many features with the
common demyelinating form of GBS, including elevated CSF protein
levels and the Edx findings of acquired demyelination.
Most cases occur in adults, and males are affected slightly more often
than females.
The incidence of CIDP is lower than that of GBS, but due to the
protracted course, the prevalence is greater.

7.4. ALS (Amyotrophic Lateral Sclerosis and Other Motor


Neuron Diseases)

ALS is the most common progressive motor neuron disease.


It is a prime example of a neurodegenerative disease and is arguably
the
most devastating of the neurodegenerative disorders that produces
progressive weakness, usually with mixed UMN & LMN signs.
The pathologic hallmark of motor neuron degenerative disorders is death
of lower motor neurons (consisting of anterior horn cells in the spinal
cord and their brainstem homologues innervating bulbar muscles) and
upper, or corticospinal, motor neurons (originating in layer five of the
motor cortex and descending via the pyramidal tract to synapse with
lower motor neurons, either directly or indirectly via interneurons)
Symptoms begin insidiously in older adults (usually >60 yrs) and
progress inexorably
In typical pts, there is asymmetric limb weakness with a mixture of UMN
& LMN features
Sensory & sphincter disturbances are usually absent
MRI is normal
EMG typically shows denervation in clinically affected muscles.
Unusual variants of ALS… Primary Lateral Sclerosis

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Chapter 8; Meningitis (ማጅራት ገትር)


Dr. Mulualem. G, Dr. Robel. D

Clinical features and how to write hx of meningitis


patient

History

➢ Pt’s may present with


Headache
Neck stiffness
Vomiting
➢ Triads of meningitis18 include fever, headache and neck stiffness (Nuchal
rigidity) → triads happen in 44% of pts
➢ 2 of 4 (fever, headache, stiff neck, change in Mentation) present in 95%
➢ Fever and either headache, stiff neck or an altered level of consciousness will
be present in nearly every patient
▪ >75% of patients have a decreased level of consciousness which ranges
from lethargy to coma
➢ Seizure Occur in 20-40% as initial presentation or during the course of the
illness
▪ Focal seizures are usually due to
• Structural causes
• Focal arterial ischemia or infarction,
• Cortical venous thrombosis with haemorrhage, or
• Focal edema
▪ Generalized seizure and status epilepticus may be due to
• Hyponatremia,
• Cerebral anoxia, or
• Toxic effects of antimicrobials such as high dose penicillin
➢ Presentation may be atypical (eg, lethargy without fever) in the elderly and
immunosuppressed.

Patient history characterization


➢ Headache
Gradual in onset
Intermittent / persistent
Globalized
Dull aching type
Severe/moderate
Aggravated by coughing, sitting position, loud voice

18
Relieved by sleeping and keeping silent

According to UpToDate 2018 triads include fever, nuchal rigidity and change in mental status
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✓ Worse during awakening from sleep


Occurs ‘’X’’ times per month and lasts for ‘’Y’’ minutes
May/may not be responsive to analgesics
Remark; accentuation of headache by horizontal rotation of the head
is sensitive maneuver (known as Jolt accentuation of headache)
➢ Neck stiffness
➢ Fever
Low grade (in viral, fungal and TB meningitis) or high grade (in
pyogenic/bacterial meningitis)
Intermittent / persistent
Associated with chills and rigor. In most cases (especially in viral
fungal and TB meningitis) there may not be chills or rigor
➢ Vomiting
Projectile (if there is increased ICP), if vomiting is projectile there is
no preceding nausea i.e. projectile doesn’t merely mean project
forward
➢ Photophobia
➢ Associated with Abnormal body movement
Starts abruptly
With or without warning manifestations
Generalized/partial
With up rolling of the eyes and drooling of saliva
Followed by excessive salivation, bleeding from the tongue (tongue
bite), urinary or faecal incontinence (observed by one of family
members)
Finally, LOC → ask duration of LOC which is mostly less than 5
minutes
➢ Night sweat
Common in TB meningitis
➢ Weight loss

Risk factors

➢ URTI (sinusitis, otitis media → S.pneumonia)


➢ Pyogenic chest infection
➢ Pyogenic Dental infection → also high risk for brain abscess
➢ Chronic alcohol intake → S.pneumonia, N.meningitidis, brain abscess
➢ DM → S.pneumonia
➢ Immunocompromising condition → S.pneumonia, N.meningitidis
Old age
Malignancy (especially hematologic malignancy)
Malnutrition
Steroid use
Chemoradiotherapy
Chronic medical disease like RVI, DM, CLD, CKD…
Pregnancy
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Splenectomy
✓ RF for infection by encapsulated microorganisms like
S.pneumonia
➢ Overcrowding (dormitory life, refuges, military camp) → meningococcal infection
through nasal droplets, viral meningoencephalitis
➢ Skin or oral lesions → viral meningoencephalitis
➢ Geographic location
The largest burden of meningococcal disease occurs in an area of
sub-Saharan Africa known as Meningitis belt which stretches from
Senegal in the west to Ethiopia in the east (26 countries)
North western part of Ethiopia is in the area of meningitis belt
(Gondar, quara, metema, armachiho, metekel….)

Complication of meningitis

Acute complications Chronic complications


Raised ICP Hearing loss and blindness
Seizure epilepsy
Brain abscess Cognitive impairment
DIC → especially in Focal paralysis
meningococcal infection Subdural effusion
Cerebral oedema Hydrocephalus
Coma Ataxia
DHN Bilateral adrenal haemorrhage
Respiratory arrest
Pericardial effusion

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Sample history

Chief compliant

headache of one-week duration

HPI

This patient was last relatively healthy a week back, at which time she began
to experience a gradual onset of globalized, dull aching, persistent type of
headache which is moderate in intensity, aggravated by coughing, sitting
position and loud voice, relieved by sleeping and keeping silent associated
with high grade intermittent fever with chills and rigors.

Two days before admission the headache got worsen and developed painful
neck stiffness associated with 3 episodes of non-projectile, nonfoul smelling,
non-blood tingled vomiting of ingested matter but no photophobia. She also
developed 2 episodes of generalized abnormal body movements which Starts
abruptly without warning manifestations, with up rolling of eyes, bleeding from
tongue followed by excessive salivation and urinary incontinence which is
observed by her brother. Finally, she loses her consciousness and gains her
consciousness approximately 5 to 10 minutes later in each episode.

She neither visit any health facility nor took any antipain or antibiotics. Finally,
her families bring her to our hospital when she develops abnormal body
movement.

No hx of discharge from the nose, ear, upper facial pain, ear/nose pain,
morning frontal headache or rhinorrhea (URTI → RF)
No hx of smoking or chronic alcohol intake (RF)
No hx of cough, chest pain or contact with a known TB patient (meningitis
from respiratory source like TB meningitis, bacterial meningitis /S.pneumonia, H.influenza/)
No hx of skin rash, joint pain (skin lesions like vesicles are RF for viral meningitis and
petechae suggest meningococcal infection)
No hx of abdominal surgery (splenectomy → RF)
No hx of DM, HTN or Asthma (Chronic medical condition and immunocompromisation → RF)
She was not screened for RVI but no history of MSP, chronic diarrhea,
oral thrush or body rash (immunocompromisation → RF)
No hx of blindness or hearing difficulty (chronic CXN)
No hx of gum bleeding, epistaxis, or bleeding from other sites (DIC → CXN)
No hx of head trauma or neuro surgery (RF for brain abscess, SAH → DDX)
No hx of swelling over the neck, axilla or groin (carcinomatous meningitis → DDX)
No hx of MSP, penile or vaginal discharge (syphilitic meningitis → DDX)
Lives in malaria non endemic area and no hx of malarial attack or
travel hx to malaria endemic area (cerebral mmalaria → DDX)
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No hx of drug intake (NSAIDS, antiepileptics, steroids → cause headache and neck stiffness →
DDX, Steroids are immunosuppressive as RF, if empirical antibiotics was given it is better to consider
partially treated meningitis)

Finally, she was admitted to our hospital supported physically by her


families

Physical examination (pertinent findings)

1 GA

2 Vital signs

Cushing triad from raised ICP


1. BP → HTN
2. PR → bradycardia
3. RR → irregular breathing pattern

3 HEENT

Ear/nose tenderness, ear discharge, rhinorrhea (sinusitis, otitis media → RF)


A history of head trauma with or without skull fracture or presence of a
chronically draining ear is associated with pneumococcal involvement.
Funduscopic findings: papilledema, absent venous pulsations
4 LGS

Parotid enlargement → mumps

5 RS

6 CVS

7 Abdominal examination

8 GUS

9 MSS

10 IS

Skin rash: Erythematous maculopapular, petechial, or purpuric over the


trunk, LL, conjunctiva or mucous membrane (typical for meningococcal, may
present with H. influenza and rare with pneumococcal)
Grouped vesicles → VZV

NS
+ve Meningeal irritation signs (Kerning sign, Brudzinski sign, Neck stiffness)
o Nuchal rigidity (Sensitivity 30%)
o Kernig’s sign → Patient supine, hip flexed at 90, knee flexed at 90;
+ve if passive extension of knee results in resistance
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o Brudzinski’s sign → Patient supine and limbs supine; +ve if passive


neck flexion if followed by involuntary hip and/or knee flexion.

➢ Kernig’s and Brudzinski’s signs are +ve in only 5% of Pts, but will be very
specific for meningeal irritation if present.
➢ May be negative in
✓ Very young or elderly patients
✓ Immunocompromised
✓ Severe coma
✓ Partially treated meningitis
Some patients may have focal neurologic findings (about 30%; hemiparesis,
aphasia, visual field cuts, CN palsies)
Raised ICP signs
✓ Change in mentation is the earliest sign
✓ Papilledema
✓ Dilated and poorly reactive pupil which indicate CN III palsy
✓ CN VI palsy
✓ Decerebrate posture
✓ Cushing reflex (bradycardia, hypertension, and irregular respirations).
Altered level of consciousness → viral meningoencephalitis
Aphasia, ataxia, seizure → viral meningoencephalitis (seizure happens in
bacterial meningitis also)

DDX
1. Meningitis
Pyogenic meningitis → i.e. bacterial meningitis
Viral (aseptic) meningitis
TB meningitis
✓ Phases of TB
☛ Prodromal phase → nonspecific smx like fever, night
sweat, weight loss…
☛ Meningitis phase → nuchal rigidity, CN palsy (single
CN involved)
☛ Coma (paralysis) → weakness, multiple CN involvement
Fungal meningitis
Chemical meningitis → also aseptic like viral
Syphilitic meningitis → meningitis occur in all stages of syphilis
Carcinomatous meningitis
✓ Cmnly from ALL, AML, Lymphoma
✓ Initially manifest with cmn C/F of leukaemia (bone pain, BM
failure smx) then progress to meningitis
2. Cerebral malaria
Acute CXN of malaria
Infection with P. falciparum
Have nuchal rigidity, fever and headache
Cmn in endemic area
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In repeated malarial attack if the last attack is ≥ 10 years, no risk of


cerebral malaria (i.e. for cerebral malaria the last attack should be <
10 years)
LOC for > 30 minutes
✓ Repeated seizure without gaining consciousness
✓ Cerebral malaria is unlikely in fully awake patients
3. Brain abscess
Triads of brain abscess include fever, headache, FND
Rupture of the abscess is the cause of meningeal irritation
4. Typhoidal meningitis
Rare
Have psychotic features
1st manifest as
✓ Abdominal pain
✓ Diarrhoea
✓ Stepladder fever
✓ Headache
✓ prostration
✓ It needs at least weeks to develop meningitis
Cmn in poor socioeconomic status
5. SAH
‘’The worst headache ever’’
The preceding mild to moderate headache caused by vascular
aneurysm
Change in mentation
FND (e.g. Stroke)
6. Epidural or subdural empyema
7. Encephalitis → have associated bizarre behaviour and confusion
8. Vasculitis in cranium → thrombophlebitis (giant cell arthritis)
9. Migraine

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IX

N.B.
High index of clinical suspicion is very important for early diagnosis of
meningitis to avoid death or unfavorable complications.

❖ LP (CSF Analysis) → refer short case of Nitsbin (click here → CSF analysis)
o If LP is delayed (e.g after CT scan) or not indicated (uncontrolled
significant bleeding tendencies), withdraw two sets of blood culture
prior to antibiotics. Repeated (follow-up) LP is important if poor
clinical response after 48hrs of appropriate antibiotic, or CSF shunt
present, otherwise may not be necessary.
❖ Blood cultures before antibiotics are administered. Initial blood tests should
include two sets of blood cultures.
Culture can be done also from CSF, throat swab, stool, urine based
on aetiology
+ve for HiB, S.pneumonia, N.mengitidis
❖ CBC
Neutrophilic dominant leucocytosis in pyogenic meningitis
Leucocytosis also expected in brain abscess
Leukopenia and thrombocytopenia with poor outcome in bacterial
meningitis
❖ PICT
❖ Serum electrolyte
❖ OFT → RFT, LFT
❖ ESR & CRP
❖ PT & PTT → to r/o DIC
❖ Head CT
to rule out mass effect before LP (To r/o space occupying lesions
if raised ICP is suspected and LP is contra indicated)
o however, in patients with mass effect, herniation may occur
without LP and may not occur even with LP
CT scan before LP in those with high-risk feature
✓ age>60 year
✓ immunosuppressed
✓ history of CNS disease,
✓ new-onset seizure
✓ change in mental state
✓ focal neurologic findings
✓ papilledema
CT Can identify
✓ CNS tumor
✓ SAH
✓ EDH/SDH
❖ MRI
Superior than CT to demonstrate cerebral edema and ischaemia
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Can show diffuse meningeal enhancement


R/o space occupying lesions
❖ CXR
To identify the source of infection with cmn etiologies affecting chest
and meninges like bacterial meningitis (S.pneumonia, H.influenza), TB
meningitis
❖ PCR
For CNS viral/mycoplasma infection
Has high sensitivity

Discussion

Meningitis

➢ Meningitis is an inflammation of the meninges in response to an infection.


➢ Bacterial meningitis is an acute purulent infection within the sub-arachnoid
space.
➢ It is associated with a CNS inflammatory reaction that may result in
decreased consciousness, seizures, raised intracranial pressure (ICP), and
stroke.
➢ The meninges, the subarachnoid space, and the brain parenchyma are all
frequently involved in the inflammatory reaction –meningo-encephalitis.
➢ The organisms most often responsible for community-acquired bacterial
meningitis are
o Streptococcus pneumoniae (50%)
o Neisseria meningitidis (25%)
o Group B streptococci (15%), and
o Listeria monocytogenes (10%).
➢ S. pneumoniae is the most common cause of meningitis in adults >20 years
of age accounting for nearly half of the cases
➢ Haemophilus influenzae type b accounts for <10% of cases of bacterial
meningitis in most series.
➢ Also caused by viral infections (HSV, Enteroviruses, HIV, VZV, etc), fungal
infections (Cryptococcus neoformans in immune-suppressed host) and M.TB.
➢ There had been multiple epidemic outbreaks of N.meningitidis and cause
death to millions in Ethiopia.
➢ Ethiopia is one of the countries in the so called "meningitis belt" of the Sub-
Saharan Africa. Several devastating epidemics have occurred cycling on an
average of 8-12 years in this geographic area. One striking feature of the
epidemic has been its seasonality by which it tends to occur during the dry
and windy season between January and May. All regions of the country are
at risk for meningitis outbreak.

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Picture; Meningitis belt

➢ Group B streptococcus, or S. agalactiae, was previously responsible for


meningitis predominantly in neonates, but it has been reported with increasing
frequency in individuals >50 years of age, particularly those with underlying
diseases.
➢ L. monocytogenes is an increasingly important cause of meningitis in
neonates (<1 month of age), pregnant women, individuals >60 years, and
immuno compromised individuals of all ages.
➢ Staphylococcus aureus and coagulase-negative staphylococci are important
causes of meningitis that occurs following invasive neurosurgical procedures,
particularly shunting procedures for hydrocephalus, or as a complication of the
use of subcutaneous Ommaya reservoirs for administration of intra-thecal
chemotherapy.

Meningitis Vs encephalitis
Meningitis Encephalitis
Inflammation predominantly affecting Inflammation of the brain parenchyma
the subarachnoid space
Commonly caused by bacterial Caused by viral aetiologies
aetiologies
Nuchal rigidity is the prominent ➢ Presents with focal or generalized
symptom neuropsychological dysfunction
➢ Bizarre behaviour and confusion are
common features

Pathophysiology
➢ Colonization of the nasopharynx by attaching to the epithelial cells
➢ Invasion of the intravascular space
➢ Avoid phagocytosis by neutrophils and complement mediated bactericidal
activity in the bloodstream because of the presence of a polysaccharide
capsule
➢ Directly infect choroid plexus epithelial cells to reach the CSF
➢ Multiply rapidly within the CSF due to the paucity of effective host immune
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defences in the CSF


➢ Bacterial proliferation induces inflammatory response and the formation of
purulent exudate in the subarachnoid space

Clinical presentation and diagnosis → see the approach section above

Management of meningitis

Management algorithm for adults with suspected bacterial meningitis

Suspicion of bacterial meningitis

Immunocompromize, history of CNS disease, new onset seizure,


papilledema, altered consciousness or focal neurological deficit

Yes
Blood culture and lumbar No Blood culture urgently
puncture (LP) urgently
Give empiric antibiotic

Give empiric antibiotic


Perform CT scan of head

CSF finding consistent


with bacterial meningitis
Contraindications for LP
s
No Yes
No Yes
Consider alternative diagnosis Positive CSF gram stain
Perform LP Continue treatment for
No Yes bacteria or consider
Continue empiric Adjust (targeted) alternative diagnosis
antibiotic therapy antimicrobial therapy

Algorithm: Management algorithm for adults with suspected bacterial meningitis

➢ Acute bacterial meningitis is a medical emergency. In untreated cases the


mortality approaches 100%.
➢ Institute empiric antimicrobial therapy promptly and adjust it after isolating
the etiologic agent. Delayed treatment of bacterial meningitis results in an
increased mortality (in-hospital mortality increases by 1.1 per hour of delay)
and unfavorable outcomes at discharge.
➢ The duration of pathogen-directed therapy depends on the causative
organism.

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Supportive Therapy:
➢ Hydration: both under and over hydration may have unfavorable consequences.
An IV maintenance fluid might be preferred over restricted fluid intake in the
first 48 hours in settings with high mortality and lately presenting patients.
➢ Nutrition support if required (NGT if necessary)
➢ Analgesia and/or antipyretic:
o Paracetamol, 1 g, PO, 4 - 6 hourly when required, with maximum daily
dose of: 4 g in 24 hours.
o Alternative: Ibuprofen, 400 mg, PO, TID with meals, if needed.
➢ Close supervision with regular monitoring of vital signs and neurological state.
➢ Institution of coma care for complicated cases.
➢ The use of adjunctive corticosteroids is controversial. Based on the existing
current evidence they are not recommended in low- and middle-income
countries as they do not demonstrated benefit
o If used; Dexamethasone 10 mg IV QID for 04 days

Empiric antibiotic treatment


➢ The initial approach to treatment in a patient with suspected Acute bacterial
meningitis includes performance of a LP to determine whether the CSF findings
are consistent with the diagnosis (Algorithm above).
➢ The duration of therapy is 10 to 14 days, for uncomplicated meningitis.
However, it can be adjusted depending on the specific causative pathogen,
once identified (7 days for meningococcus and H. influenzae, 10-14 days for
pneumococcus, up to 21 days for group B Streptococcus, Staphylococcus
aureus, Listeria monocytogenes, and gram-negative meningitis.
➢ Immunosuppressed (HIV positive, uncontrolled diabetes, patients taking high
dose corticosteroids) individuals may also need antifungal and/or viral coverage.

Table 1: Empiric antibiotic recommendations for acute bacterial meningitis*


Empiric therapy for COMMUNITY ACQUIRED acute bacterial meningitis
Population Likely pathogen First line Second line
Age < 1 Gram negatives ➢ Ampicillin, 150 to 200 mg/kg/day in ➢ Ampicillin PLUS
month Staphylococcus, divided doses every 3 to 4 hours, IV ➢ gentamycin, 2 to
(rarely up Enterococcus, PLUS 2.5 mg/kg/dose, IV,
to 3 Pneumococcus ➢ Cefotaxime, 225 to 300 mg/kg/day, IV, TID
months) TID or QID OR
➢ Meropenem only
Duration; for up to 21 days (if specific o 40 mg/kg, IV,
agent not identified) TID (maxi: 2g,
TID)
1 month/3 S. pneumoniae, ➢ Ceftriaxone, 100mg/kg/day, IV BID -
months to 50
Years
H. influenzae,
Meningococcus
PLUS
➢ Vancomycin, 15 mg/kg/dose, IV, QID
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Duration; for 10-14 days (If specific agent not


identified)
>50 years, S. pneumoniae, ➢ Ceftriaxone, 2 g, IV, BID Plus ➢ Ampicillin Plus
alcoholism or Meningococcus, ➢ Ampicillin, 3g, IV, QID (2g IV q4h) PLUS ➢ Gentamycin, 5
other Listeria, gram ➢ Vancomycin, 1g, IV, BID mg/kg/day, IV, TID
diseases of negative bacilli Duration; for up to 21 days OR
impaired ➢ Ceftazidime, 2g IV,
imunity TID or QID
With or without
➢ Vancomycin
Empiric therapy for HOSPITAL ACQUIRED acute bacterial meningitis (regardless of age)
Hospital acquired meningitis/ First Line Second line
ventriculitis, or for a patient ➢ Vancomycin, 1g, IV, BID Plus ➢ Vancomycin Plus
with post- neurosurgery ➢ Ceftazidime, 2g IV, TID or QID or ➢ Meropenem, 2g IV,
ventriculostomy/lumbar catheter, ➢ Cefepime, 2 g IV, BID or TID TID
ventriculoperitoneal (atrial)
shunt or penetrating trauma Meropenem can be
without basillar skul fracture. Duration; for up to 21 days or individualized used in place of
The likely pathogens are MDR cefepime or ceftazidime
gram negative pathogens like if indicated by
Acinetobacter, Pseudomonas, microbiologic data
Klebsiella and MRSA
*Penicillin allergy:

➢ Fluroquinolones for sever allergy (e.g anaphylaxis) in place of 3rd generation cephalosporins.
Cephalosporin or carbapenems can be retained for mild cases (e.g. no hives or anaphylaxis etc).
➢ WHO recommends chloramphenicol as an alternative for penicillin allergy in meningitis endemic
countries. However, recent data demonstrated increased mortality with CAF
o CAF, 500mg I.V. QID
➢ For listeria, cotrimoxazole should be used in place of ampicillin.
o Cotrimoxazole, 20mg/kg/day, BID to QID

➢ Vancomycin should be added to either third generation cephalosporins or ampicillin if S.pneumoniae


resistance in the locality is high, patient had prolonged or multiple antibiotics exposures within the past
three months or for a patient with suspected coagulase negative staphylococcus infection or for any
patient with high suspicion of MRSA
➢ Acyclovir 10mg/kg,IV (infuse over 1h) TID for 14-21d
o This is added in a situation where HSV-1 encephalitis is likely. Early diagnosis and treatment are
imperative. Mortality is reduced from >70% to <20% with IV acyclovir treatment.

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Increased ICP
➢ Admit to ICU
➢ Elevation of the patient’s head to 30-450
➢ Intubation and hyperventilation (Paco2 25-30 mmHg)
➢ mannitol

Supportive Therapy
➢ Hydration: both under and over hydration may have unfavorable
consequences.
➢ IV maintenance fluid IS preferred over restricted fluid intake in the first 48
hours in settings with high mortality and lately presenting patients.
➢ Nutrition support if required (NG tube feeding, if necessary)
➢ Analgesia and/or antipyretic:
o Tepid sponging
o Paracetamol oral, 1 g 4–6 hourly when required, maximum daily dose of:
4 g in 24 hours. Alternative: Ibuprofen, Diclofenac

Prevention
➢ Prophylaxis of contacts: Close household contacts for H. influenza and N.
meningitides. eg. Ciprofloxacin, oral, 500 mg as a single dose.
➢ Avoiding sharing utensils or close contacts with people with upper respiratory
tract infections.
➢ Prompt treatment of primary infection (e.g. upper respiratory tract infections)
➢ Using tissue or sleeve to cover sneezes and coughs and avoid kissing during
infection.
➢ Avoiding overcrowding
➢ Proper hand washing and other peculiar precautions.
➢ Immunization as per national schedules (Ethiopia introduced H. influenza B
vaccine (Hib) since 2007 and Pneumococcal Conjugate Vaccine (PCV) since
2013)
➢ Mass immunization if N. Meningitis epidemic (Men A vaccine is available in
Ethiopia)

Special population considerations


Pregnant:
➢ Same principles as outlined in this topic can be used while aware of
hemodynamics alterations during pregnancy.
➢ Floroquinolones and tetracyclines (if used required) are not recommended in
pregnancy.
➢ Cotrimoxazole is not recommended in the third trimester of pregnancy to 6
weeks (age of infant) due to a risk of kernicterus in the infant.
➢ Caution should also be exercised in the use of aminoglycosides during
pregnancy as they are rarely linked with hearing loss of infants.
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Prognosis
➢ Mortality rate is
o 3 - 7% for meningitis caused by H. influenzae, N. meningitidis, or group
B streptococci
o 15% for that due to L. monocytogenes; and
o 20% for S. pneumoniae.
➢ Poor prognostic factors
o Decreased level of consciousness on admission
o Onset of seizures within 24 h of admission
o Signs of increased ICP
o Young age (infancy) and age >50
o The presence of co-morbid conditions including shock and/or the need for
mechanical ventilation, and Delay in the initiation of treatment.

Cryptococcal meningitis
Refer from chapter 5; RVI (click here → Cryptococcal meningitis)

TB Meningitis
Refer from Chapter 3; TB (click here →

Tuberculous meningitis)

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Chapter 9; CLD/ Chronic liver disease/ (የጉበት በሽታ)

Chapter 9; CLD/ Chronic liver


disease/ (የጉበት በሽታ)
Dr. Mulualem. G

Clinical features and how to write hx of CLD patient


History

☛ N.B. All the manifestations (history and P/E) we discussed here range
from acute hepatitis to end stage cirrhosis. So, you have to correlate
with your patient condition

➢ Pt’s may present with


Abdominal distension
LOC in hepatic encephalopathy
➢ Abdominal distension
From which quadrant does the swelling starts? (left or right, upper or
lower)
Gradual in onset
Painless
Persistent → increase in size and progress to involve the whole
abdomen and lower extremities with in “X” months.
Together with dragging sensation and fullness in the left upper
abdomen

What is the difference between abdominal swelling and abdominal distension?

➢ Abdominal distension occurs when gas (air) or fluid accumulates in the


abdomen causing its outward expansion beyond the normal girth of the
stomach. Underlying causes include ascites, Intestinal obstruction etc.
➢ The term Abdominal swelling is used when there is intraabdominal organ
enlargement causing increased abdominal girth (e.g. hepatosplenomegaly) or
mass arising from the abdomen
➢ Even though it’s not correct, some authors use both terms interchangeably

➢ RUQ abdominal pain


Stabbing
Constant
Mild to moderate in severity
Radiates to the back
➢ Pruritis (itching sensation)
because of bile salt products deposited in the skin
Happen before jaundice 528
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Cmn in cholestasis and it is the earliest smx of primary biliary


cirrhosis
➢ Jaundice (yellowish discoloration)
Eye (sclera), skin
Progressively deepen
Ask who noticed the discoloration
➢ Dark (coca or tea colored) urine → due to bilirubinuria
➢ Stool colour change
Pale/tarry/clay coloured stool → due to urobilinogens or urobilins
excretion in stool. (for more click here → Jaundice and hyper
bilirubinemia)
Foul smelling
Scanty in amount
Melena or haematochezia
➢ Loss of libido, impotence, amenorrhea
➢ Hepatic encephalopathy features
Confusion
Sleep disturbance
Restlessness and aggressiveness
Difficult to concentrate
Forgetfulness
Abnormal body movement
LOC
✓ While resting on bed or doing his/her daily activity
✓ When does s/he gain consciousness?
✓ Is there fall down injury or not?
➢ Other nonspecific smx’s
Weight loss,
Nausea
Anorexia
Easy fatigability
Fever → high grade, intermittent, associated with chills, rigor and
profuse sweating

N.B

➢ Dark urine + jaundice is specific for liver


disease
➢ smx’s, signs and laboratory abnormalities
should persist for ≥ 6months to consider
CLD

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Clinical features based on type and duration of liver disease

Acute infection (Acute hepatitis)


➢ Largely asymptomatic
➢ Some patients may have: jaundice, nausea, vomiting, fatigue, RUQ abdominal
pain.
➢ Rarely patients may progress to acute liver failure: encephalopathy, ascites,
bleeding diathesis

Chronic infection (Chronic hepatitis)


➢ Largely asymptomatic
➢ Some patients may have non-specific symptoms which can be intermittent or
persistent: fatigue/lack of energy, poor appetite

Decompensated Liver Cirrhosis


➢ Nonspecific symptoms: fatigue, weight loss, poor appetite
➢ Jaundice
➢ Ascites
➢ Variceal bleeding
➢ Encephalopathy (mild to severe)
➢ Bleeding

HCC (Hepatocellular Carcinoma)


➢ Weight loss
➢ Hard irregular liver mass on physical examination

Risk factors

➢ Chronic alcohol intake and smoking


Quantity and duration of alcohol intake are the most important risk factors
involved in the development of alcoholic liver disease.
Gender is a strong determinant for alcoholic liver disease.
Women are more susceptible to alcoholic liver injury when compared to
men. They develop advanced liver disease with substantially less alcohol
intake
The current recommendation is not to take alcohol, No alcohol is safe
according to WHO19.
Significant alcohol intake (based on beer bottle)
✓ 1 bottle of beer contain 11-15 g of alcohol

19
Previously, a maximum 1 drink for women and 2 drinks for men per day were recommended.
One drink is roughly equivalent to a bottle of beer, a glass of wine, or a unit of spirit. 530
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Both of them should have taken these


✓ women ≥ 2 bottle (22-30g) per day
amount of alcohol for ≥ 10 years to
✓ men ≥ 3 bottle (33-45g) per day
consider significant alcohol intake.

▪ In men, 40 - 80 g/d of ethanol produces fatty liver;


160 g/d for 10 - 20 years causes hepatitis or cirrhosis
(25-fold increased risk). Only 15% of alcoholics develop
alcoholic liver disease.
▪ Women exhibit increased susceptibility to alcoholic liver
disease at amounts >20 g/d
▪ Gender-dependent differences result from Poorly
understood effects of estrogen and the metabolism of
alcohol [by alcohol dehydrogenase].
▪ Some ethanol is broken down in the stomach by
gastric alcohol dehydrogenase, which lowers the
amount available for absorption by producing
acetaldehyde.
▪ This enzyme is present at higher levels in men than in
women, which may account for the fact that women
usually develop a higher blood ethanol level than men
after consuming the same dose per kilogram of body
weight.
▪ The volume of distribution of ethanol is also gender
dependent due to difference in body fat percentages:
0.6 L/kg in men and 0.7 L/kg in women.
In rough estimation One beer, 4 ounces of wine, or one ounce of 80%
spirits all contain 12 g of alcohol.
How can we estimate the gram of alcohol from 1 bottle of Beer?
✓ If 1 bottle of beer = 330ml = have 5% alcohol
5
5% of 330ml = 100
𝑥 330𝑚𝑙 = 16.5 𝑚𝑙
1u = 1ml = 0.8 g
16.5ml = ?
16.5 x 0.8 g = 13.2 g
So, 330ml of 5% alcohol beer contain approximately 13g
alcohol
Approximate equivalent concentration of local alcoholic drinks with western
drinks listed as follows
✓ Tella with beer
✓ Tejj (estimated 11 - 17 % alcohol) with wine
✓ Areki (estimated 40 - 70 % alcohol) with spirits
The roles of beverage type(s), i.e. wine, beer, or spirits, and pattern of
drinking (daily versus binge drinking) are less clear.
CAGE criteria to screen alcohol dependence/abuse
✓ C → cutting down (assuming to decrease alcohol intake)
✓ A → annoyance when criticized
✓ G → guilty feeling
✓ E → Eye openers (take alcohol in the morning motivation)
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▪ From these one +ve answer suggest alcohol use


problem
▪ ≥ 2 affirmative answer to CAGE suggest alcohol abuse
or dependence
✓ Also ask the following to asses alcohol dependence
▪ Black outs (loss of memory during drinking)
▪ Job loss
▪ Marital conflict up to family loss
▪ Legal problems
▪ Drinking while driving or operating machinery
▪ seizure
➢ Obesity (high level of fat in the body)
➢ MSP, blood transfusion, tattoos, IV drug abuse, contact with jaundiced patient
→ risk of hepatitis virus infection
➢ Herbal medication use → herbal medicines are hepatotoxic
➢ Occupation → health care professionals
➢ Drugs
▪ Carbamazepine → cholestatic jaundice
▪ NSAID’s (e.g. paracetamol) → hepatotoxic
▪ Ant TB drugs especially pyrazinamide followed by INH are
hepatotoxic
▪ Methyldopa, ketoconazole → drug induced hepatitis
➢ Diet
▪ Aflatoxin is RF for HCC
▪ Iron → hemochromatosis
▪ Previously Increased protein in diet was considered as a precipitant
for HE. But currently understood that, CLD patients are at risk of
malnutrition, so don’t restrict high protein diet)
➢ Aetiologies
Family hx (genetics and inherited)
✓ Hemochromatosis
✓ Wilson’s disease
✓ AAT (alfa 1 antitrypsin) deficiency
✓ NAFLD (non-alcoholic fatty liver disease) /NASH (Nonalcoholic
steatohepatitis)
✓ Primary biliary cirrhosis
✓ PSC (primary sclerosing cholangitis)
✓ Cystic fibrosis
Acquired
✓ Viral infections (HBV, HCV, CMV, EBV)
✓ Alcoholic liver disease
✓ Autoimmune hepatitis

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Liver cirrhosis and Complication of CLD

If the Clinical complications of cirrhosis become evident, the patient have


Decompensated CLD

➢ Portal HTN related CXN


Ascites, Splenomegaly, hypersplenism
SBP
Gastroesophageal varices
Hemorrhoids (rectal varices)
Portal hypertensive gastropathy
➢ Hepatic insufficiency related CXN
Hepatic encephalopathy (HE)
Hepatopulmonary sxx (HPS)
Hepatorenal sxx (HRS) → Type I & Type II
Synthetic dysfunction
✓ Hypoalbuminemia
✓ Coagulopathy → Factor deficiency, fibrinolysis,
thrombocytopenia
Malnutrition
Hematologic abnormalities → Anemia, Hemolysis, Thrombocytopenia,
Neutropenia
Bone disease → Osteopenia, Osteoporosis, Osteomalacia
➢ HCC (Hepatocellular carcinoma)

 For more see the section below on Liver Cirrhosis and Complications of CLD
with their Treatment

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Sample history

Sample history of a patient from tach armachiho with the DX of Decompensated CLD
(evidenced by ascites + Splenomegaly 2ry to portal HTN) secondary to Alcoholic Liver
disease r/o Chronic viral hepatitis

Chief compliant
abdominal distension of 3 months duration

HPI

This patient was last relatively healthy 03 months back, at which time he noticed
Abdominal distension which initially started from RLQ, which gradually increase in size
and progress to involve the whole abdomen and lower extremities within one month
duration. Together with dragging sensation in the left upper abdomen, sense of fullness
and early satiety.

Four months before the onset of abdominal distension, he experienced a stabbing RUQ
abdominal pain which is moderate in severity and radiates to the back associated with
low grade intermittent fever, coca colored urine and his families accidentally noticed
yellowish discoloration of his eyes but no stool color change or itching sensation. He has
also unquantified but significant weight loss to the extent his trousers become loose, loss
of appetite and easy fatigability.

For these, he visited a traditional healer where he was given unspecified herbal
medication and cauterized at his arms, forearms, over the abdomen and back but he
didn’t get any relief. Finally, he came to our hospital for better investigation and
management.
He drinks traditional areki half bottle 2 - 3 times per week for 5 years
and then changed his drink to a beer of 10 to 15 bottles every
Tuesday, Saturday and Sunday (average 37 bottles per week) for the
past 8 years that means he drinks for a total of 13 years. which is
estimated to be 70g alcohol intake daily for 13 years. (RF, hint for estimation; 37
bottles divided by 7 days = 5.3 bottles daily, estimated alcohol content of one bottle is 13.2 g → look at RF
section above, 5.3 x 13.2 g = 69.77 g ≈ 70g)
No hx of blood transfusion, tattooing, contact with a jaundiced patient,
IV drug abuse or MSP, (RF for hepatitis virus transmission)
No hx of drug intake other than mentioned above (mentioned above under RF of
CLD)
No family hx of similar illness (genetics → etiology)

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He usually eats injera made of ‘‘teff’’ and ‘‘machilla’’ and ‘’wott’’ made of
‘‘atter’’ and ‘‘dagusa’’ 3-4 times per day. Occasionally he eats meat
during holidays (aflatoxin is RF for HCC, hemochromatosis)
No hx of reddish discoloration of urine, pain during urination, urgency,
frequency or flank pain (HRS → CXN)
No hx of nasal bleeding, bloody vomiting or melena (bleeding tendency from
coagulopathy, variceal bleeding/painless, coffee ground appearance,nonprojectile/ → CXN)
No hx of tinnitus, blurring of vision, light headedness or easy fatigability
(anaemia 2ry to blood loss especially in variceal bleeding which may lead to shock, vitamin B12 deficiency
or IDA → CXN)
No hx of sleep disturbance, confusion, Forgetfulness, Abnormal body
movement or LOC (HE → CXN)
Has hx of river water contact but no hx of post river water contact
itching (HSS → DDX)
No hx of dyspnea, orthopnea, PND or palpitation (CHF → DDX)
No hx of chronic cough, contact with chronic cougher or previous TB
treatment
No self/family hx of DM, HTN or asthma (DM cause Fatty liver disease, NAFLD in HTN
and metabolic sxx)
He was screened for RVI 2 months back and found to be NR.

Finally, He was admitted to our hospital supported physically by his families

Physical examination (pertinent findings)

1 GA

Chronically sick looking


Fetor hepaticus → Musty odor in breath as a result of increased dimethyl
sulfide.

2 Vital signs

Tachypnea (kusmauls breathing) → HE


Febrile → hepatitis
Orthodeoxia
BMI may be misinterpreted due to edema. But, if BMI is very low even in
ascites, it indicates significant weight loss

3 HEENT

Icteric sclera (jaundice)


Pale conjunctiva (anaemia) 2ry to
✓ Variceal bleeding
✓ Hypersplenism
▪ Splenomegaly + pancytopenia + normal cellular BM
(compensatory proliferative response in BM)
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▪ Cell count corrected in post splenectomy


✓ Nutritional deficiency → IDA, Vitamin B12 deficiency
✓ Direct alcohol toxicity to BM
Epistaxis
Xanthelasma in eye and hand crease
Kayser fleischer ring on cornea during slit lamp examination → Wilson’s
disease

LGS
Gynecomastia in males
o This is caused by increased estradiol due to decreased estrogen
metabolism in liver
o can occur in up to 66% of patients.
o Rarely from side effect of spironolactone treatment for ascites
Parotid enlargement
o likely due to alcohol use and not cirrhosis per se.
o ?2ry to collagen deposition
Testicular atrophy → due to hyper estroginism (estradiol)

5 RS

kusmauls breathing → acidosis 2ry to HE


cyanosis
clubbing
pleural effusion → right sided and transudative effusion due to local
extension from ascites through diaphragmatic pores

6 CVS

cording of arteries because of fat malabsorption → fat streak


RSHF as a cause of cardiac cirrhosis or LSHF result in → pulmonary HTN
→ RSHF → cardiac cirrhosis

7 Abdominal examination

HSM (hepatosplenomegaly) → liver size Can be enlarged, normal, or


shrunken
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▪ later liver may not be palpable due to end stage cirrhosis


▪ splenomegaly is 2ry to portal HTN
Ascites
▪ symmetrically distended abdomen
▪ flanks are full
▪ eversion of umbilicus with transverse or circular slit
▪ fluid thrill and shifting dullness
▪ superficially distended and tortuous abdominal vessels
✓ drain away from umbilicus during palpation which indicate
portal HTN (William Harvey method)

▪ straie alba/atrophica
N.B
✓ Straie gravidarum→ in pregnancy
✓ Purple straie → cushing sxx
caput medusae
o Latin word for head of medusa. In cirrhosis, distended and engorged
superficial epigastric veins which are seen radiating from umbilicus
across the abdomen and apparently similar to medusa head
o In portal hypertension, the umbilical vein may open.
o Blood from the portal venous system may be shunted through the
periumbilical veins into the umbilical vein and ultimately to the
abdominal wall veins, manifesting as caput medusa.

Picture; caput medusae (head of medusa) from Greek mythology, which had
venomous snakes in place of hair
bruit over the liver 2ry to HCC
tenderness and rebound tenderness → SBP
hemorrhoid in DRE

8 GUS

Loss of male type hair distribution (i.e. pubic hair loss) 537
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Testicular atrophy → due to hyper estroginism (estradiol)


Amenorrhea or menorrhagia in females

9 MSS

Bilateral pitting leg oedema


Dupytren’s contracture
▪ Thickening and shortening of palmar fascia that leads to flexion
deformities of the fingers.
▪ Thought to be caused by fibroblastic proliferation and disorderly
collagen deposition.
▪ It is relatively common (33% of patients).
▪ Cmn in alcoholics

Thenar and hypothenar muscle atrophy

10 IS

Spider angioma or spider nevi


▪ Telangiectasia which consist of central arteriole with radiating small
vessels because of an increase in estradiol.
▪ Occur in about 1/3 of cases
▪ Found in the distribution of SVC (i.e. above the nipple line)
▪ May be found in Rheumatoid arthritis, thyrotoxicosis, pregnancy

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Palmar erythema → Exaggerations of normal speckled mottling of the palm,


because of altered sex hormone metabolism.

Figure; Palmar erythema. This figure shows palmar erythema in a patient with
alcoholic cirrhosis. The erythema is peripheral over the palm with central pallor.

Leukonychia (from Greek word leuko → white, nychia → nail) and terry
nails

Palmar pallor
Skin pigmentation → in hemochromatosis
Bruising / purpura
Axillary and pubic hair loss
Scratch marks due to pruritis

11 NS → usually HE features

Asterixis
o Bilateral asynchronous flapping of outstretched, dorsiflexed hands
seen in patients with HE.
o Asterixis can be elicited by having patients extend their arms and
bend their wrists back. 539
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o In this maneuver, patients who are encephalopathic have a ‘’liver


flap’’ — i.e., a sudden forward movement of the wrist.
o This requires patients to be able to cooperate with the examiner and
obviously cannot be elicited in patients who are severely
encephalopathic or in hepatic coma.
Construction apraxia
Coma
hyperreflexia

N.B

❖ physical examination findings related to hyper estroginism in males (especially


in alcohol users) include
Gynecomastia
Testicular atrophy
Loss of male pattern hair distribution
❖ Peripheral Stigmata of liver disease
▪ HANDS:
✓ Palmar Erythema
✓ Clubbing
✓ Dupytrens
✓ Leuconychia
✓ Flapping tremor
▪ HEENT/UPPER BODY
✓ Jaundice
✓ Spider Angiomata
✓ Gynaecomastia and scant body hair
✓ Scratch marks
▪ ABDOMEN
✓ Ascites
✓ Hepatosplenomegally
✓ Caput Medusa
✓ Hemorrhoids on PR
✓ Small testes

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DDX

DDX for patients presenting with abdominal distension (ascites)

CLD 2ry to
▪ Viral hepatitis
▪ Alcoholic liver disease
▪ Autoimmune hepatitis
▪ HSS
✓ hepatocellular function remains normal and cirrhosis is rare
✓ Chronic schistosomiasis after 5-10 years
✓ Post river water contact itching may be forgotten so, endemicity is
important than asking post river water contact itching (e.g. living around
lake tana)
✓ Phases of schistosomiasis
o Dermatitis/swimmer’s itch
▪ popular pruritic rash at skin penetration site in 24-48hrs
o Katayama fever
▪ serum sickness like illness
▪ associated with excess antigenemia and formation of
soluble immune complexes
o Chronic schistosomiasis
✓ Granulomatous reaction around the ova results in organomegaly,
obstruction and fibrosis
✓ Fibrosis of the portal veins known as periportal fibrosis or Symmers'
clay pipe–stem which result in portal HTN (which in turn result in
ascites, varices & splenomegaly)
✓ Similar pathologic changes occur in other organs also
o bladder → obstructive uropathy, urosepsis, risk of bladder cancer
(SCC). S.hematobium is the etiologic agent
o Lung → pulmonary HTN and corpulmonale
o Brain and spinal cord → transverse myelitis
o GIT – bloody diarrhea and abdominal pain
o For more click here and refer ‘’ 9.2. Intestinal Helminthic
Infestations (የአንጀት ጥገኛ ተውሳክ ፣የአንጀት ትላትል) and blood
flukes section from Short case of Nitsibin → 9.2.4.
Schistosomiasis (ቢሊሃርዚያ)
▪ Drug associated chronic hepatitis
o Direct toxic effect (Dose dependent) → Acetaminophen, Carbon
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o Idiosyncratic → isoniazid, valproate, phenytoin, Ciprofloxacin,


Augmentin
o Other → Estrogenic/androgenic steroids, pyrazinamide,
methotrexate
▪ HCC → usually a complication of cirrhosis
▪ Genetics
✓ Hereditary Hemochromatosis
✓ Wilson disease
✓ AAT (α1 antitrypsin) deficiency
✓ cystic fibrosis
▪ Cardiac cirrhosis
▪ Metabolic disorders
o NAFLD (non-alcoholic fatty liver disease)
o NASH (non-alcoholic steatohepatitis)
▪ Infiltrative disorders
o Lipid storage diseases (Gaucher's and Niemann-Pick disease)
o Amyloidosis
o sarcoidosis
▪ Budd chiarri SXX
✓ Hepatic vein outflow obstruction by thrombus
✓ Triads include
i. Abdominal pain
ii. Ascites
iii. hepatomegaly
✓ Other manifestations
▪ Jaundice
▪ Splenomegaly
▪ encephalopathy
▪ Cryptogenic chronic hepatitis
▪ Idiopathic

TB peritonitis
✓ disseminated TB to liver and peritoneum
✓ present with very huge ascites
✓ cmn in our setup
lymphoma
✓ peritoneal carcinomatosis causing ascites with liver involvement
RSHF
Constrictive pericarditis
Nephrotic sxx
Chronic pancreatitis
Meig’s sxx → ovarian ca + pleural and peritoneal effusion
IVC sxx
Hypothyroidism → rare
PLE (protein losing enteropathy) → very rare condition

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N.B

6F’S in abdominal distension

Fluid → ascites
Feces → failure to pass feces but no flatus indicates
incomplete intestinal obstruction
Flatus → failure to pass both feces and flatus indicates
complete intestinal obstruction
Fat → obesity
Fetus → pregnancy
Fatal growth → organomegaly, malignancy, AAA (abdominal
aorta anourysm)

DDX for HE presenting with LOC

HE
Cerebral malaria
Acute alcohol toxicity
SDH
Meningoencephalitis
DKA
Metabolic encephalopathy
Sedation overdose

DDX for oesophageal varices presenting with upper GI bleeding


Oesophageal varices
PUD
Mallory Weiss tear
Erosive esophagitis
Gastric ca
Gastro duodenal erosions
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For more refer under short case of nitsibin (click here → 9.4.1. Upper GI
bleeding)

N.B
Portosystemic anastomotic area include
Haemorrhoidal plexus
Gastro oesophageal junction
Retroperitoneal area
Peri umbilical area

DDX for hepatomegaly with cirrhosis

Alcoholic liver disease


Infiltrative conditions
✓ Hemochromatosis
✓ Wilson disease
✓ sarcoidosis
HCC coming after cirrhosis
Cirrhosis in early stage

Ass’t example
Decompensated CLD (evidenced by ascites + SBP + Splenomegaly 2ry to
portal HTN) secondary to Alcoholic Liver disease r/o Chronic viral hepatitis

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IX

1. LFT and liver enzymes → for normal values refer short case of nitsibin (click here
→ Chapter 27; Reference Intervals for Laboratory Tests)
LFT
✓ Serum bilirubin level → indicates metabolic activity
✓ Albumin and total protein → indicates synthetic function
✓ PT, aPTT and INR → prolongs earlier than hypoalbuminemia,
also indicates synthetic function

N.B
☛ albumin completely synthesized by liver. But globulin
synthesized also by lymphoid tissue. So, in CLD there will be
low albumin/due to impaired synthetic function of the liver / with
high globulin.
☛ Unconjugated (indirect) hyperbilirubinemia is present when the
direct fraction is <15% of the total serum bilirubin.

𝒅𝒊𝒓𝒆𝒄𝒕 𝒃𝒊𝒍𝒊𝒓𝒖𝒃𝒊𝒏
𝒊. 𝒆 𝒓𝒂𝒕𝒊𝒐 = 𝒙 𝟏𝟎𝟎 %
𝑻𝒐𝒕𝒂𝒍 𝒃𝒊𝒍𝒊𝒓𝒖𝒃𝒊𝒏
𝑹𝒂𝒕𝒊𝒐 > 𝟏𝟓% 𝒊𝒎𝒑𝒍𝒊𝒆𝒔 𝒅𝒊𝒓𝒆𝒄𝒕 𝒉𝒚𝒑𝒆𝒓𝒃𝒊𝒍𝒊𝒓𝒊𝒃𝒊𝒏𝒆𝒎𝒊𝒂
𝑹𝒂𝒕𝒊𝒐 < 𝟏𝟓% 𝒊𝒎𝒑𝒍𝒊𝒆𝒔 𝒊𝒏𝒅𝒊𝒓𝒆𝒄𝒕 𝒉𝒚𝒑𝒆𝒓𝒃𝒊𝒍𝒊𝒓𝒊𝒃𝒊𝒏𝒆𝒎𝒊𝒂

Liver enzymes → determines the extent of liver damage


✓ ALT (SGPT) → specific to liver
o Elevates in hepatocellular disorders than extra hepatic
or Intrahepatic obstructive disorders
o Stays longer and higher than AST
✓ AST (SGOT)
▪ nonspecific which may occur in myolysis
▪ Viral hepatitis - may reach 10 to 100 times ULN
(Upper normal limit)
▪ Cirrhosis - 4 times ULN
▪ AST: ALT ratio = 2:1 (ratio >1) is typical for alcoholic
liver disease, for others ALT > AST
▪ In alcoholic hepatitis and in contrast to other causes of
fatty liver, The AST and ALT are usually elevated 2 to
7-fold (rarely >400 IU).
✓ ALP
▪ Significantly elevated than other enzymes in obstructive
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Predominant in obstructive conditions than in


o
hepatocellular disorders - 3 to 10 times ULN
o Hepatocellular disorders - <3 times ULN.
▪ Also found in intestine, bone and placenta
▪ Simultaneous measurement with GGT confirm liver
disease
✓ GGT/GGTP
o Correlates with ALP levels
o Elevated in biliary obstruction (Obstructive jaundice)
o Typically, much higher in CLD from alcohol

N.B

In Hepatocellular pattern of jaundice ALT/AST elevated out of


proportion to ALP and the reverse is true in cholestatic pattern
of jaundice.

(AST → aspartate aminotransferase = SGOT → serum glutamate oxaloacetate


transaminase, ALT → alanine aminotransferase = SGPT → serum glutamate
pyruvate transaminase, ALP → alkaline phosphatase, GGT/GGTP → Gamma-
glutamyl transferase / γ-glutamyl transpeptidase/)

2. Viral markers
HBsAg
✓ First evidence of infection (before biochemical abnormality)
✓ Signifies Infection & implies infectivity
✓ Commonly done in our setup
HCV Antibody → commonly done in our setup
HBcAg → Induces cellular immune response
HBeAg → Marker for active viral replication / INFECTIVITY
HBxAg
Anti HBsAg
✓ Antibody which confers PROTECTIVITY
✓ signifies recovery from HBV infection, non-infectivity,
vaccination
Anti HBcAg
✓ Antibody detected in anyone with previous exposure
✓ Does NOT confer protectivity
✓ IgM → acute infection / lasts 3-6 months.
✓ IgG → implies chronic hepatitis infection
✓ present in “window period”
Anti HBeAg
✓ Antibody which indicates antigen is cleared / virus not
replicating
✓ Decrease infectivity
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HBV DNA (PCR) → Best indicator of viral replication, Usually


parallel’s HBeAg
HCV RNA (PCR)
3. Ascitic fluid analysis → refer short case of nitsibin (click here → Ascitic fluid
analysis)
4. CBC
Anaemia 2ry to
✓ Variceal bleeding
✓ Hypersplenism
▪ Splenomegaly + pancytopenia + normal cellular BM
(compensatory proliferative response in BM)
▪ Cell count corrected in post splenectomy
✓ Nutritional deficiency → IDA, Vitamin B12 deficiency
✓ Direct alcohol toxicity to BM
Leukocytosis in SBP
Thrombocytopenia or pancytopenia
Macrocytosis in the absence of anaemia → alcoholic liver disease or
from Vitamin B12 deficiency
5. PM (peripheral morphology)
Microcystic hypochromic anaemia → IDA
Macrocytosis /megaloblastic anaemia/ → Vitamin B12 deficiency
6. Co-infection: HIV and HCV screening
7. Serum electrolyte
Hypokalaemia which cause HE by
i. Resulting systemic alkalosis which prevent conversion of NH3
(toxic ammonia) to NH4 (non-toxic ammonia)
ii. Directly stimulate renal ammonia production
Hyponatremia → from diuretic effect, liver disease by itself (due to inability
to excrete free water resulting from high levels of ADH and aldosterone)
8. U/A → Bilirubinuria /can be detected in dipstick examination/, toxins, copper
and ceruloplasmin
9. Abdominal U/s
Show architecture of liver i.e. cirrhotic change in liver (where it may show a
small and nodular liver in advanced cirrhosis along with increased
echogenicity with irregular appearing areas),
Determine size of portal vein or portal vein dilatation and HVPG for Portal
HTN diagnosis.
o A normal Hepatic venous pressure gradient (HVPG) is
between 1 and 5 mmHg.
o Portal hypertension is present if the HVPG is ≥6 mmHg.
Portal hypertension typically becomes clinically significant when
the HVPG is ≥10 mmHg
o On the other hand, portal HTN can be diagnosed if portal
vein diameter is > 12mm, it strongly suggests portal HTN if
diameter is > 15mm.
To detect intra-abdominal mass (HCC, lymphoma) and LAP
Detecting fatty infiltration of the liver in NAFLD/NASH.
Screen for Budd-Chiari syndrome (by assessing flow in the hepatic vein)
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Can detect minimal ascites as little as 100ml of ascitic fluid (ascites can
be appreciated by physical examination /to detect flank dullness/ if the fluid
volume is ≥ 1500ml)
10. CXR, ECG, ECHO → if RSHF suspected only
11. Serum ferritin level, Transferrin saturation → if hereditary hemochromatosis
suspected. Both of these will be elevated in symptomatic patient
𝐒𝐞𝐫𝐮𝐦 𝐈𝐫𝐨𝐧
Transferrin saturation = 𝐓𝐈𝐁𝐂(𝐓𝐨𝐭𝐚𝐥 𝐢𝐫𝐨𝐧 𝐛𝐢𝐧𝐝𝐢𝐧𝐠 𝐜𝐚𝐩𝐚𝐜𝐢𝐭𝐲)
𝑋 100 %
ferritin is an acute-phase reactant and can be elevated in RA, lymphoma
or other cancers, in NASH (Nonalcoholic steato hepatitis) patient in the
absence of iron overload
If the ferritin is >1000 g/L, considered liver biopsy to look for iron
deposition
12. serum AAT and serum albumin level
13. Serum ceruloplasmin and copper level
Ceruloplasmin is transport protein of copper
Decreased ceruloplasmin and increased serum copper level expected in
Wilson disease
14. Serum autoantibodies (like ANA) → if autoimmune hepatitis is suspected
15. Abdominal CT and MRI → Screening for HCC if clinical suspected: If there is
liver mass (CT scan of the abdomen with or without alpha fetoprotein)
16. Upper GI endoscopy and proctoscopy
For oesophageal varices and haemorrhoid respectively
Usually used for mgt purpose rather than Ix especially upper GI endoscopy
for endoscopy guided ligation of variceal bleeding
17. EEG → for HE grading, usually not done in our setup
18. Serum alfa feto protein (AFP) level → for HCC
19. Liver biopsy
Important for alcoholic liver disease
The gold standard for diagnosis of cirrhosis is a liver biopsy, through a
percutaneous, trans jugular, laparoscopic, or fine-needle approach. But
biopsy is not necessary if the clinical, laboratory, and radiologic data
suggests cirrhosis.
Furthermore, there is a small but significant risk to liver biopsy, and
cirrhosis itself predisposes for complications due to liver biopsy.
Depending on the size of the nodules there are three macroscopic types of
cirrhosis:
o Micronodular cirrhosis (Laennec's cirrhosis or portal cirrhosis):
regenerating nodules are < 3 mm.
o Macronodular cirrhosis (post-necrotic cirrhosis): The nodules are > 3
mm
o Mixed cirrhosis: Consists in a variety of nodules with different sizes.

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N.B
Non-invasive screening for liver fibrosis: use one of the score available e.g. APRI
score
APRI Score
𝐀𝐒𝐓
[𝐔𝐍𝐋 𝐨𝐟 𝐀𝐋𝐓] 𝒙 𝟏𝟎𝟎
𝑨𝑷𝑹𝑰 𝒔𝒄𝒐𝒓𝒆 =
𝐩𝐥𝐚𝐭𝐞𝐥𝐞𝐭 𝐜𝐨𝐮𝐧𝐭 (𝟏𝟎𝟗/𝐋)
o APRI >0.5 but ≤ 1.5: Significant fibrosis or cirrhosis possible
o APRI >1.5 but ≤ 2: Likely significant fibrosis, cirrhosis possible
o APRI >2: Likely cirrhosis
Upper Normal limits (UNL) for normal ALT
o 30 U/L for men and 19 U/L for women
o Use the above cut point rather than the highly variable upper normal
limits of different laboratories.
Transient elastography (Fibro scan) if readily available

Evaluation of abnormal liver tests

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Discussion

Chronic liver disease (CLD)

CLD encompasses a wide spectrum of disorders including infectious,


metabolic, genetic, drug-induced, idiopathic, structural and
autoimmune diseases.
It includes
Chronic Hepatitis
Cirrhosis
Hepatocellular Carcinoma

9.1 Liver Cirrhosis and Complications of CLD with their


Treatment

Cirrhosis
Definition: irreversible, chronic parenchymal injury with fibrosis and nodular
degeneration causing distortion of vascular bed of liver & disorganization of
normal architecture.
Cirrhosis represents a late stage of progressive hepatic fibrosis with
distortion of the architecture of the liver with formation of regenerative
nodules.
It can result from any cause of chronic liver disease e.g. chronic viral
hepatitis, alcoholic liver disease.
Patients with cirrhosis develop a variety of complications which cause
marked morbidity and mortality.
o The common complications include ascites, SBP, variceal bleeding,
HE, HRS and HCC.
Causes of cirrhosis
o Alcoholism
o chronic viral hepatitis (Hep. B &C)
o Autoimmune hepatitis
o nonalcoholic steatohepatitis 550
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o biliary cirrhosis
▪ Primary biliary cirrhosis
▪ Primary sclerosing cholangitis
o cardiac cirrhosis
o Inherited metabolic liver disease
▪ Hemochromatosis
▪ Wilson’s disease
▪ AAT deficiency
▪ Cystic fibrosis
Factors which lead to cirrhosis include
o Viral factors → HBV
o Host factors
▪ Immunosuppression
▪ NAFLD
▪ Chronic alcohol intake
▪ Hepatotoxic drugs
▪ Concomitant infection → HBV + HCV, HBV+HDV
o External factors

Childs-Pugh classification
Don’t try to rehearse this, just know the name and the principle only.
It is a scoring system used to assess how risky surgery will be in pts with
liver disease
MELD scores and MAYO scores used to assess pts for liver transplant and
transplant allocation

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Generally, liver damage from cirrhosis cannot be reversed, but treatment


could stop or delay further progression and reduce complications.
A healthy diet is encouraged, as cirrhosis may be an energy-consuming
process.
o Weigh the risk and benefit of low protein diet (i.e. fear of
encephalopathy in high protein diet, but malnutrition risk of CLD by
itself requiring high protein diet).
Bed rest or hospitalization
o for poor oral intake (need for IV medication), significant vomiting.
o Patients with decompensated cirrhosis generally require admission to
hospital, with close monitoring of the fluid balance, mental status,
and emphasis on adequate nutrition and medical treatment.
Maintain ABC of life in patient presenting with severe and life-threatening
complications
Monitor weight and vital sign regularly
IV dextrose for patients with poor oral intake.
Avoid administration of saline as it would add to the already high total body
sodium content that typically occurs in cirrhosis.
Avoid constipation and other precipitants of HE. Laxatives, such as
lactulose, decrease risk of constipation.
Avoid alcohol, smoking and other identified risk factors
Identifying and treatment of Specific underlying cause of CLD
Preventing further liver damage
o Regardless of underlying cause of cirrhosis, alcohol and paracetamol,
as well as other potentially damaging substances, are discouraged.
o Vaccination of susceptible patients should be considered for Hepatitis
A and Hepatitis B.
Identifying and treatment of cxn
Close follow-up

9.1.1 Portal hypertension related cxn

9.1.1.1 Portal Hypertension

Portal hypertension is defined as the elevation of the hepatic venous


pressure gradient (HVPG) to >5 mmHg.
o HVPG is defined as the difference in pressure between portal vein
and inferior vena cava.
o HVPG is used as a measure of portal venous pressure. A normal
HVPG is between 1 and 5 mmHg.
Portal hypertension is present if the HVPG is ≥6 mmHg. Portal
hypertension typically becomes clinically significant when the HVPG is ≥10
mmHg, at which point varices may develop. Once the HVPG is ≥12 mmHg,
patients are at risk for variceal bleeding and the development of ascites.
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There are two simultaneously occurring processes in the pathogenesis of


Portal hypertension. These are;
o Increased intrahepatic resistance to the passage of blood flow
through the liver
o Increased splanchnic blood flow secondary to vasodilation
In industrialized countries, portal hypertension is typically the result of
cirrhosis, with noncirrhotic portal hypertension accounting for < 10 % of
cases. In other parts of the world, noncirrhotic portal hypertension due to
causes such as schistosomiasis and portal vein thrombosis are the leading
causes of portal hypertension
The causes of portal hypertension can be:
o Prehepatic
o Intrahepatic
o Post hepatic

Table; Classification of Portal Hypertension


Causes
I. Prehepatic ➢ Portal vein thrombosis
➢ Splenic vein thrombosis
➢ Massive splenomegaly (Banti’s syndrome)
II. Hepatic ➢ Presinusoidal
o Schistosomiasis
o Congenital hepatic fibrosis
➢ Sinusoidal
o Cirrhosis—many causes
o Alcoholic hepatitis
➢ Post sinusoidal
o Hepatic sinusoidal obstruction (veno-occlusive
syndrome)

III. Post hepatic ➢ Budd-Chiari syndrome


➢ Inferior vena caval webs
➢ Cardiac causes:
o Restrictive cardiomyopathy
o Constrictive pericarditis
o Severe CHF

9.1.1.2 Ascites

➢ Ascites is the accumulation of fluid within the peritoneal cavity.


➢ The most common cause of ascites is portal hypertension related to cirrhosis.
➢ However, malignant or infectious causes of ascites can be present as well, and
careful differentiation of these other causes are obviously important for patient
care. This can be differentiated by SAAG from Ascitic fluid analysis (refer short
case of nitsibin (click here → Ascitic fluid analysis))
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Management
➢ Salt restriction (< 2 g/day) (post at the bedside of the pt like this → ‘’salt free
diet/ ጨው ክልክል’’)
➢ See general management principles above

First line
➢ Spironolactone
o Starting dose 100 mg/day daily or BID
o If there is no response; increase doses every 3-7days (in 100 mg steps).
Maximum dose 400mg/day
o Serum potassium should be checked regularly: at start, at dose
increments and on each follow up visit

Add- on or alternative
➢ Furosemide
o Starting dose: 20mg, BID, Increments by 40mg/day. Maximum dose:
160 mg/day (80mg BID)
o Ass add-on: in patients who do not respond to spironolactone (body
weight reduction less than 2 kg in one week)
o As an alternative: in patients who have hyperkalemia or impaired kidney
function at baseline or develop later

N.B
Keep spironolactone to Lasix ratio of 5 : 2 to prevent hypokalemia since
spironolactone is potassium sparing diuretic
Spironolactone is preferred in ascites from CLD unlike other causes of
ascites because of the following reasons
o Loop diuretics are less effective in ascites from CLD because there
is low albumin for their mechanism of action
o RAAS is the cause of ascites in CLD
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o To prevent dehydration from lasix (since loop diuretics like Lasix are
strong diuretics which may cause dehydration. Hypokalemia and
dehydration are precipitant of hepatic encephalopathy)
loop diuretics like Lasix are strong diuretics and preferred in other causes
of ascites like CHF, Nephrotic syndrome, AKI/CKD….

➢ If ascites is still present despite the above measurements, it is defined as


refractory ascites.
➢ Alternative treatment modalities include:
o large-volume paracentesis (Therapeutic tap) for huge ascites; Look at
paracentesis and ascitic fluid analysis under short case of nitsibin (click here →
Peritoneal tap (paracentesis))
o TIPS (Trans jugular intrahepatic portosystemic shunt) procedure
o Liver transplant

9.1.1.3 Spontaneous bacterial peritonitis (SBP)

SBP is defined as a spontaneous ascitic fluid infection without an evident


intra-abdominal source.
It is common in patients who have low protein ascites (<1g/dL). i.e. Low
ascitic fluid albumin level and advanced CLD are risk factor for SBP. This
is because of albumin have opsonizing (protective) property.
Pathogenesis: the source of infection is mostly hematogenous. Bacterial
translocation from gut flora → mesenteric lymph nodes → bacteremia and
infection of the ascitic fluid.
It is a complication of Ascites in 8% of cases
Etiologies:
o E. coli → most common cause
o S. viridans
o S. aureus
o Enterococcus sp
o Klebsiella
Clinical manifestations:
o Fever
o abdominal pain and tenderness
o diarrhea
o rarely worsening of jaundice and HE (altered mental status)
Diagnosis:
o Positive ascitic fluid bacterial culture and
o ANC (Absolute neutrophil count) > 250 cells / μL

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Bacterial peritonitis
SBP Secondary peritonitis due to rupture of abdominal viscus
➢ WBC > ➢ WBC > 10,000/mm3 (significant leucocytosis)
500/mm3 ➢ Multiple organisms identified
(neutrophil ≥ ➢ Increased LDH level
50%) ➢ Glucose < 50
➢ Mono microbial ➢ Protein significantly decreased
➢ PH
➢ With obvious cause of 2ry peritonitis like intestinal
perforation
➢ Failure to improve after standard treatment with in 48
hr’s

Spontaneous bacterial peritonitis variants that do not require surgery

Variant Ascitic fluid culture Absolute PMN per mm3


Classic SBP (Ascites + Mono Positive ≥250
bacterial infection + ANC ≥250)
Culture-negative neutrocytic No growth
ascites
Monomicrobial non-neutrocytic Positive < 250
bacterascites (single organism)
Polymicrobial bacterascites Positive

Treatment of SBP
First line:
✓ Ceftriaxone, 1g, IV, BID for 7-10 days
Alternative:
✓ Ciprofloxacin, 200mg, IV, BID for 7-10 days

Prophylaxis for SBP


➢ Indications to start prophylaxis
o Patients who recover from an episode of SBP
o Advanced cirrhosis and ascitic fluid protein <1.5 g/dl without prior SBP
o In patients with GI bleeding and severe liver disease
First line:
✓ Norfloxacin, 400mg, P.O. daily
Alternatives
✓ Cotrimoxazole (TMP-SMZ), 960mg PO, daily
✓ Ciprofloxacin 500mg PO, daily
➢ Duration of prophylaxis: Generally indefinite but if there is long-lasting
improvement with disappearance of ascites, prophylaxis can be discontinued.
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9.1.1.4 Esophageal varices and Variceal bleeding

➢ Screening studies have shown that approximately one third of patients with
histologically confirmed cirrhosis have varices. Approximately 5 - 15% of
cirrhotic patients per year develop varices.
➢ Varices develop in order to decompress the hypertensive portal vein and return
blood to the systemic circulation
➢ Clinical feature
o Signs and symptoms of CLD
o Painless but massive hematemesis
o Hypotension with/without shock
➢ Investigation
o Emergency endoscopy
o blood type and cross match
o CBC, OFT, PT and PTT…

Approach to the management of variceal hemorrhage

There are four major issues related to the prevention and treatment of
variceal hemorrhage:
Prediction of patient at risk
Primary and pre-primary prophylaxis against variceal hemorrhage in patients
with cirrhosis
Treatment of an active bleeding
Prevention of rebleeding

1) Predictive Factors for risk of variceal hemorrhage in patients with cirrhosis

Location of varices
Size of varices
Appearance of varices
Clinical features of the patient
Variceal pressure

10) Prevention of variceal bleeding (Both Pre-primary and Primary, some expertise
uses the term primary and secondary)
➢ Primary prophylaxis aims to prevent variceal hemorrhage in patients with
esophageal varices who do not have a history of hemorrhage.
➢ Pre-primary prophylaxis refers to measures aimed at preventing the
development of varices.
➢ These measures are aimed at achieving one of the following results:
o Decreasing portal hypertension
✓ beta blockers → Propranolol, 20mg - 40mg, PO, BID or TID. Start low
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✓ surgical portal decompression


✓ TIPS (trans jugular intrahepatic portosystemic shunts) → functions like
side-to-side surgical portocaval shunt, but does not require general
anesthesia or major surgery for placement.
o Treating the varices directly
✓ Endoscopic variceal band ligation

11) Management of Active Bleeding


There are three primary goals of management during the active bleeding
episode:
i. Hemodynamic resuscitation
ii. Treatment of complications
iii. Treatment of bleeding
I. Hemodynamic resuscitation
➢ airway stabilization
➢ Blood loss should be replaced by packed cells and clotting factors should be
replaced as needed If platelet is < 50,000/mm3 in an actively bleeding patient
➢ Patients must be monitored carefully to avoid over transfusion with volume
overload because of the risk of rebound portal hypertension and induction of
rebleeding

II. Treatment of complications


The principal complications that cause death are
o Aspiration pneumonia
o Sepsis
o acute-on-chronic liver failure
o hepatic encephalopathy, and
o renal failure

III. Treatment of bleeding

Pharmacologic treatment

➢ Intravenous vasopressin and its analogs intravenous vasopressin directly


constricts mesenteric arterioles and decreases portal venous inflow, thereby
reducing portal pressure
➢ somatostatin and their analogs - Somatostatin inhibits the release of vasodilator
hormones such as glucagon, indirectly causing splanchnic vasoconstriction and
decreased portal inflow.

Endoscopic treatment

endoscopic therapy can be done at the time of diagnosis and it’s the
definitive treatment of choice for active variceal hemorrhage
There are two forms of endoscopic treatment
o Sclerotherapy involves injection of a sclerosant solution into the
varices through an injection needle
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o Variceal band ligation involves placing small elastic bands around


varices in the distal 5 cm of the esophagus
Balloon tamponade → is an effective way to achieve short-term hemostasis,
but due to complications and rebleeding upon balloon deflation, its use is
reserved for temporary stabilization of patients until more definitive treatment
can be instituted.

IV. Prevention of Rebleeding

➢ Band ligation
➢ Non selective beta blockers
➢ Beta blockers plus band ligation → Combination therapy with a beta blocker
plus endoscopic band ligation is more effective at preventing rebleeding than
band ligation alone or beta blockers alone.

N.B
➢ For active bleeding stop any anti HTN (Propranolol, Lasix, Spironolactone) b/c
of Risk of OHT.
➢ Keep NPO and Start IV antibiotics for any active UGI Bleeding and also If the
Bleeding within 01 week start IV Antibiotics.
➢ If Bleeding is before 01 week and no active bleeding currently, no need of
Antibiotics and Anti HTN can be re initiated
➢ An indication for Transfusion is when hemoglobin is ≤ 7 g/dl. This is because
Transfusion may increase bleeding due to transfusion related pressure effect.
➢ Each Bleeding in Esophageal bleeding will increase death rate by 30 %
➢ Definitive management is is EBL (Endoscopic band Ligation) after stablization

9.1.2 Hepatic insufficiency related CXN

9.1.2.1 Hepatic Encephalopathy (HE)


Hepatic Encephalopathy is an alteration in mental status and cognitive
function occurring in the presence of liver failure.
It is potentially reversible neuropsychiatric abnormality
Pathogenesis
o Gut derived neurotoxins → Porto systemic shunt of nitrogenous
chemicals (e.g. NH3) which are toxic to brain
o Hepatic insufficiency → liver failed to detoxify NH3 and other
neurotoxic chemicals
o False neurotransmitters and mercaptans
o Ammonia level is typically elevated in HE patients
Look at clinical features of HE from CLD hx section above
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Precipitating Factors

➢ Dehydration and Hypovolemia


➢ Electrolyte imbalance (e.g. hypokalemia)
➢ GI bleeding → increase ammonia production
➢ Infections (e.g. SBP)
➢ Hypoglycemia
➢ High protein diet → increased nitrogenous chemical n production by colonic
bacteria
➢ Constipation
➢ Hypoxia
➢ Sedatives

Clinical Assessment

Signs and symptoms suggesting of Precipitating factors


Clinical scale for assessment of hepatic encephalopathy
o Modified West Haven criteria (0—4)
o Sonic (unimpaired, covert, overt)

Clinical grading of HE (Modified West Haven criteria)

Clinical grade Signs Flapping tremor


Grade I ➢ Alert, slow mentation Infrequent
(Prodrome) ➢ Reversed sleep awake pattern → sleep in
the day and awake at night
➢ Euphoric, occasionally depression, poor
concentration, slow mentation and affect
Grade II Lethargy, drowsy, personality changes, Easily elicited
(Impending coma) disorientation
Grade III Stupor but easily arousable, incoherent speech, Usually present
(early coma) Marked confusion
Grade IV Coma, unresponsive but may response to Usually absent
(deep coma) painful stimulus

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Management of HE

Management principles
o supportive care
o Treatment of precipitating factors
o Treatment of concomitant cause of encephalopathy
o Specific treatment for HE

Supportive Care

➢ Patients that exhibit grade 3 or higher HE should be transferred to ICU


➢ Provision of nutrition for the unconscious
➢ Provision of oxygen
➢ Frequent positioning

Treatment of precipitating factors

➢ Correction of dehydration
➢ Correction of electrolyte imbalance
➢ Treatment of infection
➢ Control of GI bleeding
➢ Dietary protein management → In the past, restriction of dietary protein was
considered for patients with encephalopathy; however, the negative impact of
that maneuver on overall nutrition is thought to outweigh the benefit when
treating encephalopathy, and it is thus discouraged. There may be some
benefit to replacing animal-based protein with vegetable-based protein in some
patients with encephalopathy that is difficult to manage.

Treatment of concomitant cause of encephalopathy


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➢ Concomitant cause of encephalopathy and HE are diagnosed and treated at


the same time (e.g. Sepsis, hypoglycemia)

Provision of specific treatment for HE


➢ Lactulose
o A non-absorbable disaccharide which results in colonic acidification
o The usual dosage is 10 - 30mL PO (Via NG tube) TID.
o The goal of lactulose is to promote 2-3 soft stools per day and no
diarrhea
o Dose for Overt hepatic encephalopathy episodes, treatment:
✓ Route not specified: 16.7 g (25 mL) every 1 to 2 hours until at least 2
soft or loose bowel movements are produced daily; titrate to maintain 2
to 3 bowel movements daily.
o Dose for Subclinical (minimal) hepatic encephalopathy:
✓ 20 to 40 g (30 to 60 mL) daily in 2 to 3 divided doses to maintain 2
to 3 bowel movements daily for up to 3 months

PLUS
➢ Metronidazole, 250mg, PO, TID, for 5 to 10 days or
➢ Neomycin, 4 to 12 g daily divided every 4 to 6 hours for 5 to 6 days
o For Chronic hepatic insufficiency: 4 g PO daily for an indefinite period
or
➢ Rifaximin, 400 mg PO TID, for 5 to 10 days

PLUS
➢ Zinc supplementation

9.1.2.2 Hepatorenal Syndrome (HRS)

HRS usually represents the end stage of sequence of reduction in renal


function induced increasingly by severe hepatic injury.
It's is a firm of functional renal failure without renal pathology.
It occurs in 10% of patients with advanced liver disease and Acute Liver
Failure.
HRS is a diagnosis by exclusion w/c is characterized by:
o progressive rise in serum creatinine
o a benign urine sediment
o no or minimal proteinuria
o low rate of sodium excretion(<10meq/l)
o oliguria in a Patient who has established acute or chronic liver
disease

Types of HRS

Type 1 HRS
o more serious type 562
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o 2X increase serum creatinine to a level > 2.5 mg/dl within 2 wks


Type2 HRS
o decreased GFR with an increase in serum creatinine but is fairly
stable and with better outcome
o major feature is ascites that is resistant to diuretics

Precipitants

➢ Onset of HRS is typically gradual but it Can be precipitated by:


o bacterial infection E.g. SBP
o GI bleeding

Pathogenesis

arterial vasodilation in splanchnic circulation due to portal HTN → Nitric


oxide (No): most important vasodilator

Diagnosis: based on clinical criteria

➢ No specific test to establish diagnosis


o HRS Should be considered after exclusion of other potential cause
➢ The following diagnostic criteria is proposed for HRS
o Chronic or acute hepatic disease with advanced hepatic failure and portal
HTN
o Sr. Creatinine > 1.5 gm/dl progressing over days to wks
o absence of any apparent cause of AKI but the presence of another renal
diagnosis (e.g. diabetic nephropathy) does not necessarily exclude HRS

Treatment

Ideal therapy is improvement of liver function. However, when patient is not


responding in short term, medical therapy is recommended
o In ICU pts: norepinephrine + albumin
o In non-ICU pts: based on availability of drugs
In highly selected pts, who fail to respond to medication: Trans jugular
intrahepatic Porto systemic shunt (TIPS)
Patients who fail to respond, develops severely impaired renal function and
may need liver transplant or may recover if liver injury is reversible (dialysis
as a bridge is recommended)

Prevention

HRS regularly develops in pts with SBP or severe alcoholic hepatitis. The
following therapies may Prevent development of HRS
o IV albumin
o Norfloxacin
o pentoxifylline

Prognosis

➢ overall mortality of pts. with liver-failure is substantially worse if they develop


HRS
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9.1.2.3 Hepatopulmonary syndrome (HPS)

➢ HPS is considered when the following triad exists:


i. Liver disease
ii. Impaired oxygenation
• most sensitive measure being alveolar-arterial(A-a) O2 gradient >
15 mm Hg. Also, Pa02 < 80 mm Hg
• For pts > 65 year - A-a gradient > 20 mm Hg, Pa O2 < 70 mm
Hg
iii. Intrapulmonary vascular abnormality
• referred to as intrapulmonary Vascular dilatation (IPVD). IPVD can
be diagnosed by contrast echo, nuclear scanning or pulmonary
angiography
➢ The unique Pathological feature of HPS is gross dilatation of pulmonary
precapillary and capillary vessels
➢ It’s Mostly associated with portal HTN
➢ Prevalence: 4 - 47% (depend on diagnostic criteria)
➢ Other test: CXR, HRCT, PFT

Clinical manifestation of HPS


➢ Consequence of both hepatic & Pulmonary dysfunction
➢ More than 80% present with smx of liver disease. The remaining 20% present
with dyspnea as 1st manifestation but not specific to HPS (it can be due to
hepatic hydrothorax, Porto Pulmonary HTN, anemia, ascites…Etc.)
➢ Platypnea and orthodeoxia rather are more specific for HPS
o Platypnea (dyspnea in upright position) is an increase in dyspnea induced
by moving into an upright position and relieved by recumbency
o orthodeoxia is a decrease in arterial O2 tension (by > 4 mm Hg) or
desaturation (by > 5%) when pt moves from supine to up right.
o If they coexist together it is called platypnea-orthodeoxia SXX
➢ What is the mechanism of platypnea?

Liver unable to clear circulatory vasodilators (e.g NO)

Dilation of intrapulmonary vessels when patient is


upright

gravity dependent shunt of blood to basal area during


standing which lead to hypoxia

Treatment
➢ No effective medical therapy
➢ Rather supplemental O2 and liver transplantation have promising out come
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Prognosis
➢ Prognosis of Pt with HPS is worse than that of cirrhosis pt without HPS
(median survival is 24 months for pt with HPS and 5 yr Survival is only 23%
while pt without HPS have 5 yr survival of 63% & median Survival of
87months).
➢ But with liver transplantation survival is comparable.

9.1.2.4 Synthetic dysfunction

A. Hypoalbuminemia
B. Coagulopathy in liver disease

➢ Clotting process is a dynamic aggregation of multiple process, which can be


Viewed as occurring in 4 phases:
o initiation & formation of Platelet plug
o Propagation of clotting by coagulation cascade
o Termination of clotting by antithrombin
o Removal of clot
➢ Liver is responsible for production of almost all protein including coagulation
factors except factor8.
➢ In patient with liver disease there is rebalanced hemostasis. therefore, either an
increased risk of bleeding as well as thrombosis.
➢ Coagulation abnormality can be Hypocoagulability or Hypercoagulability.
➢ Hypocoagulability → increased bleeding risk
o decreased production of coagulation factors
o Abnormalities of platelet number and function
o Mechanism → decreased hepatic synthesis of thrombopoietin, bone
marrow suppression (e.g. HCV infection, alcohol use) or hypersplenism
o infection and endogenous heparinoids
o hyperfibrinolysis
➢ Hypercoagulability → increased thrombotic risk
o decreased production of natural anticoagulant (macro thrombi, micro
thrombi)

Tests of coagulation in liver disease


➢ PT, aPPT and INR
➢ Platelet level and function: bleeding time
➢ Fibrinogen and individual factor levels
➢ Fibrin degradation product and D-dimer
➢ Thrombin generation testing
➢ Thromboelastography and thromboelastometry
➢ Sonorheometry
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Treatment of bleeding
➢ Proper treatment requires answers to the following questions
o Any comorbidity presents?
o Is vit k deficiency present (more likely in primary cholestatic diseases)?
o Is DIC present?
o Is platelet count adequate?
o What is the status of fibrinogen and is fibrinolysis present?
o Is there danger of volume overload?
o Is there oral mucosal bleeding w/c can be corrected by antifibrinolytics?

Prevention and treatment of thrombosis

➢ Venous thromboembolism prophylaxis in hospitalized patients


➢ Antiplatelet and anticoagulant therapy

9.2 Causes of CLD

➢ There are various disorders that cause CLD (look at DDX above)
➢ We will discuss some of the causes here (viral hepatitis, alcoholic liver
disease, autoimmune hepatitis, Wilson disease, hemochromatosis, AAT
deficiency, NAFLD and NASH)

9.2.1 Viral Hepatitis (ሄፓታይቲስ ቫይረስ እና የጉበት ብግነት)

➢ Viral hepatitis is a systemic infection affecting the liver predominantly.


➢ Almost all cases of viral hepatitis are caused by one of five viral agents: HAV,
HBV, HCV, the HBV-associated delta agent or HDV, and HEV.
➢ All these human hepatitis viruses are RNA viruses, except for hepatitis B,
which is a DNA virus but replicates like a retrovirus.
➢ Although these agents can be distinguished by their molecular and antigenic
properties, all types of viral hepatitis produce clinically similar illnesses.
➢ These range from asymptomatic and inapparent to fulminant and fatal acute
infections common to all types, on the one hand, and from subclinical
persistent infections to rapidly progressive CLD with cirrhosis and even HCC,
common to the bloodborne types (HBV, HCV, and HDV), on the other.

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Table; hepatotropic viruses


Virus HAV HBV HCV HDV HEV
Group Enterovirus Hepadnavirus Flavivirus Delta particle (incomplete virus)
DNA/RNA RNA DNA RNA
Size 27 nm 40-42 nm 30-35 nm 35 nm 27 nm
Remarks called called serum previously defective RNA
infectious hepatitis called non - virus; needs
hepatitis A non - B, HBV to infect
now HCV
Faeco- Yes NO Yes
oral
Spread Blood Uncommon Yes
Saliva Yes -----
Sexual Uncommon Yes Uncommon Yes Uncommon
Vertical No Yes Uncommon Yes No
Chronic Incidence Not known 5-10% >50% -----
infection Severity Mild Often severe Moderate Unknown Mild to moderate

Active Vaccine Vaccine No ? Prevented No


by HBV
Prevention infection
Passive serum globulins No
Antigen HAV Ag HBSAg, HCV Ag HBSAg, HEV Ag
HBcAg, HDV
HBeAg
Antibody Anti- HAV Anti- HBSAg, Anti- HCV Anti- HBSAg, Anti- HEV
Anti- HBcAg, Anti- HDV
Anti- HBeAg
Prognosis Good Worst with Moderate Same as with Good
age

➢ Non hepatotropic viruses (viruses that indirectly affect the liver) include; EBV,
CMV, HSV, measles, Ebola, & others
➢ Viral hepatitis can be;
o Acute viral hepatitis or
o Chronic viral hepatitis

Acute viral hepatitis


➢ It is defined by the sudden onset of significant aminotransferase elevation as a
consequence of diffuse necro inflammatory liver injury. Symptoms may be
variable. This condition may resolve or progress to fulminant failure or chronic
hepatitis.

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Acute Liver Failure and Fulminant Hepatitis


➢ Acute liver failure (ALF) refers to the rapid development of severe acute liver
injury with impaired synthetic liver function and hepatic encephalopathy in a
person who previously had a normal liver or well-compensated liver disease.
➢ Fulminant hepatitis (FH) refers to the development of hepatic encephalopathy
within 8 weeks of the onset of symptoms in a patient with a previously healthy
liver or the appearance of encephalopathy within 2 weeks of developing
jaundice.
➢ Causes of ALF or FH are similar to that of acute hepatitis.
➢ Clinical features; Jaundice, Bleeding, Ascites and edema, Hepatic
encephalopathy, Decreased urine out put

Treatment

➢ Patients should be treated in an ICU setting.


➢ Secure air way, IV line, correct hypoglycemia and hypotension, insert NG tube
if unconscious
➢ If you are in primary hospital, Catheterize the urinary bladder and refer to a
referral hospital with ICU facilities.

Chronic hepatitis

➢ is defined as the presence of persistent (at least 6 months) necro inflammatory


injury that can lead to cirrhosis.
➢ Persistently abnormal serum transaminase levels and characteristic histologic
findings.
➢ We can classify chronic hepatitis based on its etiologic, histologic
activity(grade) and degree of progression/stage.
➢ Etiologic → Chronic viral hepatitis (most common cause of CLD) which include;
HBV, HBV and HDV coinfection, HCV
➢ Grade: histologic assessment of necro inflammatory activity.
o Mild
o Moderate
o Severe
➢ By stage: degree of fibrosis
o Stage 0 = no fibrosis
o Stage 1 = mild fibrosis
o Stage 2 = moderate fibrosis
o Stage 3 = severe fibrosis
o Stage 4 = cirrhosis

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Hepatitis B Virus infection


➢ Hepatitis B virus (HBV) is a double-stranded hepatotrophic DNA virus.
➢ HBV infection is a global health problem.
➢ The prevalence of HBV is highest in sub-Saharan Africa and East Asia.
➢ Though there is no a nationwide epidemiology study, several studies indicate
that Ethiopia has a high burden of HBV infection.
➢ HBV is transmitted by percutaneous or mucosal exposure to infected blood or
body fluids (saliva, menstrual, vaginal, and seminal fluids).
➢ Mother to child (perinatal) transmission is an important route of transmission.
➢ Transmission within a household, particularly to children is also an important
contributor.
➢ Sexual transmission may occur in those with multiple sex partners.
➢ The risk of developing chronic infection is 90% following perinatal infection (up
to 6 months of age) but decreases to 20 - 60% between the ages of 6
months and 5 years. Infection in adulthood leads to chronic hepatitis in < 5%
of cases
➢ HBV infection causes a number of clinical problems: acute hepatitis, chronic
hepatitis, liver cirrhosis, HCC, and extrahepatic features (e.g. glomerulonephritis,
vasculitis)
➢ Liver cirrhosis and HCC are the two major causes of death in patients with
chronic HBV infection
➢ Chronic HBV infection is a dynamic process due to viral replication and the
host immune response.
➢ viral replication status (HBeAg status), HBV DNA level (viral load), ALT values
and status of liver inflammation, HBV infection is divided into five phases. (see
the table 2 below)
➢ Having evidence of HBV infection does not necessarily indicate liver injury
(hepatitis) or the consequences of liver injury (liver cirrhosis and HCC).
➢ The presence of liver injury (hepatitis) is confirmed by a rise in transaminases
(mainly ALT) or imaging/clinical evidence of liver fibrosis and cirrhosis. (for
terminologies see table 1 below)

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Table1. Important terminologies in the natural history of HBV infection


Acute HBV infection ➢ New-onset hepatitis B infection that may or may not be symptomatic.
➢ Diagnosis is based on detection of HBsAg and IgM antibodies to
hepatitis B core antigen (anti-HBc).
Chronic HBV infection Persistence of HBsAg for ≥ 6 months after acute infection with HBV.
HBeAg seroconversion Loss of HBeAg and development of anti-HBe antibody
HBsAg seroconversion Loss of HBsAg and development of anti-HBs
HBeAg reversion Reappearance of HBeAg in a person who was previously HBeAg
negative
Cirrhosis ➢ An advanced stage of liver disease as evidenced by imaging or
biopsy. Characterized by:
o Extensive hepatic fibrosis
o Nodularity of the liver and alteration of liver architecture
Decompensated Clinical complications of cirrhosis become evident
cirrhosis o Jaundice
o Ascites
o SBP
o Esophageal varices and bleeding
o Hepatic encephalopathy
o Renal impairment

Diagnosis and diagnostic evaluation

➢ The diagnosis of HBV infection starts with HBsAg. If +ve do the IX listed
under Ix section above
➢ In addition to those suspected of having liver disease, certain group of
individuals need routine screening with HBsAg.
o Pregnant mothers
o Infants born to infected mothers
o Health care workers (including health professionals and supporting staff)
o Hemodialysis patients and organ transplant recipients
o People with multiple sexual partners and I.V drug users
o Sexual partners of infected individuals
o HIV or HCV positive patients

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Table 2. Phases of chronic HBV infection


HBsAg HBeAg HBV DNA ALT Liver Previous
disease (Old)
(fibrosis terminology
or
cirrhosis)
HBeAg phase HBeAg +ve high (usually normal None to Immune
positive 1 chronic >107 IU/ml) mild tolerant
HBV

infection Positive
with no
evidence of

current

hepatitis
phase HBeAg high (104 - Elevated present Immune
2 +ve 107 IU/ml) (persistently (moderate reactive
or HBeAg
chronic or
severe) positive
HBV intermittently)
hepatitis
HBeAg phase HBeAg -ve Positive Negative low (<2,000 Normal None Inactive
Negative 3 chronic IU/ml) or carrier
HBV undetectable
infection
with no

evidence of
current
hepatitis
phase HBeAg - high (>2,000 Elevated Present HBeAg
4 ve IU/ml) (persistently (moderate negative
or chronic
chronic or
severe) hepatitis
HBV intermittently)
hepatitis
HBsAg- phase Negative HBV Normal None occult HBV
negative 5 antibodies = infection
phase +ve anti-
HBcAg with
or without
anti-HBsAg.

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Follow up tests

➢ In patients with chronic HBV but no indications for antiviral therapy, liver injury
as well as viral replication can be variable; hence, regular monitoring is
required.
o ALT, APRI score, clinical evaluation every 3 months in all patients
o HBeAg initially negative: HBeAg and HBV DNA level every 6 -12 months
o HBeAg positive initially: HBV DNA level every 6 -12 months

Treatment
Objectives of treatment
The main objectives of HBV treatment
o Reduce progression to cirrhosis, HCC and associated mortality
o Improve liver fibrosis
o Preventing acute or subacute liver failure in acute HBV infection
o Controlling extrahepatic manifestations.
o Prevention of HBV reactivation.
o Prevention of mother to child transmission.
Intermediate objectives of treatment
o Suppression of HBV DNA levels
o Induction of HBeAg loss, with or without anti-HBe seroconversion
o Biochemical response; ALT normalization
o HBsAg loss: optimal goal but rarely achievable

Pharmacologic treatment
o Patients with HBsAg positivity with or without elevated transaminases or
evidence of CLD need evaluation for indications of therapy i.e. HBeAg
status, HBV DNA level

Indications for antivirals in chronic HBV infection.


➢ Indications are determined based on the presence or absence of cirrhosis,
APRI score (see IX section above), ALT, HBV DNA level, and HBeAg.
➢ The following are the indications
o All patients with cirrhosis (decompensated) and any detectable viral load:
Irrespective of ALT and HBeAg status.
o If no liver cirrhosis, one of the following is an indication for antiviral
treatment
✓ HBV DNA > 20,000 IU/ml and elevated ALT (above the UNL):
Irrespective of HBeAg status
✓ Detectable HBV DNA and APRI score ≥ 2 or elevated ALT (above
UNL): Irrespective of HBeAg status
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✓ Age above 30, HBeAg-positive and HBV DNA > 2,000: Irrespective of
ALT
✓ Co-infection with HIV.
✓ Patients with chronic HBV to be started on immunosuppresses.
✓ Extra hepatic manifestation

Indications for antiviral in acute HBV infection


➢ The presence acute liver failure or fulminant hepatitis with detectable HBV
DNA.

Antiviral choices
First line
✓ Tenofovir (Tenofovir disoproxil fumarate) (TDF) 300mg, PO, daily
• Avoid in patients with GFR <60ml/min

OR
✓ Entecavir 0.5mg, PO, daily.
• For patients with decompensated cirrhosis or those with previous
exposure to Lamivudine the dose should be increased to 1mg,
daily.
• Entecavir is preferred over Tenofovir in patients age > 60, CKD,
osteoporosis or steroid use.
Alternatives
✓ Telbivudine 600mg, PO, daily.
• It should only be used when both first lines are not available or
in patients with renal impairment when Entecavir is not available.

Monitoring treatment response


➢ HBV DNA: every 3 months until undetectable then every 6 months.
➢ ALT: every 3 months.
➢ HBeAg and antibody to HBeAg (anti-HBe): every 6 months in patients who are
HBeAg-positive.
➢ Monitoring side effects of tenofovir: serum creatinine and phosphate every 3-6
months.

Duration of antiviral therapy


➢ Most patients require indefinite treatment
➢ For patients with cirrhosis treatment should be continued indefinitely.
➢ For patients without cirrhosis: HBeAg seroconversion to negative and
development of HBeAb, if initially HBeAg is positive is considered as possible
endpoint of treatment.

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➢ For patients without cirrhosis and initially HBeAg is negative, it’s only loss of
HBsAg which is considered an endpoint but it happens very rarely; hence,
treatment is generally indefinite.

Treatment in special population

HBV/ HIV co-infection


➢ HIV co-infection profoundly affects almost every aspect of HBV infection and
includes more rapid progression to cirrhosis and HCC, higher liver-related
mortality, and decreased treatment response compared with persons without
HIV co-infection
➢ HIV/HBV-co-infected persons also demonstrated rapid HIV disease progression
compared to HIV-infected alone, and had an impaired recovery of CD4 cells.
➢ HIV patients are among the high-risk groups for HBV and should be given
priority for screening. i.e. all HIV patients should get screened for HBV and
evaluated for chronic infection.

Treatment options
➢ ART should be initiated in all HIV patients regardless of WHO staging or CD4
count in individuals co-infected with HIV and HBV with evidence of severe
CLD.
➢ If HBV treatment is indicated among HBV/HIV co-infection, combination ART
should be initiated with drugs containing TDF + 3TC (or FTC) + EFV as a
preferred regimen.
➢ Use of lamivudine as mono-therapy in any of these diseases is contraindicated
due to high resistance.
➢ When switching treatment in patients with HIV on ART failure, the regimen that
will continue should have two of the drugs having activity against HBV.
➢ If tenofovir-associated renal toxicity occurs, the dose of tenofovir should be
adjusted according to the renal clearance.

HCV coinfection:
➢ Treatment of HCV with direct-acting antivirals (DAAs) may cause reactivation of
HBV.
➢ Patients fulfilling the standard criteria for HBV treatment should receive
treatment.
➢ HBsAg-positive patients undergoing HCV treatment with DAA therapy should be
given concomitant treatment.

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Pregnancy:
➢ In all pregnant women with high HBV DNA levels >200,000 IU/ml Tenofovir
(TDF) should be started at 24 - 18 weeks of gestation and continue for up
to 12 weeks after delivery.
➢ Pregnant women already on NA therapy, Tenofovir should be continued, if on
another agent it should be switched to Tenofovir.
➢ Tenofovir is not contraindicated in breast feeding.

HBV vaccination in adults


Indications for vaccination
➢ Healthcare workers
➢ Immune-compromised individuals including HIV
➢ Organ transplant recipients
➢ Patients on maintenance hemodialysis
➢ Children 1-5 years who missed immunization for HBV
➢ Sexual partners and close contacts of infected individuals receive three doses
of HBV vaccine.

Vaccination schedule
✓ Standard schedule: 0, 1, and 6 months.
✓ Accelerated schedule: 0, 1 and 2 months.
• Accelerated schedule, if requested for rapid protection within 48
hours of exposure: 0, 7 and 21 days.
• After an accelerated course, a booster at one year is
recommended.

HBV Immunoglobulin
➢ HBV immunoglobulin provides passive immunity
➢ Indications: In individuals who have not been immunized or have not completed
the immunization and have the one of the following indications
o Perinatal exposure of an infant born to a HBsAg positive mother within
24 hours.
o Percutaneous or mucosal exposure to HBsAg-positive blood preferably
within 24-48 hr.
o Sexual exposure to an HBsAg-positive person

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Hepatitis C virus infection


➢ HCV is a small, RNA-enveloped virus with a highly variable genome.
➢ It has multiple genotypes and sub genotypes. There are currently 7 genotypes
identified with variable geographic distribution
➢ HCV is prevalent in Ethiopia and the commonest genotypes are genotype 4
(60%), followed by genotype 1 (20%).
➢ Risk factors for acquiring HCV: blood transfusion, IV drug use, cut or injury by
bloody object, ear piercing or tattooing
➢ HCV can cause acute and chronic hepatitis, liver cirrhosis, and HCC.
➢ HCV can also cause a number of extrahepatic manifestations:
Glomerulonephritis, vasculitis, thyroiditis, Sjogren syndrome, increase diabetes,
porphyria cutanea tarda and lichen planus.
➢ Male gender, age above 40 or advanced age during infection, alcohol intake,
HBV or HCV coinfection, fatty liver and obesity increase the risk of liver
cirrhosis.

Diagnosis and investigation


Whom to screen for HCV?
o Pregnant women
o Patients with liver disease
o Individuals with HBV and HCV infection
o Commercial sex workers and prisoners
o Individuals with risk of acquiring infection (e.g. IV drug use, tattooing,
body piercing)
Screening test
o Serum anti-HCV antibody rapid test or enzyme immunoassay EIA (ELISA)
o In the case of suspected acute hepatitis C, in immunocompromised
patients and in patients on hemodialysis, HCV RNA testing can be done
as an initial test.

Confirmatory test

➢ If anti-HCV antibodies are detected, HCV RNA should be determined by a


sensitive molecular method with a lower limit of detection ≤15 IU/ml) to confirm
the diagnosis.
➢ If anti-HCV antibody-positive, but HCV RNA-negative individuals, HCV RNA
levels should be repeated after 6 -12 months, to confirm past infection.

Investigations before initiation of treatment

➢ CBC, Liver enzymes and function test (AST, ALT, ALP, Bilirubin, ALB and
INR), Serum Creatinine, BUN
➢ Quantitative HCV RNA (IU/ml)
➢ Prégnancy test for reproductive Age group women.
➢ HIV and HBV screening
➢ Other tests; see IX section above

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Treatment

➢ All patients with HCV should be offered treatment. Those with liver disease or
extrahepatic manifestations should be treated more urgently.

Objectives of treatment
➢ To eradicate HCV RNA (attainment of a sustained virologic response (SVR)).
➢ SVR is defined as an undetectable HCV RNA level after 12 weeks of therapy.

Who should be treated with direct acting antivirals (DAA)?


➢ All patients with HCV infection, who are willing to be treated, should be
treated.
➢ Treatment should be started without delay in patients with significant fibrosis or
cirrhosis, including decompensated cirrhosis; patients with clinically significant
extra-hepatic manifestations.

Which agent to use?


➢ A simplified, pangenotypic anti-HCV treatment is preferred.
➢ Pre-treatment assessment can be limited to proof of HCV.

First line pangenotypic regimen


✓ Sofosbuvir/velpatasvir combination (400 mg of sofosbuvir and 100 mg
of velpatasvir), one tablet, daily for 12 weeks.

Alternative regimen
✓ Sofosbuvir 400 mg, PO, daily plus Daclatasvir 60mg PO, daily for 12
weeks or
✓ Sofosbuvir 400mg, PO, daily plus Ledipasvir 90mg, PO, daily for 12
weeks.
o For cirrhotic patient duration will be extended to 24 weeks for above
treatment options.

OR
✓ Sofosbuvir 400mg, PO, daily plus Ribavirin 1g (weight < 75kg), 1200mg
(weight ≥ 75Kg) twice on divided doses for 24 weeks.

Treatment monitoring
➢ HCV RNA at baseline, at the end of therapy (12 weeks) and after completion
of treatment.
➢ Toxicity of concurrent drugs given for comorbidities and potential drug-drug
interactions should be monitored.
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HCV/HIV co-infection

➢ HIV patients are among high risk groups for HCV. Therefore, all HIV patients
should be screened and confirmation Viral load test should be done for HCV
screened positives
➢ All chronic HCV infected individuals should be treated to eradicate the virus
and achieve cure so that complications can be avoided.
➢ Follow up quantitative or qualitative HCV RNA viral load is required to confirm
if the patient has achieved Sustained Virologic Response (SVR). This should
be performed 12 weeks after the completion of therapy.
➢ Treatment of HCV in HIV infected individuals is not different from non-HIV
infected or HCV mono-infected. In case of Sofosbuvir + Daclatasvir
combination, dose of Daclatasvir be adjusted to 90 mg with Efavirenz and 30
mg with Atazanavir/r instead of 60mg dose of non RVI patients

9.2.2 Alcoholic liver disease


➢ Chronic and excessive alcohol ingestion is one of the major causes of liver
disease.
➢ The pathology of alcoholic liver disease consists of 3 major lesions, with the
injury rarely existing in a pure form:

1. Fatty Liver → present in >90% of binge and chronic drinkers

2. Alcoholic Hepatitis → less common (10 - 20% of alcoholics) but


precursor to cirrhosis. alcohol is considered a direct hepatotoxin which
involves the complex interaction of facilitating factors, such as Amount and
frequency of intake, diet, and gender. (see risk factor section of CLD
above)

3. Cirrhosis

➢ The transition between fatty liver and the development of alcoholic hepatitis is
blurred. In fatty liver stage, cessation of drinking results in normalization of
hepatic architecture and fat content within the liver.
➢ Clinically, Differentiation of alcoholic fatty liver from nonalcoholic fatty liver is
difficult unless an accurate drinking history is ascertained
➢ Alcoholic hepatitis is thought to be a precursor to the development of cirrhosis.
However, like fatty liver, it is po tentially reversible with cessation of drinking.
➢ Cirrhosis is present in up to 50% of patients with biopsy-proven alcoholic
hepatitis and its regression is uncertain, even with abstention of alcohol.
➢ Chronic infection with HCV is an important comorbidity in the progression of
alcoholic liver disease to cirrhosis in chronic and excessive drinkers.
o Even moderate alcohol intake of 20 - 50 g/d increases the risk of
cirrhosis and HCC in HCV-infected individuals.
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o Patients with both alcoholic liver injury and HCV infection develop
decompensated liver disease at a younger age and have poorer overall
survival.

Management

➢ Complete abstinence from alcohol is the cornerstone in the treatment of


alcoholic liver disease.
➢ nutritional and psychosocial support
➢ glucocorticoids have been extensively evaluated in the treatment of alcoholic
hepatitis
o Patients with severe alcoholic hepatitis should be given prednisone, 32 -
40 mg/d, for 4 weeks, followed by a steroid taper
o Women with encephalopathy from severe alcoholic hepatitis may be
particularly good candidates for glucocorticoids
o Exclusion criteria include active GI bleeding, renal failure, or pancreatitis.
➢ alternative to glucocorticoids for severe alcoholic hepatitis.
o nonspecific TNF inhibitors (e.g. pentoxifylline)

Treatment algorithm for alcoholic hepatitis

Prognosis

➢ Critically ill patients with alcoholic hepatitis have short-term (30-day) mortality
rates >50%.
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➢ The mortality of patients with alcoholic hepatitis concurrent with cirrhosis is


nearly 60% at 4 years
➢ The presence of Ascites, Variceal hemorrhage, Deep encephalopathy, or
Hepatorenal syndrome Predicts a dismal prognosis.

9.2.3 Autoimmune hepatitis


➢ Autoimmune hepatitis is a chronic disorder of unknown etiology characterized
by continuing hepatocellular necrosis and inflammation, usually with fibrosis,
which can progress to cirrhosis and liver failure.
➢ Affects women more than men (3.6:1)
➢ Characteristics include: Presence of autoimmune antibody, Evidence of
hepatitis, Elevation of serum globulins
➢ The prominence of extrahepatic features of autoimmunity as well as sero
immunologic abnormalities in this disorder supports an autoimmune process in
its pathogenesis;
➢ Autoantibodies and other typical features of autoimmunity, however, do not
occur in all cases;
➢ Among the broader categories of "idiopathic" or cryptogenic chronic hepatitis,
many, perhaps the majority, are probably autoimmune in origin.
➢ The immune pathogenesis is Unknown, but assumed to be the result of a cell
mediated immunologic attack directed against liver cells.
➢ Genetically predisposed individual with exposure to an environmental agent
triggers the autoimmune pathogenic process.
➢ Overlap syndromes include; Primary Biliary Cirrhosis, Primary Sclerosing
Cholangitis, Chronic Hepatitis C.

Classification
I. Type I autoimmune hepatitis

o It Is the classic syndrome occurring in young women.


o ANA or Anti-Smooth Muscle antibody positive (Titer usually > 1:100)
o Bimodal age distribution (ages 10-20 and 45-70)
o Female : Male ratio = 3.6 : 1
o Associated with extrahepatic manifestations: Autoimmune thyroiditis,
graves’ disease, chronic Ulcerative Colitis. Less commonly with RA,
pernicious anemia, systemic sclerosis, ITP, SLE
o 40% present with acute onset of symptoms similar to toxic hepatitis or
acute viral hepatitis
II. Type II autoimmune hepatitis
o Often seen in children
o It Is not associated with ANA. 580
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III. Type III autoimmune hepatitis

o These patients lack ANA


o Most of these patients are women and have clinical features similar to,
perhaps more severe than, those of patients with type I autoimmune
hepatitis.

Diagnosis

Diagnostic Criteria
➢ Exclusion of other causes of liver disease (genetic disorders, viral hepatitis,
drug hepatotoxicity, & alcohol).
➢ Marked hyperglobulinemia and high-titer circulating ANA and other
autoantibodies;
➢ Characteristic histologic features (interface hepatitis, plasma cells, rosettes)

Factors that weigh in favor of the diagnosis include:


➢ Female gender
➢ Predominant aminotransferase elevation → >10 times normal in severe cases
➢ concurrent other autoimmune diseases → Occasionally arthritis, maculopapular
eruptions (including cutaneous vasculitis), erythema nodosum, colitis, pleurisy,
pericarditis, anemia, azotemia, and sicca syndrome (keratoconjunctivitis,
xerostomia) occur.
➢ Many patients with autoimmune hepatitis have normal serum bilirubin, alkaline
phosphatase, and globulin levels with only minimal aminotransferase elevations.
➢ In severe cases, the serum bilirubin level is moderately elevated (3 - 10
mg/dL).

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Management

➢ Treatment Should be based on: Severity of symptoms, Degree of elevation in


transaminases and IgG, Histologic findings, Potential side effects of treatment.
➢ Unfortunately, therapy has not been shown to prevent ultimate progression to
cirrhosis
➢ AASLD Recommendations
o Treat if serum aminotransferases are > 10 times normal
o Treat if serum aminotransferases are > 5 times normal and IgG is
elevated to > 2 times normal
o In patients with inactive cirrhosis → evaluate for preexisting comorbidities
(hep C), pregnancy, and drug intolerances (increased risk of steroid side
effects in pts with DM, osteoporosis, HTN)
o The mainstay of management in autoimmune hepatitis is glucocorticoid
therapy.
✓ Prednisone 60mg PO daily with a taper down to 30mg at the 4th week
into treatment and then maintenance of 20mg daily until reach endpoint
✓ Reasons for Prednisone only: Cytopenia, TPMT deficiency, Malignancy,
Pregnancy
COMBINATION THERAPY
✓ Prednisone: start at 30mg daily and taper down to 15mg at week 4,
then maintain on 10mg daily until therapy endpoint PLUS
✓ Azathioprine 50mg daily
o The advantage of the combination approach is a reduction Over the span
of an 18-month course of therapy in serious, life-threatening complications
of steroid therapy from 66% down to under 20%
o 6-mercaptopurine may be substituted for its prodrug azathioprine, but this
is rarely required
o Azathioprine alone, however, is not effective in achieving remission, nor is
alternative for glucocorticoid therapy.

TREATMENT REMISSION

➢ Disappearance of symptoms
➢ Normal serum bilirubin and IgG
➢ Serum aminotransferases normal or less than twice normal
➢ Normal hepatic tissue or minimal inflammation and no interface hepatitis.
➢ Action: d/c azathioprine and taper prednisone

TREATMENT FAILURE

➢ Worsening clinical, laboratory and histologic findins despite compliance with


therapy
➢ Increase in aminotransferases by >60%
➢ Action: increase prednisone to 60mg daily and azathioprine to 150mg daily for
one month
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➢ Treatment failures are frequent in patients with established cirrhosis, HLA-DR3


or in patients who present with disease at a younger age and with a longer
duration of symptoms

INCOMPLETE RESPONSE
➢ Some or no improvement in clinical, laboratory or histologic feature
➢ Failure to achieve remission after 3 years
➢ Action: indefinite treatment

LIVER TRANSPLANTATION

➢ Patients with ascites and hepatic encephalopathy → consider liver transplant if


they have failed glucocorticoid therapy.
➢ Considered in patients with multi lobar necrosis and have at least one
laboratory parameter which does not normalize within 2 weeks of treatment
(these patients have a high immediate mortality rate).
➢ Considered in pts who worsen while on glucocorticoid therapy.

Prognosis
➢ If untreated approximately 40% die within 6 months, 40% will develop cirrhosis
➢ the natural history of milder disease is variable, often accentuated by
spontaneous remissions and exacerbations. In treated autoimmune hepatitis, the
10-year survival is 80 - 90%.
➢ 13-20% of patients can have spontaneous resolution.
➢ Poor prognostic signs include:
o The presence histologically of multi lobular collapse at the time of initial
presentation
o ascites and hepatic encephalopathy
o Failure of the bilirubin to improve after 2 weeks of therapy
➢ Death may result from hepatic failure, hepatic coma, other complications of
cirrhosis (e.g., variceal hemorrhage), and intercurrent infection.
➢ In patients with established cirrhosis, HCC may be a late complication but
occurs less frequently than in cirrhosis associated with viral hepatitis.

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9.2.4 Genetic, metabolic and infiltrative diseases


affecting the liver
➢ Inherited disorders include hemochromatosis, Wilson's disease, α 1 antitrypsin
(α1AT) deficiency, and cystic fibrosis (CF).
o Hemochromatosis is the most common inherited disorder affecting
Caucasian populations
o A hint for diagnosis of genetic disorders may be existent of disease at a
relatively young age or a family history of liver disease.
➢ From metabolic disorders, nonalcoholic fatty liver disease (NAFLD) is the most
common cause of elevated liver enzymes. nonalcoholic steatohepatitis (NASH)
is relatively rare
➢ Infiltrative disorders of the liver are relatively rare → Lipid storage diseases
(Gaucher's and Niemann-Pick disease), Amyloidosis, sarcoidosis, etc

9.2.4.1 Hereditary Hemochromatosis

➢ Hemochromatosis is Iron in Hepatocytes.


➢ Hemochromatosis can be
➢ Primary or Hereditary hemochromatosis; Common in young age and usually
have positive family history, in addition to liver it can also affect heart,
pancreas (Causing DM which is more common than DM from Wilsons
disease), skin, GI malignancy (e.g. HCC)
➢ Secondary hemochromatosis; secondary to hemolytic anemia, dietary Iron
overload, blood transfusion etc.
➢ Hereditary hemochromatosis (HH) is a common inherited disorder of iron
metabolism.
➢ Most patients with HH are asymptomatic; however, when patients present with
symptoms, they are frequently nonspecific and include weakness, fatigue,
lethargy, and weight loss.
➢ Specific, organ-related symptoms include abdominal pain, arthralgias, and
symptoms and signs of chronic liver disease.
➢ Look at IX section of CLD for serum ferritin interpretation

Treatment

➢ weekly phlebotomy aimed to reduce iron stores, recognizing that each unit of
blood contains 200 to 250 mg of iron.
➢ Maintenance phlebotomy is required in most patients and usually can be
achieved with 1 unit of blood removed every 2 - 3 months

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9.2.4.2 Wilson’s disease


➢ Wilson's disease is an inherited disorder of copper homeostasis. in patients
with mutations in ATP7B, copper is retained in the liver, leading to increased
copper storage & ultimately liver disease as a result
➢ The clinical presentation of Wilson's disease is variable and includes chronic
hepatitis, hepatic steatosis, and cirrhosis in adolescents and young adults
➢ Wilson's disease is a multisystem disease with predilection to liver. It can also
involve Brain (various speech and movement disorders), Pancreas (DM), eyes
(Kayser-Fleischer rings), heart (rCMP), and hematologic disorders.
➢ Neurologic manifestations indicate that liver disease is present and include
various speech and movement disorders (Dysarthria, Dystonia, Tremor,
Parkinsonism, Choreoathetosis, Cerebellar ataxia, Cognitive impairment…).
➢ Diagnosis includes the demonstration of:
A reduced ceruloplasmin level
An elevated hepatic copper level
Increased urinary excretion of copper and
The presence of Kayser-Fleischer rings in the corneas of the eyes

Treatment

Treatment consists of copper-chelating medications such as D-penicillamine and


trientine.
A role for zinc acetate has also been established.
Medical treatment is lifelong, and severe relapses leading to liver failure and
death can occur with cessation of therapy.
Liver transplantation is curative with respect to the underlying metabolic defect
and restores the normal phenotype with respect to copper homeostasis.
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9.2.4.3 AAT (α1 ANTITRYPSIN) deficiency


➢ AAT is a glycoprotein produced in hepatocytes, phagocytes, and epithelial cells
in the lungs, which inhibits serine proteases, primarily neutrophil elastase.
➢ In AAT deficiency, increased amounts of neutrophil elastase can result in
progressive lung injury from degradation of elastin leading to premature
emphysema.
➢ AAT deficiency is known to be a cause of liver disease in infancy, early
childhood, adolescence, and in adults.
➢ The natural history of AAT deficiency is quite variable. Because of genetic
variation, many individuals never develop disease, whereas others can develop
childhood cirrhosis leading to liver transplantation.
➢ A hint to diagnosis may be coexistent lung disease at a relatively young age
or a family history of liver and/or lung disease.
➢ Liver disease may be asymptomatic other than fatigue, or patients may present
with complications of decompensated liver disease.
➢ Diagnosis of AAT deficiency is confirmed by blood tests showing reduced
levels of serum AAT
➢ Liver biopsy is often performed to determine stage of hepatic fibrosis and
shows characteristic PAS-positive, diastase-resistant globules in the periphery of
the hepatic lobule.

Treatment

➢ Treatment of AAT deficiency is usually nonspecific and supportive.


➢ For patients with liver involvement, other sources of liver injury, such as
alcohol, should be avoided.
➢ Evidence for other liver diseases (e.g., viral hepatitis B and C
➢ hemochromatosis, NAFLD, etc.) should be sought and treated if possible.
➢ Smoking can worsen lung disease progression in AAT and should be
discontinued.
➢ Patients with lung disease may be eligible to receive infusions of AT, which
has been shown to halt further damage to the lungs.
➢ If liver disease becomes decompensated, transplantation should be pursued
and is curative.
➢ Finally, risk of HCC is significantly increased in patients with cirrhosis due to
AAT deficiency.

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9.2.4.4 Nonalcoholic Fatty Liver Diseases (NAFLD) and


Nonalcoholic Steatohepatitis (NASH)
➢ Nonalcoholic fatty liver disease (NAFLD) is the most common CLD in many
parts of the world, including the United States (25%). This data is from the
westerns. but in our set up, even though there is no national data, NAFLD
and NASH are rare to consider
➢ NAFLD is strongly associated with overweight/obesity and insulin resistance.
➢ However, it can also occur in lean individuals and is particularly common in
those with a paucity of adipose depots (i.e., lipodystrophy).
➢ Risk factors for NAFLD include; increased BMI (50–90% of NAFLD patients
are obese), insulin resistance/type II DM, and other parameters indicative of
the metabolic syndrome (e.g., systemic hypertension, dyslipidemia,
hyperuricemia/gout, cardiovascular disease) in the patient or family members.
➢ On the other way, NAFLD is an independent risk factor for metabolic
syndrome. Patients with NASH are at 2-3 fold increased risk for the
development of metabolic syndrome.
➢ Ethnic/racial factors also appear to influence liver fat accumulation
➢ NAFLD encompasses a spectrum of liver pathology with different clinical
prognoses.
➢ The simple accumulation of triglyceride within hepatocytes (hepatic steatosis) is
on the most clinically benign extreme of the spectrum. On the opposite, most
clinically ominous extreme, are cirrhosis and primary liver cancer.
➢ The risk of developing cirrhosis is extremely low in individuals with chronic
hepatic steatosis, but increases as steatosis becomes complicated by
histologically conspicuous hepatocyte death and inflammation (i.e., nonalcoholic
steatohepatitis [NASH]).
➢ NASH literally means fat in hepatocytes and it is histologic definition form of
NAFLD.
➢ NASH itself is also a heterogeneous condition; sometimes it improves to
steatosis or normal histology, sometimes it remains relatively stable for years,
but sometimes it results in progressive accumulation of fibrous scar that
eventuates in cirrhosis.
➢ Many patients can have advanced fibrosis with NASH and even cirrhosis due
to NASH with normal liver enzymes
➢ Once NAFLD-related cirrhosis develops, the annual incidence of primary liver
cancer can be as high as 3%.
➢ NASH is present in about 25% of individuals who have NAFLD
➢ The mechanisms underlying the pathogenesis and progression of NAFLD are
not entirely clear.
➢ Hepatic steatosis is proven to result when hepatocyte mechanisms for
triglyceride synthesis (e.g., lipid uptake and de novo lipogenesis) overwhelm
mechanisms for triglyceride disposal (e.g., degradative metabolism and
lipoprotein export), leading to accumulation of fat (i.e., triglyceride) within
hepatocytes. So, the net result is hepatic triglyceride accumulation (i.e.,
steatosis). Obesity and Insulin resistance are the most important risk factors for
NASH pathogenesis.
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➢ Triglyceride per se is not hepatotoxic. However, its precursors (e.g., fatty acids
and diacylglycerols) and metabolic by-products (e.g., reactive oxygen species)
may damage hepatocytes, leading to hepatocyte death and
lipotoxicity.
➢ NASH is the morphologic manifestation of lipotoxicity and resultant wound
healing responses
➢ Cirrhosis and liver cancer are potential outcomes of chronic NASH.

DIAGNOSIS

➢ The diagnosis of NAFLD and NASH is clinical.


➢ Diagnosing NAFLD requires demonstration of increased liver fat in the absence
of hazardous levels of alcohol consumption (<20 g/d of alcohol be consumed
to exclude alcoholic liver disease).
➢ hazardous levels of alcohol consumption defined as > 1 drink per day in
women or > 2 drinks per day in men based on epidemiologic evidence that
the prevalence of serum aminotransferase elevations increases when alcohol
consumption habitually exceeds these levels.
➢ One drink is defined as having 10 g of ethanol and, thus, is equivalent to one
can of beer, 4 ounces of wine, or 1.5 ounces (one shot) of distilled spirits.
➢ It is a diagnosis of exclusion. Other causes of liver fat accumulation
(particularly exposure to certain drugs) and liver injury (e.g., viral hepatitis,
autoimmune liver disease, iron or copper overload, α1 antitrypsin deficiency)
must also be excluded.
➢ Confidence in the diagnosis of NAFLD is increased by identification of NAFLD
risk factors.
➢ There is yet no one specific blood test for NAFLD
➢ Abdominal Ultrasound; is an acceptable first-line test; CT or MRI enhances
sensitivity for liver fat detection but adds expense.
➢ It is important to emphasize that the liver may not be enlarged, Lever enzymes
and LFT (e.g., bilirubin, albumin, prothrombin time) may be completely normal,
in individuals with NAFLD
➢ In Liver biopsy, the histologic features of NASH are very similar to those seen
in alcoholic liver disease; Mallory's hyaline can be seen in both disorders,
although the number of hepatocytes containing Mallory's hyaline and the size
of the deposits are frequently greater in alcoholic liver disease than in NASH.

TREATMENT

➢ Treatment of NAFLD can be divided into three components:


o Specific therapy of NAFLD-related liver disease
o Treatment of NAFLD associated comorbidities
o Treatment of the complications of advanced NAFLD → Which involves
management of the complications of cirrhosis and portal hypertension,
including primary liver cancers.
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➢ At present, there are no approved therapies for the treatment of NAFLD. Thus,
the current approach to NAFLD management focuses on treatment to improve
the risk factors for NASH ((i.e., obesity, insulin resistance, metabolic syndrome,
dyslipidemia)
➢ Lifestyle changes and dietary modification are the foundation for NAFLD
treatment.
➢ Only patients with NASH or those with features of hepatic fibrosis on liver
biopsy are considered currently for targeted pharmacologic therapies.
➢ No agent has yet been approved by the FDA for the treatment of NAFLD.
Hence, this remains an area of active research.

9.2.4.5 Other causes of CLD

Primary biliary cirrhosis

➢ May be asymptomatic or complain of fatigue, pruritus, and non-jaundice skin


hyperpigmentation with hepatomegaly.
➢ There is prominent alkaline phosphatase elevation as well as elevations in
cholesterol and bilirubin.
➢ Gold standard diagnosis is antimitochondrial antibodies with liver biopsy as
confirmation if showing florid bile duct lesions.
➢ It is more common in women.

Primary sclerosing cholangitis (PSC)

➢ PSC is a progressive cholestatic disorder presenting with pruritus, steatorrhea,


fat soluble vitamin deficiencies, and metabolic bone disease.
➢ There is a strong association with IBD, especially ulcerative colitis.
➢ Diagnosis is best with contrast cholangiography showing diffuse, multifocal
strictures and focal dilation of bile ducts, leading to a beaded appearance.
➢ Non-specific serum immunoglobulins may also be elevated.

9.3 Jaundice and hyper bilirubinemia


➢ Jaundice, or icterus, is a yellowish discoloration of tissue resulting from the
deposition of bilirubin.
➢ Hyperbilirubinemia is chemical definition for increased serum bilirubin levels
➢ Tissue deposition of bilirubin occurs only in the presence of serum
hyperbilirubinemia and is a sign of either liver disease or, less often, a
hemolytic disorder.
➢ Increased serum bilirubin levels occur when an imbalance exists between
bilirubin production and clearance.
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➢ As serum bilirubin levels rise, the skin will eventually become yellow in light-
skinned patients and even green if the process is long-standing. The green
color is produced by oxidation of bilirubin to biliverdin.
➢ Another sensitive indicator of increased serum bilirubin is darkening of the
urine (tea- or cola-colored), which is due to the renal excretion of conjugated
bilirubin.
o Bilirubinuria indicates an elevation of the direct serum bilirubin fraction
and, therefore, the presence of liver disease

Production and Metabolism of Bilirubin


➢ Bilirubin is the end product of heme degradation
➢ The formation of bilirubin occurs in reticuloendothelial cells, primarily in the
spleen and liver.
➢ Hemoglobin (breakdown in RBC) → heme (catalyzed by heme oxygenase) →
biliverdin + carbon monoxide + iron (biliverdin catalyzed by biliverdin reductase)
→ bilirubin
➢ Bilirubin is virtually insoluble in water. To be transported in blood, bilirubin
must be solubilized by its reversible, noncovalent binding to albumin
➢ Transfer of bilirubin from blood to bile involves four distinct but interrelated
steps
o 1st; Hepatocellular uptake
o 2nd; Intracellular binding
o 3rd; Conjugation
o 4th; Biliary excretion
➢ Unconjugated bilirubin bound to albumin is transported to the liver. After
entering the hepatocyte, unconjugated bilirubin is bound in the cytosol to a
number of proteins including proteins in the glutathione-S-transferase
superfamily
➢ In the endoplasmic reticulum, bilirubin is solubilized by conjugation to
glucuronic acid
➢ Bilirubin is conjugated with one or two glucuronic acid moieties by a specific
uridine diphosphate (UDP)-glucuronosyltransferase to form bilirubin mono- and
diglucuronide, respectively. These glucuronide conjugates are highly soluble in
water.
➢ The now hydrophilic bilirubin conjugates diffuse from the endoplasmic reticulum
to the canalicular membrane,
➢ Conjugation is obligatory for excretion of bilirubin across the bile canalicular
membrane into bile. So, the conjugated bilirubin excreted into bile drains into
the duodenum and passes unchanged through the proximal small bowel.
Conjugated bilirubin is not taken up by the intestinal mucosa.
➢ When the conjugated bilirubin reaches the distal ileum and colon, It is
hydrolyzed to unconjugated bilirubin by bacterial β-glucuronidases.
➢ The unconjugated bilirubin is reduced by normal gut bacteria to form
urobilinogens.
o About 80 - 90% of these products are excreted in feces, either
unchanged or oxidized to orange derivatives called urobilins.
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o The remaining 10 - 20% of the urobilinogens are passively absorbed,


enter the portal venous blood, and are reexcreted by the liver.
o A small fraction (usually <3 mg/dL) escapes hepatic uptake, filters across
the renal glomerulus, and is excreted in urine.
➢ Unconjugated bilirubin is not excreted in urine, as it is too tightly bound to
albumin for effective glomerular filtration and there is no tubular mechanism for
its renal secretion.
➢ In contrast, the bilirubin conjugates are readily filtered at the glomerulus and
can appear in urine in disorders characterized by increased bilirubin conjugates
in the circulation.
➢ It should be kept in mind that the kidney can serve as an “overflow valve” for
conjugated bilirubin.

Measurement of Serum Bilirubin


➢ The terms direct and indirect bilirubin — that is, conjugated and unconjugated
bilirubin, respectively — are based on the original van den Bergh reaction.
➢ With the van den Bergh method, the normal serum bilirubin concentration
usually is between 1 and 1.5 mg/dL. Total serum bilirubin concentrations are
between 0.2 and 0.9 mg/dL in 95% of a normal population.
➢ With this method, the direct fraction provides an approximation of the
conjugated bilirubin level in serum. The indirect fraction is the difference
between the total and the direct bilirubin levels and provides an estimate of
the unconjugated bilirubin in serum.
➢ Unconjugated (indirect) hyperbilirubinemia is present when the direct fraction is
<15% of the total serum bilirubin.

𝒅𝒊𝒓𝒆𝒄𝒕 𝒃𝒊𝒍𝒊𝒓𝒖𝒃𝒊𝒏
𝒊. 𝒆 𝒓𝒂𝒕𝒊𝒐 = 𝒙 𝟏𝟎𝟎 %
𝑻𝒐𝒕𝒂𝒍 𝒃𝒊𝒍𝒊𝒓𝒖𝒃𝒊𝒏
𝑹𝒂𝒕𝒊𝒐 > 𝟏𝟓% 𝒊𝒎𝒑𝒍𝒊𝒆𝒔 𝒅𝒊𝒓𝒆𝒄𝒕 𝒉𝒚𝒑𝒆𝒓𝒃𝒊𝒍𝒊𝒓𝒊𝒃𝒊𝒏𝒆𝒎𝒊𝒂
𝑹𝒂𝒕𝒊𝒐 < 𝟏𝟓% 𝒊𝒎𝒑𝒍𝒊𝒆𝒔 𝒊𝒏𝒅𝒊𝒓𝒆𝒄𝒕 𝒉𝒚𝒑𝒆𝒓𝒃𝒊𝒍𝒊𝒓𝒊𝒃𝒊𝒏𝒆𝒎𝒊𝒂

➢ The presence of even limited amounts of true conjugated bilirubin in serum


suggests significant hepatobiliary pathology.
➢ As conjugated hyperbilirubinemia is always associated with bilirubinuria (except
in the presence of delta bilirubin in prolonged cholestasis when jaundice is
overt), detection of bilirubin in urine via dipstick test
is extremely helpful to confirm the presence of conjugated hyperbilirubinemia in
a patient with mildly elevated direct fraction.
➢ Unconjugated bilirubin is always bound to albumin in the serum, is not filtered
by the kidney, and is not found in the urine.
➢ Any bilirubin found in the urine is conjugated bilirubin.
➢ The presence of bilirubinuria on urine dipstick test (Ictotest) indicates an
elevation of the conjugated bilirubin fraction that cannot be excreted from the
liver, and implies the presence of hepatobiliary disease.
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Approach to a Patient with Jaundice

FIGURE 45-1 Evaluation of the patient with jaundice; ALT, alanine


aminotransferase; AMA, antimitochondrial antibody; ANA, antinuclear antibody; AST,
aspartate aminotransferase; CMV, cytomegalovirus; EBV, Epstein-Barr virus; LKM,
liver-kidney microsomal antibody; MRCP, magnetic resonance
cholangiopancreatography; SMA, smooth-muscle antibody; SPEP, serum protein
electrophoresis.

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TABLE 45-3 Cholestatic Conditions That May Produce Jaundice

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Disorders of Bilirubin metabolism leading to unconjugated hyperbilirubinemia

➢ Increased Bilirubin production.


o Hemolysis
o Ineffective Erythropoiesis
o Degradation of the hemoglobin of extravascular collections of erythrocytes,
such as those seen in massive tissue infarctions or large hematomas
➢ Decreased Hepatic bilirubin clearance
o Decreased Hepatic Uptake. E.g. Gilbert’s syndrome, Several drugs and
cholecystographic contrast agents.
o Impaired Conjugation; Physiologic neonatal jaundice, Acquired Conjugation
defects
o Hereditary defects in bilirubin conjugation; Crigler-Najjar Syndrome, Type I
and type II, Gilbert’s Syndrome

Disorders of Bilirubin metabolism leading to mixed or predominantly conjugated


hyperbilirubinemia

➢ Almost all are Familial defects in hepatic excretory function which include;
o Dubin-Johnson Syndrome
o Rotor Syndrome
o Benign Recurrent Intrahepatic Cholestasis
o Progressive Familial Intrahepatic Cholestasis

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Chapter 10; DM /Diabetes


Mellitus/ (የስኳር በሽታ)
Dr. Mulualem. G

Clinical features and how to write hx of DM patient


History

N.B Type one DM patients usually present with poly symptoms. But type two
DM patients may present with complication or Asymptomatic and
diagnosed accidentally while patients visit a health facility for other
reason.
Poly symptoms (3P)
➢ Poly urea → Write in terms of Day to Night ratio (e.g. poly urea of 8:6
day to night ratio).
☛ The 24-hour urine voided by a healthy adult range from
600 to 2000ml
☛ Polyuria considered when there is consistent elimination of
an abnormally large volume of urine, > 3000ml/24hr
o (>3 liters per day or if not quantified a history of
increase in urination frequency with increase in
volume of urine)
➢ Polydipsia → ask How much litre of water he/she drinks per day
➢ Polyphagia → less common smx than Polydipsia and Poly urea

Weight loss despite increased appetite


Generalized weakness or malaise
DKA smx’s like Vomiting, Abdominal pain and LOC
Some type 2 DM patients can present with chronic complications of diabetes
mellitus. Other features of DM are
 Blurred vision or Visual impairment
 Recurrent skin infections
 Recurrent itching of the vulva (candida infections)
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 Abnormal sensory/ motor neurologic findings on extremities


▪ Numbness or pain over the lower limbs
 Foot abnormalities (various deformities, ulcers, and ischemia) could be a
presenting signs.
 Symptoms and Signs of Acute complications
Hyperglycemia features include → 3P, DKA/HHS, blurring of vision, dry mouth
and other signs of DHN especially in HHS
In a patient with established DM, the initial assessment should also include
special emphasis on prior diabetes care, including the type of therapy, prior
HbA1c levels, self-monitoring blood glucose results, frequency of hypoglycemia,
presence of DM specific complications, and assessment of the patient’s
knowledge about diabetes, exercise, and nutrition.

Risk factors
For Type II DM* For Type I DM*
The ADA recommends screening All Individuals >40 ✓ Genetic (abnormality in HLA region on
years every 3 years and Screening individuals at An Chromosome 6)
Earlier Age if they are Overweight [ BMI >25 kg/m2] and o The concordance of type 1 DM
in identical twins ranges between
Have One additional Risk Factor for diabetes
40 and 60%, indicating that
Individuals with any one of the following need screening additional modifying factors are
for type II diabetes. If the result is normal, repeat likely involved in determining
screening every 3 years; but if the result is in the whether diabetes develops.
prediabetes range repeat the test every year. o Although the risk of developing
type 1 DM is increased tenfold in
✓ HTN relatives of individuals with the
✓ Dyslipidemia (HDL < 35mg/dl and/or triglyceride level > disease, the risk is relatively low:
250mg/dl) 3–4% if the Parent has type 1
✓ Family history (First-degree relative with diabetes) diabetes and 5–15% in a Sibling
o Type II DM pts have strong genetic association (depending on which HLA
than type I DM haplotypes are shared). Hence,
o The concordance of type II DM in identical twins most individuals with type 1 DM
is between 70 and 90%. do not have a first-degree
o If both parents have type II DM, the risk relative with this disorder.
approaches 40%. ✓ Autoimmunity→ like Hashimoto’s
✓ Environmental factors thyroiditis
o Overweight or central obesity (BMI >25kg/m2) ✓ Environmental factors
▪ ≥ 80% of type II DM pt’s are Obese o Diet→cow milk during infancy→
o Physical inactivity antibody to cow insulin is similar
o Increased intake of Raw meat, fat and lipid to human insulin known as
containing food antigen mimickeracy
o Smoking o Toxin → which affect pancreatic
o Alcohol intake B cells
o Mumps, rubella, coxsackie
✓ Old age (age ≥ 45)
✓ Ethnicity→ common in African American
✓ Individuals with prediabetes should be tested yearly
infection
✓ Young age (age <30)
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✓ PCOS (polycystic ovary sxx) in females or acanthosis


nigricans
✓ History of atherosclerotic Cardiovascular disease
✓ Drugs → steroids (prednisolone), Phenytoin, thiazide
✓ Women with history of GDM (gestational DM)
✓ Chronic pancreatitis
✓ Pheochromocytoma
✓ Acromegaly
*no clear-cut boundary for Type I & II DM in RF. One can be RF for the other.

N.B Metabolic SXX


✓ a.k.a syndrome x, insulin resistance sxx, obesity dyslipidaemia sxx
✓ It Includes (Mnemonics → Angeles Have Healthy Life style)
o Abdominal obesity (BMI > 40 kg/m2 for male and >30 kg/m2 for
female or waist circumference >102 cm for male and >88 for
female)
o Hyperglycemia (DM)
o HTN
o Lipid abnormality (Hyperlipidemia, dyslipidemia)

Complication of DM

1. Acute complications
▪ DKA
▪ HHS
▪ Hypoglycaemia
▪ Infection
▪ Lactic acidosis
➢ Acute complications may occur at any stage of the disease

Chronic complications

➢ Chronic Complications begin to appear during the Second Decade of


hyperglycemia.
➢ Individuals with previously undetected Type II DM may present with chronic
complications of DM at the time of diagnosis.
➢ Classified as microvascular, macrovascular and avascular complications
❖ Micro vascular
▪ Retinopathy (Non proliferative or proliferative), Macular oedema
Almost everyone with Type I DM will eventually develop
Nonproliferative Retinopathy. But luckily, the retinopathy that
destroys vision, Proliferative Retinopathy, is far less common.
▪ Neuropathy
It can be Mono neuropathy, poly neuropathy, mono neuropathy
multiplex or autonomic neuropathy
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Most common (50-75%) cause of non-traumatic foot Amputation


▪ Nephropathy
DM is most common cause of renal insufficiency or renal failure.
ESRD is more common in Type I DM than Type II DM
Diabetic Nephropathy have 5 stages
1) Renomegaly, increased GFR
2) Basement membrane thickening
3) Micro albuminuria (30-300 mg/dl)
4) Macro albuminuria (>300 mg/dl)
5) ESRD (End stage renal disease), Uraemia, HTN
❖ Macro vascular
▪ CAD (coronary artery disease like MI & IHD. N.B DM is the most
common cause of Silent MI (the so called ‘’DM is silent killer’’))
▪ CVA (cerebrovascular Attack like stroke & TIA)
▪ PAD (Peripheral arterial disease)
❖ Avascular
▪ GIT
Gastro paresis → manifest with Diarrhoea, post prandial bloating,
fullness and discomfort, intestinal obstruction
Motility disorders → atony (manifest with constipation) or
hypersonic (manifest with Diabetic Diarrhoea)
▪ GUS → uropathy, sexual dysfunction (like decreased libido, impotence)
▪ Skin → diabetic foot ulcer (cellulitis, gangrene)
▪ Infections → UTI, pneumonia, periodontal infection, Malignant Otitis
externa (specific to DM), Rhino orbito cerebro mucoro mycosis (extremely
rare but specific to DM)
▪ Cataract, glaucoma
▪ Bone destruction
▪ Others which are specific to DM
Acalculous cholecystitis
Tubular papillary necrosis (ATN)
Volvo vaginal candidiasis, oral candidiasis

Look at Screening and management of Chronic complications of DM below


under management section

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Sample history
Chief compliant

polydipsia and polyuria of three weeks duration

HPI

This patient was last relatively healthy 03 weeks back at which time he started to
experience polyuria of 7- 8 times during night and 10-12 times during daytime with
increased feeling of thirst for which he drinks 4 - 6 liters of water per day but no
polyphagia.

Associated with this he also experienced unquantified but significant weight loss to
the extent his trousers become loose despite increased appetite, generalized
weakness to the extent he couldn’t perform his routine daily activities.

For this complaint he visited a private clinic in Gondar town where he was told to
have increased blood sugar level and referred to our hospital for better investigation
and management. From the referral paper, RBS was 350mg/dl and repeated on next
day of first determination and the value was 289 mg/dl, FBS was 194 mg/dl, from
U/A glucose was +2 and ketone free but no treatment given.

▪ No family hx of similar illness (Genetics)


▪ No self or family hx of HTN (RF)
▪ No hx smoking or chronic alcohol intake (RF)
▪ No hx of Drug (prednisolone, thiazide, phenytoin predispose to DM, lithium and diuretics are
DDX for polyuria)
▪ He/she usually eats injera made of ‘‘teff’’ and ‘‘machilla’’ and ‘’wott’’
made of ‘‘atter’’ and ‘‘dagusa’’ 3-4 times per day. Occasionally he
eats meat during holidays (Increased intake of Raw meat, fat and lipid containing food are
RF for DM)
▪ No hx of Anterior neck swelling, heat intolerance, profuse sweating,
sleep disturbance, palpitation, tremor or irritability (autoimmune disease like
Hashimoto’s thyroiditis can occur concomitantly with Type I DM)
▪ No hx of LOC, Abdominal pain or Vomiting (DKA→CXN)
▪ No hx of blurring of vision, eye pain or discharge (retinopathy →CXN)
▪ No hx of Flank pain, dysuria, hematuria, urgency or frequency
(Nephropathy, UTI →CXN)
▪ No hx of numbness, tingling, burning sensation, or wound over the
body (DM patients don’t sense pain during trauma due to neuropathy which predispose to Diabetic
ulcer →CXN)
▪ No hx of body weakness or sensory loss (CVA like stroke →CXN)
▪ No hx of chest pain, Dyspnea, orthopnea, PND or Palpitation (CAD/MI/
ending up in CHF →CXN)
▪ No hx of cough, fever or fast breathing (pneumonia →CXN)
▪ No hx of intermittent claudication, bluish discoloration of skin, cold


skin or skin Ulcer (PAD →CXN)
No hx Nausea, vomiting, diarrhoea, or constipation (Gastroparesis, motility
disorder →CXN)
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▪ No hx of Head injury or Neurosurgery (central Diabetic Insidious→ DDX)

Finally, he was admitted to our hospital walking by himself.

Physical examination (pertinent findings)

In your physical examination assess signs of DKA and Diabetic Foot


ulcer together with these pertinent findings.

1 GA

✓ Obesity
✓ Cushionoid face
Vital signs
✓ OHT→ due to Autonomic neuropathy
✓ HTN → >130/80 is HTN in DM
✓ Resting tachycardia → due to Autonomic neuropathy
✓ Obesity → calculate BMI and measure Waist circumference

o CALCULATE BMI AND CLASSIFY AS FOLLOWS

o WAIST CIRCUMFERENCE
▪ Normal
• Males <94 cm
• Females <80 cm
▪ Measure midway between lower costal margin & iliac crest as shown
in the picture below.

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HEENT
✓ Hair loss
✓ Periorbital swelling → Mucor mycosis
✓ Active Ear discharge → Malignant otitis externa
✓ Oral thrush → oral candidiasis
✓ Poor dental hygiene (tooth loss)
✓ Xanthelasma → N.B it is common around eye lids and Achilles tendon
✓ Cataract
LGS
✓ Thyroid enlargement → poly glandular autoimmune disorder (PGAID)
✓ Loss of sweating → due to Autonomic neuropathy
RS
✓ Signs of consolidation → pneumonia (common infection in DM)
CVS
✓ Arterial examination especially posterior tibial artery and dorsalis pedis
artery (PAD)
✓ IHD
Abdominal examination
✓ Hepatomegaly → from fatty liver
✓ Abdominal distention → from Gastroparesis or atony
✓ Intestinal obstruction → from autonomic neuropathy
✓ Murphy sign +ve → acalculous cholecystitis
GUS
✓ Supra pubic tenderness or CVAT → UTI, pyelonephritis
✓ Active vaginal discharge or whitish plaque → vaginal candidiasis (common
than oral candidiasis)
✓ Urinary bladder atony → voiding difficulty → due to Autonomic neuropathy
✓ Impotence → due to Autonomic neuropathy
MSS
✓ Diabetic foot ulcer
✓ Deformities → hammer toes, claw toes, prayers hand sign
✓ Duptyrens contracture

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Image; prayers sign


IS
✓ Cold/dry skin, crackles, fissures → autonomic neuropathy
✓ Hair loss
✓ Skin atrophy
✓ Acanthosis nigricans
✓ Infections
✓ Insulin injection sites
NS
✓ GCS
o LOC → DKA
✓ Cranial nerve
o Cranial nerve palsy (CN III, IV, VI and VII)
✓ Motor
o Muscle wasting
o Hypotonia
o Decreased power
o Hyporeflexia
o Peripheral neuropathy
▪ Motor neuropathy → foot drop, wrist drop, mono neuropathy
multiplex
✓ Sensory
o Peripheral neuropathy → distal symmetric polyneuropathy (DSPN)
which is glove and stocking pattern with sensory loss or
paraesthesia. Pain and temperature loss are common.
✓ Autonomic neuropathy
• Urinary bladder atony → voiding difficulty
• Impotence
• Resting tachycardia
• Loss of sweating
• GI neuropathy → Gastroparesis, Diabetic diarrhoea

N.B several Rare Infections are seen almost exclusively in the diabetic population.
Examples include
❖ Rhino-cerebral Mucor-mycosis
❖ Emphysematous Infections of the Gall Bladder and Urinary Tract
❖ "Malignant" or Invasive Otitis Externa.
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DDX

For Patient presenting with polyuria and/or polydipsia

1. DM
2. Diabetic insipidus (DI)
DI is a disorder resulting from abnormalities of Antidiuretic hormone (ADH)
production from the hypothalamus or ADH action in the kidney. Final common
pathway → no response to ADH
Characterized by polyuria and polydipsia → the passage of copious amounts of
dilute urine (low specific gravity, usually < 1.010).
There are 4 Types of DI, the 1st two are common forms
Nephrogenic DI → a.k.a peripheral DI. Due to increased resistance of ADH
receptors in kidney to ADH
✓ Nephrogenic causes
• Congenital
• Acquired
o CRF
o Lithium
o Hypokalemia
o Hypercalcemia
Neuropathic DI → a.k.a central, hypothalamic, pituitary or neurohypophyseal DI.
Caused by decreased secretion or lack of secretion of ADH from posterior
pituitary. Head injury or neurosurgery are risk factors for central DI.
▪ Central/Cranial causes
➢ Congenital
➢ Acquired
 Post traumatic
 Iatrogenic (post-surgical)
 Tumours
 Infection
 Idiopathic
Gestational DI → Caused by a deficiency of the antidiuretic hormone,
vasopressin, that occurs only during pregnancy
Dipsogenic DI → a form of primary polydipsia. Caused by Abnormal thirst and
Excessive intake of water or other liquids

3. Drugs → lithium, diuretics (Furosemide, thiazide), Alcohol


4. Pheochromocytoma
5. AKI/CKD
6. Psychogenic polydipsia → patient drinks as he/she assume of being dry
mouth, common in mental disorders
7. Hypercalcemia/hypokalaemia
8. Addison’s disease
9. ? Cushing sxx 603
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IX

1. Baseline investigations for Type 2 DM


➢ Urine analysis-If proteinuria is detected, repeat after 3 months, if still
there refer to specialist or manage as per diabetic nephropathy protocol
➢ Lipid profile, SGOT/SGPT /ALP – (if available)
➢ Serum Creatinine – (if available)- If abnormal – refer to internist or
nephrologist
N.B – For both Type 1 and Type 2 DM patients, check urine for
ketones if blood glucose
≥250 mg/dl

2. Blood sugar → look at table below under discussion part for ADA diagnostic
criteria of DM
✓ RBS
N.B FBS and HbA1c are
✓ FBS
✓ OGTT reliable for screening
✓ HbA1c → tells about the past 3 months sugar level. Normal value is 4 -
5.6% of body Haemoglobin.
3. U/A → what do you expect from U/A
✓ Glucosuria (glucose +2, +3…)
✓ Ketonuria from DKA (ketone +2, +3…)
✓ Albuminuria from DM nephropathy
✓ WBC casts → suggest infection like UTI, pneumonia, sepsis
4. CBC → what do you expect from CBC
✓ Leukocytosis
✓ Anemia
✓ Ketone bodies
5. Serum electrolyte → hyperkalaemia despite decreased K+ level in cells because
acidosis impairs H+/ K+ pump (i.e. impair K+ absorption from blood stream). K+
Increase in blood during analysis but hypokalaemia in cells.
6. RFT
7. Lipid profile → increased LDL, Triglyceride, and cholesterol but decreased HDL
8. PICT
9. ECG & CXR → if indicated
10. Serum insulin level and C-peptide → C-peptide < 0.6 ng/dl in Type I DM
and > 1 ng/dl in >1-2 years for type II DM (Serum insulin or C-peptide
measurements do not always distinguish type 1 from type 2 DM, but a low C-
peptide level confirms a patient's need for insulin.
11. Islet cell auto antibody → Anti - GAD (Glutamic acid decarboxylase) & Anti -
insulin antibody
12. Blood and urine culture
13. Serum PH and ketone
14. ABG (Arterial blood gas) analysis 604
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✓ PH → acidosis
✓ Serum bicarbonate → low which shows metabolic acidosis
✓ Anion gap = 2Na+ - (CI- + HCO3-) or (Na+ + K+) - (CI- + HCO3-)
✓ O2 & CO2 → low CO2 due to respiratory compensation.

In newly diagnosed patients


➢ Diagnostic tests: Fasting or random blood glucose, glycated hemoglobin
(HbA1c)
➢ Urine ketones
➢ Urine albumin
➢ BUN and creatinine
➢ Fasting lipid profile
➢ ECG (adults)
In diagnosed patients, follow up investigations
➢ Glycemic control: HbA1c, FBS together with post prandial plasma glucose (i.e.
RBS 2hr after breakfast, 2hr after lunch, and 2hr after dinner)
➢ Screening for complications: Urine albumin/protein, retinal screening by
ophthalmologist, serum creatinine and urea.
➢ Other cardiovascular risk screening: Lipid profile (if not already on statin).

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Discussion

Diabetes Mellitus (DM) was derived from two words;


 Diabetes = “siphon” or “running through” meaning Large urine volume and
 Mellitus = sweet to indicate Glucose in urine.
Diabetes is defined by the WHO as a metabolic disorder characterized by
chronic hyperglycemia associated with disturbances of carbohydrate, fat and
protein metabolism resulting from defects in insulin secretion, insulin action
(Insulin resistance), or both.
DM refers to a heterogenous group of common metabolic disorders that share
the phenotype of hyperglycemia.
Several distinct types of DM are caused by a complex interaction of genetics
and environmental factors.
Depending on the etiology of the DM, factors contributing to hyperglycemia
include Reduced Insulin Secretion, Decreased Glucose Utilization, and
Increased Glucose Production.
Diabetes is the leading cause of cardiovascular disease, CKD (ESRD), visual
loss and non-traumatic amputations worldwide.

Etiologic classification of diabetes mellitus

The classification of diabetes includes four clinical classes


1. Type I diabetes → results from beta cell destruction, leading to absolute insulin
deficiency (complete or near-total insulin deficiency).
A. Immune-mediated
B. Idiopathic
2. Type II diabetes
➢ It is a heterogeneous group of disorders characterized by variable degrees of
insulin resistance, impaired insulin secretion, and increased glucose production.
➢ May range from predominantly insulin resistance with relative insulin deficiency
to a predominantly insulin secretary defect with insulin resistance
3. Gestational diabetes mellitus (GDM) → diabetes diagnosed during pregnancy in
previously non-diabetic woman
4. Other specific types of diabetes
➢ Chromosomal abnormalities (from MODY 1 to MODY 6, MODY = Maturity
onset diabetes of the young /in youth/)
 MODY is a subtype of DM characterized by autosomal dominant
inheritance, early onset of hyperglycemia (Usually <25 years), and
impairment in insulin secretion
➢ Genetic defects in insulin action
➢ Diseases of the exocrine pancreas (Pancreatitis, Trauma/pancreatectomy,
Neoplasia, Cystic fibrosis, Hemochromatosis….)
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➢ Endocrinopathies (Hyperthyroidism, Acromegaly, Cushing's


syndrome,Glucagonoma, Somatostatinoma, Pheochromocytoma,
Aldosteronoma…)
➢ Drug or chemical induced (Glucocorticoids, Thyroid hormone, Thiazides,
Pentamidine, Nicotinic acid, Beta-adrenergic agonists, Alpha interferon…)
➢ Infections (Congenital rubella, CMV…)
➢ Other genetic syndromes sometimes associated with diabetes (Down syndrome,
Klinefelter syndrome, Turner syndrome, Porphyria, Friederich's ataxia….)
➢ MRDM (Malnutrition related DM)
➢ Others

The clinical course and treatment of the different types of diabetes are
different; hence, classification of the type of diabetes is very important to
determine therapy.
The traditional thinking that type II diabetes as the disease of adults and type
I diabetes as the disease of children is not accurate as both diseases can
occur in both age groups. So, age is not a criterion in the classification
system.
The terms insulin-dependent diabetes mellitus (IDDM) and non-insulin-
dependent diabetes mellitus (NIDDM) from previous classifications are obsolete
nowadays.
Since many individuals with type II DM eventually require insulin treatment for
control of glycemia, the use of the term NIDDM generated considerable
confusion.

SCREENING FOR PREDIABETES AND TYPE 2 DM

For those with no symptoms, then screening should be done if they have
one or more of the following indications

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* First degree relatives include: parents, siblings, and offspring (Children)


**In women with GDM, screen for DM 4-6 weeks after delivery with OGTT,
if not possible, do FBG at 6 weeks, based on results, treat accordingly, if
normal, follow every 3 years.

Suggestive clues to Differentiate Type I DM from Type II DM*


Type I DM Type II DM
Common in young age (usually < 30) Common in middle aged and elderly
Normal BMI or lean body mass > 80 % of pts are obese, but elderly may
Usually No immediate family hx be lean
Short duration of symptoms (days to weeks) Usually have +ve family hx
and present with poly symptoms Asymptomatic or present with complication
Can present with DKA (skin infections, pruritis, vulvovaginitis,
Management is based on Insulin only vascular and avascular cxn) and Symptoms
GDM is rare in Type I DM may persist for months or years (i.e. chronic
Associated with other auto immune disease cxn are cmn)
(like hashimoto’s thyroiditis, autoimmune Can present with HHS
hemolytic anemia, pernicious anemia, coeliac Oral hypoglycemic drugs are mainstay of
disease, vitiligo) treatment (unless insulin indicated)
destruction of the pancreatic beta cells and GDM is common in Type II DM
insulin deficiency. Associated with metabolic syndrome (DM,
HTN, Dyslipidemia, Abdominal obesity)
Impaired Insulin Secretion and Insulin
Resistance are central to the development of
Type II DM. 608
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*no clear-cut boundary for Type I & II DM clinically.

Table. Current ADA diagnostic criteria for diabetes mellitus


Diagnostic test Normal Pre-diabetes Diabetes Remarks
Fasting blood 75 to < 100 100-125mg/dl >126 At least 2 tests needed*
glucose (FBS) 
mg/dL mg/dl
Hemoglobin A1C 4.0 – 5.6% 5.7-6.4% > 6.5% At least 2 tests needed*
(HbA1C) #

02-hour plasma < 140 mg/dl 140-199mg/dl >200mg/dl At least 2 tests needed
glucose tolerance
test (OGTT)
Random blood >200mg/dl DM diagnosed Only if RBS
glucose (RBS) >200mg/dl is accompanied
- - by Classic Symptoms of DM
(Polyuria, Polydipsia, Weight
Loss)
1 mmol/l = 18 mg/dl (e.g >126 mg/dl means > 7.0 mmol/l)
* If both fasting blood sugar and hemoglobin A1C are done initially and both are in the diabetic
range, repeat test is not necessary for the diagnosis.
#
If there is significant discrepancy between HbA1C and blood glucose measurements, use the
blood glucose level. HbA1C Does not matter when the test is taken (before or after meals)

Fasting is defined as no caloric intake for at least 8 hours, Can drink pure water. FBS 101-125
mg/dl is Impaired Fasting Blood Glucose. Repeat test in 1 Year. Advise on Healthy Life-Style
counselling.

OGTT test should be performed (as described by the WHO), using a glucose load containing the
equivalent of 75-gram anhydrous glucose dissolved in water. Then measure glucose level after 2
hrs of taking 75-gram glucose (in our set up we use 9 vials of D40, since 1vial of D40 is 8gram,
which means 8 x 9 = 72gram)

Some use the term "increased risk for diabetes" (ADA) or "intermediate hyperglycemia" (WHO)
rather than "prediabetes."

Prediabetes patients are at Greater Risk of progressing to Type II Diabetes and have an
increased risk of Cardiovascular Disease.

Insulin secretion and action

Glucose is the key regulator of insulin secretion by the pancreatic beta cell,
although amino acids, ketones, various nutrients, gastrointestinal peptides, and
neurotransmitters also influence insulin secretion.
Insulin is the most important regulator of this Metabolic Equilibrium, but neural
input, metabolic signals, and other hormones (e.g., glucagon) result in
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In the Fasting State


low insulin levels Increase Glucose Production by Promoting Hepatic
Gluconeogenesis and Glycogenolysis and Reduce Glucose Uptake In Insulin-
Sensitive Tissues (Skeletal Muscle and Fat), Thereby promoting mobilization of
Stored Precursors such as Amino Acids and Free Fatty Acids (Lipolysis).
Glucagon, secreted by Pancreatic Alpha Cells when blood glucose or insulin
levels are low, Stimulates Glycogenolysis and Gluconeogenesis by the Liver
and Renal Medulla.

Postprandially

the glucose load elicits a rise in insulin and fall in glucagon, leading to a
reversal of these processes.
Insulin, An Anabolic Hormone, Promotes the Storage of Carbohydrate and Fat
and Protein Synthesis.
The major portion of Postprandial Glucose is utilized by Skeletal Muscle, an
effect of insulin-stimulated glucose uptake.
Other tissues, most notably the Brain, utilize glucose in an insulin-independent
fashion.

Pathophysiology

Type I DM
Type 1 DM is the result of interactions of Genetic, Environmental, and
Immunologic Factors that ultimately lead to the destruction of the pancreatic
beta cells and insulin deficiency.
Type 1 DM results from Autoimmune Beta Cell Destruction, and most, but not
all, individuals have evidence of Islet-directed Autoimmunity.
Individuals with a Genetic Susceptibility have normal beta cell mass at birth but
begin to lose beta cells secondary to autoimmune destruction that occurs over
months to years.
This autoimmune process is thought to be triggered by an Infectious or
Environmental Stimulus and to be sustained by a Beta Cell–specific Molecule.
Features of diabetes do not become evident until a majority of beta cells are
destroyed (70 - 80%).
After the initial clinical presentation of type 1 DM, a "honeymoon" phase may
ensue in the first 1 or 2 years after the onset of diabetes.
During which time Glycemic control is achieved with Modest Doses of Insulin
or, rarely, Insulin is Not Needed.
However, this fleeting phase of endogenous insulin production from residual
beta cells disappears as the autoimmune process destroys remaining beta
cells, and the individual becomes insulin deficient.
Some individuals with long-standing type 1 diabetes produce a small amount of
insulin (As reflected by C-peptide production)
And some individuals have insulin-positive cells in the pancreas at autopsy.
Islet Cell Autoantibodies (ICAs) are present in the majority of individuals
(>85%) diagnosed with New-onset type 1 DM.
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Type II DM
Type 2 DM is characterized by Impaired Insulin Secretion, Insulin Resistance,
Excessive Hepatic Glucose Production, and Abnormal Fat Metabolism. Insulin
Resistance and Abnormal Insulin Secretion are central to the development of
Type II DM.
Although the primary defect is controversial, most studies support the view that
Insulin Resistance precedes an Insulin Secretory Defect but that diabetes
develops only when insulin secretion becomes inadequate.
In the early stages of the disorder, glucose tolerance remains near-normal,
despite insulin resistance, because the pancreatic beta cells compensate by
increasing insulin output
In Asian, African, and Latin American), DM that is Ketosis Prone (Often
Obese) or Ketosis-Resistant (Often Lean) is commonly seen.
The disease is polygenic and multifactorial, since in addition to Genetic
Susceptibility, Environmental Factors (Such as Obesity, Nutrition, and Physical
Activity) modulate the phenotype.
Even though, HLA gene Abnormality is speculated in type I DM, the genes
that predispose to type 2 DM are incompletely identified. Genetic
Polymorphisms associated with type 2 diabetes have also been found

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Management of DM

Principle of management

Medical Nutrition Therapy (MNT)


Pharmacologic treatment with insulin or oral hypoglycemic drugs
Diabetics education about
 Diet
▪ When they feel hypoglycemia, they have to take table sugar or candy
(they should have candy in their pocket)
▪ Avoid alcohol; which expose to comorbidities like HTN and patient
may miss his/her drug because of alcohol intoxication
▪ Take mixed food; variation between breakfast and dinner if possible
▪ Take vegetable
▪ Avoid refined food since they have high sugar content
▪ Avoid raw meat and fat intake
 DM natural history
 Type and Route of administration of Insulin.
▪ In our setup, patients differentiate regular insulin and NPH based on
color. (regular insulin = ውሃው፣ ውሃ የሚመስለው and NPH = ወተቱ ፣
ወተት መልኩ)

Administration
▪ Morning → periumbilical
▪ Evening → extremities
• This variation is because of exercise increase insulin absorption
(extremities involved in daytime activity)
 storage of insulin
 Self-blood glucose monitoring (SBGM)
 Sign and symptoms of hypoglycemia and hyperglycemia
 Stop smoking and Moderation of alcohol intake
 Exercise
 Foot care
Screening for micro and macro vascular complications
Treatment of infections (e.g. UTI, Pneumonia, vulvovaginitis/candidiasis/)
Follow up

Non pharmacologic treatment for both Type I and Type II DM


A. Medical Nutrition Therapy (MNT): general guidance
Principles of nutritional therapy
Focus on supporting the patient on choosing healthy eating behaviors.
Consider the literacy of the individual, access to food, and willingness.
Try to maintain the pleasure of eating as much as possible
Respect and address the individual preferences, cultural, and religious choices.
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Be practical
Limit food choices when only supported by scientific evidences
Help overweight and obese individuals to decrease body weight
Help attain individualized glycemic, blood pressure, and lipid goals.

General advice
Avoid refined sugars: soft drinks with sugar, or adding sugar/honey to
teas/other drinks.
Carbohydrate
 Reduce overall carbohydrate intake
 Carbohydrate sources high in fiber and minimally processed are preferred:
whole grains, non-starchy vegetables, fruits, and dairy products Be
encouraged to have complex carbohydrates
Fat
 Reduce saturated fat (animal fat) intake: butter, ghee, fatty cuts of meat,
cheese.
 Reduce Trans-fat (hydrogenated oil): solidified vegetable oils
 Mono-saturated and polyunsaturated vegetable oils are preferred
Protein
 Should be left to the individual choice.
 When there is CKD, reduction (not stopping) protein intake.
Sweetened beverages
 Individuals who have had the habit sugar added beverages, taking low-
calorie or nonnutritive- beverages can serve as short-term transition.
However, they should be encouraged to replace with water intake.

B. Exercise
Regular moderate-intensity aerobic physical activity: for at least 30 minutes at
least 5 days a week (at least 150 min/week)
Encourage resistance training 3 times per week.

C. Weight management
For obese and overweight individuals
 Eating plans (focusing on reduction of overall carbohydrate intake) and
exercise
D. Stop smoking
E. Moderation of alcohol intake
A maximum 1 drink for women and 2 drinks for men.
- One drink is roughly equivalent to a bottle of beer, a glass of wine, or a
unit of spirit.
F. Self-blood glucose monitoring (SBGM)
G. Screening for micro and macro vascular complications

Pharmacologic treatment → management of blood sugar 613


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Target blood glucose


➢ Target should be individualized.
➢ In young patients with recent diagnosis, without significant chronic
complications, tight glycemic control should be encouraged.
➢ Individuals for whom less stringent (HbA1C < 8 to 8.5%) should be considered
 History of severe hypoglycemia
 The elderly and those limited life expectancy
 Established cardiovascular disease
 Advanced microvascular disease e.g. advanced chronic kidney disease
 Significant comorbid conditions e.g. liver disease, malignancy
 Long duration of diabetes

Target in most non-pregnant adults without significant comorbidities:20

Table; Glycemic targets for non-pregnant adults without significant comorbidities


TARGET Remark
FBS 100 -130mg/dl In young, highly motivated, well supported patients
HbA1C < 7.5% a HA1C target <6.5% and FBS of 80-130mg/dl can
be aimed, if it can be achieved without causing
recurrent hypoglycemia.
Post meal < 180mg/dl Done 1-2hr from the beginning of meal
glucose level

Treatment of Type - I DM

Pharmacologic
❖ Insulin is the main stay of treatment in type I diabetes

Table; properties of insulin preparations


PREPARATIONS ONSET (hr) PEAK (hr) DURATION (hr)
Short acting Regular 0.5-1 2-4 6-8
Lispro
Aspart 0.25 1 3-4
Glulisine
Intermediate NPH
acting a.k.a Isophane 1-2 6-8 12-16
NPH stands for Neutral
Protamine Hagedorn

20
Reference from 2021 STG for General Hospitals in Ethiopia. According to Harrison 20th edition, the target
range of glycemic control is RBS < 180mg/dl, FBS = 80 - 130mg/dl, HbA1c < 7.0 %. As recommended by the
ADA; goals should be individualized for each patient with a different goal for different patients. HbA1c is primary
goal.
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Long acting Glargine 1 None 11-24


Detemir 1 3-9 6-23

❖ Insulin regimen in type I Diabetes Mellitus:


1)Conventional insulin therapy
➢ It encompasses simpler non-physiologic insulin regimens.
➢ These include single daily injections, or two injections per day (including a
combination short-acting and -NPH insulin)
➢ The conventional insulin regimen uses a mixture of regular insulin and NPH
administered before breakfast and before the evening meal
➢ 2/3rd of the total daily dose is injected in the morning and 1/3rd in the evening.
➢ Approximately 2/3rd of each injection comprises NPH and 1/3rd is regular insulin

2) Intensive insulin therapy


➢ Intensive insulin therapy is a regimen trying to simulate the normal physiology
with basal doses (consisting of intermediate or long acting insulin) given either
once or twice daily and bolus dose (consisting of regular or rapid acting
insulin) given with each meal with the bolus dose adjusted based on
anticipated carbohydrate intake.
➢ It describes treatment with >3 injections/day or continuous insulin infusion
➢ It requires frequent monitoring of blood sugar: fasting, before lunch, before
dinner & before bed.
➢ It also requires the following
 Counting and recording carbohydrates.
 Adjusting insulin doses in response to given glucose patterns.
 Coordinating diet, exercise, and insulin therapy.
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 Responding appropriately to hypoglycemia

3) Designing insulin therapy


➢ Total insulin dose per day Initiation, 0.2 to 0.4 units/kg/day
➢ Maintenance → highly variable roughly 0.6 to 0.7 units/kg/day
➢ For doses above 20units divided in to two (about 2/3 in the morning and 1/3
in the evening)
➢ Regimen options-with NPH and regular insulin

❖ Preferred regimen: Intensive Insulin therapy (i.e. NPH with


premeal regular insulin)
➢ NPH before breakfast and at bed time PLUS
➢ Regular Insulin three times daily injection: before breakfast, lunch, and dinner

❖ Other options: If the patient work, routines, social circumstances, and support
do not allow the patient to do the preferred regimen
➢ Mixed NPH and regular insulin → 70/30 (70% NPH & 30% regular)
➢ NPH with pre-breakfast and pre-dinner regular insulin
➢ Twice daily NPH injections only: Before breakfast and before bedtime

Intensive treatment reduced the risks of retinopathy, nephropathy, and


neuropathy by 35% to 90% compared with conventional treatment and was
found most effective when began early before complications were detectable.
Studies have shown that instituting intensive therapy early on in the disease
had benefits that extended even after intensive therapy has been discontinued.
This is called a " metabolic memory". Hence intensive treatment should be
started as soon as is safely possible after onset of Type 1 DM and maintained
thereafter.

HONEYMOON PERIOD

After several weeks of exogenous insulin treatment & excellent metabolic


control has been established
Dependency on exogenous insulin decreases or ceases entirely for weeks to
months
Temporary remission (honeymoon phase) is marked by an increase in serum
C-peptide levels which indicates an increase in endogenous insulin secretion
Within 5 years after diagnosis of childhood type 1 diabetes mellitus, C-peptide
virtually disappears from the serum.

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COMPLICATIONS OF INSULIN THERAPY

Hypoglycemia
Weight Gain
 Possible causes:
▪ Improvement in glycemic control
▪ Increased food intake to treat or prevent hypoglycemia.
▪ Insulin itself may stimulate appetite.
Worsening Retinopathy
Insulin Allergy
Lipodystrophy (hypertrophy /atrophy)
 Repeated single site injection
 Easily accessible sites commonly affected
 Forms lump at injection site
 Less painful so patient tends to choose it for injection.
 Insulin absorption from this site is not reliable so patients advised to
rotate injection sites and to avoid the lipodystrophy site
Dawn Phenomenon and Somogyi Phenomenon
 There are several reasons that blood glucose levels increase in the early
morning hours before breakfast.
 The most common is a simple decline in insulin levels.
 This usually results in routinely elevated morning glucose.
 The dawn phenomenon
▪ Is thought to be mainly caused by overnight growth hormone
secretion and increased insulin clearance.
▪ It is a normal physiologic process seen in most adolescents without
diabetes, who compensate with more insulin output. A child with
T1DM cannot compensate.
▪ The dawn phenomenon is usually recurrent and modestly elevates
most morning glucose levels.
 Somogyi phenomenon
▪ Rarely, high morning glucose is caused by the Somogyi phenomenon,
a theoretical rebound from late-night or early-morning hypoglycemia,
thought to be from an exaggerated counter-regulatory response.
▪ It is unlikely to be a common cause, in that most children remain
hypoglycemic (do not rebound) once night time glucose levels decline.
▪ Check BG @ 2-3 am for a couple of days to clarify ambiguously
elevated morning glucose levels.

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PRACTICAL TIPS ABOUT INSULIN THERAPY

➢ Insulin storage:
 Store insulin preferably @ 2-8 0c, in a fridge (do not freeze)
 In separate container
 Not in a fridge door
 Check expiry date
 If fridge not available, can be kept in a cool, dark, well ventilated
place (usually wet sand bag→ Locally prepared from Sand and water
put on water highland)
 Note: a vial in use is stable @ 25oc for 6 wks, @ 37oc for 4 wks
➢ To mix cloudy insulin, roll between hands
➢ Transporting insulin – advise pts to:
 Carry adequate supply
 Valid prescription
 Carry insulin in a hand bag
 Avoid keeping insulin in direct contact with ice pack
 Avoid direct contact with sunlight
➢ Mixing Insulins:
 Inject equivalent volume of air in to the vials before drawing insulin
 Draw soluble insulin first, then the intermediate
 Avoid contaminating short acting insulin with the intermediate acting
one
 Should be injected within 5 minutes of mixing
 If there is difficulty mixing, better inject separately
 Do not mix insulin analogues
➢ Injection sites: Abdomen, thighs, buttock, arms
 Fast absorption from abdomen, slow from thigh
 Preferred sites for soluble insulin – abdomen
 For longer acting insulin - the thighs
 Injecting on exercising muscle may lead to faster insulin absorption
and can predispose to hypoglycemia hence avoid it
 Use one area for a particular time of the day
 Rotate injection areas
 Avoid injecting into lipodystrophy site
 Rate of absorption- abdomen> arm>leg and buttock
➢ Injection techniques:
 No need of cleaning with alcohol, if need be, clean with water
 Make a skin fold - inject @ 900 in most; with long needles or very
thin pt.--@ 450
 Slight bleeding is ok
 Never give intermediate acting insulin IV
➢ Before changing insulin dosages Check
 Insulin storage
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 Patient compliance
 Injection techniques (re-suspension, dosages, mixing procedures, &
injecting)
 Injection sites
 Eating plans, exercise, BG monitoring compliance
 Other factors e.g. stress, infection, other illnesses
 N.B. If food is not readily available, be cautious in dose escalation

Treatment of Type - II DM

Blood glucose lowering medicines

Initial treatment:

Metformin does not cause weight gain or hypoglycemia and is the

recommended initial treatment for people who do not achieve the

desired glycemic control with diet and physical activity.

✓ Start 500mg PO at bedtime. Increase the dosage gradually

according to the diabetes protocol.

A second-generation sulfonylurea like glibenclamide or glimepiride can

be used as initial (first-line) treatment when metformin is

contraindicated or not tolerated.

Sulfonylureas may cause weight gain and hypoglycemia.

Insulin therapy can be considered when there are symptoms of diabetes

or the HbA1c level is greater than 9% or FBS > 300mg/dl

Intensification of treatment when metformin alone fails to control

glycaemia:

✓ Consider adding glibenclamide 5mg or glimepiride 2mg

Intensification of treatment when metformin and sulfonylurea fail to

control glycaemia:
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✓ Refer for insulin treatment or add human insulin to oral

medications

Remember:

✓ There is a risk of hypoglycemia with sulfonylurea and insulin use if

you delay your mealtime or eat less than usual, or the medicine is

too much.

✓ Medications must be supported by healthy eating and regular

physical activity. Quitting smoking and stopping harmful use of

alcohol are especially important.

Management of Type 2 DM with Insulin

✓ If goal not achieved with lifestyle changes and oral agents:

▪ Stop glibenclamide/glimepiride and add NPH 10 iu bedtime

and escalate insulin dose by 2 iu every 3 days by checking FBG

▪ If a dose of >20 iu is needed at bedtime, split into morning

and evening dose (2/3rd am and 1/3rd pm).

▪ Continue Metformin with same dose

▪ Monitor for hypoglycemia.

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Notes on the Type 2 DM Management flow chart:

Glibenclamide is mostly escalated from 5 mg /d → 5 mg BID → 10mg

(am)/5(pm) → 10 mg BID

When initiating Glimepiride or glibenclamide or insulin advise patients

on symptoms of hypoglycemia such as sweating, hunger, fatigue,

tremor or altered mentation.

✓ If any of these occurs check blood glucose at the time to confirm

low blood glucose or treat for hypoglycemia

✓ decrease the dose of glibenclamide or glimepiride and escalate

slowly (as in 1 mg Glimepiride or 2.5 mg Glibenclamide).

✓ If on insulin, reduce dose by 4 iu and escalate by 2 IU every week.

Glimepiride is preferred over glibenclamide but is more expensive.

Figure; Follow up of DM

First line: Metformin


✓ Initial dose 500mg to 1000mg/day daily or in two divided doses with meals.
✓ Titrate dose every two weeks depending on the FBS
✓ Maximum dose = 2000mg/day (1000mg BID)
• Metformin is contraindicated in patients with advanced CKD (eGFR
<30ml/min), advanced CLD, and hypoxia.
Alternative to Metformin
✓ If Metformin is contraindicated a sulfonylurea can be started
✓ Basal insulin can also be started as an alternative (see for indications for
starting insulin in type 2 diabetes below)

Add on to Metformin: If glycemic target is not achieved by metformin alone after


three months, add either of the following.
✓ Sulfonylureas: Glibenclamide, Glimepiride, Gliclazide OR
✓ Basal insulin
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Initiating two oral agents at diagnosis


✓ Patients with severe hyperglycemia at presentation (HbA1C >10% or FBS >250
mg/dl or RBS consistently >300 mg/d) and prefer oral agents than insulin,
need to be started on a combination of metformin and sulfonylurea.

Sulfonylureas
✓ Glibenclamide (Glyburide)
• Starting dose is 2.5-5mg/day, 30 minutes before breakfast.
• Titrate dose slowly to maximum of 20mg/day
• When 10mg/day is needed, divide the total dose into two, with the larger
dose in the morning.
• Avoid in the elderly and patients with renal impairment.
✓ Glimepiride
• Starting dose is 1-2 mg/day, 30 minutes before breakfast.
• Titrate dose slowly to maximum of 8mg/day
✓ Gliclazide, modified release
• Starting dose 30mg/day
• Titrate the dose slowly to a maximum dose 120mg/day

The major side effect of sulfonylureas is hypoglycemia.


• Individuals should be educated about the risk, manifestations, prevention
and treatment of hypoglycemia.
• Sulfonylureas should be avoided or given at lower doses in individuals at
high risk of hypoglycemia (e.g. the elderly, with significant comorbidities,
history of hypoglycemia)

Insulin therapy in type II diabetes


✓ Indications for insulin therapy
• Failure to control blood glucose with oral medicines
• Temporary use for major stress, e.g. surgery, medical illness
• Severe kidney or liver failure
• Pregnancy
• In patients difficult to distinguish type 1 from type 2 diabetes
• Ketonuria
• Unexplained weight loss accompanied by poorly controlled blood sugar
• Initial therapy for a patient presenting with very high blood sugar
o HbA1C >10% or FBS >250 mg/dl or RBS consistently >300 mg/d

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INSULIN INITIATION REGIMENS


➢ Basal insulin
 If started on as an add on therapy to Metformin
▪ Starting dose = NPH 10 units at bed time

▪ A higher dose might be started for higher blood glucose

▪ Dose increment 2-4 units in 3-7 days with self-monitoring of

blood sugar until fasting glucose < 130 mg/dl

▪ if the bed time insulin is ≥24 units, split 2/3 in AM + 1/3 in PM

 If started as a replacement for oral agents


▪ Starting dose = NPH 15 -20 units at bed time

▪ A higher dose might be started for higher blood glucose

▪ For doses above 20 units divided in to two (about 2/3 in the

morning and 1/3 in the evening)

▪ Dose increment 2- 4 units in 3-7 days with self-monitoring

➢ Intensive insulin therapy/Multiple Daily Injections (MDI)


 Intensive insulin therapy is when regular insulin added before meal
(i.e. Adding RI Before breakfast, before lunch and before dinner in
addition to standing dose (daily or BID) of basal insulin (NPH)
 Indications to start
▪ If FBS is well controlled but HbA1c is above target
▪ If HbA1c is above target despite increasing basal insulin to
>0.5 unit/Kg/day
 Dosing prandial regular insulin
▪ Starting dose of prandial insulin:
o 0.3-0.5 units/kg total
o if insulin is ≥24 units, split 2/3 in AM + 1/3 in PM
o Usually Regular insulin 4 units
▪ Preferred time: before the largest meal of the day
▪ Dose increment 1-2 units in 2-3 days with self-monitoring
of the next pre-meal blood glucose
➢ Pre-mixed insulin
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 10 units bid OR 0.3-0.5 units/kg divided in 2/3 in AM + 1/3 in


PM (Common trend in Ethiopia is mixed Insulin, 20 AM and 10
PM)
 Most difficult to titrate

PRACTICAL ASPECTS OF INSULIN INITIATION

➢ Start low and titrate up


➢ Basal insulin therapy:
 Begin at 0.1 to 0.2 U/kg of body weight = ~ 10 units at bed time
and titrate to achieve target fasting, if the bed time insulin is ≥24
units, split 2/3 in AM + 1/3 in PM
 Continue metformin therapy
 Continue sulfonylureas during the day if started with bed time
NPH
➢ If patients have post prandial high blood glucose (>180 mg/dl):
 Continue Metformin and DPP-IV inhibitors (e.g. Saxagliptin,
Vildagliptin) if possible
 Stop sulfonylureas
 Calculate 0.3 to 0.5 u of insulin/kg body weight
 Premixed insulin twice daily: divide as 2/3 in AM and 1/3 at
supper and titrate
 Patients can also mix NPH insulin and regular insulin in 2/3 and
1/3 proportions respectively
 Have patients work closely with diabetes nurse educator or
frequent follow ups in the office for adjustment.
➢ Insulin therapy requires a structured program employing active insulin
dose titration that encompasses:
 injection technique, including rotating injection sites and avoiding
repeated injections at the same point within site
 self-monitoring
 dose titration to target levels
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 management of hypoglycaemia

Other oral diabetic medications for the care of patients with type
II DM.

Sulfonylureas or basal insulin to be the preferred add-on therapies next to


metformin. This is mainly based on cost related factors.
✓ For patients who can afford to buy or get access to these medications,
decision on which agent to add to Metformin, combine with Metformin from the
beginning or sometimes start an initial treatment should be individualized based
on the following factors.
• The need for weight loss
• Risk of hypoglycemia in the patient
• the presence of cardiovascular disease
• The presence of CKD.

Table; available medications in Ethiopia


Class of Available drugs and in Ethiopia Clinical sates in which the drug is most
medication beneficial
SGLT2 Dapagliflozin, 5 or 10mg, po, daily Heart failure
inhibitors Early stages of CKD
(Sodium Compelling need to decrease the risk
glucose hypoglycemia
transporter Compelling need to decrease weight loss
or reduce weight
-2
Need to improve glycemic control
inhibitors) Additional benefit of BP lowering
Avoid in advanced CKD
DPP4- Saxagliptin, 2.5 - 5mg, po, daily Compelling need to decrease the risk
inhibitors Vildagliptin, 50mg, po, daily or hypoglycemia
(Dipeptidyl BID Need for intensification of glycemic control
peptidase - Weight neutral (no increment or significant
4 Each of these drugs are also decrement)
available as FDC with Metformin Dose reduction need in patients with CKD.
inhibitors)
500mg or 1000mg)

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Management of other cardiovascular (CV)risks


1) Cardiovascular risk calculation
All patients 10-year cardiovascular risk factor needs to be calculated
2) Blood pressure management (See section on hypertension from chapter 1; click
here → Hypertension (የደም ግፊት) and HHD )
➢ Target blood pressure: <130/80mmHg
➢ First line if there is proteinuria: ACE inhibitors or ARBs
➢ First line if no proteinuria: CCB, thiazide diuretics or ACE inhibitors or ARBs.
➢ Preferred two drug combinations for patients with proteinuria
 ACE inhibitors/ARB + CCB
 ACE inhibitors/ARB + Thiazide diuretics
➢ Preferred combination for patients with no proteinuria
 CCB + ACE inhibitors/ARB
 CCB + Thiazide diuretics
➢ Preferred 3 drug combinations
 ACE inhibitors/ARB + CCB + Thiazide diuretic

3) Lipid lowering therapy


Indications
 Age above 40 without additional CV risk
▪ Start moderate intensity statin
▪ Make it high intensity if there is additional CV risk
 All ages with a history of cardiovascular risk
▪ Start high intensity statin
 Age 20-39 years with one or more CV risk factor

4) Antiplatelet therapy
➢ Aspirin (81-162mg/day)
 It is only indicated for patients who have CV disease (coronary artery
disease, ischemic stroke or peripheral arterial disease)
 Give ASA 75-100mg PO (usually 81mg, PO, daily) for Primary
prevention
▪ Males > 50 yrs, Females > 60 yrs + 1 CV risk factor
▪ DM patients with increased cardiovascular risk after excluding
risk of bleeding

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Follow up on Chronic OPD (RECOMMENDED


SCHEDULES FOR ONGOING MEDICAL CAREOF
DIABETES)
Glycemic Control → The ABCs
 A → HbA1C is the blood glucose check “with a memory.” It allows one
to determine average blood glucose control over the past 2 to 3
months. The ADA recommends an A1C below 7.
 B→ BP, The ADA recommends a BP < 130/80.
 C → is for cholesterol
Escalate or deescalate medication dose based on target glucose level
Screen and treat complication based on the above table schedule
Look at follow up investigations above (investigation section)
Once good glycemic control has been attained, Follow patients every
3 months*
For those able to afford a glucometer, advise on self-monitoring of
blood glucose (SMBG)
For Type 2 DM patients not on insulin SMBG may only be needed
when changing diet, physical activity or medications and when
HgA1c is abnormal despite a normal FBG if (HgA1c is available) to
check for post prandial hyperglycemia
For patients on insulin, they should measure fasting and post
prandial measurements as frequently as possible
If HgA1C test is available, check it 2 -4 x/year
Self-Monitoring of Blood Glucose (≥3/day in those on multiple daily
injection of insulin with/ without oral antihyperglycemic (OAHA)
medications, individualize for those in good control with OAHA)
DM Management patient education (annual)
Medical Nutritional Therapy (annual)
Eye exam (at Diagnosis for type 2 DM, annual or Q2-3yrs)
Foot exam (by patients daily, by doctor 1-2x/yr)
Microalbuminuria (annual)
BP measurement (Quarterly)
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Lipid profile (annual)


Others: immunization, antiplatelets

*Frequency of follow up may be more frequent if indications are


there such as change in dose, hypoglycemia, recent illness or
development of microvascular or macrovascular complications

Hypertension management in Diabetes

➢ If BP ≥ 140/90 mmHG on multiple occasions start anti-


hypertensive medications
➢ If BP>160/100 start with a combination of antihypertensive
➢ Target blood pressure is <140/90mmHG
➢ Can use hypertensive treatment regimen similar to the general
population for those with no protein on their urine (Refer to
national hypertensive protocol for details)
➢ If there is proteinuria preferably start/add Enalapril or Lisinopril 5
mg/day.
➢ Any one of ACEIs, ARBs, CCBs or Diuretics can be used for those without
cardiovascular disease or albuminuria
➢ ACEIs or ARBs for those with cardiovascular disease or albuminuria
➢ 2 or more drugs are needed in those with BP ≥ 160/100mmHg
➢ Administer one of the drugs at bed time
➢ ACEI and ARBs are contraindicated in pregnancy

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Dyslipidemia management in Diabetes

➢ Check lipid profile at diagnosis, 6 months after treatment initiation


and then yearly in type 2 DM patients
➢ Start atorvastatin 40 mg /d or simvastatin 20mg/d for all diabetic
patients age >40 years of age and LDL 70-190 mg/dl
➢ If ASCVD risk is >20% (Laboratory based) or LDL>190 mg/dl or
there is established ASCVD start Atorvastatin 40 mg/day
➢ Give Statins (Simvastatin,Atorvastatin,Rosuvastatin or Lovastatin) for the
following group Diabetes Patients :
 DM patients age 20 – 39 years with ASCVD risk factors may be
treated with statins and Life style modification- Consult
internist/or Endocrinologist/or cardiologist
 DM Patient age 40 – 75 without ASCVD risk factor – maybe
started with moderate intensity statins
 DM patients with age 50 – 70 years with high ASCVD risk should
receive High intensity statin therapy
 High Intensity Statin Therapy – Lowers LDL by ≥ 50 %
▪ Atorvastatin –40 -80 mg/d
▪ Rosuvastatin – 20 – 40 mg/d
 Moderate Intensity statin Therapy – Lowers LDL by 30 – 40%
▪ Atorvastatin – 10 – 20 mg/d
▪ Rosuvastatin - 5 – 10 mg/d
▪ Simvastatin 20 – 40 mg/d
▪ Lovastatin – 40 mg/d

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10.1. ACUTE COMPLICATIONS


OF DIABETES

10.1.1. DKA and HHS


Clinical features and how to write hx of DKA patient

History
DKA patients usually present with LOC or severe abdominal pain and vomiting
that mimics acute abdomen.

✓ If a known DM patient ask those questions mentioned under Diabetic foot


ulcer
▪ Poly symptoms (3P)
o Poly urea → Write in terms of Day to Night ratio (e.g. poly urea of
8:6 day to night ratio).
☛ The 24-hour urine voided by a healthy adult range from 600
to 2000ml
☛ Polyuria considered when there is consistent elimination of an
abnormally large volume of urine, > 3000ml/24h
o Polydipsia → ask How much litre of water he/she drinks per day
o Polyphagia → less common smx than Polydipsia and Polyuria
▪ Per umbilical abdominal pain that mimic acute abdomen
▪ Vomiting, Nausea, Anorexia, weakness
▪ LOC
▪ Symptoms of infection or other precipitants

Precipitant factors for DKA & HHS → 4I’s


• Infection (30-50%) → pneumonia, UTI, Gastroenteritis, malaria or other AFI,
Seps, meningitis, …
• Inadequate Insulin Rx (20-40%) → due to omissions and non-adherence (in
our set up) or insulin pump failure (in westerns set up)
• Infarction → MI, cerebral infarction (Stroke), mesenteric infarction (intestinal
or mesenteric thrombosis), peripheral infarction, (N.B MI is silent in DM)
• In addition (Others)
o previously undiagnosed and untreated diabetes
o surgery
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o CVA
o SDH
o Acute PE
o Intestinal obstruction
o Acute pancreatitis
o Severe burn, hyper/hypothermia
o Endocrine disorders→ thyrotoxicosis, Cushing sxx, acromegaly
o Drugs→ Steroids, cocaine, olanzapine, lithium, alcohol
o Pregnancy
o psychological stress
o no precipitant factors could be found in up to 20-30% of cases

Complication of DKA
DKA, if not detected and treated early it may end up with complications like;

• Cerebral edema → ranging from LOC up to death


• Aspiration — patients with altered state of consciousness and vomiting are at
increased risk for aspiration
• Pulmonary edema
• Electrolyte and acid base disturbance → like hypokalemia
• Cardiac arrhythmia — Cardiac arrhythmias may be seen with either
hypokalemia or hyperkalemia. In addition, asystole can be caused by
inappropriate administration of IV potassium during treatment of
hypokalemia.
• Venous thrombosis and DVT → may in part be due to a prothrombotic
state associated with DKA
• Pancreatic enzyme elevations

Sample history

Chief compliant

Abdominal pain and vomiting of 03 days duration

HPI

A known DM patient for the past 4 years taking insulin injection 20 units in the
morning and 10 units at night. With alternative injection sites between his upper arms,
thighs and periumbilical area. Stores his insulin in wet sand bag. He was adherent for
his medication with regular follow up every 2 - 3 months in UOG hospital.

Currently presented with severe, crampy, localized, Peri umbilical abdominal pain and
non-blood tingled, non-projectile, non-foul-smelling Vomiting of ingested matter 3 - 4
times per day of 03 days duration, but no change in mentation.
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A week before the onset of these symptoms, he was experiencing polyuria of 6 - 8


times during night and 9 -10 times during daytime with increased feeling of thirst for
which he drinks 3 - 5 liters of water per day but no polyphagia. But he didn’t seek
treatment because he assumes it as it was similar to the symptoms he experienced
during initial diagnosis and planning to tell his doctor during follow up.

➢ Ask those +ve and -ve statements listed on the sample hx of a DM patient
above.
➢ Two weeks before admission, he also experienced dry cough occurring mostly
at night which was exacerbated by deep breathing associated with chest pain
and high grade intermittent fever where he visited a private clinic and he was
given a tablet to be taken 3 times per day for 7 days and another tablet to be
taken once daily for 3 days and he was improved. (pneumonia is precipitant factor for
this patient)
➢ No hx of burning sensation during urination, flank pain or hematuria (UTI as
precipitant)
➢ No hx of diarrhea, nausea or vomiting (gastroenteritis as precipitant)
➢ He is not from malaria endemic area and no travel hx to malaria endemic
area (malaria as precipitant)
➢ No hx chest pain, dyspnea or family hx of sudden cardiac death (MI as precipitant
factor)
➢ No hx of headache, body weakness or head trauma (stroke, SDH as precipitant factor)

Physical examination (pertinent findings)

✓ Assess all pertinent findings listed above for DM pt’

1 GA

✓ ASL→ from abdominal pain


✓ LOC (comma)
✓ Respiratory distress
✓ Fruity breath from Acetone, sweaty and sickly smell

2 Vital signs

✓ Hypotension or OHT → from dehydration


✓ Tachycardia (fast and weak pulse)
✓ Hypothermia
✓ Kussmauls breathing (deep, fast and laboured breathing followed by apnea)

3 HEENT

✓ Dehydration signs (Dry mucous membrane, sunkening of eyeball)

4 LGS

5 RS

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✓ Decreased JVP

7 Abdominal examination

✓ Abdominal tenderness
✓ Reduced skin turgor(dehydration)

8 GUS

9 MSS

10 IS

✓ Dry skin

11. NS

✓ Mental confusion up to coma (lethargy, obtunded) from cerebral edema

N.B Dehydration signs are common in DKA (more common in HHS than DKA)

✓ Sunkening of the eye ball, Dry buccal mucosa


✓ Slow skin turgor in the abdomen
✓ Eagerness to drink
✓ Decreased level of consciousness

DDX of DKA

For poly symptoms refer DDX for DM above

For LOC (coma)

1. HHS
2. Alcoholic ketoacidosis
3. Starvation ketoacidosis
4. Lactic acidosis
5. CKD
6. Drugs → salicyclates, methanol, ethylene glycol
7. For more refer on NS examination /coma/ (click here → 1.4.5 Coma)

IX

1. Blood sugar level → hyperglycaemia (usually >300mg/dl)


2. U/A→ what do you expect from U/A
a. Glucosuria (> 3+)
b. Ketonuria (> 2+) → N.B ketonuria is usually +ve in DKA and poorly
correlates with ketonemia
c. UTI
3. Pregnancy test (Urine HCG) in women of child bearing age
4. CBC → ketonemia, leukocytosis from infection
5. RFT → BUN/creatinine ratio → azotemia
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6. Serum electrolyte → wide Anion gap, hyponatremia/hypokalemia


7. Calculate plasma osmolality → normal value is 300-320 mosmol/kg
𝑮𝒍𝒖𝒄𝒐𝒔𝒆 𝑩𝑼𝑵 𝑬𝒕𝒉𝒂𝒏𝒐𝒍
𝐩𝐥𝐚𝐬𝐦𝐚 𝐨𝐬𝐦𝐨𝐥𝐚𝐥𝐢𝐭𝐲 = 𝟐𝑵𝒂 + + → (+ 𝒊𝒇 𝒑𝒕 𝒊𝒏𝒈𝒆𝒔𝒕 𝒆𝒕𝒉𝒂𝒏𝒐𝒍)
𝟏𝟖 𝟐. 𝟖 𝟑. 𝟕
8. Search for precipitant
a. CXR→ pneumonia
b. Urine culture → UTI
c. Blood film → malaria
d. Echo, ECG, Cardiac markers → MI
e. CT, carotid Doppler → CVA, SDH
9. Other IX for DM→ refer DM

Discussion

Diabetic ketoacidosis (DKA) is a condition in which there is a severe


deficiency of insulin resulting in very high blood glucose.
Fat is broken down as an alternative source of energy with
ketones/ketoacids as a by-product.
This state of severe hyperglycaemia and ketone body production results in
severe metabolic, fluid and electrolyte abnormalities.
DKA often occurs in type 1 diabetes patients but may also occur in type 2
diabetes.
It is characterized by:
o Hyperglycemia (BG>250mg/dl)
o Ketosis (urine ketone ≥ 2+) and
o Acidosis
Hyperglycaemic hyperosmolar state (HHS) is a hyperglycaemic emergency
that occurs in type 2 DM due to relative insulin deficiency and inadequate
fluid intake.
Apart from acidosis the manifestations, risk factors and management of
HHS is similar to DKA
N.B ketone bodies include
☛ Beta hydroxy butrate
☛ Aceto acetate
☛ acetone

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Table; Diagnostic criteria for DKA and HHS

Parameters DKA HHS21


Mild Moderate Severe
Clinical Oriented, Oriented but Kussmaul or Stupor/coma
alert but sleepy, depressed
fatigued arousable, respirations;
Kussmaul sleepy to depressed
respirations; sensorium to coma
RBS (mg/dl) >250 > 600
Arterial PH 7.25 - 7.30 7 - 7.24 <7 >7.30
Serum bicarbonate 15 – 18 10 to <15 <10 > 15
(mEq/l)
Anion gap >10 >12 >12 Variable
(Na+ - (cl + HCO3))
Osmolality (Mosm/kg) Variable >320
Urine ketone Positive Small
Serum ketone Positive Small

Diagnosis of DKA is confirmed:


o Based on clinical symptoms and signs and
o RBS > 250 mg/dl
o Positive Urine ketone (2+ and above)
o Glucosuria

Difference between DKA and HHS

DKA HHS
RBS > 250 mg/dl RBS > 600 mg/dl
Common in type 1 DM Common in type 2 DM
Present with severe abdominal Present with profound
pain, vomiting or LOC dehydration, hypotension,
Strong hx of poly smx’s and tachycardia or LOC
weight loss Weak hx of polyuria or weight
Urine and serum ketone highly loss
rise Urine and serum ketone normal
5% mortality or slightly rise
Have 3 cardinal features 15% mortality
☛ Hyperglycaemia Severe osmotic diuresis, insulin
☛ Acidosis sufficient to suppress lipolysis
☛ ketosis Osmolality > 320
Variable osmolality

21
HHS patients are critical and it is not expected in stable and conscious patients
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Management of DKA

Principles of mgt

➢ ABCD of life
➢ Resuscitation by expanding intravascular volume (fluid replacement therapy)
➢ Potassium replacement therapy
➢ Insulin therapy
➢ Treat complications
➢ Treat precipitating factors
➢ Monitoring

1. Initial evaluation
✓ Vital signs including saturation
✓ Take weight for calculation
✓ Assess dehydration (Pulse volume, buccal
mucosa, capillary refill, sunken eye balls)
✓ Look for signs of cerebral edema (headache, repeated vomiting, and high
blood pressure)
✓ Check level of consciousness (alert, sleepy and comatose)
✓ Mild DKA can be managed in Wards, Moderate and severe DKA needs
ICU Admission
✓ Ensure appropriate life support (Airway, Breathing, Circulation, etc.)
✓ In coma or severe vomiting- insert airway and drain stomach with NG tube

2. Fluid Management

➢ Replace fluids: Individualize fluid needs based on the patient hydration status;
the following is a guide to severely dehydrated patients.
o N.B The fluid deficit in DKA often 3 to 5 liters but in HHS it is up 10 liters
or more
o Initial fluid
✓ 1 L of NS over the first 1 hour.
✓ Reassess for hydration status: if still severely dehydrated, give
another 1000ml NS over the next 01 hour.
o Subsequent fluid
✓ Subsequent management based on vital signs, free water deficit and
urine output
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o If patient is asymptomatic and urine ketone +1, recheck urine


ketone after 1 hr
o If urine ketone becomes negative escalate treatment and follow
patient frequently as outpatient
o If ketone ≥+2 or if symptomatic with ketonuria of +1, give 1st
dose of Regular insulin
✓ Replace fluid deficits gradually over 24-48 hrs (Overall 6 liters for
DKA and 9 liters for HHS)
o Generally, replace 50% of total deficit in 8 hrs, the rest in 16 hr
✓ Depends on the hydration status and urine output of the patient.
✓ On average give about 250 mL/hour (1000ml over 04 hour) in the
first 24 hours or until patient is able to take enough oral fluids.
✓ Reassess the patient hydration status to decide subsequent Iv fluid
needs.

o Changing fluid
✓ Change the NS to DNS (5%DW9D) when plasma glucose reaches
250 mg/dl in DKA and 300mg/dl in HHS. (i.e. If blood glucose drops
below 250mg/dl Change fluid to 5% DW in ½ NS (half of the fluid
NS and half DW)). This will continue until urine is ketone free.
✓ As long as the patient remains acidotic, insulin administration should
never be stopped. if instead drop in the blood sugar need to be
addressed by adding or increasing glucose administration in the IV
fluid;
✓ Maintain the blood glucose between 150 and 250 mg per dL.
o Fluid is used to treat
✓ DHN
✓ Hyperglycaemia (since fluid induce glucosuria)
✓ Metabolic acidosis
o HHS requires more fluid.
o Assess hydration status, BP and urine output frequently.
o In patients with impaired kidney function and cardiac disease more frequent
monitoring must be performed to avoid iatrogenic fluid overload.

3. Administer short-acting insulin

o Don’t start Insulin in the first hour of management! It should be started


after an hour of fluid resuscitation in order to steadily decrease the acidosis
and it increases complication like shock, hypokalemia and cerebral edema
o Regular Insulin
Initial Bolus
✓ 10 units IV Stat (Bolus), (N.B. 10 IU is considering 70 kg
Average adult so, use 0.1 IU/kg bolus) then
Maintenance
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✓ If there is perfuser: 0.1units/kg/hr by continuous IV infusion.


(dilute 50 units regular insulin in 50 ml NS to make 1 Iu=1ml
soln. Run 0.1IU /kg /hour with a syringe per fuser)
o If IV access not available and patient has no altered
mentation) give 0.2 u/kg/hr sc)
✓ If there is no perfuser: 5 units, IV, every 1 hour22. IV regular insulin
should be continued until the acidosis resolves and the patient is
metabolically stable (i.e. until the patient is out of DKA). Then
change to transition phase dose (look at below).
o Goal 23

✓ Reduce serum glucose by 50 to 70 mg/dl in the 2-3 hours


✓ If Blood glucose (BG) does not decrease by 50-70 mg/dL
within 1 hr, increase rate by 50% of the regular insulin
✓ Continue titration as needed
✓ If the drop is faster, reduce the dose by half for continuous
infusion and give the IV insulin every 2 hour. i.e. When BG
<200mg/dL Decrease insulin to 50% of current rate /reduce the
infusion by half/ (from 0.1units/kg/hr to 0.05units/kg/hr)
o More rapid correction of the serum glucose can precipitate the
development of cerebral edema.
✓ Determine RBS every one hr, urine ketone and glucose every 2hr
✓ Postpone insulin Rx if hypertensive or hypokalemic
✓ If blood glucose falls below 250mg/dl shift to 5% D/W (DNS) And
decrease hourly insulin dose by 50%
✓ Don’t Omit Insulin, as far as possible, is the principle

4. Potassium replacement therapy

o All patients with DKA have potassium depletion irrespective of the serum K+
level.
o N.B. total K+ level is low in DKA, but serum K+ level can be normal, high
or low
o Add intravenous KCl in the IV fluids (20-40 meq of KCl in each bag of NS)
N.B. 1 vail of Kcl = 20 meq
✓ If the initial serum K+ is >5.5 mEq/L → monitor
✓ Add 40 meq of Kcl (2vial) in each IV fluid when serum K+ is within
3.3 - 4.5 mEq/L

22
IV administration of regular insulin is usually preferred because it ensures rapid distribution and allows
adjustment of the infusion rate as the patient responds to therapy. DKA can also be treated with SC short-acting
insulin analogues.
23
Acidosis and ketosis resolve more slowly than hyperglycemia. As ketoacidosis improves, β-hydroxybutyrate is
converted to acetoacetate. Ketone body levels may appear to increase if measured by laboratory assays that use
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✓ Add 20 meq of Kcl (1vial) in each IV fluid when serum K+ is within


4.6 - 5.5 mEq/L
✓ If <3 mEq/L after the initial bolus: upto KCl of ≥ 60 mEq/ L may be
necessary.
✓ If the initial serum K+ is <3.3 mEq/L, do not administer insulin
until the K+ is corrected.
✓ If the initial serum K+ is > 5.5 mEq/L, do not supplement KCl
until the level reaches < 5.5.
✓ If lab not available:
o 2 vials of KCL in every bag of fluid once urine output is
adequate (>50 ml/hr)
o delay initiation of K+ replacement until there is a reasonable
urine put (>50 ml/hr)
o The serum potassium should be maintained between 4.0 and 5.0 mmol/l
o If possible, determine K+ level every 6hr
o The maximum recommended rate of intravenous potassium replacement is
usually 0.5 mEq /kg/h. and If hypokalemia persists despite a maximum rate
of potassium replacement, then the rate of insulin infusion can be reduced
(decrease by half dose)

5. Treat complication of DKA mgt


❖ Hypoglycaemia
❖ Hypokalemia
❖ Non cardiogenic pulmonary edema
❖ Cerebral edema → manifest with decreased level of consciousness
(lethargy, obtunded, coma), headache. It is fatal cxn
▪ Click here for details of Cerebral edema Diagnosis and
management → Pediatrics DM and DKA Case Management
✓ Precipitant identification and treatment
o Noncompliance, infection, trauma, infarction.
o Initiate appropriate workup for precipitating event (CBC, S/E, U/A, CXR,
ECG, cultures)

✓ Monitoring (Follow up of response)

o Random Blood sugar q 1 hr


o Urinary ketones q2 hr
o If possible
✓ Electrolytes, primarily Na+ and K+ q6hr for first 24 h.
✓ BUN and creatinine – daily (refer if abnormality persists for 2 days)
Mental status: expect improvement with treatment if DKA or HHS are the
o

o
primary cause. Consider further evaluation if not improving
Input/output, hydration status, vital signs
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Continuation of treatment
o The above treatment should continue until the patient is stable, clinically
acidosis improves, and patient is able to take oral feeding.
o The urine ketone might still be positive, as it usually lags behind the
improvement of acidosis.

Transition
o Once the patient is able to take oral feeding and clinically the acidosis
improved (i.e out of DKA).
✓ Reduce regular insulin: 2-3 units hourly (5 units every 2 hour) or for
continuous infusion by 0.05/kg per hour
✓ Overlap regular insulin infusion with subcutaneous (SC) NPH insulin
for 2-3 hours to avoid rebound hyperglycemia. And this facilitates
transition to an outpatient insulin regimen and reduces length of
hospital stay.24
o In the other way, Because of the short half-life of IV regular
insulin, it is necessary to administer long-acting insulin (NPH)
prior to discontinuation of the insulin infusion (2–3 h before the
infusion is stopped) to avoid a period of insulin deficiency.
o NPH insulin dosing
▪ If previously on insulin: start the pre DKA or pre-HHS
dose
▪ If Insulin naïve: 80% of the 24-hour requirement or 0.5 to
0.8 IU/kg/day /some says 0.5 to 1 IU/kg/day/ (divided in to
basal and bolus)
✓ After 2-3 hr of overlap
o Discontinue Regular insulin infusion
o Continue Sc NPH as morning and evening dose and
o Start sliding scale method of Regular insulin IV dose (correction
dose mgt) → Look at below

N.B.
➢ Management of HHS is similar to the management of DKA but fluid
replacement is usually much higher (up to 8- 10 liters). Potassium replacement
is not usually needed unless indicated by low serum potassium level.

24
It is crucial to continue the insulin infusion until adequate insulin levels are achieved by administering Sc NPH.
Even relatively brief periods of inadequate insulin administration in this transition phase may result in DKA
relapse.
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When do you say patient is out of DKA (Resolution of


DKA)?

❖ Recovery of clinical condition → we use in our set up


☛ Recovery to mental Alertness
☛ Able to take PO feeding
☛ Norma respiration (No kussmauls breathing, desaturation or SOB
☛ If precipitant treated
❖ Blood glucose < 250 mg/dl → we use in our set up
❖ Serum ketone -ve
❖ Serum bicarbonate >18
❖ PH > 7.3 not available in our set up
❖ Anoin gap <12
❖ Osmolarity <320 mosmol/kg

MANAGEMENT OF DIABETES IN A HOSPITALIZED PATIENT

➢ Glycemic goals for hospitalized patients: 140 - 180 mg/dL


➢ The use of “sliding scale,” Regular insulin alone, where no insulin is given
unless the blood glucose is elevated, is inadequate for inpatient glucose
management and should not be used.
➢ Regular insulin dose should include corrective or supplemental insulin based
on the patient’s insulin sensitivity and the blood glucose. For example,
if the patient is thin (and likely insulin-sensitive), a corrective insulin
supplement might be 1 unit for each 50 mg/dL over the glucose target (i.e. >
180mg/dl). If the patient is obese and insulin-resistant, then the insulin
supplement might be 2 units for each 50 mg/dL over the glucose target.
➢ It is critical to individualize the regimen and adjust the basal or “scheduled”
insulin dose frequently, based on the corrective insulin required.

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Correction dose (Sliding scale)


➢ Correction dose will be given when the patient is out of DKA / usually pt
transferred from ED to ward/
➢ Measure RBS every 1 hour then give Regular insulin IV push based on the
following table

Table; Sliding scale


RBS (in Mg/dl) Regular insulin dose (IU), IV route
For thin and insulin- For obese and insulin-
sensitive pt* resistant pt*
≤ 180 – 200 Omit omit
201 – 250 2 2
251 – 300 3 4
301 – 350 4 6
351 – 400 5 8
401 – 450 6 10
451 – 500 7
501 – 550 8
551 – 600 9
>600 (High) 10
* Most experts recommend 1 IU increment for each 50 mg/dl increment from
180
* Minimum threshold of RBS to add insulin varies from setup to setup. For
example, 180, 200 and 250. We recommend to use threshold starting from
200 (i.e. < 200 → omit, 201 – 250 → 1 IU….)
* This table is from Harrison 21st edition.

☛ In addition to RI, continue subcutaneous NPH insulin dosing that is


given at transition phase above.
☛ When RBS is in the target range sliding scale will be omitted. After
sliding scale, follow RBS q 4hr, then QID and consider discharge to
Diabetic clinic with written diabetic education and short appointment
after diabetic education in wards.

Insulin dose during discharge


➢ NPH dose is the same as given at transition phase which can vary based on
RBS control.
➢ For Regular insulin dosage, calculate the total amount of regular insulin given
as correction dose over 24hrs → then give 2/3rd of the total dose in the
morning and 1/3rd in the evening

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➢ Then from the total dose of insulin requirement the content should be mixed
with 2/3rd of NPH and 1/3rd of regular for both morning and night doses via
subcutaneous route
➢ e.g. if total amount of regular insulin given over 24hr as correction dose is 12
IU of regular insulin, and NPH was 24 IU. The total summation (mixed) will
become 36 IU → 2/3rd of 36 IU = 24 IU, 1/3rd of 36 IU = 12 IU, so give 24
IU (16 IU of NPH and 8 IU of RI) in the morning and 12 IU (8 IU NPH and 4
IU RI) in the evening
▪ Some experts prefer the evening dose to be 1:1 ratio of NPH and
regular insulin. For the above example; 6 IU of NPH and 6 IU of RI as
evening dose.
➢ If the patient was on NPH previously with poor control of DM and RI given as
correction dose, then at discharge;
▪ Give 2/3rd of total RI given over 24 hour which will be added in
previous dose. From the 2/3rd of total correction dose 2/3rd will be given
in the morning and 1/3rd in the evening
▪ E.g. if a patient was taking NPH 20 IU in the morning and 10 IU in the
evening. Total dose is 30 IU.
• If he took 14 IU of RI as correction dose over 24 hrs then 2/3rd
of 14 IU is 9 IU
• 2/3rd of 9 IU is 6 IU, which will be added in morning dose
• 1/3rd of 9 IU is 3 IU, which will be approximated to 4 IU for
administration and added in evening dose
• So, at discharge morning dose = 20 IU + 6 IU = 26 IU; evening
dose = 10 IU + 4 IU = 14 IU
• Discharge with short appointment

DKA follow up sheet


Date Time BP PR RR T0 Mentation RBS/hr Urine Urine Insulin input Out put sign
glucose/ ketone dose
2hrs /2hrs (IU, IV)

If possible

➢ Electrolytes, primarily Na+ and K+ q6hr


➢ BUN and creatinine – daily

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Assume you are in a primary hospital where chemistry


machine is not available for electrolyte determination, so
you can order like these

- Secure double IV line


- Resuscitate with 2 – 3 bags of NS over 2hr’s
- Then give Regular insulin 10 IU, IV Followed by 5
IU, IV, Q1hr
- 2 vials of KCL in every bag of fluid once
urine output is adequate (>50 ml/hr)
- Change fluid to DNS if RBS is < 250mg/dl (see
transition period part above)
- Determine RBS Q1hr & Urine ketone Q 2hr’s
- Follow with DKA follow up sheet

➢ N.B for DKA in Type II DM patients


✓ Oral glucose lowering agents should be discontinued upon admission and are
not useful in regulating the plasma glucose in clinical situations where the
insulin requirements and glucose intake are changing rapidly. Moreover, these
oral agents may be dangerous if the patient is fasting (e.g., hypoglycemia with
sulfonylureas)
✓ Once clinically stable, oral glucose-lowering agents may be resumed in
anticipation of discharge.
✓ Ketosis is one of the indications to start insulin alone or in combination with
oral hypoglycemic agents (look at Type II DM mgt above)

10.1.1.1. Fluid Management of DKA in CHF, CKD,


HTN and CLD patients
➢ For 3rd Edition

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10.1.2. Hypoglycaemia

Hypoglycemia is a blood sugar level low enough to cause symptoms and


signs. A value <70mg/dl in diabetes and <55mg/dl in non-diabetic patient
defines hypoglycemia.
Some patients might be symptomatic at levels>70mg/dl and some might not
develop symptoms at level <70mg/dl
It is a clinical syndrome in which low serum (or plasma) glucose concentrations
leads to symptoms of sympathoadrenal activation and neuroglycopenia.
Hypoglycemia occurs in most patients with type 1 diabetes and some type 2
diabetics.
It can cause significant morbidity and may be lethal if not promptly recognized
and managed.
It is a common complication of glucose lowering therapy in diabetes
(Commonly from Sulfonylureas and insulin).
The elderly, patients with impaired kidney function and multiple comorbidities
are at higher risk of hypoglycemia.
Pseudohypoglycemia → the person with diabetes reports typical smx’s of
hypoglycemia but RBS >70 mg/dl. These patients commonly have chronically
high blood sugar.

Whipple’s triad → useful for the Dx of hypoglycemia in general.


1. Symptoms and signs of hypoglycemia
2. Documented low blood glucose level (<70mg/dl in diabetes and
<55mg/dl in non-diabetic patient) measured with a precise method (not a
glucometer)
3. Relief of symptoms up on correction of the low blood glucose.

Hypoglycemia unawareness-absent symptoms in spite of having


low blood glucose levels (usually related to autonomic diabetic
neuropathy)

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Clinical features

The symptoms of hypoglycemia are classified in to autonomic and


neuroglycopenic

Autonomic (You are hungry) Neuroglycopenic (brain glucose


Adrenergic Cholinergic deprivation) → Your nerves are hungry
Palpitation and Hunger Difficulty concentrating
tachycardia Sweating Difficulty in speaking
Tremor sensation of Abnormal behavior
Anxiety warmth Loss of memory
Nausea Paresthesia Blurred vision
(Tingling) Incoordination
Confusion
LOC
Seizure
Fatigue
Dizziness
Headache
Drowsiness

Mnemonic for C/F of hypoglycemia → ‘’He IS TIRED’’


☛ Headache
☛ Irritable
☛ Sweating
☛ Tachycardia
☛ Incoordination
☛ Restless
☛ Excessive hunger
☛ Dizziness

Major causes of hypoglycemia:

In DM Patient
✓ Insulin a n d sulfonylureas e x c es s dose or previous doses with
unaccustomed exercise
✓ Omission of meals.
✓ Development of CKD, AKI, and sepsis.
In non-diabetic patients with critical illnesses
✓ Hepatic or renal failure
✓ Adrenal insufficiency
✓ Sepsis
✓ Malaria.
In Seemingly normal patients
✓ Exercise
✓ Other drugs and alcohol consumption
✓ Endogenous hyperinsulinemia
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✓ Accidental or surreptitious use sulfonylureas or insulin.

NB: Hypoglycemia caused by sulfonylureas can be prolonged for several days.


Hence these patients should not be discharged with emergency room correction of
hypoglycemia alone

Investigations and diagnosis

Diagnosis

➢ Hypoglycemia in diabetes diagnosed with either of the following


o RBS <70mg/dl in diabetes and <55mg/dl in non-diabetic patient.
o Presence of symptoms which improve with treatment
➢ Classification of diabetes associated hypoglycemia based on severity
Level (severity) Characteristics
1 (mild) RBS = 54-70 mg/dl
2 (moderate) RBS <54 mg/dl
3 (severe) Altered mentation and/or physical status requiring
assistance for treatment of hypoglycemia

Investigations
✓ Glycemia related: FBS, postprandial blood sugar and HbA1c
✓ Creatinine and urea

Management of hypoglycaemia

Non-pharmacologic

➢ The main stay of management of level 1-2 (mild to moderate) and level-3
(severe) hypoglycemia with preserved consciousness taking or providing
glucose rich food/drinks(sweets).
o Pure glucose is preferred but any carbohydrate rich food can be
used
If RBG/FBG < 70 mg/dl
✓ Give oral glucose 20g (4 teaspoons of sugar, 4 hard candies, 200ml of
Mirinda® or Cola®, or 60 ml of 40% dextrose PO)
✓ Give the patient food as soon as she/he can eat safely.
✓ Identify cause and educate about meals and doses, and reduce dose of
glibenclamide/glimepiride, or insulin if the drugs are the suspected
causes
✓ If incomplete recovery, refer same day.
✓ Discuss referral if hypoglycemia recurrent or if patient had altered mental
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✓ Discuss hypoglycemia risk factors with the patient (skipping meals,


physical activity more intense than usual, alcohol ingestion) and adjust
medication if necessary.
✓ Monitor blood sugar every 20-30 minutes
✓ If no improvement repeat the above
✓ Once blood sugar improves, the patient must take a meal or snack
o Alternatives: regular soft drinks
✓ 200ml of Mirinda® or Cola® contains about 20gram sugar can replace the
above.
o Avoid protein rich foods as they increase insulin response
➢ For hypoglycemia unawareness: a 2-3 weeks period of avoiding
hypoglycemia through frequent self-monitoring of blood glucose and keeping
the blood glucose at higher levels may restore awareness.

Pharmacologic
➢ If unable to take orally, give instead glucose 40% 50mL IV over 2-3
minutes.
➢ In patients who present to health facilities with decreased level of
consciousness from severe hypoglycaemia
N.B 1 vial of D40 = 20ml = 8g. How?
o 40% Dextrose/D40/ 40 % of 20ml =
𝟒𝟎
𝒙 𝟐𝟎𝒎𝒍 = 𝟖𝒎𝒍 = 𝟖𝒈
𝟏𝟎𝟎
✓ Give 03 vials (60ml = 24g), IV, fast
✓ Monitor blood sugar every 20-30 minutes
✓ If blood sugar is still <70mg/dl after 15 minutes, give another
03 vials of 40% dextrose and start 10% dextrose (i.e. D10)
infusion.
✓ Maintain with glucose 10% solution.
✓ Continue to monitor blood sugar every 20-30 minutes.

✓ In some references; it says, 40-60ml of D40 over 1 to 3


minutes through a large vein, followed by D 10%
✓ Glucose IV, 500ml, 4 hourly until the patient is able to eat
normally.
✓ Glucagon SC/IM 1mg in adults particularly in type I DM
patients.
✓ When the patient can take orally give regular meal or snack.

Prevention of hypoglycemia in diabetics

✓ Self-monitoring of blood sugar


✓ Patient, family/care giver education
o A standardized education on rigorous avoidance of hypoglycemia
o On conditions which increase the risk of hypoglycemia
✓ Fasting or delayed meals
✓ Consumption of alcohol
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✓ Intense exercise
o Symptoms of hypoglycemia and possibility of hypoglycemia
unawareness
o Treatment of hypoglycemia at earliest warning symptoms or at
<70mg/dl
o Adjusting glycemic targets to higher levels, if hypoglycemia is
recurrent
o Reporting episodes of hypoglycemia to physician

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10.2. CHRONIC COMPLICATIONS


OF DIABETES
Prevention of these complications can be achieved through optimal glycemic
control, optimal blood pressure management, lipid control, quitting smoking and
maintaining a healthy life style.

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Table: screening and management of chronic complication of diabetes

Initial screening Follow up screening Prevention & Treatment


Nephropathy T1DM → after 5 years No nephropathy → annually Optimize glycemic control
T2DM → at diagnosis Nephropathy → 2x/yr Optimize BP control
Screening tool: if eGFR < 30ml/min consult ACEi/ARB for proteinuria
 U/A→ Albuminuria nephrologist together with
 Creatinine, eGFR endocrinologist
Retinopathy T1DM → after 5 year No retinopathy → in 1-2yr Optimize glycemic control
T2DM → at diagnosis Retinopathy →1yr Optimize BP control
Before and at time of Sight threatening Optimize lipid control
pregnancy retinopathy needs more Pan retinal laser
Screening tool: frequent evaluation photocoagulation
 Dilated eye Intra vitreous injections of
examination by anti-vascular endothelial
ophthalmologist growth factor
ASA is not recommended in
patients with retinopathy
Neuropathy T1DM → after 5 years Annually Optimize glycemic control
T2DM → at diagnosis Symptomatic management

Screening tool Painful neuropathy


 Careful history Amitriptyline: 12.5-50mg PO/bedtime
 Temperature/
pinprick & vibration Gastroparesis
sensation Plasil,10mg PO, TID (syrup preferred)
 10-g monofilament
testing Alternatives (2nd line)
Domperidone 10mg PO TID
Erythromycin syrup, 50-250mg, TID

Diabetic diarrhea
Symptomatic treatment
 Loperamide 2-4mg, PO, TID or QID or
 Codeine 30mg, PO, TID or QID
Treatment of bacterial overgrowth: Antibiotics for 7-
10days
 Norfloxacin 400mg, PO, BID Or
 Metronidazole 500mg, PO, TID
PLUS
 Cephalexin 500mg, PO, TID or
 Cotrimoxazole 960mg BID

Postural hypotension
Change posture slowly
Elevate head by 10-200
Dorsiflexion of feet and handgrip (before standing
Tensing legs by crossing (when standing)

Bladder dysfunction
Remove drugs which worsen it (Amitriptyline, CCB)
Strict voluntary voiding schedule
Crede maneuver (lower abdominal pressure by
hands) 652
If severe: Self intermittent catheterization
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Erectile dysfunction
Use PDE5 inhibitors
 Sildenafil 25 -100mg (start with 50mg)
 Vardenafil 10-20mg
 Tadalafil 10-20mg
If refractory
 Tadalafil 2.5-5mg/daily

Take 01hr before sexual encounter


On empty stomach
Avoid use with nitrates

Diabetic foot Initial visit Every visit Look at diabetic foot ulcer section
Screening tools below
 Assessment of skin
& foot deformities
 Neurologic exam
 PAD evaluation

10.2.1. Diabetic nephropathy


➢ Diabetic nephropathy is the leading cause CKD and ESRD.
➢ An important marker of increased cardiovascular risk. It carries a mortality rate
~50% from Cardio Vascular causes.
➢ Its pathogenesis is related to chronic hyperglycemia
➢ Occurs in 20-40% of diabetic patients
➢ Type 1: 10-20 years after initial diagnosis
➢ Type 2: May even be present at time of diagnosis (long pre-clinical period)
➢ Usually progresses from albuminuria to overt CKD
➢ Intervention at the stage of Micro albuminuria can retard the progression to
end stage renal disease (ESRD)

ALBUMINURIA
Defined and staged by level urinary albumin excretion

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DIABETIC NEPHROPATHY SCREENING

➢ Screen for albuminuria


 Type 1: 5 years after diagnosis
 Type 2: At the time of diagnosis
 In every pregnant lady
 Thereafter, screening should be done yearly
➢ Measure serum creatinine at least yearly
➢ If no proteinuria, continue screening every year
➢ If patient has proteinuria do RFT
➢ If RFT abnormal, refer to specialist
➢ If RFT normal repeat urine analysis after 3 months
➢ If proteinuria is persistent start on Enalapril 5 mg/d
➢ Appoint every month and do RFT test on every appointment
➢ If creatinine has increased by more than 30% discontinue enalapril If
not, escalate enalapril by 5 mg each month until 20 mg /d and maintain
on that dose
➢ Check RFT every 6 months after that

10.2.2. Diabetic Retinopathy

➢ See the table above

10.2.3. Diabetic neuropathy


➢ Most common of the chronic DM complications
➢ Occurs in ~50% of individuals with long-standing type 1 & type 2 DM
➢ Impairs quality of life


Development of neuropathy correlates with duration of DM & glycemic control.
Risk factors are
 Obesity
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 Hypertension
 Smoking
 Alcohol use and
 Dyslipidemia.
➢ Most important risk factor for foot ulcer and amputation
➢ Clinical evaluation for diabetic neuropathy includes detailed history on
symptoms like burning, tingling and pains; erectile dysfunction in men; glycemic
control; presence other risk factors, and detailed neurologic exam especially
sensory, reflex and motor exam of the extremities.
➢ May manifest as polyneuropathy, mononeuropathy, and/or autonomic
neuropathy
➢ Start screening for neuropathy using the 60 second tool mentioned
below when DM is diagnosed.
 If negative screening, then continue screening yearly
 If abnormal, refer for management to tertiary center
➢ If referral not possible and patient has no urgent referral needs such as
an ulcer or absent pulses or a hot swollen foot indicating Charcot’s
arthropathy, then advise on foot care and evaluate the foot every 3
months.

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A. DISTAL SYMMETRIC POLYNEUROPATHY

➢ Commonest type of diabetic neuropathy.


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➢ Distal symmetric sensory or sensorimotor neuropathy


➢ Decreased pain sensation and vasculopathy → ulcer risk
➢ Patients complain of numbness, tingling, sharpness, or burning that begins in
the feet / hands & spreads proximally
➢ Pain is present at rest and worsens at night.
➢ Physical examination reveals sensory loss, loss of ankle deep-tendon reflexes,
and abnormal position sense
➢ It is a diagnosis of exclusion

B. AUTONOMIC NEUROPATHY

C. DIABETIC POLYRADICULOPATHY

D. MONONEUROPATHY

TREATMENT OF DIABETIC NEUROPATHY

➢ Improve glycemic profile


➢ May use analgesics initially
➢ If patient has symptoms of peripheral neuropathy such as numbness
and burning sensation in the foot or hands (that aggravate mostly at
night) then do Thyroid Function Test and serum vitamin B12 levels if
available
➢ If not possible to do these tests, then start on Amitriptyline 25 mg/d at
bedtime– may increase dose gradually
➢ Pregabalin can also be used
➢ Carbamazepine 200mg at bedtime & increased gradually
➢ If it doesn’t improve, refer to a tertiary center for neurologist Evaluation.
➢ Give diabetes foot care education for all patients with diabetes in groups
and separately every visit to the health facility.

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10.2.4. Diabetic foot ulcer


Clinical features and how to write hx of Diabetic foot ulcer

History
If a known DM patient → ask the following on your HPI

➢ Type I DM
o For how long he/she was diagnosed to have DM
o Ask the dose and frequency of insulin injection. → Usually a mixture
of 2/3 of NPH and 1/3 of regular insulin. From this mixture 2/3 of
the dose taken in the morning and 1/3 at night.
o Specify alternative injection sites
o Where he/she does store their insulin→ wet sand bags or refrigerator
o Adherent or not
o Where was the follow up and frequency (every month, every two
months….)
o How was his/her smx’s in between… improving, worsening or no
change at all… if not improving or worsening what was the reason
(non-adherence, wrong diagnosis ……)

Reporting format example

A known DM pt for the past 6 years or you can say 6 years back s/he
was told to have DM (you can ask what was the presentation at that time and how Dx was
made… no need to write on your HPI) taking insulin injection 20 units in the
morning and 10 units at night. With alternative injection sites between
his/her upper arms, thighs and periumbilical area. Stores his/her insulin in
wet sand bag /refrigerator/. S/he was adherent for his/her medication with
regular follow up every 3 months here in our hospital.

➢ Type II DM
o For how long he/she was diagnosed to have DM
o What medication he was taking and ask the dose and frequency of
each medication. If the pt’ doesn’t remember or doesn’t know the
name of the drug ask the colour, frequency, and route of the
medication (e.g he/she was taking white coloured tablet 3 times per
day).
o Does he/she start insulin other than oral hypoglycaemic drugs? If
yes what is the reason of shifting to insulin.
o Adherent or not
o Where was the follow up and frequency (every month, every two
months….)
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o How was his/her smx’s in between… improving, worsening or no


change at all… if not improving or worsening what was the reason
(non-adherence, wrong diagnosis ……)

Reporting format example

A known DM pt for the past 6 years or you can say 6 years back he
was told to have DM (you can ask what was the presentation at that time and how Dx was
made… no need to write on your HPI) On metformin 500 mg, PO, daily . He was
adherent for his medication with regular follow up every 3 months here in
our hospital.

Then ask clinical features of foot ulcer

➢ intermittent claudication
o Left/right calf stabbing type of pain which radiates to toes → usually
after waking of >200 meters
o Occur while walking and relieved by massage, sitting or lying down
➢ Numbness which spread upwards usually up to the knees (ask with in how
many days it reaches the knee).
➢ Burning sensation (over where?) which worsen by walking and relieved by
massage, cold water and pain killer
➢ Foot swelling→ where?
o Gradual in onset
o Overlying skin colour change
▪ Blackish discoloration of overlying skin→ up to where?
Subside or not?
o Painful or painless?
o Ulcerated or not?
o If ulcerated
▪ When does it ulcerate?
▪ What is the colour of discharge?
▪ Size→ Usually small in size, which increase gradually (with in
how many days does it attain it’s current size)
➢ Associated smx’s like fever, chills, palpitation, headache…. when does they
occur and frequency of smx’s within the day (morning, afternoon, night,
throw-out the day)?

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Risk factors
✓ Long standing DM → Diabetes >10 years' Duration
✓ Poor glycemic control
✓ Wearing unfit shoes
✓ Waking bare foot
✓ Unclean foot
✓ Trauma
✓ Male Sex
✓ Abnormal Structure of Foot (Bony Abnormalities, Callus, Thickened Nails)
✓ PAD
✓ Smoking
✓ History of Previous Ulcer or Amputation
✓ Previous Foot Ulcers
✓ Poor Sight
✓ Old age
✓ Concurrent DM complications
• Chronic sensory motor neuropathy or autonomic neuropathy
• Vascular disease like ischemia
• Infection
• Impaired immune function

Diabetic foot Triad

Neuropathy

Trauma

Ulcer
Ischemia Infection

Diabetic Neuropathy (80% of pts)

➢ 7% annual risk of ulceration


➢ Sensory, motor, and autonomic
➢ Decrease pain sensation and perception of pressure
➢ Ms imbalance leading to deformities
o Hammer toes, Claw toes Prominent metatarsal heads
➢ Reduced sweating, dry skin, and development of cracks and fissures

Peripheral Vascular Disease

➢ Increased incidence by 2-4fold 660


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➢ Promotes development of critical limb ischemia, poor wound healing and


tissue loss

N.B Complications of DM like Diabetic foot ulcer are common in Type II DM than
Type I DM

Complication of Diabetic foot ulcer

▪ Cellulitis
▪ Abscess formation
▪ Joint sepsis
▪ Osteomyelitis
▪ Gangrene and Amputation→ DM is the most common cause of non-
traumatic foot amputation

Sample history

Chief compliant

Left foot ulceration of 1-month duration

HPI

A known DM patient for the past 8 years on metformin 1gm, PO, BID and
Glibenclamide 10 mg, PO, BID for 5 years and she was adherent for her
medication with regular follow up every 3 months here in Black Lion Hospital. For
the last 3 years insulin was added because she was told that her blood glucose
level was not well controlled by oral hypoglycemic drugs. Currently she took 24
units of insulin in the morning and 12 units at night with alternative injection sites
between her upper arms, thighs and periumbilical area.Stores her insulin in
refrigerator.

She was relatively healthy until three months ago at which time she started to
experience a gradual onset of left calf stabbing pain which radiates to the toes
and numbness of both feet. Both symptoms were intermittent occurring mainly
when walking and relived by massaging of the legs, sitting and lying down. The
numbness started to spread upwards from the toes and involved the knees within
2 weeks duration associated with burning sensation of the left sole of the foot
which was constant but increased in intensity when walking while painkillers and
massaging in cold water eased the pain. Following this she came to Black Lion
Hospital. Since no bed was available, she was scheduled to come three weeks
later and was sent home.

She missed her appointment due to unknown reason and around one month
before admission, she noticed swelling of the left foot and a small black
discoloration on the plantar surface of the left big toe. The swelling involved up to
the knee but subsided after 4 days of constant massaging while the black 661
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discoloration of the toe increased in size and ulcerated one week later with non-
foul-smelling blood mixed pussy discharge. The ulcer was small at first but within
the following two weeks it enlarged constantly involving the whole plantar surface
of the left big toe. One week before admission she started experiencing a sudden
onset of intermittent fever accompanied by sweating, chills, rigor, palpitations and
numbing global headache.

Following this she came to black lion hospital emergency OPD and was admitted
to B8 ward on the same day.

➢ Ask those +ve and -ve statements listed on the sample hx of a DM


patient above.
➢ She has a history of foot ulcer two years ago on the same toe. She went to
Ras Desta Hospital and was advised to have an amputation of the toe but she
refused and was discharged. But the patient claims that after two weeks of
washing the foot with salt water the ulcer subsided and disappeared.
➢ She has history of blurring of vision 8 years back at the time of diagnosis of
the diabetes. Laser eye surgery was done at Menelik hospital on the left eye
but the patient refused for the right eye due to discomfort. Following that the
eye sight on the left eye corrected but on the right eye, the blurring of vision
and shadowing progressed to total blindness.
➢ She wears well fitted shoes and doesn’t walk bare foot (RF)
➢ She dry skin of foot after washing leg, check between toes, and she
adds lotion to leg (unclean foot is RF)
➢ No hx of Leg trauma (traumatic ulcer →DDX)

Physical examination (pertinent findings)

✓ Assess all pertinent findings listed above for DM pt’


✓ Arterial examination especially posterior tibial artery and dorsalis pedis
artery (asses for PAD)
✓ Do full musculoskeletal examination (look, feel, move and measure)
✓ Characterize the ulcer
❖ Location → Great Toe and MTP areas are most common. Toes
(51%), Plantar metatarsal head (28%), Dorsum of foot (14%),
multiple ulcer (7%)
❖ Single or multiple
❖ Margin → regular/irregular, sloughing or not
❖ Type and colour of discharge
❖ Surrounding skin colour change (gangrene) and erythema (measure
the size)
❖ Compare temperature with surrounding skin
❖ Surrounding tenderness
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❖ Size (length and diameter i.e. ‘’X’’ by ‘’Y’’ cm). Wound Depth should
be determined by inspection and probing with a blunt-tipped
sterile instrument.
❖ Floor bleed during touching or not
❖ Is the bone visible or not?

✓ Assess systemic cxn like fever


✓ Measure ABI (ankle brachial index)

𝐒𝐁𝐏 𝐨𝐟 𝐚𝐧𝐤𝐥𝐞
𝐀𝐁𝐈 = 𝐒𝐁𝐏 𝐎𝐅 𝐁𝐫𝐚𝐜𝐤𝐢𝐚𝐥 𝐚𝐫𝐭𝐞𝐫𝐲
= 𝟎. 𝟗 − 𝟏. 𝟏

➢ SBP of ankle measured by Doppler ultrasound guided BP measurement but


SBP of arm can be measured by sphygmomanometer (by any BP cuff
available in the ward)
➢ ABI < 0.9 is evidence for PAD, > 1.1 is evidence for vessel wall calcification

Evaluation for the foot at risk


✓ Look for PAD → Foot Pulses, Doppler
✓ Look for Neuropathy → Tuning Fork, Monofilament

Picture; left) Monofilament Testing, right) Monofilament Testing Areas

✓ Anatomic Deformities → Charcot’s Foot, Hammer Toes, Clawed Toes

Picture; Charcot foot

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DDX for foot ulceration in DM patient

1. Diabetic foot ulcer


2. PAD → refer nitsibin under CHF (click here → Peripheral Arterial Disease
(Chronic Arterial Insufficiency)
3. Leprosy → Anaesthetic skin lesion, swelling
4. Venous ulcer → usually after varicose vein
5. Arterial ulcer
6. Haemolytic anemia → non healing ulcer from SCA or autoimmune
haemolytic anemia
7. Gumatous ulcer
8. Traumatic ulcer
9. Cellulitis
10. TB (mycobacterium ulcerans) → rare ulcer which is known as Bruli ulcer
11. Madura foot
12. Anthrax
13. Neuropathic ulcer (peripheral neuropathy)
14. Tropical ulcer (pressure ulcer)
15. Malignant ulcer
16. Specific ulcer
17. SCC (marjolin ulcer)

IX

1) Blood sugar level → hyperglycaemia


2) Discharge analysis & culture for infection
▪ Infected ulcer is a clinical diagnosis, since superficial culture of any
ulceration will likely find multiple possible bacterial species.
▪ The infection surrounding the foot ulcer is often the result of multiple
organisms (Gram +ve, Gram -ve and Anaerobes), And Gas Gangrene
may develop in the absence of Clostridial Infection.
▪ Cultures taken from the Surface of the ulcer are not helpful. But, A
culture from the debrided ulcer base or from purulent drainage or
aspiration of the wound is the most helpful.
3) U/A → glucosuria, ketonuria
4) CBC → leucocytosis
5) X-ray of the involved area if bone is involved (osteomyelitis)
6) MRI of the foot may be the most specific modality
7) Doppler ultrasound of supplying artery to see its patency
8) Pancreatic function test → amylase
9) If Surgical Debridement is necessary → Bone Biopsy and Culture
10) Other IX listed in DM → refer DM

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Discussion

❖ Diabetic foot ulcers are Slowly healing plantar ulcers that result from
apparently insignificant trauma
❖ The lifetime risk of a foot ulcer in patients with diabetes (type 1 or 2) may
be as high as 25 %.
❖ Diabetic foot ulcers are a major cause of morbidity and mortality,
accounting for approximately 2/3rd of all nontraumatic amputations performed
in the United States
❖ Left untreated, superficial ulcers may penetrate to underlying tissues,
leading to complications including cellulitis, abscess formation, joint sepsis,
and osteomyelitis
❖ Gangrene may occur, and amputation may be required in severe cases.
❖ To varying degrees, the diabetic foot is characterized by the combination of
chronic sensorimotor neuropathy, vascular disease, autonomic neuropathy,
and impaired immune function
❖ Once an ulcer has formed, it should be treated aggressively with antibiotics,
appropriate local wound care, and debridement of necrotic tissue

Ulcer Classification

The first step in managing diabetic foot ulcers is assessing, grading, and
classifying the ulcer.
Classification is based upon clinical evaluation of the extent and depth of the
ulcer and the presence of infection or ischemia, which determine the nature
and intensity of treatment.
To assess for ischemia, all patients with diabetic foot ulcers should have
ankle-brachial index (ABI) and toe pressure measurements.
There are many Classification systems of diabetic foot ulcer. We will see
common ones here.
 Wagner classification system
 University of Texas classification system
 IDSA classification system
 WIFI classification system
 PEDIS classification system
(where; IWGDF = International Working Group on the Diabetic Foot,
IDSA = Infectious disease society of America, WIFI =
Wound/Ischemia/Foot Infection, PEDIS = Perfusion, extent, depth,
infection, and sensation)

N.B.
➢ Only two classification systems have been developed that provide stratification
that aligns to clinical decision-making: IWGDF/IDSA and WIFI.
➢ whilst the IWGDF/IDSA is incorporated into the WIFI, in situations where only
infection is being assessed and equipment is not available to use WIFI, the
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➢ IDSA is the recommended classification system for management and clinical


use in our setup.

✓ Wagner classification system


It is an early and often still used classification system at hyperbaric-based
wound healing centers was originally proposed by Wagner.
This classification was based upon clinical evaluation (depth of ulcer and
presence of necrosis) alone and did not account for variability in the vascular
status of the foot.
The Wagner system is predictive of poor outcome, but only up to grade 3.
Even though we are using in our setup, it is outdated from use in most
countries because it is a local grading system which doesn’t consider systemic
conditions like loss of protective sensation, infection, and ischemia.
It includes:
 Grade 1: Skin and subcutaneous tissue
 Grade 2: To bone
 Grade 3: Abscess or osteitis
 Grade 4: Partial foot gangrene
 Grade 5: Whole foot gangrene

✓ University of Texas system


An update to the Wagner system was introduced at the University of Texas
(UT), San Antonio in the United States.
While similar to Wagner in its first three categories, this later system eliminated
grades 4 and 5 and added stages A to D for each of the grades.
The UT system was the first diabetic foot ulcer classification to be validated.
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Stage:
➢ Stage A: Noninfected
➢ Stage B: Infected
➢ Stage C: Ischemic
➢ Stage D: Infected and ischemic

Grade
✓ Grade 0: Pre- or post-ulcerative (Stages A to D)

✓ Grade 1: Full-thickness ulcer not involving tendon, capsule, or bone (Stages


A to D)

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✓ Grade 2: Tendon or capsular involvement without bone palpable (Stages A to


D)

✓ Grade 3: Probes to bone (Stages A to D)


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3. IDSA classification system


IWGDF/ISDA classification consists of 4 grades of severity for diabetic foot
infection.
It was originally developed as part of the PEDIS classification for research
purposes and is used as a guideline for management, in particular to identify
which patients required hospital admission for IV antibiotics.
It has also been validated for risk of both major and minor amputation.

Table. IWGDF/IDSA classification System

Clinical manifestations Infection PEDIS


severity grade
Wound lacking purulence or No manifestations of Uninfected 1
inflammation
Presence of ≥2 manifestations of inflammation Mild 2
(purulence, or erythema, tenderness, warmth, or
induration)
Any cellulitis/erythema extends ≤2cm around the
ulcer
infection is limited to the skin or superficial
subcutaneous tissues
no other local complications or systemic illness
Infection (as above) in a patient who is systemically Moderate 3
well and metabolically stable but which has ≥1 of
the following characteristics:
1) cellulitis extending >2cm
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2) lymphangitic streaking
3) spread beneath the superficial fascia
4) deep tissue abscess
5) gangrene
6) involvement of muscle, tendon, joint or bone
Infection in a patient with systemic toxicity or Severe 4
metabolic instability (e.g. fever, chills, tachycardia,
hypotension, confusion, vomiting, leukocytosis,
acidosis, severe hyperglycemia /DKA or HHS/, or
azotemia)

4. Threatened limb classification: Wound/Ischemia/Foot Infection


(WIFI) classification system

Figure; WIFI classification system;

6. PEDIS classification system.


PEDIS stands for Perfusion, extent/size, depth/tissue loss, infection, and
sensation
It is primarily used for research purposes. and not designed for prognostic
purposes. It does not include patient factors (ESRD), or either the location or
the number of foot ulcers.

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Management of Diabetic foot ulcer


➢ The optimal therapy for Foot Ulcers and Amputations is Prevention through
 Identification of High-risk Patients
▪ High-risk patients should be identified during the Routine Foot
Examination performed on all patients with DM
 Education of the Patient, and
 Institution of Measures to Prevent Ulceration.

Patient Education should emphasize


 Careful selection of Footwear
 Daily inspection of the feet to detect early signs of poor-fitting footwear or
minor trauma

For DM patients ‘’mirrors are


not only for face, but also for
feet beauty checkup’’

 Daily Foot Hygiene to keep the skin clean and moist


 Avoidance of self-treatment of foot abnormalities and high-risk behavior
(e.g., walking barefoot), and
 Prompt consultation with a health care provider if an abnormality arises.
 Patients at high risk for ulceration or amputation may benefit from
evaluation by a Foot Care Specialist.

Foot care prescription for diabetic patients with lower extremity sensory neuropathy

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Do’s and Don'ts of foot care

Do’s Don'ts
Don’t apply hot water or irritant
Control blood sugar level
chemicals
check feet daily
Wash feet daily Don’t ignore numbness
Don’t treat calluses, corns, or ingrown
Keep toenails short
toenails at home
Protect feet
Don’t cross your legs or ankles for a
Look inside shoes before
long period of time. Doing so can
putting them on
create pressure points and lead to
Always wear socks
unwanted breaks in skin
Do exercise to augment
controlling of blood sugar Don’t go bare foot
Don’t wear unfit shoes or tight socks
level
Don’t forget you follow up at health
Etc.
facility
etc.

Interventions directed at Risk Factor Modification include


 Orthotic Shoes and Devices
 Callus Management
 Nail Care and
 Prophylactic Measures to reduce Increased Skin Pressure from
Abnormal Bony Architecture.
Attention to other Risk Factors for Vascular Disease (Smoking, Dyslipidemia,
Hypertension) and Improved Glycemic Control are also important.
 One of the biggest threats to the feet is smoking!
 Smoking affects small blood vessels by decreasing their blood flow to the
feet making wounds heal slower.
 Cessation of smoking is a good way to decrease the likelihood serious
problems, such as amputation.

Despite preventive measures, Foot Ulceration and Infection are common and
represent a serious problem.
Due to the Multifactorial Pathogenesis of lower extremity ulcers, Management
of these lesions is multidisciplinary and often demands expertise in
 Orthopedics
 Vascular Surgery
 Endocrinology
 Podiatry and
 Infectious Diseases.

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ADA recommend 6 Interventions with demonstrated efficacy in Diabetic Foot


Wounds:

1) Mechanical Off-loading
2) Debridement or local wound care
3) Wound Dressings,
4) Appropriate Use of Antibiotics (treatment of infection)
5) Revascularization and
6) Limited Amputation.

I. Off-Loading
➢ It is the complete avoidance of weight bearing on the ulcer Which removes the
mechanical trauma that retards wound healing.
➢ Bed Rest and a variety of Orthotic Devices or Contact Casting limit weight
bearing on wounds or pressure points.

II. Surgical Debridement


➢ Indicated If infection surrounding the ulcer is not improving with IV antibiotics
and Debridement of necrotic tissue
➢ It is important and effective but clear efficacy of other modalities for wound
cleaning (Enzymes, Soaking, Whirlpools) is lacking.

III. Dressings
➢ Dressings such as Hydrocolloid Dressings promote wound healing by creating
a moist environment and protecting the wound.
➢ Antiseptic agents should be avoided.
➢ Topical antibiotics are of limited value.
➢ Physiotherapy, Orthotic Evaluation, and Rehabilitation Should occur once the
infection is controlled.

IV. Appropriate Use of Antibiotics (treatment of infection)

➢ Mild or Non-limb-threatening Infections (e.g. Cellulitis Without Ulceration) can be


treated with Oral broad-spectrum Antibiotics (Cephalosporin, Clindamycin or
metronidazole, Amoxicillin/Clavulanate, and Fluoroquinolones), Local Wound
Care (Avoidance of weight bearing over the ulcer), and Close Surveillance for
progression of infection.
➢ More Severe Ulcers may require IV Antibiotics as well as Bed Rest and
Local Wound Care.
➢ Strict control of glycemia should be a goal.
➢ IV Antibiotics should provide Broad-spectrum Coverage directed toward S.
Aureus, Streptococci, Gram -ve Aerobes, and Anaerobic Bacteria.
➢ Initial Antimicrobial Regimens include Ertapenem, Piperacillin/Tazobactam,
Cefotetan, Ampicillin/Sulbactam, Linezolid, or combination of Clindamycin and a
Fluoroquinolone.
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➢ Severe Infections, or Infections that do not improve after 48 h of Antibiotic


Therapy, require expansion of antimicrobial therapy to treat MRSA (e.g.,
Vancomycin) and Pseudomonas Aeruginosa.
➢ If the infection surrounding the ulcer is not improving with IV antibiotics,
Reassessment of antibiotic coverage and Reconsideration of the need for
surgical debridement or Revascularization are indicated.
➢ With Clinical Improvement, Oral antibiotics and local wound care can be
continued on an outpatient basis with close follow-up.
➢ Peripheral Arterial Bypass Procedures are often effective in promoting wound
healing and decreasing the need for amputation of the ischemic limb.

Management based on IDSA classification of severity of infection

Uninfected
 Treatment of risk factor and follow up
Mild infection
 Can be treated with broad spectrum oral antibiotics at OPD with close
follow up.
 Antibiotics include; Cephalosporin, Clindamycin or metronidazole,
Amoxicillin/Clavulanate, and Fluoroquinolones
Moderate to severe infections
 Need hospital admission for IV antibiotics (ceftriaxone or cefotaxime with
metronidazole are available in most setups of Ethiopia).
 Consider anaerobic coverage
 Modify Antibiotics based on culture result
 Duration is at least for 4 to 6 weeks (parenteral antibiotics for at least 2
weeks, the rest completed with PO antibiotics)
 Surgical debridement required for tissue abscess and local gangrene.
 Those with extensive and life-threatening gangrene may require
amputation.

Management based on Wagner Grading

Grade 0: No Ulcer, Risk Factors Present


 Education about foot care
Grade 1: Superficial Ulcer
 Relief of Pressure
 Good local wound care
 Treatment of Infection: PO antibiotics
Grade 2: Deep Ulcer + Infection, No Bony Involvement
 Treat as Grade 1, if no Improvement → Admit and extensive
debridement
Grade 3: Infected Ulcer with Bony Involvement
 Admit to Hospital
 Relief pressure
 Local wound care
 Debridement 675
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 Initiate Antibiotics: Triple antibiotics


Grade 4: Localized Gangrene
 Treat Like Grade 3
 Improve Circulation
 Diffuse Arterial Disease May Require Major Amputation
Grade 5: Gangrene of Whole Foot
 Urgent Hospital Admission
 Antibiotics
 Surgical consultation and Amputation

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10.3. Pediatrics DM and DKA Case


Management
Dr. Mulualem Gashaw (MD, GP)
Reviewed by
Dr. Kidan Mihret (MD+, Pediatrician) and Dr. Melkam Desta (MD+, Pediatrician)

CASE STUDY

➢ A 6 year’s old child brought to pediatrics OPD with a complaint of abdominal


discomfort of one day duration.
➢ The child had managed to spend the day in school but her
condition seemed to have worsened since coming home and had been
vomiting twice
➢ There was no apparent fever, diarrhea, rash, pain elsewhere, photophobia or
altered behavior, or dysuria, and some simple painkillers had made very little
difference.
➢ No other family member was currently unwell with any gastrointestinal
conditions and no obvious unusual food intake in the last three days.
➢ The child vomited once more during this time but on evaluation by the clinician
she looked well, smiled and did not appear clinically
dehydrated or in distress.
➢ She was apyrexial, the abdomen felt soft and did not reveal any specific
tenderness, guarding or rebound, and the bowel sounds were normal.
➢ The clinician reassured the mother and gave her daughter albendazole for
possible intestinal parasitosis.
➢ As they were leaving the exam room the daughter asked her
mother for water, and the mother mentioned to the clinician that her daughter
was unusually thirsty the past few days.
1. What is the differential diagnosis for this child’s problem?
2. What additional information do you like to know?
3. What additional tests do you like to do?

➢ She has started bed wetting at night for the past 3 days which the mother
didn’t know.
➢ Two weeks ago the child was 20kgs.
➢ Her current weight is 18 kg
➢ Height is 110cm
➢ RBS:300mg/dl
➢ Urine ketone: +2
➢ Stool exam:-ve
➢ Urine Microscopy was WBC 2-3/HPF
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➢ How will you manage this patient?

DM definition

➢ Look at Adult section

Etiologic classification of diabetes mellitus

The classification of diabetes includes 4 clinical classes


➢ Type I diabetes
 Immune-mediated
 Idiopathic
Type 1 Diabetes accounts for over 90% of childhood and adolescent
diabetes
Common from 6 months to young adulthood for pediatric age

➢ Type II diabetes
 Type 2 Diabetes is becoming more common in adolescents,
particularly in the peripubertal period25, and accounts for a significant
proportion of youth onset diabetes in certain at risk populations.
➢ Other specific types of diabetes
 Common forms of monogenic diabetes
▪ Neonatal diabetes mellitus [NDM]
o Age less than 12 months and especially in first 6
months of life
▪ Chromosomal abnormalities (from MODY 1 to MODY 6, MODY
= Maturity onset diabetes of the young /in youth/)
 Genetic defects in insulin action
 Diseases of the exocrine pancreas (Pancreatitis,
Trauma/pancreatectomy, Neoplasia, Cystic fibrosis,
Hemochromatosis….)
 Endocrinopathies (Hyperthyroidism, Acromegaly, Cushing's syndrome,
Glucagonoma, Somatostatinoma, Pheochromocytoma, Aldosteronoma…)
 Drug or chemical induced (Glucocorticoids, Thyroid hormone,
Thiazides, Pentamidine, Nicotinic acid, Beta-adrenergic agonists, Alpha
interferon…)
 Infections (Congenital rubella, CMV…)
 Other genetic syndromes sometimes associated with diabetes (Down
syndrome, Klinefelter syndrome, Turner syndrome, Porphyria,
Friederich's ataxia….)
 MRDM (Malnutrition related DM)

25
In average puberity in males is from 11.5 to 16 years old and in females from 10 to 16
years old. But it differs from person to person which is the start of SMR Stage 2 (SMR =
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 Others
➢ Gestational diabetes mellitus (GDM)
➢ Look at Adult section for more

Suggestive clues to Differentiate Type I DM from Type II DM

➢ Type I DM common 6 months to young adulthood, Type II DM Usually


pubertal (or later) for pediatric age
➢ For details Look at Adult section

Table. Current ADA diagnostic criteria for diabetes mellitus

➢ Look at Adult section

CLINICAL PRESENTATION

Childhood type 1 diabetes mellitus (T1DM) can present in several different


ways:
 Classic new onset of chronic 3P’s;
▪ Polydipsia
▪ Polyuria
▪ Polyphagia and weight loss with hyperglycemia and ketonemia (or
ketonuria)
 DKA- the commonest presentation in Ethiopia
 Silent (asymptomatic) incidental discovery

Diabetic ketoacidosis (DKA)

DKA (hyperglycemia and ketoacidosis) is a condition in which there is a severe


deficiency of insulin resulting in very high blood glucose.
The diagnosis of DKA is based on the triad of hyperglycemia, ketosis and
metabolic acidosis
Fat is broken down as an alternative source of energy with ketones/ketoacids
as a by-product.
This state of severe hyperglycemia and ketone body production results in
severe metabolic, fluid and electrolyte abnormalities.
DKA often occurs in type 1 diabetes patients but may also occur in type 2
diabetes.
In Ethiopia 80% of patients present with DKA as an initial presentation.
 In the western populations the reported frequency is around 15-65%
In addition to polyuria, polydipsia, and weight loss, patients with DKA may
present with
 Nausea, vomiting, abdominal pain,
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 Acetone/ fruity odor


 Deep and rapid breathing (Kussmaul’s breathing)
 Neurologic findings including drowsiness, confusion, lethargy or coma.
DKA can be misinterpreted as an acute vomiting illness because classic
pediatric symptoms of dehydration (decreased urination) are masked by the
polyuria that is associated with glucosuria.
Young children (<6 years of age) or those from an adverse socioeconomic
background are more likely to have DKA as their initial presentation of T1DM.
Among children, Those <3 years of age, almost all had DKA as their initial
presentation of T1DM.
The fundamental pathophysiology of this potentially life –thteatening
complication (i.e DKA) is the same as in adults. However, the child differs from
the adult in the following characteristics.
 Difficult to obtain the classical history
 Hyperventilation may be due to pneumonia or asthma
 Abdominal pain –simulate acute abdomen and lead to referral to a
surgeon
 Polyuria and enuresis – may be due Misdiagnosed as UTI
 Vomiting may be misdiagnosed as sepsis or gastroenteritis

Who is at risk of DKA?

➢ Infections (the most common cause)


➢ Children who omit insulin
➢ young children <5 yrs
➢ Unstable family circumstances
➢ Children with poor metabolic control
➢ Adolescent girls

DKA Severity classification

➢ Look at adult section

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Management of DKA In Pediatrics Age Group

Goals of therapy
➢ Correct acidosis and reverse ketosis
➢ Correct dehydration
➢ Restore blood glucose to near normal
➢ Monitor for complications of DKA and its treatment
➢ Identify and treat any precipitating event

Principles of Management

ABCD of life And Initial assessment


Resuscitation by expanding intravascular volume (fluid replacement therapy)
Insulin therapy
Potassium replacement therapy
Treat complications
Treat precipitating factors
Monitoring

1. Initial evaluation
➢ Vital signs including saturation
➢ Take weight for calculation
➢ Assess dehydration (Pulse volume, buccal
mucosa, capillary refill, sunken eye balls
➢ Look for signs of cerebral edema (headache, repeated vomiting, and high
blood pressure)
➢ Check level of consciousness (alert, sleepy and comatose)
➢ Mild DKA can be managed in Wards, Moderate and severe DKA needs ICU
Admission
➢ Ensure appropriate life support (Airway, Breathing, Circulation, etc.)
➢ In coma or severe vomiting- insert airway and drain stomach with NG tube

Investigations

➢ RBS
➢ U/A – Check glucose and ketones
➢ Electrolyte- potassium and sodium (if available)


ECG - if it is available (check T-wave)
RFT (BUN and Creatinine)
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2. Fluid Management

Initial Fluid Management (Bolus)

➢ For mild DKA → give Po fluid (water and any food-based fluids non sugar)
➢ For Moderate DKA → Give 10 ml/kg, N/S over 01 hour
➢ For Severe DKA → Give 20 ml/kg over 2 hours
✓ 20 ml/kg fast if in shock, Repeat second 20ml/kg if still in shock
➢ Mannitol at bedside for severe DKA, Incase Cerebral edema happens

Deficit Therapy

➢ For mild DKA continue with PO fluid and feeding if there is no vomiting and if
the child remains alert
✓ i.e For mild DKA, only the Maintenance fluid amount in the form of ORS
can be given over 24 hrs
➢ For Moderate and severe DKA calculate the amount of fluids as follows:
✓ Calculate the maintenance fluid for two days (48 hours) + Deficit fluid
calculated as 85 ml/kg and minus the bolus fluid = To be given over 48
hours
✓ i.e
𝑴𝒂𝒊𝒏𝒕𝒆𝒏𝒂𝒏𝒄𝒆 𝒇𝒍𝒖𝒊𝒅 (𝟒𝟖 𝒉𝒐𝒖𝒓𝒔) + 𝑫𝒆𝒇𝒊𝒄𝒊𝒕 𝒇𝒍𝒖𝒊𝒅 ( 𝟖𝟓 𝑿 𝑾𝒕)− 𝑴𝒊𝒏𝒖𝒔 𝑩𝒐𝒍𝒖𝒔 𝒇𝒍𝒖𝒊𝒅 ( 𝒘𝒉𝒊𝒄𝒉 𝒚𝒐𝒖 𝒈𝒂𝒗𝒆 𝒂𝒃𝒐𝒗𝒆 )
𝟒𝟖𝒉𝒓𝒔

Maintenance fluid calculation


Weight in kg Amount of fluid /kg/day
0-10 kg 100 ml/kg/day
11-20 kg 1000ml (100 X the 1st 10 kg) + 50 ml/kg/day for
the next kg
>20 kg 1500ml (100 X the 1st 10 kg + 50 x the 2nd 10kg)
+ 20 ml/kg/day for the remaining kg

➢ Slow rehydration is the current recommendation


➢ If the child has signs of cerebral edema refer the child to tertiary hospital
➢ If the child has fever which persisted after fluid management or if the child has
clear focus of infection please starts them on antibiotics.

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Table; from Nelson 21st edition

3. Insulin Therapy

➢ Start regular insulin after starting fluid management


✓ Don’t start Insulin in the first hour of management! It should be started
after 01 hour of fluid resuscitation in order to steadily decrease the
acidosis and it increases complication like shock, and
hypokalemia and cerebral edema
➢ Initial Bolus
✓ 0.5 u/kg, ½ IM and ½ Sc, Stat (some references say that, ½ IM and ½
IV)26
Then
➢ Maintenance
✓ Continue with 0.5 u/kg, sc, every 6 hourly (QID)27

26
An IV insulin bolus should not be used at the start of therapy; it is unnecessary can
precipitate shock by rapidly decreasing osmotic pressure, and can exacerbate hypokalemia.
(ISPAD 2022 Guideline)

27
According to Pediatric Diabetic ketoacidosis management protocol, Tibebe Ghion specialized hospital,
Bahirdar, Mastewal Ambaw (MD, Pediatrician), December 2019
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✓ 0.05- 0.1 units/kg/hr (Usually 0.1 units/kg/hr) if continuous IV infusion is


Available
✓ Adjust insulin dose to lower blood glucose no greater than 100 mg/dl/hr, to
stabilize at 150-200 mg/dl and also if there is hypokalemia that has
persisted despite administration of K+
✓ The insulin infusion can be lowered by 50-75% if needed.
➢ Change the NS to DNS when the plasma glucose has decreased to 250 mg -
300 mg/dl.
➢ If RBS < 150 mg/dl- make the fluid half 10% DW and half 0.9 NS
➢ RBS should be 150 to 250mg/dl until the acidosis clears.
➢ Don’t omit insulin is the key principle
➢ Continue the management until the child is out of DKA (until urine ketone is
free).
➢ Once the child is out of DKA, start them with NPH and Regular insulin with an
initial total daily dose of 0.5 to1.0 units/kg and re-adjust the dose based on
their glucose level

When Do we say child is out of DKA?


➢ Clinical Response
✓ Recovery to mental Alertness
✓ Able to take PO feeding
✓ Norma respiration (No kussmauls breathing, desaturation or SOB)
✓ If precipitant treated
➢ Laboratory Response
✓ Blood glucose < 250 mg/dl
✓ Serum Ketone Negative

4. Potassium replacement therapy

➢ Add intravenous KCl in the IV fluids (20-40 meq of KCl in each bag of NS)
N.B. 1 vail of Kcl = 20 meq (sometimes there is 1vial =40 meq
preparation)
➢ Add 2 vials (40meq) of KCL in every bag of fluid (1000ml of NS) once urine
output is adequate (>50 ml/hr)

<<Initial dose SC: 0.3 unit/kg, followed 2 hour later by SC insulin 0.2 units/kg every two hours can be used
in our hospital (TGSH). Insulin can temporarily be reduced by half if hypoglycemia and hypokalemia
persist.

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Benefits of this way of insulin therapy
-Easy Route
-constant dose
-comparable efficacy with the standard (i.e. 0.1IU/Kg/hr continuous infusion)
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➢ Delay initiation of K+ replacement until there is a reasonable urine put (>50


ml/hr)
➢ If you are able to get the serum potassium soon after patient
presentation
✓ If potassium is < 3.3 mmol/L → 60 mEq/L(03 vial) should be
added.
✓ If the initial serum [K+] is 3.3 to 4.5 mmol → give 40 mEq/L (02 Vial) of
potassium.
✓ If the serum [K+] is 4.6 to 5.5 → 20 mEq/L (01 vial) of potassium should
be added.
✓ If the [K+] is above 5.5 → potassium should be withheld in the initial
fluids.
✓ If rehydrating with ORS, no added potassium is needed

5.Treat complication of DKA Management


➢ Cerebral edema
➢ Hypoglycemia
✓ If the blood glucose falls below 70 mg/dl, give a bolus of 2 ml/kg
of 10% glucose and increase the glucose concentration of the
infusion.
✓ As far as possible Avoid hypoglycemia and Cerebral edema
➢ Hypokalemia
✓ Insulin can temporarily be reduced by half if hypoglycemia and
hypokalemia persists
➢ Non cardiogenic pulmonary edema
➢ Aspiration pneumonia
➢ Acute renal failure

Cerebral edema

➢ cerebral edema is the most important complication of DKA management


➢ Rare but often fatal, Mortality rate of up to 24%
➢ Often unpredictable; pathophysiology not well known
➢ Cerebral edema most commonly occurs in the first 12 hours, often secondary
to vigorous rehydration.
➢ Rehydration should occur more slowly in children with DKA.
➢ Strict observations throughout the 24 hours is mandatory.
➢ It accounts for the majority of deaths (60 to 90 percent) in DKA.
➢ From 10% to 25% of survivors of cerebral edema have significant residual
morbidity.

Who is at risk of Cerebral Edema?

➢ Administration of excess hypotonic fluids


➢ Those who took bolus of insulin
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➢ When RBS decreases by more than 100mg/dl/hr


➢ Infants and young children
➢ Higher sodium and BUN at presentation
➢ Rapid correction of PH with bicarbonate
➢ Severe acidosis
➢ Prevention is mandatory and very important

Diagnosis of cerebral edema

➢ It is a clinical diagnosis
➢ Neuroimaging is not required for diagnosis of cerebral edema
➢ 2 major or, 1 major and 2 minor (sensitivity of 92%)

Major criteria

➢ Altered mentation, confusion


➢ Age inappropriate incontinence
➢ Sustained heart rate decelerations more than 20 bpm (bradycardia)

Minor criteria

➢ Vomiting
➢ Headache
➢ Lethargy → decrease or fluctuation in level of consciousness
➢ Age < 5yrs
➢ Hypertension28
➢ Abnormal respiratory pattern.

Management of Cerebral edema

➢ Reduce the rate of fluid administration by 1⁄3rd


➢ Immediate IV Mannitol, 0.25 to 1 g/kg/dose (Usually 1 g/kg/dose), IV, infused
over 20 to 30 minutes (i.e. 5ml / kg 20% solution); repeat as needed (every 4-
6 hrs) to maintain serum osmolality <300 to 320 mOsm/kg
✓ Usual prescription → Mannitol, 1 g/kg/dose, IV, followed by a maintenance
dose of 0.5g/kg every 4-6hrs
➢ Elevate The head of the bed 30 degrees and give oxygen
➢ Intubation may be necessary for a patient with impending Respiratory failure

28
Hypertension occurs commonly in children with DKA and should not be considered a warning sign for
cerebral injury, in the absence of other findings.
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6. Precipitant identification and treatment


➢ Noncompliance, infection, trauma, emotional factors eg puberty or family crises
or exam at school.
➢ Through examination of every system is important
➢ Initiate appropriate workup for precipitating event (CBC, S/E, U/A, CXR,
cultures)
➢ If infection is suspected due to fever, start broad-spectrum antibiotics and send
appropriate investigations

7. Monitoring
➢ A well-organized follow up sheet ensures all parameters are being observed.
➢ Vital signs and mental status q 01 hour until the acidosis clears
➢ RBS q 1-2hr
➢ Urinary ketones q4hr
➢ Electrolytes, primarily Na+ and K+ baseline and every 24 hours, if possible
➢ Assess for complications

DKA follow up sheet


Date Time BP PR RR T0 Menta RBS Urine Urine Insulin dose input Out put sign
tion /1hr glucose/ ketone/ (IU, Sc)
4hrs 4hrs

MANAGEMENT OF DIABETES IN A HOSPITALIZED


CHILD AND ADOLESCENT PATIENTS

Types of Insulin
➢ In Ethiopia human insulin is the most commonly available form. This comes in
three forms:
✓ Short-acting (regular/soluble) - e.g. Actrapid, Humulin R
✓ Intermediate-acting - NPH insulin – e.g. HumulinI, NPH, Protaphane,
Insulatard
✓ Pre-mixed short-acting (regular) and intermediate-acting (NPH) insulins –
usually in the combination 30/70 or 25/75 → Preferred in Long term
management of pediatrics age T1DM

Insulin requirements (Dose)


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Table Reference; Nelson 21st edition

➢ Insulin requirement is based upon the body weight, age, and pubertal stage of
the child.
➢ In general, the newly diagnosed child requires an initial total daily insulin dose
of 0.5 to1.0 units/kg.
➢ Pre-pubertal children (outside the partial remission phase) usually require 0.5-
1.0 IU/kg/day.
➢ Pre-pubertal children usually require lower doses, and the dose requirement
may be as low as 0.25units/kg for a variable period following diagnosis mainly
during the partial remission phase (honey moon period).
➢ During puberty, requirements may rise substantially above 1 and even up to 2
U/kg/day.

Table; Insulin Dose OF TYPE1 DM Without DKA Based on Age

Age in year ➢ Insulin Dose (unit/kg/day)

1. ≤ 5 years and during ➢ ≤ 0.5


honey moon phase

2. 6 year ➢ 0.6

3. 7 year ➢ 0.7

4. 8 year ➢ 0.8

5. 9 year ➢ 0.9

6. ≥ 10 Years ➢ 1.0

➢ This will be a starting dose then we can decrease or increase the


dose based on their glucose level until we reach their target glucose
level.

Reference; National Training on DM for Health Care Workers, Participant’s Manual (Draft
Revised Version) Addis Ababa January 2021

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➢ Higher doses are needed in pubertal children, patients in ketoacidosis, or in


patients receiving glucocorticoid therapy.
➢ The ’correct’ dose of insulin is that which achieves the best attainable
glycaemic control for an individual child or adolescent, without causing obvious
hypoglycaemia, and resulting in normal growth and development.
➢ In infants and toddlers who receive their insulin by syringe, the insulin dose
may be so small that dilution is required to allow for easier and more precise
administration. The smallest dose of insulin that can be accurately administered
without dilution using a syringe is 0.5 units.

Table; Target Premeal and 30-Day Average Blood Glucose Ranges and the
Corresponding Hemoglobin A1c for Each Age Group #

#
Reference; Nelson Textbook of Pediatrics, 21st Edition

Table; Target Blood Glucose Ranges*

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*Reference; National Training on DM for Health Care Workers, Participant’s


Manual (Draft Revised Version) Addis Ababa January 2021

INSULIN REGIMENS

➢ The two most common regimens used are:


✓ Twice-daily insulin using both short-acting and also intermediate-acting
insulin.
☛ (If these insulins are not always available, pre-mixed insulin can be
used as an alternative regimen).
✓ Basal bolus regimen (the preferred option) - with short acting insulin given
with main meals (usually TID) and long acting /intermediate-acting insulin
given daily or BID (evening, or morning and evening).

➢ Insulin can also be given by an insulin pump but this is very expensive and
requires expert education to initiate and monitor therapy.

INITIATING INSULIN THERAPY IN A CHILD NOT IN DKA

➢ Admit Child
➢ Start the child on both NPH and regular insulin with the recommended dose
for his/her age based on their weight.
➢ Monitor blood glucose and document trends and watch for hypoglycemia
➢ Adjust the dose based on the glucose level

Exercise

➢ Calculate insulin dosing for a 7 years old child weighing 22kg child newly
diagnosed with Type 1 DM with no signs of DKA.

Answer

➢ 7 years old boy weighing 22 kg. At the start point here is the recommendation
➢ The recommended dose for this age 0.7 unit/kg/day. So the total daily dose is
15.4 units, we need to round off to 15 units. We need to avoid the fraction
when we write dose on the order sheet or on prescription (2/3 of the daily
dose to be given in the morning and 1/3 of the daily
dose in the evening and, 2/3 of the daily dose NPH and 1/3 of the daily dose
regular insulin)
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➢ So the morning dose will be 10 (2/3 of this will be 6.7 NPH and 1/3 of this
will be 3.3 regular, this is the calculation when we prescribe this, we need to
round off to 7 NPH and 3 Regular)
➢ The evening dose will be 5 (2/3 of this 3.3 and 1/3 of this 1.7 so we need to
round off these numbers to 3 units NPH and 2 units’ regular insulin)
➢ Usual recommended form of writing on the order sheet or on the prescription
is as follows:
➢ Morning 7/3 units and Evening 3/2 units (i.e. 7NPH/3RI morning and
3NPH/2RI evening) → in odd numbers better to round to the next even
number (e.g if 7 make it either 6 or 8)

Approaches of in insulin delivery


A) TWO INJECTIONS PER DAY

➢ A starting point is to give two-thirds of the total daily insulin in the morning
before breakfast and one-third before the evening meal.
➢ For mixed insulin, always think of the components separately (i.e. 10 units of
mix 70/30 equals 3 units of short-acting (regular) and 7 units of intermediate-
acting (NPH)), and adjust doses as above. Pre mixed insulin usually it is not
recommended in pediatrics .

B) BASAL BOLUS REGIMEN

A starting point is:

➢ If short-acting (regular) and intermediate-acting insulin is used, give:


✓ 70% of the total daily dose as short-acting (regular) insulin (divided up
between 3-4 pre-meal boluses)
✓ 30% of the total daily dose as a single evening injection of intermediate-
acting insulin
➢ If short-acting (regular) and long-acting analogue insulins are used, give:
✓ 60- 70% of the total daily dose as short-acting (regular) insulin (divided up
between 3-4 pre-meal boluses)
✓ 30-40% of the total daily dose as a single evening injection of long-acting
analogue insulin. (Sometimes this dose does not last for 24 hours and
then can be split into two doses morning and evening).

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MIXING INSULINS IN THE SAME SYRINGE

➢ It is very common to combine intermediate-acting and short-acting/rapid-acting


insulins, in order to cover both basal needs plus the extra need from eating.
➢ Short-acting insulin or rapid-acting analogues can be combined with
intermediate-acting insulins (e.g. NPH) in the same syringe.
➢ Begin by injecting air into both bottles.
➢ The short-acting insulin is generally drawn into the syringe first.
➢ If the intermediate-acting insulin is a “cloudy” insulin, mix by tipping the
vial/bottle up and down 10 – 20 times.
➢ Do not shake the insulin as these damages the insulin, RATHER ROLL OVER
THE HANDS To mix NPH
➢ The doses can be adapted every day according to food intake, physical
activity, and blood glucose readings.

Before Discharge; Basic and Advanced Diabetes Education For


Family and Adolescent patients about

✓ Nutritional Management
✓ Self-monitoring of blood glucose
✓ Insulin dose, storage, SC administration skill
✓ No form of exercise, including competitive sports, should be forbidden to
the child with diabetes
✓ Features of hypoglycemia and hyperglycemia and what to do if it happens

Table; Algorism for Insulin Initiation and dose adjustment in Type


1 Diabetes in Children and Adolescents

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Table; Screening Guidelines for Long-Term Complications

Further reading

➢ Nelson Textbook of Pediatrics, 21st Edition


➢ ISPAD Clinical Practice Consensus Guidelines 2022:
➢ National Training on DM for Health Care Workers, Participant’s Manual (Draft Revised Version)
Addis Ababa January 202
➢ STANDARD TREATMENT GUIDELINES FOR GENERAL HOSPITALS, FOURTH EDITION, 2021
➢ DKA protocol for Emergency and critical unit of Tikur Anbessa Specialized Hospital (TASH), By
Tigist Bacha, MD, MPH, Consultant pediatric emergency and critical care Specialist
➢ Pediatric Diabetic ketoacidosis management protocol, Tibebe Ghion specialized hospital ,
Bahirdar, Mastewal Ambaw (MD, Pediatrician), December 2019

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Chapter 11; AKI/Acute kidney injury/


and CKD/ Chronic kidney disease
(የኩላሊት በሽታ)
Dr. Mulualem. G, Dr. Robel. D

Clinical features and how to write hx of CKD patient


History

➢ Pt’s may present with


Generalized body swelling (GBS)
Vomiting
Decreased urine out put
Easy fatigability and ureamic complication
Symptoms of anemia
➢ GBS
▪ Site → swelling over the face and around the eyes (i.e. facial puffiness)
▪ Duration → long standing (e.g. 4 months duration)
▪ Progression… e.g. progress to the legs with in ‘’X’’ days and finally to
the whole body with in ‘’Y’’ days
▪ Diurnal variation → more prominent early in the morning/while s/he
awakes from sleep.
▪ How the pt noticed the swelling
▪ Painful or not → Mostly painless
N.B body swelling

➢ In cardic pt. →start from leg and goes upward


➢ In renal disease → begin from face (morning facial
puffines)
➢ In liver disease → start with abdominal distension which
may progress to GBS
➢ SOB → exertional dyspnoea
➢ Haematuria, flank pain (stabbing type of pain)
➢ Change in urine amount (oliguria, anuria → estimate the amount in terms
of ml per day) or in the other way frequency, urgency, dysuria…
After long period of these symptoms pt may present with vomiting
➢ Fever
High grade
Intermittent
Associated with night sweat, chills/rigor
➢ Weight loss 694
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Risk factors

➢ See etiologies of AKI from Discussion part below


➢ HTN → HTN and CKD are interchangeable cause of one another
➢ DM
➢ Dyslipidaemia,
➢ Sedentary life style
➢ Old age
➢ Auto immune disease (e.g. glomerulonephritis)
➢ Family history → RF for PCKD
➢ Previous AKI
➢ Drugs
Immunosuppressive drugs
Nephrotoxic drugs are reversible factor for renal failure (NSAID’s,
ACE-I/ARB, cyclosporin cause AKI 2ry to acute tubular necrosis →
CKD)
➢ African ancestors
➢ Evidence of kidney damage
Proteinuria
Abnormal urinary sediment (casts)
Structural urinary tract abnormality
➢ Aetiologies → top 5 aetiologies for CKD
1. Diabetic nephropathy → cmn cause of CKD in north America and
Europe
2. Glomerulonephritis → cmn cause of CKD in developing countries
(especially post streptococcal GN) like in our setup (Ethiopia)
3. Hypertensive nephropathy
4. PCKD
5. Cystic and tubule interstitial nephropathy

Complication of AKI

➢ Uremia and complications of uremia (asterixis, pericardial


rub or effusion, encephalopathy, uremic bleeding)
➢ Hypervolemia and hypovolemia
➢ Electrolyte disturbance
o Hyponatremia
o Hyperkalemia
o Hyperphosphatemia and Hypocalcemia
▪ Degree of Hyperphosphatemia and Hypocalcemia is moderate
when compared to CKD
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➢ Metabolic acidosis
➢ Hematologic complications
o Anemia
▪ The degree of anemia in AKI is usually mild to moderate
▪ Severe anemia is common in CKD and the cause is
Multifactorial.
o Bleeding
➢ Infections
o Infections are a common precipitant of AKI and also a dreaded
complication of AKI.
➢ cardiac complications of AKI
o Arrhythmias
o Pericarditis
o Pericardial effusion.
o In addition, volume overload and uremia may lead to cardiac injury
and impaired cardiac function.
➢ Malnutrition

Complication of CKD

➢ Fluid, electrolyte and acid base disturbance


➢ Disorders of calcium and phosphate metabolism
o Bone fracture, bone pain
➢ Cardiac and vascular calcification
o CAD/coronary arterial disease/
o CVD/cerebrovascular disease like stroke/
o PAD/peripheral arterial disease/)
➢ HTN and Left Ventricular Hypertrophy, DCMP, pericarditis, Heart Failure
➢ Anaemia → Causes of Anemia in CKD include
o Relative deficiency of erythropoietin
o Diminished red blood cell survival
o Bleeding diathesis
o IDA (Iron deficiency due to poor dietary absorption and GI blood
loss)
o Hyperparathyroidism/bone marrow fibrosis
o Anemia of chronic disease (Chronic inflammation
o Folate or vitamin B 12 deficiency
o Hemoglobinopathy
o Comorbid conditions: hypo-/hyperthyroidism, pregnancy, HIV-
associated disease, autoimmune disease, immunosuppressive drugs
➢ Uremic fetor
o a urea-like odor on the breath, derives from the breakdown of urea
to ammonia in saliva and is often associated with an unpleasant
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➢ Infection
o Patients having CKD also at risk for developing TB
➢ Ureamic Gastropathy, PUD
➢ CNS, ANS and PNS neuropathy
➢ Uremic encephalopathy
➢ Impaired Glucose metabolism
o Hypoglycaemia and DM treatment CXN → CKD with DM patients are
at risk of hypoglycemia because of decreased urinary insulin
excretion
o Iinsulin should be adjusted to prevent hypoglycemia
➢ Pruritus from uremia

Sample history

Sample hx of a pt’ from Maksegnit with a DX of AKI on CKD. (sample taken from
our friend Dr. Natnael Bedilu (GP), which was his round case during our C-I
attachment)

Chief compliant
GBS of 2 weeks duration

HPI
This patient was last relatively healthy 2 weeks back, at which time his father noticed
swelling around the eyes and face that was more marked early in the morning. Over
a period of 3 days the swelling progress to involve the abdomen and the legs then
becomes generalized. Concomitantly the patient starts to experience shortness of
breath which was felt initially while doing supra ordinary activities like going uphill’s
which later worsen over a week to be felt at ordinary activities like going 15minute
walk to the school he was attending associated with palpitation but no orthopnea,
PND, chest pain or intermittent claudication.

One week before admission, he started to experience a decreased in urine amount of


approximately 200 to 250ml per day, bilateral stabbing type of flank pain with no
radiation or a known aggravating or relieving factor but no frequency, urgency, pain
during micturition or urine color change.

In addition to this the patient was complaining of nausea, loss of appetite and dull
aching type of epigastric pain without radiation or any aggravating or relieving factor
but no history of vomiting, bowel habit change or weight loss. (ureamic sxx, ESRD, Gastritis
and PUD → CXN)

For this compliant he visited local health center at tseda where he was given
unspecified white oval tablet to be taken 3X per day prescribed for 10 days but he
discontinued the treatment since he was not getting any improvement of the
symptoms and he come to our hospital for better investigation and management.
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12 years back he had experienced reddish discoloration of urine and generalized


body swelling for which he was admitted at UOG hospital where he was told that he
was having kidney disease. He was then given unspecified tablets and injectable
medications and he was on salt free diet. After 3 weeks of hospital stay, he was
discharged with follow up and improved. He was relatively fine until the current
admission.
No hx of DM, HTN or asthma (DM and HTN cause CKD, DM cause 2ry nephrotic sxx →
RF)
No hx of drug intake other than those mentioned above (Drugs like
Aminoglycosides, NSAID’s, Metformin are RF for Intrinsic AKI and CKD)
No family hx of similar illness (RF for PCKD)
No hx of tinnitus, blurring of vision, light headedness or easy fatigability
(anaemia → CXN)
No hx of LOC, confusion, bizarre behaviour, forgetfulness, disturbance of
speech, visual disturbance or abnormal body movement (ureamic encephalopathy
→ CXN)
No hx of nasal/gum bleeding or bleeding from other sites (hematologic CXN of
CKD)
He has dyspnoea but no hx of chest pain, orthopnea or PND (IHD,
pericarditis, CHF → CXN of CKD or DDX for GBS)
No hx of malar rash, photosensitivity or joint pain (SLE cause 2ry Nephrotic SXX
→ DDX)
No hx of chronic cough, contact with chronic cougher or previous TB
treatment (TB enteritis, renal TB → DDX, Patients having CKD also at risk for developing TB)
No hx of RUQ abdominal pain, yellowish discoloration of the eye or
contact with a jaundiced person (CLD → DDX)

Finally, he was admitted to our hospital supported physically by his families

Physical examination (pertinent findings)

1 GA → coma (uremic encephalopathy)

2 Vital signs

➢ HTN → HTN as a cause of CKD or HTN 2ry to CKD


➢ OHT (orthostatic hypotension) → hypovolemia 2ry to extra cellular fluid
depletion, ANS neuropathy
➢ Tachypnoea → from uremic acidosis
➢ Tachycardia → extra cellular fluid depletion

3 HEENT

➢ Facial puffiness (part of GBS)


➢ Pale conjunctiva → anaemia

4 LGS
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5 RS

➢ Kussmaul’s breathing 2ry to uremic acidosis


➢ Pleural effusion (part of GBS)

6 CVS

➢ CHF features
➢ Pericardial friction rub and knock from pericarditis

7 Abdominal examination

➢ Ascites (part of GBS)

8 GUS

9 MSS

➢ Oedema (part of GBS)


➢ Bone tenderness and fracture
➢ PAD features

10 IS

11 NS

➢ Stroke features
➢ Coma

DDX for GBS

1. CKD
2. Nephrotic sxx
3. CHF
4. Constrictive pericarditis
5. CLD
6. Advanced Lymphoma (NHL)
7. Disseminated TB to pleura, Peritoneum…..
8. Hypothyroidism
9. ? PLE

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IX

U/A
✓ Abnormal sediment or cast
o Wax and broad casts, fat casts are commonly seen in CKD.
o Hyaline cast → suggest prerenal azotemia (prerenal AKI)
o RBC cast → RPGN
o WBC cast → Interstitial Nephritis or pyelonephritis
✓ Proteinuria (Albuminuria) → indicate kidney damage
✓ Haematuria → glomerulonephritis
Urine culture and sensitivity → UTI (Pyelonephritis)
RFT (BUN and Creatinine)
✓ Creatinine clearance (GFR) estimate by Cockcroft-Gault equation in
adults and older adolescents (age ≥18 years).
(140 − 𝑎𝑔𝑒) 𝑥 𝑤𝑒𝑖𝑔ℎ𝑡(𝑖𝑛 𝑘𝑔)
(𝑚𝑢𝑙𝑡𝑖𝑝𝑙𝑦 𝑡ℎ𝑒 𝑟𝑒𝑠𝑢𝑙𝑡 𝑤𝑖𝑡ℎ 0.85 𝑓𝑜𝑟 𝑓𝑒𝑚𝑎𝑙𝑒𝑠)
72 𝑥 𝑠𝑒𝑟𝑢𝑚 𝑐𝑟𝑒𝑎𝑡𝑖𝑛𝑖𝑛𝑒 𝑙𝑒𝑣𝑒𝑙 (𝑚𝑔/𝑑𝑙)

✓ BUN/creatinine ratio is normal at 10 to 15:1 in ATN (measured in


mg/dL), but is often > 20:1 in prerenal disease
✓ Serum creatinine rises progressively and usually at a daily rate > 0.3
to 0.5 mg/dL/day in ATN.

What is the relationship between Urea and BUN?

✓ Urea contains Nitrogen, Carbon, oxygen, hydrogen and the like.


From which 46 % is Nitrogen. Molecular Formula = CO(NH2)2
✓ Urea reflects the whole of the molecule (molecular weight/MW/ of
60).
✓ BUN reflects only the nitrogen content of urea (MW 28)
✓ Urea = 2.14 X BUN (since 60⁄28 = 2.14)

Serum albumin level (LFT) → hypoalbuminemia from albuminuria


RBS, FBS, HbA1C → To R/O diabetic nephropathy
CBC
✓ Anaemia → NcNc Anaemia
✓ Leucocytosis → UTI (Pyelonephritis)
Serum electrolyte → fluid and electrolyte disturbance in CKD
✓ Hyperkalaemia
✓ Hypokalemia
o Patients may also have hypokalemia due to interactable
ureamic gastropathy (vomiting) and poor intake.
✓ Hyperphosphatemia with hypocalcaemia in chronic renal failure
✓ Hyperuricaemia (raised level of uric acid)
Abdominal U/S
✓ Estimate renal size (if small kidney → CKD diagnosed possibly, if
normal size acute attack rather than chronic)
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✓ There are exceptions of CKD with normal or increased kidney size
such as
o PCKD
o HIVAN
o Diabetic Nephropathy
o Amyloidosis
✓ Other features of CKD in U/S
o Loss of corticomedulary differentiation
o Cortical thining and increased echogenicity
✓ To r/o Obstructive uropathy
Doppler U/S and MRA of renal artery
ECG, ECO, CXR → pericarditis (diffuse ST segment elevation), pericardial
effusion, CHF, LVH 2ry to HTN
Immunologic test → SLE, vasculitis
Renal Biopsy
✓ Reserved only for patients having near normal kidney size when Dx
by other Ix modality is difficult
✓ Renal biopsy in AKI
o If the cause of AKI is not apparent based on the clinical
context, physical examination, laboratory studies, and
radiologic evaluation, kidney biopsy should be considered.
o The procedure is most often used in AKI when prerenal
azotemia, postrenal AKI, and ischemic or nephrotoxic AKI
have been deemed unlikely, and other possible diagnoses are
being considered such as
▪ Glomerulonephritis
▪ Vasculitis
▪ interstitial nephritis
▪ myeloma kidney
▪ HUS and TTP
▪ allograft dysfunction.
o The kidney biopsy can provide definitive diagnostic and
prognostic information about AKI and CKD
o Kidney biopsy is associated with a risk of bleeding, which can
be severe and organ- or life-threatening in patients with
thrombocytopenia or coagulopathy.
✓ C/I to renal biopsy
– Bilateral small (shrunken) kidney → size < 8.5cm
– PCKD
– Uncontrolled HTN
– active urinary tract infection
– UTI / peri nephritis
– Bleeding diathesis
– Morbid obesity (BMI > 40 Kg/m2)
– Respiratory distress is relative C/I
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Discussion

11.1 Acute Kidney Injury (AKI)


AKI is defined by the impairment of kidney filtration and excretory function over
days to weeks, resulting in the retention of nitrogenous and other waste
products normally cleared by the kidneys.
AKI is not a single disease but, rather, a designation for a heterogeneous
group of conditions that share common diagnostic features: specifically, an
increase in serum creatinine (SCr) concentration often associated with a
reduction in urine volume.
AKI is a clinical diagnosis and not a structural one.
A patient may have AKI with or without injury to the kidney parenchyma.
AKI can range in severity from asymptomatic and transient changes in
laboratory parameters of GFR, to overwhelming and rapidly fatal derangements
in effective circulating volume regulation and electrolyte and acid-base
composition of the plasma.

Diagnostic Definition of AKI


➢ AKI is diagnosed if any one of the following criteria is fulfilled.
☛ Increase in serum creatinine from the baseline by > 0.3mg/dl, which
is known to have occurred occur in <48 hours. Or
☛ Increase in serum creatinine by 50% (1.5-fold) form baseline, which
is known or presumed to have occurred within one week (the prior
7 days). Or
☛ Urine output <0.5ml/kg/hr for ≥ 6 hours (for an average adult <
200ml/6 hours)

Staging AKI: According to the KDIGO (Kidney Disease Improving Global


Outcomes) staging, AKI is staged in to three.

Table. Staging of AKI according to KIDGO*


Stages Creatinine-based Urine-out put base

Stage 1 Increase from baseline: 1.5 - 1.9 < 0.5 ml/kg/h for 6 - 12
times (>50% but <100%) or > hours
0.3mg/dl
Stage 2 Increase from baseline 2.0 -2.9 Urine output < 0.5 ml/kg/h for
times (>100% but < 300%) ≥ 12 hours
Stage 3 Increase from baseline ➢ <0.3 ml/kg/h for >24 hours
➢ 3 times (>300%) OR OR
➢ An increase to a level >4.0 ➢ Anuria for >12 hour
mg/dl Or
➢ Initiation of renal replacement
therapy
* KIDGO is a modification to RIFLE (Risk, Injury, Failure, Loss, ESRD) and AKIN
.
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Distinction between AKI and CKD


The distinction between AKI and CKD is important for proper diagnosis and
treatment.
The distinction is straightforward when a recent baseline SCr concentration is
available, but more difficult in the many instances in which the baseline is
unknown.
In such cases, clues suggestive of CKD
o Radiologic studies (e.g., small, shrunken kidneys with cortical thinning on
renal ultrasound, or evidence of renal osteodystrophy)
o Normocytic anemia in the absence of blood loss
o Secondary hyperparathyroidism with hyperphosphatemia and hypocalcemia,
consistent with CKD.
o Old records of elevated Cr (i.e. constantly elevated creatinine like 4.0, 3.9,
3.5, 4.3…..)
o Symptoms of uremia
o Patients having underlying uncontrolled or poorly controlled HTN and DM
o Previous history of AKI
No set of tests, however, can rule out AKI superimposed on CKD because
AKI is a frequent complication in patients with CKD, further complicating the
distinction.
Serial blood tests showing a continued substantial rise of SCr represents clear
evidence of AKI.
Once the diagnosis of AKI is established, its cause needs to be determined
since the elevation of SCr or reduction in urine output can be due to a large
number of physiological and pathophysiological processes.

Etiologies and pathophysiology


The causes of AKI have traditionally been divided into three broad categories:
prerenal azotemia (55%), intrinsic renal parenchymal disease (40%), and
postrenal obstruction (5%)

1. Prerenal azotemia (55%)


➢ Prerenal azotemia (from “azo,” meaning nitrogen, and “-emia,” meaning
in the blood) is the most common form of AKI.
➢ It is the designation for a rise in SCr or BUN concentration due to inadequate
renal plasma flow and intraglomerular hydrostatic pressure to support normal
glomerular filtration.
➢ The most common clinical conditions associated with prerenal azotemia are
✓ Hypovolemia (any cause e.g. Burns and Acute Pancreatitis, bleeding,
profuse vomiting…)
✓ decreased cardiac output (Heart Failure), and
✓ medications that interfere with renal autoregulatory responses such
as NSAID and ARB
2. Intrinsic renal parenchymal disease (40%)
➢ The most common causes of intrinsic AKI are
✓ Sepsis
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✓ Ischemic acute tubular necrosis (ATN) and
✓ Nephrotoxic ATN → both endogenous and exogenous. Examples include
▪ antibiotics (aminoglycoside and amphotericin B, Vancomycin,
penicillins, cephalosporins, quinolones, sulfonamides, and
rifampin.)
▪ Aminoglycosides are commonest causes of nephrotoxic ATN (in
this case polyuria is common presentation rather than oliguria)
▪ antiviral drugs (e.g. Acyclovir, Foscarnet, pentamidine, tenofovir,
and cidofovir)
▪ intravenous iodinated contrast
▪ Chemotherapeutic Agents (e.g. Cisplatin, carboplatin,
bevacizumab, mitomycin C and gemcitabine)
▪ Toxic Ingestions (e.g. Ethylene glycol)
▪ Endogenous Toxins (e,g. myoglobin from Rhabdomyolysis,
hemoglobin from massive hemolysis, uric acid, and myeloma
light chains.)
➢ In many cases, prerenal azotemia advances to tubular injury classically termed
“acute tubular necrosis
➢ other less common causes of intrinsic AKI include
✓ acute glomerulonephritis
✓ acute interstitial nephritis

3. postrenal obstruction (5%)

Postrenal AKI occurs when the normally unidirectional flow of urine is acutely
blocked either partially or totally, leading to increased retrograde hydrostatic
pressure and interference with glomerular filtration
For AKI to occur in individuals with two healthy functional kidneys, obstruction
must affect both kidneys in order to observe large increases in SCr.
Unilateral obstruction may cause AKI in the setting of significant underlying
CKD or, in rare cases, from reflex vasospasm of the contralateral kidney.
Obstruction to urinary flow may be caused by functional or structural
derangements anywhere from the renal pelvis to the tip of the urethra
Causes of obstruction include
o Bladder neck obstruction is a common cause of postrenal AKI
▪ BOO (Bladder outlet obstruction)
▪ Prostate cancer
▪ Neurogenic bladder, or
▪ therapy with anticholinergic drugs.
o Obstructed Foley catheters (if not recognized and relieved.)
o Urethral strictures
o bilateral ureteral obstruction
o Stones, blood clots, external compression, tumor, retroperitoneal fibrosis

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Figure; Classification of the major causes of acute kidney injury.


ACE-I, angiotensin-converting enzyme inhibitor-I; ARB, angiotensin receptor blocker; TTP-HUS,
thrombotic thrombocytopenic purpura–hemolytic-uremic syndrome.

The cause of AKI in a single patient can be multiple (multifactorial). This


particularly true in critically sick hospitalized patients.
Whenever a diagnosis of AKI is made, the specific etiology/etiologies should be
carefully searched.
AKI is a common problem clinical problem; it is much more common in
hospitalized patients than in the community.
The common causes of dialysis requiring AKI in Ethiopia used to be severe
malaria and septic abortion but recently there is a significant shift in the
etiology. Hypovolemia with or without sepsis, glomerulonephritis, and obstetric
causes (mainly driven by pre-eclampsia) are the leading causes.
The elderly, diabetics, patients with underlying CKD, patients with heart failure
or liver disease are at high risk of developing AKI.

Clinical features
➢ The clinical features of AKI are dominated by those of the underlying cause
unless the AKI is severe.
Symptoms
Prerenal azotemia should be suspected in the setting of vomiting, diarrhea,
glycosuria causing polyuria, and several medications including diuretics,
NSAIDs, ACE inhibitors, and ARBs
A reduction in urine output (oliguria, defined as <400 mL/24 h) usually denotes
more severe AKI (i.e., lower GFR) than when urine output is preserved.
Red or brown urine may be seen with or without gross hematuria
Fatigue
Body swelling
Shortness of breath
Poor appetite, nausea and vomiting
Hiccups
Bleeding, mucocutaneous
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Symptoms of the underlying cause: e.g. tea/cola colored urine in
glomerulonephritis, fever in sepsis/malaria

Signs

Orthostatic hypotension, tachycardia, reduced JVP, decreased skin turgor, and


dry mucous membranes are often present in prerenal azotemia.
Peripheral edema
Signs of pulmonary congestion: bilateral lower lung zone crackles
Signs of pleural effusion or ascites
Change in mental status/flapping tremor/seizure
Signs of pericarditis or pericardial effusion
Signs of the underlying disease: e.g. Cutaneous and joint manifestations in SLE
with glomerulonephritis, low BP and signs of dehydration in patients with pre-
renal azotemia or ischemic ATN

Investigations and diagnosis


Diagnosis
➢ The diagnosis of AKI is made based on serum creatinine and/or urine output
criteria mentioned above. See the diagnostic and staging criteria above.
➢ Differentiating AKI from chronic kidney disease (CKD) is very important,
although it might not always be straight forward.
➢ The presence of a previous creatinine determination helps in differentiating AKI
from CKD.
➢ Bilateral small sized kidneys (<9cm longitudinally) indicate CKD; however, not
all patients with CKD have small size kidneys.

Investigations
Serum urea and creatinine
Urinalysis

Figure; Interpretation of urinary sediment findings in acute kidney injury (AKI). 706
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ATN, acute tubular necrosis; GN, glomerulonephritis; HUS, hemolytic-uremic syndrome; RBCs,
red blood cells; RTE, renal tubular epithelial; TTP, thrombotic thrombocytopenic purpura; WBCs,
white blood cells.

Serum electrolytes
Abdominal ultrasound: to exclude urinary tract obstruction and assess kidney
size
Other investigation should be done based on the suspected specific cause
Renal biopsy:

Treatment of AKI
Objectives of treatment
➢ Correct reversible causes of AKI
➢ Avoid worsening of kidney injury
➢ Maintain normal volume and electrolyte status
➢ Avoid overdoses of medications with renal clearance
✓ Dose adjustment of Nephrotoxic drugs for those having AKI to decrease
worsening

The management of individuals with and at risk for AKI varies according to the
underlying cause
Common to all are several principles

Non pharmacologic treatment

1. Maintain Fluid & electrolyte balance


✓ Strict fluid input and output chart or daily weighing
☛ For pre renal AKI the management is fluid replacement since it is
caused by fluid loss.
✓ Decrease salt intake in fluid overloaded patients
✓ Free water restriction in hyponatremia
✓ Decrease foods rich in potassium
✓ Avoid nephrotoxic drugs related to pre renal insult (ACE- I, NSAIDs)
2. Surgical intervention: For obstructive uropathy
3. Prevent further kidney injury
✓ Avoid nephrotoxic medications and radiocontrast agents
✓ Adjust doses of medicines with renal clearance
✓ Treat Heart Failure
4. Dialysis: if the patients live far from a hospital with dialysis service, referral
should be made before the indications for dialysis develop.
 Indications for dialysis → Indications for urgent dialysis (when
condition refractory to conventional therapy): Mnemonics → AEIOU
✓ Acid-base disturbance → academia (metabolic acidosis)
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✓ Electrolyte disorder → refractory hyperkalemia /> 6.5 mmol/l/,
hypercalcemia (tumor lysis)
✓ Intoxication → methanol, ethyleneglycol, salicylates
✓ Overload of volume i.e. refractory fluid overload (Pulmonary
edema and anuria)
✓ Uremia (severe complications of uremia) → asterixis, pericarditis,
encephalopathy, uremic bleeding

Pharmacologic treatment
➢ There is no specific pharmacologic treatment for AKI caused by ischemic or
nephrotoxic acute tubular necrosis.
➢ The specific treatment depends on the cause of the AKI.
➢ Intravenous fluids
✓ Indicated only in patients who are hypotensive or dehydrated on clinical
evaluation.
✓ In patients with hypovolemia or clinical hydration, fluids should be given to
keep the fluid balance in the positive side.
✓ Do not give (“challenge’) fluid for all patients unless there is evidence of
volume depletion)
✓ Urine output and fluid balance should closely followed as oliguric patients
can easily develop pulmonary edema.
➢ Furosemide:
✓ Indicated in patients with signs of fluid overload (edema, evidence of
pulmonary congestion or high BP)
✓ Starting dose 40mg, intravenously. If no response increase the dose every
1-2 hour till adequate response.
✓ Do not go beyond 200mg/dose.
✓ Doses above 100mg should be given diluted (1-2mg/ml of fluid) and given
slowly (4mg/min).
☛ E.g. 200mg in 100ml NS/01 hr, 160mg in 100mL NS/ 40min
✓ Response can be considered adequate, if the urine output is 50-100ml in
01 hour, or 100-200ml in 02 hours.
➢ Treatment of hyperkalemia → Click and see section on

➢ 14.2.2 Hyperkalemia
➢ Treatment of hypertensive emergency → see section on hypertension from
chapter one (click here → Hypertension (የደም ግፊት) and HHD)
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➢ Treatment of specific cause:

The following patients with AKI need to be managed in a hospital with a


nephrology and dialysis services.
o Worsening AKI despite efforts to manage the possible causes
o Glomerulonephritis considered to be the cause of AKI
o AKI of unknown etiology
o Any indications for dialysis

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Prevention
➢ A significant proportion of AKI is preventable.
✓ Rapid and adequate fluid replacement in volume depleted patients
✓ Early detection and management of sepsis, malaria, pre-eclampsia
✓ Avoiding nephrotoxic medications in high risk patients, whenever possible
e.g. NSAIDS, aminoglycosides, iodinated intravenous contrast agents.
✓ Close monitoring of renal function and urine output in hospitalized patients
✓ Dose adjustment of drugs with renal clearance.

Outcome and Prognosis


Prerenal azotemia carries a better prognosis than most cases of intrinsic AKI.
o Exception of the cardiorenal and hepatorenal syndromes, and postrenal
azotemia
The kidneys may recover even after severe, dialysis-requiring AKI.
Survivors of an episode of AKI requiring temporary dialysis, however, are at
extremely high risk for progressive CKD, and up to 10% may develop ESRD
(end-stage renal disease).
Post discharge care under the supervision of a nephrologist for aggressive
secondary prevention of kidney disease is prudent.
Patients with AKI are more likely to die prematurely after they leave the
hospital even if their kidney function has recovered.

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11.2 Chronic Kidney Disease (CKD)

CKD is defined as the presence of kidney damage for more than 3 months as
evidenced decreased GFR of < 60m/min or the presence of other markers of
kidney damage with or without decreased GFR
Other makers of kidney damage
o Abnormalities on urinalysis: Persistent proteinuria is the most important
one.
o Abnormalities on imaging: shrunken kidneys, polycystic kidneys,
hydronephrosis.
o Histologic abnormalities findings on renal biopsy specimens
CKD encompasses a spectrum of pathophysiologic processes associated with
abnormal kidney function and a progressive decline in GFR.
The risk of CKD progression is closely linked to both the GFR and the amount
of albuminuria.
For determination of estimated GFR in adult patients with stable serum
creatinine, use the MDRD (Modification of Diet in Renal Disease Study) or
CKD-EPI (Chronic Kidney Disease Epidemiology Collaboration) formula, which
are freely accessible on line.

In our setup, during our internship, we were using Cockcroft-Gault equation for
GFR estimation, since it was easy for calculation (we used it from UpToDate
2018, we are not sure for the approval by KIDGO)
o Creatinine clearance (GFR) estimate by Cockcroft-Gault equation in adults
and older adolescents (age ≥18 years).
(140 − 𝑎𝑔𝑒) 𝑥 𝑤𝑒𝑖𝑔ℎ𝑡(𝑖𝑛 𝑘𝑔)
𝐺𝐹𝑅 =
72 𝑥 𝑠𝑒𝑟𝑢𝑚 𝑐𝑟𝑒𝑎𝑡𝑖𝑛𝑖𝑛𝑒 𝑙𝑒𝑣𝑒𝑙(𝑖𝑛 𝑚𝑔/𝑑𝑙)

(𝑚𝑢𝑙𝑡𝑖𝑝𝑙𝑦 𝑡ℎ𝑒 𝑟𝑒𝑠𝑢𝑙𝑡 𝑤𝑖𝑡ℎ 0.85 𝑓𝑜𝑟 𝑓𝑒𝑚𝑎𝑙𝑒𝑠) 712


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The five most frequent causes of CKD, cumulatively accounting for >90% of
the CKD disease burden worldwide (Relative contribution of each category varies
with geographic region and race)
o Diabetic nephropathy
o Glomerulonephritis
o Hypertension-associated CKD
o PCKD (polycystic kidney disease) / Autosomal dominant form/
o Other cystic and tubulointerstitial nephropathy
End stage renal disease (ESRD) → refers to a state of advanced CKD with
estimated GFR being < 15ml/min where lifelong renal replacement therapy
(dialysis or kidney transplantation) is necessary to sustain a reasonable quality
of life and survival.

KDIGO (Kidney Disease Improving Global Outcome) classification


of CKD

Table. KIDGO Classification of CKD based on CAG (cause, albuminuria and GFR)
GFR categories (ml/min/1.73 m2) description and range
Categories (G) Description GFR (ml/min/1.73m2)
G1 Normal or high ≥ 90
G2 Mildly decreased 60-89
G3 G3a Mildly to moderately 45-59
decreased

G3b Moderately to severely 30-44


decreased
G4 Severely decreased 15-29
G5 Kidney failure <15
Persistent albuminuria or proteinuria categories description and range
Category (A) Description 24hr urine albumin 24hr urine protein (mg)
(mg)
A1 Normal to mildly < 30 <150
increased
A2 Moderately increased 30-300 150-500
A3 Severely increased >300 >500
CAUSE (C):
Determine possible cause by taking history, physical examination and doing relevant
investigations.
➢ Diabetic Nephropathy
➢ Primary glomerular disease (Glomerulonephritis)
➢ Hypertension associated CKD
➢ PCKD
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➢ Obstructive uropathy
➢ Autoimmune diseases

Clinical features
Symptoms
Generally asymptomatic in the early stages (Stages 1 and 2 /i.e G1 and G2/CKD are
usually asymptomatic)
As CKD advances some non-specific symptoms might develop
Common but nonspecific symptoms:
o Nocturia
o Fatigue
o Loss of appetite, nausea, vomiting, hiccup
o Weight loss
o Muscle cramps, paresthesia
o Pruritus
o Body swelling, shortness of breath
o Sleep disturbance, depression, anxiety, sexual dysfunction
Signs
There are specific signs for CKD.
Early stages of CKD might not have any signs apart from signs of the
underlying disease
Advanced stages
o Edema, pleural effusion or crackles on lower lung field
o Dry skin, excoriation marks, papular eruptions, uremic frost
o Pericardial friction rub or distant heart sounds
o Uremic fetor, decrement in cognition, flapping tremor, lethargy

Investigations and diagnosis


Diagnosis
➢ The diagnosis is of CKD is made based on the KDIGO criteria mentioned
above.
➢ Once the diagnosis of CKD is established cause identification and staging
should be made based on the CAG system (C-cause A-albuminuria level and
G-GFR level).
➢ Example if a patient with CKD presumed to be due to diabetic kidney disease
has eGFR of 40m/min and 24hr protein is 1200mg.
C= Diabetes G=G3b A= A3 (Stage: G3b A3 CKD due to diabetic kidney
disease)

Investigations
Serum creatinine and urea: Estimated GFR
Urinalysis
Quantification of proteinuria or albuminuria: 24urine protein/albumin, spot urine
albumin to creatinine ratio (ACR)
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Abdominal ultrasound
Calcium, Phosphate, PTH levels (preferably intact PTH level than total PTH)
Alkaline phosphatase
Serum electrolytes
Abdominal ultrasound
CBC

Estimated GFR (eGFR) should be used for follow up of patients with CKD
than serum creatinine alone

Treatment of CKD

Objectives of treatment
Slow the progression of decline in GFR
Prevent, detect and manage complications
Improve quality of life and survival

Principles of CKD management:


➢ Establish the cause of CKD and treat (if possible)
➢ Identify and manage unexpected (acute) deterioration in kidney function
➢ Preventing or slowing disease progression
➢ Treatment of the complications
➢ Identification and adequate preparation for RRT

1. Treatment of reversible causes

Surgical management of Urinary tract obstruction


Management of Fluid loss, sepsis etc.

2. Slowing the rate of progression

General health advice e.g. smoking cessation, weight reduction for obese
individuals
Restrict salt intake
Dietary protein reduction
o Physicians should not overemphasize on protein restriction as the benefits
are modest.
o In malnourished individuals, which many advanced CKD patients are,
protein restriction should not be advised.
Medication Dose Adjustment
o Some drugs that should be avoided include
▪ Metformin and other oral anti-hyperglycemics that are eliminated by the
kidney. → Metformin should be restricted for stage II and above CKD.
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▪ NSAIDs
▪ Meperidine
o Many antibiotics, antihypertensives, and antiarrhythmics may require a
reduction in dosage or change in the dose interval.
o Several online Web-based databases for dose adjustment of medications
according to stage of CKD or estimated GFR are available (e.g.
http://www.globalrph.com/ index_renal.htm).
o Or you can search a specific drug dose adjustment for renal impairment, from
UpToDate as shown in the picture below

Picture; diagrammatic example on, how to search, a specific drug dose adjustment
for renal impairment, from UpToDate

o Nephrotoxic radiocontrast agents and gadolinium should be avoided or


used according to strict guidelines when medically necessary
Treatment and control of hypertension
o Target blood pressure < 130/80 mmHg
▪ HTN should be controlled in CKD since it is one of the progression
factor
o First line: ACE inhibitors or angiotensin receptor blockers (ARBs)…see
section on hypertension from chapter one for the options (click here →
Hypertension (የደም ግፊት) and HHD).
▪ Avoid ACE inhibitors/ARBs if patient has hyperkalemia.
▪ Serum creatinine and potassium should be followed one to two weeks
following initiation or dose increment.
▪ If serum potassium or creatinine can’t be followed, don’t start ACE
inhibitors/ARBs in patients with CKD.
▪ Up to 20-30% increment in creatinine is expected; hence, if the rise in
creatinine is less than 30%, the ACEi/ARB needs to be continued with
close monitoring. If the increase is above 30% or <30% but
progressively increasing, the drug should be discontinued.
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o Add-on and Alternatives
▪ If BP is not controlled to the target with ACE inhibitors/ARBs or ACE
inhibitors are contraindicated, add or replace by other antihypertensive.
▪ Long acting calcium channel blocker (CCB): Amlodpine or
sustained/extended release Nifedipine OR
▪ Loop diuretics (if eGFR is <30m/min) or thiazide diuretics ( if
GFR>30ml/min) OR
▪ A combination of long acting CCB and diuretics (loop or thiazide,
based on the eGFR)
▪ If the above three (ACEi/ARB + CCB + diuretic) or two (CCB +
Diuretic) fail achieve target BP add a beta-blocker.

Treatment and control of proteinuria


o First line
▪ ACE inhibitors or ARBs.
• ACE inhibitors (particularly Enalapril) are preferred over ARBs due
to their low cost and wide availability

First line

• Enalapril: starting dose 5mg BID, Maximum dose 20mg BID…

Alternatives

• Lisinopril: starting dose 5mg/day, Maximum dose 40mg/day


• Perindopril: starting dose 5mg/day. Maximum dose 15mg/day

ARB’s

• Telmisartan: Starting dose: 40mg/day maximum dose 80mg/day


• Irbesartan: Starting dose: 75-150mg/day, maximum dose
300mg/day
• Losartan: Starting dose 50mg/day maximum dose 100mg/day
• Valsartan: Starting dose 80 -160mg/day, maximum dose
320mg/day
• Candesartan: Starting dose 8-16mg/day maximum dose 32mg/day

Control of hyperglycemia in Diabetes


o In early CKD good blood sugar control is essential and helps to decrease
progression of CKD.
o In advanced CKD (Stage G4 and above or in patients on dialysis) the risk
of hypoglycemia is very high and tight glycemic control should be avoided.
o Although individualization based on age, expected survival, rates of
hypoglycemia, additional comorbidities is need, in patients with
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eGFR<30ml/min a HbA1C target of about 7.5% is acceptable (if achieved
without significant hypoglycemia)
o In patients with advanced CKD eGFR <30ml/min
▪ Metformin should be discontinued.
▪ Long acting sulfonylureas (particularly the commonly used
Glibenclamide) should be avoided.
▪ nsulin based therapy is preferred.

3. Treatment of the complications

Treatment of anemia of CKD


o Cause of anemia is multifactorial in CKD. So, cause should be identified
first.
o Indications to start treatment: Hemoglobin < 10g/dl or symptomatic.
o Iron
▪ Serum iron studies: Ferritin and transferrin saturation (TSAT) helps to
guide iron therapy
Serum iron
TSAT = 𝑋 100%, TIBC = Total Iron binding capacity
TIBC
▪ TSAT < 20% should be treated with iron.
▪ If iron studies cannot be done, most patients with CKD are iron
deficient and should be started on therapeutic iron.
▪ Ferritin can be high even in iron deficient CKD patients; hence high
ferritin should not be a reason to differ iron.
▪ Preferred: Intravenous iron
o Iron sucrose
▪ For patients not on hemodialysis:
• Iron sucrose 200mg, IV, administer over 5 minutes, every 3 days
for a total of 5 doses (a total of 1000mg). This dose is usually
sufficient but if hemoglobin is not corrected, additional doses can
be given. OR
• Iron sucrose 200mg diluted in 100ml NS; administer over 30
minutes.
▪ For patients on hemodialysis
• Iron sucrose 100mg, IV, over 2-5 minutes, given early during
dialysis sessions (within the first hour) until iron deficiency is
corrected. It needs to be given again, if iron deficiency persists or
recurs.
▪ Alternative: Options
• Ferrous sulfate, 325mg (65mg elemental iron) before meal OR
• Ferrous gluconate, 325mg P.O. (39mg elemental iron), 1-2tabs,
TID OR
• Ferrous fumarate, 325mg P.O., (107 elemental iron), one tab, daily
to twice per day.
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▪ For patients who do not tolerate ferrous sulfate tablets, they may be
advised to take it with meals, or to take a smaller dose, or elixir
(solution) forms.
• Iron hydroxide polymaltose syrup (Each 5ml contains 50mg
elemental iron), 10ml PO, BID to TID. OR
• Ferrous gluconate syrup (Each 5ml contains 24mg elemental iron),
15ml, PO TID.OR
• Ferric ammonium citrate syrup (Each 15ml contains 32.8mg
elemental iron), give 30ml, TID.

Erythropoiesis stimulation agents (ESA):

Epoetin (alpha/beta) → Erythropoitin stimulating agents


o Initiate if Hemoglobin is < 10g/dl after iron therapy.
o CKD patients on hemodialysis
▪ Initial dose: 4000IU, IV, 3 times a week
o CKD patients not on dialysis
▪ Initial dose: 4000IU, SC, 3 times a week
o Dosage adjustments for CKD patients (either on dialysis or not on
dialysis):
o Do not increase dose more frequently than every 4 weeks (dose
decreases may occur more frequently).
▪ If hemoglobin does not increase by >1 g/dl after 4 weeks: Increase
dose by 25%
▪ If hemoglobin increases >1 g/dl in any 2-week period: Reduce dose
by 25-50%
o Expected complication of Erythropoitin stimulating agents
▪ Increased risk of thrombo embolic conditions
▪ HTN
▪ Headache
▪ Urticarial…..

Treatment of hyperphosphatemia:
o Phosphate binders are indicated if serum phosphorus is > 5.5mg/dl

First line
o Sevelamer (as hydrochloride or carbonate)
▪ Initial dose 800mg, PO, TID with meal. If serum phosphorus >9mg/dl,
1600mg, PO TID can be started.
▪ Adjust the dose to target to a target serum phosphorus near normal

Alternative:
(< 5.5mg/dl)
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o Calcium carbonate: starting dose 500 - 1000mg, PO, TID, chew, with meal
o Calcium acetate: starting dose 1334mg, PO, TID with meal
o If total serum calcium increase >10mg/dl: hold calcium
o If there is hypocalcemia, calcium-based phosphate binders are preferred
over sevelamer.

Treatment of secondary hyperparathyroidism


o The main stay of treatment is correcting phosphorus and serum calcium
o Serum PTH (preferably intact PTH) should not be overcorrected: 2-9 times
the upper limit of normal is acceptable.
o If PTH level is above nine times the upper limit after correction of
phosphorus and calcium use either of the following: Calcitriol or synthetic
vitamin D analog (alfacalcidol or paricalcitol).
▪ Alfacalcidol: starting dose 2.5 to 5 µg/day. OR
▪ Paricalcitol: starting dose 1 µg/day or 2 µg 3x/week. OR
▪ Calcitriol: 0.25 - 0.5 µg /day

Treatment of fluid overload (edematous state)


o Furosemide, 40-120mg, PO/IV, BID or TID.
o Higher dose and more frequent dosing intervals are required in advanced
CKD.

Treatment of hyperkalemia → click and see section on 14.2. Electrolyte


disturbance, sub-section

14.2.2 Hyperkalemia from short case of Nitsbin

4. Identification and adequate preparation for RRT

Renal replacement therapy (RRT) for ESRD: Dialysis and kidney


transplantations are the options
o Renal transplantation is the preferred modality of RRT
o Preemptive kidney transplantation is preferable (Before initiating dialysis)
Indications for RRT
o For preemptive kidney transplant: patients with GFR <20ml/min are
candidates
o For dialysis → hemodialysis or peritoneal dialysis
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▪ Hemodialysis
• Effective than peritoneal dialysis. So, it is the preferred way of
dialysis
• Mechanism → Diffusion and ultra filtration
▪ peritoneal dialysis → cost effective but it have risk of infection
▪ Patients with GFR<15ml/min and symptomatic
▪ Starting dialysis based on low GFR alone without symptoms is not
beneficial.

N.B.

Cardiovascular complications are common cause of mortality in CKD patients


All AKI/CKD Patients need nephrologist evaluation. But, in the following
conditions, Nephrologist intervention in referral setup is mandatory.
o Patients with known causes of CKD (e.g. diabetic kidney disease,
obstructive uropathy) when the GFR is less than 30ml/min.
o If the cause of CKD is not known or suspected to be glomerular disease

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syndrome/Nts/)

Chapter 12; Glomerular disease


(Nephrotic syndrome/NS/ and
Nephritic syndrome/Nts/)
Dr. Mulualem. G

Clinical features and how to write hx of NS/NtS pt’


History

Characterization of patient history

➢ Pt’s may present with


o GBS
GBS
o Insidious in onset
o 1st started from periorbital area
o Worsen in the morning and relieved during day time
o Few days to weeks later the swelling starts to involve the legs,
abdomen and become Generalized
Hematuria (NtS)
Decreased UOP (oliguria), Foaminess of urine (Proteinuria)
Low grade intermittent fever
Days to weeks before the onset of illness
o Pussy patch on the scalp (Pyoderma) later become red and bogy
with scaling and hair loss
o Skin lesions in the other body part
o Sore throat

N.B
PSGN usually develops
▪ 1 to 2 weeks after sore throat (Pharyngitis)
▪ 3 to 6 weeks after skin infection (Pyoderma)
Vomiting → non projectile, non bilous, non-blood tingled, non-foul-
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Diarrhoea → unquantified/ quantified (E.g. Voluminous), non-bloody, non-
mucoid, non foul smelling, watery/not, diarrhoea of “x” to “y” times per
day
Abdominal pain
Sunkening of the eyes
Loss of appetite

Risk factors

For NS

✓ Common in males → Male to female ratio = 2;1 in NS


✓ Age = NS is common in children 2 to 6 years
✓ Preciding Viral infection

For NtS (APSGN)

✓ Common in males → Male to female ratio = 2;1 in NS


✓ Age = NtS is also common in children 5 to 12 years
✓ Poor hygiene
✓ Low socioeconomic status
✓ Preceding bacterial infection → pyoderma, pharyngitis
✓ Genetics → common in siblings

Complication of NS/NtS

Complication of NS
➢ Infection → S. pneumonia, E.coli
✓ Infection is because of
☛ Urinary loss of protiens like Ig and properdin factor B
☛ Edema is culture media for bacteria
☛ Defective cell mediated immunity
☛ Immune suppressive treatment
✓ Examples of infections include
☛ Spontaneous peritonitis
☛ Sepsis
☛ Pneumonia
☛ Cellulitis
☛ Recurrent UTI
☛ Scrotal swelling
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➢ Thrombosis
✓ This is due to
☛ Loss of anti-thrombin II, protein C and S
☛ Relative Immobilization
✓ Examples include
☛ Bilateral Renovascular thrombosis
▪ The worrest cxn which is extremely fatal but rare in
occurrence
▪ Clinical features → flank pain, headache ( from HTN),
vomiting, massive hematuria, proteinuria, palpable flank
mass
☛ Pulmonary embolism
☛ Sagittal sinus thrombosis
☛ Indwelling arterial and venous thrombosis

Complication of NtS (APSGN)


➢ ARF
➢ Cxn of HTN and Hypervolemia → N.B. around 60 % of APSGN patients
will develop HTN
✓ CHF
✓ Hypertensive encephalopathy (10)
➢ Electrolyte and metabolic disturbance
✓ Hyperkalemia
✓ Hypocalcemia → Tetany
✓ Hyperphosphatemia
✓ Acidosis
✓ Uremia
➢ Seizure

Sample history

Sample history of a patient from Debark with the DX of Acute PSGN +


Stage II HTN

C.C → GBS of 10 days duration

HPI
This patient was last relatively healthy 10 days back at which time he
experienced Insidious onset of body swelling which 1st started from
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periorbital area, Worsen in the morning and relieved during day time.
Seven days prior to admission, the swelling starts to involve the legs,
abdomen and become Generalized with in 2 days. Associated with this he
had redish discoloration of urine, decreased Urine amount together with low
grade intermittent fever but no Foaminess of urine Days to weeks before
the onset of illness

Two months prior to his illness he had pussy patch on the scalp and
skin which later become red and bogy with scaling and hair loss but no
Sore throat

Two weeks before admission he experienced non projectile, non bilous,


non-blood tingled, non-foul-smelling vomiting of ingested matter 3 to 4 times
per day but no diarrhoea or abdominal pain.
For these complaints he visited Debark General Hospital where urine IX
was done, unspecified white PO medication was given to be taken two
times per day and referred to our hospital for better IX and Mgt.

✓ No self or Family hx of similar illness (Genetics → RF)


✓ No hx of easy fatigability, blurring of vision, light headedness,
tinnitus or vertigo
✓ No self or Family hx of DM, HTN or Asthma
✓ No hx of blood transfusion, tattooing, contact with a jaundiced patient, IV
drug abuse or MSP (RF for hepatitis virus transmission → HBV, HCV → PIGN)
✓ No hx of malarial attack or travel hx to malaria endemic area
(PIGN)He was screened for RVI 2 months back and found to be NR
(PIGN)
✓ No hx of swelling over the neck, axilla or groin (Lymphoma → GBS DDX)
✓ No hx of chronic cough, contact with chronic cougher, or a known
TB patient (TB peritonitis → DDX)
✓ No hx of dyspnea, orthopnea, PND or palpitation (CHF → DDX)
✓ No hx of malar rash or photosensitivity (SLE)
✓ No self or family hx of hearing or visual impairment (Alport SXX)

Finally, he was admitted to our hospital supported physically by his families

Physical examination (pertinent findings)

1 GA
✓ RD from
☛ Ascites → if infected → peritonitis
☛ Pleural effusion
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☛ Renal vein thrombosis
✓ Grossly edematous
✓ Grossly pale → anemia 2ry to
☛ Hemolysis
☛ Erythropoietin deficiency
☛ Hemodilution
☛ Acidosis (Hypoxia)
☛ Loss of ferritin (Iron binding immunoglobulin)
8. Vital signs
✓ HTN
✓ Tachycardia → from peritonitis, effusion, Bilateral RVT (renal venous
thrombosis)
✓ Fever
☛ If not on steroid
☛ Peritonitis
☛ Lung infection

3 HEENT
✓ Facial puffiness
✓ Whitish discoloration around the uveola ( Streptopharyngitis)
✓ Icteric Screla → PIGN ( from HBV, HCV)

4 LGS
✓ LAP → Lymphoma causing NS

5 RS
✓ Pleural effusion
✓ Pulmonary edema

6 CVS
7 Abdominal examination
✓ Ascites
✓ Peritonitis

8 GUS
9 MSS
✓ Edema (Anasarca)

10 IS
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11 NS

DDX

✓ Nephrotic/Nephritic sxx
✓ CHF
✓ Constrictive pericarditis
✓ Disseminated TB (TB pericarditis, TB peritonitis)
✓ AKI
✓ Advanced Lymphoma
✓ SLE

IX

1) U/A
✓ Color → red (Hematuria)
✓ Blood → degree of hematuria
✓ Protein → nephrotic range ( +3, +4)
✓ RBC casts → AGN
✓ Hyaline cast → Lipiduria in NS
✓ WBC → PMN in PSGN
✓ Urine protein to creatinine ratio > 2 in NS
2) CBC
✓ Anemia 2ry to
☛ Hemodilution in renal insufficiency 2ry to APSGN, HUS
☛ Hemolysis in HUS
☛ Erythropoietin deficiency
☛ Leukocytosis → APSGN, Complicated NS
3) PICT →2ry NS
4) BUN and Creatinine
✓ Usually normal
✓ Asses AKI
5) Serum albumin level
✓ Decrease in NS (< 2.5 g/dl)
6) Lipid profile (CL, TG)
7) Serum compliment
→ raised in NS
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✓ C3 level (see discussion part of NtS)
✓ C3 level predict course and prognosis of AGN
☛ In the 1st 2 weeks C3 is low in 90 % of AGN patients
☛ After 6 to 8 weeks C3 level will be Normal
✓ Even though very important test, Not available in most set ups of
Ethiopia
8) CXR → CHF, RD, 2ry infection (Pneumonia)
9) Serum electrolyte → dilutional Hyponatremia, hypophosphatemia
10) ASO titre → following pharyngitis, rarely elevated in skin infection
11) Throat culture → Supportive
12) Renal Biopsy
✓ Indication for APSGN
☛ Acute renal failure (ARF) which persist for > 2 month
☛ Decreased C3 level and ARF persist for > 2 month
☛ Absence of strep infection
✓ Indication for NS
☛ Unlike pediatric patients almost all non-diabetic adult patients with
nephrotic syndrome need renal biopsy to confirm the etiology.
Hence, they need to be referred to a hospital with nephrology
service.
☛ Indication for of Biopsy in pediatrics patients
▪ Sustained hypertension
▪ Hematuria
▪ Renal insufficiency
▪ 2ry cause (e.g. SLE)
▪ Hypocomplimentation
▪ In children aged 1 to 8 years
13) Streptozyme test (in western setup)

☛ DNAse
☛ Hyaluronidase
☛ Streptokinase

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Discussion

12.1 Nephrotic syndrome (NS)

Nephrotic syndrome (NS) is a clinical sate which results from heavy (massive)
proteinuria.
The presence of nephrotic syndrome (NS) is a definitive indicator of glomerular
pathology.
Nephrotic syndrome is defined if all the following 1st three clinical and
laboratory findings are fulfilled
Heavy proteinuria: defined as urine protein >3000mg (3gm) in a 24hr urine
protein
Hypoalbuminemia: Defined as serum albumin <3g/dl
Edema/anasarca
Hyperlipidemia (hypercholesterolemia) → usually severe, is a common
finding. Some experts include it as requirement for the diagnosis of NS..
Hypertension
Minimal microscopic hematuria;
Notice
o Proteinuria (nephrotic range) and edema are marked in nephrotic syndrome
than nephritic syndrome
o Hypertension and Hematuria are marked in nephritic syndrome than
nephrotic syndrome
Some patients might have heavy proteinuria (>3000mg in 24-hour urine) but do
not have the other features of the NS. They are said to have nephrotic range
proteinuria, but not the nephrotic syndrome.
If left undiagnosed or untreated, some of these syndromes will progressively
damage enough glomeruli to cause a fall in GFR, producing renal failure
The GFR in these patients may initially be normal or, rarely, higher than
normal, but with persistent hyperfiltration and continued nephron loss, it
typically declines over months to years.
Patients with a basement membrane syndrome either have genetically
abnormal basement membranes (Alport’s syndrome) or an autoimmune
response to basement membrane collagen IV (Goodpasture’s syndrome)
associated with microscopic hematuria, mild to heavy proteinuria, and
hypertension with variable elevations in serum creatinine.
Increased susceptibility to infection, venous thrombosis, and acute kidney injury
are the major complications of the NS. 729
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Nephrotic syndrome is not a single disease. It is a manifestation of several
diseases. Hence, once the presence of NS is confirmed, the etiology should be
identified.
Nephrotic syndrome in adults is different from pediatric NS in etiology, the
needed investigation, treatment, and outcome. Hence, adult NS should never
be treated like pediatric NS.
The causes of nephrotic syndrome are classified in to two major groups:
Primary (diseases limited to the glomeruli) and secondary (systemic diseases
with glomerular manifestations or complications)
Diabetes (diabetic kidney disease) is the leading cause of nephrotic range
proteinuria worldwide.

Table. Major causes of nephrotic syndrome in adults


Major cause of primary nephrotic Major causes of secondary nephrotic syndrome
syndrome
➢ Primary Focal segmental ➢ Diabetic Nephropathy
glomerulosclerosis (FSGS) ➢ Autoimmune disease: SLE
➢ Minimal change disease (MCD) ➢ Infectious: HBV, HCV, HIV, Syphilis,
➢ Primary membranous nephropathy Schistosomiasis
(MN) ➢ Amyloidosis: primary or secondary amyloidosis
➢ Primary membranoproliferative ➢ Drugs: NSAIDS
glomerulonephritis (MPGN) ➢ Preeclampsia
➢ Malignancy: Multiple myeloma, lymphoma,
carcinomas

Clinical features

Symptoms and signs


Symptoms and signs related to the nephrotic state
o Body swelling: Periorbital edema, peripheral edema, scrotal or labial edema
o Third space fluid collection: ascites, pleural effusion
o Fatigue and shortness of breath
o Urine: excessive foaming
o Nail: white horizontal bands on the nail
Clinical features suggestive of specific secondary causes
o Diabetes: Known history of diabetes, presence of diabetic retinopathy
o SLE: diffuse non-scarring hair loss, malar rash, photosensitivity, polyarthritis
o Preeclampsia: third trimester pregnancy or peripartal state with high BP
o Multiple myeloma: bone pain, pathological fracture, anemia
o Lymphoma: Lymphadenopathy, splenomegaly
o Carcinomas: Local symptoms (breast lump, abdominal mass,
cough/hemoptysis, lymphadenopathy)

Diagnosis and investigation

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The following steps are helpful in guiding the diagnosis of nephrotic syndrome in
adults
Step 1: Confirming the presence of nephrotic syndrome:
o 24-hour urine protein
o Serum albumin
o Lipid profile
Step 2: Investigation for common causes of nephrotic syndrome
o Retinal screening for diabetic retinopathy: any time for type 2 diabetics and
after a minimum of five year of type 1 diabetes
o HBSAg, HCV antibody, HIV screening, VDRL(RPR), ANA
o AntiPLA2R antibody: For screening primary membranous nephropathy
o Work up for multiple myeloma: If suspected, serum free light chains and
serum electrophoresis.
o Work up for other malignancies: only if there are clinical clues.
Step 3: Renal biopsy
o Unlike pediatric patients almost all non-diabetic adult patients with
nephrotic syndrome need renal biopsy to confirm the etiology. Hence, they
need to be referred to a hospital with nephrology service.
Investigations: Additional helpful investigations
Urinalysis: hematuria and proteinuria
o Hematuria can be gross or microscopic hematuria. More common in
nephritic syndrome than nephrotic syndrome
o In early nephropathy, such as in diabetic nephropathy, proteinuria
increases to 30 - 300 mg/24 h and is called microalbuminuria and
represents the presence of renal disease.
o Greater than 300 mg/24 h of albuminuria represents frank proteinuria and
more advanced renal disease

Table; Urine Assays for Albuminuria/Proteinuria


24h Albumin 24h Albumin to Dipstick
(mg/24hr) Albumin creatinine ratio proteinuria
(mg/24hr) (mg)
Normal 8 – 10 <150 <30 –
Microalbuminuria 30 – 300 – 30 - 300 -/Trace/1+
Proteinuria >300 >150 >300 Trace - 3+

Renal function tests (serum creatinine): AKI can occur as a complication of the
NS or over-diuresis or could be part the glomerular disease (nephrotic-nephritic
presentation)
Serum electrolytes: As baseline for diuretic therapy
Abdominal ultrasound: to see kidney sizes
Investigations when complications are suspected: e.g. if deep vein thrombosis
(a common complication is suspected), do doppler ultrasound of suspected limb
veins.
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Treatment

Non-pharmacologic treatment
➢ Salt restriction
➢ Fluid restriction (less than 1 - 1.5 liter/day)
➢ Encourage ambulation
➢ Protein should not be restricted rather encourage patients to take adequate
protein and high calorie diet

Pharmacologic treatment
1. Treatment of the edematous state
Loop diuretics: nephrotic syndrome is associated with relative diuretic resistance
o Oral Furosemide:
▪ Starting dose 40mg, PO, BID -TID.
▪ Increase the dose to 80 mg PO BID-TID, then 120mg. PO, BID-TID.
o Aim: decrease weight by 0.5 to 1kg/day.
o IV Furosemide: If no adequate weight loss with increasing dose, admit for
IV Furosemide
▪ Start with 40mg, IV, TID.
▪ Increase the dose to 80 mg IV TID, then 120mg. PO, TID
▪ If no adequate response with IV Furosemide, add hydrochlorothiazide
12.5 to 25mg BID (to be given 30 minutes before the IV Furosemide)
o Add prophylactic KCl tablets (600mg BID-TID) or Spironolactone 25-50mg
PO/daily and monitor serum electrolytes every 2-3days.
2. Anti-proteinuric treatment
ACE inhibitors or Angiotensin receptor blockers (ARBS)
o Start after adequate diuresis.
o The kidney function must be stable before starting.
o The dose should be escalated gradually with monitoring of serum
creatinine and potassium. Monitoring should be done within 2 weeks of
initiation and dose escalation.
o ACE inhibitors (particularly Enalapril) are preferred over ARBs due to their
low cost and wide availability.
Preferred
o Enalapril: starting dose 5mg BID, Maximum dose 20mg BID
Alternatives
o Lisinopril: starting dose 5mg/day, Maximum dose 40mg/day
o Perindopril: starting dose 5mg/day. Maximum dose 15mg/day
ARB
o Telmisartan: Starting dose: 40mg/day maximum dose 80mg/day
o Irbesartan: Starting dose: 75-150mg/day, maximum dose 300mg/day
o Losartan: Starting dose 50mg/day maximum dose 100mg/day
o Valsartan: Starting dose 80 -160mg/day, maximum dose 320mg/day
o Candesartan: Starting dose 8-16mg/day maximum dose 32mg/day 732
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3. Pharmacologic treatment for complications of the nephrotic syndrome


Treatment of hyperlipidemia: as per dyslipidemia treatment guideline (see
section on dyslipidemia). Many patients require statins due to sever
hyperlipidemia.
Prophylactic anticoagulation: Indicated if serum albumin is <2g/dl and patient is
hospitalized
o UFH, 5,000IU, BID until discharge Or
o Enoxaparin 40mg, SC, daily until discharge
Therapeutic (Full dose) anticoagulation: Indications
o If there is active venous thromboembolic disease (e.g. DVT/PE, renal vein
thrombosis)
o If albumin is low and the following risk factors are found: Pregnancy,
active malignancy, recent major surgery, NYHA class III or IV heart failure
or morbid obesity
▪ UFH, 17,500 SC, BID or Enoxaparin 1mg/kg/dose BID + Warfarin, 2
to 5 mg PO daily (dose to be adjusted according to INR, usual
maintenance dose ranges from 2 to 10 mg daily)
▪ Overlap heparin with warfarin until two therapeutic INRs (2-3)
achieved, and then followed by Warfarin alone.
▪ Duration of anticoagulation: Until the nephrotic syndrome resolves or 6-
12 months (if it does not resolve).
4. Treatment of the specific cause of the nephrotic syndrome
Empiric steroid or any immunosuppressive should not be started for adults with
nephrotic syndrome without doing renal biopsy; hence, all adult patients with
non-diabetic nephrotic should be referred to a hospital with nephrology service.

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12.2 Nephritic syndrome

Acute nephritic syndromes classically present with


o Hypertension
o hematuria with red blood cell casts
o pyuria, and
o mild to moderate proteinuria (1 - 2 g/24 h).
Extensive inflammatory damage to glomeruli causes a fall in GFR and
eventually produces uremic symptoms with salt and water retention, leading to
edema and hypertension
If glomerular inflammation develops slowly, the serum creatinine will rise
gradually over many weeks, but if the serum creatinine rises quickly,
particularly over a few days, acute nephritis is sometimes called rapidly
progressive glomerulonephritis (RPGN)
o The histopathologic term crescentic glomerulonephritis is the pathologic
equivalent of the clinical presentation of RPGN.

Table; Causes of Nephritic syndrome


PSGN (Poststreptococcal glomerulonephritis) a
o The most common forms of glomerulonephritis in our setup especially in
children. In adults, post infectious Glomerulonephritis (PIGN) is common
cause
IgA nephropathy a
o The most common forms of glomerulonephritis worldwide
o Previously termed as Berger disease (from the scientist who first described
the glomerulonephritis)
Systemic causes
o Subacute bacterial endocarditis a
o Lupus nephritis a
Antiglomerular basement membrane disease a
Membranoproliferative glomerulonephritis a
Mesangioproliferative glomerulonephritis
Henoch-Schönlein purpura a
Cryoglobulinemia a
C3 Glomerulopathies
ANCA small-vessel vasculitisa
o Granulomatosis with polyangiitis (Wegener’s)
o Microscopic polyangiitis
o Churg-Strauss syndrome
a
Can present as rapidly progressive glomerulonephritis (RPGN); sometimes called
crescentic glomerulonephritis.

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Causes of Nephritic SXX

C 3 Level

Normal Low

Primary Secondary
Primary Secondary

PSGN SLE
RPGN HUS
MPGN IE
IgA N HSP Shunt Nephritis
PIGN GPS after VPS
Alport SXX

Diagram; Causes of Nephritic syndrome; RPGN = Rapidly proliferative Glomerulonephritis,


IgAN = immunoglobin A nephropathy, PIGN = Post infectious Glomerulonephritis, HUS = Hemolytic uremic
syndrome, HSP =Henoch schonlein purpura, GPS = Good Pasture syndrome, PSGN =Post streptococcal
Glomerulonephritis, MPGN =Membranoproliferative Glomerulonephritis, SLE =Systemic Lupus erythematosus, IE =
Infective endocarditis, VPS = Ventriculoperitoneal shunt for hydrocephalus

➢ Alport SXX characterized by, = Renal failure + Blindness + Deafness


➢ HUS preceded by Bloody diarrhea (Dysentery)
➢ HSP can affect → Skin (Skin rash), GI, renal, rarely joint
➢ GPS → antibody against Glomerular and pulmonary basement membrane
resulting in renal problem, cough and hemoptysis respectively
➢ PSGN resolve after 6week unlike others

Acute glomerulonephritis (AGN) and rapidly progressive


glomerulonephritis (RPGN)

Acute glomerulonephritis (AGN) and rapidly progressive glomerulonephritis


(RPGN) are important causes of AKI. in that they have clearly identifiable
clinical features and can rapidly progress to ESRD
AGN and RPGN present more or less in a similar fashion. Their presentation
is commonly described as the nephritic syndrome.
The clinical difference between AGN and RPGN: It is not easy to clinically
differentiate between the two.
o In RPGN: The kidney function keeps of deteriorating over days to weeks,
unless treated. It progresses to ESRD unless treated early.
o In infection related AGN: The kidney function usually improves.
The most common causes of self-limiting AGN are bacterial infections (also
called infection related glomerulonephritis).
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As opposed to pediatric AGN, where the commonest cause is streptococcal
infection of the skin or the throat, adult AGN can occur following any bacterial
infection at any site.
The most important causes of RPGN are autoimmune diseases: SLE (systemic
lupus erythematosus), systemic small vessel vasculitis (ANCA-vasculitis),
antibody direct to glomerular basement membrane (Anti-GBM disease).
The histopathologic finding in both AGN and RPGN is described as diffuse
proliferative glomerulonephritis (DPGN) and crescentic glomerulonephritis
respectively.

Clinical features
Clinical features of the AGN/RPGN: the nephritic syndrome
o Acute onset body swelling (Edema) and shortness of breath
o Decreased urine amount (oliguria)
o Reddish urinary discoloration (typically tea or cola colored urine)
o High blood pressure
Clinical features of suggesting the underlying causes (systemic diseases)
o Hair loss/diffuse non-scaring alopecia – SLE
o Malar rash, photosensitive rash, non-pruritic rash over the body– SLE
o Joint pain, evidence of arthritis (swelling and tenderness of joints) – SLE
o Hemoptysis, cough and dyspnea – Vasculitis, Anti-GBM disease or
pulmonary edema
o Petechiae/purpura – Vasculitis or SLE
o Pleural effusion – Part of the complication or SLE associated
o Pericarditis (friction rub or distant heart sound) – SLE or uremic
pericarditis
o Cardiac murmurs – Infective endocarditis or SLE
o Focal neurologic deficit – SLE (Lupus cerebritis) or vasculitis
Clinical features related to marked decrement in the kidney function
o Pulmonary crackles – pulmonary congestion
o Nausea and vomiting – uremic gastropathy
o Change in mental status – uremic or hypertensive encephalopathy
o Mucocutaneous bleeding – uremic bleeding

Diagnosis and investigations


Diagnosis
The diagnosis of AGN or RPGN should be made clinically in any patient
presenting with the nephritic syndrome (acute onset body swelling, tea/cola
colored urine, oliguria, and high BP)
Further investigations are needed for three purposes: For confirming the
nephritic syndrome, for identifying possible etiologies, and complications.

Investigations
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i. Investigation for evidencing the presence of the nephritic syndrome (AGN/RPGN)

Urinalysis:
o Hematuria and proteinuria
o The RBCs in the urinalysis: Significant proportion are dysmorphic
o RBC casts: may or may not be present. Their presence is not mandatory
for diagnosis)
24hour urine protein: above 500mg (usually>1000mg), it can sometimes be
nephrotic range(>3000mg)
Serum creatinine and ureaii

ii. Investigations for assessing potential complications


Serum electrolytes: particularly serum potassium (to look for hyperkalemia).
Chest X-ray: for evidence of pulmonary edema or pleural effusion.

iii. Investigations for identifying possible etiology

Basic serologies: to be done at initial evaluation


o Anti-streptolysin titer (ASO): For preceding streptococcal infection
▪ It may be falsely low or negative in patients with skin infections.
▪ It remains a useful test in those with pharyngitis but antibiotics may
decrease the titer
o The streptozyme test
▪ It is a much better than ASO alone (has high sensitivity and
specificity) for checking a preceding streptococcal infection.
o Hepatitis B (HBV) and C (HCV) serology: HBSAg and HCV antibody.
o HIV screening
o ANA (anti-nuclear antibody)

Additional important diagnostic investigations: to be ordered by specialist who


would decide on definitive management
o Anti-double strand DNA antibody(anti-dsDNA)
o Anti-neutrophil cytoplasmic antibody test (ANCA)
o Anti-glomerular basement antibody (Anti-GBM antibody)
o Serum complement level (complement -3 and 4/C3 and C4 levels)
o Renal biopsy
iv. Investigation for looking evidence of chronicity

o Abdominal ultrasound: bilateral small kidneys in adults (<9cm longitudinally)


indicate chronic kidney disease. Normal or increased kidney size can be
found in both acute and chronic glomerular diseases.

Treatment

Non-pharmacologic treatment
Salt and fluid restrictions
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Dialysis: if there are indications (see the topic acute kidney injury for
indications)

Pharmacologic treatment
1. Supportive (symptomatic) management
Loop diuretics
o Oral Furosemide:
▪ For patients with mild peripheral edema.
▪ Starting dose 40mg PO BID.
▪ Follow every 2-3 days, increase the dose to higher dose (Maximum
dose 600mg/day) or admit for IV diuresis, if response is suboptimal or
there is worsening.
o IV Furosemide:
▪ For patients with pulmonary congestion or sever edematous state
▪ Start with 40mg IV, stat. See response every 2 hours. If urine output
of 150ml and above is achieved in 2 hours and give the 40mg IV BID
or TID.
▪ If urine output is <150ml in 2hours, increase the dose by 40mg and
reassess the urine output in another 2 hours.
▪ Give the dose which resulted in adequate once diuresis
(>150ml/2hour) as standing e.g. 80mg or 120 IV BID or TID.
Maximum bolus dose 200mg.
▪ IV Furosemide above 100mg should be given slowly (over 15-
20minutes)
o Avoid prophylactic potassium tablet or spironolactone: due to the risk of
hyperkalemia in patients with AGN/RPGN.

Antihypertensives
o Loop diuretics are the preferred Antihypertensives: see above on diuretic
o Additional Antihypertensive: If BP is not well controlled with loop diuretics
alone
▪ Add Calcium channel blocker on loopr diuretics:
• Amlodpine 5-10mg PO once daily OR
• Nifedipine 20-40mg PO BID.
▪ If a third agent is needed (on top of Furosemide and Calcium channel
blocker combination) add a beta-blocker:
• Carvedilol 6.25 to 25mg BID or
• Bisoprolol 2.5 to10mg/day or
• Metoprolol 25-100mg/day or
• Atenolol 25-100mg/day
▪ Avoid ACE inhibitors, Angiotensin receptor blockers (ARBS): due to
the risk of hyperkalemia and potential for deterioration in kidney
function.
▪ Avoid Spironolactone in patients with AGN/RPGN: due to risk of
hyperkalemia and worsening kidney function.
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Management of hyperkalemia
o Start shifting treatment with regular insulin if serum potassium is
>6.0mmol/l
▪ Regular Insulin: 10IU regular insulin IV, immediately followed by
03vials (60ml) of 40% dextrose IV, to be given every 6 hour. Monitor
blood sugar every 4-6 hourly.
▪ If potassium is >7mmol/l or there are ECG changes hyperkalemia start
IV calcium
• Calcium gluconate (10%) 10ml, IV, to be given over 5 minutes
followed by regular insulin (as above).

2. Definitive management of the underlying cause

Definitive management of the underlying cause might require early initiation of


intensive immunosuppressive therapy; hence, patients should be referred to
nephrologist as soon as possible.
Options of Immunosupressive drugs include
o Glucocorticoids
o Methotrexate
o Cyclophosphamide
o Hydroxychloroquine
o Sulfasalazine
o Azathioprine
o Chlorambucil
o Cyclosporine
o Tacrolimus

Poststreptococcal glomerulonephritis (PSGN)

➢ PSGN is prototypical for acute endocapillary proliferative glomerulonephritis.


➢ The incidence of PSGN has dramatically decreased in developed countries and
in these locations is typically sporadic.
➢ Acute PSGN in underdeveloped countries is epidemic and usually affects
children between the ages of 2 and 14 years, but in developed countries is
more typical in the elderly, especially in association with debilitating conditions.
✓ It is also common in our setup especially in children
➢ It is more common in males, and the familial or cohabitant incidence is as
high as 40%.
➢ Skin and throat infections with particular M types of streptococci (nephritogenic
strains) antedate glomerular disease
✓ PSGN due to impetigo develops 2 - 6 weeks after skin infection and 1 - 3
weeks after streptococcal pharyngitis.
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➢ PSGN is an immune-mediated disease involving putative streptococcal antigens,
circulating immune complexes, and activation of complement in association with
cell-mediated injury.

Clinical features

The classic presentation is an acute nephritic picture with


o Hematuria
o Pyuria
o Red blood cell casts
o Edema
o Hypertension, and
o Oliguric renal failure
Symptoms and signs may be severe enough to appear as RPGN.
Systemic symptoms of headache, malaise, anorexia, and flank pain (due to
swelling of the renal capsule) in as many as 50% of cases.
5% of children and 20% of adults have proteinuria in the nephrotic range
A subclinical disease is reported in some series to be 4 - 5 times as common
as clinical nephritis, and these latter cases are characterized by asymptomatic
microscopic hematuria with low serum C3 complement levels.

Investigations

In the first week of symptoms, 90% of patients will have a depressed CH50
and decreased levels of C3 with normal levels of C4.
Positive rheumatoid factor (30 - 40%)
Positive cultures for streptococcal infection (10–70%)
Increased titers of ASO (30%), anti-DNAse (70%), or antihyaluronidase
antibodies (40%) can help confirm the diagnosis.

Treatment

➢ Treatment is supportive, with control of hypertension, edema, and dialysis as


needed.
➢ Antibiotic treatment for streptococcal infection should be given to all patients
and their cohabitants.
➢ There is no role for immunosuppressive therapy, even in the setting of
crescents.

Prognosis and outcomes

Recurrent PSGN is rare despite repeated streptococcal infections.


Early death is rare in children but does occur in the elderly.
Overall, the prognosis is good, with permanent renal failure being very
uncommon in the past (<1%) but with recently, an increased risk of CKD in
adulthood.
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syndrome/Nts/)
Complete resolution of the hematuria and proteinuria in the majority
of children occurs within 3-6 weeks of the onset of nephritis but 3-10%
of children may have persistent microscopic hematuria, non-nephrotic
proteinuria, or hypertension.
The prognosis in elderly patients is worse with a high incidence of azotemia
(up to 60%), nephrotic-range proteinuria, and ESRD.

IgA nephropathy

Berger first described the glomerulonephritis now termed IgA nephropathy.


It is classically characterized by episodic hematuria associated with
the deposition of IgA in the mesangium.
IgA nephropathy is one of the most common forms of glomerulonephritis
worldwide.
There is a male preponderance, a peak incidence in the 2nd and 3rd decades
of life, and rare familial clustering.
IgA nephropathy is predominantly a sporadic disease but susceptibility to it has
been shown uncommonly to have a genetic component depending on
geography and the existence of “founder effects.”
Clinical and laboratory evidence suggests close similarities between
Henoch-Schönlein purpura and IgA nephropathy.
Henoch-Schönlein purpura is distinguished clinically from IgA nephropathy by
o prominent systemic symptoms
o a younger age (<20 years old)
o preceding infection, and
o abdominal complaints.
Deposits of IgA are also found in the glomerular mesangium in a variety of
systemic diseases, including
o CLD
o Crohn’s disease
o GI adenocarcinoma
o chronic bronchiectasis
o idiopathic interstitial pneumonia
o leprosy
o ankylosing spondylitis
o Sjögren’s syndrome.
IgA deposition in these entities is not usually associated with clinically
significant
glomerular inflammation or renal dysfunction and thus is not called IgA
nephropathy.
IgA nephropathy is an immune complex–mediated glomerulonephritis defined
by the presence of diffuse mesangial IgA deposits often associated with
mesangial hypercellularity.
A second hit, such as a viral or other antigen exposure, may be necessary for
disease manifestation.
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Despite the presence of elevated serum IgA levels in 20 - 50% of patients,
and IgA deposition in skin biopsies in 15 - 55% of patients, a renal biopsy is
necessary to confirm the diagnosis.

Clinical features
➢ The two most common presentations of IgA nephropathy are
✓ recurrent episodes of macroscopic hematuria during or immediately
following an upper respiratory infection often accompanied by proteinuria or
✓ persistent asymptomatic microscopic hematuria.
➢ Nephrotic syndrome is uncommon.
➢ Proteinuria can also first appear late in the course of the disease.
➢ Rarely patients present with acute renal failure and a rapidly progressive
clinical picture.
➢ IgA nephropathy is a benign disease for the majority of patients, and 5 - 30%
of patients may go into a complete remission, with others having hematuria but
well-preserved renal function.
➢ In the minority of patients who have progressive disease, progression is slow,
with renal failure seen in only 25–30% of patients with IgA nephropathy over
20–25 years.
➢ Risk factors for the loss of renal function include
✓ the presence of hypertension or proteinuria
☛ persistent proteinuria for ≥ 6 months has poor prognosis
✓ the absence of episodes of macroscopic hematuria
☛ male sex
☛ older age of onset, and
☛ extensive glomerulosclerosis or interstitial fibrosis on renal biopsy.

Management

➢ There is no agreement on optimal treatment.


➢ Some suggestions include
✓ ACE inhibitors
✓ steroid treatment or other immunosuppressive therapy in patients with
persistent proteinuria after ACE inhibitor therapy
✓ Tonsillectomy
✓ Fish oil
✓ When presenting as RPGN, steroids, cytotoxic agents, and plasmapheresis.

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Chapter 12; Glomerular disease (Nephrotic syndrome/NS/ and Nephritic
syndrome/Nts/)

Lupus nephritis
➢ Lupus nephritis is a common and serious complication of systemic lupus
erythematosus (SLE).
➢ Clinical manifestations of renal disease are present in 30% of patients at the
time of diagnosis, and the majority will develop renal abnormalities in the
course of their disease; it is more common in blacks, Asians, and Hispanics
than it is in whites
➢ Lupus nephritis results from the deposition of circulating immune complexes
➢ The most common clinical sign of renal disease is proteinuria, but hematuria,
hypertension, varying degrees of renal failure, and active urine sediment with
red blood cell casts can all be present
➢ A kidney biopsy should be performed in most patients with renal involvement
to establish the histologic subtype, which guides therapy.

➢ The subject of lupus nephritis is presented under acute nephritic syndromes


because of the aggressive and important proliferative lesions seen in class III–
V renal diseases.
➢ Class III describes focal lesions involving <50% of the glomeruli with
proliferation or scarring, often involving only a segment of the glomerulus.
Class III lesions have the most varied course.
➢ Hematuria and proteinuria are present, and some patients also have an active
urinary sediment, nephrotic syndrome, hypertension, and a decreased GFR.
➢ Patients with mild proliferation involving a small percentage of glomeruli
respond well to therapy with steroids alone, and <5% progress to renal failure
over 5 years.
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➢ Patients with more severe proliferation involving a greater percentage of
glomeruli have a far worse prognosis and lower remission rates.
➢ Treatment of those patients is the same as that for class IV lesions.
➢ Class IV describes diffuse lesions with >50% of the glomeruli involved and
proliferative endocapillary lesions with or without extracapillary lesions that may
be segmental (IV-S), involving <50% of the glomerular tuft, or global (IV-G),
involving >50%.
➢ Patients with class IV lesions commonly have high anti-DNA antibody titers,
low serum complement, hematuria, red blood cell casts, proteinuria,
hypertension, and decreased renal function; 50% of patients have nephrotic-
range proteinuria.
➢ Patients with crescents on biopsy often have a rapidly progressive decline in
renal function.
➢ Without treatment, this aggressive lesion has the worst renal prognosis, with
class IV-S worse than class IV-G. However, if a remission—defined as a return
to near-normal renal function and proteinuria ≤330 mg/dL per day—is achieved
with treatment, renal outcomes are excellent.
➢ Current evidence suggests that inducing a remission with administration of
high-dose steroids and either cyclophosphamide or mycophenolate mofetil for
2–6 months, followed by maintenance therapy with lower doses of steroids
and mycophenolate mofetil or azathioprine, best balances the likelihood of
successful remission with the side effects of therapy.
➢ There is no consensus on use of high-dose intravenous methylprednisolone
versus oral prednisone, monthly intravenous cyclophosphamide versus daily oral
cyclophosphamide, or other immunosuppressants such as cyclosporine,
tacrolimus, or rituximab.
➢ Nephrologists tend to avoid prolonged use of cyclophosphamide in patients of
childbearing age without first banking eggs or sperm.
➢ 60 % of patients with class V present with nephrotic syndrome or lesser
amounts of proteinuria.
➢ Patients with lupus nephritis class V, like patients with idiopathic membranous
nephropathy (IMN), are predisposed to renal vein thrombosis and other
thrombotic complications.
➢ A minority of patients with class V will present with hypertension and renal
dysfunction
➢ Patients with severe nephrotic syndrome, elevated serum creatinine, and a
progressive course will probably benefit from therapy with steroids in
combination with other immunosuppressive agents.
➢ Therapy with inhibitors of the renin-angiotensin system also may attenuate the
proteinuria.
➢ Antiphospholipid antibodies present in lupus may result in glomerular
microthromboses and a thrombotic microangiopathy.
➢ The renal prognosis is worse despite anticoagulant therapy.
➢ Lupus patients with class VI lesions have >90% sclerotic glomeruli and ESRD
with interstitial fibrosis.
➢ Up to 20% of patients with lupus nephritis will reach end-stage disease,
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➢ Patients with lupus nephritis have a markedly increased mortality compared
with the general population.
➢ Renal transplantation in renal failure from lupus, usually performed after ∼6
months of inactive disease, results in allograft survival rates comparable to
patients transplanted for other reasons.

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Chapter 13; Leishmaniasis (ካላዛር/ጓቋ/ድባ/ እና ቁንጭር)

Chapter 13; Leishmaniasis


(ካላዛር/ጓቋ/ድባ/ እና ቁንጭር)
Dr. Mulualem. G, Dr. Robel. D

Clinical features and how to write hx of VL patient


History

The approach we discussed here is about Visceral leishmaniasis/VL/. Other


forms of leishmaniasis such as cutaneous leishmaniasis are discussed in
the discussion part only.

VL case definition → N.B case definition is very important in case of


epidemics
“A person who presents with fever for more than 2 weeks and an enlarged ,
spleen (splenomegaly) and/or enlarged lymph nodes (lymphadenopathy), or ,
either loss of weight, anemia or leucopenia while living in a known VL endemic
area or having travelled to an endemic area’’.
Visceral Leishmaniasis should always be suspected when an individual
presents with prolonged fever from the endemic areas.
The Diagnosis of VL relies on clinical, serological, parasitological and molecular
findings.
The definitive diagnosis is demonstration of the parasite in a tissue aspirate.

Clinical Diagnosis
Clinical signs and symptoms associated with VL include fever for more than
two weeks, fatigue, weakness, loss of appetite, weight loss, malaise, cough,
diarrhea, epistaxis, cachexia, abdominal pain, anemia, pancytopenia, and,
associated with parasitic invasion of blood and reticulo-endothelial system,
enlargement of lymph nodes, spleen, and liver.
Some of these clinical signs and symptoms are similar to other diseases
prevalent in the areas where VL is endemic.
The clinical diagnosis of VL is therefore based on the standard case
definition of visceral Leishmaniasis, as given above
Symptoms often persist for several weeks to months before patients seek
medical care or die from the bacterial co-infection, massive bleeding or severe
anemia.

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Characterization of patient history

➢ Pt’s may present with (i.e the chief compliant maybe;)


Fever
Abdominal Swelling over the LUQ (ጓቋ)
Anaemia features
➢ Fever
Chronic fever lasting for ≥ 2 weeks
Gradual in onset
High gr ade and intermittent / sometimes Low grade and
continuous
Associated with chills and rigor
Peak in the afternoon and night, relieved in the morning
✓ Usually double or triple onset daily
➢ Swelling over the LUQ of abdomen
Painless
Starts from the LUQ and grows towards the umbilicus (mid
abdomen) which increase in size progressively to involve the
whole abdomen with in ‘’X’’ days
Associated with
✓ Dragging sensation and feeling of abdominal fullness
✓ Early satiety
✓ Anorexia, vomiting and weight loss
How many days after the onset of fever, does the swelling
begins? → e.g. pt noticed the swelling 2 weeks after the onset
of fever
➢ Easy fatigability (weakness)
From supra ordinary to sub ordinary activity through time to
the extent s/he unable to perform his/her daily activities
➢ Anaemia smx’s
➢ Weight loss
➢ If s/he Lives in kalazar and malaria endemic area (RF)
✓ Or travel hx to endemic area (when, how long s/he stayed there)
✓ Similar illness in the vicinity
✓ Malarial attack (how many times is the recurrence; last malarial

attack is ‘’X’’ months back) (→ chronic CXN of malaria/HMS/ is DDX for VL)

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N.B What is the difference between abdominal swelling and


abdominal distension?
weight loss despite increased appetite in
➢ Abdominal distension occurs when gas (air) or fluid
o Kalazar accumulates in the abdomen causing its outward
o DM expansion beyond the normal girth of the stomach.
o Thyrotoxicosis Underlying causes include ascites, Intestinal
o Malabsorption obstruction etc.
➢ The term Abdominal swelling is used when there is
intraabdominal organ enlargement causing increased
abdominal girth (e.g. hepatosplenomegaly) or mass
arising from the abdomen

The clinical manifestations of the disease are caused by multiple factors. The
most common causes are mainly due to:
▪ Splenomegaly resulting in
• Sequestration of blood
• Pressure effect of massive spleen
▪ Pancytopenia resulting in
• Low hemoglobin
• Low WBC → low immunity and high incidence of infections
• Low platelets → bleeding

Risk factors (especially to be infected by sand flies)

✓ Some of the factors found to be associated with the spread include;


o Living in endemic area or travel history to endemic area (living in
lowland area and forest)
o Poor socioeconomic status (poverty and malnutrition) associated with
presence of the sand fly vector and reservoirs.
o Male gender → engaged in outside activity (sleeping outside the
house during farming)
o Occupation → farmer
✓ Immunocompromisation
o Leishmania/HIV co-infection is an important factor for the spread of
the disease
✓ Age → youngsters have acute manifestation
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Complication of VL

➢ 2ry infection
The infection of the lymphoid tissue results in suppression of the
immune response
which is a predisposition for other infections.
commonly encountered infections include;
o Ear infection (e.g. Otitis media)
o Pneumonia
o TB (2ry TB infection is common in VL patients)
o GI infection (gastroenteritis, dysentery, diarrhea)
▪ Diarrhea and cough can occur due to mucosal
involvement of the gastro-intestinal and respiratory tract.
o sepsis
▪ for VL patients, Signs of bacterial co-infection should
be ruled out because bacterial pneumonia and gastro-
intestinal infections are common.
➢ Anaemia → 2ry to
Hypersplenism
Haemolysis
Bleeding
Short life span of RBC
Ineffective erythropoiesis → due to infiltration of BM by parasite
o All cell lines are often affected causing pancytopenia
➢ Bleeding
Due to pancytopenia or post SSG treatment
➢ In Patients with an advanced stage of the disease;
o Cachexia and edematous from hypoalbuminemia or CHF due to the
anemia.
o Hepatic dysfunction, jaundice and ascites can also occur.
o Chronic diarrhea, malabsorption → rarely due to invasion of the
intestine by parasite
➢ Malnutrition
o Over 1/3rd of VL patients present with moderate to severe state of
malnutrition which further predisposes them to infections and affects
the prognosis of VL treatment.
➢ PKDL (post kalazar dermal leshmaniasis)
o Chronic skin rash (erythematous macule, plaque and nodule)
following clinical response to VL treatment

N.B
Common cause of death in VL are bleeding,
severe anemia and 2ry infection
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Sample history

Chief compliant

fever of 2 months duration

HPI

This patient was last relatively healthy two months back, at which time he
began to experience insidious onset of low-grade intermittent fever sometimes
high grade especially in the afternoon and night. for such compliant he visited
a nearby clinic and was given a white circular tablet to be taken twice a day
and unspecified injection but no improvement.

A month after the onset of fever he noticed a painless abdominal swelling


which begins over the LUQ of abdomen and grows towards the umbilicus (mid
abdomen) then increase in size progressively to involve the whole abdomen
within three weeks duration associated with dragging sensation and feeling of
abdominal fullness, early satiety, anorexia and unquantified but significant
weight loss to the extent his trousers become loose.

Two weeks before admission he started to experience easy fatigability to the


extent that he couldn’t be able to perform his routine daily activities associated
with blurring of vision, palpitation and light headedness but no tinnitus, vertigo,
dyspnea, orthopnea or PND.

For this he visited quara primary hospital where unspecified blood tests were
done, transfused with one bag of blood and he was told that he may have
kalazar (“guaqua”) and referred to our leishmaniasis center for confirmation
and better management.

He lives in kalazar and malaria endemic area and there is similar illness
in the vicinity. He had Hx of repeated malaria attack. His last attack
was 2yrs back where he was treated and got relieved. But he has no
hx of kalazar attack
No hx of HTN, DM or asthma (immunocompromisation → RF)
No hx of nasal bleeding, gum bleeding, melena or haematochezia (bleeding
disorder → CXN)
No hx of abdominal pain, diarrhoea or vomiting (gastroenteritis, dysentery → CXN)
No hx of yellowish discoloration of the eyes, RUQ abdominal pain,
itching sensation, stool or urine colour change (cirrhosis→ CXN or amoebic liver
abscess → DDX)
No hx of river water contact or post river water contact itching
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No hx of bone pain, nasal bleeding, pesticide/herbicide exposure,


chemoradiotherapy, swelling over the neck, axilla or groin (haematologic
malignancy/CML, NHL/ → DDX)
No hx of chronic cough, contact with chronic cougher or previous TB
treatment (Disseminated TB to spleen → DDX)
No hx of sore throat, reddish discoloration of urine, dental/oral
manipulation, IV drug abuse or intracardiac device (SBE/subacute bacterial
endocarditis/→ DDX)
No hx of malar rash, photo sensitivity or joint pain (SLE → DDX)
No hx of raw milk drinking or participation in cattle delivery (brucellosis →
DDX)

Finally, he was admitted to our hospital walking by himself

Physical examination (pertinent findings)

1 GA
Cachexia (in advanced VL)
Ashen Gray appearance (darkening of face)
o The term ‘’kala-azar’’, from Hindu for “black fever”, may be related
to this clinical feature

2 Vital signs
Febrile
Tachycardia and bounding pulse → sign of high output failure (CHF)
in response to anaemia

3 HEENT
Pale conjunctiva → anaemia
Active nasal bleeding or clotted blood over the nostrils → bleeding
2ry to thrombocytopenia
Ear discharge, sinusitis → 2ry infection
Subconjunctival haemorrhage → IE, VL
Jaundice → haemolytic anaemia

4 LGS
LAP → VL, NHL/HL, Other malignancies

5 RS
6 CVS 751
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CHF 2ry to severe anaemia → S3 gallop, raised JVP, ESM (ejection


systolic murmur)
Valvular lesion due to IE

7 Abdominal examination
HSM (Hepatosplenomegaly) ± (LAP, per splenitis)
✓ Non tender (rarely tender due to capsular pressure)
✓ Soft
✓ Firm in consistency
✓ Smooth surface
✓ Massive splenomegaly
▪ The accumulation of infected mononuclear phagocytic cells in the spleen
and the kupfer cells in the liver result in the hypertrophy of the organs
to a clinical apparent hepatosplenomegaly.

8 GUS
9 MSS
Oedema → advanced kalazar, lymphoma, CHF 2ry to severe
anaemia
Spine tenderness → NHL

10 IS
Pallor → anaemia
Dry, scaly skin (sometimes diffuse, warty, non-ulcerated skin lesion)
Purpura, petechiae → bleeding tendency
Hyperpigmentation and ashen Gray appearance
12 NS

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DDX

1. Lymphoma (NHL)
Extra nodal involvement of lymphoma includes BM (DDX for
VL), thyroid, lung, brain, skin, testes
LAP→ painless, discrete, firm
HSM
Fever, weight loss, night sweat, easy fatigability
Bone pain
Paraplegia

N.B
Lymphoma can be classified as

Very aggressive
✓ Burkitt lymphoma
✓ ALL (Acute lymphoblastic leukemia)
✓ Oncologic emergencies
Aggressive
✓ Mantle cell lymphoma
✓ DLBCL (diffuse large B cell lymphoma)
Indolent

2. Leukaemia (CML)
▪ These patients have fever, malaise, bleeding tendencies, weight loss and
splenomegaly.
▪ They are also susceptible to other infections.
▪ Blood tests in the laboratory show a high white blood cell count.
▪ Phases of CML include;
a) Chronic phase (<10 % blast cells)
✓ Low grade fever, night sweat, fatigue
✓ Bone pain due to infiltration by malignant cells
✓ HSM
✓ Leucocytosis (hyper viscosity SXX) sensitive to treatment
b) Accelerated phase (10 - 20 % blast cells)
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✓ Bone pain
✓ Splenomegaly
c) Blastcrisis (>10 % blast cells)
✓ Have acute leukaemia manifestations (AML→ 80%, ALL
→ 20%)
✓ BM failure → bleeding, infection
✓ Resistant to treatment
3. Malignancy in general → FUO
N.B FUO (fever of unknown origin caused by)
Malignancy
TB
Intra-abdominal abscess
CTD (connective tissue disorders)
4. MPD (myeloproliferative disorders)
5. SBE (IE)
Sub-acute (2 - 3 weeks)
RF include → dental/oral manipulation, IV drug abuse,
intracardiac device
Manifest with → sore throat, reddish discoloration of urine
(haematuria), abnormal body movement, fever, tipped
splenomegaly
6. Malaria
▪ Symptoms of acute malaria generally stays for few days, whereas
symptoms of VL tend to be chronic.
▪ However, repeated attacks of malaria can cause chronic malaria that
manifests itself with fever, severe anemia, splenomegaly, loss of weight
and other constitutional symptoms that looks like VL.
▪ Treatment for malaria improves the patient situation. If no improvement
VL may be considered.

7. HMS (Hyperactive malarial Splenomegaly) or Hyperactive


Tropical Splenomegaly
▪ Tropical splenomegaly can also occur in the setting of chronic malaria.
▪ It is an immunological reaction to malaria.
▪ The patients may have had massive splenomegaly (often combined with
Hepatomegaly) for years.
▪ There is no fever.
▪ It is a diagnosis by exclusion of other differentials for patients from
malaria-endemic areas with a huge spleen.
▪ refer chronic CXN of malaria under short case of Nitsibin (click here →
Malaria (ወባ))

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8. Disseminated TB to spleen
▪ The patients will present with malnutrition and a history of fever and
other constitutional symptoms of TB for several months.
▪ They may have an enlarged spleen (tipped splenomegaly) or lymph
nodes as in miliary Tuberculosis.
9. HSS
▪ The patients can have a very large liver and spleen, which they have
often had for a very long time.
▪ Patients may not have fever but can present with ascites and other
portal hypertension signs.
▪ Stool or urine analysis will show eggs of Schistosoma.
▪ Refer from the following
• HSS from DDX of CLD under long case of Nitsibin (click here → Chapter
9; CLD/ Chronic liver disease/ (የጉበት በሽታ))
• ‘’Intestinal Helminthic Infestations (የአንጀት ጥገኛ ተውሳክ ፣የአንጀት ትላትል)
and blood flukes’’ section from Short case of Nitsibin (click here → 9.2.4.
Schistosomiasis (ቢሊሃርዚ ያ))

10. Splenic abscess


▪ Present with Fever, Left upper quadrant pain and Splenomegaly
• These patients have high grade fever and a very tender spleen.
▪ Presentation frequently is delayed
▪ May have risk factors such as Immunosuppression (including HIV
infection and chemotherapy), Trauma
▪ The diagnosis is confirmed by abdominal ultrasound or CT scan

11. Amebic liver abscess


▪ Patients usually present with one to two weeks of right upper quadrant
pain and fever
▪ other symptoms may include sweating, malaise, weight loss, and
anorexia

12. SLE
Common source of FUO
Present with photo sensitivity, malar rash, migratory joint pain,
myalgia, arthralgia

13. Typhoid Fever


▪ The classic presentation includes high fever, malaise, diffuse abdominal
pain, and constipation or diarrhea.
▪ Patients usually have a slow heart rate (bradycardia), and, in severe
cases, can progress to impaired mental status (confusion) or other
serious complications.
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14. Typhus → Typhus is also an acute febrile illness characterized by an


abrupt onset of fever, headache and a maculopapular or petechial rash.

15. Brucellosis
▪ rare, mis diagnosed as TB
▪ there is history of contact with animal abortus
▪ Patients have a long history of fever, small or moderate splenomegaly
and an enlarged liver.
▪ Usually there is also involvement of the joints or bones that results in
musculoskeletal pains and arthritis.

16. HIV/AIDS
▪ HIV damages the immune system so that the body of an infected person
cannot properly fight against diseases.
▪ Patients often suffer from recurrent diarrhoea, which may lead to
malnutrition/wasting and dehydration, as in a kala azar patient.

17. IM (infectious mononucleosis)

IX

Investigations to be done for VL patient include;

➢ Leishmanial diagnostic investigations (see the algorithm below)


▪ Parasite detection from Aspiration
▪ Antibody detection
▪ Antigen detection
▪ Molecular techniques
➢ Other non-Leishmanial tests

1. Aspiration
Gold standard diagnostic IX modality
Amastigotes (ovoid body) seen from the aspirate
o As discussed above, The Diagnosis of VL relies on clinical,
serological, parasitological and molecular findings.
o Definitive diagnosis of VL is made by visualization of the
amastigote form of the parasite by microscopic examination of
aspirates from lymph nodes, bone marrow or spleen aspiration.
RK39, LD body from PM and kalazar latex agglutination test confirmed
by aspiration
Used for VL or hematologic malignancy DX (mainly for leukaemia,
lymphoma staging /BM involvement/)
This diagnosis has a high specificity but the sensitivity of the
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Organs to be aspirated for VL Sensitivity


1. Spleen ≥ 95% (93 – 99%)
2. BM 70% (53-86%)
3. LN 58% (53-65%)

However, this is an invasive procedure which requires a hospital setting


with blood transfusion service and experienced clinicians for the
procedure. Thus, it may not always be applicable especially in remote
regions where VL is endemic.
Refer splenic, BM and LN aspiration from short case of Nitsibin (click here →
Splenic Aspiration , BM aspiration, LN aspiration )

After aspiration sample can be used for microscope smear evaluation or


Culture in NNN media

b. Microscopic smear evaluation

Pictures (National malaria guideline 2nd edition); Identification of the Leishmania


parasite; Leishmania amastigotes are oval or round and are usually seen in the
cytoplasm of monocytes. Free parasites may be seen if the host cells are
ruptured during preparation of the film.

FIGURE 221-1(Harrison 21st edition); A macrophage with numerous intracellular


amastigotes (2 - 4 μm) in a Giemsa-stained splenic smear from a patient with
visceral leishmaniasis. Each amastigote contains a nucleus and a characteristic
kinetoplast consisting of multiple copies of mitochondrial DNA. A few
extracellular parasites are also visible.

Leishmania amastigotes seen and indicate the grade. Examine at least


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The average amastigote density is graded as follows;


o 6+: > 100 parasites per field (viewed with a 10× eyepiece and
100× oil-immersion lens)
o 5+: 10 - 100 parasites per field
o 4+: 1 - 10 parasites per field
o 3+: 1 - 10 parasites per 10 fields
o 2+: 1 - 10 parasites per 100 fields
o 1+: 1 - 10 parasites per 1000 fields
o 0: 0 parasite per 1000 fields

c. Culture in NNN (Novy-mcNeal-Nicolle) media

Promastigote grows within 4 weeks after inoculation


This technique remains restricted to referral hospitals or research
centers.

2. Antibody Detection
Immunodiagnostic techniques, which have been extensively used for the
diagnosis of VL include;
o Enzyme-linked immunosorbent assay (ELISA)
o Immunofluorescent antibody test (IFAT)
o Freeze-dried direct agglutination test (FD-DAT) or aqueous
antigen direct agglutination test (AQ-DAT)
o Fast Agglutination Screening Test (FAST)
o Indirect hemagglutination test (IHA)
o rK39 immunochromatographic (rk39-ICT) strip test and
o rK39 ELISA
However, all of these tests have two major limitations;
o First, they do not distinguish between present and past infections,
as the serum antibody level remains high after successful
treatment. Detection of relapse is not possible with these
methods.
o Second, all these tests fail to differentiate between symptomatic
and asymptomatic infections.
o As a consequence, a significant proportion of healthy individuals
in the endemic area with no history of VL are positive for anti-
Leishmanial antibodies.
The performance of the various serological tests in the diagnosis of VL
is found to be
good to excellent; their sensitivity and specificity is ranging from 70 to
100%.
However, the facilitation of some of these tests (ELISA, IFAT, IHA) in
the field where the disease is prevalent is limited because they need
well-equipped laboratory and skilled personnel.
Of all these tests, DAT and rK39 have been extensively evaluated and
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rK39 (recombinant kinase 39) strip test


Common and available in Ethiopia.
Serologic (antibody strip) test for VL
Have 72% to 94 % sensitivity and 67 % to 98 % specificity
✓ More Specific and sensitive (reach up to 99%) in non-endemic
area like south east Asia (India)
✓ Not specific in endemic area like east Africa (Ethiopia, Sudan,
Kenya)
Used for screening purpose
Rk-39 may be False positive in the following conditions
o If Vrial markers (HBsAg or HCV ab) are +ve
o RVI patient
o TB
o HMS
o Leukemia
For more refer ‘’Common Laboratory Investigations with practical points
and procedures’’ from Short case of Nitsibin (click here → 26.5.9 rk- 39
Rapid Diagnostic Test)

DAT (direct agglutination test)


✓ Has 95% sensitivity and 72 % to 93 % specificity
✓ Anti-leishmanial titre (IgG)
✓ DAT is a semi-quantitative test that uses V-shaped micro-titter
plates in which increasing dilutions of patients’ serum or blood
are mixed with killed and stained freeze dried or aqueous
Leishmania donovani promastigotes.
✓ If specific antibodies are present agglutination will be visible
within 18 hours

3. Antigen Detection Test


The antigen detection test is an ideal test because it is more specific
than the antibody-based immunodiagnostic test.
It helps to distinguish active from past infections.
This method is also useful in cases with a deficient antibody production,
as in AIDS patients.
A urine latex agglutination (KATEX) that detects heat-stable, low
molecular weight carbohydrate antigen in the urine of VL patients has
been developed.
The evaluation of the performance of KATEX at the Indian subcontinent
and East Africa has shown that this test has a good specificity but only
a low to moderate sensitivity.

4. Leishmania skin test (Montenegro skin test)


✓ Intra dermal inoculation of leishmania (i.e. whole or killed promastigote)
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✓ +ve test; if there is induration/erythema ≥ 5mm within 48 - 72 hr’s of


inoculation
✓ +ve after 2 - 24 months of infection
5. PM (peripheral morphology)
LD (leishmania donovani) body → amastigote seen by microscopy
PM also important for hematologic malignancy (e.g. full of neutrophil in
CML
6. CBC
Anaemia or pancytopenia
Hyper gamma albuminemia (activation of poly clonal B cells)
Eosinophilia (reactive lymphocytosis/monocytosis)
7. Coagulation profile
8. PICT
Screen all VL pt for RVI and Treat VL 1st then initiate ART. If not, they
will develop IRIS
For mgt purpose (e.g Ambisome is used in RVI - VL treatment)
9. OFT
✓ LFT and Liver enzymes
✓ RFT → amphotericin B, SSG and paromomycin are nephrotoxic
10. ECG, CXR, ECHO
Done as baseline and follow up
ECG for SSG treatment CXN (arrythmia)
CXR for 2ry infection like TB, Pneumonia (2ry TB infection is cmn in VL
patients)
11. Molecular Techniques
Compared to the other diagnostic techniques available, the molecular
approaches remain expensive and technically highly demanding. Their
applicability in the endemic areas is highly questionable (in our setup to
costly not applicable).
molecular methods for Leishmaniasis diagnosis include
o pulsed-field gel electrophoresis
o multilocus enzyme electrophoresis and
o PCR-based assay

PCR-based assay

PCR based assays currently constitute the main molecular diagnostic


approach of Leishmaniasis.
The major importance of is its high sensitivity and specificity (up to
100%) irrespective of the species or genus.
Second, the burden of infection could be assessed by PCR. This may
be highly relevant in monitoring disease progression and outcome of an
anti-Leishmanial therapy.
Third, the viability of detected parasites could be demonstrated by other
forms of nucleic acid-based techniques, reverse transcription real time
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PCR (which is expensive), or less expensive protocol quantitative nucleic


acid sequence-based amplification [QT-NASBA].
Fourth, Leishmania species and strain identification can be performed by
a series of PCR-based assays. This is useful for the clinical
management due to the link between Leishmania species, and disease
severity and treatment outcome.
Finally, a molecular diagnosis might allow defining parasite-specific
features, such as virulence and drug resistance, and so-called parasite
tracking, if highly discriminatory fingerprinting tools are employed.
However, PCR-based protocols need standardization and optimization.
12. Animal inoculation
Inoculate by infected specimen
Then examine the animal for sign of infection
13. Chromosomal study
✓ Philadelphia chromosome of CML
✓ So, for CML do chromosomal study (not available in our setup) and PM

Tip→ from the above list those written in bold


and blue letter commonly done in our set up

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Diagnosis Algorithm for VL in Ethiopia

Figure: Diagnosis Algorithm for VL in Ethiopia

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Discussion

13.1 Leishmaniasis
➢ Leishmaniasis is a vector-borne disease caused by protozoan parasite of the
genus Leishmania.
➢ It is transmitted by the vector phlebotomine sand fly.
➢ Some of the Leishmania species known to cause disease in humans are:
▪ L. donovani species complex (including L. donovani and L.
infantum/chagasi)
▪ L. major
▪ L. tropica
▪ L. aethiopica,
▪ L. braziliensis and
▪ L. mexicana species complex.

Epidemiology

➢ The disease is endemic in environments that range from deserts to rain forests
in rural and urban settings in over 98 countries of the tropics, subtropics, and
southern Europe.
➢ Estimations of the burden caused by the Leishmaniasis disease in the world is
challenging.

Leishmaniasis burden In Ethiopia

➢ In Ethiopia, cutaneous leishmania (CL) is distributed mainly in the highlands on


an elevation between 1,400 - 3,175 meters above sea level.
➢ According to the 2012 WHO global Leishmaniasis estimate, Ethiopia is one of
the 10 high burden countries for CL.
➢ VL is predominantly found in the lowlands with varying degrees of endemicity.
➢ It is estimated that the annual burden of VL ranges from 2,000 to 4,500
cases.
➢ The endemicity of VL was recently extended to at least five administrative
regions, namely, Amhara, Tigray, SNNPR, Oromia and Somali. In addition,
there have been recent outbreaks in northern and southern parts of the
country: Libo Kemkem Woreda in Amhara region, T/Adiabo Woreda in Tigray
region and Imey in Somali region.

Life cycle of Leishmania

Leishmania parasites are digenetic parasites that need two hosts, the sandfly
and a mammalian host, to complete their life cycle (see picture below).
Over 20 Leishmania species are pathogenic to humans and 30 sandfly species
are proven in the vectors.
There are two ways of transmission of Leishmaniasis. These are;
▪ Zoonotic → which includes animal reservoir hosts, mainly dogs, in the
transmission cycle, or
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▪ Anthroponotic → in which humans are the sole source of infection for


the vector.
Moreover, different species of phlebotomine sandflies need different habitats to
survive and have different biting preferences (in/outdoor, forest/ village,
day/night). This has consequences for the transmission of the disease and
control measures to be applied.
VL in Ethiopia is caused by L. donovani with an anthroponotic transmission.

Picture; Life cycle of Leishmania; Leishmaniasis is transmitted by the bite of infected


female phlebotomine sandflies. The sandfly injects the infective stage (ie, promastigotes)
from its proboscis during blood meals (1). Promastigotes that reach the puncture wound
are phagocytized by macrophages and other types of mononuclear phagocytic cells (2). In
these cells, progmastigotes transform into the tissue stage of the parasite (ie, amastigotes)
(3), which multiply by simple division and proceed to infect other mononuclear phagocytic
cells (4). Parasite, host, and other factors affect whether the infection becomes
symptomatic and whether cutaneous or visceral leishmaniasis results. Sandflies become
infected by ingesting infected cells during blood meals (5,6). In sandflies, amastigotes
transform into promastigotes, develop in the gut (in the hindgut for leishmanial organisms
in the Viannia subgenus; in the midgut for organisms in the Leishmania subgenus) (7) and
migrate to the proboscis (8).

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Table; Leishmania Parasite, Their significance and Vectors


In Ethiopia
Old/new world Parasite Significance Vectors
Old world L. aethiopica Cutaneous leishmaniasis (CL), P. longipes
Diffuse cutaneous leishmaniasis P. pedifer
(DCL), Mucocutaneous P. sergenti
leishmaniasis (MCL)
L. tropica Cutaneous leishmaniasis (CL) P. sergenti
P. saevus
L. major P.
duboscqi
New world L. donovani Visceral leishmaniasis (VL) P. martini,
P. Celiae
P.
orientalis
All over the world
Old world L. aethiopica Cutaneous leishmaniasis (CL)
L. tropica
L. major
New world L. panamensis
L. guyanensis
L. peruviana
L.mexicana
L. brazilliensis
Old world L. aethiopica Mucocutaneous leishmaniasis (MCL)
new world L. panamensis
L. guyanensis
L. brazilliensis
Old world L. aethiopica Diffuse cutaneous leishmaniasis
new world L. amzonensis (DCL)
L.mexicana
Old world L. donovani Visceral leishmaniasis (VL)
old & new L. Infantum
world
new world L. Chagasi

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The clinical forms range from the self-healing localized cutaneous form (LCL)
to the more complicated non-self-limiting mucocutaneous form (MCL) and
diffused cutaneous (DCL) forms to the potentially fatal visceral form (VL, also
called kala-azar).

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13.2 VL; Visceral Leishmaniasis/kala-azar/ (ካላዛር ፣ ጓቋ፣ ድባ)

➢ VL (also known as kala-azar, a Hindi term meaning “black fever”) is is the


severe form of the disease, caused by the Leishmania donovani complex,
which includes L. donovani and Leishmania infantum (the latter designated
Leishmania chagasi in the New World); these species are responsible for
anthroponotic and zoonotic transmission, respectively.
➢ India and neighboring Bangladesh, Sudan and neighboring South Sudan,
Ethiopia, and Brazil are the four largest foci of VL and account for 90% of the
world’s VL burden.
➢ VL in Ethiopia is caused by L. donovani by an anthroponotic transmission.
➢ Most infections in immunocompetent individuals remain asymptomatic.
➢ The parasites replicate within the mononuclear phagocytic cells and
disseminate throughout the reticulo-endothelial system when the immunity is
weak.
➢ The incubation period typically ranges from 2–6 months, but it can also range
from a few weeks to years.
➢ See clinical features from approach part above.

13.2.1 Management of VL

The objectives of VL treatment are to:


▪ Reduce the parasite burden
▪ Prevent drug resistance
▪ Avoid toxic drug effects, and
▪ Improve the clinical condition of patients and to manage complications
(anemia, malnutrition and secondary infections)

Supportive Management

Nutrition:
▪ VL patients require adequate nutrition, vitamin and micro-nutrient
supplementation to speed up recovery, improve treatment response and
decrease or avoid the risk of relapse.
▪ Measure nutritional status with BMI or weight for height and follow the
national nutrition guideline (national protocol) for management.
Management of Anemia:
▪ VL patients often present with moderate to severe degree of anemia due
to bone marrow infiltration by the Leishmania parasite, hypersplenism,
auto-immune reactions or bleeding.
▪ Epistaxis could occur due to thrombocytopenia and mucosal infection. If it
is severe nasal packing and posterior epistaxis balloon might be
required.
▪ The anemia may require transfusion if severe.

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First-Line Regimens for Primary VL

The first-line drugs for the management of primary visceral Leishmaniasis in


Ethiopia are a combination of antimonials with aminiglycosides and Liposomal
Amphotericin B for special situations as described below.
▪ Antimonials include Sodium Stibogluconate (generic SSG), and
meglumine antimoniate (Glucantime).
▪ The half-life of antimonials is about 2 hours and their elimination is
through the kidneys.
▪ SSG and Glucantime have similar mechanism of action, efficacy and side
effects.
▪ Preparation; Sodium Stibogluconate = 100mg/ml, Glucantime = 81mg/ml

Combination Therapy: Sodium Stibogluconate (SSG) and Paromomycin

sodium stibogluconate (20mg/kg /day), and paromomycin (15mg/kg /day), IM,


daily for 17 days
The preferred choice for its better safety and affordability. And also efficacy of
90-94% in Ethiopia
The efficacy of the combination therapy is similar to that of the pentavalent
antimonials monotherapy, with the advantage of a decreased toxicity, shorter
treatment duration and cheaper cost.
Currently SSG and paromomycin can be administered at the same time but in
two separate injections, i.e., one in either buttock or the PM injection in
another IM area. Please, also note that the Paromomycin injection is a very
small volume injection.
Several studies in India have recently shown that three separate combinations
demonstrate high cure rates. These have yet to be investigated in the
Ethiopian context. These include;
▪ liposomal amphotericin B (LAmB) plus miltefosine, or
▪ LAmB plus Paromomycin, or
▪ Miltefosine plus Paromomycin

B. Sodium Stibogluconate or Meglumin Antimoniate (Monotherapy)

SSG, 20mg/kg/day, IM or or by a slow IV infusion within 5 minutes., daily for


30 days
In the absence of or in case of stock ruptures of Paromomycin, Pentavalent
antimonials can be used in monotherapy
Consideration should be given in Leishmaniasis patients with edema to avoid
overdosage.
Weekly weight measurements need to be made and the dosage should be
recalculated accordingly.

Precautions during the use of antimonials : These may require stoppage of the
drug and a possible shift of treatment to AmBisome:

Acute pancreatitis with abdominal pain and vomiting


Jaundice developing while on treatment
Elevated liver function tests (5 times of the normal value)
Elevated creatinine level
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Evidence of cardio-toxicity
Uninterrupted severe vomiting
Declining hematologic parameters, and
Failure to respond to treatment after two weeks of drug treatment

➢ VL Patients, who require a close follow-up during treatment with antimonials


include, those with;
▪ A very high or low age
▪ Severe illness
▪ Severe anemia
▪ HIV co-infection or
▪ Severe malnutrition
➢ Although resistance to antimonials is an issue in other countries, the response
rate for SSG in Ethiopia is good currently especially for those who are not co-
infected with HIV.

Liposomal Amphotericin B (LAmB, AmBisome)

Liposomal Amphotericin B is the safest drug, it is also the most expensive


one.
It is the first-line treatment for VL in special situations. Hence, Liposomal
Amphotericin B is recommended in those patients with;
▪ Pregnancy → As the use of antimonials is not safe in pregnant women
due to the higher risk of miscarriage, its use is not recommended where
there is an alternative drug to use.
▪ HIV-co-infection → this is because, the use of antimonials in
Leishmania/HIV co-infected patients is found to be less effective with
higher and frequent relapse rates and severe (fatal) toxicity.
▪ Severe illness
▪ Severe anemia
▪ Severe malnutrition
▪ Extremes of age (below 2 years or above 45 years).
▪ In special situations with severe risk factors for death at the patient’s
admission, antimonials toxicity has proved to be very high and, therefore,
LAmB is preferable if available for these patients.

Second-Line Treatment for Primary Visceral Leishmaniasis

The second line treatment for VL in Ethiopia is Liposomal Amphotericin.


Indications for the use of second-line VL treatment are;
▪ Drug toxicity
▪ Relapse
▪ Treatment failure
▪ Very severe illness
▪ Pregnancy and
▪ VL/HIV co-infection.

Liposomal Amphotericin B (AmBisome)


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➢ Dosage and Administration:


▪ AmBisome, 5mg/kg/day over a period of 6 days (i.e. 30mg/kg in total).
▪ It is administered by reconstitution with 5% D/W; with a volume of 100ml
of D/W for 50mg of AmBisome
• AmBisome vials contain 50 mg/ml.
• for 100mg or 2 vials of AmBisome 200ml of D/W, for 3 or more
vials use all the 500ml D/W.
▪ It is advised to use whole vials to avoid wastage but the drug should be
discarded after 24 hours of reconstitution.
▪ The infusion can run over 30 to 60 minutes
➢ Liposomal Amphotericin is a lipid formulation of Amphotericin B in which the
drug is packaged with cholesterol and other phospholipids within a small
unilamellar liposome.
➢ This is an extremely safe and efficacious drug for the treatment of visceral
Leishmaniasis.
➢ ts main disadvantage is its high cost.

Miltefosine

This is the only oral anti-leishmanial drug


Taken at a dose of; 2-3mg/kg/day (100mg/day for > 25kg) for 28 days.
Miltefosine is an alkyl phospholipid (hexadecacylphosfocholine), originally
developed as an oral anticancer drug that has shown to have anti-
leishmanial activity.
In one study in Ethiopia, Miltefosine was found to be less effective but safer
than antimonials in HIV/VL co-infected patients.
Miltefosine is potentially teratogenic and, thus, it is contraindicated during
pregnancy.
▪ Lactating women and women of childbearing age must use effective
contraception during the treatment and for 3 months afterwards.

C) Paromomycin (Aminosidine)

Paromomycin is an aminoglycoside antibiotic (Pharmacologic Category;


Amebicide).
paromomycin (15mg/kg /day), IM. The 15mg/kg sulphate is equivalent to
11mg/kg base, whereas 20mg/kg sulphate is equivalent to 16mg/kg base.

Primary VL treatment algorism

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13.2.2 Patient Follow-Up in Management of VL

Patient monitoring is vital during VL treatment as the currently used


antileishmanial drugs are toxic.
Hence, patients should be invariably admitted for visceral Leishmaniasis
treatment, close monitoring of drug adverse effects, supportive management,
and follow-up of patient’s progress
During treatment patients require a strict follow-up of their response to
treatment and drug side effects.
Follow-up on clinical parameters including
▪ Fever
▪ spleen size and
▪ patient wellbeing is important.
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laboratory tests for follow up include;


▪ a hematologic profile
▪ chemistry
▪ ECG
▪ Radiography.
Prevention and treatment of secondary infections, diagnosis and treatment of
complications and nutritional supplementation are important during the treatment
of visceral Leishmaniasis.
At the end of therapy, the outcome of the treatment should be recorded based
on the status of the patient as discharged/improved, cured, treatment failure,
relapse, referred or defaulted.
At discharge, the patient should be given regular appointments 3 and 6
months after the treatment.
The patient should be advised to visit the health facility for recurrence of the
clinical features and/or appearance of skin rash.

Evaluating Cure

➢ At the end of VL treatment, patients should be re-assessed for response


clinically or using laboratory tests.

Clinical Response

Many patients get worse during the first few days of treatment with SSG.
After 7 to 10 days, patients become afebrile and begin to look stronger with
increased alertness and
appetite.
By day 14, the spleen size regresses, the Hgb level rises and there is weight
gain in the absence of edema.
At the end of successful treatment, patients look improved, afebrile, and usually
have a smaller spleen size than on admission and have an increased Hgb
level.
Look for signs of co-existing TB or HIV, both of them will increase the risk of
treatment failure.
Cure is best defined as the absence of clinical features of the disease after
completion of the recommended dose and duration of treatment for VL in
addition to a negative parasitological test for LD bodies.

Initial Parasitological Cure

➢ Test of cure (TOC) is performed at the end of treatment when there is no or


insufficient clinical improvement and in treatment of relapse for decision to stop
treatment.
➢ There is no clinical sign that best correlates with a positive test of cure or that
predicts an increased risk of relapse.
➢ Clinical evaluation should get the priority over a test of cure for every patient
under the currently available invasive procedures.
➢ TOC should be reserved for cases where response is in doubt, in the
treatment of relapses and for monitoring emergence of drug resistance.
➢ In addition, TOC is done to assure that discharge is appropriate for patients
who may have difficulty returning for follow-up.
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➢ There must be 2 negative tests of cure (TOC) results before discharging


patients with VL relapse.
➢ The tests are done one week apart to ensure that there is at least a week of
treatment after the first negative TOC.
➢ The likelihood for a positive TOC after treating a relapse is higher than 10%
and any further relapses will be more difficult to cure.
➢ In some situations, it is better to refer patients with VL relapse for treatment
into a hospital setting.

Positive Parasitology (TOC) at the End of Treatment

f the TOC is scanty positive, continue the same treatment until two consecutive
weekly aspirates are negative.
The limit of duration of therapy is 60 days for SSG and a total dose of
40mg/kg for AmBisome, if at this point the TOC is still positive, use a 2nd line
treatment.
Non-response is defined as failure to decrease the parasitological grade after
adequate treatment.

Definitive Test of Cure

➢ It is not a routine practice to do TOC at the 6th month of patient follow-up if


the patient does not fit for clinical visceral Leishmaniasis.
➢ Relapse is diagnosed when a patient with VL treatment history presents with
clinical visceral Leishmaniasis and is diagnosed with positive parasitology (LD
bodies) after successful completion of the treatment.
➢ Re-infection is possible for VL but most cases are considered as relapse and
treated accordingly.
➢ Clinical judgement will always play the final role in any decision-making
process given the variability of individual VL cases.

13.2.3 VL Relapse
A patient who is diagnosed with VL for the first time is called a primary VL
case.
A definitive cure is the absence of VL signs and symptoms and a negative
test of cure 6 months after initial cure, i.e., 6 months after active diseases
treatment.
Patient follow-up is important to establish a definite cure with proper evaluation
on appointment or when presented with fever, loss of weight, anemia and
splenomegaly.
▪ For definitive cure, one looks at the clinical picture of the patient; tissue
aspirate may not be necessary at follow-up sessions unless a relapse is
clinically suspected.
If a person returns with clinical features and a positive parasitology consistent
with visceral Leishmaniasis, after having been successfully treated for primary
VL and discharged improved or with a negative test of cure (TOC), the patient
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It is impossible to differentiate relapse from new infection but various molecular


studies proved relapse to be more common than re-infection.
In immune-competent individuals, VL relapses can occur in up to 5% of the
patients treated, whereas VL relapses can occur in up to 50% in HIV/VL co-
infected cases.
Most relapses occur within the first 6 months of initial treatment and are
referred to as a first relapse if the relapse occurs for the first time and
subsequent relapses are called second, third and so on depending on the
number of relapses.
Risk factors for a VL relapse in HIV patients are:
▪ AIDS patients not on ART
▪ Low CD4+ count
▪ Previous VL episodes and failure to achieve clinical or parasitological
cure during the first episode.
ART could help to delay VL relapse but it does not prevent it. Sometimes
relapses tend to have a higher parasite load and are often difficult to treat.

Treatment Regimens for First VL Relapse (see the Treatment


Algorithm!)

➢ If possible, the regimen used for the treatment of relapses should be a


different drug than that used for primary VL.
➢ The use of combination therapy with SSG and Paromomycin is recommended
if it was not used for the treatment of prior VL episodes.
➢ When choosing a drug for treating a relapse the response to the initial
treatment should be considered.
➢ The following regimens are recommended for the treatment of VL relapses
▪ Liposomal amphotericin B 5mg/kg/day for a period of 6 days.
• The treatment period can be extended up to 14 doses for better
therapeutic advantages.
▪ SSG 20 mg/kg/day for 40days until 2 consecutive weekly aspirates for
parasitology
are negative.
• If Test of cure (TOC) is still positive, SSG should be given for a
total of 60 days with close monitoring of drug toxicity and TOC
checked again, if positivity persists, then 2nd line treatment must be
used.
▪ SSG/PM combination: SSG (30 days) and Paromomycin (17 days) can
be used for VL relapse treatment.

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Note:

Severely ill VL patients may require an extended dose of AmBisome if the test
of cure (TOC) is positive after the end of 40mg/kg total dose of AmBisome.
Patients with an extended dose of SSG require close safety monitoring.

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13.2.4 Treatment of VL by Drug Interruption

➢ VL treatment can be interrupted by the treating clinician due to a medical


reason by the treating clinician or by a failure of the patient.
➢ These patients are at high risk and also potential sources of disease
transmission. Therefore, they should be treated.
➢ The treatment of VL after drug interruption depends on the duration of the
interruption period as summarized in the table below:

The duration of Action


treatment interruption
< 5 days Continue the same treatment until the full course
without compensating the missed treatment days.
between 5 - 10 days Continue the same treatment until the full course but
with compensation.
> 10 days Restart treatment as day one.

➢ These group of patients require test of cure (ToC) at the end of the treatment

Prognosis of VL Treatment

If untreated, VL is invariably fatal. In a well-established treatment center, the


mortality of patients with VL treatment is below 10%.
Predictors of bad prognosis are;
▪ AIDS patients with a low CD4 count
▪ Very young or very old patients
▪ Patients with suffer from the disease for more than 5 months prior to
their presentation
▪ Severe anemia
▪ Severe malnutrition
▪ Severe opportunistic infections
▪ Thrombocytopenia
▪ Relapsing course of the disease
▪ Patients with vomiting
▪ Patients in a state of collapse, and
▪ Patients without secondary prophylaxis.

13.2.5 RVI - VL co infection


VL is an AIDS-defining condition and co-infected patients present the WHO
stage 4 (CDC stage C) of the disease.
They have very low CD4+ cell counts and high viral loads (1000 to 1 million
copies).
In some parts of Ethiopia (e.g. Humera), about 30% of all VL patients are co-
infected with HIV.
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▪ HIV infection increases the risk of developing VL by a factor between


100 and 1000 in endemic areas.
▪ It reduces the likelihood of therapeutic response, and greatly increases
the probability of relapse.
▪ At the same time, VL promotes the clinical progression of the HIV
disease and the development of AIDS-defining conditions.
▪ As the two diseases target similar immune cells, together they exert a
synergistic damaging effect on the cellular immune response with a
significant reduction of the TLC and CD4 cells.
▪ Atypical presentations of Leishmaniasis are reported in HIV patients,
especially in those with a CD4 count less than
200-cells/μL.
▪ Relapses are more common in this group of patients.

Diagnosis

➢ Disease manifestations of VL in HIV-infected individuals without severe


immuno-suppression are similar to those in immuno-competent persons.
➢ Among those with advanced immuno-suppression and low CD4+ T-lymphocyte
counts, manifestations of Leishmaniasis may be more severe, atypical and with
a chronic and relapsing course after treatment.
➢ Although a deficit in host humoral and cellular response induced by both, HIV
and Leishmania infections, results in a somewhat reduced sensitivity of
serological and delayed-type IV hypersensitivity-based tests, studies in Ethiopian
co-infected patients have demonstrated acceptable sensitivity.
➢ The gold standard for the diagnosis of Leishmaniasis in HIV-infected patients
remains the isolation or identification of the parasite in spleen, lymph node or
bone marrow aspiration.
➢ Amastigotes can also be found in the peripheral blood of a proportion of HIV-
infected individuals.
➢ Where HIV counseling and access to antiretroviral treatment are available, all
VL patients should be screened for HIV. Vice versa, in endemic foci for VL,
the HIV services should suspect VL in patients with clinical symptoms for VL
or unexplained deterioration of an HIV patient after other opportunistic
infections are ruled out.
➢ The presence of a HIV co-infection may alter the clinical presentation of
patients so that atypical sites (non-reticuloendothelial organs) tend to be more
involved. These include;
▪ Oral mucosa
▪ Gastrointestinal and
▪ Concomitant diffuse skin involvement by the parasite
Generally, the presence of a co-infection with HIV alters;
▪ The clinical picture
▪ The laboratory diagnosis and interpretation
▪ The response to treatment
▪ The occurrence of side effects, and
▪ The frequency of recurrences after treatment.

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Treatment of First Episode (Primary) Kala Azar in VL/HIV Co-


Infected Patients
(see the Treatment Algorithm below)

If VL is present in an HIV-positive patient, ART should be started after VL


treatment, regardless of the CD4+ cell count.
When there is a history of VL, but the patient is currently asymptomatic, a
CD4+ count should be done and the national HIV treatment guidelines should
be followed.
Start ART ASAP to prevent further opportunistic infections and VL relapses,
although ART alone will not prevent VL relapses.
All anti-Leishmanial drugs are less effective in HIV-positive patients and the
risk of relapse is high with them.
Most relapses occur within 3-9 months, successive relapses become less
typical and less acute, but more frequent.
Moreover, with each relapse, patients become less responsive to treatment and
eventually unresponsive to all drugs.
Due to the overlapping toxicity between drugs (SSG and Amphotericin B) and
some of the ARVs, ART should be initiated after completing VL treatment,
unless the risk of delaying ART outweighs the risk of potential drug toxicity.
In patients already on ART, VL treatment with AmBisome is preferred and ART
can be continued.
SSG is more toxic in HIV patients, necessitating careful monitoring.
It is advisable to provide bed nets to VL/HIV co-infected patients because it
might help in reducing the risk of transmission.
Anti-leishmanial drug combination therapy may be the way to delay the
emergence of resistance and increase antimicrobial activity. However, it is
probable that even drug combinations will not prevent relapses altogether,
leaving ART as the key in reducing and postponing relapses.

First-Line Drugs for First Episode (Primary) Kala Azar in VL/HIV Co-Infected
Patients:

➢ AmBisome (LAmB)
▪ AmBisome with a total dose of 40mg/kg in divided dose can be used for
the treatment of VL in HIV co-infected individuals.
▪ If TOC is still positive but with a significant parasite load reduction, the
treatment with AmBisome can be repeated until TOC becomes negative.
▪ If TOC positivity persists after repeating AmBisome, a compassionate
treatment regimen should be used.
▪ However, if the parasite load does not decrease significantly after the
initial AmBisome 40mg/kg therapy, SSG for 60 days and above should
be considered as therapy bearing in mind that safety
monitoring by qualified medical personnel is necessary.
▪ If even after the SSG therapy TOC is still positive, a compassionate
regimen should be used.

Second-Line Drug for Primary Kala Azar in VL/HIV Co-Infected Patients:


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Pentavalent antimonials
▪ It is administered at a dose of 20mg antimony/kg/day, IV or IM, for 30
days.
▪ Adverse effects of the drug are more frequent in HIV infected patients.

Risk factors for death

➢ Risk factors for death That should be considered for all VL patients (with more
emphasis for VL/HIV co-infected individuals) include;
▪ Malnutrition
▪ Concomitant opportunistic infection (TB or pneumonia)
▪ Diarrhea or vomiting
▪ Anemia
▪ Bleeding and
▪ Signs of toxicity during treatment (heart failure, arrhythmia, pancreatitis,
jaundice, kidney failure, anemia, severe vomiting or diarrhea).
➢ After treatment of the first episode, assess for fever, weight, general condition,
spleen size, and hematologic values to see the clinical improvement and ideally
demonstrate parasitological cure (TOC) to endure that discharge is appropriate.
➢ If the test is positive, continue treatment, or substitute to a second-line regimen
and exclude other opportunistic infections

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Note:

In VL/HIV co-infected individuals, SSG 60+ may be considered while safety


monitoring is warranted to the patient.
The 40mg/kg AmBisome schedule is on days 1 to 5 and then on the 10th,
17th and 24th day.
If the Test of cure (TOC) is positive after treatment with AmBisome 40mg total
dose, compassionate treatment may be required. These include SSG/PM,
SSG 60+, AmBisome /Miltefosine combinations, etc.

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Management of VL Relapses in VL/HIV Co-Infected Patients

➢ Relapse of VL is a common phenomenon in HIV co-infected cases.


➢ This poses challenges to the control of Leishmaniasis.
➢ The drug chosen to treat relapse should be different from that used to treat
the first episode. However, in case of multiple relapses, the drug of choice
should not be a drug that has shown to be ineffective during any of the
previous treatment episodes.
➢ To avoid the development of drug resistance as a consequence of repeated
relapses, and to increase treatment efficacy, combinations of drugs should
ideally be used. However, there is still a lack of evidence for the best
combination for co-infected patients.
➢ The physician’s decision on combination treatment or compassionate treatment
should, therefore, be made on an individual basis.
➢ Due to lower efficacy of anti-Leishmanial drugs in HIV/VL extended treatment
courses may be required to achieve cure.
➢ In order to distinguish between drug unresponsiveness and partial or slow drug
responsiveness, it is recommended to do a TOC at the end of the standard
treatment.
▪ If there has been no parasitological response to treatment (demonstrated
by the same parasite grade found in the TOC as for diagnosis, or,
alternatively,) drug unresponsiveness is demonstrated, and treatment
should be continued with another anti-Leishmanial drug
▪ If standard treatment has resulted in a partial but significant
parasitological response (demonstrated by parasite density in the TOC
being at least two grades lower compared to the diagnostic assessment)
treatment with the same drug may be continued until two subsequent
negative TOCs have been obtained.

13.2.6 Post kala-azar Dermal Leishmaniasis (PKDL)


VL due to L. donovani occurs with a post treatment complication called PKDL.
PKDL is characterized by the occurrence of painless skin lesions relatively
common towards the end of treatment (more common in Sudan with about
50% of the cases) or shortly after treatment.
PKDL is rare in Ethiopian VL patients but it is relatively common in
Leishmania/ HIV co-infection.
PKDL patients harbor Leishmania parasites in the skin lesions and these can
be potential sources of infection and disease transmission.
Patients should be advised to seek medical attention and use impregnated bed
nets if they develop skin rash following treatment.
Depending on the severity of the lesion, PKDL can be graded (see table
below) which will facilitate treatment decisions.
Occasionally, PKDL may occur prior to the VL (Pre-kala azar dermal
Leishmaniasis) or concomitantly (para-kala azar dermal Leishmaniasis) to the
active VL disease.

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Table; Grading PKDL Lesions:


Grade 1 Scattered macular, papular or nodular skin rashes mainly on the
face and around the mouth, with or without some lesions on the
upper chest and upper limbs.

Grade 2 Dense macular, papular or nodular rashes covering most of the


face and which are extending to the chest, back, upper arms
and legs.
If lesions are extensive or blackened, this is called PKDL grade
2 severe form.
Grade 3 Dense macular, papular or nodular rashes covering most of the
body including hands and feet. Here, crusting, ulcers, sloughing,
scaling, blackening of skin and spreading of the lesions to
mucosa of the lips and the palate occur.

FIGURE 221-4 (Harrison 20th edition); Post - kala-azar dermal leishmaniasis in an Indian
patient. Note nodules of varying size involving the entire face. The face is erythematous,
and the surface of some of the large nodules is discolored.

Treatment of PKDL (Pre-, Para-, Post-Kala Azar Dermal Leishmaniasis)

➢ Not all PKDL patients need treatment; decision can be made depending on
severity of the lesion (PKDL Grade).
➢ As PKDL patients harbor the parasite, they can be a potential source of
infection and disease transmission.
➢ Patients should be advised to seek medical attention and use impregnated bed
nets (ITNs) if they develop skin rash following VL treatment.
➢ Most PKDL cases are Grade 1. The majority of the lesions heal spontaneously
within 12 months but need close follow-up.
➢ Indication for treatment;
▪ PKDL patients with a severe form of Grade 2 and Grade 3 lesions
and/or disfiguring disease
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▪ Those with lesions that have existed for more than 6 months
▪ Those with concomitant anterior uveitis/conjunctivitis and
▪ Young children with oral lesions that interfere with feeding

Antileishmanial options
Antimonials (SSG 20mg/kg/day for 30 days).
▪ Treat until lesions are flattened or are no longer palpable but
discoloration can still be visible.
▪ Do not wait until lesions disappear, sometimes longer treatment courses
are needed.
▪ Follow-up is passive as there are no parasite criteria for cure due to the
difficulties of demonstrating the parasite in the lesions.
▪ SSG toxicity is rare in PKDL treatment.
Miltefosine,100mg daily for 28 days
▪ Miltefosine has shown a beneficial effect for the management of PKDL in
large series of Indian patients.
▪ It demonstrated a shorter duration of therapy and a better compliance by
increasing the dose or duration of therapy.
▪ Instead of 100mg daily for 12 weeks, increasing the daily dose by using
50mg twice or trice per day could shorten the duration of therapy.
▪ In Ethiopia, two cases of PKDL have been successfully treated with
Miltefosine 100mg daily for 28 days. Thus, Miltefosine may provide an
opportunity for treating PKDL.

13.2.7 VL Treatment in Special Groups

Pregnancy:

➢ Evidence for the safety of anti-Leishmanial drugs is scarce.


➢ No VL drug is proven to be safe in pregnancy.
➢ Pregnant women should, therefore, be treated with the safest available anti-
Leishmanial drug as the disease is life threatening for the mother and may
have consequences for the fetus.
➢ Liposomal Amphotericin B is relatively safe and effective, while conventional
amphotericin B is nephrotoxic. Pregnant women are particularly vulnerable to
this.
➢ Dosage and administration are similar to other group of patients.
➢ In situations where there is no option, risk-benefit has to be assessed in the
use of SSG especially in the first trimester.

Malaria and VL:

➢ Due to the overlap in epidemiologic occurrence of both diseases, it is not


uncommon to find these fatal diseases occurring simultaneously.
➢ Malaria will be severe in patients with VL because VL patients are already
weak, with an ineffective spleen function and are already anemic.
➢ Screening for malaria is recommended for all VL patients admitted from malaria
endemic areas.
➢ Treatment of both diseases at a time needs attention due to the overlap of
drug side effects.
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➢ The following points should be taken into considerations during the


management of malaria-VL co-infection:
▪ SSG should not be used with quinine (due to the cardio-toxicity of both
drugs).
▪ Use ACT (Coartem) in uncomplicated falciparum malaria cases or
Artemether (intramuscular) in severe malaria cases.
▪ If treatment with quinine is inevitable, stop SSG while quinine is being
given. After quinine treatment is finished, resume SSG to complete the
recommended duration of treatment starting 24 hours after the last dose
of quinine.
▪ If quinine needs to be used, consider shortening quinine usage for 3-5
days and finish with Coartem full dose to help to resume SSG within a
short period.
▪ Consider Artemether as a suitable alternative for quinine.

3. Management of Concomitant Infections in VL

➢ Patients with VL are generally immuno-compromized and can get infections


with bacteria, parasites and mycobacteria
➢ Pneumonia
▪ It is one of the commonest co-morbidities with VL leading to increased
morbidity.
▪ VL patients with pneumonia require vigorous treatment with broad-
spectrum antibiotics.
▪ Consider also tuberculosis if there is no response to an appropriate
antibiotic treatment
Diarrhea
▪ Diarrhea is the principal cause of death in VL patients.
▪ The diarrhea may be watery, mucoid or bloody with variable causative
agents.
▪ It needs aggressive therapy with hydration and proper antibiotics.
▪ The choice of antibiotics is based on the result of stool examination.
Other infections that can occur with VL, like skin infections, cancrum oris, and
otitis media, also require treatment.

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13.3. Cutaneous Leishmaniasis (CL) /ቁንጭር/

L. aethiopica causes more than 99.9% of the CL cases in Ethiopia.


▪ L. major and L. tropica have been isolated from sandfly vectors and one
case of CL due to L. tropica was reported
CL can be broadly divided into Old World and New World forms (see table from
life cycle of leishmania above).
▪ Old World CL caused by Leishmania tropica is anthroponotic and is
confined to urban or suburban areas throughout its range.
• Zoonotic CL is most commonly due to Leishmania major, which
naturally parasitizes several species of desert rodents that act as
reservoirs over wide areas of the Middle East, Africa, and central
Asia.
▪ New World CL is mainly zoonotic and is most often caused by
Leishmania mexicana, Leishmania (Viannia) panamensis, and Leishmania
amazonensis.
• A wide range of forest animals act as reservoirs, and human
infections with these species are predominantly rural.
Local outbreaks of human disease are common.
Major outbreaks currently affect Afghanistan, Syria, Iraq, Lebanon, and Turkey
in association with refugees and population movement.
CL is increasingly seen in tourists and military personnel on mission in CL-
endemic regions of countries and as a co-infection in HIV-infected patients.
Leishmania aethiopica is restricted to the highlands of Ethiopia, Kenya, and
Uganda, where it is a natural parasite of hyraxes.

Clinical Features

➢ A typical history (an insect bite followed by the events leading to ulceration) in
a resident of or a traveler to an endemic focus strongly suggests CL.
➢ A few days or weeks after the bite of a sandfly, a papule develops and grows
into a nodule that ulcerates over weeks or months.
➢ The base of the ulcer, which is usually painless, consists of necrotic tissue
and crusted serum, but secondary bacterial infection sometimes occurs.
➢ The margins of the ulcer are raised and indurated. Lesions may be single or
multiple and vary in size from 0.5 to >3 cm (see figure below).
➢ Lymphatic spread and lymph gland involvement may be palpable LAP and may
precede the appearance of the skin lesion.
➢ There may be satellite lesions, especially in L. major and L. tropica infections
➢ The lesions usually heal spontaneously after 2–15 months. Lesions due to L.
major and L. mexicana tend to heal rapidly, whereas those due to L. tropica
and parasites of subspecies Viannia heal more slowly.
➢ L. mexicana is responsible for chiclero’s ulcer, the so-called self-healing sore of
Mexico.
➢ CL lesions on exposed body parts (e.g., the face and hands), permanent scar
formation, and social stigmatization may cause anxiety and depression and
may affect the quality of life of CL patients.

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Chapter 13; Leishmaniasis (ካላዛር/ጓቋ/ድባ/ እና ቁንጭር)

FIGURE 221-5 Cutaneous leishmaniasis in a Bolivian child. There are multiple


ulcers resulting from several sandfly bites. The edges of the ulcers are raised.

Differential Diagnosis

➢ Cutaneous tuberculosis
➢ fungal infections
➢ leprosy
➢ sarcoidosis, and
➢ malignant ulcers

Laboratory Diagnosis

Demonstration of amastigotes in material obtained from a lesion remains the


diagnostic gold standard.
▪ Microscopic examination of slit skin smears, aspirates, or biopsies of the
lesion is used for detection of parasites.
Culture of smear or biopsy material may yield Leishmania.
PCR is more sensitive than microscopy and culture and allows identification of
Leishmania to the species level.

Treatment of Cutaneous Leishmaniasis

➢ The goals of therapy in cutaneous Leishmaniasis are;


▪ To kill the parasite
▪ To control its spread into mucosal disease,
▪ To accelerate healing and to reduce scarring, especially in cosmetic
sites.
➢ Although lesions heal spontaneously in the majority of cases, their spread or
persistence indicates that treatment may be needed.
➢ Treatment Options → There are 3 options for treatment of CL, which should
be discussed with the patient:
▪ To withhold treatment,
▪ Topical or local treatment, and
▪ Treatment with systemic drugs.
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Chapter 13; Leishmaniasis (ካላዛር/ጓቋ/ድባ/ እና ቁንጭር)

➢ The decision which option to offer depends on the nature of the lesions and
the ability of the patient to attend for treatment and to return for follow-up.

Withhold Treatment
As the majority of CL lesions heal spontaneously within a year, the best
treatment for patients who fulfill the following criteria are to withhold
treatment or to accept local treatment:
▪ Fewer than 2 lesions requiring immediate treatment;
▪ Lesions are smaller than 5 cm in diameter
▪ Absence of indurations or firmness of surrounding skin, on palpation no
mucosal involvement, or lesions are not close to the nose or the lips;
▪ Lesions are not on the border of the lip, the nostrils or the eyes;
▪ No potentially disfiguring or disabling lesion (on the nose, the joints, the
toes, or the fingers);
▪ No immuno-suppression
Patients who fulfill the above criteria need follow-ups to evaluate the progress
of the lesion(s) and to decide on their subsequent treatment.

B. Local Treatments
➢ A bacterial superinfection is uncommon, but when suspected, it should be
managed with appropriate antibiotics
➢ wound care before starting the CL treatment.
➢ Two methods of local CL treatment are commonly used in Ethiopia. These are;
▪ Intra-lesional administration of Sodium Stibogluconate (SSG)
▪ Cryotherapy
➢ Other local CL treatment methods, not applicable currently in Ethiopia, include;
▪ Curettage Under Local Anesthetic
▪ Thermotherapy under Local Anesthetic
▪ Topical Ointments
• One or a few small lesions due to “self-healing species” can be
treated with topical agents
• In Peru, Topical imiquimod (5 - 7.5%) plus parenteral antimonials
have been shown to cure CL more rapidly than antimonials alone.
• An ointment containing 15% paromomycin sulfate, either alone or
with 0.5% gentamicin or 12% methylbenzonium chloride for 20
days.
➢ Intra-Lesion Administration of SSG:
▪ Small lesions (≤3 cm in diameter) may conveniently be treated weekly
with intra-lesional SSG for 4 to 6 weeks (until cure)
• an intralesional injection of a pentavalent antimonial at a dose
adequate to blanch the lesion (0.2 - 2 mL).
▪ But training and meticulous technique are essential for this method, in
which the injection must be administered intralesionally and NOT beneath
or around the lesion.
▪ Using a 1ml syringe with a fine intradermal needle, undiluted SSG is
injected into the lesion until it blanches. About 0.2-0.5ml may be
adequate for the first injection of a small nodule.
▪ Weekly reassessment is recommended with SSG re-injections if clinically
indicated.
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▪ Once the lesion has been disrupted, up to 2ml SSG may be needed to
infiltrate residual thickened areas.

C. Systemic Treatment

Systemic treatment is indicated for;


▪ Lesions over the face, hands, or joints
▪ Multiple lesions; More than 4 lesions
▪ Large ulcers
▪ Lymphatic spread; Lesions accompanied by nodular lymphangitis
▪ CL with the potential for development of ML
▪ CL in HIV-co-infected patients.
▪ ML or DCL
▪ Lesions which are bothersome to the patient but unsuitable for local
treatment
▪ Large lesions unsuitable for local treatment
▪ Patients not responding to topical treatment

first-line drug for all forms of CL


➢ Pentavalent Antimony Compounds (SSG) or Meglumine Antimoniate (MA)
▪ Dosage: 20mg SSG/kg/day IM or IV for 4 - 8 weeks29

Plus
➢ Paromomycin (16 mg/kg, IM daily for 20 to 30 days)
▪ CL due to L. aethiopica, which responds to paromomycin but not to
antimonials. So, in Ethiopia SSG is used with paromomycin due to Its
action as a synergistic with SSG against isolates of L. aethiopica
▪ CL caused by Leishmania (Viannia) guyanensis, for which pentamidine
isethionate is the drug of choice (two injections of 4 mg of salt/kg
separated by a 48-h interval) but not SSG

Relapses usually respond to a second course of treatment

Alternative
➢ Miltefosine and Liposomal Amphotericin B
▪ Miltefosine (2.5 mg/kg for 28 days) and Liposomal Amphotericin B are
effective in the treatment of CL in several countries, but have not yet
been used for L. aethiopica infections.

Adjuvant therapy

Azoles and triazoles have been used with mixed responses in both Old and
New World CL, but have not been adequately assessed for this indication in
clinical trials.
▪ In L. major infection, oral fluconazole (200 mg/d for 6 weeks) resulted in
a higher rate of cure and also cured infection faster.

29
Harrison [21st edition] recommends SSG, 20 mg/kg for 20 days, national Guideline of
788
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Chapter 13; Leishmaniasis (ካላዛር/ጓቋ/ድባ/ እና ቁንጭር)

▪ Ketoconazole (600 mg/d for 28 days) is effective in CL due to L. (V.)


panamensis and L. mexicana in Panama and Guatemala.

Follow-Up
➢ It is recommended that patients are routinely followed up 6 weeks and 6
months after the completion of treatment.
➢ Patients should be advised that recurrence is possible and that they should
return if that happens. Most relapses occur within 6 months after treatment.

13.4 Diffuse Cutaneous Leishmaniasis (DCL)

DCL is a rare form of leishmaniasis caused by L. amazonensis and L.


mexicana in South and Central America and by L. aethiopica in Ethiopia and
Kenya.
DCL is characterized by the lack of a cell-mediated immune response to the
parasite, the uncontrolled multiplication of which thus continues unabated.
Profound immunosuppression leads to widespread cutaneous disease.
Lesions may initially be confined to the face or a limb but spread over months
or years to other areas of the skin.
They may be symmetrically or asymmetrically distributed and include papules,
nodules, plaques, and areas of diffuse infiltration.
These lesions do not ulcerate.
The overlying skin is usually erythematous in pale-skinned patients.
The lesions are teeming with parasites, which are therefore easy to recover.
DCL does not heal spontaneously and is difficult to treat.
If relapse and drug resistance are to be prevented, treatment should be
continued for some time after lesions have healed and parasites can no longer
be isolated.
In the New World, repeated 20-day courses of pentavalent antimonials are
given, with an intervening drug-free period of 10 days.
Miltefosine has been used for several months with a good initial response.
Combinations should be tried.
In Ethiopia, a combination of paromomycin (14 to 15 mg/kg per day) and
sodium stibogluconate (10 mg/kg per day) is effective.
▪ paromomycin plus SSG in a synergistic dose, until amastigotes are no
longer found in slit skin smears and then for several more weeks or
months.

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Chapter 13; Leishmaniasis (ካላዛር/ጓቋ/ድባ/ እና ቁንጭር)

13.5 Mucocutaneous/Mucosal Leishmaniasis (ML)


➢ ML is typically caused by L. (V.) braziliensis and rarely by L. amazonensis, L.
(V.) guyanensis, and L. (V.) panamensis.
▪ In L. (V.) braziliensis infections, cutaneous lesions may be simultaneously
accompanied by mucosal spread of the disease or followed by spread
years later.
➢ Young men with chronic lesions of CL are at particular risk.
➢ Overall, ~3% of infected persons develop ML.
➢ Not every patient with ML has a history of prior CL.
➢ ML is almost entirely confined to the Americas. In rare cases, ML may also be
caused by Old World species like L. major, L. infantum (L. chagasi), or L.
donovani.

Clinical Features

The parasite spreads via the lymphatics or the bloodstream to mucosal tissues
of the upper respiratory tract.
Intense inflammation leads to destruction, and severe disability ensues.
Lesions in or around the nose or mouth (see figure below) are the typical
presentation of ML.
Patients usually provide a history of self-healed CL preceding ML by 1 to 5
years.
Typically, ML presents as nasal stuffiness and bleeding followed by destruction
of nasal cartilage,perforation of the nasal septum, and collapse of the nasal
bridge.
Subsequent involvement of the pharynx and larynx leads to difficulty in
swallowing and phonation.
The lips, cheeks, and soft palate may also be affected.
Secondary bacterial infection is common, and aspiration pneumonia may be
fatal.
ML does not heal spontaneously.

FIGURE 221-6; Mucosal leishmaniasis in a Brazilian patient. There is extensive


inflammation around the nose and mouth, destruction of the nasal mucosa,
ulceration of the upper lip and nose, and destruction of the nasal septum. 790
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Chapter 13; Leishmaniasis (ካላዛር/ጓቋ/ድባ/ እና ቁንጭር)

Laboratory Diagnosis

➢ Tissue biopsy is essential for identification of parasites, but the rate of


detection is poor unless PCR techniques are used.

Treatment of Mucosal Leishmaniasis

➢ The regimen of choice is a pentavalent antimonial agent administered at a


dose of 20 mg of SSG/kg for 30 days.
➢ Patients with ML require long-term follow-up with repeated oropharyngeal and
nasal examination.
➢ With failure of therapy or relapse, patients may receive another course of an
antimonial but then become unresponsive, presumably because of resistance in
the parasite.
▪ In this situation, AmB should be used. An AmB deoxycholate dose
totaling 25 - 45 mg/kg is appropriate.
▪ LAmB, 2 - 3 mg/kg for 20 days is considered adequate.
➢ Miltefosine (2.5 mg/kg for 28 days).
➢ The more extensive the disease, the worse the prognosis; thus prompt,
effective treatment and regular follow-up are essential.

Prevention and Control


➢ Vector Control
▪ Insecticide Application
▪ Use of Long-Lasting Insecticide Treated Nets (LLITN)
▪ Repellents (Chemical or Natural)
▪ Combination of several control methods
➢ Health Education and Social Mobilization through health
development army
➢ Information System → Integrated Disease Surveillance (IDS) is the major
strategy and mainstay of the Disease Surveillance in Ethiopia.

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Chapter 14; Leukaemia (የደም ካንሰር)

Chapter 14; Leukaemia (የደም ካንሰር)


Dr. Asmare.W, Dr. Mulualem. G

Clinical features and how to write hx of Leukaemia Patient

History

Clinical Diagnosis

➢ Acute leukemias present within a relatively short period of time. The


presentations are not specific.
➢ Some of the clinical presentations are the following:
▪ Anemia: due to bone marrow failure and/or bleeding
• Fatigue
• Shortness of breath on exertion
• Pallor
▪ Bleeding: Thrombocytopenia due to bone marrow failure
• Mucocutaneous bleeding: gum bleeding, epistaxis, cutaneous
bleeding, gastrointestinal bleeding and petechiae/purpura, excessive
menstrual bleeding
▪ Infections: Dysfunctional leucocytes and/or bone marrow failure
• Fever
• Focuses of infections: cellulitis, perianal abscess, gingival infection,
pneumonia, urinary tract infection
▪ Other hematologic findings
• Bone pain and sternal tenderness
• Lymphadenopathy
• Splenomegaly
• Hepatomegaly

Characterization of patient history


➢ Pt’s may present with
▪ Fever → chronic fever commonly more than 2 weeks
▪ Come for chemotherapy
➢ Fever
▪ Low grade
▪ Intermittent
▪ Worsen at night
▪ Associated with profuse sweating
➢ B symptoms → fever, sweating, weight loss
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Chapter 14; Leukaemia (የደም ካንሰር)

➢ Significant weight loss


▪ E.g. significant weight loss from 53 kg to 45 kg which is 15% of
his/her initial body weight or
▪ Unquantified but significant weight loss to the extent his/her closes
become loose (if s/he didn’t remember his/her initial body weight
but claim that S/he lose his/her body weight)
➢ Bone pain
▪ Intermittent
▪ Which bone → Over the thigh, below the knee, vertebral bone, ribs
e.t.c
➢ Joint pain
▪ Gradual in onset
▪ Intermittent
▪ Non migratory
▪ Aching type
▪ Aggravating and relieving factor
▪ Initially from “x” joint to “y” (e.g. initially ankle joint pain later
progress to involve knee joint bilaterally)
▪ To the extent the pain limits his/her daily activity
▪ Associated with swelling/ or not
➢ Bleeding → when and from where
▪ Gum bleeding
▪ Nasal bleeding → massive, recurrent, bilateral
▪ Bleeding from other sites
➢ Anaemia symptoms → Easy fatigability, light headedness, blurring of
vision, Light headedness, tinnitus, vertigo.
➢ LAP
▪ E.g. Swelling over the neck, latter under armpits, groin area
bilaterally
▪ Initially pea sized, which increase progressively to attain it’s current
size with in “x” weeks/months
▪ Discharge from the swelling or not
➢ Abdominal swelling → Organomegaly, it is not localized mass unlike
lymphoma
▪ Painless
▪ Over the right/ left upper quadrant
▪ Associated with early satiety and loss of appetite
➢ Vomiting and diarrhoea → characterize it
➢ Headache
▪ Gradual in onset
▪ Globalized
▪ Dull aching type
▪ Aggravating and relieving factors 793
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Chapter 14; Leukaemia (የደም ካንሰር)

➢ Dropping of his/her hair → alopecia


➢ Numbness or tingling sensation over the foot
➢ Leukemic meningitis features
▪ Headache
▪ Nausea and vomiting
▪ FND
▪ Seizure

Risk factors

➢ Environmental → herbicide or benzine exposure → from poisoning or


environmental exposure
➢ Ionizing radiation, chemical Toxins (Benzine in AML)
➢ Infection → HTLV_1, EBV → Mature B_cell ALL, Burkit lymphoma
➢ Immunodeficiency syndrome → ataxia telangiectasia
➢ Genetic
▪ Familial → twin concordance (identical twin = 20 %), Fanconi
anemia, Bloom SXX, ataxia telangiectasia
▪ Congenital or acquired chromosomal anomaly
➢ Age → young for ALL, old age for AML, CML/CLL
➢ Drugs
➢ Ankylating agents (chemo radio therapy)
➢ Epipodophyllotoxin

Complication of Leukaemia

➢ Tumour Lysis syndrome → commonly a feature of lymphoma


▪ Hyperkalaemia ( î k+)
▪ Hyperphosphatemia ( î PO43-)
▪ Hypocalcaemia (Ca2+ )
▪ Hyperuricemia ( î uric acid)
▪ AKI → end result of the above abnormalities
➢ Metastasis
➢ Bleeding
➢ Anaemia
➢ Malnutrition
➢ Immunosuppression
➢ Oncologic emergency → refer from Lymphoma (Click here → 15,2 Non
Hodkins lymphoma )
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Chapter 14; Leukaemia (የደም ካንሰር)

▪ Obstruction → Intestinal obstruction, Airway obstruction


▪ Paraplegia
▪ Tumour lysis syndrome
• SVC (Superior vana cava) syndrome
• Superior mediastinal sxx
➢ Death

Sample history one

C.C → Fever of 02 months duration


HPI
This patient was Last relatively healthy 02 months back at which time
she began to experience a low-grade intermittent fever with profuse
sweating but no chills or rigor. Associated with this she had a gradual
onset, intermittent, non-migratory, aching type of joint pain that was initially
at the right knee which later progressively involve the right ankle and left
knee joint within a week period of time. The joint pain was not associated
with any swelling but the extent of the pain limits her from doing her daily
activities. The pain worsened by activities but no relieving factor were
noticed by the patient. Together with this she also had intermittent bone
pain on both of her lower extremities below the knee.

A week later she began to experience easy fatigability at ordinary


activities like going to church, blurring of vision, palpitation but no tinnitus
or vertigo. At the same time, she started to develop painless swelling over
her groin bilaterally which was initially pea sized which grows progressively
to attain its current size within two weeks. Within few days after the
appearance of the first swelling similar painless swelling started to grow
around the same area of the groin, lateral part of the neck and axilla
bilaterally together with dragging sensation in the left upper abdomen,
sense of fullness and early satiety.

Beside to these complaints she has a loss of appetite and unquantified


but significant weight loss to the extent her cloths become loose. For these
complaints she visited a local health center 3 days before admission where
she was given unspecified PO medication to be taken 3 times per day for
10 days but no improvement. Later she was referred to our hospital for
better investigation and management.
➢ No hx of exposure to herbicides, pesticides, benzine or Radio
chemotherapy (RF)
➢ No hx of similar illness in the family (Genetics → RF) 795
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Chapter 14; Leukaemia (የደም ካንሰር)

➢ No hx of drug intake other than those mentioned above (chemo radio therapy →
RF)
➢ She was screened for RVI 5 months back and found to be NR
➢ She usually eats injera made of ‘‘teff’’ and ‘‘machilla’’ and ‘’wott’’ made
of ‘‘atter’’ and ‘‘dagusa’’ 3-4 times per day. Occasionally she eats meat
during holidays.
➢ No hx of gum bleeding, Nasal bleeding, or Bleeding from other sites
(CXN)
➢ No hx of abdominal pain or diarrhoea.
➢ No hx of cough, chest pain, dyspnoea or haemoptysis (Lung Metastasis → CXN)
➢ No hx of chronic cough, contact with chronic cougher or a known TB pt,
no hx of previous TB RX
➢ She is not from malaria/kalazar endemic area, no travel hx to endemic
area or previous attack (VL, HMS → DDX)
➢ No hx of photosensitivity, malar rash or joint pain (SLE → DDX)
➢ No self or family hx of HTN, DM or asthma

Finally, she was admitted to our hospital supported physically by her


families

Sample history two

C.C → Comes for chemotherapy


HPI
This is 55 years old male patient diagnosed to have hematologic
malignancy (CLL) 5 years back after he presented with… (List his smx
from the above). Dx was made after BM aspiration and CBC was done. He
was admitted for 3 weeks at UOG hospital oncology ward. After that he
was put on chemotherapy and have good adherence. After starting
chemotherapy, the swelling over the neck and axilla (i.e. LAP) began to
rapidly repress in 2 weeks and then no swelling at all. His symptoms (List
them) completely resolved and his appetite began to improve with
considerable weight gain

List +ve and -ve statements listed in the above case


➢ No hx of RUQ abdominal pain, yellowish discoloration of the eyes, urine
or stool colour change (hepatotoxicity of drugs)
➢ No hx of Flank pain, decreased UOP or hematuria (Nephrotoxicity of
drugs)
➢ Has hair loss but no numbness or tingling sensation
➢ No hx of body weakness

Finally, he was admitted to our hospital walking by him self


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Chapter 14; Leukaemia (የደም ካንሰር)

Physical examination (pertinent findings)

1 GA
➢ Acute sick looking
➢ Chronically sick looking
➢ Respiratory distress → Due to Severe anemia, Mediastinal LAP
compressing the Airway

2 Vital signs
3 HEENT
➢ Easily pluckable SCALP hair
➢ Conjunctival pallor, pale buccal mucosa → anemia
➢ Dry blood in nostrils, Gum bleeding, bleeding from the nose, mucosal
membrane hemorrhage → bleeding
➢ Periauricular swelling

4 LGS
➢ Multiple and significant LAP → Neck, axilla, groin
➢ Characterize LAP
▪ Size (“X” by “y” cm)
▪ Location
▪ Tenderness → non-tender
▪ Consistency → Firm, hard
▪ Rubbery
▪ Matted or discrete
▪ Attached to the underlying structure or overlying skin
▪ Mobile

5 RS
➢ Pleural effusion signs
➢ Consolidation → Pneumonia infection from immunosuppression

6 CVS
➢ ESM (ejection systolic murmur) over the erb’s point→ Anemia

7 Abdominal examination
➢ HSM (Hepatosplenomegaly)
➢ Ascites 797
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8 GUS
➢ Testicular mass in males

9 MSS
➢ Bone tenderness → usually over the Tibia, Femur, sternal tenderness
➢ Joint swelling or effusion
➢ Acute gouty arthritis → may also present at this time, due to overproduction of
uric acid.

10 IS
➢ Some/ severe palmar pallor → anemia
➢ Multiple purple to dark flat skin spots usually over the abdomen
➢ Ulceration
➢ Petechiae, purpura, echymosis

11 NS
➢ Meningeal irritation signs → leukemic meningitis

DDX for chronic fever

1) ALL/AML
2) CLL/CML
3) HL/NHL
4) Disseminated TB (to BM, Liver, spleen, LN)
5) VL
6) Aplastic anaemia
7) Sub-acute IE
8) Solid Tumour
▪ Rhabdomyosarcoma
▪ Neuroblastoma
▪ Retinoblastoma
▪ Ewing sarcoma
9) SLE
10) Brucellosis
11) IM (infectious mononucleosis)
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Chapter 14; Leukaemia (የደም ካንሰር)

IX

Diagnostic IX
1. CBC → WBC may be Low, high or normal in Leukaemia
▪ Pancytopenia
▪ Leucocytosis → WBC > 50,000/ml at dx is poor prognosis
▪ Marked leukocytosis or Pancytopenia indicate the possibility of
acute leukemia. However, the leukocyte count can rarely be
normal.
2. PM (Peripheral morphology) → Blasts (> 5% in ALL)
3. BM aspiration and Biopsy
▪ BM replaced by leukemic lymphoblast
▪ ALL diagnosed when > 25 % of BM cell is Lymphoblast
4. LN biopsy, FNAC (Cytology)
▪ Peripheral smear
▪ RBC morphology
▪ WBC
▪ Platelet
5. Splenic aspiration → VL, Malignant infiltration

Baseline IX
6. BG and Rh, cross match → If HgB < 8, Transfuse
7. OFT → RFT, LFT → before starting chemotherapy
8. Liver enzymes → AST (SGOT), ALT (SGPT) → before starting
chemotherapy
9. CXR
▪ Mediastinal mass
▪ Hilar LAP
▪ Disseminated TB (primary focus from Lung)
▪ Pneumonia super infection
10. Abdominal U/S
▪ Intraabdominal LAP
▪ Hepatic/splenic infiltration


Ascites
Oncologic emergency like obstruction 799
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11. PICT
12. Viral markers → HBsAg, HCVab
13. BF → For every febrile patient to r/o malaria
14. AFB → disseminated TB is DDX

Other IX based on indication


15. Serum electrolyte → Tumor lysis SXX
16. ECHO and ECG
17. LP → Leukemic meningitis, before Rx (Chemotherapy)
18. Coagulation profile
19. X-ray of extremities
▪ Pathologic #
▪ Focal lytic lesions
▪ Periosteal new bone lesions
20. LDH Level → to asses tumour burden
21. Serum Uric acid level → to asses tumour burden
22. ANA → SLE
23. Blood culture → Subacute IE
24. Infectious agent Serology → Not available in Ethiopia
▪ CMV
▪ EBV

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Chapter 14; Leukaemia (የደም ካንሰር)

Discussion

Table; Differentiation features of leukemia


Differe Leukemia
ntiation AML ALL CLL CML
feature
s
Age The most common most common in CLL is the most 15 to 20 % of leukemias
group acute leukemia in childhood, with a common leukemia in adults. The median
adults. The median peak incidence at in adults in age at presentation is
age at diagnosis is 67 2 - 5 years Western countries approximately 50 years
years
mainly a disease
of older adults,
with a median
age at diagnosis
of approximately
70 years
IX ➢ Myeloblasts on ➢ Lymphoblasts Absolute ➢ Philadelphia (Ph)
peripheral smear. on peripheral lymphocytosis (> chromosome
Auer rods, which 5000/ μL or 5 x ➢ Blast cells constitute
smear.
are pathognomonic 109/L ) majority of cell lines
of myeloblasts in ➢ Bone marrow ➢ suspected in
PM. contains more patients with
➢ Bone marrow than 25 % Leucocytosis, usually
contains more than lymphoblasts exceeding 30,000/µl,
20 % Myeloblasts
with elevated
granulocyte counts
(neutrophils,
basophils or
eosinophils).

First cancers for Treatment of CML with


Chemo which an effective targeted tyrosine kinase
therapy chemotherapeutic inhibitors is highly
respon treatment was effective, safe and
se developed.
available in Ethiopia.

Progno Poor Good Good


sis

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Leukemia
➢ Leukemia is a clonal, neoplastic disorder characterized by proliferation and
accumulation of immature and malignantly transformed cells in the bone
marrow and peripheral blood.
➢ Clinically and pathologically, leukemia is subdivided into a variety of large
groups. The first division is between its acute and chronic forms:

Acute leukemia
➢ Is characterized by a rapid increase in the number of immature blood cells.
➢ The crowding that results from such cells makes the bone marrow unable to
produce healthy blood cells.
➢ Immediate treatment is required in acute leukemia because of the rapid
progression and accumulation of the malignant cells, which then spill over into
the bloodstream and spread to other organs of the body.
➢ Acute forms of leukemia are the most common forms of leukemia in children.

Chronic leukemia

➢ Is characterized by the excessive build-up of relatively mature, but still


abnormal, white blood cells.
➢ Typically taking months or years to progress, the cells are produced at a much
higher rate than normal, resulting in many abnormal white blood cells.
➢ Whereas acute leukemia must be treated immediately, chronic forms are
sometimes monitored for some time before treatment to ensure maximum
effectiveness of therapy.
➢ Chronic leukemia mostly occurs in older people, but can occur in any age
group.
➢ Additionally, the diseases are subdivided according to which kind of blood cell
is affected. This divides leukemia into lymphoblastic or lymphocytic leukemia
and myeloid or myelogenous leukemia
▪ Acute myelogenous leukemia (AML)
▪ Acute lymphoblastic leukemia (ALL)
▪ Chronic myelogenous leukemia (CML)
▪ Chronic lymphocytic leukemia (CLL)

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14.1 Acute Leukaemia

14.1.1 Acute myelogenous leukemia (AML)


➢ It is a neoplastic disease characterized by infiltration of the blood, bone
marrow, and other tissues by proliferative, clonal undifferentiated cells of the
hematopoietic system.
➢ This leukemia comprises a spectrum of malignancies that, untreated, range
from rapidly fatal to slowly growing.
➢ AML incidence increases with age; it is 1.7 in individuals age <65 years and
15.9 in those age >65 years. The median age at diagnosis is 67 years

EPIDEMIOLOGY

➢ AML is the most common acute leukemia in adults and accounts for
approximately 80 % of cases in this group. In contrast, AML accounts for < 10
% of acute leukemias in children < 10 years of age.
➢ In adults, the median age at diagnosis is approximately 65 years.
➢ The incidence increases with age with approximately 2 and 20 cases per
100,000 population for those under or over 65 years, respectively.
➢ The male : female ratio is approximately 5:3.
➢ This incidence is similar among persons of different races.

ETIOLOGY;

➢ Those have been implicated in the development of AML include.


▪ Heredity
▪ Radiation
▪ Chemical and other occupational exposures
▪ Drugs
➢ No direct evidence suggests a viral etiology.

CLASSIFICATION
➢ Following diagnosis, AML is classified using the WHO classification system
based upon a combination of morphology, immunophenotype, genetics, and
clinical features.
➢ The classification attempts to identify biologic entities in the hopes that future
work will elucidate molecular pathways that might be amenable to targeted
therapies.
➢ There are six main groups of AML recognized in this classification system
▪ AML with recurrent genetic abnormalities
▪ AML with myelodysplasia-related features
▪ Therapy-related AML and MD
▪ AML, not otherwise specified
▪ Myeloid sarcoma
▪ Myeloid proliferations related to Down syndrome 803
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➢ The French-American-British (FAB) classification system divides AML into 8


subtypes, M0 through to M7, based on the type of cell from which the
leukemia developed and its degree of maturity.
▪ AML with minimal differentiation (M0) – 6 % of AML, NOS (<5 % of
total AML)
▪ AML without maturation (M1) – 25 % of AML, NOS (5 to 10 % of total
AML)
▪ AML with maturation (M2) – 28 % of AML, NOS (10 to 14 % of total
AML)
▪ Acute myelomonocytic leukemia (M4) – 21 % of AML, NOS (5 to 10 %
of total AML)
▪ Acute monoblastic and monocytic leukemia (M5) – 15 % of AML, NOS
(5 to 10 % of total AML)
▪ Pure erythroid leukemia (M6) – 4 % of AML, NOS (<5 % of total AML)
▪ Acute megakaryoblastic leukemia (M7) – 1 % of AML, NOS (<1 % of
total AML

CLINICAL PRESENTATION

➢ Patients with AML most often present with nonspecific symptoms that
begin gradually or abruptly and are the consequence of anemia,
leukocytosis, leukopenia or leukocyte dysfunction, or thrombocytopenia.
➢ Nearly half have had symptoms for ≤ 3 months before the leukemia
was diagnosed.
➢ Half of patients mention fatigue as the first symptom, but most complain
of fatigue or weakness at the time of diagnosis.
➢ Anorexia and weight loss are common.
➢ Fever with or without an identifiable infection is the initial symptom in
approximately 10% of patients.
➢ Signs of abnormal hemostasis (bleeding, easy bruising) are noted first in
5% of patients.
➢ On occasion, bone pain, lymphadenopathy, nonspecific cough, headache,
or diaphoresis is the presenting symptom
➢ Rarely patients may present with symptoms from a myeloid sarcoma
that is a tumor mass consisting of myeloid blasts occurring at anatomic
sites other than bone marrow. Sites involved are most commonly the
skin, lymph node, gastrointestinal tract, soft tissue, and testis.
➢ General fatigue is present in the majority of patients and often precedes
the diagnosis for a number of months.
➢ Pallor and weakness are common and attributed to the anemia.
➢ Bone pain is infrequent in adults with AML, although some individuals
describe sternal discomfort or tenderness, occasionally with aching in the
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long bones. This may be especially severe in the lower extremities, due
to expansion of the medullary cavity by the leukemic process.

Diagnosis
PATHOLOGIC FEATURES;

➢ Peripheral blood
▪ Analysis of the peripheral blood at presentation usually reveals a
normocytic, normochromic anemia that can vary in severity.
▪ The reticulocyte count is normal or decreased.
▪ Approximately 75 % of patients have platelet counts below
100,000 cells/µL (100 x 109/L) at diagnosis, and approximately 25 % will
have counts below 25,000 cells/µL.
▪ Both morphologic and functional platelet abnormalities may be seen.
▪ The median leukocyte count at diagnosis is approximately
15,000 cells/µL; 20 % of patients have a leukocyte count above
100,000 cells/µL and 25 to 40 % of patients have a leukocyte count less
than 5000 cells/µL.
▪ The vast majority of patients (95 %) will have circulating myeloblasts that
can be detected on the peripheral smear.
▪ There may or may not be evidence of myelodysplasia.

Myeloblasts
➢ They are immature cells with large nuclei, usually with prominent nucleoli, and
a variable amount of pale blue cytoplasm (sometimes with faint granulation)
after staining with Wright Giemsa.
➢ The nuclear to cytoplasmic ratio and morphology vary depending upon the
maturity of the cell.
➢ Auer rods, which are pathognomonic of myeloblasts, vary in frequency
depending upon the AML subtype.
➢ They can be identified as pink/red rod-like granular structures in the cytoplasm.
➢ Sometimes the Auer rods are multiple, and sometimes they form a dense
clump and are referred to as "Auer bodies."

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FIGURE 104-1 (Harrison 21st edition) Morphology of acute myeloid leukemia (AML) cells.
A. Uniform population of primitive myeloblasts with immature chromatin, nucleoli in some
cells, and primary cytoplasmic granules. B. Leukemic myeloblast containing an Auer rod.
C. Promyelocytic leukemia cells with prominent cytoplasmic primary granules. D.
Peroxidase stain shows dark blue color characteristic of peroxidase in granules in AML.

A myeloperoxidase reaction
➢ It is easy to perform, can be done in less than a few minutes, and is a simple
means of determining if the blasts are myeloid.
➢ Absence of a reaction product does not rule out AML, as some cases are
negative.
➢ Evaluation of myeloperoxidase reactivity must be focused on the blast
population and not on mature or maturing myeloid elements on the smear.

Flow cytometry
➢ Flow cytometry of the peripheral blood or marrow aspirate can identify
circulating myeloblasts in the majority of patients by characteristic patterns of
surface antigen expression.
➢ The specific pattern differs among the AML subtypes, but the majority of cases
express CD34, HLA-DR, CD117, CD13, and CD33. 806
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➢ Myeloblasts may express T or B cell antigens, most commonly in


cytogenetically defined subtypes of AML (eg, CD19 expression in AML
with RUNX1-RUNX1T1, CD2 expression in APL) and in acute leukemias of
ambiguous lineage (mixed phenotype acute leukemia [MPAL]).
➢ Care must be taken in interpreting the antigen profile, and in distinguishing
AML from ALL or MPAL.
➢ In general, the panel of antigens analyzed must contain multiple myeloid, B
and T cell markers; the presence of a single B or T cell marker (eg, CD19 or
CD7) is insufficient for diagnosing MPAL.

Bone marrow biopsy and aspirate

Blast count
➢ Bone marrow aspiration and biopsy (usually unilateral) is a key component to
the diagnosis of AML.
➢ The bone marrow is usually hypercellular due to a partial or almost total
replacement of the normal cellular components of the marrow by immature or
undifferentiated cells, although AML can sometimes present with a hypocellular
marrow
➢ The bone marrow biopsy gives a general overview of the degree of
involvement and specific histologic features associated with the process (eg,
fibrosis, necrosis).
➢ The aspirate provides material for a 500-cell differential count to determine the
percentage of blasts in the marrow; it also provides for detailed cytologic
evaluation of the blasts and other cells that may be residual normal
hematopoietic elements or abnormal cells maturing from the blasts.
➢ The differential count from the aspirate is critical because the blast percentage
from the flow specimen may be influenced by hemodilution and artifacts
produced by the variability by which the specimen is prepared (eg, red cell
lysis techniques, density gradient centrifugation) and the approach through
which different cell populations are selected for gating.

Cell origin
➢ The blasts in AML must be identified as cells of the myeloid, monocytic,
erythroid, or megakaryocytic lineage and are distinguished from blasts of the
lymphoid lineage seen in acute lymphoblastic leukemia.
➢ The non-lymphoid lineage of the AML blasts can be identified by any of the
following:
▪ The presence of an Auer rod on microscopy.
▪ Cytochemical studies demonstrating positivity for Sudan black B,
myeloperoxidase, chloroacetate esterase, or nonspecific esterase.

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▪ Flow cytometry identifying the expression of myeloid antigens. It is


notable that up to 20 % of AML will demonstrate co-expression of
lymphoid markers (eg, CD7, CD19, CD2).
▪ The outcome after treatment with AML directed therapy is not affected by
the co-expression of "lymphoid" antigens.
▪ "True" mixed phenotype acute leukemia (MPAL) is very uncommon and
the diagnosis requires co-expression of unambiguous myeloid markers
and the presence of lymphoid markers for B lineage.
▪ Specific cytogenetic abnormalities that are seen only in myeloid
leukemias (eg, t(1;22)(p13;q13).

Cytogenetic features
➢ All patients with suspected AML should undergo metaphase cytogenetic
analysis of their bone marrow biopsy specimen.
➢ Approximately 50 % of patients with newly diagnosed AML will demonstrate
cytogenetic abnormalities.
➢ A combination of conventional karyotypic analysis plus reverse transcriptase
polymerase chain reaction (RT-PCR) or fluorescent in situ hybridization (FISH)
for specific abnormalities can aid in the diagnosis, treatment, and post-
treatment monitoring of patients with AML:

Molecular studies
➢ Abnormalities in certain genes, such as mutations in FLT3, nucleophosmin
(NPM1), KIT, CEBPA, or RUNX1 as well as gene expression profiles confer
prognostic significance in adult patients with AML.
➢ The diagnosis of AML requires both of the following:
▪ Documentation of bone marrow infiltration – Blast forms must account
for at least 20 % of the total cells of the bone marrow aspirate (from a
500-cell differential count).
▪ Whether or not a blast percentage can be determined in the bone
marrow, the presence of > 20 % blasts in the peripheral blood is also
diagnostic of AML. Exceptions to this include leukemias with certain
genetic abnormalities, such as those with t(8;21), inv(16), or t(15;17), and
myeloid sarcoma, which are considered diagnostic of AML without regard
to the blast count.
▪ The leukemic cells must be of myeloid origin as demonstrated by either
the presence of Auer rods, cytochemical positivity for myeloperoxidase, or
presence of sufficient myeloid/monocytic markers recognized by
immunophenotyping.

M3 morphology (acute promyelocytic leukemia)

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➢ Acute promyelocytic leukemia (APML, APL) is the M3 subtype of AML, a


cancer of the white blood cells.
➢ In APL, there is an abnormal accumulation of immature granulocytes called
promyelocytes.
➢ The disease is characterized by a chromosomal translocation involving the
retinoic acid receptor alpha (RARα or RARA) gene and is distinguished from
other forms of AML by its responsiveness to all-trans retinoic acid (ATRA; also
known as tretinoin) therapy
➢ APL is characterized by the presence of atypical promyelocytes in the
peripheral blood and bone marrow. These cells are typically large with a
creased, folded, or bilobed nucleus and cytoplasm filled with bright pink,
reddish-blue or dark purple granules.
➢ APL represents a medical emergency with a high rate of early mortality, often
due to hemorrhage from a characteristic coagulopathy.
➢ It is critical to start treatment with a differentiation agent (eg, all-trans retinoic
acid) without delay as soon as the diagnosis is suspected based upon
cytologic criteria, and even before definitive cytogenetic or molecular
confirmation of the diagnosis has been made.
➢ Depending on geographic variations, APL accounts for 5 to 20 % of cases of
AML.
➢ Patients with AML in general, and APL in particular, typically present with
symptoms related to complications of pancytopenia (ie, anemia, neutropenia,
and thrombocytopenia), including weakness and easy fatigability, infections of
variable severity, and/or hemorrhagic findings such as gingival bleeding,
ecchymoses, epistaxis, or menorrhagia. Combinations of these symptoms are
common.
➢ Unique to APL is a presentation with bleeding secondary to DIC
➢ Coagulopathy associated with APL is complex and involves both DIC and
primary hyper fibrinolysis and is either present at diagnosis or occurs soon
after the initiation of cytotoxic chemotherapy. This complication constitutes a
medical emergency, because, if left untreated, it can cause pulmonary or
cerebrovascular hemorrhage in up to 40 % of patients and a 10 to 20 %
incidence of early hemorrhagic death.
➢ Adverse risk factors were a total WBC count > 10,000/µL and a platelet count
≤ 40,000/µL. Using these two parameters, three prognostic categories could be
distinguished, with the following estimated probabilities of 3 -year relapse-free
survival (RFS):
▪ Low risk – WBC ≤10,000/µL and platelets >40,000/µL; RFS 98 %
▪ Intermediate – WBC ≤10,000/µL and platelets ≤40,000/µL; RFS 89 %
▪ High risk – WBC >10,000/µL; RFS 70 %
➢ APL is unique among leukemias due to its sensitivity to all-trans retinoic acid
(ATRA; tretinoin), the acid form of vitamin A Unlike other chemotherapies,
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➢ ATRA induces the terminal differentiation of the leukemic promyelocytes, after


which these differentiated malignant cells undergo spontaneous apoptosis on
their own.
➢ ATRA alone is capable of inducing remission but it is short-lived in the
absence of concurrent "traditional" chemotherapy.

14.1.2 Acute lymphoblastic leukemia (ALL)


➢ ALL, is an acute form of leukemia characterized by the overproduction and
accumulation of cancerous, immature white blood cells, known as lymphoblasts.
➢ In persons with ALL, lymphoblasts are overproduced in the bone marrow and
continuously multiply, causing damage and death by inhibiting the production of
normal cells (such as RBC, WBC and platelets) in the bone marrow and by
spreading (infiltrating) to other organs.
➢ ALL is most common in childhood, with a peak incidence at 2–5 years of age
and another peak in old age.
➢ ALL was one of the first cancers for which an effective chemotherapeutic
treatment was developed.
➢ ALL is associated with exposure to radiation and chemicals in animals and
humans.
➢ High level radiation exposure is a known risk factor for developing leukemia,
as found by studies of survivors of atom bomb exposure in Hiroshima and
Nagasaki.
➢ In animals, exposure to benzene and other chemicals can cause leukemia

EARLY SIGNS AND SYMPTOMS

➢ The most common presenting symptoms of ALL are nonspecific and may be
difficult to distinguish from common, self-limited diseases of childhood.
➢ In a meta-analysis, more than half of children with childhood leukemia had at
least one of the following 5 features on presentation:
▪ Palpable liver
▪ Palpable spleen
▪ Pallor
▪ Fever, or
▪ bruising.
➢ Hepatosplenomegaly — Hepatomegaly (64 % ) and/or splenomegaly (61% ) are
the most common clinical findings in association with childhood leukemia.
These abnormalities may also manifest as symptoms of anorexia, weight loss,
abdominal distension or abdominal pain, or an abdominal mass noted by a
family member or clinician.
➢ Lymphadenopathy — nearly half of children with ALL present with
lymphadenopathy, which is one of the indications of extramedullary leukemic
spread. As a general rule, a lymph node is considered enlarged if it is >10
mm in its greatest diameter. Exceptions to this rule include the following:
▪ Epitrochlear nodes are enlarged if they are >5 mm.
▪ Inguinal nodes are enlarged if they are >15 mm in greatest diameter.
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▪ Cervical nodes are enlarged if they are >20 mm.


➢ Lymphadenopathy associated with malignancy usually is non-tender, firm,
rubbery, and matted. Persistent or progressive lymphadenopathy that does not
respond to antibiotic therapy suggests the need for more extensive evaluation.
➢ Musculoskeletal pain — although bone pain occurs commonly among
children, particularly adolescents, it may be a symptom of ALL. Early
bone marrow examination should be considered in any child who has
persistent bone pain and peripheral blood abnormalities.

DIAGNOSTIC EVALUATION

➢ Peripheral blood abnormalities


▪ Most children with ALL have anemia and/or thrombocytopenia with
either normal or slightly increased WBC counts, and lymphoblasts
on peripheral smear.
▪ These findings suggest the need for bone marrow examination,
which should be performed for the following indications:
• Atypical cells in the peripheral blood
• Unexplained depression of more than one peripheral blood
element (cytopenias). Cytopenias are defined as an absolute
neutrophil count (ANC) of <500/µL, Hgb <8 g/dL, or a platelet
count <150,000/µL.
• Unexplained lymphadenopathy or hepatosplenomegaly
associated with cytopenias.
➢ Morphology
▪ In the WHO classification system for hematologic malignancies, the
lymphoblastic neoplasms (which may present as
leukemia and/or lymphoma) are divided into two general categories
based upon lineage
o Precursor B cell lymphoblastic leukemia/lymphoma, also
called precursor B cell acute lymphoblastic leukemia
(precursor B cell ALL)
o Precursor T cell
lymphoblastic leukemia/lymphoma (precursor T-LBL), also
called precursor T cell acute lymphoblastic leukemia (T
cell ALL)
▪ These two entities are morphologically indistinguishable.
▪ On peripheral blood smears and bone marrow aspirates, lymphoblasts
vary from small cells with scant cytoplasm, condensed nuclear chromatin,
and indistinct nucleoli to larger cells with moderate amounts of
cytoplasm, dispersed chromatin, and multiple nucleoli.
▪ The former FAB L3 category is currently described as
Burkitt lymphoma/leukemia in the WHO classification.
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➢ Immunophenotype
▪ leukemia cells in ALL are classified according to immunophenotype using
an extensive panel of monoclonal antibodies to cell surface "cluster of
differentiation" (CD) markers.
▪ Markers used to classify cells by lineage are the same as those used in
adult ALL.
▪ Approximately 70 to 80 % of cases of childhood ALL are of B-precursor
lineage (i.e, precursor B cell leukemia or early pre-B cell ALL).
▪ B-precursor leukemia typically is CD10+, CD19+, and sometimes CD20+.
▪ Leukemic lymphoblasts with the L3 morphology usually have markers for
mature B cell ALL (CDs 10 ± 19, 20, 22, 25, and surface
immunoglobulin).
▪ Cases of T cell ALL (i.e, precursor T lymphoblastic leukemia), which
comprise 15 to 17 percent of all cases of ALL, are positive for CD2, 3,
4, 5, 7, and 8.
➢ Cytogenetics
▪ Chromosomal abnormalities are common in childhood ALL.
▪ Although not specifically used for diagnosis, cytogenetic findings are an
essential part of the risk group stratification of childhood ALL and help to
guide therapy.
▪ Cytogenetics must be considered in the context of other risk factors and
response to the first month of chemotherapy.
▪ The diagnosis of CNS leukemia requires one of the following:
• Cytologic confirmation of the presence of leukemic cells in the CSF
• Clinical signs of CNS leukemia such as facial nerve
palsy, brain/eye involvement, or hypothalamic syndrome
• A tumor mass involving the CNS as determined by imaging studies
▪ ALL can present clinically as either a mass lesion or as leukemia.
▪ Although the distinction in some patients is arbitrary, ALL is the preferred
term in the US when the bone marrow contains more than 25 %
lymphoblasts, whereas lymphoma is the preferred term when the process
is confined to a mass lesion with minimal or no blood and bone marrow
involvement.
▪ CNS involvement is often categorized into three groups:
• CNS1 – no blasts in the CSF
• CNS2 – <5 blasts in the CSF with or without RBC
• CNS3 – >5 blasts in CSF

TREATMENT

➢ Transfusion: Packed RBC transfusion of severe anemia, platelet


transfusion or severe thrombocytopenia
➢ Treatment of infection/neutropenic fever
➢ Chemotherapy is the initial treatment of choice. Most ALL patients will receive
a combination of medications. There are no surgical options because of the
body-wide distribution of the malignant cells.
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➢ In general, cytotoxic chemotherapy for ALL combines multiple antileukemic


drugs in various combinations. Chemotherapy for ALL consists of three phases:
▪ Remission induction
▪ Intensification and
▪ Maintenance therapy.

Phase Description Agents


Remission ➢ The aim of remission induction is to ➢ Combination of prednisolone or
induction rapidly kill most tumor cells and get the dexamethasone, vincristine,
patient into remission. asparaginase (better tolerance in
➢ This is defined as the presence of less pediatric patients), and daunorubicin
than 5% leukemic blasts in the bone (used in Adult ALL) is used to induce
marrow, normal blood cells and absence remission.
of tumor cells from blood, and absence ➢ CNS prophylaxis can be achieved via
of other signs and symptoms of the irradiation, cytarabine + methotrexate,
disease. or liposomal cytarabine.
➢ CNS prophylaxis should begin during ➢ In Philadelphia chromosome-positive
this phase of treatment and continue ALL, the intensity of initial induction
during the consolidation/intensification treatment may be less than has been
period. traditionally given.
➢ The rationale is based on the presence
of CNS involvement in 10%-40% of
adult patients at diagnosis.
Consolidati ➢ Intensification uses high doses of ➢ Typical intensification protocols use
on/intensifi intravenous multidrug chemotherapy to vincristine, cyclophosphamide,
cation further reduce tumor burden. cytarabine, daunorubicin, etoposide,
➢ Since ALL cells sometimes penetrate thioguanine or mercaptopurine given
the CNS, most protocols include as blocks in different combinations.
delivery of chemotherapy into the CNS ➢ For CNS protection, intrathecal
fluid (termed intrathecal chemotherapy). methotrexate or cytarabine is usually
➢ Some centers deliver the drug through used combined with or without cranio-
Ommaya reservoir (a device surgically spinal irradiation (the use of radiation
placed under the scalp and used to therapy to the head and spine).
deliver drugs to the CNS fluid and to ➢ CNS relapse is treated with intrathecal
extract CNS fluid for various tests). administration of hydrocortisone,
Other centers would perform multiple LP methotrexate, and cytarabine.
as needed for testing and treatment
delivery (In Ethiopia intrathecal
chemotherapy is through LP).
Maintenan ➢ The aim of maintenance therapy is to ➢ For this purpose, daily oral
ce therapy kill any residual cell that was not killed mercaptopurine, once weekly oral
by remission induction and methotrexate, once monthly 5-day
intensification regimens. course of intravenous vincristine and
➢ Although such cells are few, they will oral corticosteroids are usually used.
cause relapse if not eradicated. ➢ The length of maintenance therapy is
3 years for boys, 2 years for girls and
adults

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14.2 Chronic Leukaemia

14.2.1 Chronic Lymphatic Leukemia (CLL)

➢ CLL is characterized by the progressive accumulation of usually monoclonal,


functionally incompetent lymphocytes, mature appearing lymphoid cells.
➢ Patients with CLL commonly develop complications associated with the intrinsic
immune dysfunction that results in immunodeficiency and the development of
autoimmune disorders
➢ Small lymphocytic lymphoma (SLL) is a similar disease with predominate lymph
node enlargement.
➢ CLL and small lymphocytic lymphoma (SLL) are considered part of a spectrum
of the same disease. Both are characterized by clonal proliferation of mature
B-lymphocytes.
➢ In SLL, there is more lymph node involvement and less bone marrow and
peripheral blood involvement; in CLL, the bone marrow and the peripheral
blood are more affected.
➢ The clinical presentation of CLL or SLL relate to tissue infiltration
(lymphadenopathy, organomegaly), peripheral blood cytopenia (anemia,
bleeding, infections), or immune suppression (infections and
malignancies) and autoimmune phenomenon (hemolytic anemia).

EPIDEMIOLOGY

➢ CLL is the most common leukemia in adults in Western countries, accounting


for approximately 25 to 30 % of all leukemias in the United States.
➢ The disorder is more common in men, with a male to female ratio of
approximately 1.3:1 to 1.7:1.
➢ CLL is considered to be mainly a disease of older adults, with a median age
at diagnosis of approximately 70 years; however, it is not unusual to make this
diagnosis in younger individuals from 30 to 39 years of age.
➢ Genetic rather than environmental factors are the most likely explanation for
these differences.

CLINICAL PRESENTATION
➢ The clinical presentation of CLL or SLL relate to;
▪ Tissue infiltration (lymphadenopathy, organomegaly)
▪ Peripheral blood cytopenia (anemia, bleeding, infections), or
▪ Immune suppression (infections and malignancies) and
▪ Autoimmune phenomenon (hemolytic anemia).
➢ Most patients feel entirely well with no symptoms when a routine blood count
reveals an absolute lymphocytosis, leading to a diagnosis of CLL.
➢ 5 to 10 % of patients present with the typical "B" symptoms of lymphoma
which include one or more of the following:
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Chapter 14; Leukaemia (የደም ካንሰር)

▪ Unintentional weight loss ≥10 % of body weight within the previous six
months.
▪ Fevers of >100.5°F (>38°C) for ≥2 weeks without evidence of infection.
▪ Drenching night sweats without evidence of infection.
➢ Extreme fatigue (ie, ECOG Performance status 2 or worse; cannot work or
unable to perform usual activities)
➢ Recurrent infections (pneumonia, UTI) caused by usual bacterial
pathogens.
➢ Symptoms of anemia: fatigue, exertional shortness of breath
➢ Symptoms related to enlarged lymph nodes, splenomegaly or
hepatomegaly

Signs
➢ Lymphadenopathy
▪ The most common abnormal finding on physical examination of the
patient with CLL is lymphadenopathy, present in 50 to 90 % of patients
among various series.
▪ Lymph node enlargement may be generalized or localized, and individual
lymph nodes can vary greatly in size.
▪ The most commonly affected sites are cervical, supraclavicular, and
axillary.
▪ Characteristically, enlarged nodes in CLL are firm, rounded, discrete,
nontender, and freely mobile upon palpation. Exceptions to these
generalizations are encountered, particularly when the nodes have grown
rapidly.
▪ Occasionally, several enlarged nodes in the same anatomical site (eg,
cervical triangle, axilla or femoral-inguinal areas) may become confluent,
forming large spherical lymphoid masses.
▪ In addition, new lymph nodes may appear in places other than the usual
lymph node-bearing sites, such as over the sacrum or the thorax.
➢ Splenomegaly
▪ The spleen is the second most frequently enlarged lymphoid organ,
being palpably enlarged in 25 to 55 % of cases.
▪ As is the case with enlarged lymph nodes, an enlarged spleen in CLL is
usually painless and nontender to palpation, with a sharp edge and a
smooth firm surface. Painful and infarcted splenic enlargement is an
unusual presenting feature.
➢ Hepatomegaly
▪ Enlargement of the liver may be noted at the time of initial diagnosis in
15 to 25 % of cases.
▪ The liver is usually only mildly enlarged, ranging from 2 to 6 cm below
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▪ Upon palpation, the liver is usually nontender and firm with a smooth
surface.
➢ Skin
▪ Infiltration with CLL cells may occur in any organ, but, at the time of
diagnosis, the skin (leukemia cutis) is the most commonly involved non-
lymphoid organ.
▪ These lesions most commonly involve the face and can manifest as
macules, papules, plaques, nodules, ulcers, or blisters. Diagnosis is made
based upon biopsy of the involved skin.

DIAGNOSIS

➢ The diagnosis of CLL should be strongly considered in patients with absolute


lymphocyte count above 5000/ μL. However, confirmation requires review of
peripheral blood smear morphology by hematologist or pathologist
➢ Definitive diagnosis of CLL requires the presence of the following three
parameters.
▪ Absolute lymphocytosis defined as lymphocyte count more than 5000
cells/μl.
▪ Confirming the presence of excess mature appearing lymphocytes on the
peripheral blood smear.
▪ Immunophenotyping (Flow cytometry) from peripheral blood: to confirm
the presence B-cell markers on the neoplastic lymphoid cells and their
clonality.

LABORATORY ABNORMALITIES.
➢ Lymphocytosis
▪ The most noteworthy laboratory abnormality found in CLL is
lymphocytosis in the peripheral blood and bone marrow.
▪ Although the absolute blood lymphocyte threshold for diagnosing CLL has
been placed at >5000/µL [5 x 109/L] B lymphocytes, a significant
proportion of patients present with counts as high as 100,000/microL [100
x 109/L].
➢ Cytopenias
▪ Pancytopenia may be observed at the time of initial diagnosis, and are
usually not severe.
▪ These can be related to autoimmune hemolytic anemia, pure red cell
aplasia, autoimmune thrombocytopenia, or agranulocytosis
▪ Patients with CLL have an increased incidence of autoimmune hemolytic
anemia (AIHA). The direct antiglobulin (Coombs) test (DAT) may be
positive at some time during the course of the disease in up to 35 % of
cases; overt AIHA occurs in 11 % of cases.
➢ Other abnormal findings — There are no characteristic abnormalities in blood
chemistry, but elevated levels of serum LDH and beta-2 microglobulin were
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Chapter 14; Leukaemia (የደም ካንሰር)

advanced CLL entering a therapeutic trial. Elevations of uric acid, hepatic


enzymes (ALT or AST) and, rarely, calcium may also be observed.

PATHOLOGIC FEATURES

➢ Morphology
▪ The peripheral blood smear of patients with CLL demonstrates a
lymphocytosis.
▪ The leukemic cells are typically small, mature appearing lymphocytes with
a dense nucleus, partially aggregated (clumped) chromatin, and without
discernible nucleoli.
▪ There is a narrow border of clear to slightly basophilic cytoplasm.
➢ Immunophenotype
▪ Immunophenotypic analysis, usually by flow cytometry, is a key
component to the diagnosis of CLL.
▪ There are three major characteristic immunophenotypic findings:
• Expression of B cell associated antigens including CD19, CD20,
and CD23.
• Expression of CD5, an antigen commonly expressed by T cells.
• Low levels of surface membrane immunoglobulin (ie, SmIg weak).
The immunoglobulin is most often IgM or both IgM and IgD, and
only a single immunoglobulin light chain is expressed (ie, either
kappa or lambda but not both), confirming the clonal nature of
these cells. In rare cases, several Ig clones may coexist.
➢ Bone marrow aspirate and biopsy
▪ Bone marrow aspirate and biopsy are not required for the diagnosis of
CLL.
▪ If bone marrow biopsy and aspiration are performed at the time of initial
diagnosis, they usually demonstrate normal to increased cellularity, with
lymphocytes accounting for >30 % of all nucleated cells.
➢ Lymph node biopsy
▪ CLL and SLL are considered to be the same disease with different
clinically manifestations.
▪ Historically, the diagnosis of SLL was made via a lymph node biopsy in
a patient presenting with lymphadenopathy but without peripheral
lymphocytosis, while CLL was diagnosed through examination of the
peripheral blood and bone marrow in patients with lymphocytosis.
▪ Currently, the diagnosis of SLL is reserved for patients demonstrating
lymph node pathology consistent with CLL/SLL but with an absolute
peripheral clonal lymphocyte count that does not exceed 5000/µL [5 x
109/L] and no evidence of neutropenia, anemia, or thrombocytopenia
related to the disease.

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Table. Staging of CLL


Staging
Rai stage Risk Features Overall survival
in years
0 Low Lymphocytosis in the peripheral >10
blood and bone marrow only
I/II Intermediate Lymphadenopathy +/- 7
hepatosplenomegaly
III/IV High Anemia +/- thrombocytopenia <4

Binet
stage
A Low < 3 areas of lymphadenopathy 12
B Intermediate >3 areas of lymphadenopathy 7
C High Anemia, thrombocytopenia or 2 – 4
both

Treatment options
Treatment should be decided and provided by a hematologist.
1. Wait and watch with no treatment: for asymptomatic patients
2. Combination chemotherapy
3. Targeted therapies
4. Monoclonal antibody therapies

Indications for treatment


➢ Symptomatic disease:
▪ B-symptoms
▪ Bulky lymph node or
▪ Splenomegaly > 6cm below the left costal margin.
➢ Anemia
➢ Thrombocytopenia

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Chapter 14; Leukaemia (የደም ካንሰር)

14.2.2 Chronic myelogenous leukemia (CML)


➢ CML, (a.k.a chronic myelocytic, chronic myelogenous, or chronic granulocytic
leukemia) is a myeloproliferative neoplasm characterized by the dysregulated
production and uncontrolled proliferation of mature and maturing granulocytes
with fairly normal differentiation.
➢ In addition to CML the other diseases classified as myeloproliferative are;
▪ Polycythemia vera (PV)
▪ Essential thrombocythemia (ET), and
▪ Primary myelofibrosis.
➢ CML results from a chromosomal abnormality. Two adjacent
chromosomes are involved; namely, chromosome number 9 and 22. A
portion of chromosome 9 moves to the end of chromosome 22 and a
portion of chromosome 22 moves to the end of chromosome 9, a
process called translocation. The abnormal chromosome is called the
Philadelphia (Ph) chromosome.
➢ The break on chromosome 9 leads to a mutation of a gene called
“ABL” (for Herbert Abelson). The break on chromosome 22 involves a
gene called “BCR” (for breakpoint cluster region). The resulting fusion
gene is called the BCR-ABL gene.
➢ The BCR-ABL fusion gene directs the production of an abnormal
enzyme called BCR-ABL tyrosine kinase.
➢ This abnormal enzyme causes the leukemic changes in the bone
marrow myeloid precursor cells.
➢ This enzyme is the primary target of the current treatment of CML.
➢ The clinical hallmark of CML is the uncontrolled production of mature and
maturing granulocytes, predominantly neutrophils, but also basophils and
eosinophils.
➢ In the absence of treatment, CML has a triphasic or biphasic clinical course as
it progresses from a chronic phase to an accelerated phase and on to a
terminal blast crisis.
➢ Sometimes it goes from chronic phase directly to blast crisis, particularly when
the blast phase is lymphoid.

EPIDEMIOLOGY
➢ CML accounts for approximately 15 to 20 % of leukemias in adults. It has an
annual incidence of 1 to 2 cases per 100,000, with a slight male
predominance.
➢ The median age at presentation is approximately 50 years for patients enrolled
on clinical studies, but the actual median age from cancer registry data may
be 10 years older.
➢ Exposure to ionizing radiation is the only known risk factor.

CLINICAL MANIFESTATIONS

➢ CML has a triphasic or biphasic clinical course:


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▪ A chronic phase, which is present at the time of diagnosis in


approximately 85 % of patients;
▪ An accelerated phase, in which neutrophil differentiation becomes
progressively impaired and leukocyte counts are more difficult to control
with treatment; defined as the presence of one of the following
• Blast cells constituting 10 to 19% of the cells in the peripheral
blood or bone marrow
• Basophilia > 20% of the cells in the peripheral blood
• Persistent thrombocytopenia <100,000/µl
• Persistent thrombocytosis >100,000/µl unresponsive to therapy
• Increasing spleen size and WBC count unresponsive to therapy
• Cytogenic clonal evolution
▪ Blast crisis, a condition resembling acute leukemia in which myeloid or
lymphoid blasts proliferate in an uncontrolled manner. Defined as the
presence of one of the following
• Blasts ≥ 20% in the peripheral blood or bone marrow
• Extramedullary blast proliferation, apart from the spleen
• Large foci or clusters of blasts in the bone marrow biopsy
➢ The clinical findings at diagnosis of CML vary among reported series and also
depend upon the stage of disease at diagnosis.
➢ 20 to 50 % of patients are asymptomatic, with the disease first being
suspected from routine blood tests.
➢ Among symptomatic patients, systemic symptoms are common such as
▪ Fatigue (34 %)
▪ Malaise (3 %)
▪ Weight loss (20 %)
▪ Excessive sweating (15 %)
▪ Abdominal fullness (15 %), and
▪ Bleeding episodes due to platelet dysfunction (21 %).
➢ Abdominal pain and discomfort may include left upper quadrant pain
(sometimes referred to the left shoulder) and early satiety, due to the enlarged
spleen with or without perisplenitis and/or splenic infarction.
➢ Tenderness over the lower sternum, due to an expanding bone marrow, is
sometimes seen.
➢ Acute gouty arthritis may also present at this time, due to overproduction of
uric acid.
➢ Other frequent findings include
▪ Splenomegaly (present in 48 and 76 % in two series)
▪ Anemia (45 and 62 %)
▪ WBC count above 100,000/µL (52 and 72 %), and
▪ Platelet count above 600,000 to 700,000/µL (15 and 34 %).
➢ Involvement of extramedullary tissues such as the lymph nodes, skin, and soft
tissues is generally limited to patients with blast crisis.
➢ In accelerated phase patients tend to be more symptomatic. Spleen size
increases, and symptoms of anemia. The presentation in blast crisis phase like
that of acute leukemia (infection, bleeding, and rapid deterioration in clinical
status).
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Chapter 14; Leukaemia (የደም ካንሰር)

DIAGNOSIS

➢ When to suspect CML?


▪ CML should be suspected in patients with Leucocytosis, usually
exceeding 30,000/µl, with elevated granulocyte counts (neutrophils,
basophils or eosinophils).
▪ The peripheral smear typically demonstrates a leucocytosis with a median
white count of approximately 100,000/µL (range 12 to 1000/µL).
▪ The platelet count can be normal or elevated. Platelet counts
above 600,000/µL are seen in 15 to 30 % of patients.
▪ Low platelet counts or thrombocytopenia, if present at diagnosis, should
make one reconsider other diagnostic possibilities, such as one of the
myelodysplastic syndromes.
▪ Other supportive features: splenomegaly and thrombocytosis
(increased platelet count)

Diagnosis confirmation

→ The diagnosis of CML requires the following important diagnostic studies

➢ Peripheral blood smear


▪ It shows increased granulocyte cell lines at all stages of
development (mature, intermediately mature and immature).
▪ The white blood cell differential typically shows virtually all cells of the
neutrophilic series, from myeloblasts to mature neutrophils with peaks in
the percent myelocytes and segmented neutrophils.
▪ Blasts typically account for < 2 %.
▪ The presence of a greater percent of myelocytes than the more mature
metamyelocytes ("leukemic hiatus" or "myelocyte bulge") is one of the
classic findings in CML.
▪ A normochromic, normocytic anemia is seen in 45 to 60 % of patients.

➢ Bone marrow aspiration


▪ Hypercellular marrow with increased myeloid to erythroid ratio.
▪ Bone marrow aspiration and biopsy demonstrates granulocytic hyperplasia
with a maturation pattern that reflects that seen in the peripheral smear.
▪ There is usually a widened area of immature neutrophils in the
paratrabecular cuff and mature neutrophils are found in the intertrabecular
areas.
▪ The peripheral blood and bone marrow aspirate differential count are key
components of determining the disease stage.
▪ In general, peripheral blood and bone marrow blasts between 10 and 19
% are diagnostic of accelerated phase disease, while blasts over 20 %
are diagnostic of blast crisis.
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➢ Genetics
▪ Confirmation of the presence of either Philadelphia chromosome or
the abnormal fusion gene (BCR-ABL)
▪ The diagnosis of CML is first suspected by identifying the typical findings
in the blood and bone marrow, and then confirmed by the demonstration
of the Philadelphia chromosome, the BCR-ABL1 fusion gene or the BCR-
ABL1 fusion mRNA by conventional cytogenetics, fluorescence in situ
hybridization (FISH) analysis, or reverse transcription polymerase chain
reaction (RT-PCR).

TREATMENT

➢ Overview — the two main treatment options for patients with newly diagnosed
chronic phase (CP) CML are:
▪ BCR-ABL1 tyrosine kinase inhibitors (TKIs)
➢ Treatment of CML with targeted tyrosine kinase inhibitors is highly
effective, safe and available in Ethiopia.
➢ Tyrosine kinase inhibitors (TKIs): Imatinib mesylate, Nilotinib, Bosutinib,
and Ponatinib.
➢ Imatinib mesylate is used as first line in most patients.
➢ The goal of treatment is not only to achieve clinical and hematologic
remission but also a complete molecular remission.
➢ Allogeneic hematopoietic cell transplantation (HCT).

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CHAPTER 15; Lymphomas (የደም ካንሰር)

CHAPTER 15; Lymphomas (የደም


ካንሰር)
Dr. Asmare.W, Dr.Mulualem. G

Clinical features and how to write hx of Lymphoma pt’


History

Clinical Diagnosis

➢ Painless lymph node enlargement (Lymphadenopathy)


▪ In indolent lymphomas the lymph node enlargement can be waxing
and waning.
▪ The spread in NHL tend to be unpredictable, skipping lymph node
regions.
▪ Compressive symptoms: Shortness of breath, abdominal mass
➢ B-symptoms
▪ Weight loss: ≥ 10% weight loss in < 06 months
▪ Unexplained fever (>38.5o C) or drenching night sweats.
➢ Fatigue
➢ Extra-nodal symptoms
➢ GI symptoms: Diarrhea, GI bleeding, early satiety.
➢ Testicular enlargement
➢ CNS symptoms: Headache, weakness of extremities

Signs
➢ Enlarged lymph nodes: all lymph node regions need to be examine
➢ Splenomegaly
➢ Hepatomegaly
➢ Abdominal mass
➢ Pallor

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Characterization of patient history

➢ Pt’s may present with


▪ Bilateral neck swelling
▪ Fever → chronic fever commonly more than 2 weeks
➢ Bilateral neck swelling (LAP)
▪ E.g. Swelling over the neck, latter under armpits, groin area
bilaterally
▪ Initially pea sized, which increase progressively to attain it’s current
size with in “x” weeks/months
▪ Discharge from the swelling or not
▪ Gradual in onset
▪ Together with bilateral swellings of the arm pit and the inguinal
area
➢ Fatigue
➢ Fever
▪ Low grade
▪ Intermittent
▪ Worsen at night
▪ Associated with profuse sweating
▪ B symptoms → fever, sweating, weight loss
➢ Significant weight loss
▪ E.g. significant weight loss from 53 kg to 45 kg which is 15% of
his/her initial body weight or
▪ Unquantified but significant weight loss to the extent his/her closes
become loose (if s/he didn’t remember his/her initial body weight
but claim that S/he lose his/her body weight)
➢ Abdominal swelling → Organomegaly, it is not localized mass unlike
lymphoma
▪ Painless
▪ Over the right/ left upper quadrant
▪ Associated with early satiety and loss of appetite
➢ Vomiting and diarrhoea → characterize it

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Risk factors

RF for HL

➢ Infection → EBV, HHV6


➢ Family history
▪ 99 times increased in monozygotic twins
▪ 7 times increased in sibilinges
➢ Low Socio-economic status
➢ Higher education level

RF for NHL

➢ Immunodeficiency
▪ Inherited
• SCID (Severe combined immunodeficiency)
• Wiskott-Aldrich syndrome
▪ Acquired
• Malnutrition
• Malignancy
• RVI
• Steroids
• DM
➢ Autoimmune disorders
▪ Autoimmune hemolytic anemia
▪ RA
▪ SLE
➢ Inflammatory disorders
▪ IBD treated with azathioprine/6-MP
➢ Chemicals and drugs
▪ Phenytoin
▪ Dioxin
▪ Chemoradiotherapy
➢ Infectious Agents
▪ HIV
▪ TB
▪ H.pylori
▪ HCV
▪ C. jejuni
▪ EBV
▪ HTLV
▪ HHS-8
➢ Genetics → Ataxia telangiectasia, Bloom sxx, down sxx
Lymphomatoid Papulosis
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CHAPTER 15; Lymphomas (የደም ካንሰር)

Complication of Lymphoma

➢ See complications of Leukaemia


➢ Oncologic Emergency → Prompt recognition and therapy is critical for these
situations, which may be life-threatening and/or interfere with and delay
treatment of the underlying NHL. These can include:
▪ Spinal cord compression
▪ Pericardial tamponade
▪ Hypercalcemia (eg, adult T cell leukemia-lymphoma)
▪ Superior or inferior vena cava obstruction
▪ Hyperleukocytosis (eg, B or T cell lymphoblastic leukemia/lymphoma)
▪ Acute airway obstruction (eg, mediastinal lymphoma)
▪ Lymphomatous meningitis and/or CNS mass lesions
▪ Hyperuricemia and tumor lysis syndrome
▪ Hyperviscosity syndrome (eg, lymphoplasmacytic lymphoma with
Waldenstrom macroglobulinemia)
▪ Intestinal obstruction, intussusception
▪ Ureteral obstruction, unilateral or bilateral hydronephrosis
▪ Severe hepatic dysfunction
▪ Venous thromboembolic disease
▪ Severe autoimmune hemolytic anemia and/or thrombocytopenia (eg, small
lymphocytic lymphoma)
➢ Complications of chemotherapy
▪ Acute
• Serous mucositis
• Infection
• Cytopenia
• Electrolyte imbalance
• Poor nutrition
▪ Chronic cxn
• Cardiac toxicity
• Gonadal toxicity with infertility
• 2ry malignancy

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Sample history

C.C → Bilateral neck swelling of 1-year duration


HPI
This patient was last relatively healthy 1 year ago at which time he
started to experience bilateral gradual swelling of the lateral neck. Initially
the swellings at first were bean sized but later progressively increase in
size to attain its current size within 6 months. It was itching, non-movable
and painless. After few weeks he started to develop Low grade Intermittent
fever which Worsen at night Associated with profuse sweating and gradual
loss of appetite. 9 months before admission he also started to experience
gradual onset of fatigue, bilateral swellings over the arm pit and the
inguinal area which had the same properties as the primary swelling. He
has also Unquantified but significant weight loss to the extent his trousers
become loose Abdominal swelling. He has also Painless swelling left upper
quadrant of abdomen with dragging sensation Associated with early satiety.

For these complaints he Visited a local traditional healer who gave


him a topical remedy to rub on the swelling. After few days of applying the
substance the swelling over later neck started to ulcerate and bleed for few
minutes.

Due to this he went to a private clinic which upon history and


physical examination referred him to a health centre near town. There he
had unspecified laboratory examination the result of which the source of
history doesn’t know but was again referred to our Hospital for better
investigation and management.

➢ No hx of exposure to herbicides, pesticides, benzine or Radio


chemotherapy (RF)
➢ No hx of similar illness in the family (Genetics → RF)
➢ No hx of drug intake other than those mentioned above (Phenytoin, Dioxin,
chemo radio therapy → RF)
➢ She was screened for RVI 5 months back and found to be NR (RVI → RF)
➢ No hx of chronic cough, contact with chronic cougher or a known TB pt,

no hx of previous TB RX (TB → RF)


➢ She usually eats injera made of ‘‘teff’’ and ‘‘machilla’’ and ‘’wott’’ made
of ‘‘atter’’ and ‘‘dagusa’’ 3-4 times per day. Occasionally she eats meat
during holidays.
➢ No hx of photosensitivity, malar rash or joint pain (SLE → RF)
➢ No hx of gum bleeding, Nasal bleeding, or Bleeding from other sites
(CXN)
➢ No hx of abdominal pain, Abdominal distension or bowel habit change
(Intestinal obstruction → CXN).
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➢ No hx of cough, chest pain, dyspnoea or haemoptysis (Lung Metastasis → CXN)


➢ No hx of palpitation, leg edema, orthopnea or PND (Pericardial tamponade
→ CXN)
➢ No hx of Flank pain, decreased UOP or hematuria (Ureteral obstruction, unilateral
or bilateral hydronephrosis → CXN)
➢ No hx of Headache, Nausea, vomiting, body weakness or Seizure
(Leukemic meningitis features → CXN)
➢ She is not from malaria/kalazar endemic area, no travel hx to endemic
area or previous attack (VL, HMS → DDX)
➢ No self or family hx of HTN, DM or asthma

Finally, he was admitted to our hospital supported physically by her families

Physical examination (pertinent findings)

1 GA
➢ RD 2ry to
▪ Mediastinal LAP causing Airway obstruction which is an oncologic
emergency
▪ Severe anemia

2 Vital signs
3 HEENT
➢ Dry blood on Nostrils
➢ Mass in the jaw or neck → Burkitt lymphoma
➢ Icteric sclera → Obstructive jaundice 2ry to NHL
➢ Unilateral tonsillar hypertrophy
➢ Active Rhinorrhea

4 LGS
➢ LAP → Bulky (> 10cm in size), non-tender, firm, rubbery, cervical or
supra clavicular LAP
5. RS

➢ Pleural effusion from NHL


➢ SVC (Superior vana cava) syndrome, Superior mediastinal sxx →
oncologic emergency
6. CVS
➢ Pericardial effusion (cardiac Tamponade)
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➢ Beck’s triad of cardiac tamponade include


1) Distended neck vein
2) Hypotension
3) Distant / muffled heart sounds
7. Abdominal examination
➢ HSM
➢ Palpable abdominal mass → NHL
➢ Ascites → NHL
➢ Peritonitis features → guarding, rigidity, rebound tenderness → NHL
➢ Abdominal distension 2ry to intussusception in young children → NHL as
leading point
8. GUS
➢ Testicular enlargement
9. MSS
10. IS
11. NS
➢ Paraplegia → from paraspinal metastasis of NHL (Spinal cord
compression)
➢ CN palsy
➢ Hearing loss

DDX

12)Non- Hodgkin’s Lymphoma (NHL)


13)Hodgkin’s Disease (Hodgkin’s Lymphoma/HL/)
14)Tuberculosis (Disseminated)
15)CLL
16)Melanoma
17)Small cell carcinoma of Lung
18)HIV
19)Toxoplasmosis
20)Sarcoidosis
21)SLE
22)Syphilis
23)Brucellosis
24)IM (Infectious mononucleosis)
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IX

Diagnostic IX
1. CBC → Pancytopenia
2. PM (Peripheral morphology)
3. BM aspiration and Biopsy
4. LN biopsy, FNAC (Cytology)
• Peripheral smear
• RBC morphology
• WBC
• Platelet
5. Splenic aspiration → Malignant infiltration

Baseline IX
6. BG and Rh, cross match → If HgB < 8, Transfuse
7. OFT → RFT, LFT → before starting chemotherapy
8. Liver enzymes → AST (SGOT), ALT (SGPT) → before starting
chemotherapy
9. CXR
☛ Mediastinal mass
☛ Hilar Lymphadenopathy
☛ Pleural effusion from NHL
☛ Disseminated TB (primary focus from Lung)
☛ Pneumonia super infection
10. ESR → Persistent elevation is poor prognosis
11. Abdominal U/S
☛ Intraabdominal LAP
☛ Hepatic/splenic infiltration
☛ Ascites
☛ Oncologic emergency like obstruction
12. PICT
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14. BF
15. AFB

Other IX based on indication


16. Serum electrolyte → Tumor lysis SXX (see from
leukemia click here →)
17. ECHO and ECG
18. LP → Leukemic meningitis, before Rx (Chemotherapy)
19. Coagulation profile
20. X-ray of extremities → Pathologic #
21. LDH Level → to asses tumour burden
22. Serum Uric acid level → to asses tumour burden
Peritoneal, pleural and pericardial aspiration → if there is effusion

23. Infectious agent Serology → Not available in Ethiopia


▪ EBV
▪ HHV 6

Staging investigations:
▪ Chest x-ray
▪ Abdominal ultrasound or CT-scan
▪ Bone aspiration or biopsy

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Discussion

➢ Lymphomas are neoplastic transformation of the cells of lymphoid tissues. The


origins could be in nodal sites (lymph nodes) or extra-nodal sites e.g. GI,
CNS.
➢ There are dozens of subtypes of lymphomas. The two main categories of
lymphomas are Hodgkin's lymphomas (HL) and the non-Hodgkin lymphomas
(NHL).
➢ WHO includes two other categories as types of lymphoma: multiple myeloma
and immunoproliferative diseases.
➢ About 90% of lymphomas are non-Hodgkin lymphomas.
➢ Lymphomas and leukemia’s are a part of the broader group of tumors of the
hematopoietic and lymphoid tissues.
➢ HIV infection with severe immunosuppression is associated with
increased incidence of sets of aggressive/highly aggressive lymphomas
which are called HIV-associated lymphomas. These include:
▪ Primary CNS lymphoma
▪ Primary effusive lymphoma
▪ HIV-associated large B-cell lymphoma, and
▪ HIV-associated Burkitt‘s lymphoma.

Source; Robbins and Cotran Pathologic Basis of Disease, 9th Edition

15.1 Hodgkin’s lymphoma (HL)

➢ HL, formerly called Hodgkin's disease, arises from germinal center or post-
germinal center B cells.
➢ HL has a unique cellular composition, containing a minority of neoplastic cells
(Reed-Sternberg cells and their variants) in an inflammatory background.
➢ It is separated from the other B cell lymphomas based on its unique
clinicopathologic features, and can be divided into two major sub-groups, based
on the appearance and immunophenotype of the tumor cells.
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➢ Hodgkin ‘s lymphoma is a distinct group of lymphomas with few histologic sub-


types.
➢ It predominately involves lymph nodes; extra-nodal involvement is not common.
➢ HL arises in a single node or chain of nodes and spreads first to anatomically
contiguous lymphoid tissues.
➢ HL also has distinctive morphologic features. It is characterized by the
presence of neoplastic giant cells called ReedSternberg cells.
➢ It progresses from one lymph node region to other in fairly predictable fashion.

Source; Robbins and Cotran Pathologic Basis of Disease, 9th Edition

Classification.

The WHO classification recognizes five subtypes of HL:


➢ Classical HL
▪ Nodular sclerosis
▪ Mixed cellularity
▪ Lymphocyte-rich
▪ Lymphocyte depletion
➢ Lymphocyte predominance
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➢ Classical HL
▪ The tumor cells in this group are derived from germinal center B cells,
but typically fail to express many of the genes and gene products that
define normal germinal center B cells.
▪ Based on differences in the appearance of the tumor cells and the
composition of the reactive background, classical HL is further divided
into the following subtypes:
• Nodular sclerosis classical HL (NSHL)
• Mixed cellularity classical HL (MCHL)
• Lymphocyte rich classical HL (LRHL)
• Lymphocyte depleted classical HL (LDHL)
➢ Nodular lymphocyte predominant HL – The tumor cells in this subtype retain
the immunophenotypic features of germinal center B cells.

EPIDEMIOLOGY
Represents ~10% of all cases of malignant lymphoma.
Typically affects young adults Presents with painless lymphadenopathy involving
the neck and chest; systemic symptoms are common.
HL has a bimodal age distribution curve. The pattern of age-specific incidence
differs by geographic location and appears to parallel the level of industrial
development: In the US and other economically advantaged countries, there is
one peak in young adults (approximately age 20 years) and one in adults of
older age (approximately age 65 years); the majority of patients are young
adults.
In the US and Europe, the approximate percentage of classic HL cases from
each subgroup are as follows:
▪ Nodular sclerosis classical HL (70 %)
▪ Mixed cellularity classical HL (20 to 25 %)
▪ Lymphocyte rich classical HL (5 %)
▪ Lymphocyte depleted classical HL (<1 %)

Risk factors
Socioeconomic status and the environment
▪ In economically advantaged countries, the risk of developing HL as a
young adult is consistently associated with factors indicative of a high
standard of living in early childhood, including single family housing and
small family size.
▪ These associations appear to be specific for the nodular sclerosis
subtype of HL and for disease occurring from early childhood through
middle adulthood.
Immunosuppression
▪ the incidence of HL is increased in a number of settings associated with
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transplantation, therapy with immunosuppressive drugs (e.g, in patients


with autoimmune disease), and HIV infection.
Autoimmune disorders
▪ Patients with a history of autoimmune disorders are at increased risk for
the development of HL and can pose challenging management issues
due to comorbidities and late treatment related toxicities.
▪ A personal history of rheumatoid arthritis, SLE or sarcoidosis
▪ A family history of sarcoidosis or ulcerative colitis
EBV infection
▪ Incidence of HL is high among pts with history of EBV.
▪ The risk of EBV positive pts are four times; latency period is 4 years.

CLINICAL PRESENTATION
Non tender lymphadenopathy central pattern, 70 - 80 % left supraclavicular
and mediastinal B symptoms
▪ Common in patients with advanced stage disease.
Pruritis, typically is not associated with a rash
Intense pain in the sites of disease upon alcohol ingestion
Obstructive symptoms
Fluid collections in the third space
Organomegally
The clinical presentation also varies according to the histologic subtype of
▪ Classic HL NS
• Accounts for 70% of cases in the Western world.
• Mediastinal involvement is common
• Males and females are affected in equal proportion
• Most patients are between the ages of 15 and 35 years.
▪ Mixed cellularity
• The second-most-common subtype in the industrial world,
representing 20% of cHL.
• The median age of presentation is 38
• Males are affected more commonly.
• Patients typically present with peripheral lymphadenopathy
• Splenic involvement occurs in 30%
• Advanced at the time of presentation
• Associated with a poorer prognosis than NS.
▪ LR cHL
• Early stage disease
• Peripheral nodes
• Patients are older 43 years
▪ LD cHL
• Is the least common subtype
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• It is more common in the industrial world and in HIV-infected


individuals
• The median age of onset is in the 30
• Males are more often affected
• Extra nodal and intra-abdominal disease commonly is seen
• Advanced stage disease and systemic symptoms are common
Bone marrow involvement 50%
▪ Has the worst prognosis
▪ Extra nodal and intra-abdominal disease commonly is seen
▪ Advanced stage disease and systemic symptoms are common.
Spleen involvement in CHL
▪ In pt with LAP below the diaphragm
▪ Systemic symptoms
▪ MC
▪ Can occur without splenomegaly
▪ Splenomegaly can be found without tumor involvement

Diagnosis
LN biopsy is diagnostic
▪ RSC with surrounding inflammatory cells
▪ RSC not specific for HL
Immunostaining
▪ Confirm the diagnosis of HL
▪ cHL is positive for
• CD 30 in all cases
• CD 15 in 85 %
• CD 20 in 20%
• Negative CD 45
Lab features; No diagnostic lab features
▪ CBC; anemia, thrombocytopenia, lymphopenia
▪ ESR elevated
▪ LFT increased
▪ LDH and , uric acid will be elevated
▪ Serum albumin will be low
▪ B2 microglobuline high
▪ HIV test
Imaging
▪ CXR, CT, PET
▪ Cardiac evaluation and pulmonary function tests
▪ BM biopsy for staging, can be deferred in most patients

STAGING 836
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➢ Main determinant of prognosis and treatment


➢ The Ann Arbor staging system has been employed in HL for more than 25
years.
➢ The Ann Arbor staging system with Cotswolds modifications is the current
staging system

➢ There are four stages

Table: Ann Arbor staging of lymphoma


Stage Area of involvement
I ➢ Involvement of a single lymph node region or a single
lymphoid organ (e.g. spleen, thymus).(I)
OR
➢ Involvement of non-lymphoid organ(site) without any
lymph node involvement(IE)
II ➢ Involvment of two or more lymph node regions or
lymphoid organ on the same side of diaphragm.(II)
OR
➢ Involvement of a single non-lymphoid organ(site) with
regional lymph node +/- non-regional lymph node on the
same side of the diaphragm.(IIE)
III ➢ Multiple lymph node regions or lymphoid organ on both
sides of diaphragm with or without non-lymphoid organ
(site) involvement.
▪ When extra lymphoid organ is involved =III E
▪ When spleen is involved = III S
▪ When both are involved = III E, S
IV Any involvement of the liver or bone marrow, lungs (other
than direct extension, or cerebrospinal fluid.
Additional A: No B-symptoms
characterization B: B -symptoms
E: Involvement of extra lymphoid organ (site)
S: Splenic involvement

N.B, all cases are sub classified to indicate the absence (A) or presence (B)
of one or more of the following three systemic symptoms
▪ Significant unexplained fever, night sweats, or unexplained weight loss
exceeding 10 % of body weight during the six months prior to diagnosis.

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Depends on the stage of the disease and the presence of adverse prognostic
factors.
Treatment group includes
▪ Early stage favorable and unfavorable
▪ Advanced stage
Treatment of early stage HL
Early stage Includes CS I and II; Further classified in to two
▪ Early stage favorable; no risk factors
▪ Early stage unfavorable; one or more risk factors
Risk factors in early stage Hodgkin lymphoma. A number of prognostic
indicators have been identified in early stage cHL
The GHSG scale includes five risk factors
▪ Bulky mediastinal disease
▪ ESR of ≥30 in the presence of B symptoms or ≥50 without B symptoms
▪ Extranodal extension of disease
▪ Three or more lymph node sites of involvement.
The EORTC scale includes
▪ Age ≥50 years
▪ Bulky mediastinal disease
▪ ESR of ≥30 in the presence of B symptoms or ≥50 without B symptom
▪ Four or more nodal sites of involvement
Therapeutic options include combined modality therapy:
Early Favorable disease
▪ Two to four cycles of ABVD30 plus IFRT31 20- 30 GY
▪ Stanford V for 8 weeks plus 30 GY IFRT to sites > 5cm
Early unfavorable disease non-bulky disease
▪ Four cycles of ABVD plus 30 GY IFRT
▪ Two cycles of escalated BEACOPP32 plus two cycles of ABVD plus 30
GY IFRT
For patients with bulky disease
▪ 4 to 6 cycles of ABVD or stanford V followed by 36 GY IFRT

Treatment of advanced stage HL


Advanced stage includes- CS III and CS IV
Options of treatment
▪ ABVD 6 cycles
▪ Stanford V with IFRT
▪ Escalated BEACOPP

30
ABVD = Adriamycin(doxorubicin), Bleomycin, Vinblastin, Dacarbazin
31
IFRT = Involved Field Radiotherapy
32
BEACOPP (escalated) = Bleomycin, Etoposide, Adriamycin, cyclophosphamide,
oncovin(vincristin), procarbazin, Prednisone, G-csf.
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International Prognostic Score in advanced-stage HL.


▪ Age >45 years
▪ Male
▪ WBC >15,000/mm3
▪ Hgb <10.5 g/dl
▪ Absolute lymphocyte count <600/mm3 or <8% of WBC
▪ Albumin <4.0 g/dl
▪ Stage IV disease.

15,2 Non Hodkins lymphoma

Non-Hodgkin’s lymphomas (NHL) are cancers of mature B, T, and natural killer


(NK) cells.
They were distinguished from Hodgkin’s lymphoma (HL) upon recognition of the
Reed-Sternberg (RS) cell and differ from HL with respect to their biologic and
clinical characteristics.
Whereas ∼80–85% of patients with HL will be cured of their lymphoma by
chemotherapy with or without radiotherapy, the prognosis and natural history of
NHL tends to be more variable.
NHL can be classified as either a mature B-NHL or a mature T/NK-NHL
depending on whether the cancerous lymphocyte is a B, T, or NK cell,
respectively.
The vast majority of NHLS are B-cell in origin.
Within each category are lymphomas that grow quickly and behave
aggressively, as well as lymphomas that are more indolent, or slow growing, in
nature.
For a list of the WHO classification of lymphoid neoplasms.

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Source; Robbins and Cotran Pathologic Basis of Disease, 9th Edition


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TABLE 108-1 (Harrison 21st edition) WHO Classification of Lymphoid


Malignancies

Epidemiology
Incidence of NHL has been increasing steadily in North America and other
industrial countries with a doubling of cases between 1970 and 1990 and
stabilization thereafter.
Fifth most common ca in USA – 4.2% of all cases of ca
▪ Mean age at Dx 45- 55 years
▪ More common in male
▪ Higher in whites than blacks
Risk factors
▪ Infection; EBV, HTLV-I, HHV-8, HCV, H. Pylori, Chlamydia psittaci,
Campylobacter jejuni, Borrelia burgdorferi
▪ Occupational exposure to certain pesticides and herbicides
▪ Drugs
▪ Congenital disease; ataxia-telangiectasia, Wiskott-Aldrich syndrome.
▪ Acquired; Immunosuppression associated with HIV infection, Iatrogenically
induced immune suppression in the organ transplantation setting,
Autoimmune disorders: - rheumatoid arthritis, Sjögren syndrome, and
Hashimoto thyroiditis, IBD, SLE;HL.

CLINICAL PRESENTATION
The clinical presentation of NHL varies tremendously depending upon the type
of lymphoma and the areas of involvement.
Some NHLs behave indolently with LAP waxing and waning over years. Others
are highly aggressive, resulting in death within weeks if left untreated. In
typical cases:
Aggressive lymphomas commonly present acutely or subacutely with a rapidly
growing mass, systemic B symptoms (ie, fever, night sweats, weight
loss), and/or elevated levels of serum lactate dehydrogenase and uric acid.
Examples of lymphomas with this aggressive or highly aggressive presentation
include
▪ Diffuse large B cell lymphoma
▪ Burkitt lymphoma
▪ Adult T cell leukemia-lymphoma, and
▪ Precursor B and T lymphoblastic leukemia/lymphoma.
Indolent lymphomas are often insidious, presenting only with slow growing LAP,
hepatomegaly, splenomegaly, or cytopenias.
Examples of lymphomas that typically have indolent presentations include
▪ Follicular lymphoma
▪ Chronic lymphocytic leukemia/small lymphocytic lymphoma, and
▪ Splenic marginal zone lymphoma. 841
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The natural history of these tumors shows significant patient-to-patient


variability.
Less common presentations include skin rash, pruritus, exaggerated
(hypersensitivity) reactions to insect stings or bites, generalized fatigue,
malaise, fever of unknown origin, ascites, and effusions.
Approximately 50 % of patients develop extranodal disease (secondary
extranodal disease) during the course of their disease, while between 10 and
35 % of patients have primary extranodal lymphoma at diagnosis.
The initial presentation may reflect involvement of extranodal tissues, as
follows:
▪ Patients with primary GI tract lymphoma may present with anorexia,
weight loss, nausea and vomiting, chronic pain, abdominal fullness, early
satiety, symptoms associated with visceral obstruction, or even acute
perforation and GI hemorrhage. Occasional patients will present with
malabsorption syndrome.
▪ Patients with primary CNS lymphoma may present with headache,
lethargy, focal neurologic symptoms, seizures, paralysis, spinal cord
compression (0.1 to 6.5 percent of patients), or lymphomatous
meningitis.

Oncologic emergencies

Potentially emergent complications of NHL need to be considered during the


initial workup and evaluation.
Prompt recognition and therapy is critical for these situations, which may be
life-threatening and/or interfere with and delay treatment of the underlying NHL
These can include:
▪ Spinal cord compression
▪ Pericardial tamponade
▪ Hypercalcemia (eg, adult T cell leukemia-lymphoma)
▪ Superior or inferior vena cava obstruction
▪ Hyperleukocytosis (eg, B or T cell lymphoblastic leukemia/lymphoma)
▪ Acute airway obstruction (eg, mediastinal lymphoma)
▪ Lymphomatous meningitis and/or CNS mass lesions
▪ Hyperuricemia and tumor lysis syndrome
▪ Hyperviscosity syndrome (eg, lymphoplasmacytic lymphoma with
Waldenstrom macroglobulinemia)
▪ Intestinal obstruction, intussusception
▪ Ureteral obstruction, unilateral or bilateral hydronephrosis
▪ Severe hepatic dysfunction
▪ Venous thromboembolic disease
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▪ Severe autoimmune hemolytic anemia and/or thrombocytopenia (eg, small


lymphocytic lymphoma

If patients with NHL develop angioedema, they may have an acquired form of
C1 inhibitor deficiency that requires emergent treatment with infused C1
inhibitor concentrates
Systemic complaints (B symptoms) — Up to 40 % of patients with NHL present
with systemic complaints of fever, weight loss, or night sweats (ie, B
symptoms).
These complaints are of importance in determining prognosis, and have been
formally defined as follows:
▪ Fever – Temperature >38°C (>100.4°F)
▪ Weight loss – Unexplained loss of >10 percent of body weight over the
past six months
▪ Sweats – The presence of drenching night sweats
Lymphadenopathy — More than two-thirds of patients with NHL present with
peripheral lymphadenopathy that is generally painless.
Fever of unknown origin; NHL, especially one of the aggressive or highly
aggressive variants, is a common cause of FUO due to malignancy.
Hepatosplenomegaly

DIAGNOSIS and Investigations


The diagnosis lymphoma needs lymph node biopsy.
FNAC is not enough
Once a diagnosis of lymphoma is made further investigations are needed for
staging, prognosis, and for treatment purposes.
▪ CBC
▪ Uric acid level
▪ LDH
▪ LFT
▪ BUN and Creatinine
▪ Hepatitis B and C virus serologies, HIV screening
▪ Staging investigations: Chest x-ray, abdominal ultrasound or CT-scan,
bone aspiration or biopsy

TREATMENT
Indolent
▪ Potential cure only through HSCT (Hematopoietic stem cell
transplantation).
▪ Watchful waiting early on for some patients
▪ Chemotherapy/immunotherapy/radiotherapy/ combination with indication
Aggressive
▪ Chemotherapy as soon as the dx is established 843
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▪ Radiotherapy for the right indications


▪ HSCT
Highly aggressive
▪ Highly chemo sensitive. SO, Chemotherapy ASAP
NB; The most common chemotherapy used for non-Hodgkin lymphoma is
CHOP-R. (C-cyclophosphamide, H-hydroxydaunorubicin, O-oncovin, P-
prednisone, R-rituximab)

15.3 Special considerations

15.3.1 Tumor lysis syndrome (TLS)

It is an oncologic emergency that is caused by massive tumor cell lysis with


the release of large amounts of potassium, phosphate, and nucleic acids into
the systemic circulation.
Catabolism of the nucleic acids to uric acid leads to hyperuricemia, and the
marked increase in uric acid excretion can result in the precipitation of uric
acid in the renal tubules and can also induce renal vasoconstriction, impaired
autoregulation, decreased renal blood flow, and inflammation, resulting in acute
kidney injury.
Hyperphosphatemia with calcium phosphate deposition in the renal tubules can
also cause acute kidney injury.
TLS most often occurs after the initiation of cytotoxic therapy in patients with
high-grade lymphomas (particularly the Burkitt subtype) and acute lymphoblastic
leukemia. However, TLS can occur spontaneously and with other tumor types
that have a high proliferative rate, large tumor burden, or high sensitivity to
cytotoxic therapy.

PATHOGENESIS
In the setting of a malignancy with a high proliferative rate, large tumor
burden, and/or a high sensitivity to treatment, initiation of cytotoxic
chemotherapy, cytolytic antibody therapy, radiation therapy, or sometimes
glucocorticoid therapy alone can result in the rapid lysis of tumor cells.
These releases massive quantities of intracellular contents (potassium,
phosphate, and nucleic acids that can be metabolized to uric acid) into the
systemic circulation. The metabolic consequences include;
▪ Hyperkalemia
▪ Hyperphosphatemia
• The phosphorus concentration in malignant cells is up to four times
higher than in normal cells. Thus, rapid tumor breakdown often 844
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leads to hyperphosphatemia, which can cause secondary


hypocalcemia.
• When the calcium concentration times phosphate concentration (the
calcium phosphate product) exceeds 60 mg2/dL2, there is an
increased risk of calcium phosphate precipitation in the renal
tubules, which can lead to acute kidney injury.
• In addition, precipitation in the heart may lead to cardiac
arrhythmias. Renal replacement therapy may be needed if the
calcium phosphate product is ≥70 mg2/dL2.
▪ secondary hypocalcemia
▪ hyperuricemia
• Hyperuricemia is a consequence of the catabolism of purine nucleic
acids to hypoxanthine and xanthine, and then to uric acid via the
enzyme xanthine oxidase
▪ Acute kidney injury.

Xanthinuria
Allopurinol blocks the catabolism of hypoxanthine and xanthine, leading to an
increase in the levels of these metabolites.
Xanthine is much less soluble than uric acid, and urinary alkalinization
increases the solubility of xanthine much less than the solubility of uric acid
because the pKa is much higher for xanthine
Thus, patients with massive TLS who are receiving allopurinol are at risk for
xanthine precipitation in the tubules, resulting in xanthine nephropathy or
xanthine stone formation.

CLINICAL MANIFESTATIONS
The symptoms associated with tumor lysis syndrome (TLS) largely reflect the
associated metabolic abnormalities (hyperkalemia, hyperphosphatemia, and
hypocalcemia).
They include nausea, vomiting, diarrhea, anorexia, lethargy, hematuria, heart
failure, cardiac dysrhythmias, seizures, muscle cramps, tetany, syncope, and
possible sudden death.
Cairo-Bishop definition — The Cairo-Bishop definition, proposed in 2004, provided
specific laboratory criteria for the diagnosis of TLS both at presentation and
within seven days of treatment. It also incorporated a grading system to help
delineate the degree of severity of TLS.
Laboratory TLS was defined as any ≥ 2 abnormal serum values
(hyperuricemia, hyperkalemia, hyperphosphatemia and hypocalcemia), present
within 3 days before or 7 days after instituting chemotherapy in the setting of
adequate hydration (with or without alkalinization) and use of a hypouricemic
agent.
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Clinical TLS was defined as laboratory TLS plus ≥ 1 of the following that was
not directly or probably attributable to a therapeutic agent:
▪ Increased serum creatinine concentration (≥1.5 times the upper limit of
normal [ULN])
▪ Cardiac arrhythmia/sudden death, or a
▪ Seizure.

Table; RISK STRATIFICATION


High Risk Intermidiate risk Low Risk
Risk of TLS >5 % 1 to 5 % <1 %
All Burkitt leukemia, serum LDH level
stage III or IV Burkitt ≥ 2 times the
lymphoma or early stage upper limit of
Burkitt lymphoma normal (≥2X ULN)

Early stage Burkitt lymphoma Serum LDH level <2X


ULN
Other ALL WBC ≥100,000 WBC <100,000/µL and
per serum LDH level <2X
µL and/or serum ULN
LDH level ≥2X
ULN
AML WBC count WBC 25,000 WBC count <25,000/µL and
≥100,000 per µL to 100,000/µL or serum LDH level <2X ULN
<25,000/µL and LDH ≥
2X ULN

Stage III or IV lymphoblastic serum LDH level


lymphoma or early stage ≥2X ULN
lymphoblastic lymphoma
Early stage lymphoblastic serum LDH level <2X
lymphoma ULN
Chronic lymphocytic leukemia treated treated
(CLL/SLL) with venetoclax and with fludarabine, rituximab, WBC count ≤50,000/µL
lymph node ≥10 or lenalidomide, and not treated
cm or lymph or venetoclax with lymph with fludarabine/rituximab or
nodes ≥5 cm plus nodes ≥5 cm or an venetoclax
absolute absolute lymphocyte
lymphocyte count count ≥25 x
≥25 x 109/L, and 109/L, and/or those with a
elevated serum
uric acid level
high WBC
count (≥50,000/µL)
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Adult T- serum LDH level serum LDH level above


cell lymphoma/leukemia, diffuse above the ULN but without bulky
large B-cell lymphoma, ULN and a bulky disease
peripheral T-cell lymphoma, tumor mass
transformed lymphoma, or
mantle cell lymphoma

Prevention and treatment

PREVENTION; The main prophylactic strategies are intravenous (IV) hydration


and the use of hypouricemic agents, such as allopurinol and rasburicase.

▪ IV hydration
• Aggressive IV hydration is the cornerstone of preventing TLS and
is recommended prior to therapy in all patients at intermediate or
high risk for TLS.
• The goal of IV hydration is to improve renal perfusion and
glomerular filtration, and induce a high urine output to minimize the
likelihood of uric acid or calcium phosphate precipitation in the
tubules.
▪ Allopurinol
• For the initial management of adult and pediatric patients at
intermediate risk for TLS we suggest allopurinol rather
than rasburicase, as long as pretreatment uric acid levels are not
elevated (i.e., <8 mg/dL [476 µmol/L]), although administration of a
single dose of rasburicase is a reasonable alternative in this
setting.
▪ Rasburicase
• For the initial management of most pediatric and adult patients at
high risk for TLS, especially those with impaired renal or cardiac
function, we recommend rasburicase rather than allopurinol.
• An alternative approach to allopurinol for lowering serum uric acid
levels is to promote the degradation of uric acid by the
administration of urate oxidase (uricase), which catalyzes oxidation
of uric acid to the much more water-soluble compound allantoin.
▪ Urinary alkalinization
• The role of urinary alkalinization with
either acetazolamide and/or sodium bicarbonate is unclear and
controversial.

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• In the past, alkalinization to a urine pH of 6.5 to 7 or even higher


was recommended to increase uric acid solubility, thereby
diminishing the likelihood of uric acid precipitation in the tubules

TREATMENT OF ESTABLISHED TLS

Electrolyte abnormalities…manage accordingly


Renal replacement therapy- Among the indications for renal replacement
therapy in patients with TLS are
▪ Severe oliguria or anuria
▪ Intractable fluid overload
▪ Persistent hyperkalemia
▪ Hyperphosphatemia-induced symptomatic hypocalcemia
▪ A calcium-phosphate product ≥70 mg2/dL2

15.3.2 Hyperleukocytosis and leukostasis in hematologic


malignancies

Hyperleukocytosis refers to a laboratory abnormality that has been variably


defined as a total leukemia blood cell count > 50 x 109/L (50,000/µL) or 100 x
109/L (100,000/µL).
In contrast, leukostasis (also called symptomatic hyperleukocytosis) is a medical
emergency most commonly seen in patients with AML or CML in blast crisis. It
is characterized by an extremely elevated blast cell count and symptoms of
decreased tissue perfusion.
Leukostasis is a pathologic diagnosis in which white cell plugs are seen in the
microvasculature.
Clinically, leukostasis is typically diagnosed empirically when a patient with
leukemia and hyperleukocytosis presents with respiratory or neurological
distress.
Prompt treatment is indicated since, if left untreated, the one-week mortality
rate is approximately 20 to 40 %.

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EPIDEMIOLOGY
The incidence of hyperleukocytosis and leukostasis vary by leukemia type and
patient population.
In general, symptoms of leukostasis are more common in leukemias with large,
poorly deformable blasts, such as AML.

AML ALL CLL CML


Hyperleukocytosis Present in 10 Seen in 10 to 30 % A significant Patients with CML
to 20 % of of patients with newly proportion of typically present with
patients with diagnosed ALL. patients with CLL leukocytosis and a
newly present with median WBC count of
diagnosed hyperleukocytosis approximately 100 x
AML. 109/L (100,000/ µL).

Most often, these are


segmented neutrophils,
metamyelocytes, and
myelocytes.

Symptoms of Occur less frequently and typically Rare unless the very uncommon in
leukostasis affect patients with WBC counts over WBC count patients in chronic
100 x 109/L (100,000/µL). exceeds 400 x phase but can be seen
109/L (400,000/µL). occasionally in patients
with myeloid blast crisis
and very elevated blast
counts.

Other Features TLS and DIC are


more common
complications related
to the elevated WBC
count.
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SIGNS AND SYMPTOMS


Although pathologic evidence of leukostasis can be found in most organs in
patients with extremely high WBC counts, the main clinical symptoms of
leukostasis and causes of early death are related to involvement of the CNS
(~40 %) and lungs (~30 %).
Pulmonary signs and symptoms
▪ Include dyspnea and hypoxia with or without diffuse interstitial or alveolar
infiltrates on imaging studies.
▪ Measurement of the arterial pO2 can be falsely decreased in patients
with hyperleukocytosis, since the WBCs in the test tube utilize oxygen.
Pulse oximetry provides a more accurate assessment of O2 saturation in
this setting.
Neurological signs and symptoms
▪ Include visual changes, headache, dizziness, tinnitus, gait instability,
confusion, somnolence, and, occasionally, coma.
▪ In addition, patients who present with hyperleukocytosis have an
increased risk of intracranial hemorrhage that persists for at least a week
after the reduction of WBC, perhaps from a reperfusion injury as areas
of the brain that were ischemic from leukostasis regain blood flow.
▪ Because there can be other structural causes of CNS symptoms, brain
imaging with noncontrasted CT or MRI is indicated in patients with
neurologic abnormalities.
▪ Clinicians must be cautious about using intravenous contrast dye at a
time when renal function may be compromised by leukostasis or tumor
lysis syndrome, and dehydration.
Approximately 80 % of patients with leukostasis are febrile, which may be due
to inflammation associated with leukostasis or concurrent infection. Since an
infectious cause cannot be easily excluded, we treat empirically for infection in
all such patients.
Less common signs or symptoms of leukostasis include ECG signs of
myocardial ischemia or right ventricular overload, worsening renal insufficiency,
priapism, acute limb ischemia, or bowel infarction

DIAGNOSIS
Leukostasis (symptomatic hyperleukocytosis) is diagnosed empirically when a
patient with leukemia and WBC count over 100 x 109/L (100,000 µL) presents
with symptoms thought to be due to tissue hypoxia, most commonly respiratory
or neurological distress.
The diagnosis requires a high degree of suspicion, and some patients have
pathologically proven leukostasis at WBC counts below this level.
Pathologically, leukostasis is diagnosed when a biopsy of involved tissue
demonstrates white cell plugs in the microvasculature. 850
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A pathologic diagnosis of leukostasis is rarely obtained because of the risks


associated with biopsy of affected tissues.

MANAGEMENT
Cytoreduction - can be achieved through the use of chemotherapy
(hydroxyurea or remission induction chemotherapy) or leukapheresis.
The initial management of a patient with hyperleukocytosis is directed at rapid
lowering of the WBC count.
▪ For patients with symptomatic or asymptomatic hyperleukocytosis, we
suggest initial cytoreduction with induction chemotherapy rather
than hydroxyurea or leukapheresis.
▪ For patients with asymptomatic hyperleukocytosis who must have
induction chemotherapy delayed, we suggest cytoreduction
with hydroxyurea rather than leukapheresis
▪ For patients with symptoms of leukostasis who must have induction
chemotherapy delayed, we suggest initial leukapheresis in addition
to hydroxyurea (if possible) to lower or stabilize the WBC count.
Supportive care measures:
▪ Red blood cell transfusions should be withheld, if possible, until the blast
count is reduced. If a transfusion is necessary, it should be administered
slowly.
▪ Most patients with hyperleukocytosis are candidates for tumor lysis
syndrome prophylaxis with aggressive intravenous hydration
and allopurinol or rasburicase to decrease serum uric acid levels.
▪ Coagulation abnormalities require aggressive treatment with platelet
transfusions and coagulation factors.

15.3.3 Neutropenic fever

It is the development of fever, often with other signs of infection, in a patient


with neutropenia, an abnormally low number of neutrophil granulocytes in the
blood.
Fever → defined as a single oral temperature of ≥38.3°C (101°F) or a
temperature of ≥38.0°C (100.4°F) sustained over a one-hour period.
Neutropenia — The definition of neutropenia varies from institution to institution,
▪ Neutropenia is usually defined as an absolute neutrophil count (ANC)
<1500 cells/µL, and
(𝑷𝑴𝑵𝒔+𝑩𝒂𝒏𝒅𝒔) %
▪ ANC = WBC count X
𝟏𝟎𝟎
• Where;
o ANC = Absolute Neutrophil count
o PMNs= Poly morph nuclear cells (i.e. Neutrophil)

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▪ Severe neutropenia is usually defined as an ANC <500 cells/µL or an


ANC that is expected to decrease to <500 cells/µL over the next 48
hours.
▪ The risk of clinically important infection rises as the neutrophil count falls
below 500 cells/µL and is higher in those with a prolonged duration of
neutropenia (>7 days).
▪ For the purposes of this discussion, we are defining neutropenia as an
ANC <500 cells/µL.
Neutropenic fever syndromes
▪ A number of neutropenic fever syndromes have been described.
▪ The International Immunocompromised Host Society has classified initial
neutropenic fever syndromes into the following three categories:
• Microbiologically documented infection – Neutropenic fever with a
clinical focus of infection and an associated pathogen
• Clinically documented infection – Neutropenic fever with a clinical
focus (eg, cellulitis, pneumonia) but without the isolation of an
associated pathogen
• Unexplained fever – Neutropenic fever with neither a clinical focus
of infection nor an identified pathogen

RISK OF SERIOUS COMPLICATIONS


▪ This risk assessment dictates the approach to therapy, including the
need for inpatient admission, intravenous (IV) antibiotics, and prolonged
hospitalization.
▪ Low-risk patients are defined as those who are expected to be
neutropenic (absolute neutrophil count [ANC] <500 cells/µL) for ≤7 days
and those with no comorbidities or evidence of significant hepatic or
renal dysfunction.
▪ We define high-risk patients as those who are expected to be
neutropenic (ANC <500 cells/microL) for >7 days.
▪ Patients with neutropenic fever who have ongoing comorbidities or
evidence of significant hepatic or renal dysfunction are also considered to
be high risk, regardless of the duration of neutropenia.

Microbiology and other diagnostic testing;


▪ Stool exam
▪ Urine Analysis
▪ Skin → aspirate or biopsy lesions for bacterial and fungal stains and
cultures, and
▪ BAL, AFB
▪ CSF analysis
▪ Imaging
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APPROACHES TO MANAGEMENT
Primary prophylaxis
▪ Involves the administration of an antimicrobial drug to prevent infection in
patients at increased risk.
Secondary prophylaxis
▪ Involves the administration of prophylactic doses of an antimicrobial drug
to prevent recurrent infection
Empiric therapy
▪ In patients with chemotherapy-induced neutropenia, empiric therapy
involves the initiation of therapy at the time of the onset of neutropenic
fever but before a firm diagnosis of infection has been established.
▪ Empiric antimicrobial therapy is a standard part of the management of
neutropenic fever.
Preemptive therapy
▪ Involves the initiation of therapy based upon screening with a sensitive
microbiology assay (eg, antigen detection or molecular assays) in an
attempt to detect the presence of a putative pathogen or early subclinical
infection.
▪ Patients whose infections are detected using a preemptive approach are
treated to avoid progression to invasive disease.
▪ A preemptive approach is sometimes used for antifungal therapy.

The following observations have been made about bacterial infections in


neutropenic patients:
▪ Bacteria are the most frequent infectious causes of neutropenic fever.
▪ Gram-negative bacteria (eg, P. aeruginosa)
▪ S. epidermidis
▪ S. aureus (MRSA)
▪ Fungal pathogens
▪ Viral pathogens

EMPIRIC THERAPY
General principles
▪ Fever in a neutropenic patient is a medical emergency.
▪ Broad-spectrum antibiotics should be given ASAP (within 60 minutes of
triage) and at full doses, adjusted for renal and/or hepatic function.
▪ The diagnostic evaluation should be obtained quickly.
▪ In high-risk patients, antibiotics should be administered IV in a hospital
setting.
▪ Moniter patients frequently with respect to vital signs, performance status
(the clinical burden of the neutropenic fever syndrome), and the ability to
achieve adequate oral intake in the presence of oral or gastrointestinal
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▪ Temporarily holding administration of systemic chemotherapy should be


considered during the management of the sepsis syndrome until the
patient stabilizes.
▪ Attention to fluid and electrolyte management is important given the
dehydrating effects of fever, vomiting, and/or diarrhea.
▪ Urine output of >0.5 mL/kg per hour should be maintained.
Antibiotic options include
▪ Cefepime – 2 g IV TID
▪ Meropenem – 1 g IV TID
▪ Imipenem-cilastatin – 500 mg IV QID
▪ Piperacillin-tazobactam – 4.5 g IV TID to QID; if there is significant
concern for Pseudomonas infection (particularly in those who are severely
ill or were not receiving fluoroquinolone prophylaxis at the time of onset
of illness), 4.5 g IV every 6 QID should be given
▪ Ceftazidime – 2 g IV TID
Other antibiotics (eg, aminoglycosides, fluoroquinolones, and/or vancomycin) may
be added to the initial regimen in patients with complicated presentations such
as,
▪ hypotension and/or mental status changes
▪ focal findings (eg, pneumonia or cellulitis), or
▪ if antimicrobial resistance is suspected or proven.
Vancomycin (or other agents that target gram-positive cocci) is not recommended
as a standard part of the initial regimen but should be added in certain
patients, such as those with suspected catheter-related infection, skin or soft
tissue infection, pneumonia, or hemodynamic instability.

15.3.4 Neutropenic enterocolitis (typhlitis)

➢ Neutropenic enterocolitis is a life-threatening, necrotizing enterocolitis occurring


primarily in neutropenic patients. A.k.a "necrotizing enterocolitis" and "ileocecal
syndrome."
➢ "Typhlitis" (from the Greek word "typhlon," or cecum) describes neutropenic
enterocolitis of the ileocecal region; we prefer the more inclusive term
"neutropenic enterocolitis," since other parts of the small and/or large intestine
are often involved.
➢ The pathogenesis of neutropenic enterocolitis is incompletely understood.
➢ The cecum is usually affected, and the process often extends into the
ascending colon and terminal ileum.
➢ The predilection for the cecum is possibly related to its distensibility and its
diminished vascularization relative to the rest of the colon.
➢ Gross and histologic examinations may reveal bowel wall thickening, discrete or
confluent ulcers, mucosal loss, intramural edema, hemorrhage, and necrosis.
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➢ Pathogens include P. aeruginosa, E.coli, Klebsiella spp, viridans group


streptococci, enterococci, Bacteroides spp, Clostridium spp, and Candida spp

CLINICAL MANIFESTATIONS
➢ Signs and symptoms — Neutropenic enterocolitis must be considered in any
severely neutropenic patient (ANC <500 cells/µL) who presents with fever and
abdominal pain.
➢ The location of abdominal pain depends upon the location of the neutropenic
colitis and is often in the right lower quadrant.
➢ Symptoms, including fever, frequently appear during the third week (median 17
days) after receiving cytotoxic chemotherapy, at a time when neutropenia is
most profound.
➢ Additional symptoms may include abdominal distension, cramping, tenderness,
nausea, vomiting, watery or bloody diarrhea, and frank hematochezia.
➢ Paralytic ileus may occur but is uncommon.
➢ Peritoneal signs and shock suggest the possibility of bowel wall perforation.
➢ Stomatitis and pharyngitis, suggesting the presence of widespread mucositis,
may be present.
➢ Patients may remain febrile until recovery from neutropenia, independent of
antimicrobial therapy.
➢ Patients developing neutropenic enterocolitis during chemotherapy are prone to
develop this complication again during subsequent treatments.

DIAGNOSIS;
➢ Abdominal CT
▪ Bowel wall thickening (100 %)
▪ Mesenteric stranding (51 %)
▪ Bowel dilatation (38 %)
▪ Mucosal enhancement (28 %) and
▪ Pneumatosis (21 %).
➢ Abdominal U/S or X-ray
➢ Blood and stool cultures and
➢ C. difficile toxin assays

TREATMENT
➢ Nonsurgical management → in those patients without complicated neutropenic
enterocolitis (i.e., perforation or severe bleeding)
▪ Broad-spectrum antimicrobials → agents that are active
against Pseudomonas aeruginosa, Escherichia coli, other enteric gram-
negative bacilli, and anaerobes.
• Piperacillin-tazobactam, 4.5 g IV QID


Cefepime plus metronidazole 2 g IV TID
Ceftazidime plus metronidazole 2 g IV TID 855
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• An antipseudomonal carbapenem (imipenem or meropenem) →


Reserved for patients who are allergic to the other options or who
are infected or colonized with an organism that is resistant to the
other recommended agents (eg, extended-spectrum beta-
lactamase–producing Enterobacteriaceae).
▪ An antifungal agent
• Should be started in neutropenic patients with protracted fever (>72
hours) despite broad-spectrum antibiotics.
• Examples
o echinocandin for Candida species and
o voriconazole or amphotericin B formulations for both yeasts
and molds.
▪ Bowel rest
▪ Nasogastric suction,
▪ Intravenous fluids
▪ Nutritional support, and
▪ Blood product support (packed RBC and fresh frozen plasma as
needed).
Surgical intervention → for those with free perforation or another process that
cannot be controlled medically (eg, persistent bleeding despite correction of
coagulopathy and cytopenias).

PROGNOSIS
➢ Initial reports of patients with neutropenic enterocolitis described mortality rates
between of ≥ 50 %.
➢ Most deaths are attributed to transmural bowel necrosis, perforation, and
sepsis.
➢ More recently, early recognition and progress in management have reduced
mortality substantially, although no large series have been published.

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Chapter 16; Case reporting format for bedside,


round, exam and case discussion
Dr. Mulualem. G,

➢ This is a case report of CLD patient from my clinical year attachment bedside
case at UOG Hospital.

History

Identification

➢ This is Ato Meazaw wubie, a 56 years old, male, married, orthodox Christian,
farmer, from Tach armachiho woreda, north Gondar zone, admitted to
University of Gondar hospital, department of Internal medicine, Medical ward D,
bed no #27 on Tikimt 24/2010 E.C.

Previous Admission

➢ None
➢ If there is previous admission which is unrelated to the current illness, you can
document like these; E.g. 2003 E.C, TASH, Addis Ababa, HIV-associated
cerebral toxoplasmosis, admitted for 03 months, treated with ART drugs and
anti-toxoplasmosis drugs and discharged improved.

Chief compliant

➢ Abdominal distension of 03 months duration

HPI
This patient was last relatively healthy 03 months back, at which time he noticed
Abdominal distension which initially started from RLQ, which gradually increase in
size and progress to involve the whole abdomen and lower extremities within one
month duration. Together with dragging sensation in the left upper abdomen,
sense of fullness and early satiety.

04 months before the onset of abdominal distension, he experienced a stabbing


RUQ abdominal pain which is moderate in severity and radiates to the back
associated with low grade intermittent fever, coca colored urine and his families
accidentally noticed yellowish discoloration of his eyes but no stool color change
or itching sensation.

He has also unquantified but significant weight loss to the extent his trousers
become loose, loss of appetite and easy fatigability.

For these, he visited a traditional healer where he was given unspecified herbal
medication and cauterized at his arms, forearms, over the abdomen and back but
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he didn’t get any relief. Finally, he came to our hospital for better investigation
and management.

➢ He drinks traditional areki half bottle 2 - 3 times per week for 5 years
and then changed his drink to a beer of 10 to 15 bottles every
Tuesday, Saturday and Sunday (average 37 bottles per week) for the
past 8 years that means he drinks for a total of 13 years. which is
estimated to be 70g alcohol intake daily for 13 years.
➢ No hx of blood transfusion, tattooing, contact with a jaundiced patient, IV drug
abuse or MSP
➢ No hx of drug intake other than mentioned above
➢ No family hx of similar illness
➢ He usually eats injera made of ‘‘teff’’ and ‘‘machilla’’ and ‘’wott’’ made of
‘‘atter’’ and ‘‘dagusa’’ 3-4 times per day. Occasionally he eats meat during
holidays
➢ He has coca colored discoloration of urine but no pain during urination,
urgency, frequency or flank pain
➢ No hx of nasal bleeding, bloody vomiting or melena
➢ He has easy fatigability but no hx of tinnitus, blurring of vision or light
headedness
➢ No hx of sleep disturbance, confusion, Forgetfulness, Abnormal body movement
or LOC
➢ Has hx of river water contact but no hx of post river water contact itching
➢ No hx of dyspnea, orthopnea, PND or palpitation
➢ No hx of chronic cough, contact with chronic cougher or previous TB treatment
➢ No self/family hx of DM, HTN or asthma
➢ He was screened for RVI 2 months back and found to be NR.

Finally, he was admitted to our hospital supported physically by his families

Past illnesses

➢ No history of childhood illnesses like chicken pox, mumps or small pox. Not
vaccinated.
➢ No history of previous surgery, trauma, psychiatry problems or drug allergy.

Review of system /ROS

H.E.E.N.T
▪ Head: No history of headache or head injury
▪ Eyes: No history of blurring of vision, pain in the eyes, eye itching, or
spontaneous
lacrimation
▪ Ears: No history of Earache, difficulty of hearing, ear discharge, vertigo
or tinnitus
▪ Nose: No history of nasal bleeding or discharge
▪ Mouth and throat: No history of gum bleeding, tooth extraction 858
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LGS: No history of swelling in the neck, axilla or groin, No history of heat or


cold intolerance.
RS; No history of cough, chest pain or fast breathing
CVS: Mentioned on HPI
GIS; Mentioned on HPI
GUS: Mentioned on HPI
IGS: No history of skin rash or ulcers
MSS: No history of loss of limb function, joint pain swelling over the
extremities or deformity.
CNS: No hx of weakness of extremities. See HPI

Personal History

➢ He was born and raised in Tach armachiho in 1954 E.C, where he lived all
his life. He had a healthy childhood and was an active boy who liked helping
his father around the farm. He didn’t attend formal education but he is able to
read and write.
➢ He is a farmer and also raises cattle, sheep and goat. He claims his income
is enough to support the family.
➢ He has 4 boys and one daughter. All are alive and healthy.

Family History

➢ Both his father and mother are dead. His father died while he was child at
unknown age by unknown cause while his mother died 5 years ago at age 69
by natural cause.
➢ He has two sisters and one brother. All are alive & well.
➢ No family history of DM, hypertension, Asthma, tuberculosis, allergy or sudden
deaths.

Physical examination

General Appearance

➢ conscious & cooperative, chronically sick looking, not in cardiopulmonary stress,


looks well nourished

Vital signs

➢ BP: 110/70mmHg, right arm, sitting position → normotensive


➢ PR:95 beat per minute/bpm, at right radial artery, regular & full volume →
normal
➢ RR: 18 breath/min, shallow & regular → normal
➢ T0: 36.20c, at axillary, at 8:00 DLT
➢ MUAC: 24 cm
➢ BMI: not done (since he has ascites)

H.E.E.N.T
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➢ Head: Normal male type hair distribution, No visible scar over the scalp or
tenderness
➢ Ears: Normal contour of pinna, Clear external ear canal, No mastoid or tragus
tenderness
➢ Eyes: Icteric sclera, Pink conjunctivae, No periorbital edema
➢ Nose: central nasal septum. There is no polyp or active discharge
➢ Mouse and throat: No fissure or ulceration on the lip, the gums are intact, no
active bleeding. There are no carious teeth, extraction, dentures or filling. no
atrophied papillae of tongue, the buccal mucosa is pink & wet.

Lymphoglandular system (LGS)

➢ There is no significantly enlarged lymphadenopathy in peripherally accessible


lymph node areas
➢ The thyroid gland is not enlarged
➢ There is no breast lump (gynecomastia)
➢ No parotid gland enlargement
➢ No testicular atrophy

Respiratory System (RS)

Inspection
▪ There is grade II clubbing of fingers, but no central or peripheral
cyanosis
▪ Symmetric chest wall that moves with respiration
▪ No chest wall deformity
▪ No subcostal or intercostal retraction
▪ No use of accessory muscles of respiration\
▪ Shallow and regular breathing pattern
Palpation
▪ There is no chest wall tenderness or subcutaneous emphysema
▪ Centrally located trachea
▪ Comparable tactile fremitus bilaterally
▪ Symmetrically normal chest expansion bilaterally which slides 5cm by
measuring tape method.
Percussion
▪ Resonant percussion note all over the lung field
▪ There is no dullness
▪ diaphragmatic excursion = 5cm bilaterally
Auscultation
▪ Vesicular breath sound all over the lung field
▪ No added respiratory sound
▪ Comparably normal air entry bilaterally

Cardiovascular system (CVS)

Arterial examination
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▪ All accessible peripheral arteries are palpable, full in volume and regular
in rhythm
Venous examination
▪ No distended neck veins
▪ JVP = 3cm
Precordial Examination
▪ Inspection
• Active precordium
• AI @5th ICS medial to left MCL
• No precordial buldge or scar
▪ Palpation
• Palpable heart sounds
• PMI @5th ICS medial to left MCL which is Localized, tapping and
non-sustained
• No heave or thrill
▪ Auscultation
• S1 & S2 are well heard
• No murmur or gallop

Abdominal examination

Inspection
▪ Grossly / Symmetrically distended abdomen
▪ Flanks are full
▪ Everted umbilicus with circular slit
▪ superficially distended and tortuous abdominal vessels which drain away
from umbilicus during palpation
▪ No visible scar, straie, pigmentation or peristalsis
▪ Hernia sites are free
Auscultation
▪ Normoactive bowel sounds (18 kicks/min)
▪ No bruit over abdominal aorta, renal arteries, iliac arteries, liver or spleen
Palpation
▪ Superficial palpation
• No superficial tenderness
• No superficially palpable mass
▪ Deep palpation
• Enlarged/ ballotable mass over the LUQ which is 13 cm from left
costal margin along the splenic growth line, non-tender, firm in
consistency, smooth surface, sharp edge, Palpable medial notch,
doesn’t allow finger to pass below left costal margin, Moves with
respiration, Not bimanually palpable
• No direct/rebound tenderness, guarding or rigidity
• Liver is not palpable
• kidney is not bimanually palpable bilaterally.
Percussion
▪ Tympanic percussion note except the flanks (i.e. dullness over the flanks) 861
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▪ There is shifting dullness of 2cm but no fluid thrill


▪ TVLS = 10cm along MCL

Genitourinary System (GUS)

No costo-vertebral angle tenderness (CVAT)

Integumentary System (IS)

No spider angioma or spider nevi


No palmar erythema, palmar or plantar pallor
No skin or nail pigmentation
No bruising or purpura
No axillary or pubic hair loss
No scratch marks

N.B. these finding are pertinent negative for CLD, in other cases you can report
like these;

➢ No palmar or plantar pallor


➢ No rash, scar or ulcer

Musculoskeletal System

Look; there is leg swelling but no deformity


Feel; There is grade II pedal and pretibial pitting edema, no tenderness
Move; intact active and passive range of movement in all extremities
Measure; comparable circumference and length of extremities

Nervous system

Level of consciousness
▪ GCS = 15/15 (E4V5M6), conscious and alert
CN examination
▪ CN-I: He can smell soap via each nostril.
▪ CN-II:
• He can differentiate 2 fingers at about 6 meters. (Visual Acuity)
• He sees waggling of finger approximately 1000 from axis of eye.
(Visual Fields)
• He differentiates green and red colours. (Colour Appreciation)
• Normal direct and consensual pupillary light reflex
▪ CN-III, IV & VI:
• The eyes can move in all directions. There is no nystagmus or
diplopia. The pupils are round, regular in outline and equal in size.
They react to light directly and consensually.
▪ CN-V:
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• He identifies light touch and pin prick over the mandibular,


maxillary and ophthalmic areas of the face.
• He closes his eyes at the touch of the cornea with a cotton swab.
• Contraction of the temporal and masseter muscles is symmetrical
and strong while clenching his teeth.
▪ CN-VII:
• The face is symmetrical at rest and during voluntary movements
(smiling, frowning).
• He can smile, frown his forehead, puff out his cheeks
• can close both eyes equally and forcefully against resistance.
• Intact nasolabial fold
• Intact corneal reflex
▪ CN-VIII:
• He can hear rubbing of the fingers on both ears.
▪ CN-IX & X:
• The soft palate rises in the midline when saying ‘ah!
• Centrally located uvula
• He can swallow his saliva
▪ CN-XI:
• The Sternocleidomastoid and trapezius muscles contract on turning
the head and on shrugging the shoulder against resistance,
respectively
▪ CN-XII:
• The tongue protrudes in the midline and shows no fasciculation or
atrophy.
Motor examination
▪ Inspection
• The limbs are centrally positioned, no inward or outward rotation
• Comparable muscle bulk between the left and the right side of
both upper and lower extremities.
• There is no spontaneous as well as induced fasciculation.
▪ Palpation
• Tone and power

TONE POWER
Upper Lower Upper Lower
Right Normo- Normo-tonic 5/5 5/5
tonic
Left Normo- Normo-tonic 5/5 5/5
tonic

• Reflexes
o Superficial
✓ Abdominal reflex is present both in upper and lower
quadrants.
✓ Corneal reflex is intact in both eyes.
✓ Plantar reflex is down going on both sides.
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o DTR

Biceps Triceps Brachioradialis Patellar Ankle


Right ++ ++ ++ ++ ++
Left ++ ++ ++ ++ ++

Sensory examination
▪ Primary sensory exam
• He identifies light touch and pin prick over the extremities and
trunk.
• He is able to recognize different movements of the toes with his
eyes closed. (Position sense)
• Vibration sense was not assessed due to lack of Tuning Fork.
▪ Cortical sensory exam
• He appreciates the form of a key by means of only touch
(Stereognosis)
• He recognizes writings of different numbers on his palm
(Graphesthesia)
• He is able to differentiate 2 pin pricks up to 4 mm apart over the
finger tips (2 pt discrimination).
Coordination
▪ Finger to nose, heal to shin and rapid alternating movement of the arm
were done without any abnormalities.
Meningeal irritation signs
▪ No neck stiffness.
▪ Kernig's Sign is negative.
▪ Brudzinski's Sign is negative

Subjective summary

➢ A 56 years old male patient presented with abdominal distension of 3 months


duration associated with dragging sensation in the left upper abdomen, sense
of fullness and early satiety.
➢ 04 months before the onset of abdominal distension, he experienced a
stabbing RUQ abdominal pain, low grade intermittent fever, coca colored urine
and yellowish discoloration of the eyes.
➢ He has also unquantified but significant weight loss, loss of appetite and easy
fatigability.
➢ He has history of herbal medication intake and chronic alcohol intake for the
past 13th years.

Objective summary
➢ conscious & cooperative, chronically sick looking, not in cardiopulmonary stress,
looks well nourished
➢ BP: 110/70mmHg
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➢ PR: 95 bpm
➢ RR: 18 breath/min
➢ T0: 36.20c
➢ He has
▪ Icteric sclera
▪ grade II clubbing of fingers
▪ Grossly distended abdomen
▪ Flank fullness
▪ Everted umbilicus with circular slit
▪ superficially distended and tortuous abdominal vessels which drain away
from umbilicus during palpation
▪ shifting dullness of 2cm
▪ flank dullness
▪ Ballotable mass over the LUQ which is 13 cm from left costal margin
along the splenic growth line, non-tender, firm in consistency, smooth
surface, sharp edge, Palpable medial notch, doesn’t allow finger to pass
below left costal margin, Moves with respiration, Not bimanually palpable
→ marked splenomegaly
▪ grade II pedal and pretibial pitting edema

Investigations done

Investigation Result Interpretation


CBC WBC = 6.6 x 103 Moderate anaemia
Neut = 85.8 % Thrombocytopenia
Lymph = 9.9 %
HGB = 9.1 mg/dl
HCT = 27.1 mg/dl
PLT = 111 x 103
MCV = 88.3
MCH = 29.6
MCHC = 33.6
U/A WBC = 2/HPF Non revealing
PH = 6.0
SPG = 1.010
Protein = +1
Others = neg
Liver enzymes SGOT = 58 (1.4 X UNL*) Normal
SGPT = 30
LFT Albumin = 3.6 g/dl Low
Total protein = 5.1 g/dl
Ascetic fluid Cell count = 150/mm3, Neut = 80%, Lymph = 10.1% Normal
analysis Glucose = 53 mg/dl
Protein = 8mg/dl
AFB = neg
Gram stain = neg

PM
Serum
Culture = no organism identified
NcNc
NA+ = 142.8 Normal
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electrolytes K+ = 3.53
Cl- = 103
PICT NR
RBS 156mg/dl Normal
RFT Creatinine = 0.54 Normal
Urea = 12
* UNL = Upper normal limit

Recommended Investigations to be done

A) HBsAg
B) Direct and total bilirubin
C) Abdominal U/S
D) Echo

DDX from most likely to list likely

i. Chronic liver disease (CLD)


ii. Right sided heart failure
iii. Chronic constrictive pericarditis
iv. Nephrotic syndrome

Discussion on differentials from least likely to most likely

Nephrotic syndrome (NS)

Definition;
Etiology; write from the corresponding topics of nitsbin above,
Pathophysiology; Harrison and uptodate (this is for other DDX also)
Epidemiology;
Clinical features;

Conclusion;
This patient has ascites with grade II pedal and pretibial edema, easy fatigability
and loss of appetite which support nephrotic syndrome. But stabbing RUQ
abdominal pain jaundice and the pattern of edema can’t be explained by NS. For
the diagnosis of NS, Nephrotic range proteinuria and Serum albumin concentration
< 3 g/dL are used. But this patient has only protein +1 and serum albumin of
3.6g/dl which doesn’t support NS. Epidemiologically, unlike children, NS is not
common in adults. So, nephrotic syndrome as a diagnosis is unlikely for this case.

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Chronic constrictive pericarditis

Conclusion;
This patient has ascites with grade II pedal and pretibial edema, easy fatigability
and weight loss which goes with constrictive pericarditis. The absence of
retrosternal chest pain, elevated JVP, tender hepatomegaly and pericardial friction
rub goes against constrictive pericarditis. In developing world infectious (especially
TB) is the most common cause of constrictive pericarditis. This patient has no hx
of contact or TB infection and from ascitic fluid analysis AFB is negative which
may help us to r/o constrictive pericarditis. So, constrictive pericarditis as a
diagnosis is less likely for this case.

Right sided heart failure (RSHF)


Conclusion;
This patient has ascites with grade II pedal and pretibial edema, easy fatigability,
weight loss and splenomegaly which goes with RSHF. The absence of elevated
JVP, tender hepatomegaly goes against RSHF. RSHF is usually from left sided
heart failure (LSHF) and Isolated RSHF is cor pulmonale. This patient has no hx
of LSHF or cor pulmonale which may help us to r/o RSHF. So, right sided heart
failure as a diagnosis is less likely for this case. But I strongly recommend
Echocardiography for this patient.

Chronic liver disease (CLD)

Conclusion;
This patient has Ascites, leg edema and splenomegaly which can be explained by
Portal Hypertension secondary to decompensated CLD.

04 months before the onset of abdominal distension, he also experienced a


stabbing RUQ abdominal pain, low grade intermittent fever, coca colored urine and
yellowish discoloration of the eyes, which suggest there was hepatitis which end
up with cirrhosis.

He has history of chronic alcohol intake for the past 13th years which strongly
suggest alcoholic liver disease.

Grade II clubbing, icteric sclera can be explained by peripheral stigmata of CLD.


Investigation wise the presence of anemia, thrombocytopenia and hypoalbuminemia
suggest lifer synesthetic dysfunction. So, CLD is the most likely diagnosis for this
case

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Final assessment

Decompensated CLD (evidenced by ascites + Splenomegaly


2ry to portal HTN) secondary to Alcoholic Liver disease r/o
Chronic viral hepatitis

References

➢ Harrison’s principle of internal medicine 21st edition


➢ UpToDate, © 2018, version 2.0

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Part II; Short cases

Part II
Part II; Short cases
Short cases

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Chapter 1; Physical examination

Chapter 1; Physical examination


Dr. Mulualem. G

Tips for short exams


☛ You are going to be asked by your senior to do one system examination (e.g do
posterior chest exam, do precordial examination, show me lower motor
examination)
☛ During exams you are evaluated not only with your scientific background but also
with, your confidence, skill of examination and ability to pick up findings, patient
approach (like introducing yourself and greeting)
☛ After completing the examination, you are expected to
✓ Conclude your physical findings (for example; after doing from inspection
to auscultation of posterior chest examination, your conclusion may be
pleural effusion)
✓ List down possible DDX of your findings from cmn to less cmn in order
✓ Investigation for your Top DDX
✓ Mgt principle for your Top DDX

1.1 Respiratory System

You may be asked the following in RS examination


☛ Do posterior chest examination → most cmnly asked
☛ Do anterior chest examination
☛ Do respiratory system examination

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1.1.1 Physical examination findings

N.B normal RR = 8 - 22 BPM

Examination techniques Possible abnormal findings and their causes


❖ Cyanosis and ☛ Clubbing
clubbing ✓ Grading
❖ Symmetry 1. Sponginess or softening of nail fold
❖ Shape (chest wall 2. Obliteration of hyponychial angle (nail fold ≥ 1800)
deformity) 3. Curvature (convexity) → like bird’s peak
❖ Subcostal or 4. Biconvexity (drum steak appearance)
intercostal retraction, 5. Associated arthropathy
use of accessory ✓ Causes of clubbing
muscles of respiration Respiratory system→ ABCDE CVS GIT → 4C’s
❖ Breathing pattern A. Lung Abscess 1. IE 1. Cirrhosis
✓ Shallow and B. Bronchiectasis 2. Cyanotic 2. Cancer (GI
regular or not C. Cancer (Bronchogenic CHD (PDA, lymphoma)
ca, mesothelial ca or TOF) 3. IBD (CD)
metastasis to lung) 4. Coeliac
D. Desaturation (hypoxia) disease
E. Empyema → TB
F. Fibrosing alveolitis
(cystic fibrosis)

In a normal finger, the length of the perpendicular


dropped from point A to point B should be
greater than a similar line from C to D. In
clubbing, the relationships are reversed – that is,
the distance C-D is greater than the distance A-
B. The other important change is the angle
described by A-C-E. In the normal finger this is
Inspection (5 S)

usually <180 degrees, whereas in clubbing it is


>180 degrees.

☛ Respiratory distress signs


✓ Tachypnoea
✓ Flaring of the alanasae
✓ Use of accessory muscles of respiration
❖ Sternomastoid muscle
❖ Strap muscles (sternothyroid, sternohyoid, thyrohyoid)
❖ platysma
✓ Sub clavicular, subcostal or intercostal retraction
☛ Chest lag/delay
✓ Ipsilateral
Pleural effusion
Pneumothorax
Consolidation
Atelectasis
fibrosis
✓ bilateral
Emphysema
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ILD
Bilateral fibrotic lung
☛ Abnormal breathing patterns → causing examples
✓ Tachypnia → severe pneumonia, decreased CO
✓ Bradypnea → barbiturate poisoning
✓ Paradoxical breathing → diaphragmatic paralysis
✓ Kussmauls breathing (deep, labored, fast breathing followed by apnoea)
→ Metabolic acidosis (DKA, ureamic encephalopathy, hepatic
encephalopathy)
✓ Chyne stokes breathing → CHF, stroke
✓ Apneustic breathing → pontine damage
✓ Ataxic breathing → medullary compression (trans tentorial herniation)
☛ Chest wall deformities → causing examples
✓ Barrel chest → COPD (emphysema), Chronic asthma, aging
✓ Pectus excavatum (funnel chest)
✓ Pectus carinatum (pigeon chest)
✓ Kyphosis
✓ Scoliosis
✓ Kyphoscoliosis →idiopathic, rickets, severe childhood asthma

Reporting format for normal chest inspection finding


☛ There is no central or peripheral cyanosis or clubbing, symmetric chest wall that moves with respiration,
no chest wall deformity, no subcostal or intercostal retraction, no use of accessory muscles of
respiration, shallow and regular breathing pattern

Tenderness and ❖ Chest wall tenderness → rib fracture


Palpation (4T)

subcutaneous ❖ Subcutaneous emphysema → pneumothorax


emphysema ❖ Tracheal deviation
Tracheal location and Away from the lesion Towards the lesion
tracheal tug (normally ➢ Massive pleural effusion ➢ Upper lobe
trachea slightly ➢ Pneumothorax fibrosis
deviate to the right ➢ Mediastinal mass ➢ Atelectasis
side) N.B 4T’s of mediastinal mass ➢ Pneumonectom
Tactile fremitus Terrible lymphoma (NHL is cmn) y
Chest expansion Thyroid mass (retrosternal extension of
(normal = 4 -6cm) thyroid mass)
✓ Tape method Teratoma
✓ Hand grip Thymoma
method ➢ COPD

❖ Tracheal tug → COPD


❖ Increased tactile fremitus → consolidation
❖ Decreased chest expansion
Ipsilaterally (over the affected Bilaterally
side of lung)
Pleural effusion Emphysema
Pneumothorax ILD
Consolidation Bilateral fibrotic lung
Atelectasis
fibrosis

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Reporting format for normal chest palpation finding


☛ There is no chest wall tenderness or subcutaneous emphysema, centrally located trachea, comparable
tactile fremitus bilaterally, symmetrically normal chest expansion bilaterally which slides 5cm by
measuring tape method.
➢ Percussion note ➢ Dullness to percussion
✓ Relative dullness → consolidation
Normal = resonant ✓ Stony (absolute) dullness → pleural effusion, hemothorax, empyema
➢ Diaphragmatic ➢ Hyper resonant percussion note → emphysema, pneumothorax
excurtion ➢ Diaphragmatic excursion decreases ipsilaterally in
Percussion

✓ normal = 5 - ✓ Pleural effusion


6 cm ✓ Pneumothorax
N.B. you can’t do ✓ Fibrosis
diaphragmatic excursion ✓ Atelectasis
in
☛ if there is dullness
☛ tender chest wall
☛ respiratory distress
and patient with O2
☛ if patient is not
cooperative (e.g.
coma)
Reporting format for normal chest percussion finding
☛ Resonant percussion note all over the lung field, there is no dullness, diaphragmatic excursion = 5cm
bilaterally
☛ Breath sound ➢ Bronchial breath sound
✓ Vesicular → ✓ Consolidation
normal ✓ On top of pleural effusion
✓ Broncho ✓ Fibrosis
vesicular ➢ Added respiratory sounds
✓ Bronchial ✓ Crackles
✓ Tracheal Fine crackles (rales) coarse crackles (crepitation)
☛ Added respiratory Pulmonary Consolidation
sounds edema TB
☛ Air entry (bilateral basal COPD
rales)
Bronchiectasis
Fibrosing
akveolitis
Auscultation

✓ Wheeze →Bronchial asthma, COPD, bronchiectasis, foreign body


obstruction (unilateral wheeze), hilar LAP of TB, cardiac asthma (pulmonary
edema from CHF→ have basal rales with wheeze), tracheal fibrosis
✓ Rhonchi → usually over the bronchi (i.e. large airways), COPD
✓ Pleural friction rub → pleurisy from TB/ pneumonia, pulmonary infarction
✓ Transmitted voice sounds (vocal resonance) → heard clearly in
consolidation
Aegophony
Bronchophony
Whispering pectoriloeqy
➢ Airy entry
✓ Decreased/ absent → pleural effusion, pneumothorax, atelectasis, pleural
thickening
✓ Increased → consolidation
✓ Decreased → COPD
Reporting format for normal chest auscultation finding
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1.1.2 pleural effusion

Findings DDX IX Mgt


principle
✓ Trachea Transudative Exudative 1. Pleural fluid analysis → refer ✓ Put on
deviated nitsibin under pleural tap intranasal O2
1. CHF 1) Pneumonia with
away from a 2. CBC if saturation is
2. Constrictive Parapneumonic
massive 3. CXR < 90%
pericarditis effusion
effusion ✓ May not be visible if the ✓ Therapeutic
3. Nephrotic 2) Disseminated
✓ Decreased amount is <250 ml tap for huge
syndrome TB to lung and
tactile ✓ Blunted/ obliterated effusion
4. CLD (cirrhosis) pleura
fremitus costophrenic angle ✓ Chest
5. Hypothyroidism 3) Lymphoma
✓ Ipsilateral ✓ Radio-opaque density decompression
6. Meig‘s (primary effusive
extending from the base
chest lag lymphoma) ▪ Chest
syndrome ✓ Meniscus sign at upper
(reduced 4) lung cancer tube
chest surface insertion
(bronchogenic,
expansion) ✓ Mediastinal shift away from ▪ Large
mesothelioma or
✓ Stony the effusion → if huge bore
metastasis to
dullness effusion needle
lung)
✓ Absent air 5) Pulmonary insertion
entry 4. Chest U/S ✓ Antibiotics
infarction
✓ BBS Above ✓ Identify loculated effusion ✓ Management
6) Connective
the effusion ✓ differentiate fluid from fibrosis of the
tissue diseases
(not always) ✓ identification of thoracentesis underlying
(SLE)
✓ Pleural site cause
7) Traumatic
friction rub 5. Chest CT
effusion
✓ Aids in differentiation of
8) Acute ❖ Consolidation vs effusion
pancreatitis ❖ Cystic vs solid lesions
❖ Peripheral lung abscess vs
loculated empyema
✓ Aids in identification of
❖ Necrotic areas
❖ Pleural thickening, nodules,
masses
❖ Extent of tumour
6. Pleural Biopsy → diagnostic
for pleural TB
7. U/A → for NS screening
8. Serum albumin level
9. LFT → if you suspect CLD
10. ECG and Echo → if you suspect
CHF
11. TFT → if you suspect
hypothyroidism

Reporting format of pleural effusion


❖ Inspection
❖ Palpation
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Centrally located trachea, tactile fremitus decreased over the posterior lower 1/3 rd of right/left chest, decreased
chest expansion over the right side by hand grip method
❖ Percussion
Stony dullness over the posterior lower 1/3rd of right/left chest
❖ Auscultation
Absent air entry over the posterior lower 1/3rd of right/left chest

1.1.3 Consolidation

Findings DDX IX Mgt


principle
Ipsilateral chest lag Pneumonia CXR ✓ Put on
Increased tactile fremitus TB → apical ✓ Consolidation → intranasal O2
Relative dullness consolidation silhouetting sign, Air if saturation is
Auscultation findings Above pleural bronchograms < 90%
❖ Course crepitation ✓ Parapneumonic effusion ✓ Antibiotics
effusion
❖ BBS ✓ Lung abscess ✓ Management
❖ Pleural friction rub pulmonary ESR → elevated especially of the
❖ Vocal resonance haemorrhage in TB and pneumonia underlying
▪ Aegophony ARDS CBC cause
▪ Bronchophony Pulmonary ✓ leucocytosis
▪ Whispering pectoriloquy IX based on the suspected
edema
case → e.g TB work up
Aspiration
Lung abscess
Bronchiectasis
Neoplasm
(Bronchogenic
ca)
Pulmonary
infarction
Reporting format of consolidation
❖ Inspection
❖ Palpation
Centrally located trachea, tactile fremitus increased over the posterior lower 1/3 rd of right/left chest, decreased
chest expansion over the right/left side by hand grip method
❖ Percussion
relative dullness over the posterior lower 1/3rd of right/left chest
❖ Auscultation
Coarse crepitation (± BBS → it needs experienced examination) over the posterior lower 1/3 rd of right/left chest

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1.1.4 Pulmonary edema

Findings DDX IX Mgt principle


Tachypnea Cardiogenic CXR O2
Cardiorespiratory ✓ CHF ✓ bat wing Strong analgesics like morphine
distress ✓ Hypertensive appearance Lasix
Desaturation emergencies ✓ cephalization If no response to diuretics use
High/normal BP ✓ ACS (Diversion of vasodilators like Nitroglycerine.
Bilateral basal rales ✓ Arrythmia like Blood vessel
Relative dullness AF circulation towards N.B.
Decreased air entry Non cardiogenic the Early oxygenation and
Wheeze ✓ ARDS Apex) ventilation support is life saving
Raised JVP ✓ high altitude ✓ Kerl B lines Treatable precipitating causes
S3 gallop ✓ neurogenic IX for the (eg. Arrhythmia, hypertensive
pulmonary underlying cause crisis, ACS)
edema ✓ RBS → DKA
✓ ECG & ECHO → For more refer Pulmonary edema under
✓ DKA CHF from long case of nitsbin (click here →
CHF
✓ Pulmonary 1.10.2 Pulmonary edema)
Other CHF work
embolism up
✓ Eclampsia
✓ Transfusion-
related acute
lung injury
(TRALI).
✓ Opioid
overdose
Reporting format of pulmonary edema
❖ Inspection
There is subcostal and intercostal retraction, use of accessory muscles and flaring of alanasae
❖ Palpation
CVS→ bilaterally distended neck veins, JVP is 5cm above the heart level (raised),
❖ Percussion
relative dullness over the posterior lower 1/3rd of chest bilaterally
❖ Auscultation
Bilateral basal rales over the posterior lower 1/3rd of chest
Decreased air entry over the posterior lower 1/3rd of chest bilaterally

CVS → there is S3 gallop.

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1.1.5 Pneumothorax

Findings DDX IX Mgt


principle
✓ Trachea deviated away Spontaneous Traumatic 1. CXR ✓ Put on
from pneumothorax Hypo dense intranasal O2
1. Emphysema 1) penetrating
✓ Decreased tactile fremitus (extremely dark) on if saturation is
→with chest injury
✓ Ipsilateral chest lag the affected side < 90%
rupture of 2) rib fracture
(reduced chest expansion) Mediastinum shift to ✓ Immediate
bullae 3) Iatrogenic
✓ Subcutaneous emphysema opposite side chest
2. Pulmonary ✓ During
✓ Decreased tactile fremitus Tracheal shift to decompressio
TB Pleural or
✓ Hyper resonant to opposite side n
3. Rarely pericardial
percussion Visceral pleural edge ▪ Chest
Bronchial aspiration
✓ Absent air entry is visible tube
asthma and ✓ During
If there is tension Absent broncho insertion
lung central
pneumothorax vascular markings ▪ Large
abscess venous
▪ Cyanosis peripherally bore
catheterizatio
▪ Tachypnoea Loss of lung volume needle
n
▪ Hypotension on the affected side insertion
2. Pulmonary function ✓ Management
test of the
3. Other Baseline IX underlying
4. IX based on the cause
underlying cause
Reporting format of pneumothorax
❖ Inspection
❖ Palpation
Trachea deviated to the opposite side, tactile fremitus decreased over the posterior right/left chest, decreased
chest expansion over the right/left side by hand grip method
❖ Percussion
Hyper resonant to percussion over the posterior right/left chest
❖ Auscultation
Absent air entry over the posterior right/left chest

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1.1.6 Pulmonary fibrosis

Findings DDX IX Mgt


principle
Cyanosis Upper lobe; S2CHA2RT Lower lobe; RASCO ✓ Refer Refer
Clubbing long long
Trachea shifts Silicosis Rheumatoid arthritis (RA) case of case of
Sarcoidosis Asbestosis
towards the nitsibin nitsibin
Coal-worker’s Scleroderma
lesion in upper → IX of → mgt
lobe fibrosis pneumoconiosis Cryptogenic fibrosing alveolitis ILD of ILD
Histoplasmosis Others: drugs-
Decreased
Ankylosing spondylitis ✓ busulphan,
chest
expansion Allergic broncho- ✓ bleomycin,
pulmonary aspergillosis ✓ methotrexate,
ipsilaterally
Radiation ✓ hydralazine,
Fine crackles
Tuberculosis ✓ amiodarone
→Tuberculous Empyema
Reporting format of pulmonary fibrosis
❖ Inspection
There is central and peripheral cyanosis, there is grade II clubbing of fingers
❖ Palpation
Trachea deviated to the same side of lesion (please say right or left based on your finding), decreased chest expansion
over the right/left side by hand grip method
❖ Percussion
❖ Auscultation
Fine crackles over the posterior right/left chest

1.1.7 lung collapse (Atelectasis)

Findings DDX IX Mgt


principle
Trachea - deviates Obstruction (resorption) CXR ✓ Put on
towards the collapsed ✓ Mucous obstruction → cmn cause ✓ Direct signs intranasa
lung ▪ Bronchial asthma ▪ Displacement of l O2 if
▪ Due to ▪ Bronchiectasis interlobular fissure saturatio
compensatory ▪ COPD (chronic bronchitis) ▪ Loss of aeration of n is <
hyperinflation on ▪ Post-operative obstruction the lung 90%
the opposite lung ✓ Tumours or mass ▪ Vascular and Manage
Reduced chest ▪ Bronchogenic ca bronchial ment of
expansion ipsilaterally
Relative dullness over
the collapsed lung ✓
▪ Hilar LAP of TB
Compression
Pleural effusion


overcrowding
Indirect signs
Elevation of the
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Decreased/ absent air ✓ Pneumothorax hemidiaphragm


entry with/without BBS ✓ Elevated diaphragm in bed ridden pt ▪ Mediastinal
above the collapse Contraction displacement
✓ Fibrosis of lung or pleura ▪ Hilar displacement
▪ Compensatory
hyperinflation
N.B. CT scan
From the three mechanisms of lung Other Baseline IX
collapse, all are reversible except IX based on the
contraction underlying cause
Reporting format of atelectasis
❖ Inspection
❖ Palpation
Trachea deviated to the same side of lesion (please say right or left based on your finding), decreased chest expansion
over the right/left side by hand grip method
❖ Percussion
There is relative dullness over the posterior right/left chest
❖ Auscultation
Absent air entry over the posterior right/left chest

1.1.8 emphysema
Findings DDX IX Mgt
principle
Respiratory distress (use of accessory muscle of Chronic ✓ Refer long Refer
Respiration, Subcostal or intercostal muscle retraction, bronchitis case of long
tripod positioning) Pneumothorax nitsibin → IX case of
Pink puffers, tilt forward → no more used Bronchiectasis of COPD nitsibin
Pursing of lips → close lips tightly during Post TB fibrosis → mgt
Barrel shaped chest → AP diameter of chest > lateral Refractory of
diameter due to hyperinflation Asthma COPD
Hoover’s sign +ve → paradoxical inward movement of Chest wall
ribcage with respiration deformity
Decreased chest expansion bilaterally ILD(IPF)
hyper resonant percussion note CHF
loss of cardiac and liver dullness → flattening of Lung ca
diaphragm Chronic PTE
poor diaphragmatic excursion → enlarged liver volume Neuromuscular
decreased Air entry bilaterally disorders
coarse crepitation (crackles) and wheeze at lung bases CF
throughout the respiratory cycle
Reporting format of emphysema
❖ Inspection
There is use of accessory muscle of Respiration, Subcostal or intercostal muscle retraction
❖ Palpation
Centrally located Trachea, decreased chest expansion bilaterally by hand grip method
❖ Percussion
Hyper resonant to percussion over the posterior right/left chest
❖ Auscultation
Decreased air entry over the posterior chest bilaterally, coarse crepitation over the posterior chest bilaterally

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1.2 Cardiovascular System

You may be asked the following in CVS examination


☛ Do precordial examination → most cmnly asked
☛ Check for congestion (assess signs of CHF)
☛ Do CVS examination

1.2.1 Physical examination findings

N.B normal PR = 60 – 100 BPM

Examination Possible abnormal findings and their causes


techniques
General ✓ Cardio pulmonary distress
apperance ▪ Distended neck vein
▪ Raised JVP
▪ Diaphoresis and cyanosis
▪ Hyperactive precordium
✓ Cyanosis
✓ Pallor
✓ Clubbing
✓ OHT→ anaemia, autonomic neuropathy (DM, ureamia, RVI), Drugs (vasodilators, diuretics,
BP anti-depressants), endocrine (Addison’s disease, hypopituitarism), idiopathic
✓ Wide pulse pressure (difference b/n SBP and DBP 30-60 normally. If > 60 it is Wide
pulse pressure and if <30 it is narrow pulse pressure) → AR, Anaemia, thyrotoxicosis, AV
malformation, Beriberi, pregnancy, Aging (Isolated systolic HTN is common in old age)
✓ Narrow pulse pressure → AS, Blood loss, cardiac tamponade.
Pulse ✓ Rate abnormalities → normal PR = 60 – 100 BPM
✓ Rate ▪ Tachycardia → in response to hypovolemia (like bleeding), anaemia, pain,
✓ Rhythm infection …
✓ Volume ▪ bradycardia
✓ Characte ✓ volume abnormalities → normally full
r ▪ feeble pulse (very weak) → hypovolemia --
✓ Radio ▪ absent (pulse is not palpable) → shock
femoral ▪ bounding → AR
Arterial examination

delay ✓ Rhythm abnormalities → normally regular


✓ Conditio ▪ Irregularly irregular → AF
n of the ▪ Regularly irregular → ectobic beat
vessel ✓ Pulse deficit → difference between heart beat rate and peripheral arterial rate → AF
(like ✓ Different characters of pulse → their cause
cording) ▪ Water hammer (collapsing pulse)/bounding pulse → AR
▪ Pulsus paradoxus → pericardial tamponade
▪ Pulsus alterans → Advanced CHF
▪ Anacrotic pulse → AS
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▪ Bisferense pulse → AR ± AS
▪ Hypokinetic pulse → hypovolemia (constrictive pericarditis, MS), LSHF
▪ Hyperkinetic pulse → Anaemia, thyrotoxicosis, PDA, pregnancy, complete heart
block
✓ Radio femoral delay → coarctation of aorta in paediatrics
✓ Cording → DM, dyslipidemia, Aging

PR reporting example
PR = 72 BPM, regular and full in volume
Reporting of normal arterial examination
☛ All accessible peripheral arteries are palpable, full in volume and regular in rhythm
Distended
neck vein
JVP ✓ Normal→ 3-4 cm (8-9 mmhg)
✓ Raised JVP → CHF, constrictive pericarditis, SVC sxx, cardiac tamponade, rarely in CLD,
Nephrotic sxx and obstructive lung disease
✓ +ve kussmauls sign → raised JVP during inspiration
▪ Constrictive pericarditis
▪ rCMP
▪ MI (right ventricular infarction)
Venous Examination

Hepato ✓ +ve in CHF (major criteria of Framingham)


jugular reflex
Reporting of normal venous examination
☛ No distended neck vein, JVP = 3cm

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Precordial examination

Examination techniques Possible abnormal findings and their causes


❖ Activity ✓ Activity
❖ Apical impulse (AI) ▪ Active precordium → normal
❖ Precordial Buldge ▪ Hyper active precordium → HCMP, CHF (cardiomegaly)
❖ scar ▪ Quite (silent) precordium → IHD, DCMP, massive pericardial effusion
Inspection

✓ AI
▪ Normally @ 4th or 5th ICS, @ or medial to left MCL
▪ Not visible → pericardial effusion, constrictive pericarditis, highly
muscular individuals
▪ Displaced downwards and laterally → Cardiomegaly of different causes
(see below)
✓ Precordial buldge → long standing CHD
✓ Scar → evidence for surgical treatment of CHD

Reporting format for normal precordial inspection finding


☛ Active precordium, AI @5th ICS medial to left MCL, no precordial buldge or scar
Heart sounds (palpable or ✓ Heart sounds
not) ☛ Distant heart sounds → rCMP, Cardiac tamponade
PMI ▪ Beck’s triad of cardiac tamponade include
Heave and thrill 1) Distended neck vein
2) Hypotension
3) Distant / muffled heart sounds
☛ Palpable P2 at pulmonary area → Pulmonary HTN
☛ Palpable S2 at aortic area → systemic HTN
✓ PMI
Palpation

▪ Localized, tapping, non-sustained → normal


▪ Diffuse, thrusting, sustained → LVH 2ry to HTN, AS

☛ Diffuse → palpable by 2nd & 4th finger while 3rd is off from the
precordial area, > 2.5cm in size or occupy > 1 ICS
☛ Sustained → occupies more than 2/3rd of cardiac cycle
✓ Heave → indicate cardiomegaly
▪ Left parasternal heave → RVH
▪ Apical heave → LVH
✓ Thrill
▪ Palpable murmur like purring of a cat
▪ Indicate grade 4 and above murmur

Reporting format for normal precordial palpation finding


☛ Palpable heart sounds, PMI @5th ICS medial to left MCL which is Localized, tapping and non-sustained,
no heave or thrill

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✓ S1 & S2 (heart sounds) ✓ Added heart sounds


✓ Added heart sounds (S3 & ▪ S3 gallop
S4 gallop) Due to rapid ventricular filling in early diastole
✓ Murmur Normal finding in athletes
✓ Other heart sounds Physiologic S3 occurs in young adults of < 4o age
Anaemia
Thyrotoxicosis
CHF
CMP
▪ S4 gallop
Due to vigorous atrial contraction against stiff ventricle
Normal finding in athletes
HHD
AS
HCMP
✓ Other heart sounds
▪ Pericardial friction rub → ARF, acute pericarditis
Auscultation

▪ Pericardial knock → constrictive pericarditis


▪ Opening snap → MS

Reporting format for normal precordial auscultation finding


☛ S1 & S2 are well heard, no murmur or gallop

Signs of congested heart failure

1. GA
Cardiopulmonary distress
Edematous
2. Vital signs
Tachycardia ± Tachypnea
3. HEENT
Facial puffiness
4. RS
Basal rales /creptation and other pulmonary edema features
Pleural effusion
5. CVS
Distended neck vein
Raised JVP
S3 gallop
Cardiomegaly
6. Abdomen
Positive Hepatojugular reflex
Tender hepatomegaly
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7. MSS
Bilateral pitting edema

1.2.2. Murmur

Murmur characterization
Mnemonic for rehearsal of murmur characterization components

GP interprets QT interval in Light, Rapid, & Simple Method

1. Grade 5. Location of maximal intensity →


Signifies origin of murmur, shows where
✓ Systolic murmurs have 6 grades the murmur did best heard
1) Grade I - faint murmur, heard only with special efforts
2) Grade II - quiet but heard murmur ✓ MR, MS → over the mitral area
3) Grade III - moderately loud murmur ✓ TR, TS → LLSB
4) Grade IV - loud murmur accompanied by a thrill ✓ AR → erb’s point (left 2nd to 4th ICS)
5) Grade V - very loud, heard with a stethoscope partly off ✓ AS → right 2nd ICS
the chest ✓ PR, P2 accentuation → left upper
6) Grade VI- Heard with the stethoscope entirely off the chest sternal border
✓ Diastolic murmurs have only 4 grades
6. Radiation → Signifies direction of
2. Pitch blood flow
✓ High ✓ MR → to the left axilla/ base of
✓ Medium heart
✓ Low ✓ AS → to the neck
✓ TR → to the epigastrium
3. Quality
✓ Blowing → MR, TR, AR 7. Shape (configuration) → related to
✓ Rumbling → MS timing and not usually reported in
✓ Harsh physical examination
✓ Musical
✓ Crescendo → Murmur grows louder. Eg.
☛ Rasping → AS Pre-systolic murmur of MS
✓ Crescendo-decrescendo → Murmur that
4. Timing grows louder and then fall. Eg. Mid-
systolic murmur of AS
✓ Decrescendo → Murmur grows softer
➔ Identify whether the murmur is systolic, diastolic or continuous
and slowly falls. Eg. Early diastolic
in comparison to carotid pulse
murmur of AR
☛ Systolic murmurs coincide with carotid pulse, while the
✓ Plateau → Murmur has same intensity
diastolic do not
throughout. Eg. Pansystolic murmur of
✓ Systolic murmurs
MR, TR
1. Mid-systolic murmur (MSM)
❖ Begin after S1 and stops before S2
❖ E.g. Murmur of AS, PS, ASD
2. Late systolic murmur (LSM)
❖ Starts in mid or late systole and persists up to S2
8. Manoeuvre

✓ Respiration
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❖ E.g. Murmur of Mitral valve prolapse (MVP) ❖ Left-sided murmurs increase with
3. Pansystolic murmur (PSM) expiration → MR, AR
❖ Starts with S1 and stops at S2
❖ Right - sided murmurs increase
❖ E.g. Murmur of MR, TR, VSD
✓ Diastolic murmur with inspiration → TR, PR
1) Early diastolic murmur (EDM) ✓ Positioning → mostly used manoeuvre
❖ Starts after S2 and fades into silence before next S1 ❖ Tilting forward
❖ Eg. Murmur of AR, PR ☛ Increases the intensity of AR
2) Mid diastolic murmur (MDM) ❖ Leaning to left lateral position
❖ Starts after S2 and fade away or merge into a late ☛ Increases the intensity of MS
diastolic ✓ Hand grip exercise
murmur ❖ Increases the intensity of MR and
❖ Eg. Murmur of MS, ASD AR
3) Late diastolic (presystolic) murmur (LDM) ✓ Valsalva
❖ Starts late in diastole and continuous up to S1 ❖ Standing → Increases the
❖ Eg. Murmur of TS in sinus rhythm intensity of MR and decreases the
✓ Continuous murmur intensity of AS
❖ Begin in systole, peak at S2, and continue into all or ❖ Squatting → Increases the
part of diastole
intensity of AS and decreases the
❖ Eg. Murmur of PDA (continuous machinery like murmur
intensity of MR
is typical for PDA)

Characteristics of common cardiac valvular


lesions

Tip → during physical examination.


☛ for Timing → press carotid and Auscultate the murmur simultaneously for comparison
☛ for radiation → check possible sites (neck, epigastrium, axilla)
☛ do maneuvers for accentuation of murmur

MR TR AR AS MS
Grade Usually III Usually II to III
Pitch Medium to High pitched Low pitched
Quality Blowing Rasping Rumbling
Time Pan systolic murmur Early diastolic murmur Mid systolic Mid diastolic
murmur murmur
Location Best heard at the Best heard at the Best heard at the Best heard at Limited to the
Apex of the heart LLSB erb’s point the aortic area apex
Radiation to the left axilla/ to the epigastrium to the neck
base of heart
Manoeuvre Accentuated by deep Accentuated by Accentuated by
inspiration leaning forward and left lateral
expiration positioning and
exercise
Other ✓ Laterally and ✓ Laterally and down ✓ Laterally and ✓ Accentuated
associated
findings ✓

down ward
displaced AI
Muffled S1
Prominent S3



ward displaced AI
Wide pulse pressure
Water hammer pulse
Absent S2

down ward
displaced AI
Anacrotic
arterial pulse

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Opening snap
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gallop
Reporting ✓ Grade III, High ✓ Grade III, High ✓ Grade III, High ✓ Grade II, ✓ Grade II,
format pitched, pitched, Blowing, pitched, Blowing, low pitched, low pitched,
Blowing, Pansystolic early diastolic rasping, mid rumbling,
Pansystolic murmur, Best murmur, Best systolic mid
murmur, Best heard at the LLSB, heard at the erb’s murmur, diastolic
heard at the which radiates to point, accentuated Best heard murmur,
Apex of the the epigastrium, by leaning forward at the Aortic limited to
heart, which Accentuated by and expiration area, which the apex,
radiates to the deep inspiration radiates to accentuated
left axilla/ the neck by left
base of heart lateral
positioning
and
exercise
Causes ✓ Primary (organic) ✓ Acute ✓ Rheumatic ✓ Rheumatic
(DDX) ❖Acute • Rheumatic o IE fever or fever/RHD
o IE fever/RHD o Trauma ✓ CRMVHD (>95%)
Click here o Papillary • IE o Aortic dissection ✓ Congenital ✓ Other less
→ • Papillary (bicuspid, common
muscle o Trauma
muscle injury unicuspid) causes
rupture ✓ Chronic
(post-MI) ✓ Degenerative o IE
(Post MI) • Myxomatous o Primary valvular calcification o Congenita
Valvular o Chordae (tricuspid valve disease: ✓ Radiation l
heart tendineae prolapse)
• Leaflet trauma
▪ Rheumatic o Severe
mitral
rupture fever (RHD)
diseas o Blunt • Radiation ▪ IE annular
• Carcinoid heart calcificatio
e trauma
disease
▪ Congenital
n with
❖Chronic Bicuspid
(VHD) o Primary MR-
• Endomyocardial
aortic valve
leaflet
fibrosis involveme
▪ RHD • CHD in ▪ SLE nt
▪ IE children ▪ Syphilitic o SLE
▪ Mitral (Ebstein’s aortitis o RA
valve malformation of o Myxoma
▪ Ankylosing
the tricuspid
prolapse spondylitis.
valve)
(MVP) ✓ Secondary ▪ Myxomatous
▪ Trauma (functional) /cause (prolapse)
▪ Congenital of > 80% of TR/ o Aortic root
(cleft, AV • MI disease
canal) • Cardiomyopath ✓ Aortic
y (HCMP,
o Secondary dissection
DCMP)
(functional) ✓ Systemic
• Atrial fibrillation
MR (AF) severe HTN
▪ IHD • Longstanding ✓ Cystic medial
▪ DCMP pulmonary HTN degeneration
▪ HCMP • Left-sided valve of the
▪ Chronic disease ascending
Atrial aorta
Fibrillation ✓ Marfan
o Mitral annular syndrome
calcification ✓ Bicuspid
aortic valve
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✓ Nonsyndromic
familial
aneurysm
✓ Aortitis
✓ Idiopathic
dilation of the
aorta
✓ Annuloaortic
ectasia
✓ Osteogenesis
imperfecta
IX Refer long case of nitsibin → IX of HF (click here → Chapter 1; Heart failure (ልብ ድካም))
Mgt Refer long case of nitsibin → mgt of HF (click here → Management of heart failure) and VHD mgt
principle (Click here →

Valvular heart disease (VHD))

N.B

✓ Peripheral signs of AR
☛ deMusset's sign – head bob occurring with each heart beat
☛ Traube's sign – a pistol shot pulse (systolic and diastolic
sounds) heard over the femoral arteries
☛ Duroziez's sign – a systolic and diastolic bruit heard when the
femoral artery is partially compressed
☛ Quincke's pulses – capillary pulsations in the fingertips or lips
☛ Mueller's sign – systolic pulsations of the uvula
☛ Becker's sign – visible pulsations of the retinal arteries &
pupils
☛ Hill's sign – popliteal cuff systolic pressure exceeding brachial
pressure by more than 60 mmHg
☛ Mayne's sign – more than a 15 mmHg decrease in diastolic
blood pressure with arm elevation from the value obtained with
the arm in the standard position
☛ Rosenbach's sign – systolic pulsations of the liver
☛ Gerhard's sign – systolic pulsations of the spleen

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DDX for cardiomegaly


❖ HHD
❖ DCMP
❖ HCMP
❖ CAD (MI)
❖ CHD
❖ Peripartum CMP
❖ Pulmonary HTN
❖ Pericardial effusion
❖ Hemochromatosis
❖ Amyloidosis
❖ Idiopathic

DDX for Displaced PMI


❖ Cardiomegaly of different causes
❖ Chronic Pleural or pulmonary disease
❖ Deformities of chest wall or thoracic vertebrae

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1.2.3 Leg edema


Pedal and pretibial pitting edema occurs in
❖ CHF → symmetrical and worsens in the evening and improves early in the
morning
❖ Constrictive pericarditis
❖ CLD → starts with ascites which may progress to GBS
❖ Nephrotic syndrome or AKI/CKD → affects face first
❖ Advanced Lymphoma (NHL)
❖ Disseminated TB to pericardium (result in Constrictive pericarditis), pleura,
Peritoneum…
❖ Varicose veins and DVT
❖ Vasodilating drug (e.g. a calcium channel blocker)

Edema grading
✓ Palpate behind the medial malleolus and the distal shaft of the tibia, and
dorsum of foot for pitting edema by gently compressing the area for at least
15 seconds with the thumb

Grade Grading by body sites Grading by time Grading based


(mostly used clinically) to refill the pitting on compression
edema depth
I pedal and pretibial edema < 5 seconds 2cm
II Edema involving leg and thigh 5-10 seconds 2 - 4cm
III Edema involving abdominal 10-15 seconds 4 - 6 cm
wall and pre-sacrum
IV Anasarca (generalized edema > 15-20 seconds > 6 cm
including serosal fluid
accumulation)

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1.3 Abdominal examination

1.3.1 Physical examination findings

Examination techniques Possible abnormal findings and their causes


N.B.
✓ while doing abdominal examination 1st look at sclera and skin for jaundice (hepatitis)
✓ the order of examination should be Inspection → auscultation → palpation → percussion (since bowel sounds are
affected by palpation, auscultate bowel sound before palpation)
❖ Symmetry ❖ Silent abdomen → generalized peritonitis
✓ Movement with respiration ❖ Shape of abdomen
❖ Shape (check also flank ✓ Flat → normal
fullness and contour of ✓ Scaphoid → diaphragmatic hernia
umbilicus) ✓ Distended abdomen → ascites, abdominal mass, HSM, gas (intestinal
❖ Superficially distended obstruction)
abdominal veins N.B 6F’S in abdominal distension
❖ Scar Fluid → ascites
❖ Straie Feces → incomplete intestinal obstruction
❖ Pigmentation Flatus → complete intestinal obstruction
❖ Peristalsis Fat → obesity
❖ Hernia sites Fetus → pregnancy
✓ Don’t forget to ask the pt Fatal growth → organomegaly, malignancy, AAA
to cough (abdominal aorta aneurysm)
❖ Flank fullness
✓ Full flanks with abdominal distension→ ascites
✓ Full flanks without abdominal distension → Psoas abscess,
Hydronephrosis, Perinephric abscess
Inspection

❖ Contour of Umbilicus
✓ inverted with circular slit or slightly horizontal → normal
✓ Horizontal slit and everted → huge ascites or mass
✓ Horizontal slit → ascites or bilateral flank mass
✓ Vertical slit → mass
❖ superficially distended and tortuous abdominal vessels
✓ drain away from palpation during palpation which indicate portal HTN
(William Harvey method)
✓ draining towards umbilicus → IVC obstruction
❖ scar → previous surgery or trauma
❖ straie alba/atrophica → ascites
N.B
✓ Straie gravidarum→ in pregnancy
✓ Purple straie → cushing sxx
❖ Ecchymosis → herald haemorrhages (intra or retroperitoneal)
❖ Vigorous peristalisis → pyloric stenosis, intestinal obstruction
N.B.
Peristalsis and superficially distended veins should be observed sitting on bedside and by using adequate light
Reporting format for normal abdomen inspection finding
☛ Symmetrically flat abdomen that moves with respiration, flanks are not full, inverted umbilicus with
circular slit, there is no superficially distended abdominal veins, no visible scar, straie, pigmentation or
peristalsis, hernia sites are free
✓ Bowel sounds ✓ Bowel sounds
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✓ Bruit ❖ Normal → 5 - 30 kicks/minute


✓ Friction rub ❖ increased in frequency and noisy → early intestinal obstruction,
diarrhoea
❖ reduced then absent → generalized peritonitis, paralyzed ileus
✓ Bruit
❖ Over Abdominal aorta → partial obstruction of aorta
❖ Over renal arteries → renal artery stenosis
❖ Over liver → HCC, alcoholic hepatitis
❖ Over femoral and iliac arteries
✓ Friction rub
❖ Liver → liver tumour
❖ Spleen → splenic infarct
Reporting format for normal abdomen auscultation finding
☛ Normoactive bowel sounds (18 kicks/min), no bruit over abdominal aorta, renal arteries, iliac arteries or
liver
Superficial ✓ Guarding, rigidity, direct/rebound tenderness → acute abdomen (firm and
✓ Tenderness board like in generalized peritonitis)
✓ Superficial palpable mass ✓ CVAT → pyelonephritis
Deep → Search for ✓ Abdominal mass
▪ Guarding ▪ Origin from Abdominal wall → protrudes when pt head lifts up
▪ Rigidity ▪ Origin from upper abdomen which doesn’t allow finger to pass
▪ Mass above the mass → mass from liver, spleen, stomach
▪ Direct / rebound ▪ Origin from lower abdomen which doesn’t allow finger to pass
Palpation

tenderness below the mass → mass from urinary bladder, upper rectum
▪ Organomegaly (liver, ▪ Origin from RUQ → mass from Liver, right kidney, hepatic flexure
spleen, kidney) of colon
▪ Ballotable mass in
ascites
N.B
If spleen is not palpable, turn the pt to the right with flexion of left heep and knee then repeat palpation. If still
not palpable go to percussion methods (Nixon, castles, troubes)
Reporting format for normal abdomen palpation finding
☛ Superficial palpation
No superficial tenderness, no superficially palpable mass
☛ Deep palpation
No direct/rebound tenderness, guarding or rigidity, Liver and spleen are not palpable, kidney is not
bimanually palpable bilaterally.
➢ Percussion note ➢ Percussion note
➢ TVLS ✓ Tympanic → normal
✓ Should not be done in right ✓ Hyper tympanic → gas
sided pleural effusion and ✓ Dullness → organomegaly, mass, ascites (associated with shifting
ascites dullness and fluid thrill)
Percussion

➢ Spleen percussion methods ➢ TVLS


☛ 10 ± 2 cm → normal
☛ Upper border of liver is palpable at 5th ICS along the right MCL
normally
☛ TVLS > 12 cm → hepatomegaly
N.B. you can say hepatomegaly after doing TVLS, before
doing TVLS you have to report as liver is palpable ‘’X’’ cm
below the right costal margin
☛ TVLS < 8cm → shrunken liver (e.g. advanced cirrhosis)

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Spleen percussion methods


Nixon’s method
✓ Ask the patient to turn to the right side
✓ Begin percussing at the lower level of pulmonary resonance along the left posterior axillary line and proceed
diagonally along a perpendicular line towards the lower mid-anterior costal margin
✓ The upper border of dullness is normally 6-8 cm above the costal margin
✓ Dullness > 8cm suggests splenomegaly

Castell’s method
✓ Ask the pt to be on supine position
✓ Percuss the lower intercostal space at 8th or 9th interspace along left anterior axillary line during full
inspiration and expiration
✓ Dullness on full inspiration suggests splenomegaly

Traube’s method
✓ Borders of Traube’s space:
1. Superiorly 6th rib
2. laterally left mid axillary line
3. inferiorly left costal margin
✓ Ask the patient to be on supine position with the left arm slightly abducted
✓ Percuss from medial to lateral margins in normal breathing. It usually produces normal resonant sound at
traube’s space
✓ Dullness to percussion at Traube’s space suggests splenomegaly
Reporting format for normal abdomen percussion finding
☛ Tympanic percussion note all over the abdomen, no shifting dullness or fluid thrill, TVLS = 10cm
N.B DRE (digital rectal examination)
Finally, it is important to do DRE since abdominal examination without DRE is incomplete

1.3.2 Ascites

Findings DDX IX Mgt principle


✓ symmetrically distended
abdomen
Transudative Ascitic fluid
❖ Salt restriction: < 2g per day
❖ Diuretics:
▪ flanks are full CLD → refer analysis a. Spironolactone 100-
▪ eversion of umbilicus secondary causes from LFT and liver 200mg/day, escalate to a
long case of nitsibin
with transverse or enzymes max. dose of 400-
circular slit (under DDX of CLD) Viral markers 600mg/day.
▪ fluid thrill and shifting RSHF (HBsAg for b. Furosemude(lasix) 40-
Constrictive pericarditis
dullness screening) 80mg /day, escalate to a
▪ superficially distended Nephrotic sxx (NS), CXR, ECG, max. dose of 120-
and tortuous abdominal AKI, CKD ECHO → 160mg/day.
Chronic pancreatitis
vessels RSHF
▪ drain away from SLE If ascites is still present despite the
Meig’s sxx → ovarian U/A → NS
umbilicus during above measurements, it is defined as
ca + pleural and
palpation which refractory ascites.
indicate portal HTN peritoneal effusion
(William Harvey IVC sxx ❖ Alternative treatment modalities


method)
straie alba/atrophica
Hypothyroidism → rare
PLE (protein losing
enteropathy) → very
include:
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▪ associated ballotable rare condition (therapeutic tap)


2) TIPS (trans jugular intra
mass (e.g. HSM) Exudative hepatic portosystemic shunt)
Infectious → TB procedure
peritonitis 3) Liver transplant
Malignancy
(carcinomatous
infiltration) →
lymphoma, leukaemia

Reporting format of asites


❖ Inspection
Symmetrically distended abdomen that moves with respiration, flanks are full, everted umbilicus with circular slit,
there are superficially distended abdominal veins which drain away from umbilicus during palpation, no visible
scar, straie, pigmentation or peristalsis, hernia sites are free
❖ Auscultation
Normoactive bowel sounds (18 kicks/min), no bruit over abdominal aorta, renal arteries, iliac arteries or liver
❖ Palpation
Superficial palpation
No superficial tenderness, no superficially palpable mass
Deep palpation
No direct/rebound tenderness, guarding or rigidity, no ballotable organ
❖ Percussion
There is dullness over the flanks, there is shifting dullness but no fluid thrill, TVLS = 10cm

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1.3.3 Splenomegally

Findings DDX IX Mgt


(characterization) principle
Size → enlarged/palpable mass Massive Tipped RK 39
over the LUQ which is ‘’X’’ cm Splenic
from left costal margin along the VL Military TB aspiration
splenic growth line. CML, CLL IE HBsAg
Tenderness → non tender (if NHL Malaria CBC & PM
tender consider → splenic HMS SLE BM aspiration
abscess, malignancy /e.g. blast HSS Typhus / Abdominal
crisis phase of CML/) Auto immune typhoid fever U/S
Consistency → soft/firm/hard haemolytic Sepsis
Surface → smooth anaemia IM (infectious
Border → sharp edge Hairy cell mononucleosis)
Palpable medial notch leukaemia Brucellosis
Doesn’t allow finger to pass Thalassemia
below left costal margin Goucher disease
Moves with respiration Niemann pick
Not bimanually palpable disease
N.B
Splenomegaly
☛ Tipped → 1 - 2 cm
☛ Moderate → 3 - 7 cm
☛ Massive → ≥ 8 cm
Hypersplenism
☛ Splenomegaly +
☛ Pancytopenia +
☛ Normocellular BM +
☛ Correction of smx by splenectomy (normal post splenectomy cell count)

Reporting format of Splenomegaly


❖ Enlarged/palpable mass over the LUQ which is ‘’X’’ cm from left costal margin along the splenic growth line,
non-tender, firm in consistency, smooth surface, sharp edge, Palpable medial notch, Doesn’t allow finger to pass
below left costal margin, Moves with respiration, Not bimanually palpable

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How to differentiate splenomegaly from enlarged left


kidney?

Splenomegaly Enlarged left kidney


Grows along the splenic Grows antero-posteriorly
growth line Has no medial notch
Has medial notch Able to go beneath the
Unable to go beneath the costal margin
costal margin Bimanually palpable but not
Not bimanually palpable always
Dull to percussion Colonic resonance to percussion
Moves with respiration Moves with respiration

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1.3.4 Hepatomegaly, Hepatomegaly with ascites,


Hepatosplenomegaly
Findings DDX IX Mgt
principles
(characterization)
Size → Hepatomegal Hepatosplenomeg Hepatom LFT, viral ✓
enlarged/palpable y aly egaly markers
mass over the RUQ RK39
which is ‘’X’’ cm below
with CBC &
the right costal margin. ascites PM
Tenderness → non CHF, CLD 1. NHL Ascitic
tender (if tender Constrictive CML, CLL 2. CML fluid
consider → cardiac pericarditis NHL 3. CLD analysis→
congestion of liver CLD HMS if there is
Consistency → HCC HSS ascites
soft/firm/hard Pyogenic CHF Abdominal
Surface → smooth liver VL U/S
Edge → blunted in abscess Military TB
case of cardiac VL Chronic Anaemia
congestion and sharp Malaria (haemolytic
edge for other causes Typhus / anaemia,
Doesn’t allow finger to typhoid fever Megaloblastic
pass below right costal IM anaemia)
margin Brucellosis SLE
Moves with respiration Acute retroviral
Not bimanually SXX of RVI
palpable IM (infectious
mononucleosis)
Brucellosis
Goucher disease
Amyloidosis
Tender hepatomegaly
➔ Congested liver from CHF, Constrictive
pericarditis, Pericardial effusion
➔ Amoebic liver
abscess
➔ Acute viral hepatitis
➔ Infected hydatid cyst
Reporting format of Hepatomegaly
☛ Enlarged/palpable mass over the RUQ which is ‘’X’’ cm below the right costal margin, non-tender, firm in
consistency, smooth surface, sharp edge, doesn’t allow finger to pass below left costal margin, Moves
with respiration, Not bimanually palpable

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1.3.5 Renomegaly

Findings DDX IX Mgt


(characterization) principle
Size → bimanually palpable mass HIVAN (HIV associated RFT
over the left/right lower part of nephropathy) Abdominal U/S
abdomen DM nephropathy CBC
Tenderness → non tender PCKD PICT
Consistency → soft/firm/hard Hydronephrosis RBS
Surface → smooth Huge pyelonephritis
Moves with respiration Malignancy (RCC)
Amyloidosis
Obstructive uropathy (e.g
pelvic ureteral junction
obstruction)

1.3.6 Abdominal mass


Findings (characterization) DDX
Site/ location Organomegaly
☛ Specify the quadrant NHL
☛ Is it abdominal wall or intra-abdominal mass? Appendiceal mass
▪ Feel the mass while the pt lifts her/his head and shoulders off the Appendiceal
pillow to tense the abdominal wall abscess
➢ prominently protruded mass - abdominal wall mass Malignancy arising
➢ if the mass disappears- intra-abdominal mass from stomach and
☛ Identify whether abdominal or pelvic origin intestine
Size &shape HCC
Surface, edge &consistency PCKD
☛ hard, irregular and nodular → likely malignant AAA (Abdominal
☛ regular, round, smooth, tense swelling → likely cystic aortic aneurism)
☛ solid, ill-defined and tender mass suggests an inflammatory lesion Hydronephrosis
Mobility & attachment Perinephric
abscess
☛ mass arising from the liver, spleen, kidneys, gall bladder and stomach moves
Psoas abscess
down ward during inspiration
Ovarian mass
☛ mass arising from the small bowel, transverse colon, mesentery and greater
Myoma
omentum are not usually influenced by respiratory movement
☛ Side-to-side movable lower abdominal mass favours swelling of uterine origin
but not from urinary bladder arising mass
☛ completely fixed mass suggests → retroperitoneal origin, advanced tumour,
mass resulting from severe chronic inflammation involving other organs (e.g.
diverticulitis of the sigmoid colon or a tuberculous ileo caecal mass).
Bimanually palpable or pulsatile
☛ Pulsatile and expansile abdominal mass favors abdominal aneurysm

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1.4 Nervous system

You may be asked the following in NS examination


☛ Do lower motor examination → most cmnly asked
☛ Do nervous system examination

1.4.1 Physical examination findings

Examination techniques Possible abnormal findings and their


causes
GCS = Glasgow coma scale
Eye Best verbal Best motor score The GCS is scored between 3 and 15
opening response response GCS
Obeys commands 6 ☛ ≥ 13 → mild brain injury
Oriented Localizing response 5 ☛ 9 - 12 → moderate brain injury
to pain
☛ ≤ 8 → severe brain injury.
Spontaneou Confused Withdrawal 4
s response to pain
GCS and FOUR score

Response Inappropriate Flexion to pain 3


to verbal words
command
Response Incomprehensib Extension to pain 2
to pain le sounds
No eye No verbal No motor response 1
opening response

FOUR score = Full Outline of Unresponsiveness.


Eye Motor Brainstem Respirat score have greater utility than the GCS in
response response reflexes ion coma diagnosis, primarily by including a
eyelids thumbs-up, pupil and not 4 brainstem examination
open or fist, or corneal intubated,
opened, peace sign reflexes regular
tracking, or present breathing
blinking to pattern
command
eyelids localizing to one pupil not 3
open but pain wide and intubated,
not tracking fixed Cheyne-
Stokes
breathing
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pattern

eyelids flexion pupil or not 2


closed but response to corneal intubated,
open to pain reflexes irregular
loud voice absent breathing
eyelids extension pupil and breathes 1
closed but response to corneal above
open to pain reflexes ventilator
pain absent rate
eyelids no response absent breathes 0
remain to pain or pupil, at
closed with generalized corneal, ventilator
pain myoclonus and cough rate or
status reflex apnea

Conventional method of assessing level of consciousness

Procedure score Mini-mental state examination (MMSE)


indicates severity of cognitive impairment
MMSE

A. Day, Date, Month, Season, Year 5


It is scored out of 30
OREINTATION Country, State, City, Hospital, 5
Floor
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B. Name 3 objects and patient 3 presence of impaired cognition (dementia)


REGISTRATION repeats ☛ Mild dementia → 21-23/30
☛ Moderate dementia → 18-21/30
C. Serial 7s or spell backwards 5
ATTENTION & ☛ Severe dementia <18/30
CALCULATION Examples of Buts’ or ifs’
D. Repeat the 3 objects mentioned 3 ☛ Betty bought a better butter to make
RECALL before a bitter butter a better butter
E. Name a pen and a pencil 9 ☛ Don’t promise a promise, if you
LANGUAGE (2points) promise keep your promise a
Buts’ or ifs’ (1point) promise
Follow 3 stage command ☛ በበግ ቤት በግ ገባ
(3points) ☛ ጫላ ጩቤ ጨበጠ
Read and obey (1point)
Write sentence and copy design
(2)
CN examination procedures
❖ CN I → Patency, odour
❖ CN II → acuity, field, pupillary reaction to light (afferent
optic nerve efferent CNIII) and accommodation
❖ CN III, IV, VI → Extraocular eye movement (superior
oblique by CN4, lateral rectus by CN 6)
❖ CN V
➔ Temporal and masseter muscle strength
➔ Pain and light touch reflex of face
➔ Corneal reflex (afferent CN5, efferent CN7)
❖ CN VII
➔ Facial drop or asymmetry
➔ Can raise eyebrows or not
➔ Open/close eyes against resistance
➔ Smile, frown
➔ Show teeth
➔ Puff out cheeks
CN

❖ CN VIII
➔ Can hear finger rub
➔ Rinne and weber test if possible
❖ CN IX & X
➔ Listen patients voice
➔ Ask to swallow
➔ Ask to say ‘’AH’’ and check location of uveola
➔ Check gag reflex
❖ CN XI
➔ Check atrophy/asymmetry of trapezius
➔ Can shrug shoulder against resistance
➔ Can turn his/her head against resistance
❖ CN XII
➔ Listen articulation of words
➔ Tongue inspection
➔ Can protrude tongue
➔ Can move tongue from side to side
➔ Push cheeks by tongue

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❖ Inspection TONE
➢ position of the extremities after repositioning by ✓ Can be normotonic, hypotonic (in flacid
the examiner lesions) or hypertonic (in spastic lesions)
☛ outward rotation → flaccid paresis/plegia Types of spasticity
☛ inward rotation → spastic paresis/plegia
➢ fasciculation 1. Klasp-knife spasticity: velocity-dependent
➢ Muscle Symmetry → compare proximal with spasticity with sudden release after reaching
distal, left with right a maximum, commonly seen in pyramidal
➢ Atrophy tract lesions
❖ Palpation 2. Lead-pipe spasticity: Increased tone
➢ Tone present throughout the range of motion is
➢ Power observed in frontal lobe disease
➢ Reflex 3. Cogwheel spasticity: Spasticity enterwined
☛ DTR ± Clonus, janderasik manoeuvre by tremor, commonly seen in extrapyramidal
☛ Superficial lesions
Plantar
Abdominal ➢ POWER
Scapular Grade Description
Anal 0/5 No muscle movement
Bulbocavernosus 1/5 Visible flicker muscle movement,
Cremasteric but no movement at the joint
Corneal 2/5 Movement at the joint (horizontal
➢ Arm drift mov’t), but not against gravity
☛ Pronator Drift 3/5 Movement against gravity, but not
☛ Cerebellar drift against added resistance
☛ Parietal drift 4/5 Movement against resistance, but
➢ Coordination less than normal
☛ Rapid Alternating Movements 5/5 Normal strength
✓ strike one hand on the thigh,
raise the hand, turn it over Power interpretation
✓ tap the distal thumb with the tip ➢ 0/5 & 1/5 → plegia
of the index finger
✓ tap your hand with the ball of
➢ 2/5 - 4/5 → paresis
each foot ➢ 5/5 → normal
☛ Point-to-Point Movements
✓ finger-to- nose test DTR Grading Scale
✓ Heel-to-Shin test
➢ Gait Grade Description
☛ Walk across the room, turn and come 0 Absent (with Jendrasik maneuver)
back 1+ or + Hypoactive (less brisk)
☛ Walk heel-to-toe in a straight line 2+ or ++ "Normal" (brisk)
(tandem walk) 3+ or Hyperactive without clonus (very
☛ Walk on their toes in a straight line +++ brisk)
☛ Walk on their heels in a straight line 4+ or Hyperactive with clonus
☛ Hop in place on each foot ++++
Motor examination

☛ Do shallow knee bend


☛ Rise from a sitting position Difference between UMNL and LMNL

Variables LMN lesion UMN lesion


Fasciculati Present absent
on
Atrophy Present none, mild
Tone
Reflex
Plantar
Hypotonia
hyporeflexia
No
hypertonia
hyperreflexia
Up
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reflex response going/Babinsk


i +ve

Plantar reflexces
✓ Upgoing /babniski +ve → normal or
UMNL
✓ Down going
✓ No response / equivocal → LMNL
❖ Primary sensory test Positive sensory phenomena by neurologic
☛ Pain, temperature, light touch → test for examination
anterolateral tract ✓ Hypesthesia/hypoesthesia
☛ Position and vibration → test for posterior tract ✓ Anesthesia
❖ Cortical sensory test ✓ Hypalgesia
☛ Extinction or simultanagnosia ✓ Hyperesthesia
Sensory examination

☛ Graphesthesia ✓ Allodynia
☛ Stereognosis ✓ Hyperalgesia
☛ Two Point Discrimination ✓ Hyperpathia
Negative sensory phenomena by neurologic
☛ Double simultaneous stimulation (DSS)
examination
✓ Impaired or absent primary sensory
modalities like to touch, vibration,
position, and temperature

❖ Signs of meningeal irritation


Meninge

☛ Neck stiffness
irritation

☛ Kernig's sign
signs

☛ Brudzinski's sign
al

☛ Jolt accentuation of headache


Reporting format for normal NS Examination finding
☛ Level of consciousness
➢ GCS = 15/15 (E4V5M6), conscious and alert
☛ CN examination
➢ CN-I:
▪ S/he can smell soap via each nostril.
➢ CN-II:
▪ S/he can differentiate 2 fingers at about 6 meters. (Visual Acuity)
▪ S/he sees waggling of finger approximately 1000 from axis of eye. (Visual Fields)
▪ S/he differentiates green and red colours. (Colour Appreciation)
▪ Normal direct and consensual pupillary light reflex
➢ CN-III, IV & VI:
▪ The eyes can move in all directions. There is no nystagmus or diplopia. The pupils
are round, regular in outline and equal in size. They react to light directly and
consensually.
➢ CN-V:
▪ S/he identifies light touch and pin prick over the mandibular, maxillary and
ophthalmic areas of the face.
▪ S/he closes her/his eyes at the touch of the cornea with a cotton swab.
▪ Contraction of the temporal and masseter muscles is symmetrical and strong while
clenching her/his teeth.
➢ CN-VII:
▪ The face is symmetrical at rest and during voluntary movements (smiling, frowning).
▪ S/he can smile, frown her/his forehead, puff out her/his cheeks
▪ can close both eyes equally and forcefully against resistance.

➢ CN-VIII:
▪ Intact nasolabial fold
▪ Intact corneal reflex 902
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▪ S/he can hear rubbing of the fingers on both ears.


➢ CN-IX & X:
▪ The soft palate rises in the midline when saying ‘ah!
▪ Centrally located uvula
▪ S/he can swallow his saliva
➢ CN-XI:
▪ The Sternocleidomastoid and trapezius muscles contract on turning the head and on
shrugging the shoulder against resistance, respectively
➢ CN-XII:
▪ The tongue protrudes in the midline and shows no fasciculation or atrophy.
☛ Motor examination
❖ Inspection
▪ The limbs are centrally positioned, no inward or outward rotation
▪ Comparable muscle bulk between the left and the right side of both upper and lower
extremities.
▪ There is no spontaneous as well as induced fasciculation.
❖ Palpation
➢ Tone and power

TONE POWER
Upper Lower Upper Lower
Right Normo-tonic Normo-tonic 5/5 5/5
Left Normo-tonic Normo-tonic 5/5 5/5

➢ Reflexes
▪ Superficial
o Abdominal reflex is present both in upper and lower quadrants.
o Corneal reflex is intact in both eyes.
o Plantar reflex is down going on both sides.
▪ DTR
Biceps Triceps Brachioradialis Patellar Ankle
Right ++ ++ ++ ++ ++
Left ++ ++ ++ ++ ++

☛ Sensory examination
Primary sensory exam
➔ S/he identifies light touch and pin prick over the extremities and trunk.
➔ S/he is able to recognize different movements of the toes with his eyes
closed. (Position sense)
➔ Vibration sense was not assessed due to lack of Tuning Fork.
Cortical sensory exam
➔ S/he appreciates the form of a key by means of only touch (Stereognosis)
➔ S/he recognizes writings of different numbers on his palm (Graphesthesia)
➔ S/he is able to differentiate 2 pin pricks up to 4 mm apart over the finger tips (2 pt
discrimination).
☛ Coordination
❖ Finger to nose, heal to shin and rapid alternating movement of the arm were done without
any abnormalities.
☛ Meningeal irritation signs
❖ No neck stiffness.
❖ Kernig's Sign is negative.
❖ Brudzinski's Sign is negative

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1.4.2 Paraplegia/paresis
Refer long case of nitsbin (click here → Chapter 7; Paraplegia (ከወገብ በታች
ሽባነት))

1.4.3 Monoplegia/paresis

Findings DDX IX Mgt


principle
✓ position of the extremities after UL only LL only Both UL and LL Refer long
repositioning by the examiner Brachial Lumbosacral TIA case of
☛ outward rotation → flaccid plexopathy plexopathy Poliomyelitis nitsibin
paresis/plegia Cauda ☛ Cause under
☛ inward rotation → spastic equina sxx radiculopathy paraplegia
paresis/plegia Vasculitis
Decreased muscle bulk of the BSS (Hemi
affected limb section of the
spontaneous as well as induced cord)
fasciculation in LMNL Cases Early stage of
hypertonic in spastic lesions and foramen
hypotonic in flacid lesions magnum sxx
power 0/5 & 1/5 in plegia, 2/5 upto ☛ Clock wise
4/5 in paresis rotation of
hyperreflexia in UMNL and weakness
hyporeflexia in LMNL
plantar reflex
☛ Upgoing /babniski +ve → normal
or UMNL
☛ Down going/No response /
equivocal → LMNL
Absent primary and cortical sensory
tests on the affected limb

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1.4.4 Quadriplegia/paresis
Findings DDX IX Mgt
principle
✓ position of the extremities after Foramen magnum sxx Refer long case of
repositioning by the examiner Cervical cord lesions (e.g. nitsibin under
☛ outward rotation → flaccid craniovertebral anomaly, trauma to paraplegia
paresis/plegia cervical cord)
☛ inward rotation → spastic TM of cervical cord
paresis/plegia GBS
Decreased muscle bulk of all 4 extremities Bilateral brainstem lesions
hypertonic in spastic lesions and hypotonic Central cord sxx involving cervical
in flacid lesions cord
power 0/5 & 1/5 in plegia, 2/5 upto 4/5 in Anterior spinal artery sxx involving
paresis cervical cord
hyperreflexia Poliomyelitis
plantar reflex → Upgoing /babniski +ve MS
Absent primary and cortical sensory tests MND
in all 4 extremities Peripheral neuropathy

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Chapter 1; Physical examination

1.4.5 Coma

DDX IX Mgt
principle
Symmetrical, Symmetrical, Asymmetrical, structural Screening ABCs:
nonstructural structural laboratories ☛ Secure IV line
Metabolic Supratentorial Supratentorial (CBC, RBS, ☛ Intubate if
☛ Hypoglycemia ☛ Sagittal sinus ☛ SDH electrolytes, GCS ≤8
☛ DKA thrombosis ☛ Bilateral ICH BUN, creatinine, ☛ Stabilize C
☛ Lactic acidosis ☛ SAH ☛ Subdural PT, PTT, ABG, Spine
☛ Hyperglycemic ☛ Trauma- empyema LFTs, drug ☛ Supplement
nonketotic contusion, ☛ Thrombophlebitis screen) O2
coma concussion ☛ Unilateral ECG ☛ Blood
☛ Hepatic ☛ Bilateral hemispheric Head CT scan pressure
encephalopathy internal carotid mass (tumor, → prioritize support as
☛ Uremia occlusion abscess, bleed) emergent if focal needed
☛ Bilateral with herniation neurologic signs, Glucose 50
☛ Hypertensive
anterior ☛ Cerebral papilledema, percent IV 50
encephalopathy
cerebral artery vasculitis fever mL (after
☛ Wernicke
occlusion LP → prioritize blood drawn,
encephalopathy ☛ Cerebral abscess
☛ Thalamic emergent after before results
☛ Dialysis ☛ TTP
hemorrhage CT scan if fever, back)
encephalopathy ☛ DIC
elevated WBC, Consider
☛ Hypoxia ☛ Hydrocephalus ☛ Multiple sclerosis meningismus; empiric
☛ Hypercapnia Infratentorial ☛ Acute otherwise do treatments:
☛ Hyper/hypother ☛ Midline disseminated according to ☛ For possible
mia brainstem encephalomyelitis level of suspicion infection →
☛ Hypernatremia tumor ☛ Subacute for diagnosis or Ceftriaxone
☛ Hyper/hypocalc ☛ Basilar bacterial if cause remains and
emia occlusion endocarditis obscure Vancomycin,
☛ Hypermagnese ☛ Pontine ☛ Nonbacterial Other laboratory
hemorrhage acyclovir
mia thrombotic tests → blood
☛ Central endocarditis ☛ For possible
☛ Hypothyroidism cultures, adrenal
pontine (marantic ingestion→
☛ Reye syndrome and thyroid tests,
Naloxone,
myelinolysis endocarditis) coagulation tests,
☛ Aminoacidemia Flumazenil,
☛ Porphyria ☛ Multifocal carboxyhemoglobi
Gastric
☛ Addisonian leukoencephalopa n, specific drug
lavage/activate
crisis thy concentrations -
d charcoal
Infections ☛ Pituitary apoplexy do according to
☛ For possible
☛ Bacterial ☛ Massive or level of suspicion
increased ICP
meningitis bilateral for diagnosis or
→ mannitol
☛ Viral supratentorial if cause remains
☛ For possible
encephalitis infarction obscure
nonconvulsive
☛ Cerebral ☛ Creutzfeldt-Jakob Brain MRI with
status→
Malaria disease DWI, if cause
Lorazepam,
☛ Adrenal remains obscure
☛ Postinfectious Phenytoin or
leukodystrophy EEG: for
encephalomyelit equivalent
☛ Leukoencephalop possible
is Treat definite
athy associated nonconvulsive
☛ Waterhouse- seizures with
seizure, or if
Friderichsen
syndrome
with
chemotherapy
Infratentorial
diagnosis
remains obscure
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Chapter 1; Physical examination

☛ Syphilis ☛ Brainstem Thiamine 100


☛ Sepsis infarction mg IV
☛ Typhoid fever ☛ Brainstem
Toxins hemorrhage
☛ Lead ☛ Brainstem
☛ Methanol thrombencephaliti
☛ Ethylene glycol s
☛ Carbon Comma mimetics
monoxide
☛ Mushrooms
☛ Thallium Locked-in syndrome
☛ Cyanide ☛ Consciousness is preserved; however,
Drugs the patient cannot move muscles in the
limbs, trunk, or face, except that
☛ Sedatives
voluntary blinking and vertical eye
☛ Barbiturates
movements remain intact.
☛ Alcohol
☛ It is a consequence of a focal injury to
☛ Opiates
the base of the pons, usually by embolic
☛ Salicylate occlusion of the basilar artery
☛ Anticholinergics Akinetic mutism
☛ Amphetamines ☛ The patient follows with the eyes but
☛ Psychotropics does not initiate other movements or
☛ Lithium obey commands. The patient's tone,
☛ Phencyclidine reflexes (including response to cold
☛ Other hypnotics caloric stimulation), and postural reflexes
☛ Tranquilizers usually remain intact
☛ Bromides ☛ A lack of motor response in an awake
☛ Paraldehyde individual might arise from injury to the
☛ Monoamine prefrontal or premotor (including
oxidase supplementary motor) areas responsible
inhibitors for initiating movements
Psychiatric Psychogenic unresponsiveness
☛ Catatonia ☛ Patients with psychogenic
Other unresponsiveness often resist passive
☛ Postictal eye opening, roll over when tickled to
seizure avoid the stimulus, turn the eyes towards
☛ Diffuse the floor regardless of which side they
ischemia are lying on, or demonstrate nonepileptic
(myocardial seizures
infarction, heart ☛ The presence of nystagmus with caloric
failure, stimulation in an apparently comatose
arrhythmia) patient supports a diagnosis of
☛ Hypotension psychogenic unresponsiveness, but is not
☛ Fat embolism perfectly specific for this diagnosis
☛ Nonconvulsive
status
epilepticus
☛ Heat stroke

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1.5 HEENT
1.5.1 physical Examination findings
1.5.2 Icteric sclera
The differential diagnosis for yellowish discoloration of the skin is limited. It
includes:

➢ Jaundice → refer under long case of Nitsbin (discussion section of


CLD)
➢ The use of the drug quinacrine
➢ Excessive exposure to phenols
➢ Carotenoderma → It occurs in healthy individuals who ingest
excessive amounts of vegetables and fruits that contain carotene,
such as carrots, leafy vegetables, squash, peaches, and oranges.
o Carotenoderma can be distinguished from jaundice
by the sparing of the sclerae.

Pale conjunctiva
1.6 LGS
1.6.1 physical Examination findings
1.6.2 LAP

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Chapter 2; common medical procedures and result analysis

Chapter 2; common medical


procedures and result analysis
Dr. Mulualem. G

2.1 LP (Lumbar puncture)


Indications Contra indications CXN
DIAGNOSIS ABSOLUTE Post puncture headache
☛ CNS infection (meningitis, ☛ Clinical evidences of increased Epidermoid tumour
encephalitis…) ICP due to CNS mass or Infection
☛ SAH obstructive Hydrocephalus. Cerebral herniation
☛ NPH ☛ CT evidence of shift Spinal Hematoma
☛ CNS/PNS Demyelinating ☛ Active Bleeding disorders
disorders ☛ Skin infection at LP site
☛ CNS Inflammatory disorders RELATIVE
Therapeutic ☛ Respiratory pattern like RDS
☛ Therapeutic LP for ☛ HTN, Bradycardia with LOC
cryptococcal meningitis → ☛ Acute spinal trauma and
Control of raised ICP: daily vertebral deformity
LP with withdrawal of 20-30ml ☛ LOC with hypotension
of CSF ☛ Status epilepticus
☛ For communicating
hydrocephalus and NPH
☛ Treatment of Idiopathic ICP
☛ Spinal artery ischemia
Others
☛ Infusion of anesthesia and
Intra-thecal chemotherapy
☛ Instillation of contrast like CT
myelography, cisternography

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Positioning
✓ Positioning depends on what is required from LP
✓ To increase yield use sitting posture
✓ For treatment purpose use sitting posture
✓ To reduce post LP headache, use fetal posture
✓ To measure CSF pressure, use fetal posture

L3-L4, L4-L5, and L5-S1 interspaces are appropriate for needle puncture. These
interspaces can be identified via palpation of bony landmarks

Procedure
Cleanse skin with povidone iodine from puncture site radially out to 10cm to allow to
dry
Drape below patient and around site with fenestrated drape
Anesthetize with lidocaine if topical not used by
✓ Intradermally raising a wheal at needle insertion site
✓ Advance needle through wheal to desired interspace → careful not to inject into
a blood vessel or spinal canal
Insert spinal needle with stylet with bevel up to keep cutting edge parallel with nerve
and ligament fibers

LP: Resulting in a “pop” with sudden decrease in resistance when the dura is pierced
and the subarachnoid space is entered

if instead CSF does not flow. The stylet should be replaced, the needle advanced or
withdrawn incrementally, with frequent removal of the stylet Until CSF is obtained or
bone encountered.
When CSF flows
☛ Take adequate sample: If needed 20 up to 30 ml
☛ Observe the appearance: Color/Consistency/Pressure
☛ If contaminated with blood: Wait until CSF clears
When CSF flows, attach a monometer to obtain pressure if desired. Pressure can only
be accurately measured in lateral decubitus position and in relaxed patient
Attach manometer with a 3-way stopcock when free flow of CSF is obtained
Read column when highest level is achieved and respiratory variation noted
The recommended studies include (this order can be changed); collect 1ml of CSF in
each of vials
✓ Tube # 1; gram stain, culture and sensitivity
✓ Tube # 2; Glucose and protein
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✓ Tube # 3; cell count and differentials


✓ Tube # 4; any special studies you require (fungal/viral/chemical studies)
Check closing pressure with manometer if desired
Re insert stylet and remove needle in one quick motion
Cleanse back and cover puncture site

LP - Click on the link below and watch the video

https://youtu.be/YmzDT-LXQPY

2.1.1 CSF analysis

Opening pressure
✓ Normal value is 70 - 180 mmH2O → see tables below
✓ Measured with manometer
✓ In our set up since we don’t have manometer, we use flow rate to estimate
opening pressure
☛ Dropping → normal opening pressure
☛ Continues flow (i.e. stream like flow) → increased opening pressure
which may suggest increased ICP and give special attention for this
patient.
Appearance and CSF pressure
☛ Turbidity
✓ Crystal clear → normal
✓ Cloudy → bacterial, TB, fungal
✓ Clear → viral
☛ Color → normal CSF has crystal color
✓ Bloody (hemorrhagic) → SAH (usually xanthochromic), traumatic
✓ If CSF is bloody, how do you differentiate traumatic CSF from SAH
Traumatic CSF SAH
Blood stopes with in short Continuous blood comes
period of time and you may throughout the procedure
see clear CSF Blood in CSF doesn’t clot
Blood in CSF clots after after centrifugation
centrifugation Xanthochromic in color (due
Bright red blood to hemolysis → bilirubin →
yellow in color)

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☛ Viscosity
Microscopic and Microbiologic tests
☛ Cell count with differential
☛ CSF organisms (gram stain)
✓ CSF gram stain has 60-90% sensitivity
☛ CSF Cytology
☛ CSF culture → has 70-80% sensitivity
Chemical analysis
☛ Glucose
☛ Protein
☛ Lactate and LDH
☛ PH
☛ Glutamine and acid-base tests
Specific tests

N.B CSF analysis in our set up

In our set up, we usually collect 2-3 ml of CSF with one bottle
(rather than using 4 bottles as a standard) and we request with
different request papers like below
✓ Request # 1; cell count with differentials
✓ Request # 2; Gram stain and AFB
✓ Request # 3; Glucose and protein
✓ Request # 4; culture
You may keep the sample for other available investigations
based on indication like
✓ Gene expert → TB meningitis
✓ Cytology → carcinomatous meningitis
✓ Indian ink → cryptococcal meningitis especially in RVI Pt

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N.B Rule of 2 → has > 98% specificity for bacterial meningitis


➔ CSF WBC > 2,000
➔ Glucose < 20
➔ Total protein > 200

Table 1: CSF findings in different forms of meningitis


Appear Opening Cell count or WBC Glucose Protein (mg/dL) Microbiology
ance Pressure count (per µL) with (mg/dL)
(mmH2O) dominant differential
count *
Normal 70-180 0-5; lymphocytes 50-75 15 – 45 No organisms
Aseptic 90-200 10-300; lymphocytes Normal Normal, may Negative finding on
meningitis clear be Slightly  workup
Viral Viral isolation, PCR
meningitis
Bacterial 200-300 100-5000; >80% PMNs < 40 High (> 100) Gram stains +ve in > 60%
meningitis (low) & Culture +ve in > 80%
Tuberculous cloudy 180-300 100- 1000; < 40 High (> 100 AFBs are infrequently
meningitis lymphocytes, (low) /100 - 800/) seen (+ve in upto 40% of
sometimes with a cases) on direct smear
predominance of of CSF sediment
neutrophils in the early Culture +ve in 50 - 80%,
stage gold standard
Gene X-pert, has
sensitivity of up to 80%
and is the preferred
initial diagnostic option
Cryptococcal 180-300 10-200; lymphocytes Reduced High (50-200) India ink (+ve 60-80%),
meningitis cryptococcal antigen (>
95 % sensitive and
specificity), culture (+ve
95-100%)
* Cell count values are variable from reference to reference. So, for clinical practice differentiate either
neutrophil dominance (bacterial meningitis) or lymphocyte dominance (other than bacterial meningitis), cell
count in thousands (bacterial meningitis) or in hundreds (other than bacterial meningitis).

Table 2; normal CSF composition

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Composition of the Cerebrospinal Fluid


☛ CSF resembles water; the protein content is low
☛ No more than 5 lymphocytes and a neutrophil are present.
☛ Glucose values are 2/3rd of those in blood.
☛ CSF glucose concentrations <2.2 mmol/L (<40 mg/dL) are abnormal,
☛ And a CSF glucose concentration of zero can be seen in bacterial meningitis.
☛ Use of the CSF/serum glucose ratio corrects for hyperglycemia that may mask a
relative decrease in the CSF glucose concentration.
☛ The CSF glucose concentration is low when the CSF/serum glucose ratio is <0.6.
☛ A CSF/serum glucose ratio <0.4 is highly suggestive of bacterial meningitis but
may also be seen in other conditions, including fungal, tuberculous, and
carcinomatous meningitis.
☛ It takes from 30 min to several hours for the concentration of CSF glucose to
reach equilibrium with blood glucose levels; Therefore, administration of 50 mL of
50% glucose (D50) prior to LP, as commonly occurs in emergency room settings,
Is unlikely to alter CSF glucose concentration significantly unless more than a few
hours have elapsed between glucose administration and LP.



Some IgG is produced in the brain and proteins are scarce
Higher levels of sodium, chloride, and magnesium and PCO2
Lower levels of potassium, calcium, bicarbonate and PH
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2.2 Pleural tap (thoracentesis)


Indications Contra indications CXN
Diagnostic Anticoagulation or a Pain at the
newly detected pleural effusion bleeding diathesis: puncture site
☛ to determine the nature of the effusion (ie, transudate, ✓ with a PT or PTT > Bleeding (e.g.
exudate) and to identify potential causes 2x midpoint of the bleeding from
☛ A unilateral effusion, especially if it is left-sided normal range (INR intercostal
☛ Bilateral effusions that are of disparate sizes >2), vessel creating
Atypical features that should prompt consideration of ✓ a platelet count < subcutaneous
diagnostic thoracentesis in a patient with suspected HF 5O,000 /mm3, hematoma,
☛ alternate etiology of the effusion (eg, bilateral effusions ✓ a serum Cr > 6 haemothorax, or
of significantly disparate sizes (especially if the effusion mg/dL hemoperitoneum)
on the left is larger than on the right) insufficient pleural fluid Pneumothorax
☛ symptoms of pleurisy ✓ <1 cm distance from Infection
☛ fever the pleural fluid line (empyema, soft
to the chest wall on tissue infection)
☛ features suggestive of infection or cancer
a decubitus chest Laceration of
☛ an echocardiogram that is inconsistent with HF
radiograph lung.
☛ a disproportionately high alveolar-arterial oxygen
Mechanical ventilation: Spleen or liver
gradient, and/or the lack of resolution with effective HF
✓ bronchopleural puncture (don’t
therapy.
fistula, if a go below 9th
☛ Normal cardiac silhouette on chest radiograph
pneumothorax does ICS)
☛ An echocardiogram that is inconsistent with heart occur Vasovagal
failure Active skin infection at events
the point of needle Seeding the
Therapeutic insertion needle tract with
tumour
symptom relief (eg, dyspnea) NB: - There is no absolute Re-expansion
if the fluid has imaging characteristics of a complicated contraindication for pulmonary
pleural effusion (eg, loculations suggesting a thoracentesis oedema (caused
parapneumonic pleural effusion) by withdrawal of
pleural conditions that risk pleural thickening and restrictive > 1000ml fluid
functional impairment, such as effusions due to post- at once)
primary or reactivation tuberculosis and hemothorax.
Therapeutic removal of small pneumothorax.

Equipment’s
✓ Sterile gloves, mask, and gown.
✓ Iodinated skin preparation with sterile sponges.
✓ Sterile towels.
✓ Local anaesthetic (1% lidocaine without epinephrine).
✓ 5-mL syringe with 25-gauge needle.
✓ 18-gauge 2-inch needle.
✓ Collection basin.
✓ 3-way stopcock.
✓ 20-60ml syringe.
✓ For therapeutic tap, in our setup, we were using IV set with needle tip and locally
available Highland/or empty RL bag as a container for fluid collection

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Patient preparation
➢ Patient should have intravenous access.
➢ Oxygen should be available.
➢ Monitor oxygen saturation with pulse oximetry.
➢ Younger patients may need sedation for procedure.
➢ Explain procedure before and during procedure.

Patient positioning
Pleural effusion.
☛ Sitting upright with arms supported on table in front of patient
☛ Lying in lateral decubitus position with effusion side down.
Pneumothorax: Supine with head of bed up 30 degrees.

procedures
Locate Effusion
✓ Chest radiograph.
✓ Manual percussion to find onset of dullness.
☛ One to two interspaces below the level at which breath sounds decrease or
disappear on auscultation, percussion becomes dull, and fremitus
disappears.
☛ Above the ninth rib, to avoid subdiaphragmatic puncture.
☛ Midway between the spine and the posterior axillary line, because the ribs
are easily palpated in this location.
✓ Effusion is usually accessible via the sixth or seventh intercostal space just distal
to the scapular tip in the mid scapular line or posterior axillary line
✓ If pneumothorax is present, it is usually accessible via the second intercostal space
anterior
Ultra-sonogram marked location.
✓ Mark location of effusion with the patient in the same position as necessary for
procedure.
✓ If possible, do not move patient after marking the location because the fluid may
shift.
Use a 25-gauge needle and 5-ml syringe to infiltrate the skin and make a wheal
under the skin.
Change needle to 18 gauge with 2-inch needle.
Going over top of sixth rib, infiltrate through wheal, over top of rib to anesthetize
the periosteum, and into pleural space.
Be sure to aspirate first, and know when you are in the pleural space.
The parietal pleura needs to be anesthetized. but, to avoid a puncture of the lung,
do not advance the needle further.
When in the pleural space, a ‘pop’ may be felt and fluid or air will enter syringe.

Removal of Pleural Effusion for Diagnostic Evaluation


➢ Remove lidocaine syringe and needle to outside the pleural space, with needle still
inserted but outside the pleural space; replace syringe with empty 20-60 ml
syringe.
➢ Reinsert needle into pleural space while applying gentle negative pressure on
syringe.
➢ When in pleural space, a ‘pop’ may be felt and fluid or air will enter syringe.
➢ Remove effusion into syringe.
➢ Remove needle and apply bandage to area.
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Thoracentesis - Click on the link below and watch the video


https://youtu.be/UBY3cQiQ6Ko

2.2.1 Pleural fluid analysis

1. Gross appearance
✓ Pale yellow (Straw) → transudative effusion, some exudates
✓ Milky → chylothorax (thrombus in left subclavian vein, malignancy, trauma,
TB)
✓ Bloody → haemothorax (malignancy, trauma, TB, pulmonary infarction),
traumatic procedure
✓ Frank pus → empyema (TB, pulmonary infection, trauma, oesophageal
rupture)
✓ Turbid → inflammatory exudate

2. Cell count with differentials


3. Gram stain and AFB
☛ AFB +ve in 10 - 25% of TB pt’s
4. Glucose and protein routinely done in our set up
5. Culture
☛ +ve in 25 - 75% of TB pt’s
6. Gene x-pert (X-pert MTB/RIF)
✓ 75% +ve

7. Others
☛ PH
☛ Cytology → sensitivity of approximately 60 % for the diagnosis of
malignant effusion (sensitivity in lung cancer; 78 % for
adenocarcinoma, 53 % for small cell carcinoma, and 25 % for
squamous cell carcinomas)
☛ LDH
☛ Amylase → increase in acute/chronic pancreatitis (one cause of exudative
effusion)
☛ ADA (Adenosine deaminase)
o may be helpful to distinguish between malignant and
tuberculous pleurisy when an exudative effusion is
lymphocytic, but initial cytology and smear and culture for
tuberculosis are negative
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o > 35 to 50 U/L in tuberculous pleural effusions (The most


common diagnostic threshold used to establish tuberculous
pleural effusions is a value >40 U/L)
o < 40 U/L in 94 % of malignant pleural effusions.

N.B
Pleural tap should be done
☛ over the area of dullness
☛ above the rib to avoid neurovascular injury
don’t go below 9th ICS to avoid visceral injury
estimated volume of fluid to be drawn
☛ for culture → 20 ml
☛ for cytology → 20 ml
☛ for biochemical and microbiology (protein, glucose, cell count, gram stain
and AFB, LDH, PH) → 10 ml

Lights Criteria
Characteristics Transudative Exudative
1. Pleural fluid protein / < 0.5 > 0.5
serum protein ratio
2. Pleural fluid LDH / < 0.6 > 0.6
serum LDH ratio
3. Pleural fluid LDH < 2/3rd the upper limit of > 2/3rd the upper limit of
the normal laboratory the normal laboratory
serum LDH level serum LDH level
At least One of the three criteria should qualify to diagnose exudative effusion

other Criteria
Criteria Transudative Exudative
1. Cell count < 100 x106 / L > 500 x106 / L
2. Differential cell Lymphocyte Different
3. Pleural fluid LDH < 0.45 times the upper > 0.45 times the upper
normal limit serum LDH normal limit serum LDH
4. LDH < 200 IU/ L > 200 IU / L
5. Pleural fluid cholesterol < 45 mg/dL > 45 mg/dL
6. Pleural fluid protein < 3 g/dL (<30g/L) > 3 g/dL (>30g/L)
7. Cause non-inflammatory inflammatory, tumour
8. Appearance light yellow yellow, purulent
9. pleural fluid pH 7.40 to 7.55 7.30 to 7.45
10. Specific gravity <1.018 >1.018
NB: - CHF patients with acute diuresis can have pleural fluid protein > 3g/dl;
However, such patients have a pleural fluid to serum albumin gradient > 1.2 g/Dl

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DDX for some abnormal pleural fluid analysis findings


LDH > 1000 IU/L
☛ Empyema
☛ Malignancy
☛ Rheumatoid disorders (SLE, RA)
Glucose
Glucose < 30 mg/dl
☛ Empyema
☛ Rheumatoid disorders
Glucose between 30 - 50 mg/dl
☛ SLE
☛ Malignancy
☛ TB
Lymphocytes
Lymphocytes 85% - 95 %
▪ TB
▪ Lymphoma
▪ Chylothorax
▪ Sarcoidosis
▪ Rheumatoid disorders
Lymphocytes between 50 - 70%
▪ Malignancy
Eosinophilia — defined by pleural fluid eosinophils representing >10 % of the
total nucleated cells
o Pneumothorax, Hemothorax, Pulmonary infarction
o Parasitic disease
o Fungal infection (coccidioidomycosis, cryptococcosis,
histoplasmosis)
o Malignancy (carcinoma, lymphoma, myeloma)
o Tuberculous pleurisy
o Parapneumonic effusions
o Chronic eosinophilic pneumonia
o Drugs
o Benign asbestos pleural effusion
Mesothelial cells
▪ prominent in transudative pleural effusions, and are variable in
exudative effusions.
▪ in exudative effusion; tuberculosis is unlikely if there are > 5%
mesothelial cells
ADA
▪ > 35 - 50 U/L (especially when lymphocytes > 75%) Supports TB
▪ < 40 U/L, suggests malignancy, rarely caused by TB
Amylase: pleural/serum Amylase ratio > 1.0
▪ Acute/chronic pancreatitis
▪ Oesophageal rupture
▪ Malignancy

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2.3 Peritoneal tap (paracentesis)

Indications Contra indications CXN


Diagnostic sampling of ascitic Absolute: - Pneumoperitoneum.
fluid ▪ Unstable airway. Perforation: Intestine, organ.
✓ e.g. identification of infectious ▪ Hemodynamically unstable Bleeding.
organism in spontaneous patient. Infection.
bacterial peritonitis. internal ▪ Intestinal perforation. Leakage of ascitic fluid
bleeding following blunt Relative: - Hypoproteinaemia if repeated
abdominal trauma, chylous ▪ Infection of the abdominal wall. tapping done
ascites after surgery, rule out ▪ Coagulopathy (prothrombin time
malignancy, > 18 seconds).
Therapeutic removal of the huge ▪ Thrombocytopenia (platelet
ascitic fluid count <100,000/µl).
▪ Recent intestinal tract surgery
(< 1 month ago).

Equipment
☛ Alcohol swabs, povidone-iodine.
☛ 23-gauge and 21-gauge needles or angiocatheters with syringes.
☛ Local anesthetic (e.g. 1% lidocaine).
☛ Large bore needle with plastic catheter.
☛ Sterile containers for fluid collection.
☛ Appropriate culture tubes for microorganisms.
☛ For therapeutic tap, in our setup, we were using IV set with needle tip and locally
available Highland/or empty RL bag as a container for fluid collection

Patient preparation and position


✓ Explain indication and risks to the patient.
✓ Inform the patient of the intention of the procedure.
✓ Supine or side.

Procedure
☛ The puncture site should be shaved, if necessary, and cleansed with povidone-
iodine.
☛ Inject local anaesthetic, infiltrating the skin first and then penetrating into deeper
layers.
☛ A small 3-mm incision can be made with a scalpel to help insert the needle. Using
Z-track technique (to prevent fluid leakage), insert the tap needle 1-2 inches into
the abdomen
☛ Obtain a sample of fluid or withdraw as much fluid as necessary with a syringe (in
case of therapeutic lavage)
☛ Remove the needle and apply a pressure dressing to the puncture site.
☛ If an incision was made, it may be closed using 1 or 2 stitches.
☛ The ascitic fluid removed may be replaced 1:1 with 5% albumin IV. 920
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Paracentesis - Click on the link below and watch the video


https://youtu.be/0bvMt-A6VhQ

2.3.1 Ascitic fluid analysis


a) Inspection of gross appearance
☛ Straw coloured → cirrhosis, budd chiarry sxx, CHF, constrictive pericarditis,
meig’s sxx
☛ Chylous (milky) → lymphatic obstruction
☛ Haemorrhagic (bloody) malignancy, abdominal trauma, TB, acute pancreatitis
☛ Cloudy → TB
b) Cell count
✓ Normal → WBC < 500/ml, neutrophil < 250/ml
✓ Neutrophil dominant → bacterial peritonitis

Bacterial peritonitis
SBP Secondary peritonitis due to rupture of abdominal
viscus
✓ WBC > 500/mm3 ✓ WBC > 10,000/mm3 (significant leucocytosis)
(neutrophil ≥ 50%) ✓ Multiple organisms identified
✓ Mono microbial ✓ Increased LDH level
✓ Glucose < 50
✓ Protein significantly decreased
✓ PH
✓ With obvious cause of 2ry peritonitis like
intestinal perforation
✓ Failure to improve after standard treatment
with in 48 hr’s

✓ Lymphocyte dominant
☛ TB peritonitis
☛ Abdominal carcinomatosis
c) Glucose and protein
d) Gram stain and AFB
e) Culture → inoculation at bedside increase sensitivity to 85% to identify infection
f) SAAG (serum ascitic albumin gradient)
☛ SAAG = serum albumin level - ascitic albumin level
☛ SAAG > 1.1 g/dl → Cause of ascites is most likely Portal HTN (e.g.
cirrhosis, chronic hepatic congestion from CHF)
☛ SAAG < 1.1 g/dl → Non-Portal HTN (e.g. TB peritonitis, Nephrotic sxx,
peritoneal carcinomatosis, hypalbuminemia)
☛ 95% accurate but can’t r/o malignancy
☛ Ascitic fluid protein < 1g/dl predispose to SBP
g) Other
✓ RBC → > 50,000 RBC/µl suggest haemorrhagic ascites
✓ PH → PH < 7 suggest bacterial infection
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✓ Cytology → for malignancy


✓ Amylase → increased level in ascites 2ry to chronic pancreatitis

N.B Ascitic fluid analysis in our set up

In our set up, we usually collect ascitic fluid with one bottle and we request with
different request papers like below
✓ Request # 1; cell count with differentials
✓ Request # 2; Gram stain and AFB
✓ Request # 3; Glucose and protein
✓ Request # 4; culture
If you suspect peritoneal carcinomatosis, you have to request cytology from ascitic fluid

2.4 BM aspiration

Indications Contra indications CXN


VL Absolute Bleeding at any site, with or
Diagnosis and staging of Osteomyelitis without development of a
hematologic disease Infection at the site of puncture hematoma
Myeloproliferative disease Relative ✓ rare if adequate pressure
Unexplained Pancytopenia Congenital factor deficiency or is applied.
assessment of overall bone acquired coagulation defect. ✓ Bleeding risk has been
marrow cellularity. Anticoagulation with warfarin or reported to be increased in
Bone marrow failure (including heparin. those with osteoporosis or
acquired aplastic anemia, Fanconi Severe thrombocytopenia extensive bony involvement
anemia, Diamond- Blackfan Infection or prior radiation at by disease, such as
syndrome). sample site. multiple myeloma.
Fever of unknown origin. Retroperitoneal haemorrhage
Storage disease. Osteomyelitis
Monitoring during chemotherapy needle breakage
or following stem cell Infection (rare)
transplantation (aspiration only). Bone pain

Equipment
Site Preparation
❖ 10% povidone-iodine.
❖ Alcohol preparation pads or swabs.
❖ Sterile gloves, gown, and drape
❖ Spinal and subcutaneous needles, 20 to 26 gauge.
❖ 1% lidocaine hydrochloride, injection.
❖ 8.4% sodium bicarbonate, injection, USP

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Marrow Aspiration
✓ Bone marrow aspiration needles
Biopsy aspiration needles recommended
sizes
Regular/Adults 4-inch, 11-gauge
Adults: 4-inch, 8-gauge
Orthopedic: 6-inch, 10/11-
gauge
Pediatric: 3½-inch, 13-gauge
Infant: 2-inch, 13-gauge

✓ Sterile syringes, 10 to 20 mL
✓ clean microscope slides
✓ wooden applicator or tooth picks
✓ spirit lamp with sufficient flame
✓ sterile cotton and gauze
✓ plaster, labels, pen and pencil/marker
✓ Container with fixative for trephine biopsy specimen.
✓ Vacutainers; one for sodium heparin and one for EDTA (ethylene diamine tetra
acetic acid).
✓ Bandages.

Choice of site
Posterior superior iliac spine
Anterior iliac crest in obese patients
1st part of body of manubrium of sternum

Procedure
Place the patient in a right or left lateral decubitus position with the back
comfortably
flexed and the top knee drawn toward the chest.
Locate the posterior iliac spine and mark it with ink or thumb nail pressure.
Using sterile technique, prepare the skin with anti-septics and drape.
Using a sterile syringe, infiltrate the marked area with local anesthesia especially
the periosteum.
Make a 3-mm skin incision with a scalpel blade over the marked area
Hold the needle with the proximal end between the palm and the index finger
against the shaft near the tip.
With the stylet locked in place, introduce the needle through the incision pointing
toward the anterior superior iliac spine and bring it into contact with the posterior
iliac spine.
Using gentle but firm pressure, advance the needle to bore through the iliac spine.
Rotate the needle in an alternating clock-wise and counter-clockwise motion.
Entrance into the marrow cavity is generally detected by decreased resistance.
Remove the stylet, and check for marrow material. If not present, proceed to bore
until marrow is found in the tips of the stylet.
With a syringe locked into the proximal portion, apply a negative pressure.
This first pull contains the marrow particles or spicules that should be used for
preparing initial smears.
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A heparinized, larger syringe (30 mL) may be used to obtain additional marrow for
cytogenetic analysis, flow cytometry, and other studies.

Bone marrow aspiration - Click on the link below and watch the video
https://youtu.be/svTQ-zJHY9M

2.5 Splenic Aspiration

Indications Contra indications CXN


VL Massive splenomegaly Bleeding
Haematologic malignancy Small spleen → led to bleeding to the extent of Splenic rupture to the
splenectomy extent of death
Thrombocytopenia (platelet count < 40,000/ml)
Massive ascites
Overlying skin infection
severe anemia (hemoglobin ≤ 5 g/l)
difference in prothrombin time between patient
and control > 5 s
signs of active bleeding (e.g. epistaxis, rectal
bleeding, skin bruises)
jaundice (a potential marker of liver dysfunction)
pregnancy → spleen barely palpable
bad general condition (e.g. cardiovascular shock,
altered consciousness)

Prerequisite
❖ The two important prerequisites for the safety of the procedure are;
• Rapidity so that the needle remains within the spleen for less than l second
and
• precision so that the entry and exit axes of the aspirating needle are
identical to avoid tearing the splenic capsule.
❖ splenic aspiration should be performed in a hospital setting where blood transfusion
is possible because the procedure is associated with a risk of fatal internal
bleeding.
❖ This procedure also requires considerable technical expertise for making the
aspiration and facilities for nursing surveillance, blood transfusion, and surgery.

Procedure

i. Clean three glass slides and label them. If culture medium is required, label in the same
way as the slides. Attach a 11/4-inch × 21-gauge (32 × 0.8-mm) needle to a 5ml syringe.
ii. Inform the patient about the procedure. Check all clinical and biological contraindications
again. Palpate the spleen and outline its margins on the patient’s abdomen with a pen.
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Chapter 2; common medical procedures and result analysis

For safety, the spleen should be palpable at least 3 cm below the costal margin on
expiration. Use an alcohol swab to clean the skin at the site of aspiration and allow the
skin to dry.
iii. With the 21-gauge (0.8 mm) needle attached to the 5ml syringe, just penetrate the
skin, midway between the edges of the spleen, 2–4cm below the costal margin. Aim
the needle cranially at an angle of 45° to the abdominal wall. The actual aspiration is
done as follows:
❖ pull the syringe plunger back to approximately the 1ml mark to apply suction and
with a quick in-and-out movement push the needle into the spleen to the full
needle depth and then withdraw it completely, maintain suction throughout.
iv. For young, restless children, have two assistants hold the child (arms folded across the
chest, with shirt raised to obstruct the line of vision, and pelvis held firmly). Carry out
the aspiration as a single-stage procedure using the same landmarks, angles and suction
as in
step 3 – all in one quick motion. The insertion should be timed with the patient’s
breathing so that the diaphragm is not moving. This should be done during fixed
expiration if the child is crying. Only a minute amount of splenic material is obtained for
culture and smear.
v. If culture is available: slowly pull the plunger back to the 2–3ml mark and, by using
sterile techniques, insert the needle into a tube containing culture medium and briskly
push the plunger into the barrel to expel the contents of the needle onto the side walls
of the tube. If necessary, repeat once or twice until splenic material is visible in the
tube. Replace the cap on the tube and invert to wash splenic material on the side of
the tube. Repeat the procedure for the second tube of culture medium. Sterile
techniques are essential throughout.
vi. Expel material gently onto glass slides, holding the needle tip on the surface of the
slide. Immediately spread evenly with the needle, using a linear (not circular) motion.
The smear should be slightly thinner than a thick blood film for malaria. Remove the
needle and use the end of it to obtain additional material from the tip of the syringe and
spread it on slides. Further material found on the end of the plunger may be dabbed
directly onto a slide and spread. Allow the slides to dry.
vii. Write the time of aspiration on the patient ‘s chart with the instructions: “Record pulse
and blood pressure every half hour for 4 hours, then every hour for 6 hours. Patient
must remain in bed for 12 hours!” Ensure that the patient understands the instructions.
Enter the procedure in the notes and sign.
viii. Take the slides (and medium) to the laboratory for preparation and microscopic
examination.

Splenic aspiration - Click on the link below and watch the video
https://youtu.be/6egWxe4VFT4

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Chapter 2; common medical procedures and result analysis

2.6 LN aspiration

Indications Contra indications CXN


TB lymphadenitis
VL
Lymphoma
Sentinel LN of any malignancy

Materials required:
❖ Sterile needle (21G)
❖ Syringe (10ml)
❖ Clean glass slide
❖ Iodine (disinfectant) or sterile cotton swabs
❖ Cotton wool

Procedure
❖ Allow the patient to lie comfortably. Prepare the syringe by pulling the piston
back as far as possible.
❖ Feel and locate a swollen gland.
❖ Disinfect the chosen site with swollen glands using a piece of cotton wool soaked
in iodine or another suitable disinfectant.
❖ Take the gland between the thumb and index finger of the left hand. Hold it
steady and make it at the same time standing out.
❖ Introduce the needle with a right angle into the center of the gland in two stages:
• First pierce the skin
• Second penetrate the gland
❖ With your left hand, gently knead the gland. With your right hand, revolve the
needle in both directions. The glandular fluid will ooze into the needle.
❖ Withdraw the needle in one rapid movement while holding the thumb over
the hub. Then apply a swab dipped in iodine to the point of entry.
❖ Attach the syringe (piston pulled back) to the needle. Place the needle on the
slide. Push the piston gently down the barrel to discharge the glandular fluid
contained in the needle onto the slide.
❖ Make a thin film using the fluid on the slide. The fluid can be discharged in more
than one slide.

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Chapter 3; Shock

Chapter 3; Shock
Dr. Mulualem. G

✓ Shock is the clinical condition of organ dysfunction resulting from an imbalance


between cellular oxygen supply and demand.
✓ There are a multitude of heterogeneous disease processes that can lead to
shock.
✓ The organ dysfunction seen in early shock is reversible with restoration of
adequate oxygen supply.
✓ Left untreated, shock transitions from this reversible phase to an irreversible
phase and death from multisystem organ dysfunction (MSOF).

Classification of shock

✓ While there is a heterogeneous list of specific conditions that can


cause shock, it can be classified into four major shock types based on the
primary physiologic derangement leading to reduced oxygen delivery and
cellular hypoxia.
✓ The four major shock types are
o Distributive
o Cardiogenic
o Hypovolemic, and
o Obstructive

Major shock types and specific disease processes that can result in that
physiologic derangement.

Hypovolemic shock
❖ Hemorrhagic shock
❖ Non hemorrhagic
▪ GI losses
▪ Burns
▪ Polyuria
• DKA
• Diabetes insipidus
Cardiogenic shock
❖ Myocardial infarction
❖ Myocarditis
❖ Arrhythmia
❖ Valvular
▪ Severe aortic valve insufficiency
▪ Severe mitral valve insufficiency
Obstructive shock
❖ Tension pneumothorax
❖ Cardiac tamponade
❖ Restrictive pericarditis
❖ Pulmonary embolism
❖ Aortic dissection
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Chapter 3; Shock

Distributive shock
❖ septic shock.
❖ Anaphylactic shock
❖ neurogenic shock
❖ Pancreatitis
❖ Severe burns
❖ Endocrine shock
❖ Adrenal crisis

Table; Hemodynamic Characteristics of the Major Types of Shock


Type Hemodynamic change
Preload Afterload SVR (systemic CO (Cardiac
vascular resistance) output)
Hypovolemic Decreased
Cardiogenic Increased Increased Increased Low
Obstructive Decreased
Distributive Decreased Decreased High

Mixed Shock

The types of shock outlined in this classification scheme are not mutually
exclusive; not uncommonly, a patient will present with more than one type of
shock.
The initial physiologic disturbance leading to reduced perfusion and cellular
hypoxia in sepsis is distributive shock. In this setting, a sepsis-induced
cardiomyopathy can develop, which reduces myocardial contractility, thus
producing a cardiogenic component to what now would be described as a
mixed type of shock.

Undifferentiated Shock

Upon initial presentation, many patients have undifferentiated shock in which


the shock type and specific disease process are not apparent.
The type of shock seen most commonly is dependent upon the clinical area of
practice.
o In the medical ICU, the largest number of patients have distributive
shock related to sepsis.
o A cardiac ICU will have a population weighted toward cardiogenic or
obstructive types of shock.
o The emergency department will see more of a mix of patients with
trauma patients presenting with hypovolemic shock and septic patients
having a distributive pathophysiology.

Stages of shock
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Chapter 3; Shock

❖ Regardless of type, shock progresses through a continuum of three


stages. These stages are;
• Compensated shock (pre-shock)
• Shock (decompensated shock), and
• Irreversible shock.
❖ Compensated shock
• The body utilizes a variety of physiologic responses to counteract the
initial insult and attempts to reestablish the adequate perfusion and
oxygen delivery.
• At this point, there are no overt signs of organ dysfunction.
• Laboratory evaluation may demonstrate mild organ dysfunction (i.e.,
elevated creatinine or troponin) or a mild elevation of lactate.
• The specific compensatory response is determined by the initial
pathophysiologic defect.
• In early sepsis with reduction in SVR, there is a compensatory rise
in HR (and CO).
• With early hemorrhagic volume loss, there will be a compensatory
increase in SVR.
❖ Shock (decompensated shock)
• As the host compensatory responses are overwhelmed, the patient
transitions into true shock with evidence organ dysfunction.
• Appropriate interventions to restore perfusion and oxygen delivery
during these initial two phases of shock can reverse the organ
dysfunction.
❖ Irreversible shock
• If untreated the patient will progress to the third phase of irreversible
shock.
• At this point, the organ dysfunction is permanent and often the
patient progresses to MSOF (multisystem organ failure).

Approach to shock patient

➢ This early recognition of the presence of shock is an essential tenet of


shock care.
➢ A second aim of the initial assessment (history, physical examination, and
diagnostic testing) is to identify either a specific shock etiology or to
determine the type of shock present.

Clinical feature of shock in general


➢ WHO criteria for shock
✓ SBP< 90mmhg
✓ Cold extremities
✓ Fast and weak pulse, or absent pulse
✓ Prolonged capillary refill time > 3 seconds (clinically 3 second is

History
approximated with counting ‘’1001, 1002, 1003 = 3sec’’)
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Chapter 3; Shock

Obtaining a concise, focused history is essential.


If the patient is unable to provide a history, ancillary information from anyone
accompanying the patient should be obtained, and a brief chart review should
be performed.
As the history is being obtained, the clinician must be attentive to any details
indicating new organ dysfunction.

➢ a newly altered mental status or decrease in renal function (oliguria).


➢ Patients with distributive shock from sepsis may present with fever and a
history revealing of a focal site of infection.
➢ Anaphylactic distributive shock may be suggested by
the onset of hives, dyspnea, and new facial edema after exposure to
common allergens.
➢ Cardiogenic shock may be identified by the onset
of exertional chest discomfort.
✓ The patient with significant arrhythmia may have an initial complaint
of palpitations with syncope or presyncope.
➢ Hypovolemic shock may be identified in patients who present
with a history of trauma (blunt or penetrating) or GI bleed (hematemesis,
melena, or bright red blood per rectum).
➢ Obstructive shock
✓ A patient with hypertension and tearing chest or back pain may be
presenting with acute aortic dissection and obstructive type shock.
✓ Acute onset chest pain with dyspnea in the setting of immobility and
or underlying malignancy raises concern for obstructive shock due to
pulmonary embolism.
➢ For most patients, the specific etiology will be less clear but the
history can be helpful in raising the likelihood of a particular type of
shock.
✓ As an example, a patient with a preexisting immune dysfunction
or medication-induced neutropenia may present with hypoperfusion
and new organ dysfunction, in which the clinician must have a high
suspicion for septic shock.
✓ Similarly, a patient with extensive cardiac disease requires a higher
suspicion for cardiogenic shock.

Physical Examination

The physical examination should be conducted with the aim of answering two
questions.
o Is shock present (either in compensated stage prior to overt evidence of
organ dysfunction or decompensated indicated by the presence of new
organ dysfunction)?
o Secondly, what type of shock is present (distributive, cardiogenic, 930
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Chapter 3; Shock

hypovolemic, or obstructive)?
The physical examination findings present during the compensated
phase of shock tend to be nonspecific. These include;
o Tachycardia → with the body’s attempt to increase CO
▪ Fast and weak pulse, or in severe cases, absent pulse
o Tachypnea → to compensate for the developing metabolic acidosis.
Hypotension (MAP of <60 mmHg or SBP < 90 mmHg)
o but this finding is not always present.
o Many patients may have underlying conditions that
cause longstanding low blood pressure without any evidence of organ
dysfunction.
o Alternatively, patients with underlying hypertension may
develop organ dysfunction at higher blood pressures.
The CNS, kidney, and skin examination are “windows” through which we can
identify organ dysfunction.
o Confusion and encephalopathy → due to decreased oxygen delivery to
the brain is manifest as
▪ In the early stage of shock, the body will redirect blood flow to
the CNS to maintain adequate perfusion. In the patient with
shock and altered mental status, all the usual compensatory
mechanisms have been outstripped by the magnitude of shock
pathophysiology.
▪ New encephalopathy represents decompensated shock.
o In patients with normal baseline renal function, oliguria
(<0.5 mL/kg per h) may indicate shock.
▪ a urinary catheter should be placed for accurate hourly
assessment of urine output
o Finally, decreased capillary refill and cold and clammy skin are signs of
hypoperfusion and shock.
Raised JVP and peripheral edema can provide insight into right-sided cardiac
pressures overload.
Pulmonary auscultation can identify signs of left-sided cardiac dysfunction.
The physical examination may be used to differentiate shock with high CO
(distributive)
from that with low CO (cardiogenic shock, hypovolemic shock, and
obstructive shock).
findings suggestive of high output shock (distributive) include;
o warm peripheral extremities
o brisk capillary refill (<2 s), and
o bounding pulses.
Findings suggestive of low CO shock (cardiogenic shock, hypovolemic shock,
and obstructive shock) include;
o cool extremities
o delayed poor capillary refill, or
o weak pulses
The JVP may be elevated cardiogenic shock (with right-sided failure) and
reduced (JVP <8 cm) in hypovolemic shock. 931
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Chapter 3; Shock

The presence of cardiogenic shock would be further supported by an S3


gallop.
Notice; patients with chronic heart failure do not present with the classical
findings of acute heart failure. At times, the physical examination may identify
the specific etiology of shock. This is particularly helpful in the patient who
cannot provide a detailed history.
Identify the site of untreated infection (cellulitis, abscess, infected pressure
injury, or focal) as a source of septic shock.
a brady- or tachyarrhythmia may be leading cause to development of shock.
large ecchymosis may indicate a significant bleed related to trauma or
spontaneous retroperitoneal bleeding.
The rectal examination may reveal GI hemorrhage.
Pulsus paradox and elevated JVP may suggest the presence of cardiac
tamponade.
Patients with a tension pneumothorax may have;
o a paucity of breath sounds over the affected side
o deviation of the trachea away from the affected
side, or
o subcutaneous emphysema.

Shock index (SI) and qSOFA score

➢ Combinations of easily assessed examination components have been


combined to create a scoring system to identify high risk patient
populations.
𝐻𝑅(𝐻𝑒𝑎𝑟𝑡 𝑟𝑎𝑡𝑒)
➢ The shock index (SI) = SBP(systolic blood pressure)
➢ normal SI = 0.5 - 0.7.
➢ An elevated SI (>0.9) has been proposed to be a more sensitive indicator
of transfusion requirement and of patients with critical bleeding among those
with hypovolemic (hemorrhagic) shock than either HR or BP alone.
➢ The SI may also identify patients at risk for postintubation hypotension.
➢ This concept of use of a clinical score to identify at-risk patients has been
extended to patients with distributive shock from sepsis.
➢ The quick Sequential Organ Failure Assessment (qSOFA) score is a rapid
assessment scale that assigns a point for;
✓ SBP <100
✓ RR >22, or
✓ altered mental status (GCS <15).
➢ A qSOFA ≥2 (with a concern for infection) is associated with a significantly
greater risk of death or prolonged ICU stay.

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Chapter 3; Shock

Initial Laboratory Evaluation of Undifferentiated Shock

CBC (with differential)


o An elevation of the WBC count may raise suspicion for an infective
process, but this is certainly not diagnostic; an accompanying left shift
may improve the sensitivity of this measure.
Urinalysis and urine sediment → to evaluate for pyuria.
RFT (BUN, creatinine)
LFT
PT, PTT, and INR
Cardiac enzymes → myocardial ischemia, myocarditis, or a pulmonary
embolism
Arterial blood gas
ECG
o There may be a bradycardia or tachycardic arrhythmia causing a
reduction in CO.
o ST segment elevation myocardial infarction may be identified.
o The presence of the S1 Q3 T3 pattern would raise concerns for
pulmonary embolism.
o Reduced voltage in the presence of electrical alternans raises the
possibility of pericardial tamponade.
Echo
o evaluate LV size, wall thickness, and ventricular function.
o Ventricular size and thickness can suggest longer standing cardiac
processes.
o Evaluation of LV function through estimation of left ventricular ejection
fraction (LVEF), and can identify shock with globally reduced LV function
or regional wall motion abnormalities.
o The assessment of RV function also examines RV size and wall
thickness (to identify conditions such as elevated pulmonary pressures
or suggest pulmonary embolism), and also evaluate the patient for
pericardial tamponade.
o also be used to assess valve function, including acute processes, such
as mitral valve rupture.
Sepsis workup
o CBC, U/A
o Cultures (Blood, urine, stool and sputum cultures)
o CXR
Lactate measurement (usually not applicable in our setup)
o It has a role in the diagnosis, risk stratification, and, potentially, the
treatment of shock.
o Increased lactate (hyperlactemia) and lactic acidosis (hyperlactemia and
pH <7.35) are common in shock.
o Lactate is a product of anaerobic glucose metabolism.

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Chapter 3; Shock

Management of shock

Key Principles in the Treatment of Shock


1. Recognize shock early
2. Assess for type of shock present
3. Initiate therapy simultaneous with the evaluation into the etiology of shock
4. Restoration of oxygen delivery is the aim of therapy
5. Identify etiologies of shock which require additional lifesaving interventions

3.1. Management of hypovolemic shock

Before considering hypovolemic shock rule out cardiogenic shock since the
fluid management in cardiogenic shock is challenging with 250ml of NS over
30 min only. If there is misdiagnosis of Cardiogenic shock as hypovolemic
shock, iatrogenic fluid overload (like pulmonary edema) will develop during
infusion of fluid and worsen the condition.
If cardiogenic shock is ruled out, search the cause of hypovolemia (is that
haemorrhagic or non-haemorrhagic)
Infusion of fluid (NS or RL), 1-2 litres fast for adults and 20 mL/kg for
paediatric patients.;
reassess the patient for adequacy of treatment by Following the BP, PR, UoP
& mental status
✓ If responsive, the fluids are slowed to maintenance rates
✓ If not responsive repeat 1x in adult (total 2x) & 2x in paediatrics (total
3x) with maximum tolerated dose being 60 - 80 ml/kg with in the first
1 - 2 hr
✓ If not responsive with the above fluid give blood
✓ If still not responsive consider septic shock
✓ if needed open double IV line.
If due to hemorrhage, apply transfusion of packed Red Blood Cells (RBC)
or whole blood 20ml/kg over 4 hrs, repeat as needed until hemoglobin level
reaches 10gm/dl and the vital signs are corrected.
Better to follow UOP with catheterization

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Chapter 3; Shock

3.2. Cardiogenic shock (pump failure)

Cardiogenic shock (CS) is a low cardiac output state resulting in life-threatening


end-organ hypoperfusion and hypoxia.
LV fails to deliver oxygenated blood to peripheral tissues due to variances in
contractility, as well as preload and afterload.
The clinical presentation is typically characterized by persistent hypotension
(SBP <90 mmHg unresponsive to volume replacement and is accompanied by
clinical features of peripheral hypoperfusion.
The in-hospital mortality rates range from 40 to 60%, depending on shock
severity and the associated underlying cause.
Acute MI with LV dysfunction remains the most frequent cause of CS.
Circulatory failure based on cardiac dysfunction may be caused by primary
myocardial failure, most commonly secondary to acute MI, and less frequently
by;
o cardiomyopathy or myocarditis
o cardiac tamponade
o arrhythmias or
o critical valvular heart disease

Clinical features
o Most patients initially are;
▪ Dyspneic
▪ appear pale
▪ cold extremity
▪ poor capillary refill
▪ apprehensive and diaphoretic
▪ mental status may be altered.
o The pulse is typically weak and rapid or occasionally severe bradycardia
due to high-grade heart block may be present.
o BP is typically reduced (<90 mmHg; or catecholamines required to maintain
blood pressure >90 mmHg), but occasionally BP may be maintained by
very high systemic vascular resistance.
o Tachypnea and jugular venous distention may be present.
o Typically, there is a weak apical pulse and soft S1, and S3 gallop may be
audible.
o Acute, severe MR and VSR usually are associated with characteristic
systolic murmurs.
o Crackles are audible in most patients with LV failure.
o Oliguria/anuria is common.

Diagnosis
For these unstable patients, supportive therapy must be initiated simultaneously
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Chapter 3; Shock

A focused history and physical examination should be performed along


with ECG, chest X-ray, and blood specimens to the laboratory
Initial Echo is an invaluable tool to elucidate the underlying cause of CS.

Management of cardiogenic shock

In addition to the usual treatment of acute MI, initial therapy is aimed at;
o maintaining adequate systemic and coronary perfusion by raising the
blood pressure with vasopressors and adjusting volume status to a
level that ensures optimum LV filling pressure
o Generally adequate perfusion occurs with a mean arterial BP of
60 - 65 mmHg or a systolic BP ~90 mmHg.
Administer O2 if SaO2<90%
o Hypoxemia and acidosis need to be corrected; up to 90% of patients
require ventilatory support, decreasing the stress from increased work
of breathing
o Often CS patients require early mechanical ventilation (~80%) for
management of acute hypoxemia, increased work of breathing, and
hemodynamic instability;
Administer NS 250ml over 30 min and see the change in BP, UOP and
worsening of HF.
✓ If BP improves then consider hypovolemic shock and continue slowly
replacing the fluid with NS.
✓ If there is no response to fluid or worsening heart failure, use either of the
following vasopressor therapies:

First line

▪ Norepinephrine (noradrenaline)
o 0.2 µg/kg/min escalated to 1µg/kg/min by doubling the
dose q20 min until BP> 90/60 mmHg (or 2 to 4 μg/min
and titrated upward based on blood pressure).
o Maintain the dose that maintained the BP> 90/60 mmHg
for 6hrs, then you will deescalate as the same as the
escalation (look at adrenaline drip preparation below).
o We recommend to use the above dose; in another
reference you may see the dose as: 0.5 - 1 mcg/minute
and titrate to desired response; 8-30 mcg/minute is usual
range
Alternative
▪ Dopamine
o 5 - 20 µg/kg/min IV diluted with dextrose 5% in Water
(D5W), or in sodium chloride solution 0.9%(NS)
o infusion at 5µg/kg/min and escalate up to 40ug/kg/min by 936
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Chapter 3; Shock

doubling the dose q20 min until BP> 90/60 mmHg.


o Maintain the dose that maintained the BP> 90/60 mmHg
for 6hrs, then you will deescalate as the same as the
escalation (look at dopamine drip preparation below).
▪ Dobutamine
o Start with 2.5 μg/kg per min to be titrated up to
40µg/kg/min IV diluted in dextrose 5%.
o Never initiate Dobutamine alone in a patient with
cardiogenic shock and Systolic BP< 70
▪ Adrenaline infusion:
o 0.01-0.5 µg /kg/minute ( 7-35 µg /minute i n a 70 kg
patient); titrate to desired response
✓ Maintain the dose of vasopressor that maintained the BP> 90/60 mmHg
for 6hrs (what is the reason behind maintaining for 6hr’s?), then you will
taper the dose of vasopressor in the same way as it was escalated if
BP is maintained. (look at dopamine and adrenaline drip preparation
below).
✓ If myocardial infarction suspected aspirin should be loaded and
immediate reperfusion.
✓ If patient has concomitant pulmonary edema resulting in hypoxia
▪ Continuous infusion of Lasix (frusemide) started at 5-10 mg/hr should
be started through another IV line (escalate dose based on Blood
Pressure).
✓ More frequent follow up of V/S, SO2 and UOP q 20-30min until patient
stabilize
✓ Further follow up and management is similar to other heart failure
syndromes.
✓ Moderate glucose control (≤180 mg/dL) should be a goal and hypoglycemia
must be avoided.
✓ Negative ionotropic agents should be discontinued.
✓ Recurrent ventricular tachycardia or rapid atrial fibrillation may require
immediate treatment
✓ Bradyarrhythmia’s may require transvenous pacing.

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Chapter 3; Shock

Dopamine drip preparation


1 ampoule of dopamine = 5ml/each ml contains 40mg/ = 200mg = 200,000 µg
Dose to be administered = 5 µg/kg/min up to 40 µg/kg/min
(N.B. dose range may differ from reference to reference)

Since weight measurement in shock pt is difficult, you may take approximated weight (let’s say 50kg weight for this
calculation, this will make 5 µg/kg/min =250 µg)

✓ Let’s say we add 4 ampoules (800,000 µg) of dopamine in 1000ml of NS or D5W. the question will be in how many
ml of NS and at what rate (drop) we get 250 µg
✓ 1000ml = 800,000 µg
?? = 250 µg

This will give us 0.3125 ml


1ml = 20 drops
0.3125ml = ???

This will give us 6 drops (i.e. 6 drops will contain 5 µg/kg/min of dopamine for this particular patient)

How shall we proceed?

✓ We will measure BP every 20 minutes


✓ If BP <90/60(not responding) double the dose like below
☛ 6dpm (5 µg/kg/min)
☛ 12dpm (10 µg/kg/min) better to put the dose in µg/kg/min than dpm in follow up
☛ 24dpm (20 µg/kg/min)
☛ 48dpm (40 µg/kg/min)
 Maximum dose; some experts say you can go up to 50 µg/kg/min
For how long shall we maintain or when to deescalate?
✓ From my practical experience, If BP ≥ 90/60, we maintain the drop for 6 hr’s before starting de-escalation (what is
the reason behind?)
✓ How to deescalate? → de-escalate as it was escalated
☛ 48dpm (40 µg/kg/min)
☛ 24dpm (20 µg/kg/min)
☛ 12dpm (10 µg/kg/min)
☛ 6dpm (5 µg/kg/min)
☛ stop

Source → https://t.me/Debolteam

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Chapter 3; Shock

Table*; Calculated dose and drop per minute of dopamine based on the
above calculation
Weight in Kg Dopamine dose (µg/min)
3 5 10 15 20 30 40
Drop/minute of dopamine
50 3 drops 5 drops 10 drops 15 drops 20 drops 30 drops 40 drops
60 3.5 drops 6 drops 12 drops 18 drops 24 drops 36 drops 48 drops
70 4.2 drops 7 drops 14 drops 21 drops 28 drops 42 drops 56 drops
80 4.8 drops 8 drops 16 drops 24 drops 32 drops 48 drops 64 drops
90 5.4 drops 9 drops 18 drops 27 drops 36 drops 54 drops 72 drops
100 6 drops 10 drops 20 drops 30 drops 40 drops 60 drops 80 drops
*Prepared by; Dr. Genet Kifle (MD, Emergency and critical care consultant)

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Chapter 3; Shock

Adrenaline/Epinephrine/ drip preparation


1 ampoule of adrenaline = 1ml = 1mg (1:1,000); there is also 0.1mg/1ml (1:10,000) preparation
Dose to be administered = 0.o1 µg/kg/min up to 0.5 µg/kg/min for cardiogenic shock (we are using 0.2
µg/kg/min as routine in our setup)
(N.B. dose range may differ from reference to reference)

Let’s take 50kg weight for this calculation, this will make 0.2 µg/kg/min =10 µg

✓ Let’s say we add 4 ampoules (4mg = 4,000 µg) of adrenaline in 500ml of NS or D5W. the question will be
in how many ml of NS and at what rate (drop) we get 10 µg
✓ 500ml = 4,000 µg
?? = 10 µg

This will give us 1.25 ml


1ml = 20 drops
1.25ml = ???

This will give us ≅25 drops (i.e. 25 drops will contain 0.2 µg/kg/min of adrenaline for this particular
patient)

How shall we proceed?

✓ We will measure BP every 20 minutes


✓ If BP <90/60 double the dose like below
☛ 25dpm (0.2 µg/kg/min)
☛ 50dpm (0.4 µg/kg/min) better to put the dose in µg/kg/min than dpm in follow up
☛ 75dpm (0.8 µg/kg/min)
✓ If BP ≥ 90/60, maintain the drop for 6 hr’s before starting de-escalation
✓ de-escalate as it was escalated
☛ 75dpm (0.8 µg/kg/min)
☛ 50dpm (0.4 µg/kg/min)
☛ 25dpm (0.2 µg/kg/min)
☛ stop

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Nor adrenaline/Norepinephrine/ drip preparation


1 ampoule of dopamine = 2ml = 4mg = 4,000 µg
Dose to be administered = 0.2 µg/kg/min up to 1 µg/kg/min (we are using 0.2 µg/kg/min as routine in our
setup)
(N.B. dose range may differ from reference to reference)

Since weight measurement in shock pt is difficult, you may take approximated weight (let’s say 50kg weight for this
calculation, this will make 0.2 µg/kg/min =10 µg)

✓ Let’s say we add 4 ampoules (16mg= 16,000 µg) of Norepinephrine in 1000ml of NS or D5W. the question will be in
how many ml of NS and at what rate (drop) we get 10 µg
✓ 1000ml = 16,000 µg
?? = 10 µg

This will give us 0.625 ml


1ml = 20 drops
0.625ml = ???

This will give us 12.5 drops ≅ 12 drops (i.e. 12 drops will contain 0.2 µg/kg/min of Noradrenaline for this particular
patient)

How shall we proceed?

✓ We will measure BP every 20 minutes


✓ If BP <90/60 (not responding) double the dose like below
☛ 12dpm (0.2 µg/kg/min)
☛ 24dpm (0.4 µg/kg/min)
☛ 36dpm (0.6 µg/kg/min)
☛ 48dpm (0.8 µg/kg/min)
For how long shall we maintain or when to deescalate?
✓ From my practical experience, If BP ≥ 90/60, we maintain the drop for 6 hr’s before starting de-escalation (what is
the reason behind?)
✓ How to deescalate? → de-escalate as it was escalated
☛ 48dpm (0.8 µg/kg/min)
☛ 36dpm (0.6 µg/kg/min)
☛ 24dpm (0.4 µg/kg/min)
☛ 12dpm (0.2 µg/kg/min)
☛ stop

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Chapter 3; Shock

3.3. Septic shock

In distributive shock, there is relative intravascular volume depletion due to


marked systemic vasodilatation. This is most commonly seen in septic shock.
Anaphylaxis, neurogenic shock and adrenal insufficiency are additional causes
of distributive shock.
What is sepsis? (refer under Short chapter 18 of Nitsbin; click here → Chapter
17; Sepsis)

Management of septic shock


Principles of management
o IV Fluids
o Vasopressor therapy.
o Broad spectrum antibiotics
o Steroids
Apply the six sepsis management bundles with in 1hr:
o Appropriate fluid management
o Oxygen delivery
o Antibiotics
o Sending specimen for culture and sensitivity
o Hourly urine out and
o Monitoring of lactate if possible.
Adequate organ system perfusion with IV fluids (large volume of IV fluids
are required in septic shock patients).
✓ Initial fluid bolus of 20 to 30 mL/kg of RL or NS.
o For pediatrics 40-60ml /kg (20ml /kg hourly bolus) can
be given
✓ Repeat 2 boluses of 20ml/kg with target of SBP >90mmhg, and
MAP>60mmhg in the first 3 hours
✓ In general, most patients with septic shock are expected to take
around 5-6 liter of IV fluids within 24 hours.
✓ Closely monitor for signs of fluid overload (jugular venous
distension, crackles on lung auscultation, pulmonary edema on
imaging, or hepatomegaly in children)
✓ Stop or decrease fluid administration if signs of fluid overload.
✓ Watch also for signs of target perfusion achievement (Mean
Arterial Pressure (MAP)>65 mmHg or age appropriate target for
children, urine output (>0.5 ml/kg/hr in adults, 1 ml/kg/hr in
children), and improvement of skin mottling, capillary refill, level
of consciousness)
If non-responsive to fluid resuscitation administer vasopressor therapy.
First line
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✓ Norepinephrine (noradrenaline), Initial: 0.5-1mcg/minute and titrate to


desired response; 8-30 mcg/minute is usual range

Alternatives

✓ Dopamine, 5-50 mcg/kg/min IV diluted with dextrose 5% in Water,


or in sodium chloride solution 0.9%;
✓ Adrenaline, I . V . infusion: Initial: 0.1-0.5 m c g /kg/minute ( 7-35
m c g /minute i n a 70 k g patient); titrate to desired response
Start Empiric therapy with broad spectrum antibiotics in septic shock patients
as soon as possible at least within 01 hour of the clinical suspicion of septic
shock and draw blood for culture.
o Ceftriaxone, 1gm, IV, BID and Metronidazole, 500mg, IV, TID
▪ In relatively stable patient
o Ceftazidime/Cefepime 2g iv TID +/-Vancomycin 1 gm IV BID
▪ In patients with who are critical, hospitalized,
immunocompromised or previous structural lung disorder:
o Meropenem 1g IV TID +/- vancomycin 1g IV BID
▪ in critical patients if there is no response with the above
alternative or culture and sensitivity result is suggestive
o When patients improve and are able to take PO
▪ Augumentin, 2gm PO BID for 7-10 days
Surgical drainage or debridement of an abscess or dead /necrotized
tissue.
Blood transfusion if Hgb is ≤ 7mg/dl in adults, Hgb is < 10 mg/dl in
pediatrics to keep adequate O2 saturation.
Collect Culture and sensitivity, organ function tests, electrolytes, and
imaging results and manage if there is any complication

If the Blood pressure doesn’t respond for the initial management with
vasopressors and fluids
✓ Hydrocortisone, 50 mg IV QID (when vasopressor dependent or
refractory septic shock)
o For a maximum of 7 days or until all vasoactive infusions
have been discontinued for at least 12 hours, whichever
comes first

Refer sepsis under short case of Nitsbin for more (click here → Chapter 17;
Sepsis)

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Chapter 3; Shock

3.4. Adrenal Crisis

Introduction and principle of management


Adrenal crisis is shock refractory to volume resuscitation and pressors.
It could be primary (autoimmune disease, adrenal hemorrhage, infection) or
secondary (prolonged use of steroid, pituitary gland disorder)
should be suspected in any patient in the emergency/ICU who develops shock
of unclear etiology, or refractory to fluid resuscitation and vasopressors
Other features of adrenal insufficiency: hyponatremia and hyperkalemia
(primary) and either hypernatremia /hyponatremia and hypokalemia (secondary)
Patient should be admitted to the ICU for rapid correction of shock and
replacement of steroid and management of other metabolic complications.

Management
Manage hypotension: IV Fluid and vasopressor
Replace steroid; Optimize maintenance dosage of steroid
Determine and manage underlying cause

a. Management of shock
➢ Manage shock with Normal saline according to shock management
guideline
➢ Use dextrose-containing saline if the patient is hypoglycemic.

b. Steroids
➢ Hydrocortisone 100-mg IV bolus:
✓ Is the drug of choice for cases of adrenal crisis or insufficiency,
especially for underlying primary insufficiency (provides both
glucocorticoid and mineralocorticoid effects).
Or
➢ Dexamethasone, 4-mg IV bolus: (preferred if rapid adrenocorticotropic
hormone stimulation test is contemplated).

➢ Patients may require lifelong glucocorticoids ± mineralocorticoid ± androgen


supplementation.
➢ Optimize Maintenance Dosage of Steroids; During periods of stress,
increase maintenance dose of chronic steroids to three times the daily
dose, to satisfy increased physiologic need for cortisol

c. Vasopressors
➢ Administer only after steroid therapy in patients unresponsive to aggressive
fluid resuscitation (choice of norepinephrine, dopamine, or phenylephrine).

d. Determine risk factors and Underlying Cause:


➢ Investigate as appropriate for underlying risk factors
✓ Sepsis, adrenal hemorrhage, CNS abnormality, prolonged steroid use.
➢ Serum cortisol >18 micrograms/dL generally rule out adrenal insufficiency
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➢ The ACTH stimulation test measures serum cortisol after stimulation by


synthetic ACTH; Serum cortisol rises significantly in secondary insufficiency.
➢ Serum ACTH: A high ACTH level is seen in primary insufficiency, and low
in secondary adrenal insufficiency.
➢ An abdominal CT scan can identify adrenal gland hemorrhage or infarction.

Management of complications
➢ Hyponatremia: 3%N/S and/or free fluid restriction
➢ Hyperkalemia: regular insulin with dextrose, calcium gluconate, sodium
bicarbonate depending on the severity of hyperkalemia and ECG changes
➢ Hypernatremia: hypotonic fluid depending on the amount of water deficit
➢ Hypokalemia: IV or PO KCl depending on the severity of hypokalemia
➢ Hypoglycemia: dextrose/ dextrose in NS
➢ Manage Coma: Repeat ABC assessment and intubate if the patient failed
to protect the air way

Follow-up
➢ Follow blood pressure during correction of shock
➢ Neuro sign chart for comatose patients
➢ Serum glucose every 6hrs
➢ Update Serum electrolyte daily
➢ ECG: related to potassium imbalances (prolonged QT, peaked T waves,
and heart block in hyperkalemia in primary adrenal insufficiency, or inverted
T waves and presence of U wave in hypokalemia in secondary adrenal
insufficiency).

3.5. Refractory shock

For 3rd edition

3.6. Shock and Pulmonary edema Management


when they happen together
For 3rd edition

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Chapter 4; Hypoglycaemia

Chapter 4; Hypoglycaemia
Dr. Mulualem. G
→ Refer under long case of DM (click here → Hypoglycaemia)

Chapter 5; DKA
→ Refer under long case of DM (click here → DKA and HHS)

Chapter 6; Thyroid storm


→ Refer from short case of Nitsbin (click here → 18.1.2. Thyroid storm / thyrotoxic
crisis )

Chapter 7; Nerveous System Related


Disorders and Infections

7.1. CVA (stroke)


→ Refer under long case of Stroke (click here → Chapter 6; Stroke)

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7.2. Seizure and epilepsy (የሚጥል


በሽታ)
Dr. Asmare. W, Dr. Mulualem. G

A seizure (from the Latin sacire, “to take possession of”) is a paroxysmal
event due to abnormal excessive or synchronous neuronal activity in the brain.
Depending on the distribution of discharges, this abnormal brain activity can
have various manifestations, ranging from dramatic convulsive activity to
experiential phenomena not readily discernible by an observer.
The meaning of the term seizure needs to be carefully distinguished from that
of epilepsy.
Epilepsy describes a condition in which a person has recurrent seizures (two
or more unprovoked seizures) due to a chronic, underlying process.
This definition implies that a person with a single seizure, or recurrent seizures
due to correctable or avoidable circumstances, does not necessarily have
epilepsy.
Epilepsy refers to a clinical phenomenon rather than a single disease entity,
because there are many forms and causes of epilepsy. However, among the
many causes of epilepsy there are various epilepsy syndromes in which the
clinical and pathologic characteristics are distinctive and suggest a specific
underlying etiology.
Epilepsy refers to a syndrome of recurrent, idiopathic seizures.
Pseudo seizures are not true seizures but are psychiatric in origin; are often
difficult to distinguish from true seizures without an EEG.
So, Epilepsy considered in one of the following conditions
o At least two unprovoked (or reflex) seizures occurring > 24 hours
apart.
o One unprovoked (or reflex) seizure and a probability of further
seizures similar to the general recurrence risk after two unprovoked
seizures (at least 60%), occurring over the next 10 years.
o A known epilepsy syndrome.

Definitions of Terminologies in seizure and epilepsy

Pre- Ictal
o Events that occur Immediately before the seizure, and include Aura and
Prodromal symptoms/signs
Aura
o Some patients describe odd, internal feelings such as fear, a sense of
impending change, detachment, depersonalization, or illusions that
objects are growing smaller (micropsia) or larger (macropsia).
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▪ These subjective, “internal” events that are not directly observable


by someone else are referred to as auras
o Aura’s of taste or smell, can occur in isolation or can precede a focal
sezure with impairement of awareness deja vu moments
Seizure (Ictal) semiology
o It is the sign and symptoms observed just before, during and immediately
after the seizure occurrence.
o Ictal Semiology means features occurring during the attack
▪ Simple: Motor; Sensory; Autonomic; Psychic….
▪ Complex: Motor; Sensory; Autonomic; Psychic….
o Motor semiology: Motor manifestations refer to involvement of the
musculature, which can be positive (increased muscle activity) or
negative (decreased muscle activity)
▪ simple motor refers to the contraction of a muscle or group of
muscles that is usually stereotyped and does not include
multiple phases.
▪ Complex motor activity: Automatism
o Motor semiologies can be tonic, myoclonic or clonic
▪ Tonic activity which means a sustained increase in muscle
contraction lasting up to minutes.
▪ A myoclonic jerk refers to a very brief involuntary contraction
usually lasting less than 100 micro sec.
▪ Clonic activity refers to a regularly repetitive jerking that is
prolonged
Post-Ictal features:
o Features occur after the seizure stops

Epidemiology

The incidence and prevalence of epilepsy increase with age in adulthood and
are highest in patients over 65 years.
The prevalence of epilepsy in older adults is approximately 2 - 5%
The annual incidence of epilepsy rises with each decade over 60 years.
Seizures in older patients are frequently underdiagnosed; hence, the incidence
of epilepsy in older patients may be two to three times higher, with an
incidence six to seven times greater than younger individuals.

Classification of seizures
Determining the type of seizure that has occurred is essential for focusing the
diagnostic approach on particular etiologies, selecting the appropriate therapy,
and providing potentially vital information regarding prognosis.
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The International League against Epilepsy (ILAE) Commission on Classification


and Terminology (2005 - 2009) has provided an updated approach to
classification of seizures.
o This system is based on the clinical features of seizures and associated
electroencephalographic findings.
Focal seizures originate within networks limited to one cerebral hemisphere
(note that the term partial seizures is no longer used).
Generalized seizures arise within and rapidly engage networks distributed
across both cerebral hemispheres.
Focal seizures are usually associated with structural abnormalities of the brain.
In contrast, generalized seizures may result from cellular, biochemical, or
structural abnormalities that have a more widespread distribution.

Picture; left) Focal seizure, right) Generalized seizure

Focal seizures
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Focal seizures arise from a neuronal network either discretely localized within
one cerebral hemisphere or more broadly distributed but still within the
hemisphere.
With the new classification system, the subcategories of “simple focal seizures”
and “complex focal seizures” have been eliminated. Instead, depending on the
presence of cognitive impairment, they can be described as focal seizures with
or without dyscognitive features.
Focal seizures can also evolve into generalized seizures. In the past this was
referred to as focal seizures with secondary generalization, but the new system
relies on specific descriptions of the type of generalized seizures that evolve
from the focal seizure.
The routine interictal (i.e., between seizures) electroencephalogram (EEG) in
patients with focal seizures is often normal or may show brief discharges
termed epileptiform spikes, or sharp waves.
Because focal seizures can arise from the medial temporal lobe or inferior
frontal lobe (i.e., regions distant from the scalp), the EEG recorded during the
seizure may be non-localizing. However, the seizure focus is often detected
using sphenoidal or surgically placed intracranial electrodes.

Focal Seizures Without Dyscognitive Features


Focal seizures can cause motor, sensory, autonomic, or psychic symptoms
without impairment of cognition.
For example, a patient having a focal motor seizure arising from the right
primary motor cortex near the area controlling hand movement will note the
onset of involuntary movements of the contralateral, left hand. These
movements are typically clonic (i.e., repetitive, flexion/extension movements);
pure tonic posturing may be seen as well.
Since the cortical region controlling hand movement is immediately adjacent to
the region for facial expression, the seizure may also cause abnormal
movements of the face synchronous with the movements of the hand.
Three additional features of focal motor seizures are worth noting.
o 1st, in some patients, the abnormal motor movements may begin
in a very restricted region such as the fingers and gradually progress
(over seconds to minutes) to include a larger portion of the extremity.
This phenomenon, known as a “Jacksonian march,” represents the spread
of seizure activity over a progressively larger region of motor cortex.
o 2nd, patients may experience a localized paresis (Todd’s paralysis) for
minutes to many hours in the involved region following the seizure.
o 3rd, in rare instances, the seizure may continue for hours or days. This
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Focal seizures may also manifest as;


o changes in somatic sensation (e.g., paresthesias)
o vision (flashing lights or formed hallucinations)
o equilibrium (sensation of falling or vertigo), or
o autonomic function (flushing, sweating, piloerection).
Focal seizures arising from the temporal or frontal cortex may also cause
alterations in hearing, olfaction, or higher cortical function (psychic symptoms).
This includes;
o the sensation of unusual, intense odors (e.g., burning rubber or kerosene)
or sounds (crude or highly complex sounds)
o an epigastric sensation that rises from the stomach or chest to the head.
Auras.

Focal Seizures with Dyscognitive Features


Focal seizures may also be accompanied by a transient impairment of the
patient’s ability to maintain normal contact with the environment.
The patient is unable to respond appropriately to visual or verbal commands
during the seizure and has impaired recollection or awareness of the ictal
phase.
The seizures frequently begin with an aura (i.e., a focal seizure without
cognitive disturbance) that is stereotypic for the patient.
The start of the ictal phase is often a sudden behavioral arrest or motionless
stare, which marks the onset of the period of impaired awareness.
The behavioral arrest is usually accompanied by automatisms, which are
involuntary, automatic behaviors that have a wide range of manifestations.
o Automatisms may consist of very basic behaviors such as chewing, lip
smacking, swallowing, or “picking” movements of the hands,
or more elaborate behaviors such as a display of emotion or running.
The patient is typically confused following the seizure, and the transition to full
recovery of consciousness may range from seconds up to an hour.
Examination immediately following the seizure may show an anterograde
amnesia or, in cases involving the dominant hemisphere, a postictal aphasia.

Evolution of Focal seizures to generalized seizures

Focal seizures can spread to involve both cerebral hemispheres and produce a
generalized seizure, usually of the tonic-clonic variety.
This evolution is observed frequently following focal seizures arising from a
focus in the frontal lobe, but may also be associated with focal seizures
occurring elsewhere in the brain.
Often, however, the focal onset is not clinically evident and may be established
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Nonetheless, distinguishing between these two entities is extremely important,


because there may be substantial differences in the evaluation and treatment
of epilepsies associated with focal versus generalized seizures.

Generalized seizures
Generalized seizures are thought to arise at some point in the brain but
immediately and rapidly engage neuronal networks in both cerebral
hemispheres.
Several types of generalized seizures have features that place them in
distinctive categories and facilitate clinical diagnosis.

Typical Absence Seizures

Typical absence seizures are characterized by sudden, brief lapses of


consciousness without loss of postural control.
The seizure typically lasts for only seconds, consciousness returns as suddenly
as it was lost, and there is no postictal confusion.
Although the brief loss of consciousness may be clinically in apparent or the
sole manifestation of the seizure discharge, absence seizures are usually
accompanied by subtle, bilateral motor signs such as rapid blinking of the
eyelids, chewing movements, or small-amplitude, clonic movements of the
hands.
Typical absence seizures are associated with a group of genetically determined
epilepsies with onset usually in childhood (ages 4 - 8 years) or early
adolescence and are the main seizure type in 15- 20% of children with
epilepsy.
The seizures can occur hundreds of times per day, but the child may be
unaware of or unable to convey their existence.
Because the clinical signs of the seizures are subtle, especially to parents who
may not have had previous experience with seizures, it is not surprising that
the first clue to absence epilepsy is often unexplained “daydreaming” and a
decline in school performance recognized by a teacher.
The electrophysiologic hallmark of typical absence seizures is a generalized,
symmetric, 3-Hz spike-and-wave discharge that begins and ends suddenly,
superimposed on a normal EEG background.

Atypical Absence Seizures

Atypical absence seizures have features that deviate both clinically and electro
physiologically from typical absence seizures.
For example, the lapse of consciousness is usually of longer duration and less
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The EEG shows a generalized, slow spike-andwave pattern with a frequency of


≤2.5 per second, as well as other abnormal activity.
Less responsive to anticonvulsants as compared to typica

Generalized, Tonic-Clonic Seizures

Generalized-onset tonic-clonic seizures are the main seizure type in ~10% of


all persons with epilepsy.
They are also the most common seizure type resulting from metabolic
derangements and are therefore frequently encountered in many different
clinical settings.
The initial phase of the seizure is usually tonic contraction of muscles
throughout the body, accounting for a number of the classic features of the
event.
Tonic contraction of the muscles of expiration and the larynx at the onset will
produce a loud moan or “ictal cry.”
Respirations are impaired, secretions pool in the oropharynx, and cyanosis
develops.
Contraction of the jaw muscles may cause biting of the tongue.
A marked enhancement of sympathetic tone leads to increases in heart rate,
blood pressure, and pupillary size.
After 10 - 20 s, the tonic phase of the seizure typically evolves into the clonic
phase, produced by the superimposition of periods of muscle relaxation on the
tonic muscle contraction.
The periods of relaxation progressively increase until the end of the ictal
phase, which usually lasts no more than 1 min.
The postictal phase is characterized by unresponsiveness, muscular flaccidity,
and excessive salivation that can cause stridorous breathing and partial airway
obstruction.
Bladder or bowel incontinence may occur at this point.
Patients gradually regain consciousness over minutes to hours, and during this
transition, there is typically a period of postictal confusion.
Patients subsequently complain of headache, fatigue, and muscle ache that
can last for many hours.
The duration of impaired consciousness in the postictal phase can be
extremely long (i.e., many hours) in patients with prolonged seizures or
underlying CNS diseases such as alcoholic cerebral atrophy.
There are a number of variants of the generalized tonic-clonic seizure,
including
o pure tonic and
o pure clonic seizures.
Brief tonic seizures lasting only a few seconds are especially noteworthy since
they are usually associated with specific epileptic syndromes having mixed
seizure phenotypes, such as the Lennox-Gastaut syndrome.
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Atonic Seizures

❖ Atonic seizures are characterized by sudden loss of postural muscle tone


lasting 1- 2 s.
❖ Consciousness is briefly impaired, but there is usually no postictal confusion.
❖ A very brief seizure may cause only a quick head drop or nodding movement,
whereas a longer seizure will cause the patient to collapse.
This can be extremely dangerous, because there is a substantial risk of direct
head injury with the fall.
❖ The EEG shows brief, generalized spike-and-wave discharges followed
immediately by diffuse slow waves that correlate with the loss of muscle tone.
❖ Similar to pure tonic seizures, atonic seizures are usually seen in association
with known epilepsy syndromes.

Myoclonic Seizures

Myoclonus is a sudden and brief muscle contraction that may involve one part
of the body or the entire body.
A normal, common physiologic form of myoclonus is the sudden jerking
movement observed while falling asleep.
Pathologic myoclonus is most commonly seen in association with metabolic
disorders, degenerative CNS diseases, or anoxic brain injury.
Myoclonic seizures usually coexist with other forms of generalized seizures but
are the predominant feature of juvenile myoclonic epilepsy.

Currently Unclassified seizures

Not all seizure types can be designated as focal or generalized, and they
should therefore be labeled as “unclassifiable” until additional evidence allows a
valid classification.
Epileptic spasms are such an example.
These are characterized by a briefly sustained flexion or extension of
predominantly proximal muscles, including truncal muscles.
Epileptic spasms occur predominantly in infants and likely result from
differences in neuronal function and connectivity in the immature versus
mature CNS.

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Epilepsy syndromes

Epilepsy syndromes are disorders in which epilepsy is a predominant feature,


and there is sufficient evidence (e.g., through clinical, EEG, radiologic, or
genetic observations) to suggest a common underlying mechanism
Examples include33
o Juvenile myoclonic epilepsy
o Lennox-Gastaut syndrome
o Mesial temporal lobe epilepsy syndrome

Causes of seizures and epilepsy


Seizures are a result of a shift in the normal balance of excitation and
inhibition within the CNS.
Given the numerous properties that control neuronal excitability, it is not
surprising that there are many different ways to perturb this normal balance,
and therefore many different causes of both seizures and epilepsy.
Causes of seizures can be remembered by the four M’s and the four I’s
The four M’s
o Metabolic and electrolyte disturbances:
▪ Hyponatremia
▪ Hypoglycemia or hyperglycemia
▪ Hypocalcemia
▪ Uremia
▪ Thyroid storm
▪ Hyperthermia (Febrile seizure is common in children)
o Mass lesions:
▪ Brain mass (primary or secondary brain tumors)
▪ Hemorrhages (ICH, SDH, EDH).
o Missing drugs (Noncompliance) with anticonvulsants in patients with
epilepsy. This is the most common reason for poor seizure control in
epileptics.
o Miscellaneous
▪ Eclampsia
▪ Hypertensive encephalopathy; severe hypertension can cause
cerebral edema
▪ Acute withdrawal from alcohol
▪ Drugs (e.g. Benzodiazepines, Barbiturates).
▪ Vascular malformation

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The four I’s


o Intoxications
▪ Cocaine
▪ Lithium
▪ Theophylline
▪ Carbon monoxide poisoning.
o Infections
▪ Malaria
▪ Meningitis (bacterial or viral)
▪ Brain abscess
▪ Sepsis.
o Ischemia; common cause of seizure in elderly patients.
▪ Stroke
▪ TIA
o Increased ICP:
▪ Trauma (SDH, EDH)
▪ Cerebral edema of different causes

Another Mnemonics for etiology of seizure → Vitamins2


Vascular: stroke, hemorrhage, hypertension, AVM (Arteriovenous malformation)
in children
Infections: meningitis, encephalitis
Trauma
Autoimmune: SLE, vasculitis, ADEM (Acute disseminated encephalomyelitis)
Metabolic/toxic
Idieopathic
Neoplastic
Structural: prior stroke, cortical malformation in pediatrics age
Syndrome: Epilepsy syndromes, genetic disorder

Causes of seizure according to Age

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➢ Head trauma is a common cause of epilepsy in adolescents and adults.


➢ The head injury can be caused by a variety of mechanisms, and the
likelihood of developing epilepsy is strongly correlated with the severity of
the injury.
➢ A patient with a penetrating head wound, depressed skull fracture,
intracranial hemorrhage, or prolonged posttraumatic coma or amnesia has a
30 - 50% risk of developing epilepsy
➢ A patient with a closed head injury and cerebral contusion has a 5-25%
risk.
➢ Recurrent seizures usually develop within 1 year after head trauma,
although intervals of >10 years are well known.
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Diagnosis and Investigations

Seizure and epilepsy are a Clinical diagnosis (see approach to the patient with
active seizure below)
If the patient has a known seizure disorder (epileptic), check adherence.
If the patient history is unclear or if this is the patient’s first seizure, do the
following Investigations;
o RBS
o CBC
o Electrolytes
o LFT
o RFT (BUN and creatinine)
o Urinalysis
o EEG
▪ Although the EEG is the most helpful diagnostic test in the
diagnosis of a seizure disorder an abnormal EEG pattern alone is
not adequate for the diagnosis of seizures.
▪ A normal EEG in a patient with a first seizure is associated with a
lower risk of recurrence.
▪ When repeated it got more sensitivity
o LP and blood cultures → if patient is febrile
o Brain imaging
▪ Almost all patients with new-onset seizures should have a brain
imaging study to determine whether there is an underlying structural
abnormality that is responsible.
▪ The only potential exception to this rule is children who have an
unambiguous history and examination suggestive of a benign,
generalized seizure disorder such as absence epilepsy.
▪ MRI has been shown to be superior to CT for the detection of
cerebral lesions associated with epilepsy.

Differential Diagnosis of seizures

Syncope
o The diagnostic dilemma encountered most frequently is the distinction
between a generalized seizure and syncope.
o Characteristics of a seizure include the presence of an aura, cyanosis,
unconsciousness, motor manifestations lasting >15 s, postictal
disorientation, muscle soreness, and sleepiness. In contrast, a syncopal
episode is more likely if the event was provoked by acute pain or anxiety
or occurred immediately after arising from the lying or sitting position.
o Patients with syncope often describe a stereotyped transition from
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nausea, and tunneling of vision, and they experience a relatively brief loss
of consciousness.
Psychogenic seizures
o Psychogenic seizures are nonepileptic behaviors that resemble seizures.
o They are often part of a conversion reaction precipitated by underlying
psychological distress.
o Certain behaviors such as side to-side turning of the head, asymmetric
and large-amplitude shaking movements of the limbs, twitching of all four
extremities without loss of consciousness, and pelvic thrusting are more
commonly associated with psychogenic rather than epileptic seizures.
TIA (Transient ischemic attack)
Migraine
Acute psychosis
Paroxysmal movement disorders

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7.2.1. Status epilepticus and management of


Active seizure in emergency setup

❖ Status epilepticus refers to continuous seizures or repetitive, discrete seizures


with impaired consciousness in the interictal period.
❖ Status epilepticus has numerous subtypes, including
 Generalized convulsive status epilepticus (GCSE) (e.g., persistent,
generalized electrographic seizures, coma, and tonic-clonic movements)
 Nonconvulsive status epilepticus (e.g., persistent absence seizures or focal
seizures with confusion or partially impaired consciousness, and minimal
motor abnormalities).
❖ The duration of seizure activity sufficient to meet the definition of status
epilepticus has traditionally been specified as 15 - 30 min. However, a more
practical definition is to consider status epilepticus as a situation in which the
duration of seizures prompts the acute use of anticonvulsant therapy.
❖ For GCSE, duration is typically when seizures last beyond 5 min.
❖ GCSE is an emergency and must be treated immediately, because
cardiorespiratory dysfunction, hyperthermia, and metabolic derangements can
develop as a consequence of prolonged seizures, and these can lead to
irreversible neuronal injury.
❖ The treatment of nonconvulsive status epilepticus is thought to be less urgent
than GCSE, because the ongoing seizures are not accompanied by the severe
metabolic disturbances seen with GCSE.

Approach to the patient with active seizure


(See the algorism’s below)

❖ When a patient presents shortly after a seizure, the first priorities


are attention to ABC of Life including;
 Vital signs
 Respiratory and cardiovascular support, and
 Treatment of seizures if they resume
❖ Life-threatening conditions such as CNS infection, metabolic derangement, or
drug toxicity must be recognized and managed appropriately.
❖ When the patient is not acutely ill, the evaluation will initially focus on whether
there is a history of earlier seizures
❖ If this is the first seizure, then the emphasis will be to:
 Establish whether the reported episode was a seizure rather than another
paroxysmal event
✓ Seizures frequently occur out-of-hospital, and the patient may
be unaware of the ictal and immediate postictal phases; thus,
witnesses to the event should be interviewed carefully.
 Determine the cause of the seizure by identifying risk factors and
precipitating events
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 Clues for a predisposition to seizures include a history of


febrile seizures, earlier auras or brief seizures not recognized as such,
and a family history of seizures.
 Epileptogenic factors such as prior head trauma, stroke, tumor, or CNS
infection should be identified.
 Precipitating factors such as sleep deprivation, systemic diseases,
electrolyte or metabolic derangements, acute infection, drugs that lower
the seizure threshold, or alcohol or illicit drug use should also be
identified.
 Decide whether anticonvulsant therapy is required in addition to treatment
for any underlying illness.
❖ In the patient with prior seizures or a known history of epilepsy, the evaluation
is directed toward:
 Identification of the underlying cause and precipitating factors, and
 Determination of the adequacy of the patient’s current therapy.
❖ While managing active seizure and life-threatening conditions, pertinent and
targeted physical examination should be done including a search for underlying
cause and precipitants
❖ All patients require a complete neurologic examination, with particular emphasis
on eliciting signs of cerebral hemispheric disease

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Indications for hospitalization

➢ Patient with first time seizure with


✓ Prolonged post ictal phase
✓ Incomplete recovery
✓ Serious seizure related injuries
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➢ Presence of neurologic or systemic disease which requires additional


evaluation and treatment.

Treatment algorism of Active generalized tonic-clonic seizure and


SE in our setup

Time Medications Other simultaneous medical


managements
Impending ✓ Diazepam 0.15 to 0.2 mg/kg (max; 10mg), IV ✓ ABC of life
and early SE
(repeat once if no response after 5 minutes) • Remove sharp and dangerous
(within 5 -
30 min) • If no IV access, Diazepam 0.2 to 0.5 mg/kg materials from the surrounding
(max; 20mg), rectally (The parenteral • Position the patient to lateral
formulation of diazepam may be given rectally if side to avoid aspiration
rectal gel is not available) • Put the patient in the recovery
• Additional drug therapy may not be required if position if S/he loses
seizure stop or the etiology of SE is rapidly consciousness
corrected • Start oxygen
• Airway compromise is an
If seizure continues
indication for intubation
• Secure IV line
• Don’t hold the patient to stop
✓ Phenytoin, 20mg/kg, IV loading (at a maximum rate the seizure episode
of 50mg/min) or the same dose of crushed tablets ✓ Do RBS
via NG tube (the usual loading dose is 1g, PO, • Give 50 ml of 50% dextrose IV
stat) or bolus if low or Unknown
✓ valproic acid, 20-30mg/kg • In our setup we use, 3 vial
(60ml) of D40 since 50%
If seizure continues
dextrose is not available
✓ Continuous monitoring of Vital
signs, O2 and ECG (if indicated)
✓ Phenytoin, 5 to 10 mg/kg, IV, 10 minutes after the ✓ Obtain laboratory tests
loading dose (at a maximum rate of 50mg/min) or ❖ CBC
the same dose of crushed tablets via NG tube (the ❖ Electrolytes
usual maintenance dose is 100 mg, PO, TID or
❖ LFT
QID)
❖ RFT (BUN and creatinine)
If seizure continues

✓ Phenobarbitone, 20mg/kg, IV (at a maximum rate of


60mg/min) or the same dose of crushed tablets via
NG tube

Established
If seizure continues
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and early ✓ Phenobarbital, 15 to 20 mg/kg (infused at 50 to perform EEG (If possible) when
refractory SE
100 mg/minute) or the same dose of crushed convulsive activity is controlled
(30 min to
48 h) tablets via NG tube ✓ Begin continuous EEG if patient
• If necessary, may repeat once after 10 minutes does not awaken rapidly or if
with an additional 5 to 10 mg/kg continuous IV treatment is used (if
• Additional respiratory support may be required available and performed with
particularly when maximizing loading dose or if experienced neurologist)
concurrent sedative therapy.
• Repeat doses administered sooner than 10 to
15 minutes may lead to CNS depression.

If seizure continues

Late
refractory SE
✓ Midazolam, IV, loading dose: 0.2 mg/kg followed by
(>48 h)
a continuous infusion 0.2 - 0.6 mg/kg/h and/or
✓ Induce anesthesia with Propofol, IV loading dose 2
mg/kg, then Continuous infusion of 2 - 10 mg/kg/h
or
✓ Phenobarbital (see the above description)

General advice after stabilization


➢ healthy lifestyle with good sleep habits
➢ Avoid unsafe activities e.g. swimming alone, mountain climbing, driving car
➢ Take showers rather than baths.
➢ Avoidance of excessive alcohol and caffeine.
➢ Consequences of poor drug compliance

Pharmacologic treatment of generalized tonic-clonic status


epilepticus (GTCSE) in western setups
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Figure; Pharmacologic treatment of generalized tonic-clonic status epilepticus (SE) in adults. CLZ,
clonazepam; ECT, electroconvulsive therapy; LCM, lacosamide; LEV, levetiracetam; LZP, lorazepam;
MDZ, midazolam; PGB, pregabalin; PHT, phenytoin or fos-phenytoin; PRO, propofol; PTB,
pentobarbital; rTMS, repetitive transcranial magnetic stimulation; THP, thiopental; TPM, topiramate;
VNS, vagus nerve stimulation; VPA, valproic acid.

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7.2.2. Treatment of Seizures and epilepsy


❖ Therapy for a patient with a seizure disorder is almost always multimodal and
includes
 Treatment of underlying conditions that cause or contribute to the seizures
 Avoidance of precipitating factors
 Suppression of recurrent seizures by prophylactic therapy with antiepileptic
medications (AED)
 Surgery, and addressing a variety of psychological and social issues.

1. Treatment of underlying conditions


❖ If the sole cause of a seizure is a metabolic disturbance such as an
abnormality of serum electrolytes or glucose, then treatment is aimed at
reversing the metabolic problem and preventing its recurrence.
 Therapy with antiepileptic drugs is usually unnecessary unless the
metabolic disorder cannot be corrected promptly and the patient is at risk
of having further seizures.
❖ If the apparent cause of a seizure was a medication (e.g., theophylline) or illicit
drug use (e.g., cocaine), then appropriate therapy is avoidance of the drug;
 there is usually no need for antiepileptic medications unless subsequent
seizures occur in the absence of these precipitants.
❖ Seizures caused by a structural CNS lesion such as a brain tumor, vascular
malformation, or brain abscess may not recur after appropriate treatment of the
underlying lesion
❖ Most patients are therefore maintained on an antiepileptic medication for at
least 1 year, and an attempt is made to withdraw medications only if the
patient has been completely seizure free.
❖ If seizures are refractory to medication, the patient may benefit from surgical
removal of the epileptic brain region.

2. Avoidance of precipitating factors


❖ Unfortunately, little is known about the specific factors that determine precisely
when a seizure will occur in a patient with epilepsy.
❖ Some patients can identify particular situations that appear to lower their
seizure threshold; these situations should be avoided.
 sleep deprivation should obviously be advised to maintain a normal sleep
schedule.
 Alcohol intake-modify their drinking habits accordingly.
 Highly specific stimuli such as a video game monitor, music, or an
individual’s voice (“reflex epilepsy”).
 Stress → physical exercise, meditation and counseling
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3. Antiepileptic drug (AED) therapy

❖ Antiepileptic drug therapy is the mainstay of treatment for most patients with
epilepsy.
❖ The overall goal is to completely prevent seizures without causing any
untoward side effects, preferably with a single medication and a dosing
schedule that is easy for the patient to follow.
❖ Seizure classification is an important element in designing the treatment plan,
because some antiepileptic drugs have different activities against various
seizure types.
❖ Indication to start AED
i. All non-symptomatic seizures two or more episodes
ii. Indication to start AED after first unprovoked seizure
 With Underlying lesions proven to be epileptogenic (i.e. Epileptiform
abnormalities on interictal EEG)
 Remote cause: identified by history or neuroimaging (e.g. brain tumor,
brain malformation, prior CNS infection)
 Abnormal neurologic examination
 A first seizure that occurs during sleep
iii. Other considerations for Indication of AED
 Recurrent idiopathic seizure
 Present with Status epileptics
 Family history of epilepsy
 Todd’s paralysis
 Potentially dangerous job workers (e.g. Machinery workers, Drivers,
swimmers…) with idiopathic seizure
❖ Patients with a history of seizures (epilepsy)
 Start treatment with one AED
 If seizures persist, increase the dosage of the first anticonvulsant until
signs of toxicity appear.
 Add a second drug if the seizures cannot be controlled with the drug of
first choice.
 If the patient remains seizure free, decrease the dose of the medication(s)
cautiously.
 Discontinuation of AED can be considered if a patient has been
completely free of seizures for at least two year; however, risk of
recurrence of seizures should be discussed with the patient.
 The decision of discontinuation should be individualized as the risk of
recurrence is variable and it should be made by a specialist (neurologist).
❖ Factors to be taken into account in choosing drugs
 Type of epilepsy
 Age & sex
 Other drugs, e.g. contraceptive pill
 Other medical conditions, e.g. liver or renal dysfunction.
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 Race
 Genotype of the epilepsy

AED choices

Table; Common AED choices for adults by seizure type in Ethiopia


Seizure type First line options Alternatives (second line)
Focal onset Seizure Carbamazepine Valproic acid
Phenytoin Phenobarbital
Generalized onset: Motor Valproic acid
Phenobarbital
Carbamazepine
Phenytoin
Absence Valproic acid phenobarbital, phenytoin
Carbamazepine

AED choices for adults by seizure type in western setup34

34
We mentioned these drugs for comparison with Ethiopia setup. Ethiopian standard consideration is based
on availability of drugs. You can use those written in western setup if they are available.
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Table. Common antiepileptic drug dosing


Drug Initial dosage Maximum dosage: Titration and administration
not necessarily
required
Carbamazepi 100 - 200 mg, PO, 2,400 mg daily ✓ Increase 200 mg/day
ne BID (usual effective dose ✓ extended release in 2 divided doses
400 -1200mg/day) ✓ Regular formulation: 2-4 divided doses
Phenobarbital 30 - 100 daily 300 mg daily ✓ Titrate in 30 mg increments per 1-2 weeks
(usual effective dose ✓ As it is sedating, give at bedtime
60 - 200mg) ✓ If morning sedation occurs divide in to 2
doses.
Phenytoin 100mg TID 600 mg daily ✓ Doses up to 200 mg 3 times a day may
(usual effective dose be necessary.
~300mg/day) ✓ Consider converting patients from TID
doses to BID and once daily doses after
good seizure control
Valproic acid ✓ 500mg daily: 3,000 mg ✓ Extended release; once
extended release (usual effective dose” ✓ Delayed release: twice daily
✓ 250mg BID: 1000- 2000mg/day)
delayed release

When to discontinue AED therapy


(It must be a neurologist decision)
❖ Overall, about 70% of children and 60% of adults who have their seizures
completely controlled with antiepileptic drugs can eventually discontinue therapy.
❖ The following patient profile yields the greatest chance of remaining seizure
free after drug withdrawal:
 Complete medical control of seizures for 1- 5 years
 Single seizure type, either focal or generalized
 Normal neurologic examination, including intelligence; and
 Normal EEG.
❖ The appropriate seizure free interval is unknown and undoubtedly varies for
different forms of epilepsy. However, it seems reasonable to attempt withdrawal
of therapy after 2 years in a patient who meets all of the above criteria, is
motivated to discontinue the medication, and clearly understands the potential
risks and benefits.
❖ In most cases, it is preferable to reduce the dose of the drug gradually over 2
- 3 months.
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❖ Most recurrences occur in the first 3 months after discontinuing therapy, and
patients should be advised to avoid potentially dangerous situations such as
driving or swimming during this period.

Treatment of refractory Epilepsy

❖ Approximately one-third of patients with epilepsy do not respond to treatment


with a single antiepileptic drug, and it becomes necessary to try a combination
of drugs to control seizures.
❖ Patients who have focal epilepsy related to an underlying structural lesion or
those with multiple seizure types and developmental delay are particularly likely
to require multiple drugs.
❖ There are currently no clear guidelines for rational polypharmacy, although in
theory a combination of drugs with different mechanisms of action may be
most useful.
❖ In most cases, the initial combination therapy combines first line drugs (i.e.,
carbamazepine, oxcarbazepine, lamotrigine, valproic acid, levetiracetam, and
phenytoin).
❖ If these drugs are unsuccessful, then the addition of other drugs such as
topiramate, zonisamide, lacosamide, or tiagabine is indicated.
❖ Patients with myoclonic seizures resistant to valproic acid may benefit from the
addition of clonazepam or clobazam, and those with absence seizures may
respond to a combination of valproic acid and ethosuximide.
❖ Treatment options in addition to Combination therapy:
 Surgery
 Responsive neuro stimulation
 Deep brain stimulation
 Laser thermo ablation
 Stereotactic radiosurgery

15. Surgical treatment of refractory Epilepsy

❖ Approximately 20 - 30% of patients with epilepsy continue to have seizures


despite efforts to find an effective combination of antiepileptic drugs.
❖ The most common surgical procedure for patients with temporal lobe epilepsy
involves resection of the anteromedial temporal lobe (temporal lobectomy) or a
more limited removal of the underlying hippocampus and amygdala
(amygdalohippocampectomy).
❖ Focal seizures arising from extratemporal regions may be abolished by a focal
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Special issues related to women & Epilepsy


1. Catamenial Epilepsy
 Some women experience a marked increase in seizure frequency around
the time of menses.
 Increase AED dosages during menses.
 Give Natural progestins or intramuscular medroxyprogesterone
2. Pregnancy

 Most uncomplicated gestation & normal baby require frequent follow up


 Seizure frequency during pregnancy will remain unchanged in ~50% of
women, increase in ~30%,
and decrease in ~20%.
 Incidence of fetal abnormalities is 5-6% (CVS & MSS), compared to 2–
3% in healthy women.
 Valproic acid is Category X drug; Teratogenic causing Neural tube
defects, craniofacial defects, cardiovascular malformations, hypospadias,
and limb malformations
 Except Topiramate, newer drugs are safer than valproate
 Management:
✓ Pregnant women should be maintained on effective AED therapy.
Because the potential harm of uncontrolled convulsive seizures on
the mother and fetus is considered greater than the teratogenic
effects of AED
✓ put on monotherapy at the lowest effective dose, especially during
the first trimester
✓ give folate (1-4mg/day)
✓ treat all pregnant mothers with oral vitamin K (20 mg/d,
phylloquinone) in the last 2 weeks of pregnancy, and the infant
should receive intramuscular vitamin K (1 mg) at birth.

3. Breast feeding

 Antiepileptic medications are excreted into breast milk to a variable


degree. 5% (valproic acid) to 300% (levetiracetam)
 Mothers with anti-epileptics are encouraged to breast feed unless there is
evidence of drug effects on the infant such as lethargy or poor feeding.
8. Contraception (OCP)
 AED’s such as carbamazepine, phenytoin, phenobarbital, and topiramate
can significantly decrease the efficacy of oral contraceptives via enzyme
induction and other mechanisms.
 Management: use other forms of contraception

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7.3. Bell’s Palsy


➢ Bell‘s palsy refers to an acute unilateral infranuclear facial palsy (the
entire hemiface affected) with no identifiable cause
➢ The prognosis is very good; 80% of patients recover fully within
weeks to months.
➢ Causes
✓ Cause is often uncertain.
✓ Possible viral etiology (herpes simplex): immunologic and ischemic
factors implicated as well.
✓ Upper respiratory infection is a common preceding event.
➢ Clinical features
✓ There is acute onset of unilateral facial weakness/paralysis. Both
upper and lower parts of the face are affected.
➢ Diagnosis
✓ Clinical, but Consider EMG testing if paresis fails to resolve within
10 days.

Treatment
➢ Non pharmacologic therapy
✓ Patient should wear eye patch at night to prevent corneal abrasion
(cornea is exposed due to weakness of orbicularis oculimuscle).
✓ Surgical decompression of CN VII is indicated if the paralysis
progresses or if tests indicate deterioration
➢ Pharmacologic
✓ If the patient presents within 72 hours of onset
➢ Steroid alone for mild to moderate disease
➢ Steroid + Acyclovir for severe disease
➢ Acyclovir alone should not be given.
➢ Dosing
➢ Prednisolone 60-80mg/day for 07 days (no tapering
needed)
➢ Acyclovir 400 mg 5 times daily for 7 days

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7.4. Parkinson’s Disease


Parkinson disease is the most common cause of hypokinetic movement
disorder.
Parkinson disease is a progressive neurodegenerative syndrome involving
multiple motor and non-motor neural circuits.
Although rare forms can occur at younger age, the most important risk factor
for Parkinson‘s disease is old age.
Onset is usually after age 50 years.
The diagnosis of Parkinson disease is essentially clinical. Laboratory studies
play no role in diagnosis.

Clinical Features

The cardinal features of Parkinson‘s disease: Remembered by the mnemonic


TRAP.
o Tremor
o Rigidity
o Akinesis/bradykinesia, +/-
o Postural instability.
Tremor
o Resting tremor: noticeable when the tremulous part is supported. Tremor
is usually noticed when the arm is passively resting on the lap of the
patient.
o Described as "pill-rolling‖
o Intermittent: may not be noticeable during examination
o Starts unilaterally in the arm: takes years before it progresses to the
contralateral side
o The legs, lips, jaw, and tongue can be involved. Head involvement is not
characteristic,
Bradykinesia (slowness of movement)
o Present in most patients starting from the onset
o Difficult symptom for patients to describe.
o Patients may describe it as: "Weakness," "incoordination," and "tiredness"
o Decreased manual dexterity of the fingers: unable to do buttoning of
clothes, tying shoelaces
o Dragging the legs, shorter (shuffling) step and unsteadiness
o Gait freezing
o Festination: an impulse to take quicker and shorter steps, resulting in an
unwanted running pace
Rigidity
o Rigidity is an increased resistance to passive movement about a joint
o Decreased arm swing with walking
Postural instability
o Appears very late in the course
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o A feeling of imbalance and a tendency to fall with a significant risk of


injury.
Other motor features
o Masked facial expression, dysarthria, hypophonia, and palilalia (repetition
of a phrase or word with increasing rapidity), dysphagia
o Micrographia
o Stooped posture, kyphosis, scoliosis
o Difficulty turning in bed
Non-motor features
o Cognitive dysfunction and dementia
o Psychosis and hallucinations
o Mood disorders: depression, anxiety, and apathy
o Sleep disturbance
o Autonomic dysfunction: postural dizziness, constipation, urinary difficulties
Progressive course

Investigations and diagnosis


The diagnosis of Parkinson disease is clinical.
The diagnosis depends on the presence of the cardinal features: bradykinesia,
rigidity, tremor, and postural instability
The gradual progression and sustained response to therapy with levodopa
support the diagnosis
Conditions that mimic Parkinson disease. Some clinical clues help in
differentiating them
1. Vascular parkinsonism
➢ Due to basal ganglia or thalamic ischemia (ischemic stroke).
➢ Focal neurologic findings may be present.
2. Drug induced parkinsonism: antipsychotic and antiemetics
3. Dementia with Lewy bodies
➢ Onset of the motor symptoms accompanied by dementia and visual
hallucinations.
➢ Marked fluctuations in attention and cognition.
4. Atypical parkinsonism (supranuclear palsy and multisystem atrophy):
➢ similar to Parkinson disease, but other motor signs appear very early in the
diseases
➢ Early development of prominent gait and speech impairment, prominent
postural instability and autonomic dysfunction.
➢ Typical resting tremor usually lacking

Treatment

➢ First line: Levodopa based therapy → Carbidopa-levodopa (10/100, 25/100,


and 25/250 mg)
✓ Dosing for 25/100 mg tablet:
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➢ Gradually titrate over several weeks to a full tablet, TID.


✓ Dosing for 25/250mg
➢ One-half tablet, BID, with meals.
✓ Gradually titrate over several weeks to a full tablet BID to TID
✓ Maintain the lowest effective dose.
✓ Levodopa should not be stopped abruptly
✓ Nausea is a common side effect but metoclopramide should be
avoided as it can aggravate parkinsonian symptom
➢ Anticholinergic drugs
✓ Indications
➢ As a monotherapy: for patients who are <70 years and have
disturbing tremor (tremor predominant disease) without
significant bradykinesia or gait disturbance.
➢ As an add-on to levodopa: in patients with more advanced
disease with persistent tremor despite treatment with levodopa.
✓ Medication: Trihexyphenidyl
➢ Starting dose 0.5 to 1 mg BID
➢ Gradually increase to 2 mg TID.

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Chapter 8; Respiratory related disorders


and infections

8.1. Pneumonia (የሳንባ ምች)


Pneumonia is an acute inflammation of the distal lung-terminal airways,
alveolar spaces, and interstisium.
Common cause of significant morbidity and mortality
The clinical presentation and the aetiology vary greatly depending on the
age of the patient, the infecting organism, the site/s the infection has
involved, the immune status of the patient and the place of acquisition
of infection.
can be classified as;
✓ Community acquired (CAP)→ most common than other type of
pneumonia
✓ Hospital acquired (HAP)
✓ Ventilator-associated pneumonia (VAP)
✓ Healthcare-associated pneumonia (HCAP)

Pathophysiology
❖ Results from the proliferation of microbial pathogens at the alveolar
level and the host’s response to those pathogens
❖ Microorganisms gain access to the lower respiratory tract in several
ways;
✓ Aspiration from oropharynx
✓ Inhalation as contaminated droplets
✓ hematogenous spread → rare

Pathology
Pneumonia evolves through 4 interrelated series of pathologic changes

1. Alveolar oedema → The presence of a proteinaceous exudate and


bacteria
2. Red hepatization phase → Erythrocytes and neutrophils predominate,
Bacteria are occasionally seen
3. Gray hepatization phase → RBCs are degraded, neutrophils
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successful containment of the infection and improvement in gas


exchange
4. Resolution phase → The debris of neutrophils, bacteria, and fibrin
are cleared

Risk factors
Intrinsic factors- host factors
Extrinsic factors- exposure to a causative agent, pulmonary irritants,
or direct pulmonary injury

Intrinsic factors Extrinsic factors- virulence factors


✓ Age ✓ C. pneumonia produce a
✓ Loss of protective upper air way cilostatic factor
reflexes ✓ M. pneumonia can shear off
☛ Altered mental status cilia
☛ Endotracheal intubation ✓ Influenza virus markedly
✓ Immunosuppression reduces tracheal mucus velocity
✓ Dysfunction of local defense ✓ S. pneumonia and N.
mechanisms meningitidis produce proteases
☛ Smoking that can split secretory IgA
☛ COPD, bronchiectasis, CF
☛ Tumors
✓ Chronic periodontitis

Diagnosis of pneumonia

Imaging
Chest X-ray

Typical consolidation
Classification of pneumonia → Lobar, bronchopneumonia, interstitial
pneumonia
May suggest etiologic diagnosis- eg- pneumatoceles suggest infection
with S. aureus
Risk factors for increased severity- cavitation or multilobar
involvement
Complications- eg- parapneumonic effusion, pneumothorax
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Etiologic Diagnosis

Clinical diagnosis with radiologic support usually suffices to diagnose


most patients with pneumonia.
Treatment directed at a specific pathogen is not generally superior to
empirical therapy based on clinical and radiologic diagnosis
Indications for etiologic diagnosis
✓ Severe CAP requiring ICU admission
✓ Severe HAP/VAP
✓ Suspicion of pathogens with important public safety implications
☛ M. tuberculosis
☛ Legionella
☛ Influenza virus
☛ Community aquired MRSA (CA-MRSA)
☛ Agents of bioterrorism
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❖ CBC
✓ Leucocytosis → Lymphocyte dominant in viral and fungal causes,
Neutrophil dominant in bacterial causes
❖ AFR (ESR and CRP)
❖ Pleural fluid analysis: any parapneumonic effusion should be analyzed.
❖ PICT and RBS
❖ electrolytes, BUN/Cr, LFTs
❖ Gram’s stain and culture of sputum
❖ Blood culture → about 10 % can be positive.
❖ Antigen tests → Urine antigen tests for pneumococcal and legionella,
Have high sensitivity and specificity
❖ PCR
❖ serology

N.B the following three are diagnostic for pneumonia

I. Typical CXR findings


II. Leucocytosis
III. Raised ESR

DDx of pneumonia

1. Acute bronchitis
2. Acute exacerbation of COPD
3. Bronchial asthma
4. Heart failure
5. Pulmonary embolism
6. Radiation pneumonitis

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8.1.1. Community-Acquired pneumonia (CAP)

Aetiology – can be caused by bacteria, fungi, viruses, and protozoa


“Typical” bacterial causes
✓ S.pneumonia- the most common cause
✓ H. influenza, M. catarrhalis (espec. in COPD’ers)
✓ Pseudomonas
✓ Klebsiella & other GNR (espec. in alcoholics & aspirators)
✓ S. aureus (espec. post-viral infection)
“Atypical” causes
✓ Mycoplasma pneumonia
✓ Chlamydia pneumonia
✓ Legionella (espec. in elderly, smokers, T immunity)
✓ Influenza viruses
✓ Adenoviruses
✓ Respiratory syncytial virus
No organism identified in 40–60% cases

Clinical manifestations
“Typical”:
acute onset of fever
cough with purulent sputum
chest pain
dyspnea
Increased or decreased tactile fremitus and dull percussion note
Crackles, BBS, and/or pleural friction rub
consolidation on CXR

“Atypical”: (originally described as culture negative): tends to present


with
insidious onset of dry cough
extra pulmonary symptoms (N/V, diarrhoea, headache, myalgias,
sore throat)
patchy interstitial pattern on CXR
elevated transaminases & low serum Na with Legionella.

N.B
☛ Signs, symptoms & imaging do not reliably distinguish between
“typical” (S. pneumo, H. flu) and “atypical” (Mycoplasma,
Chlamydia, Legionella, viral)
☛ The clinical presentation may not be so obvious in the elderly, who
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may initially display new-onset or worsening confusion


☛ Severely ill patients may have septic shock and evidence of organ
failure

Management of CAP

CAP outpatient without comorbidities or other risk


First line

✓ Amoxicillin 1g, PO, TID, for 5 - 7 days

Second line

✓ Azithromycin, 500mg po daily for 3 days (500mg P.O., first day then
250mg P.O. daily, for 4d) or
✓ Clarithromycin, 500mg P.O. BID for 5-7 days Or
✓ Doxycycline, 100mg P.O., BID for 7-10 days.

CAP outpatient + with risk or comorbidities (chronic


heart, lung, kidney or liver disease, DM, alcoholism,
malignancy, asplenia), elderly, recent antibiotic use (within
3 months)
First line

✓ Augmentin (Amoxicillin-clavulanate), 625mg P.O., TID for 5-7days


☛ Or 1g (875 mg/125 mg), PO, BID or
☛ 2g/125 mg, PO, BID
plus
✓ Azithromycin, 500mg po daily for 3 days (500mg P.O., first day then
250mg P.O., for 4d.) or
✓ Clarithromycin, 500mg P.O. BID for 5-7 days OR
✓ Doxycycline, 100mg P.O., BID for 7-10 days.

Second line

✓ Cefuroxime 250-500mg, po, bid for 5-10 days Plus


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✓ Azithromycin, 500mg po daily for 3 days (500mg P.O., first day then
250mg P.O., for 4d.) OR
✓ Clarithromycin, 500mg P.O. BID for 5-7 days

Prevention
➢ Influenza vaccination
➢ Pneumococcal vaccination is critical for at risk patients
✓ may be given for ≥65 years old patients and others with risk factors
(eg, chronic heart, lung, and liver disease, immunocompromised, and
impaired splenic function)
➢ Smoking cessation should be encouraged during the initial visit
➢ Other infection prevention measures

8.1.2. Hospital-acquired pneumonia /HAP/


(Nosocomial Pneumonias)

Hospital-acquired (or nosocomial) pneumonia (HAP) is pneumonia that


occurs 48 hours or more after admission and did not appear to be
incubating at the time of admission.
Ventilator-associated pneumonia (VAP) is a type of HAP that develops
more than 48 to 72 hours after endotracheal intubation.
Healthcare-associated pneumonia (HCAP) is used to classify patients
with multidrug resistance (MDR) pathogen risk. This is no more used
currently. Currently HCAP is classified under CAP. Specific risk factors
for resistance include recent antimicrobial use, comorbidities, functional
status, and severity of illness.

Investigation and Diagnosis

▪ Three key criteria are required for the diagnosis of HAP and VAP
1. A new or progressive lung infiltrate of infectious origin
2. Clinical presentations (after 48 hours of admission for HAP and
after 48 hours of intubation for VAP) ensuring an infection (fever,
purulent sputum, leucocytosis, decline in oxygenation)
3. A positive pathogen identified on microbiologic respiratory samples.
Despite the controversies on the type of samples taken and the
analysis method, microbiologic cultures are absolutely required for
guiding the empiric therapy in HAP/VAP and has to be taken prior
to the first antibiotic dose administration.
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Management
The antibiotic choice should depend on the epidemiology and
susceptibility of local pathogens.
Empiric treatment should include antimicrobials effective against
resistant gram-positive and gram-negative organisms particularly
S.aureus and P.aeruginosa.
The following are possible combinations: Empiric treatment for
commonly suspected etiologies of HAP.

First line

✓ Vancomycin 1g I.V. BID for 10-14 days (particularly in the ICU setup
and in ventilator associated pneumonia)
PLUS
✓ Ceftazidime, 2gm I.V. TID for 10-14days Or
✓ Cefepime, 2 g, IV, TID

2nd line

✓ Ceftriaxone, 1-2g I.V. OR I.M. BID for 7 days.


PLUS
✓ Gentamicin, 5 to 7 mg/kg IV daily for 7 days. OR
✓ Ciprofloxacin, 400 mg IV TID for 7 days. (IV can be changed to 750
mg, PO, BID once patient is stable and able to take PO)

3rd line → reserved for microbiologic data proven resistance for 1st and
2nd line options

Alternative for vancomycin


☛ Meropenem, 1gm IV (infused slowly over 30min) TID OR
☛ Imipenem-cilastatin, 500mg IV (infused slowly over 1hour) QID
Alternative for gentamycin
☛ Amikacin 15 to 20 mg/kg IV daily

If methicillin-resistant (MRSA) suspected

✓ Vancomycin, 1 g I.V. BID should be added to the existing empric


regimen

N.B. All empiric regimens are subject to modification on the arrival of


microbiologic results and other evidences. De-escalation to narrow spectrum
antibiotics and oral regimens are always
encouraged in the appropriate circumstances.
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HAP Management with one of the following

➢ Septic shock
➢ Requiring mechanical ventilation
➢ Received antibiotic in the last 90 days

A combination of three antibiotics: one from of the following lists

➢ Vancomycin 1gm (15 mg/kg), IV, BID - TID (for severe cases, loading
dose 25 –30 mg/kg, maximum 3g)

PLUS

➢ One of the following


o Ceftazidime 2 g IV TID
o Cefepime 2 g IV TID
o Meropenem 1 g IV TID
o Imipenem 500 mg IV QID
o Piperacillin-tazobactam 4.5 g IV q6h
PLUS
➢ One of the following
o Gentamicin 5–7 mg/kg IV daily
o Ciprofloxacin 400 mg IV TID

8.1.3. Aspiration pneumonia:

Aspiration pneumonia is a pulmonary reaction resulting from the


abnormal entry of fluid, particulate exogenous substances, or
endogenous secretions into the lower airways.
Most cases arise following gross "aspiration" of microorganisms from
the oral cavity or nasopharynx.
If untreated, pneumonia may complicate to lung abscess, necrotizing
pneumonia, or empyema secondary to a Broncho pleural fistula.

Conditions that predispose to aspiration

✓ Altered consciousness due to alcoholism/drug overdose, seizures/head


trauma, general anaesthesia
✓ Dysphagia due to various reasons (e.g., stricture, neoplasm,
xerostomia, etc)
✓ Neurologic disorder (e.g. cerebrovascular accident)
✓ Mechanical disruption of the usual defence barriers (e.g. intubation)
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✓ Other: Protracted vomiting, pharyngeal anaesthesia, general debility,


recumbent position, glottic insufficiency etc.

Aspiration pneumonia is caused by a compromise in the usual defences


that protect the lower airways and then introduction of inoculum
deleterious to the lower airways.
The inoculum will either be directly toxic or stimulate the inflammatory
process or obstruct the airway.
The three syndromes of aspiration are:
1. chemical pneumonitis
2. bacterial infection and
3. airway obstruction.

Clinical features
✓ Mostly indolent course over several days or weeks
Fever, cough, purulent sputum, and dyspnea
Systemic disease symptoms: night sweets, weight loss, anemia
Hemoptysis or pleurisy
Copious putrid or malodorous sputum is typical for anaerobic infection
Absence of chills or rigors

Investigations and diagnosis


✓ Chest X-ray
✓ gram stain and culture
✓ Pleural fluid analysis and blood cultures

Management of aspiration pneumonia


antibiotics are indicated only in documented respiratory tract infection
(clinical, radiologic and microbiologic confirmation required)

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Community onset Aspiration Pneumonia Mixed infection


(anaerobes and facultative anaerobes like oral streptococci)

Mild to moderate
First line

✓ Amoxicillin clavulanate 625mg PO TID or (875 mg/125 mg BID, or


2,000 mg/125 mg BID) x 7 days or
✓ Ampicillin-sulbactam 1.5 - 3 g IV QID

Second line

✓ Amoxicillin 500 mg PO TID x 7 days or


✓ Penicillin G 1 - 2 million units, IV, QID x 7 days
PLUS
✓ Metronidazole, 500 mg, PO, TID x 7 days

➢ Clindamycin 600 mg IV TID is appropriate for penicillin-allergic patients.

Severe
First line

✓ Ampicillin sulbactam 1.5 - 3 g IV QID x 7 days

Second line

✓ Ceftriaxone 1g IV BID (2 g IV daily) or


✓ Cefotaxime 1 - 2 g IV TID
PLUS
✓ Metronidazole 500 mg, IV, TID x 7 days

Hospital onset Aspiration Pneumonia


(aerobic bacteria, especially Gram -ve bacilli and S.aureus, are more likely
than the anaerobes)
First line
✓ piperacillin tazobactam 2g IV TID x 7 days

Second line

✓ Ceftazidime 2g IV TID to QID or 986


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✓ cefepime 2 g IV BID to TID or


✓ Meropenem, 1gm IV (infused slowly over 30min) TID

➢ If risk factor for MRSA (e.g MRSA colonization), add vancomycin; if


MRSA is not detected in a culture, discontinue it.

8.1.4. Severe pneumonia


Assessment of severity is important to decide the place of care of
the patient
Patients with severe pneumonia should be hospitalized
There are currently two sets of criteria
1. CURB-65
2. The pneumonia severity index (PSI)

➢ CURB-65 – easy and commonly used scoring system which stands for:

✓ Confusion* (1 point)
✓ Urea >20 mg/dL (7 mmol/L) ** (1 point)
✓ RR ≥30 bpm (1 point)
✓ SBP (<90 mmHg) or DBP (≤60 mmHg) (1 point)
✓ Age ≥65 years (1 point)

*Defined as an Abbreviated Mental Test Score ≤8 or new disorientation to


person, place, or time.
**Urea is blood urea nitrogen [BUN], expressed in mg/dL or serum urea
concentration, expressed in mmol/L.

0 to 1 point: Low severity (risk of death <3%) Outpatient treatment, PO antibiotic

2 points: Moderate severity (risk of death 9%)

High severity (risk of death 15 to In patient, IV antibiotic immediately after culture


3 to 5 points:
40%)

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ICU admission criteria

➢ CURB-65 predictive rules however, are not used as criteria for high-level
(ICU) care and treatment intensification.
➢ The Infectious Disease Society of America (IDSA) recommends either 1
major criterion or ≥ 3 minor criteria for ICU admission criteria.

➢ Major criteria (If one)


Septic shock with need for vasopressors
Respiratory failure requiring mechanical ventilation

➢ Minor criteria (≥ 3)
RR ≥ 30 bpm
Hypothermia (core temperature, <36C)
Hypotension requiring aggressive fluid resuscitation
Multilobar infiltrates
Confusion/disorientation
Uraemia (BUN level ≥20 mg/dl)
Leukopenia /infection related only/ (WBC, <4,000 cells/ml)
Thrombocytopenia (platelet count, <100,000/ml)
PaO2/FI O2 ratio ≤250

Management of Severe Pneumonia (Community acquired


hospitalized patients)

Bed rest
Frequent monitoring of V/S in order to detect complications early and
to monitor response to therapy.
Give attention to fluid and nutritional replacements.
Administer Oxygen via nasal prongs or face mask
The Antibiotic choice should be aimed at the most likely causative
agent.
Empiric treatment for pneumonia due to common organisms:

First line

✓ Ceftriaxone 1g, IV, BID for 5 to 7 days OR


✓ cefotaxime 500mg, IV, QID for 5 to 7 days
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PLUS
✓ Azithromycin, 500mg po daily for 3 days OR
✓ Clarithromycin, 500mg P.O. BID for 5-7 days

Second line

✓ Augmentin 625mg P.O., TID for 5-7days


plus
✓ Azithromycin, 500mg po daily for 3 days OR
✓ Clarithromycin, 500mg P.O. BID for 5-7 days

N.B. In a situation of beta lactam allergy, respiratory fluoroquinolones


(moxifloxacin or levofloxacin) can be used. As these medicines are second
line medicines for Tuberculosis, they should only be used when it is
absolutely important.

8.1.5. Empyema and Complicated Parapneumonic


Effusions

Uncomplicated Complicated Empyema


parapneumonic effusion parapneumonic effusion
An exudative effusion with either of An exudative effusion with Refers to invasion of
the following characteristics negative pleural fluid the pleural space by
➢ Small size (1cm in lateral culture and gram stain along a significant number
decubitus position), non-loculated: with the presence of one of of bacteria. The
gram stain, culture, glucose level the following: presence of either of
of pleural fluid being unknown ➢ Large non-loculated (free the following defines
OR flowing) pleural effusion empyema
➢ Moderate size (>1cm but <1/2 of involving >1/2 of the ➢ Gross pus OR
the hemithorax), non loculated: hemithorax ➢ Positive gram stain
gram stain and culture confirmed ➢ Loculated pleural effusion or positive culture
to be negative and pleural fluid ➢ Pleural effusion with from pleural fluid.
glucose >60mg/dl. thickened pleura
➢ Pleural fluid glucose
<60mg/dl

Clinical features
➢ The clinical features of parapneumonic effusion are similar to pneumonia.
Pleuritic chest pain and prolonged fever are more common in patients who
develop complicated parapneumonic effusion or empyema.
➢ Physical examination: signs of pleural effusion (dullness, decreased or absent
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air entry, decreased tactile fremitus) will be present.

Investigations
→ In addition to the investigations mentioned for pneumonia
❖ Pleural fluid cell count with differential, LDH, Protein, glucose, gram
stain, culture and AFB
❖ Chest ultrasound → useful for suspected loculated pleural effusion
❖ Chest CT scans → if CXR and ultrasound are not conclusive

Treatment

Table: Management of parapneumonic effusion and empyema

Types Treatment
Uncomplicated parapneumonic effusion Antibiotics alone, no drainage
Complicated parapneumonic effusion Chest tube drainage* (also called tube
thoracostomy) + Antibiotics
Empyema Urgent chest tube drainage* (tube thoracostomy) +
antibiotics
*If clinically & radiologically improve and drainage rate fall below <50 ml/day for 2 to 3
days, remove chest tube
*If no improvement: assess antibiotic coverage (re-culturing, reviewing anaerobic and MDR
pathogens coverage) and evaluate for the presence undrained loculated pockets.

Surgery (beyond chest tube drainage):


➢ Options: thoracoscopic drainage, standard thoracotomy, or open drainage
➢ Indications: Multiple loculations or lack of improvement with chest tube drainage 990
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Empiric antibiotic treatment

☛ All patients with parapneumonic effusion or empyema need an antibiotic


therapy. Antibiotics should be administered promptly (not delayed for
sampling or drainage procedures) for better outcome.
☛ Anaerobic coverage should be maintained irrespective of culture results as
anaerobic organisms are difficult to grow.
☛ The duration of antibiotic should be decided on patient by patient basis;
mainly based on clinical response. Complete radiologic resolution might take
months.

Table: Empiric therapy for adult parapneumonic effusion or empyema


patients

Types of effusion First line Second line Duration


Uncomplicated ✓ ceftriaxone ✓ amoxicillin-clavulanat
parapneumonic 1-2 wks
Effusion
Community Complicated ✓ ceftriaxone or ✓ ampicillin-sulbactam
Acquired parapneumonic plus ✓ piperacillin-tazobactam 2-3 wks
Effusion ✓ metronidazole
Empyema if allergy: 4-6 wks
✓ metronidazole
plus
✓ levofloxacin or
✓ ciprofloxacin
Uncomplicated ✓ vancomycin ✓ vancomycin
parapneumonic plus plus 1-2 wks
Effusion ✓ ceftazidime or ✓ piperacillin-tazobactam
Complicated ✓ cefepime or 2-3 wks
Hospital parapneumonic plus ✓ ticarcillin-clavulanate or
Acquired Effusion ✓ metronidazole ✓ Meropenem/imipenem
Empyema 4-6 wks
If series penicillin-allergic:
✓ vancomycin plus
✓ metronidazole plus
✓ ciprofloxacin

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Follow up
❖ Uncomplicated parapneumonic effusion
✓ repeat imaging after 48-72 hour of antibiotic treatment initiation for
any completion
❖ Complicated PE and empyema
✓ has microbiologic (easy to grow) or biochemical evidence of
infection, at risk of poor outcome (may need repeated procedure
or surgery or hospitalization)
✓ repeat CT after 48-72 hour of antibiotic treatment initiation for
response
❖ empyema
✓ If possible, discharge with 2 weeks follow up schedule
✓ If failed response:
➢ assess antibiotic coverage (re-culturing directly from the
pleural space or undrained locule but not from tube or
catheter drain) and
➢ adjust antibiotic coverage for anaerobes and MDR
pathogens and
➢ assess for a need for additional drainage

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8.2. Acute tonsillopharyngitis (የቶንሲል በሽታ ፣ የአንቃር


እና ጉሮሮ ብግነት)

Sore throat (Tonsillopharyngitis) is a symptom caused by inflammation of


pharynx, tonsils or other surrounding structures.
The inflammation can be due to infectious causes (bacterial or viral) or
non-infectious causes related to environmental exposure such as air
pollution and allergens.
Viruses are the predominate causes of sore throats, however Group A Beta
Hemolytic Streptococci are the commonest bacterial causes of sore throat
(20-40% of sore throats in children and 5-15% of sore throats in adults).

Etiology Causative organisms


Bacteria Viruses Based on age Based on findings
➢ S. pyogenes ➢ Rhinovirus ➢ < 3 years Exudates and
(GABHS) ➢ EBV  100 % viral Lymphadenopathy
➢ C. diphtheriae ➢ Adenovirus ➢ 5-15 years ➢ GABHS
➢ N. gonorrhoeae ➢ Influenza A, B 15-30 % GABHS ➢ EBV
➢ Coxsackie A ➢ Adult ➢ Adenovirus
➢ Parainfluenza 10 % GABHS ➢ HIV
➢ Candida albicans
➢ Francisella tularensis

8.2.1.1. Streptococci tonsilloPharyngitis

Infection is acquired through contact with another individual carrying the


organism.
o Respiratory droplets are the usual mechanism of spread, although
other routes, including food-borne outbreaks, have been well
described.
o Spread more in crowded areas (KG, school, army.)
Although seen in patients of all ages, GAS pharyngitis is one of the most
common bacterial infections of childhood
o Accounts for 20 - 40% of all cases of exudative pharyngitis in
children
o it is rare among those under the age of 3.
o Most common among 5-15 age group declines in late adolescence
and adulthood.
More frequent among lower socio-economic classes
Most common during winter and spring 993
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Clinical manifestations

❖ Younger children may manifest streptococcal infection with a syndrome of


fever, malaise, and lymphadenopathy without exudative pharyngitis.
❖ The incubation period is 1 - 4 days.
❖ Symptoms include;
o Sore throat or Pain on swallowing
o fever and chills (> 38 C)
o malaise, and
o Headache, nausea, vomiting and abdominal pain may be present
especially in children.
❖ Both symptoms and signs are quite variable, ranging from mild throat
discomfort with minimal physical findings to high fever and severe sore
throat
❖ Pain on swallowing that radiates to the ear.
❖ Opening the mouth is often difficult and painful if it is complicated.
❖ Usually associated with systemic symptoms like Headache and marked
feeling of malaise, chills, rigor, Nausea, vomiting
❖ Absence of coughing
❖ Absence of nose drip
❖ Absence of hoarseness
❖ Streptococcal infection is an unlikely cause when symptoms and signs
suggestive of viral infection are prominent (conjunctivitis, coryza, cough,
hoarseness, or discrete ulcerative lesions of the buccal or pharyngeal
mucosa).

Signs
❖ Tonsillar swelling with hyperemia / exudates (Inflamed and reddened
enlarged tonsils)
o Exudates are apparent in bacterial tonsillitis, hyperemia only may be
from viral causes (but this differentiation is not stereotypical)
❖ Tender cervical lymphadenopathy
o Enlarged, tender anterior cervical lymph nodes commonly accompany
exudative pharyngitis
❖ Beefy red swollen uvula, petechia on the palate and scarlatiniform rash
❖ Soft palate petechia
❖ Other features that support the diagnosis include palatal petechiae, a
scarlatiniform rash, and a strawberry tongue (eg, Scarlet fever).

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Pictures; Tonsillopharyngitis

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Diagnostic approach

Mc Isaac Scoring (The Centro Clinical Decision Rule /CDR/)

Clinical Findings Score


I. Fever > 380C 1
II. Absence of coughing 1
III. Tonsillar hypertrophy or exudates 1 (if< 6 years give 0)
IV. Swollen and tender cervical LN 1
V. Age 3 – 14 1
☛ Age > 45 -1

≥ 2 points, treat as GABHS pharyngitis (with antibiotic)


< 2 points, treat as viral pharyngitis (no antibiotic)

In Ethiopia it is recommended to use clinical decision rule for the diagnosis


of bacterial tonsillopharyngitis.

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Total score Probability of strep Suggestions


0 & 1 points < 10% No culture, no antibiotics
2 point 11-17% Take culture (or antigen test), order
3 points 28-35% antibiotics only if GABHS +ve
4 & 5 points 52% ➢ Take culture (or antigen test), order
antibiotics only if GABHS +ve
➢ If the c/f is severe, start antibiotics
without testing

8.2.1.2. Viral tonsillitis/pharyngitis

The following features strongly suggest a viral rather than a streptococcal


etiology. These are
o Cough
o Runny nose
o Conjunctivitis
o Hoarseness
o Coryza
o Anterior stomatitis
o Discrete intra-oral ulcerative lesions
o Viral exanthema
o Diarrhea and
o Absence of fever
Viral tonsilo-pharyngitis is most common.
Rhinovirus (most common).
Symptoms usually last for 3-5 days.
Having additional rhinitis, hoarseness, conjunctivitis and cough
Pharyngitis is accompanied by conjunctivitis in adenovirus infections
Oral vesicles, ulcers point to viruses

Figure: Bacterial Vs Viral Pharyngitis


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Complication of Tonsillitis due to Streptococci


Can be classified as Suppurative and Nonsuppurative or local and systemic
Suppurative complications result from the spread of infection from the
pharyngeal mucosa to deeper tissues by direct extension or by the
hematogenous or lymphatic route
o Suppurative complications of streptococcal pharyngitis have become
uncommon with the widespread use of antibiotics for most
symptomatic cases.
Nonsuppurative complications are thought to result from immune responses
to streptococcal infection.
o Penicillin treatment of streptococcal pharyngitis reduces the likelihood
of ARF but not that of PSGN.

Suppurative VS Nonsuppurative local VS systemic


Suppurative complications Local complications
➢ peritonsillar or retropharyngeal abscess ✓ peritonsillar abscess
o These local complications should be ✓ parapharyngeal abscess
considered in a patient with unusually ✓ retropharyngeal abscess
severe or prolonged symptoms or localized
pain associated with high fever and a toxic Systemic complication
appearance. ✓ Septicemia
➢ cervical lymphadenitis ✓ ARF
➢ sinusitis ✓ PSGN
➢ otitis media
➢ mastoiditis
➢ meningitis
➢ bacteremia
➢ endocarditis and
➢ pneumonia.
➢ Recurrent tonsillitis/pharyngitis

Nonsuppurative complications
➢ ARF (Acute rheumatic fever)
o Due to cross reaction to type 5 M-protein
➢ PSGN (Post streptococcal glomerulonephritis)
o PSGN is an acute glomerulonephritis (AGN)
due to nephritogenic strains
➢ Poststreptococcal reactive arthritis (PSRA)
➢ Scarlet fever
➢ Streptococcal toxic shock syndrome

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Investigation
➢ In our set up it is usually a clinical diagnosis. But ‘’Harrison’’ didn’t
recommend clinical diagnosis
o ‘’Because of the range of clinical presentations of streptococcal
pharyngitis and the large number of other agents that can produce
the same clinical picture, diagnosis of streptococcal pharyngitis on
clinical grounds alone is not reliable’’.
➢ Rapid diagnostic kit (for latex agglutination or enzyme immunoassay of
swab specimens)
✓ is a useful adjunct to throat culture.
✓ >95% specific. but, less sensitive (55–90%).
o Thus, a positive result can be relied upon for definitive
diagnosis and eliminates the need for throat culture
o A negative result should be confirmed by throat culture.
➢ Throat swab culture → Gold standard
o It is hard to differentiate viral and bacterial cause based on symptom
and sign alone. Thus, Throat swab is done to r/o bacterial cause
o Culture of a throat specimen that is properly collected (i.e., by
vigorous rubbing of a sterile swab over both tonsillar pillars) and
properly processed is the most sensitive and specific means of
definitive diagnosis.
o Not required usually. Needed only when suspicion is high and rapid
strep throat swab is negative.
o Pathogens looked for
▪ GAS
▪ C. diphteriae (rare)
▪ N. gonorrhoeae (rare)
➢ ASO
✓ May remain +ve for 1 year
➢ Peripheral smear → BF (to r/o malaria in endemic area)
➢ CBC and ESR

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Treatment of GABHS
General Management
o Analgesics/Antipyretic (paracetamol) for relief of pain and fever.
o Identification and early treatment of complications
o Avoid cold drinks
o Hydration and rest may be needed.

The goal of antibiotic therapy for streptococcal pharyngitis is multifold and


includes:
o Reducing symptom severity and duration
o Prevention of acute complications, such as otitis media, peritonsillar
abscesses, or other invasive infections
o Prevention of delayed complications or immune sequelae, particularly acute
rheumatic fever
▪ The primary benefit of treatment is the prevention of acute rheumatic
fever, which is almost completely successful if antibiotic treatment is
instituted within 9 days of illness.
o Prevention of spread to others

Adjunctive treatment
➢ Supportive care (rest, adequate fluid intake, avoidance of respiratory
irritants, soft diet) to all patients and
➢ NSAIDs or PCM for fever or pain control.

Antibiotics in Tonsillitis/pharyngitis due to GABHS

➢ Antibiotic treatment is the mainstay of care.

Table; Treatment of Tonsillopharyngitis due to group A Streptococcus


Antibiotic class Drug Dosing in adults Dosing in pediatrics
(select one)
First line Penicillin’s@ Penicillin G 1.2 million units, IM, <30kg: 600,000 units, IM, stat36
benzathine35 stat
>30 kg: the same as adult dose
Amoxicillin 500 mg, PO, TID for 50 mg/kg/day (maxi;1g/day), PO, BID
10 days or TID for 10 days

35
NEVER EVER GIVE BPG INTRAVENOUSLY THIS MAY LEAD TO IMMEDIATE DEATH!!

BPG is the drug of choice for GAβHS sore throat


36
<<National NCD management protocol 2021>> and <<NATIONAL TRAINING ON
RHEUMATIC HEART DISEASE PREVENTION & CONTROL FOR HEALTH CARE
WORKERS IN ETHIOPIA: Participant’s Manual October 2021 Addis Ababa>> says for
600,000 units for children ≤ 30kg
UpToDate 2018, says 600,000 units for children ≤ 27kg.
1000
We recommend to use national Guidelines cut point value (30 Kg)
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Penicillin V 500 mg, PO, BID to If ≤ 30 kg: 250 mg, PO, BID to TID,
TID for 10 days for 10 days

If >30 kg: the same as adult dose


Alternatives Cephalosporins Δ Cephalexin 500 mg, PO, BID for 40 mg/kg/day, PO, BID for 10 days
(used if there is 10 days (max; 500 mg/dose)
allergy to
penicillins. See Cefuroxime 250 mg, PO, BID for 10 mg/kg/dose, PO, BID, for 10 days
foot note) 10 days (max; 250 mg/dose)
Cefixime 400 mg, PO, daily to Children ≥6 months and ≤45 kg:
BID, for ≥ 10 days ✓ 8 mg/kg/day, PO, daily to BID for
≥10 days (max: 400 mg/day);
available preparation; 100mg/5ml
Children >45 kg or >12 years:
✓ The same as Adult dose
Cefpodoxime 100 mg, PO, BID for 5 mg/kg/dose, PO, BID (max; 100
5 - 10 days mg/dose), for 5 to 10 days
Cefdinir 300 mg, PO, BID for 7 mg/kg/dose, PO, BID, for 5 to 10
5 - 10 days or days or

600 mg, PO, daily 14 mg/kg/dose, daily for 10 days


for 10 days (max; 600 mg/day)
Macrolides# Azithromycin 500 mg, PO, daily 12 mg/kg (max; 500 mg/dose), PO,
for 3 days or daily for 3 days or

500 mg, PO, on day 12 mg/kg, on day 1 followed by 6


1 followed by 250 mg/kg/dose (max;250 mg/dose), PO,
mg on days 2 daily on days 2 through 5
through 5
Clarithromycin 250 mg, PO, BID, 7.5 mg/kg/dose (max; 250 mg per
for 10 days dose), PO, BID for 10 days
Erythromycin 250 mg, PO, QID, 10 mg/kg/dose, PO, QID (maxi; 250
for 10 days mg per dose) for 10 days
Lincosamides* Clindamycin 300 mg, PO, TID for 7 mg/kg/dose (max;300 mg per
10 days dose), PO, TID, for 10 days
@
Penicillin’s (oral penicillin, oral amoxicillin, or single-dose IM benzathine penicillin) are options for patients
with a history of acute rheumatic fever (who are high risk for cardiac complications compared with those
without this history)
➢ IM penicillin appears to be more effective than oral penicillin at eradication of GAS from the oropharynx
and has been most well studied for the prevention of acute rheumatic fever
Δ Cephalosporins are Potential alternatives in cases of penicillin allergy

if the nature of the allergy is mild reactions to penicillin, non-IgE-mediated reactions to penicillin (e.g.
maculopapular rash beginning days into therapy) a 1stgeneration cephalosporin such as cephalexin
For patients with mild, possibly IgE-mediated reactions (e.g. urticaria or angioedema but NOT anaphylaxis),
they use a 2nd- or 3rd-generation cephalosporin, such as cefixime, ceftriaxone, cefuroxime, cefdinir, or
cefpodoxime.
#
Macrolides are alternatives for patients with immediate hypersensitivity reaction (anaphylaxis) or another
potentially life-threatening manifestation (e.g., severe rash and fever). or other IgE-mediated reactions, who
cannot tolerate cephalosporins
In areas with resistance rates exceeding 5–10%, macrolides should be avoided unless results of
susceptibility testing are known. 1001
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cephalosporins cannot be tolerated.

Antibiotics NOT to be used for GABHS due to the high prevalence of resistance
include;

✓ Tetracycline
✓ Sulphonamides (e.g. Co-trimoxazole)
✓ Fluoroquinolones (e.g. Aminoglycosides)
✓ Chloramphenicol

➢ Follow-up culture after treatment is no longer routinely recommended but


may be warranted in selected cases, such as;
o Those involving patients or families with frequent streptococcal infections or
o Those occurring in situations in which the risk of ARF is thought to be
high (e.g., when cases of ARF have recently been reported in the
community).

Why Benzathine Penicillin is the drug of choice?


➢ Benzathine Penicillin G is preferable to the other alternative PO antibiotics
for treatment of tonsillopharyngitis.
▪ It is a single injection while oral treatment needs 10 whole days to be
effective
▪ BPG has better bactericidal effect than oral antibiotics
▪ GAβHS are universally sensitive for penicillin
▪ Oral macrolides (Erythromycin and azithromycin) show clinical
improvement but no eradication of organism.
▪ Cost effective, evidence based.
▪ Parents and patients more satisfied.
➢ In patients with a sore throat and symptoms suggestive of a GABHS
infection, antibiotic treatment using intramuscular BPG could reduce the risk
of RF by up to 80%.

Treatment of Asymptomatic Pharyngeal Colonization with GAS


When a carrier is transmitting infection to others, attempts to eradicate carriage
are warranted.
GAS (Group A streptococci) chronic carrier, treatment:
o Amoxicillin clavulanate 875/125 mg (1g), PO, BID for 10 days
▪ For pediatrics; Amoxicillin clavulanate syrup (400mg/5mL), 40
mg/kg/day, PO, TID, for 10 days (max: 2g/day)
Even though limited data, Regimens reported to have efficacy superior to that
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o a first-generation cephalosporin such as cephalexin (30 mg/kg; 500 mg


max), PO, BID for 10 days or
o Ceftriaxone, 1gm, IV, BID for severe cases
o clindamycin, 300mg (for children; 7 mg/kg; 300 mg max) PO, TID for 10
days.
o A 10-day course of vancomycin (250 mg, PO, QID) and rifampin (600 mg,
PO, BID) has eradicated rectal colonization.

Peritonsillar abscess
Inadequately treated acute or chronic tonsillitis can spread to the
surrounding tissue and form abscess called peritonsillar abscess

Clinical features

Severe pain such that the patient often refuses to eat


The head is held over to the diseased side, and rapid head movements
are avoided.
The patient has sialorrhea and oral fetor
Swelling of the regional lymph nodes
Fever with high temperatures of 39°C to 40°C and the general condition
deteriorates rapidly.
Redness, and protrusion of the tonsil, the faucial arch, the palate and the
uvula
Marked tenderness of the tonsillar area

Treatment of peritonsillar abscess

drainage of the abscess and tonsillectomy

Indication for tonsillectomy for tonsillopharyngitis patients

✓ Quality of life is affected significantly by recurrent acute pharyngitis


secondary to GAS
➢ 3 episodes yearly for ≥ 3 years or
➢ 5 episodes yearly for 2 years or
➢ 7 episodes in 1 year.
☛ Before considering tonsillectomy, each episode of pharyngitis should
be clearly documented with one or more of the following clinical
features:
1. temperature >38.3°C
2. cervical adenopathy
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4. positive test for group A streptococcal (GAS) infection


✓ Recurrent peritonsillar abscess
✓ Suspected malignancy
✓ Obstructive sleep apnea
✓ In rare cases, halitosis caused by cryptic tonsils and tonsilloliths (tonsil
stones).

✓ N.B. Tonsillectomy may decrease but does not eliminate the occurrence of
GABHS pharyngitis.

Prevention of transmission

GAS can spread among close contacts, leading to clusters of cases and
recurrent infections in households or other close-contact settings.
The rate of GAS transmission from an infectious case to close contacts is
estimated to be between 5 and 50 %.
Antibiotic use believed to eliminate GAS from the oropharynx in about 80 to
90 % of cases after 24 hours of therapy.
If untreated, approximately 50% of patients with streptococcal pharyngitis
will continue to harbor GAS in the oropharynx 3 to 4 weeks after symptom
onset.

Prevention methods
Hand hygiene
Postexposure prophylaxis
o Testing and treatment of asymptomatic persons who have been
exposed to a patient with GAS pharyngitis are not routinely
recommended
o Indication for post exposure prophylaxis
▪ Patients with a history of ARF during outbreaks of ARF
and/or PSGN, or
▪ When GAS infections are recurring in households or other
close-contact settings.

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8.3. Asthma (አስም)


➢ Asthma is a syndrome characterized by airflow obstruction that leads to
excessive narrowing with consequent reduced airflow.
➢ It is a heterogeneous disease with special type of inflammation in the
airways.
➢ Narrowing of the airways is usually reversible, but in some patients with
chronic asthma there may be an element of irreversible airflow obstruction.

Epidemiology
✓ Asthma is one of the most common chronic diseases globally and affects
~300 million people worldwide, with ~250,000 deaths annually.
✓ More common in developed countries where it affects,10-12% of adults and
15% of children
✓ In developing countries there is a rising prevalence associated with
increased urbanization.
✓ Occur at any age, peak at 3 years. 50% develop before the age of 10 and
another 35% before 40
✓ During Childhood M: F = 2:1 and in adulthood the ratio equalize.

RISK FACTORS AND TRIGGERS

Asthma is a heterogeneous disease with interplay between genetic


and environmental factors.
Risk factors distinguished from triggers;
o Risk factors are those which predispose someone to develop
asthma.
o Triggers are environmental factors that worsen asthma in a
patient with established asthma. i.e. trigger airway narrowing,
wheezing, and dyspnoea in asthmatic patients.

❖ ENDOGENOUS FACTORS
o Genetic Predisposition
o Atopy
▪ Atopy is the major risk factor for asthma
▪ Patients with asthma commonly suffer from other atopic
diseases, particularly allergic rhinitis, which may be found in >
80% of asthmatic patients, and atopic dermatitis (eczema).
▪ Atopy is due to the genetically determined production of
specific IgE antibody, with many patients showing a family
history of allergic diseases.
▪ It is likely that environmental factors in early life determine
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o Obesity → an independent risk factor for asthma, particularly in


women
o Gender

❖ ENVIRONMENTAL FACTORS
o Occupational Exposure
▪ Occupational asthma may be suspected when symptoms
improve during weekends and holidays.
▪ Occupational asthma is relatively common and may affect up
to 10% of young adults
▪ Cleaners commonly develop occupational asthma owing to
exposure to aerosols of cleaning liquids.
o Indoor and outdoor Air Pollution → Indoor air pollution is common
risk factor in our set up
▪ Indoor air pollution is also important risk factor with exposure
to nitrogen oxides from cooking stoves and exposure to
passive cigarette smoke. maternal smoking is a risk factor for
asthma.
o Diet
▪ The role of dietary factors is controversial.
▪ Diets low in antioxidants such as vitamin C and vitamin A,
magnesium, selenium, and omega-3 PUFA (fish oil) or high in
sodium and omega-6 PUFA are associated with an increased
risk of asthma.
▪ Vitamin D deficiency may also predispose to the development
of asthma.
▪ Some foods such as shellfish and nuts may induce
anaphylactic reactions that may include wheezing.
o Acetaminophen → may be linked to increased oxidative stress
especially in children

N.B Smokers with asthma have more severe disease, more frequent hospital
admissions, a faster decline in lung function, and a higher risk of death from
asthma than non-smoking asthmatics. Interferes with the anti-inflammatory actions
of corticosteroids

❖ Triggers
o Allergens
▪ Allergens Are derived from house dust mites, cat and dog fur,
cockroaches (in inner cities), grass and tree pollens, and
rodents (in laboratory workers).
▪ Other allergens, including grass pollen, ragweed, tree pollen,
and fungal spores, are seasonal.
▪ Pollens usually cause allergic rhinitis rather than asthma
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o Infections
▪ URTI such as Rhinovirus, RSV and corona virus are triggering
agents
▪ Atypical bacteria, such as Mycoplasma and Chlamydophila,
have been implicated in the mechanism of severe asthma.
▪ There is an increase in airway inflammation with increased
numbers of eosinophils and neutrophils.
o Drugs → e.g. Beta blockers like Propranolol, Metoprolol
o Stress
o Exercise and hyperventilation
▪ Exercise-induced asthma (EIA) typically begins after exercise
has ended, and recovers spontaneously within about 30
minutes.
o Cold Air
o Irritants (household sprays, paint fumes)

❖ Other Factors
o Lower maternal age
o Duration of breastfeeding
o Prematurity and low birth weight
o Inactivity

Pathophysiology of asthma
❖ Asthma is associated with a specific chronic inflammation of the respiratory
mucosa from the trachea to terminal bronchioles with a predominance in
the bronchi (cartilaginous airways)
❖ Airway inflammation in asthma is associated with airway hyper
responsiveness (AHR)
o AHR is the characteristic physiologic abnormality of asthma and
describes the excessive Broncho constrictor response to multiple
inhaled triggers that would have no effect on normal airways.
❖ Mediated by various inflammatory cells and their products
❖ Chronic inflammation is associated with structural changes in the airway
called airway remodeling
❖ Limitation of airflow
✓ Bronchoconstriction(mainly)
✓ Airway edema
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✓ Vascular congestion
✓ Luminal occlusion with exudate
❖ All the above results in
✓ Decrease FEV1, FEV1/FVC ratio & PEF
✓ Increase airway resistance and RV

Figure; Pathophysiology of asthma;


The two net results of pathophysiologic changes are;
o Airway obstruction (i.e. occlusion of the airway lumen by a mucous plug,
which is secreted from hyperplastic goblet cells) and
o Bronchoconstriction due to different neuro chemokine factors
Inhaled allergens activate mast cells with bound IgE directly leading to the
immediate release of Broncho constrictor mediators, resulting in the early response
that is reversed by bronchodilators.
The most common allergens to trigger asthma are Dermatophagoides species.
The airway mucosa is infiltrated with activated eosinophils and T lymphocytes, and
there is activation of mucosal mast cells.
The characteristic finding of Airway remodelling is thickening of the basement
membrane due to sub epithelial collagen deposition.
o It is the main cause of chronic asthma, which may later exacerbate due to
different triggering agents.
The epithelium is often shed or friable, with reduced attachments to the airway wall
and increased numbers of epithelial cells in the lumen.
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The airway wall itself may be thickened and oedematous (i.e. thickening of
basement membrane and smooth muscle).
And there is occlusion of the airway lumen by a mucous plug in fatal asthma.
which is comprised of mucous glycoproteins secreted from goblet cells (from goblet
cell hyperplasia which leads to mucus hyper secretion) and plasma proteins from
leaky bronchial vessels.
There is also vasodilation and increased numbers of blood vessels (angiogenesis).
The airways may be narrowed, erythematous, and oedematous.
Mast cells, which are found at the airway surface in asthma patients and also in
the airway smooth-muscle layer, are important in initiating the acute Broncho
constrictor responses to allergens and several other indirectly acting stimuli, by
releasing several Broncho constrictor mediators
Multiple inflammatory mediators (histamine, PG D2, and leukotriene) contract airway
smooth muscle, increase micro vascular leakage, increase airway mucus secretion,
and attract other inflammatory cells. With final effect of Bronchospasm, Mucus
secretion, AHR, & Structural changes.
Cysteinyl-leukotrienes are potent Broncho constrictors;
Cholinergic pathways, through the release of acetylcholine acting on muscarinic
receptors, cause bronchoconstriction and may be activated reflexly in asthma.

Different phenotypes of asthma.

➢ Atopic (extrinsic)
➢ Non-atopic (intrinsic)
➢ Occupational asthma
➢ Aspirin-sensitive and
➢ Paediatric asthma

Clinical features of asthma


The characteristic symptoms of asthma are wheezing, dyspnea, and
coughing, which are variable, both spontaneously and with therapy

Symptoms

❖ Wheezing (audible wheeze)


• The mere presence of wheezing doesn’t mean asthma and Lack of
wheezes does not exclude asthma.
• Wheezing in asthmatic patients is mostly diffuse and bilateral
• Persistent wheezing in a specific area of the chest may indicate
endobronchial obstruction with a foreign body (FBA).
• Left ventricular failure (cardiac asthma) may mimic the wheezing of
asthma but basilar crackles (basal rales) are present in contrast to
asthma

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• Upper airway obstruction by a tumor or laryngeal edema can mimic


severe asthma, but patients typically present with stridor localized to
large airways.
❖ Dyspnea
❖ Chest tightness
❖ Cough → may be associated with Tenacious mucus-difficult to expectorate
❖ Difficulty in filling their lung with air.
❖ Nasal itching and sneezing

Physical signs

❖ Wheeze
❖ Inspiratory, and to a greater extent expiratory rhonchi
❖ Hyperinflation
❖ Respiratory distress
❖ Skin lesion, Nasal discharge → may be related with atopy

❖ Symptoms may be worse at night and patients typically awake in the early
morning hours.
• Circadian variations in Broncho motor tone and bronchial reactivity
reach their nadir between 3 AM and 4 AM (i.e. between 9 and 10
NLT), increasing symptoms of bronchoconstriction.
❖ Some patients, particularly children, may present with a predominant non-
productive cough (“cough-variant asthma”).
❖ Prodromal symptoms may precede an attack
• Itching under the chin
• Discomfort between the scapulae
• Inexplicable fear (impending doom).
❖ Danger signs during acute attacks:
• Paradoxical breathing
• Profound diaphoresis
• Cyanosis
• Exhaustion Arrhythmia
• Silent chest on auscultation
• Mental status change (Drowsiness or confusion)
• Agitation
• SPO2 < 90 %

Features suggesting an alternate or comorbid condition


➢ Fever, Purulent sputum production, Urticaria, or Pleuritic chest pain should
raise the possibility of an alternative diagnosis such as pneumonia, flare of
bronchiectasis, anaphylaxis, or pneumothorax.

Impending respiratory failure:


➢ Cyanosis, inability to maintain respiratory effort, depressed mental status,
SpO2 <90%
➢ PaCO2 >40 mmHg 1010
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Diagnosis of asthma
1. Most of the time asthma is a clinical diagnosis
2. Peak Expiratory Flow (PEF)
o PEF meters are simple handheld devices designed as personal
monitoring tools in patients with asthma or COPD.
o A peak flow meter measures how fast air can be blown out of the
lungs.
o It is the maximum flow rate generated during a forceful exhalation,
starting from full lung inflation.
o PEF is measured in liters per minute.
o Normal adult peak flow scores range between around 400 and 700
liters per minute.

Figure: Example of a handheld Peak expiratory flow meter

Figure: How to Measure PEF using a peak flow meter

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Figure; Calculating percentage reversibility of PEFR

o A change in PEF rate of at least 20% is accepted as being


consistent with asthma. PEF rate values less than 200 L/min indicate
severe airflow obstruction.
o PEF rate can establish peak flow variability, quantify asthma severity,
and provide both patient and clinician with objective measurements
on which to base treatment decisions.
o It is affordable means of support in the diagnosis of asthma in the
primary health care level.
o The standard, however, for the diagnosis of asthma is pulmonary
function testing using spirometry

3. Spirometry
o Asthma FEV1 ↓sed but FVC is normal so FEV1/FVC ratio
decreased.
☛ In restrictive lung disease FEV1 and FVC decreased
simultaneously so the FEV1/FVC ratio is normal.
o Asthma a >12% and 200-ml increase in FEV1 15 min after an
inhaled short-acting β2-agonist (SABA; such as inhaled albuterol 400
μg) or in some patients by a 2 - 4-week trial of oral corticosteroids
(OCS) (prednisone or prednisolone 30–40 mg daily). But not in
COPD.

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Figure: Algorithm for diagnosis of Asthma using spirometry

4. Bronchoprovocation testing
5. Imaging (CXR &HRCT)

8.3.1. Acute asthma exacerbations


Asthma exacerbations are Acute or subacute worsening in symptoms and
lung function from the patient’s usual status.
May occur in patients with a pre-existing diagnosis of asthma or
occasionally as the first presentation of asthma
Usually occur in response to exposure to an external agent and poor
adherence with controller medication.
The best strategy for management of acute exacerbations of asthma is
early recognition and intervention, before attacks become severe and
potentially life-threatening.
Detecting exacerbations
o Symptoms → Breathlessness, Wheezing, Cough, and, Chest
tightness
o Peak flow → Provides an assessment of the severity of airflow
limitation

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Table; Severity of Asthma exacerbations


Parameters Mild Moderate Severe Life threatening
Dyspnea While talking At rest At rest
Talks in Sentences Phrases Words Unable to speak
Comfortable Can lie down Prefers sitting Sits up-right
Position
RR Increased Increased Often>30/min
PR <100 100-120 >120 Bradycardia
SpO2 (on air) >95% 90-95% <90%
Use of accessory Usually not Commonly Usually Paradoxical thoracic and
muscles abdominal movements
Wheeze Often end Throughout Throughout Absence of wheeze
expiratory expiration breathing cycle
Pulsus paradoxus Absent May be present Often present
(i.e. a fall in SBP
by at least 12
mmHg during
inspiration which is
an indicative of
severe airflow
obstruction)
Mentation Alert Usually agitated Agitated Drowsy or confused
A decrement in > 20 % 20 - 50 % > 50 % (i.e. PEF
PEF (peak < 50 % of
expiratory flow) baseline)
from normal, or
from the patient's
personal best value

Acute severe asthma


Exacerbations of asthma are feared by patients and may be life
threatening.

Clinical Features
Patients are aware of increasing chest tightness, wheezing, and dyspnea
that are often not or poorly relieved by their usual reliever inhaler.
In severe exacerbations patients may be so breathless that they are unable
to complete sentences and may become cyanotic.
Examination usually shows increased ventilation, hyperinflation, and
tachycardia.
Pulsus paradoxus may be present, but this is rarely a useful clinical sign.
There is a marked fall in spirometric values and PEF.
Arterial blood gases on air show hypoxemia, and PCO2 is usually low due
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A normal or rising PCO2 is an indication of impending respiratory failure


and requires immediate monitoring and therapy.

Risk factors for fatal asthma


➢ Previous severe exacerbation (e.g. intubation or ICU admission)
➢ Hospitalization for asthma in the past year
➢ Three or more emergency department visits for asthma in the past year
➢ Not currently using inhaled glucocorticoids
➢ Recent or current course of oral glucocorticoids
➢ Use of more than one canister of short-acting beta agonist per month
➢ Difficulty perceiving asthma symptoms or severity of exacerbations
➢ History of poor adherence with asthma medications and/or written asthma
action plan
➢ Illicit drug use and major psychosocial problems, including depression
➢ Comorbidities, such as cardiovascular or chronic lung disease

Asthma medications → can be divided as;

➢ Bronchodilators
➢ Controllers

1) Bronchodilators

☛ Bronchodilators act primarily on airway smooth muscle to reverse the


bronchoconstriction of asthma.
☛ This gives rapid relief of symptoms but has little or no effect on the underlying
inflammatory process.
☛ Thus, bronchodilators are not sufficient to control asthma in patients with
persistent symptoms.
☛ There are three classes of bronchodilator in current use:
1. β2-agonists
Short acting beta2 /𝛽2/ agonists (SABA) → e.g. Salbutamol
o Have a duration of action of 3 - 6 h, used as needed for immediate
symptom relief (relievers).
o SABA are the main stay of treatment and most effective bronchodilators
during exacerbations
o Salbutamol (Albuterol) Inhaler is available in Ethiopia.
Long acting beta2 agonists (LABA) → e.g. Salmeterol, Formoterol
o Usually available as Combination of ICS and bronchodilators → e.g.
fluticasone/salmeterol, budesonide/formoterol
o Have a duration of action of more than 12h and given BID 1015
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o LABAs should not be used as monotherapy since they have no anti-


inflammatory effect. Use with inhaled corticosteroids.
o They should not be used for symptom relief or exacerbations.

2. Anti-cholinergic (e.g. ipratropium bromide) → prevent cholinergic nerve-


induced bronchoconstriction and mucus secretion. They are less effective
than β2-agonists in asthma therapy as they inhibit only the cholinergic
reflex component of bronchoconstriction

3. Theophylline (e.g. aminophylline) → It has now fallen out of favor as


side effects are common, and inhaled β2-agonists are much more
effective as bronchodilators37
☛ of these, β2-agonists are by far the most effective

2) Controllers
☛ Controllers act primarily to inhibit the underlying inflammatory process
☛ They are taken daily independent of symptoms to achieve and maintain
control of persistent asthma.
☛ Important long-term control medications include
o Corticosteroids → ICS (inhaled corticosteroids) or OCS (oral
corticosteroids)
o Anti-leukotrienes → e.g. montelukast, zafirlukast. montelukast (adult
dose 10 mg once daily
o Chromones → e.g. cromolyn sodium, nedocromil sodium
o Steroid sparing → e.g. methotrexate, cyclosporine, azathioprine, gold,
IV gamma globulin
o Anti IgE → omalizumab

Currently, Anti-leukotrienes, Chromones, Steroid sparing, and Anti IgE are not
available in most set ups of Ethiopia

Corticosteroids

Corticosteroids are the most potent and consistently effective anti-inflammatory


agents currently available.

37
The 2021 STG for general hospitals of Ethiopia recommend that, ‘’Sustained-release theophylline
preparations (e.g. Theophedrine 120/11mg tablets daily to QID base) are effective in controlling nocturnal
symptoms and as added therapy in patients with moderate or severe persistent asthma whose symptoms
are inadequately controlled by ICS’’.
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They decrease both acute and chronic inflammation, resulting in reduced


symptoms and improved lung function.
These agents may also potentiate the action of beta-adrenergic agonists.
ICS (inhaled corticosteroids)
o ICS (See tables below) are by far the most effective controllers in the
management of asthma and are beneficial in treating asthma of any
severity and age.
o ICS are usually given BID, but some may be effective once daily in
mildly symptomatic patients.
o ICS rapidly improve the symptoms of asthma, and lung function improves
over several days.
o They are effective in preventing asthma symptoms, such as EIA
(Exercise induced asthma) and nocturnal exacerbations, but also prevent
severe exacerbations.
o ICS reduce AHR (Airway hyperresponsiveness), but maximal improvement
may
take several months of therapy.
o Early treatment with ICS appears to prevent irreversible changes in
airway function that occur with chronic asthma. Withdrawal of ICS results
in slow deterioration of asthma control, indicating that they suppress
inflammation and
symptoms, but do not cure the underlying condition.
o ICS are now given as first-line therapy for patients with persistent
asthma, but if they do not control symptoms at low doses, it is usual to
add a LABA as the next step.
Systemic Corticosteroids
o Corticosteroids are used intravenously (hydrocortisone or
methylprednisolone) for the treatment of acute severe asthma
o A course of OCS (usually prednisone or prednisolone 30 - 45 mg once
daily for 5 - 10 days) is used to treat acute exacerbations of asthma; no
tapering of the dose is
needed.
o Approximately 1% of asthma patients may require maintenance treatment
with OCS; the lowest dose necessary to maintain control needs to be
determined.
o Steroid-sparing therapies may be considered if side effects are a
significant problem.

➢ Add-on azithromycin (500mg, 3X/week or 250mg daily) for adult patients


with persistent symptomatic asthma despite moderate-high dose ICS and
LABA reduced asthma exacerbations.

Table: Inhaled corticosteroids (ICS) and Combinations for Adults and


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adolescents (≥12 years)


Total daily dose (µg)
Inhaled corticosteroid
Low Medium High

Fluticasone/salmeterol# (DPI) 100/50 250/50 500/50


Budesonide/formoterol* (HFA-pMDI) 80/4.5 160/4.5 320/9
Beclomethasone dipropionate# (CFC) 200 - 500 500 -1000 >1000
Beclomethasone dipropionate (HFA) 100 - 200 200 – 400 >400
Budesonide (DPI) 200 - 400 400 – 800 >800
Fluticasone propionate (DPI or HFA) 100 - 250 250 – 500 >500
Mometasone furoate (HFA-pMDI) 200-400 400
DPI → Dry Powder inhaler, MDI → Metered dose inhaler, CFC → Chloro
flouro carbon, HFA → Hydro flouro alkane

#
Beclomethasone dipropionate (CFC) is the Most commonly available ICS in
Ethiopia and Cost effective. It is available as MDI form like salbutamol. Usually
2 puff BID is enough.

Beclomethasone Dose
o Mild asthma: 50 to 100 µg, BID; maximum dose: 100 µg, BID
o Moderate asthma: 100 to 250 µg, BID; maximum dose: 250 µg, BID
o Severe asthma: 300 to 400 µg, BID; maximum dose: 400 µg, BID

*Budesonide/formoterol is available in Ethiopia as a turbuhaler and commonly


prescribed by its Brand Name as “’Symbicort”’ but it is too costly. It can be
given 1 to 2 inhalations daily to QID based on patient’s condition. Usually 1 or
2 inhalations BID is enough.

Symbicort 100 Turbuhaler, Symbicort 200 Turbuhaler: DPI:


o Initial: 1 to 2 inhalations, BID, until symptom control, then titrate to lowest
effective dosage to maintain control
o Maintenance: 1 to 2 inhalations, daily or BID (maximum: 8 inhalations/day as
temporary treatment in periods of worsening asthma)

Symbicort Maintenance and Reliever Therapy: DPI:

o Maintenance: Symbicort 100 Turbuhaler or Symbicort 200 Turbuhaler: 1 to 2


inhalations, BID, or 2 inhalations once daily
o Reliever therapy: Symbicort 100 Turbuhaler or Symbicort 200 Turbuhaler: 1
additional inhalation as needed, may repeat if no relief for up to 6 inhalations
total (maximum: 8 inhalations/day)

*When Budesonide/formoterol is prescribed as maintenance and reliever therapy,


the maximum recommended dose of formoterol in a single day is 72 µg.
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Some patients in Ethiopia use Almetamine 1tab, PO, PRN to daily dose.
Almetamine is a trade name which contains, Betamethasone, 0.25mg and
Dexchlorpheniramine 2mg. But no enough literature about Almetamine.

Aims of Asthma Therapy


➢ Minimal (ideally no) chronic symptoms, including nocturnal
➢ Minimal (infrequent) exacerbations
➢ No emergency visits
➢ Minimal (ideally no) use of a required β2-agonist
➢ No limitations on activities, including exercise
➢ Peak expiratory flow circadian variation <20%
➢ (Near) normal PEF (Peak expiratory flow)
➢ Minimal (or no) adverse effects from drugs

The basic principles of care


✓ Assess the severity of the attack
✓ Assess potential triggers
✓ Use inhaled short-acting beta agonists early and frequently, and consider
concomitant use of ipratropium for severe exacerbations
✓ Start systemic glucocorticoids if there is not an immediate and marked
response to the inhaled short-acting beta agonists
✓ Make frequent (every one to two hours) objective assessments of the
response to therapy until definite, sustained improvement is documented
▪ Good response → no wheezing or dyspnea (tachypnea in children),
PEF > 80 % predicted or personal best
▪ Incomplete response → persistent wheezing and dyspnea, PEF 50 -
79 % predicted or personal best
▪ Poor response → Marked wheezing or dyspnea, PEF < 50 %
predicted or personal best
☛ What shall we do for each response? → see the algorism below
✓ Admit patients who do not respond well after four to six hours to a setting
of high surveillance and care
▪ In our set up; Mild and moderate Acute asthma exacerbations can
be managed and discharged from emergency department (usually
from triage) after stabilizing the patient (discharge should be after
asthma education and appointment is given).
▪ Admit patients with severe attack persisting after initial treatment in
the emergency room or wards, and those with life threatening
attacks directly to ICU.
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✓ Educate patients about the principles of self-management for early


recognition and treatment of a recurrent attack and develop an "asthma
action plan" for recurrent symptoms → look at below
✓ Positioning → sitting upright and/or leaning.
✓ Consider IV hydration if necessary

Caution!!! Do not give any form of sedatives during acute attacks

Management of Mild or moderate Acute Asthma exacerbations


✓ Oxygen → if there is desaturation or significant dyspnea
▪ Start with 2L/min of Intranasal O2, increase flow rate accordingly until
oxygen saturation of > 90% is achieved
✓ Salbutamol (SABA) PLUS
☛ 4 to 6 puffs every 20 minutes in the first 1-4 hours. Then the same
dose every 1-4 hours depending on the patient need. OR
o E.g. Salbutamol puff, 6 puffs every 20 minutes in the first 1
hour, then 6 puffs every 1 hour for 4 hours then, 6 puffs
every 4hr for 24 hours.
☛ 2 - 5mg every 20 minutes for 3 doses, then 2.5 - 10mg every 1 -
4 hours as needed, or 10 - 15mg/hour continuously
✓ Hydrocortisone, 200mg, IV stat. Further IV doses are needed only if oral
dosing is not possible (100mg, IV, TID or QID).
Or
✓ Dexamethasone: 0.6mg/Kg/day (18mg maxi dose)
Followed by
✓ Prednisolone, 30 - 45 mg, PO, daily for 5 - 10 days (N.B it is available in
5 mg tab form)
▪ Should be started immediately.
▪ Discontinuation does not need tapering.

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Practical points for approaching a patient with mild or moderate


acute asthma exacerbation
✓ Asthma patients (with mild or moderate exacerbations) usually stabilized at
medical emergency. Admission required for severe attack or those not
responding /persisting/ after initial treatment)

✓ Put the patient in sitting position


✓ Secure IV line
✓ Put on Intranasal oxygen for desaturating patients
▪ Start with 2L/min of Intranasal O2, increase flow rate accordingly until
oxygen saturation of > 90% is achieved, if more than 10 L/min required
(in that case consider severe attack), use facemask
✓ Give Salbutamol puff, 4 to 6 puffs every 20 minutes in the first 1- 4 hours.
Then the same dose every 1 - 4 hours depending on the patient need
▪ E.g. Salbutamol puff, 6 puffs every 20 minutes in the first 1 hour, then 6
puffs every 1 hour for 4 hours then, 6 puffs every 4hr for 24 hours.
▪ Assess the response to therapy (dyspnea, Pulse oximetry, wheeze) every
one to two hours
✓ Hydrocortisone, 200mg IV stat.
▪ Some times 200mg, IV, Loading then 100mg, IV, QID

When patient is stable, discharge with;

✓ Salbutamol/SABA/, every 4 to 6 hours as needed


✓ Prednisolone, 30 - 45 mg, PO, daily for 5 - 10 days.
✓ Appoint after a week (if symptoms improve → discontinue prednisolone, if no
improvement, manage as chronic asthma → look at below)
✓ Asthma education including how to use MDI → look at below
▪ Even though MDI are used correctly, only 10 - 20 % of Active drug
(salbutamol, ICS) is inhaled to lungs. The rest 80 - 90 % is swallowed
in to GIT. If there is incorrect use of MDI, obviously the patient will get
less than 10 % of the drug to the targeted lung.

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Management of acute severe asthma


One of the main aims of controller therapy is to prevent exacerbations; in
this respect, ICS and combination inhalers are very effective.
Systemic corticosteroids
o Give IV hydrocortisone 200mg, IV methylprednisolone 40 to 60 mg
or oral prednisolone 40 to 60mg
A high concentration of oxygen should be given by face mask to achieve
oxygen saturation of > 90% (93 - 95 %).
High doses of SABA → The mainstay of treatment, given either by
nebulizer or via an MDI with a spacer.

Interventions to be given based on indication include; → see the algorithm below

Adrenaline 0.5 cc IM/SC, repeats after 20 min if no improvement, for


anaphylactic asthma and severe cases
Magnesium sulfate → given intravenously or by nebulizer is effective when
added to inhaled β2-agonists, and is relatively well tolerated but is not
routinely recommended.
o Magnesium sulfate, 2g, IV, in 100 ml 5% D/W, infused over 20
minutes, if not previously done, Nebulized magnesium can also be used.
A slow infusion of aminophylline → may be effective in patients who are
refractory to inhaled therapies, but it is important to monitor blood levels,
especially if patients have already been treated with oral theophylline.
▪ Aminophylline (Theophylline), 250mg (5–6 mg/kg) IV bolus slowly over
20 minutes. Maintenance: 0.5mg/kg/hour (maximum: 900mg/day).
o Decrease the dose to 0.38 mg/kg/hour (maximum: 400mg/day)
for
▪ Patients with cardiac decompensation
▪ Cor pulmonale
▪ Hepatic dysfunction
▪ Multiorgan dysfunction
▪ Old patients (>60 years):

☛ N.B. Aminophylline Should not be first line therapy in the


presence of inhaled SABA. Adding it on top of inhaled SABA
does not have significant benefit.
☛ Caution!!! When giving Aminophylline to adults who have been on
Theophylline tablets, avoid bolus injection as there is a high risk
of cardiac arrhythmias, seizures.
IV β2-agonists → may be given for severely ill patients with impending
respiratory failure,
A nebulized anticholinergic → may be added if there is not a satisfactory
response to β2-agonists alone, as there are additive effects.
▪ Ipratropium bromide (Anti-cholinergic)
o 4 - 8 puffs every 20 minutes as needed up to 3 hours. Or
o 0.25 - 0.5mg every 20 minutes for 3 doses, then as needed.
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▪ N.B. Ipratropium should be additional therapy to SABA.


Can be mixed with SABA during nebulization.
Prophylactic intubation → may be indicated for impending respiratory failure,
when the PCO2 is normal or rises.
Mechanical ventilation → For patients with respiratory failure, it is necessary
to intubate and institute ventilation.
General anesthesia → These patients may benefit from a general
anesthetic, such as halothane, if they have not responded to conventional
bronchodilators.
o Ketamine 0.2mg/kg iv bolus followed by 0.5mg/kg/hr can be considered
Antibiotics → should not be used routinely unless there are signs of
pneumonia.

Caution!!! Sedatives should never be given as they may depress ventilation.

Asthma Education before discharging the patient


➢ Reduce indoor air pollution by cooking outside or using smokeless cooking
stoves
➢ Avoid allergens that the patient is sensitive to:
☛ contact with furry animals (e.g. cats, dogs)
☛ Reduce pollen exposure
☛ Reduce exposure to house dust mite
➢ Avoidance of tobacco smoke exposure
☛ Provide advice and resources at every visit; advise against exposure of
children to ETS (house, car).
➢ Occupational asthma
☛ Ask patients with adult-onset asthma about work history. Remove
sensitizers and irritants like dust and fumes as soon as possible. Refer
for expert advice, if available.
➢ Encourage Physical activity
☛ Encouraged because of its general health benefits. Provide advice
about managing exercise-induced bronchoconstriction.
➢ Avoid medications that may worsen asthma
☛ Always ask about asthma before prescribing NSAIDs or beta-blockers.
➢ Remediation of dampness or mold in homes
☛ Reduces asthma symptoms and medication use in adults.

Goals of asthma education include:

An explanation of the nature of asthma and its inflammatory basis


A description of the different classes of drugs and their purpose in
treatment (i.e. as-needed “relievers” and regular “controllers”)
Advice on prevention strategies (allergen, irritant, and tobacco smoke 1023
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All patients should be taught how to use their inhalers correctly i.e. the
correct choice and use of inhalers and the opportunity to practice under
supervision.
In particular, they need to understand How to recognize worsening
asthma and how and when to implement their action plan
In some patients, particularly those requiring stabilization or patients who
have had a recent exacerbation or deterioration, the use of a PEF meter
and chart.

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PEF: peak expiratory flow; ICU: intensive care unit; SABA: short-acting beta agonist (eg,
albuterol); SpO2: pulse oxygen saturation; COPD: chronic obstructive pulmonary disease;
MDI: metered dose inhaler; GC: glucocorticoid; PaCO 2: carbon dioxide tension.
* Titrate oxygen to SpO2 93 to 95% for patients with severe exacerbations, particularly if
at risk for hypercapnia. Aim for SpO2 >95% in pregnant patients. Titrate to SpO2 88 to
92%, if asthma-COPD overlap.
¶ Magnesium sulfate is 4.06 mmol/g (2 g = 8.1 mmol).
Δ Please refer to the UpToDate topic on treatment of asthma exacerbations in adults.
◊ Adding ipratropium to albuterol nebulizer treatments is preferred for patients with severe
exacerbations; alternatively, SABA/ipratropium can be given via MDI 4 to 8 inhalations
every 20 minutes, as needed for up to 3 hours.
§ The dose and duration of therapy can be modified based on the patient's past history of
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8.3.2. How to use inhalers for asthma management

❖ An inhaler is a medical device used for delivering medication into the body
via the lungs.
❖ It is mainly used in the treatment of asthma and COPD.
❖ The two most common forms are:

1. Metered-dose inhaler (MDI)


2. Dry powder inhalers /DPI/ (Accuhalers and turbuhalers)

❖ Some of the types of inhalers include: Autohalers (Breath Activated aerosol


devices), Nebulizers mists and nasal inhalers
❖ Most patients (up to 80%) cannot use their inhaler correctly. This
contributes to poor symptom control and exacerbations.
❖ To ensure effective inhaler use:
✓ Choose the most appropriate device for the patient before prescribing
✓ check in haler technique at every opportunity
✓ correct using physical demonstrations, paying attention to incorrect
steps and confirm that you have checklists.

Metered-dose inhaler (MDIs)

The medicine is in a small canister, inside a plastic case. When the inhaler
is pressed, a measured dose of medicine comes through the mouthpiece.
MDIs require good technique and coordination by pressing down on the
inhaler and breathing in at the same time.
Because using the inhaler correctly can be difficult, spacer devices are
recommended for use with MDIs. The spacer is attached to the MDI to
make it easier to use the inhaler and get more medicine into the lungs.

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How to use Metered Dose Inhaler

1. Remove the cap and check the mouthpiece is clean and free of objects.
2. Shake the inhaler 4 or 5 times.
3. Holding the inhaler upright with your thumb on the base, breathe out as far
as comfortable
4. Place the mouthpiece in your mouth; closing your lips around it to form a
good seal - do not bite.
5. Start to breathe in slowly; press down firmly on the top of the canister to
release a dose; while continuing to breathe in slowly and deeply.

Figure: Metered Dose Inhaler


6. Removing the inhaler from your mouth; hold your breath for about 10
seconds, or as long as is comfortable.
7. Breathe out gently away from your inhaler mouthpiece
8. For a second dose, wait approximately 30 seconds before repeating steps
2-7
9. Replace the cap

How to use MDI - Click on the link below and watch the video
https://youtu.be/tp479j15x6Q

N.B

Even though MDI are used correctly, only 10 - 20 % of Active drug (salbutamol,
ICS) is inhaled to lungs. The rest 80 - 90 % is swallowed in to GIT. If there is
incorrect use of MDI, obviously the patient will get less than 10 % of the drug to
the targeted lung. → look at the image

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Dry Powder Inhaler (DPI)

❖ Dry powder inhalers are handheld devices that deliver medication to the
lungs and airways as you inhale through it.
❖ Examples of dry powder inhalers include: Turbuhaler; Accuhaler; Handihaler;
Ellipta inhaler and Breezhaler.
❖ The common forms available in Ethiopia are Turbuhaler (eg.Symbicort) and
Accuhaler (eg. Seritide)

Figure: Different forms of devices delivering DPIs

How to use Accuhaler® (Dry powder inhaler-DPI)

1) Check dose counter.


2) Open cover. (Use thumb grip)
3) Hold the casing of the Accuhaler® in one hand while sliding the thumb grip
away until a click is heard
4) Holding your Accuhaler® with the mouthpiece towards you slide the lever
away from you until a click is heard. This makes the dose available for
inhalation and moves the dose counter on.
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Figure: Dry Powder Inhaler (Accuhaler)

5) Holding the inhaler horizontally, breathe out as far as comfortable

6) Place the mouthpiece in your mouth; closing your lips around it to form a
good seal - do not bite
7) Breathe in as strongly and deeply as possible
8) Removing the inhaler from your mouth; hold your breath for about 10
seconds, or as long as is comfortable
9) Breathe out gently away from your inhaler mouthpiece
10) To close the Accuhaler®, slide the thumb grip back towards you as far as
it will go until it clicks.

How to use Accuhaler® - Click on the link below and watch the video
https://youtu.be/6WOEhIIIHGI

Turbuhaler (DPI)

➢ Since the turbuhaler is a breath-activated device, to use the turbuhaler


properly, you must be able to breathe in deeply. Adults and children 7
years of age and older should be able to use the turbuhaler.

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Figure: Dry Powder Inhaler (Turbuhaler)

How to use Turbuhaler (DPIs)

1) Open: unscrew and remove the cap. Hold the turbuhaler upright.
2) Load the dose: twist the base anticlockwise and then back in the other
direction until you hear a click. Your turbuhaler is now loaded with one
dose of medicine
3) Breathe out: breathe out, away from the turbuhaler. Do not blow directly into
the turbuhaler.
4) Inhale your dose: place the mouth piece in your mouth and form a seal
with your lips. Breathe in deeply. Remove the turbuhaler and hold your
breath for up to 10 seconds.
5) Close: replace the cap and twist until it is on properly.
6) Cleaning and storing your turbuhaler: wipe the mouthpiece with a clean dry
tissue. Do not wash the mouthpiece or allow it to get wet when cleaning.
Keep the cap on when not in use. The device may clog if exhaled or
dribbled into or if stored in an area of high humidity with the cap off or
unsealed.

How to use Terbuhaler® - Click on the link below and watch the video
https://youtu.be/DqoEdW6dHaI

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Common problems when using a turbuhaler

To get the most benefit, it is important to use the correct technique. Here are a
few common problems:

✓ Not holding your turbuhaler upright (vertical) while loading the dose.
✓ Covering the air inlets with your lips.
✓ Breathing in through your nose instead of your mouth.
✓ Shaking the inhaler to see how much is left.
✓ Storing your turbuhaler in a damp place with the cap off.

How to use Spacers

If patient unable to use an inhaler correctly, add a spacer to increase drug


delivery to the lungs, especially if using inhaled corticosteroids. This may
also reduce the risk of oral candida.
Clean the spacer before first use and every second week: remove the
canister and wash spacer with soapy water. Allow it to drip dry. Avoid
rinsing with water after each use.
Spacers are not commonly available in Ethiopia so a plastic water bottle.
See figure below.
To modify a 500ml plastic bottle for use as an effective spacer

Figure: How to make a spacer from a plastic bottle

How to use a bottle spacer


Use a modified 500ml plastic bottle in a similar way to a conventional
spacer

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Figure: How to use an inhaler with a spacer

Images; MDI with spacers

How to use an Inhaler with a spacer - Click on the link below and
watch the video
https://youtu.be/ma_cmlU9DxU

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8.3.3. Chronic asthma

It is a chronic inflammatory disorder of the lower airways in susceptible


individuals resulting in recurrent episodes of wheezing, dyspnea on exertion,
chest tightness and coughing particularly at night and in early morning on
daily basis with undercurrent acute exacerbation and recurrent chest
infection
This inflammation is usually associated with widespread but variable airflow
obstruction that is often reversible spontaneously or with treatment but in
some patients with chronic asthma there may be an element of irreversible
airflow obstruction
Chronic asthmatic response:
o Chronic inflammation of mucosa of lower airway → Destruction of
airway epithelium by toxic granule contents → epithelial shedding into
bronchial lumen → exposure of sensory nerve endings and
imbalance in cholinergic and peptinergic neuronal control → Airway
remodeling with subendothelial fibrosis, goblet cell hyperplasia,
smooth muscle hypertrophy, vascular changes → fixed airway
obstruction.
It is important to establish the diagnosis objectively using spirometry or
PEF/peak expiratory flow/ measurements at home.
But in our setup, diagnosis using spirometry or PEF may be impossible, so
it is better to differentiate Various severities of asthma using clinical
parameters (see the table below). These include
o Frequency of symptoms in general
o Frequency of night time symptoms which awaken the patient from
sleep
o Frequency of using SABA (salbutamol) for symptom control
o Interference with normal activity
o Exacerbations requiring OCS
o If available, pulmonary function test (FV1, FV1/FVC ratio, PEF)

Table; Classification of severity of asthma

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Table; Assessing severity and initiating treatment for patients who are not currently taking long-term control
medications. The stepwise approach is meant to assist, not replace, the clinical decision-making required to meet
individual patient needs. Level of severity is determined by assessment of both impairment and risk. Assess
impairment domain by patient's/caregiver's recall of previous two to four weeks and spirometry. Assign severity to
the most severe category in which any feature occurs. At present, data are inadequate to correlate frequencies of
exacerbations with different levels of asthma severity. In general, more frequent and intense exacerbations (eg,
requiring urgent, unscheduled care, hospitalization, or ICU admission) indicate greater underlying disease severity.
For treatment purposes, patients who had ≥2 exacerbations requiring oral systemic glucocorticoids in the past
year may be considered the same as patients who have persistent asthma, even in the absence of impairment
levels consistent with persistent asthma.

FEV1: forced expiratory volume in one second; FVC: forced vital capacity;

Even though this table is for ≥ 12 years of age, it is almost similar for < 12 years
age (if you want to cross check the details, look at the table from UpToDate 2018
‘’asthma in children younger than 12 years” as shown in the picture)

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Management of chronic asthma

➢ Triggers that worsen asthma control, such as allergens or occupational


agents, should be avoided, whereas triggers, such as exercise and fog,
which result in transient symptoms, provide an indication that more
controller therapy is needed.
➢ It is important to assess asthma control, assessed by symptoms, night
awakening, need for reliever inhalers, limitation of activity and lung function
(see the Table 281 - 4 below)

Patients with poor asthma control should be assessed for the following.

☛ Reasons for poor adherence and misunderstanding the difference between


relievers and controllers
☛ Poor inhaler technique
☛ Exposure to trigger factors at home and work
☛ Presence of gastro-esophageal acid reflux disease (GERD)
☛ Rhinitis and sinusitis
☛ Use of medications that may aggravate asthma such as aspirin, NSAID’s
and 𝛽 blockers
☛ Other medical conditions mimicking asthma symptoms (e.g. cardiac disease).

Stepwise therapy of chronic Asthma


➢ Pharmacologic therapy Depends on the severity of asthma
➢ Assess the severity of asthma and scale up or down treatment based on
the severity.
☛ For example, if symptoms are controlled after 3 months decrease the
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➢ For patients with mild, intermittent asthma, a SABA is all that is required.
However, use of a reliever medication more than twice a week indicates
the need for regular controller therapy.
➢ The treatment of choice for all patients is an ICS given twice daily. It is
usual to start with an intermediate dose (e.g. 200μg BID of beclomethasone
dipropionate) or equivalent and to decrease the dose if symptoms are
controlled after 3 months.
➢ If symptoms are not controlled, a LABA should be added, which is most
conveniently given by switching to a combination inhaler.
➢ The dose of controller should be adjusted accordingly, as judged by the
need for a rescue inhaler.
➢ Low doses of theophylline or an antileukotriene may also be considered as
an add-on therapy, but these are less effective than LABA.
➢ In patients with severe asthma, low-dose oral theophylline is also helpful,
and when there is irreversible airway narrowing, the long-acting
anticholinergic may be tried.
➢ If asthma is not controlled despite the maximal recommended dose of
inhaled therapy, it is important to check adherence and inhaler technique.
In these patients, maintenance treatment with an OCS may be needed and
the lowest dose that maintains control should be used.
➢ Once asthma is controlled, it is important to slowly decrease therapy in
order to find the optimal dose to control symptoms.

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Dose and frequency of drugs used in stepwise management of


asthma

Mild Intermittent asthma

First line

❖ Salbutamol/SABA/, inhaler 200µg/puff, 2 puffs to be taken as needed but


not more than 3-4 times a day, or tablet, 2- 4mg 3-4 times a day
o No daily medication needed. However, use of a reliever medication
more than three times a week indicates the need for regular
controller therapy.

Alternative

❖ Theophydrine (Ephedrine + Theophylline), 11mg + 120mg P.O., BID OR


TID

Mild Persistent asthma


❖ Salbutamol/SABA/, inhaler, 200 µg/puff 2 puffs to be taken, as needed but
not more than 3-4 times/day, or tablet, 2 - 4mg 3-4 times a day PLUS
❖ Beclomethasone/ICS/, oral inhalation, 50 - 100µg, BID.
☛ If symptoms are controlled after three months, decrease the dose
(down grade to intermittent dose) to 100µg, BID

Moderate Persistent asthma

❖ Salbutamol /SABA/, inhalation 200µg//puff, 1 - 2 puffs as needed PRN not


more than 3-4 times a day. PLUS
❖ Beclomethasone/ICS/, oral inhalation 100 - 250 µg, BID.
☛ Decrease the dose to 100 µg, BID if symptoms are controlled after
three months. (Preferred if symptoms are mor severe or if response
is not optimal to Beclomethasone)

PLUS
❖ Fluticasone/Salmeterol (LABA), 250/50 µg oral inhalation, BID

PLUS (if required)


❖ Ephedrine + Theophylline, 11mg + 120mg P.O., BID OR TID

Severe persistent asthma


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❖ Salbutamol/SABA/, inhalation 200/puff 1-2µg/puffs as needed PRN not more


than 3-4 times a day. PLUS
❖ Beclomethasone/ICS/, oral inhalation 300 - 400µg, BID.
☛ Decrease the dose to 100µg, BID if symptoms are controlled after
three months. (Preferred if symptoms are mor severe or if response
is not optimal to Beclomethasone)

PLUS
❖ Fluticasone/Salmeterol (LABA), 250/50µg oral inhalation, BID

PLUS (If required)


❖ Ephedrine + Theophylline, 11mg + 120mg P.O., BID OR TID

PLUS (if required)


❖ Prednisolone (OCS), 5 - 10mg P.O. daily.
☛ Doses of 20-40mg daily for seven days may be needed for short-
term exacerbations in patients not responding to the above
treatment.

REVIEWING RESPONSE AND ADJUSTING TREATMENT


How often should asthma be reviewed?
☛ 1-3 months after treatment started, then every 3-12 months.
☛ During pregnancy, every 4-6 weeks.
☛ After an exacerbation, within 1 week.

Stepping up asthma treatment;


☛ Consider stepping up if … uncontrolled symptoms, exacerbations or risks
☛ First check for common causes (symptoms not due to asthma, incorrect
inhaler technique, poor adherence, persistent environmental exposures
and drugs, comorbidities that may contribute to respiratory symptoms).

☛ Sustained step-up, for at least 2-3 months if asthma poorly controlled;


☛ Short-term step-up, for 1-2 weeks, e.g. with viral infection or allergen;
❖ May be initiated by patient with written asthma action plan.

☛ Day-to-day adjustment;
❖ For patients prescribed low-dose ICS/formoterol maintenance and
reliever regimen
Stepping down asthma treatment;
o Consider stepping down if … symptoms well controlled for 3 months +
low risk for exacerbations.
o Stopping ICS is not advised in adults with asthma because of risk of
exacerbations
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o Find each patient’s minimum effective dose that controls both


symptoms and exacerbations.

INDICATIONS FOR CONSIDERING REFERRAL TO SPECIALITY CENTER

➢ Difficulty confirming the diagnosis of asthma


➢ Suspected occupational asthma
➢ Persistent uncontrolled asthma or frequent exacerbations
➢ Risk factors for asthma-related death
➢ Significant side-effects (or risk of side-effects)
➢ Symptoms suggesting complications or sub-types of asthma
➢ Asthma with confirmed food allergy.

Special considerations

Refractory Asthma
Although most patients with asthma are easily controlled with
appropriate medication, a small proportion of patients (~5%) are
difficult to control despite maximal inhaled therapy.
There are two major patterns of difficult asthma:
☛ Some patients have persistent symptoms and poor lung function,
despite appropriate therapy,
☛ Whereas others may have normal or near normal lung function but
intermittent, severe (sometimes life-threatening) exacerbations.
The most common reason for poor control of asthma is poor
adherence with medication, particularly ICS. Compliance with ICS may
be low because patients do not feel any immediate clinical benefit or
may be concerned about side effects.
There are several factors that may make asthma more difficult to
control, including;
☛ Exposure to high, ambient levels of allergens or unidentified
occupational agents.
☛ Severe rhinosinusitis may make asthma more difficult to control
☛ Upper airway disease should be vigorously treated.
☛ Drugs such as 𝛽 blockers, aspirin, and other cyclooxygenase (COX)
inhibitors like NSAID’s may worsen asthma.
☛ Some women develop severe premenstrual worsening of asthma, which
is unresponsive to corticosteroids and requires treatment with
progesterone or gonadotropin-releasing factors.
☛ Few systemic diseases make asthma more difficult to control, but
hyper- and hypothyroidism may increase asthma symptoms and should
be investigated if suspected.
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Bronchial biopsy studies in refractory asthma may show the typical


eosinophilic pattern of inflammation, whereas others have a
predominantly neutrophilic pattern.
Structural changes in the airway, including fibrosis, angiogenesis, and
airway smooth muscle thickening, are more commonly seen in these
patients

Treatment of Refractory Asthma

Refractory asthma is difficult to control, by definition.


Check adherence and the correct use of inhalers technique
☛ Compliance may be improved by giving the ICS as a combination with
a LABA that gives symptom relief.
Identify and eliminate any underlying triggers.
Low doses of theophylline may be helpful in some patients, and
theophylline withdrawal has been found to worsen in many patients.
Many of these patients will require maintenance treatment with OCS,
and the minimal dose that achieves satisfactory control should be
determined by careful dose titration.
A few patients may benefit from infusions of β2-agonists.
In some patients with allergic asthma, omalizumab is effective,
particularly
when there are frequent exacerbations.

Corticosteroid-Resistant Asthma
It is defined by a failure to respond to a high dose of oral
prednisone/prednisolone (40 mg once daily over 2 weeks), ideally with
a 2-week run-in with matched placebo.
More common is reduced responsiveness to corticosteroids where
control of asthma requires OCS (corticosteroid-dependent asthma).
A few patients with asthma show a poor response to corticosteroid
therapy
Complete resistance to corticosteroids is extremely uncommon
There are likely to be heterogeneous mechanisms for corticosteroid
resistance;

Brittle Asthma
Some patients show chaotic variations in lung function despite taking
appropriate therapy.
There are two types of brittle asthma
☛ Type I brittle asthma → patients with this type, show a persistent
pattern of variability and may require OCS or, at times, continuous
infusion of β2-agonists
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☛ Type II brittle asthma →patients with this type, have generally normal
or near-normal lung function but precipitous, unpredictable falls in lung
function that may result in death.
▪ Difficult to manage as they do not respond well to
corticosteroids, and the worsening of asthma does not reverse
well with inhaled bronchodilators.
In some of these patients, there may be allergy to specific foods.
The most effective therapy is subcutaneous epinephrine, which
suggests that the worsening is likely to be a localized airway
anaphylactic reaction with edema.
These patients should be taught to self-administer epinephrine and
should carry a medical warning accordingly.

Asthma in Pregnancy
Approximately 1/3rd of asthmatic patients who are pregnant improve
during the course of a pregnancy, 1/3rd deteriorate, and 1/3rd are
unchanged.
It is important to maintain good control of asthma as poor control
may have adverse effects on fetal development (chronic maternal
hypoxia is risk factor for both maternal and neonatal complications,
e.g. Perinatal asphyxia).
Adherence may be a problem as there is often concern about the
effects of antiasthma medications on fetal development.
The drugs have been shown to be safe and without teratogenic
potential.
☛ These drugs include SABA, ICS, and theophylline;
There is less safety information about newer classes of drugs such
as LABA, antileukotrienes, and anti-IgE.
If an OCS is needed, it is better to use prednisone rather than
prednisolone as it cannot be converted to the active prednisolone by
the fetal liver, thus protecting the fetus from systemic effects of the
corticosteroid. There is no contraindication to breast-feeding when
patients are using these drugs.
☛ This note is from Harrison 20th edition. According to UpToDate 2018,
Hydrocortisone is Category C, Prednisolone and prednisone are
Category C/D
☛ what do we do for each Category of drugs in pregnancy? Click here
→ Chapter 23; Basics about rational use of antibiotics

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Asthma in the Elderly


Asthma may start at any age, including in elderly patients.
The principles of management are the same as in other asthmatics,
but side effects of therapy may be a problem, including muscle
tremor with β2-agonists and more systemic side effects with ICS.
Comorbidities are more frequent in this age group, and interactions
with drugs such as β2-blockers, COX inhibitors, and agents that may
affect theophylline metabolism need to be considered. COPD is more
likely in elderly patients and may coexist with asthma.
A trial of OCS may be very useful in documenting the steroid
responsiveness of asthma.

ACOS (Asthma COPD Overlap syndrome)


Refer from COPD under long case of Nitsbin (click here → COPD
(Chronic obstructive pulmonary disease) )

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Chapter 9; GI related disorders and


infections

9.1. Infectious Diarrheal Disease (የተቅማጥ በሽታ/የተቅማጥ


ልክፍት/)

9.1.1 Bloody diarrhoea /ደም የቀላቀለ ሰገራ/

9.1.1.1 Bacillary dysentery /በሲላዊ ተቅማጥ፣ በባክቴሪያ


ልክፍት የሚመጣ ተቅማጥ/
Bacillary dysentery is diarrheal disease caused commonly by bacteria,
which invade and destroy the intestinal epithelium.

Etiology
✓ The 1st three from the following are the dominant bacterial agents
causing bloody diarrhea in Ethiopia.
Salmonella
Shigella
Campylobacter
E. coli.
Entamoeba histolytica and
S. mansoni
☛ Transmission occurs via contaminated water or food.

Clinical features
− watery, mucoid or bloody diarrhea with tenesmus.
− severe abdominal cramps
− fever

Investigations
− S/E → abundance of leukocytes (pus cells)
− Stool culture, if available, can be used to guide treatment selection

Treatment

Supportive treatment
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Correct dehydration with ORS (mild to moderate dehydration) or IV


fluids (severe dehydration) is a cornerstone quality of care indicator
for all diarrheal illnesses.
Diet → continuous provision of nutritious food (small frequent feeding
as tolerated)
Relieve pain and fever if necessary
The use of anti-motility agents like loperamide is not recommended
for dysentery due to the potential for toxic mega colon.

Pharmacologic
Look at table below

recommendation:

☛ A stool examination (including culture studies if available) should


be carried before the administration of empiric antibiotics.
☛ Fluoroquinolone like ciprofloxacin are empiric first choice agents for
3 to 5 days. If susceptibility data available other drugs (e.g.
Cotrimoxazole, macrolides, tetracyclines) can also be used,
otherwise better avoided.
☛ Sever cases like septicemia should be treated with IV ceftriaxone
for at least 7 days.

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9.1.1.2 Amoeba (አሜባ)

Amoebiasis results from infection with the non-invasive Entamoeba


dispar or the invasive Entamoeba histolytica
The 3rd most common cause of death from parasitic disease.
It is most commonly contracted through ingestion of live cysts found
with fecally contaminated water, food, or hands.
Foodborne infection is caused by fecally contaminated soil or water
used for growing vegetables.
It is endemic in most developing countries including Ethiopia.

Cysts and trophozoites are passed in feces (1). Cysts are typically found in formed stool, whereas trophozoites
are typically found in diarrheal stool. Infection by Entamoeba histolytica occurs by ingestion of mature cysts (2) in
fecally contaminated food, water, or hands. Excystation (3) occurs in the small intestine and trophozoites (4) are
released, which migrate to the large intestine. The trophozoites multiply by binary fission and produce cysts (5),
and both stages are passed in the feces (1). Because of the protection conferred by their walls, the cysts can
survive days to weeks in the external environment and are responsible for transmission. Trophozoites passed in
the stool are rapidly destroyed once outside the body, and if ingested would not survive exposure to the gastric
environment. In many cases, the trophozoites remain confined to the intestinal lumen (A: noninvasive infection) of
individuals who are asymptomatic carriers, passing cysts in their stool. In some patients the trophozoites invade
the intestinal mucosa (B: intestinal disease), or, through the bloodstream, extraintestinal sites such as the liver,
brain, and lungs (C: extraintestinal disease), with resultant pathologic manifestations. It has been established that
the invasive and noninvasive forms represent two separate species, respectively E. histolytica and E. dispar.
These two species are morphologically indistinguishable unless E. histolytica is observed with ingested red blood
cells (erythrophagocystosis). Transmission can also occur through exposure to fecal matter during sexual contact
(in which case not only cysts, but also trophozoites could prove infective).

Clinical features

❖ Gradual development of diffuse lower abdominal or back pain


❖ mild diarrhea
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❖ Malaise, weight loss


❖ If caecum is involved, signs and symptoms will mimic those of
appendicitis (right lower quadrant pain)
❖ Full dysentery develops in some patients with passage of 10–12
stools per day
❖ Stools are mostly blood and mucoid

Complications o r unusual presentations:

amoebic liver abscess


amoebic colitis can be confused with IBD,
amoeboma (tender abdominal mass)

Investigations

Stool examination:

✓ Fresh stools specimens must be examined for trophozoites typical of


E. hemolytica. Cysts of both entamoeba species
✓ Entamoeba dispar or the invasive Entamoeba histolytica are very
similar therefore trophozoites that have ingested red blood cells are
diagnostic of E. hemolytica

Treatment
Non pharmacologic
❖ Hydration is important in patients who have severe dysentery

Pharmacologic
Look at table below
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9.1.2. Watery diarrhoea /ውሃ የመሰለ ተቅማጥ/

Watery diarrhea is usually the primary manifestation of an inflammatory


or non-inflammatory response to intestinal tract infection.
Viral diseases (Rotavirus, Norovirus, adenovirus…) are the commonest
causes of watery diarrhea
V.cholera and E.coli are common bacterial etiologies.
Salmonella and listeria may need to be considered in some high-risk
patients.
Bacterial causes usually have high fever or significant abdominal pain,
and duration >3 days
viral causes more likely have non-toxic feature (non bloody, watery stool;
mild disease; afebrile)
For viral causes, no need for investigation and treatment, except
supportive measures

Supportive measures for watery diarrhea

❖ Fluid and electrolyte replacement is the cornerstone for all diarrhea


patients
❖ Feeding, especially in children
❖ Antimotility drugs (eg, loperamide 4mg initially, then 2mg after every
loss stool up to 16 mg/day) will decrease the duration of the illness
in immunocompetent adults.
☛ Loperamide use should be avoided at any age in suspected or
proven cases where toxic megacolon may result in
inflammatory diarrhea or diarrhea with fever.
☛ Should be discontinued after 48 hours if no response
☛ avoided in paediatrics.
❖ Zinc and vitamin A supplementation is associated with a
protective effect in children

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9.1.2.1 Giardia (ጃርዲያ)

Giardia lamblia is a ubiquitous gastrointestinal protozoon that results in


clinical pictures ranging from asymptomatic (60%) colonization to
acute or chronic diarrheal illness.
It can occur both sporadically and in epidemics.
Giardia lamblia infects humans through ingestion of as few as 10
cysts.
The infection is more prevalent in children than adults.

Cysts are resistant forms and are responsible for transmission of giardiasis. Both cysts and trophozoites can be
found in the feces (diagnostic stages) (1). The cysts are hardy and can survive several months in cold water.
Infection occurs by the ingestion of cysts in contaminated water, food, or by the fecal-oral route (hands or
fomites) (2). In the small intestine, excystation releases trophozoites (each cyst produces two trophozoites) (3).
Trophozoites multiply by longitudinal binary fission, remaining in the lumen of the proximal small bowel where
they can be free or attached to the mucosa by a ventral sucking disk (4). Encystation occurs as the parasites
transit toward the colon. The cyst is the stage found most commonly in nondiarrheal feces (5). Because the cysts
are infectious when passed in the stool or shortly afterward, person-to-person transmission is possible. While
animals are infected with Giardia, their importance as a reservoir is unclear.

Clinical
features
☛ The most common presentation is diarrhea which is foul-smelling
with fatty stools (steatorrhea)
☛ Flatulence
☛ weight loss
☛ crampy abdominal pain with bloating
☛ failure to thrive.

Investigation
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✓ Giardia lamblia trophozoite or cyst from fecal or duodenal


samples.

Treatment
Supportive treatment
☛ Correction of fluid and electrolyte loses due to the diarrhea

Medicine Treatment

Look at table below

Prevention:

Avoid drinking water or eating foods likely contaminated (E.g. purify


drinking water, do not swallow water while swimming, and eat cooked
foods at least in risk conditions).
Strict hand washing with water and soap, alcohol-based hand rubs are
effective for trophozoites but poor for cysts
Carful diaper disposal and treatment of symptomatic children will prevent
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spread.
Breastfeeding is protective against giardiasis in nursing infants in
endemic areas
Zinc and vitamin A supplementation is associated with a protective effect
in children

9.1.2.2 Cholera (አተት፣ ኮሌራ)

❖ Cholera is an acute intestinal infection caused by ingestion of food or


water contaminated with the bacterium Vibrio cholera.
❖ A toxin-mediated acute diarrhoeal disease characterized by profuse
diarrhea and dehydration/shock that can cause death in a few hours.
❖ Can occur in endemic (usually children) or epidemic forms (all age
groups)
❖ May be fatal in less than 24 hours
❖ Caused by Vibrio cholerae: – Produces cholera toxin (responsible for
the clinical presentation

Mode of transmission

➢ The fecal-oral route.


➢ Infectious dose of > one million organisms
➢ Drinking-water that has been contaminated at its source
➢ Ice made from contaminated water.
➢ Cooking utensils washed in contaminated water
➢ Food contaminated during or after preparation
➢ Seafood, shellfish, taken from contaminated water and eaten raw or
insufficiently cooked or contaminated during preparation.
➢ Fruit and vegetables grown at or near ground level and fertilized with
night soil (human excreta), irrigated with water containing human
waste.
➢ Corpses of cholera patients are highly infectious through their excreta.
➢ Physical contact during funerals is also a major medium.
➢ Cholera treatment centers can become main sources of infection and
Contamination if hygiene and isolation measures are insufficient.

Risk factors

➢ Overcrowding (internally displaced people, refugee, camps, population


gatherings, etc.)
➢ Inadequate quantity and/or quality of water
➢ Inadequate personal hygiene
➢ Poor washing facilities
➢ Inappropriate or poor sanitation 1050
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➢ Inadequate food safety


➢ Unimmune individuals

Microbiology

➢ The species V. cholerae is classified into more than 200 serogroups


based on the carbohydrate determinants of their lipopolysaccharide
(LPS) O antigens
➢ only two – O1 and O139 – cause outbreak
➢ Persons with type O blood are at greatest risk of severe disease if
infected, while those with type AB are at least risk.

Clinical manifestations

❖ IP: 1 to 3 days
❖ Symptoms usually last 2 to 3days, can continue up to 5 days.
❖ Infected persons can transmit during 1 to 4 weeks
❖ A small number of individuals can remain healthy carriers for several
months.
❖ Approximately 80% of people infected with cholera do not have
symptoms of the cholera disease.
❖ Among symptomatic patients, approximately 20% will develop profuse
watery diarrhea (10-20 liters/day) that leads to severe dehydration
and death if not treated (cholera gravis).
• Severe disease (“cholera gravis”): The diarrhoea is classically
voluminous/ profuse (up to 1L/hr)/, non-offensive, and somewhat
looks gray or “rice-water” diarrhea with flecks of mucous
❖ Sudden onset of explosive diarrhea is the hallmark of the disease.
❖ Mild disease: loose stool or watery diarrhea
❖ Fever is absent.
❖ Dehydration, shock, electrolyte imbalance
❖ Usually: no pain, no tenesmus, no blood in stool, no fever

Mortality from cholera

❖ May reach 50 to 70% in untreated patients


❖ Reduced to <1% with just appropriate rehydration

Diagnosis

❖ Presumptive diagnosis clinically made in patients with severe acute


watery diarrhea

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Laboratory tests

➢ RDT- for screening at primary health care level


➢ Gram stain
➢ Dark field microscopy
➢ Culture-confirmatory test

➢ Isolation of Vibrio cholerae in environmental samples


➢ Confirmation of 5 to 10 stool or vomit samples is sufficient per
outbreak/woreda.
➢ The confirmation of the samples will be done at Regional reference
laboratories as well as at the National laboratory of Ethiopian Health
and Nutrition Research Institute.

Management
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❖ General Principles of Clinical Management of Cholera


• The goal of treatment is to rehydrate patients and replace
electrolytes lost in stool and vomitus.
• 80% - 90% of cholera patients can be rehydrated with oral
rehydration therapy alone.
• Severely dehydrated patients require rapid fluid replacement with
intravenous fluids.
❖ Give ORS during and after intravenous (IV) therapy as soon as the
patient can drink.
❖ Ringer’s Lactate is the preferred intravenous solution because it
contains an electrolyte composition appropriate for treating cholera
patients.
❖ For the severely dehydrated patient, antibiotics can reduce the
volume and duration of diarrhea, and shorten the period of infectivity

No dehydration

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Moderate dehydration

❖ Monitoring the progress of the patient with moderate dehydration


• Monitor the patient frequently to ensure that ORS solution is
taken satisfactorily.
• If the patient vomits, wait 10 minutes, and continue slowly
• If there are no signs of dehydration after the first 4 hours of
treatment, then follow Treatment Plan A
• If there are still signs of moderate dehydration after the first 4
hours, then repeat Treatment Plan B for 4 hours and reassess.

Severe dehydration

❖ Restore normal hydration within 3 to 6 hours.


❖ Hang the infusion bag as high as possible to facilitate rapid flow
• Large caliber catheters (16G, 18G) should be used. If large
catheters cannot be placed, two parallel IV lines can be used, to
ensure rapid administration of Ringer’s Lactate.
❖ Ringer lactate IV is the preferred fluid (Use normal saline, 5%
glucose in normal saline, if only Ringer lactate is not available)
❖ 5% glucose solution is not recommended.
❖ On average, a severely dehydrated adult patient need
• 8-10 liters of Ringer’s Lactate and
• 10 liters of ORS for a full course of treatment.

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❖ Volume:
• 100ml/kg for the first three hours (7 liters for a 70kg adult)
• The first 30ml/Kg (2 liters) should be given fast (30 minutes)
• If after the first 30ml/kg pulse is not strong, then repeat 30
ml/kg IV one more time.
• The remaining 70ml/kg (5 liters) in the remaining 2 1/2 hours.
• Adults with severe cholera require about 200ml/Kg or more (14
liters or more) in the first 24 hours
• Ongoing loss should be assessed and further replacement
should be assessed based on ongoing losses.
• Oral fluid intake (ORS should be started) as soon the patient
condition improves and is able to take orally.
❖ After 6 hours (for infants) or 3 hours (one year or older), the patient
should be completely reassessed and treated accordingly
❖ The patient’s condition must be assessed every 30 minutes during
the first 2 hours, then every hour for the next 6-12 hours.
❖ Monitoring is based on pulse and respiratory rates; and the frequency
of urine, stool, and vomiting.
❖ During treatment, the patient’s respiratory rate and pulse rate should
decrease. Regular urine output (every 3-4 hours) is a good sign that
enough fluid is given.
❖ Observe closely until a strong radial pulse is present and mental
status improves.
❖ If there is no improvement with the first bolus or if at any time the
systolic blood pressure falls ≤ 90 or danger signs reappear,
administer a second bolus

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Indications for antibiotics

➢ cholera patients hospitalized with severe dehydration


➢ Patients with high purging (at least one stool per hour during the first
4 hours of treatment) or treatment failure (the patient is still
dehydrated after completing the initial 4 hours of rehydration therapy),
regardless of the degree of dehydration; and
➢ Patients with coexisting conditions (including pregnancy) or
comorbidities (such as SAM, HIV), regardless of the degree of
dehydration.
➢ Choice of antibiotics

Identifying and Treating Complications

➢ Hypoglycemia
➢ Acute pulmonary edema
☛ Risk among elderly, young children and severely anemic patients.
Use of sodium chloride 0.9%
☛ Administer furosemide by slow IV injection:
▪ Children: 1 mg/kg/injection
▪ Adults: 40 mg/injection
➢ Renal failure (anuria)
☛ Rehydrated and try furosemide 1 mg/ kg IV under close medical
supervision.
➢ Hypokalemia
☛ Suspected if repeated episodes of painful of painful cramps occur
☛ Happen after the first 24 hours of IV of IV rehydration
☛ Add 1 or 2 grams (20-40 mEq/liter) of Potassium hydrochloride
(KCl) in one liter of Ringer lactate
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Discharging the Patient

➢ If hospitalized, first transfer to recovery area and keep under


observation and ORS for 6 hours. From recovery area, discharge
when there are no more signs of dehydration and less than 3 liquid
stools during the past 6 hours.
➢ Discharge with enough ORS bags for 2 days at home which is equal
to the number you use while treating patients using Plan A.
➢ Advise the family
☛ They have to return to health facility when they observe one the
following symptoms.
☛ increased number of watery stools
☛ eating or drinking poorly
☛ marked thirst
☛ repeated vomiting
☛ fever
☛ blood in stool

vaccination

➢ Three OCVs (WHO): Dukoral®, Shanchol™ and Euvichol-Plus®.


➢ All are oral, killed, whole-cell vaccines that provide
➢ Sustained protection of greater than 60% for at least 2 years
➢ Shanchol™ and Euvichol-Plus® -for use in mass vaccination
campaigns.
➢ Shanchol™ and Euvichol-Plus®
➢ a two-dose regimen, with the two doses given a minimum of 14
days apart.
➢ The recommended age for vaccination is 1 year or older.
➢ Two doses provide protection against cholera for at least 3 years.
➢ One dose provides short-term protection (at least 6 months), which
has important implications for outbreak management.

Prevention

➢ The promotion of adequate hygienic conditions in the community is


important to prevent an outbreak and spread of the disease.
➢ If cholera outbreak is suspected, the responsible heath authorities
should be notified. Appropriate epidemic investigation and confirmation
is needed.
➢ Patients should be treated in isolated area with infection prevention
strategies in place, trained manpower and ―cholera-beds‘
➢ Clean water supply: Water treatment with chlorination or boiling when
there is no clear water supply
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➢ Sanitation and hygiene

Chlorine Spraying bag Cholera bed

Cholera Isolation Center

PPE (Personal protective Equipments

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Different concentration of Chlorine solution ( 0.05%, 0.2 %, 0.5%, 2% and 5 %)

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Staff Rooms

Image’s; CTC (Cholera treatment center) prepared by WHO; image’s taken from
CTC of Addis Alem Primary Hospital; Bahirdar, August, 2015 E.C.

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Table -Treatment of common Infectious Diarrheal Disease


Type of Management
diarrhoeal
disease
(aetiology);
Empiric treatment
Bacillary ✓ Ciprofloxacin 500mg PO BID for 3-5 days are empiric
first choice agents.
dysentery Empiric treatment for Severe cases (septicemia):
✓ Ceftriaxone 2g IV/day for 7-10 days
Pregnant women:
✓ Ceftriaxone 2gm IV/day for 3-5 days (mild to moderate)
or 7-10 For severe disease

Treatment of invasive colitis consists of a tissue agent (e.g


metronidazole) followed by a luminal (e.g. parmomycin)
agent to eliminate intraluminal cysts.
Intraluminal infection can be treated with one of the luminal
agents.

First line
✓ Metronidazole, 500-750mg P.O., TID for 7-10 days.
➢ For children: 7.5mg/kg/dose, P.O., TID for 7-10 days.
Amoebiasis Alternative
✓ Tinidazole, 2g P.O. daily for 3 consecutive days.
(Entamoeba
➢ For children: 50-60mg/kg daily for 3 days
dispar,
Entamoeba
histolytica)
Eradication of cysts
First line
✓ Diloxanide Furoate, 500mg, PO, TID, for 10 days.
course may be repeated if necessary. Or
➢ Child over 25kg, 20mg/kg/day, TID, for 10 days;
✓ Paromomycin, 25 - 35mg/kg/day, P.O, TID, for 7 days

Special population considerations → Pregnant women:


✓ For mild to moderate amoebic colitis paromomycin is
preferred.
✓ For severe amoebic colitis treatment with metronidazole
is preferred over paromomycin.

Caution: no well controlled studies demonstrating safety


of metronidazole in pregnancy; thus, use should be
limited for sever cases.

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without any complication.

For symptomatic patients

first line
Giardiasis ✓ tinidazole, 2 g, PO, stat
(Giardia Alternatives
lamblia) ✓ Metronidazole, 250-500mg P.O., TID for 5 - 7 days or
✓ Albendazole, 400 mg, PO, daily for 5 days or
✓ Mebendazole: 200mg PO TID X 5 days, for both adults and
children.

For pregnant women


✓ with mild giardiasis, treatment might be delayed until at
least the 2nd trimester if patient is able to maintain
hydration and nutrition.
✓ If treatment is mandatory during the 1st trimester,
paromomycin 10 mg/kg, PO, TID, for 5 to 10 days
should be used. Paromomycin has a limited systemic
absorption.
✓ During the 2nd and 3rd trimesters, paromomycin,
tinidazole, or metronidazole can be used as an
alternative.
Cholera
See discussion part above
(Vibrio
cholerae)

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9.2. Intestinal Helminthic Infestations (የአንጀት ጥገኛ


ተውሳክ ፣የአንጀት ትላትል) and blood flukes

9.2.1. Ascariasis/Round worm/ (ወስፋት)

Ascariasis is one of the most common helminthic human infections


worldwide.

Adult worms (females 20 to 35 cm; males 15 to 30 cm) (1) live in the lumen of the small intestine. A
female may produce approximately 200,000 eggs per day, which are passed with the feces (2). Unfertilized
eggs may be ingested but are not infective. Fertile eggs embryonate and become infective after 18 days to
several weeks (3), depending on the environmental conditions (optimum: moist, warm, shaded soil). After
infective eggs are swallowed (4), the larvae hatch (5), invade the intestinal mucosa, and are carried via the
portal, then systemic circulation to the lungs (6). The larvae mature further in the lungs (10 to 14 days),
penetrate the alveolar walls, ascend the bronchial tree to the throat, and are swallowed (7). Upon reaching
the small intestine, they develop into adult worms (1). Between two and three months are required from
ingestion of the infective eggs to oviposition by the adult female. Adult worms can live one to two years.

Transmission

❖ Ascariasis is transmitted via ingestion of food or water contaminated


with eggs of A. lumbricoides.
❖ Also, transmission can occur when eggs are taken with dust in the
environment.
❖ Asymptomatically infected children are the main sources of continued
transmission of the diseases.
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Clinical Manifestations

✓ Most people with ascariasis are asymptomatic


✓ Only those with high worm burden exhibit clinical features of the
diseases.

Intestinal Manifestations:

✓ Abdominal discomfort; anorexia; nausea; diarrhea


✓ Growth retardation and malnutrition; steatorrhea and malabsorption
✓ Worms may obstruct lumen and cause intestinal obstruction
✓ Biliary migration of worms may cause abdominal pain, cholecystitis,
cholangitis, obstructive jaundice

Pulmonary Manifestations:

✓ Transient respiratory symptoms during migration through the lungs


✓ Rare in area where transmission is common
✓ Symptoms of Loeffler's Syndrome 1-2 weeks after ingestion of eggs
✓ Low grade fever, dry cough, burning substernal discomfort, sometimes
dyspnea and blood tinged sputum
✓ Urticaria in about 15% of the cases
✓ Infiltrates on chest X ray;
✓ blood eosinophilia
✓ Where there is seasonal transmission of the parasite, seasonal
pneumonitis with eosinophilia may develop in previously infected and
sensitized hosts.

Diagnosis
❖ Stool microscopy shows characteristic eggs.
❖ Sometimes, adult worms may be passed with the feces and confirm
diagnosis; they may also be vomited out, coughed up
❖ During the early transpulmonary migratory phase, when eosinophilic
pneumonitis occurs, larvae can be found in sputum or gastric
aspirates before diagnostic eggs appear in the stool

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Treatment

Look at table below

Follow-up

Follow with repeat S/E after 2-3 months, and those +ve for eggs
should get repeat treatment.

9.2.2. Taeniasis/Tape worm/ (ኮሶ)

There are two main species of Taenia for which humans are the only
definitive hosts. These are
1. Taenia saginata /beef tapeworm/ and
2. Taenia solium /pork tapeworm/.
T. saginata occurs worldwide but is most common in areas where
consumption of undercooked beef is customary, such as Europe and
parts of Asia.
The third species, T. asiatica, is found among pigs in some places.
Concurrent infections with more than one Taenia species have been
described.

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Figure; Taeniasis is the infection of humans with the adult tapeworm of Taenia saginata, T. solium, or T. asiatica.
Humans are the only definitive hosts for these three species. Eggs or gravid proglottids are passed with feces
(1); the eggs can survive for days to months in the environment. Cattle (T. saginata) and pigs (T. solium and T.
asiatica) become infected by ingesting vegetation contaminated with eggs or gravid proglottids (2). In the animal's
intestine, the oncospheres hatch (3), invade the intestinal wall, and migrate to the striated muscles, where they
develop into cysticerci. A cysticercus can survive for several years in the animal. Humans become infected by
ingesting raw or undercooked infected meat (4). In the human intestine, the cysticercus develops over two
months into an adult tapeworm, which can survive for years. The adult tapeworms attach to the small intestine
by their scolex (5) and reside in the small intestine (6). Length of adult worms is usually 5 m or less for T.
saginata (however it may reach up to 25 m) and 2 to 7 m for T. solium. The adults produce proglottids that
mature, become gravid, detach from the tapeworm, and migrate to the anus or are passed in the stool
(approximately six per day). T. saginata adults usually have 1000 to 2000 proglottids, while T. solium adults have
an average of 1000 proglottids. The eggs contained in the gravid proglottids are released after the proglottids are
passed with the feces. T. saginata may produce up to 100,000 and T. solium may produce 50,000 eggs per
proglottid, respectively.

Clinical manifestations

❖ Most human carriers of adult tapeworms are asymptomatic.


❖ Intermittently, patients may pass proglottids in the stool (T. solium) or
spontaneously (T. saginata) or may notice segments in their stool or
sense the movement of proglottids through the anus.
❖ There may be associated symptoms including nausea, anorexia, or
epigastric pain.
❖ Anxiety, headache, dizziness, and urticaria can also occur. A peripheral
eosinophilia (up 15 percent) may be observed.
❖ Occasionally, segments can enter the appendix, common bile duct, or
pancreatic duct and cause obstruction.
❖ Rarely, proglottids can be aspirated or regurgitated.

Diagnosis

1. microscopy

The diagnosis is generally established by identifying eggs or proglottids


in the stool.
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The eggs of Taenia species are morphologically indistinguishable


they are round with a double-walled, radially striated membrane and
measure 30 to 40 micrometers. T. saginata eggs have an acid-fast shell;
T. solium eggs are not acid fast (picture 1).
The proglottids and scolices of T. solium and T. saginata are
morphologically distinguishable and can be used to establish a species
diagnosis (picture 2). The T. saginata proglottids have 12 or more
primary uterine branches; T. solium proglottids have ≤10. These
branches can be seen on direct examination or by injecting India ink
into the segment via its lateral genital opening.
The scolex usually remains in the intestine when proglottids are passed;
it is rare for the entire worm to be eliminated spontaneously. Following
antiparasitic therapy, however, the scolex of a fully evacuated worm may
be identified in the stool. T. saginata has a scolex with four lateral
suckers and no hooks ("unarmed"). T. solium has a scolex with a well-
developed rostellum (crown) that has four suckers and a double row of
hooks ("armed").

2. Immunologic and molecular methods; ELISA, PCR


3. visualizing the worm on capsule endoscopy

Picture 1 (A, B) Taenia spp eggs in unstained wet mounts. Four hooks can clearly be seen in figure A.
(C) Cross-section of a proglottid of Taenia spp, stained with hematoxylin and eosin (H&E). Note the thick outer
tegument and the loose parenchyma filling the body. Calcareous corpuscles (red arrows), characteristic of the
cestodes, can be seen in the parenchyma. Eggs (blue arrows) can also be seen.
(D) Higher magnification of figure C showing a close-up of the eggs. Note the characteristic striations, typical for
the taeniids. Not visible in these images are the hooks commonly seen in cestode eggs. Hooks do not stain with
H&E but are refractile and visible with fine focusing of the microscope.

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Picture 2

Treatment

Look at table below

9.2.3. Hook worm (መንጠቆ)

❖ Two common species: Necator americanus and Ancylostoma


duodenale
❖ More prevalent in resource-poor countries in the tropics.
❖ Hookworm disease develops from a combination of factors
☛ a heavy worm burden;
☛ a prolonged duration of infection; and
☛ an inadequate iron intake
❖ results in iron deficiency anemia and, on occasion, hypoproteinemia

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Eggs are passed in the stool (1), and under favorable conditions (moisture, warmth, shade) larvae hatch in one
to two days. The released rhabditiform larvae grow in the feces and/or the soil (2), and after 5 to 10 days (and
two molts) they become filariform (third-stage) larvae that are infective (3). These infective larvae can
survive three to four weeks in favorable environmental conditions. On contact with the human host, the larvae
penetrate the skin and are carried through the blood vessels to the heart and then to the lungs. They penetrate
into the pulmonary alveoli, ascend the bronchial tree to the pharynx, and are swallowed (4). The larvae reach the
small intestine, where they reside and mature into adults. Adult worms live in the lumen of the small intestine,
where they attach to the intestinal wall with resultant blood loss by the host (5). Most adult worms are eliminated
in one to two years, but the longevity may reach several years. Some Ancylostoma duodenale larvae, following
penetration of the host skin, can become dormant (in the intestine or muscle). In addition, infection by A.
duodenale may probably also occur by the oral and transmammary route. Necator americanus, however, requires
a transpulmonary migration phase.

Clinical Manifestations

Most people who are infected with hookworm are asymptomatic.


Some may develop pruritic maculopapular rash at the site of skin
penetration.
Serpiginous tracks of subcutaneous migration might be seen in
previously sensitized patients.
Mild transient features of pneumonitis can be seen when worms
migrate through the lungs.
In the early intestinal phase of infection, patients may have
abdominal manifestations including abdominal discomfort, nausea,
vomiting, diarrhea, etc.
The major consequence of chronic hookworm infection is iron-
deficiency anemia.

Diagnosis

✓ Diagnosis is established by demonstrating the characteristic oval


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✓ In addition, patients will have iron deficiency anemia and eosinophilia.

Treatment

✓ Look at table below

Prevention

☛ Improved environmental sanitation and the use of latrines and public


health education.
☛ Wearing shoes is also found to prevent infection.

9.2.4. Schistosomiasis (ቢሊሃርዚያ)

Schistosomiasis is a disease caused by infection with parasitic blood


flukes. It is also known as "bilharziasis" after Theodor Bilharz
❖ 5 species of the parasitic trematode genus Schistosoma can cause
infection in humans
➢ the intestinal species → S. mansoni, S. japonicum, S. mekongi,
and S. intercalatum and
➢ the urinary species→ S. haematobium
➢ The three major species are Schistosoma mansoni (Africa and
South America), S. japonicum (East Asia), and S. haematobium
(Africa and Middle East)

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Life cycle: Eggs are eliminated with feces or urine (1). Under optimal conditions, the eggs hatch and release
miracidia (2), which swim and penetrate specific snail intermediate hosts (3). The stages in the snail include two
generations of sporocysts (4) and the production of cercariae (5). Upon release from the snail, the infective
cercariae swim, penetrate the skin of the human host (6), and shed their forked tail, becoming schistosomulae
(7). The schistosomulae migrate through several tissues and stages to their residence in the veins (8,9). Adult
worms in humans reside in the mesenteric venules in various locations, which at times seem to be specific for
each species (10). For instance, S. japonicum is more frequently found in the superior mesenteric veins draining
the small intestine (A), and S. mansoni occurs more often in the superior mesenteric veins draining the large
intestine (B). However, both species can occupy either location, and they are capable of moving between sites,
so it is not possible to state unequivocally that one species only occurs in one location. S. haematobium most
often occurs in the venous plexus of bladder (C), but it can also be found in the rectal venules. The females
(size 7 to 20 mm; males slightly smaller) deposit eggs in the small venules of the portal and perivesical systems.
The eggs are moved progressively toward the lumen of the intestine (S. mansoni and S. japonicum) and of the
bladder and ureters (S. haematobium), and are eliminated with feces or urine, respectively (1).

Clinical Features

❖ manifestations of schistosomiasis occur in three stages which vary by


species, by intensity of infection and other host factors, such as age
and genetics.

1. swimmers' itch

✓ During the phase of cercarial invasion, a form of dermatitis occurs


most often with S. mansoni and S. japonicum infections,
✓ manifesting 2 or 3 days after invasion as an itchy maculopapular
rash on the affected areas of the skin.
✓ severe when humans are exposed to avian schistosomes.
✓ is a self-limiting clinical entity

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2. Acute schistosomiasis or Katayama fever

✓ It is a systemic hypersensitivity reaction to schistosome antigens


and circulating immune complexes.
✓ The complex occurs during worm maturation and at the beginning
of oviposition (i.e., 4–8 weeks after skin invasion)
✓ a serum sickness–like syndrome with fever, generalized LAP, and
hepatosplenomegaly
✓ high degree of peripheral-blood eosinophilia.
✓ Parasite-specific antibodies may be detected before schistosome
eggs are identified in excreta
✓ generally benign

3. Chronic schistosomiasis

☛ intestinal schistosomiasis
☛ may begin a few months after infection and may last for years
☛ colicky abdominal pain, bloody diarrhea, and anemia.
☛ fatigue and an inability to perform daily routine functions
☛ growth retardation.
☛ The severity of intestinal schistosomiasis is often related to the
intensity of the worm burden
☛ colonic polyposis
☛ Hepatosplenic schistosomiasis (HSS)
☛ Hepatomegaly
▪ in 15–20% of infected individuals;
▪ correlates roughly with intensity of infection,
▪ occurs more often in children, and
▪ may be related to specific HLA haplotypes
▪ right-upper-quadrant "dragging" pain
☛ Portal hypertension with splenomegaly and varices
☛ Liver fibrosis
▪ In late-stage disease
▪ liver function deterioration
▪ ascites, hypoalbuminemia, and defects in coagulation
☛ Urinary schistosomiasis
☛ 80% have dysuria, frequency, and hematuria
☛ Urine examination
▪ blood and albumin
▪ high frequency of bacterial urinary tract infection and
✓ urinary sediment cellular metaplasia
☛ hydroureter and hydronephrosis (25–50%)
☛ bladder granulomas undergo fibrosis
▪ squamous cell carcinoma of the bladder
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☛ pulmonary schistosomiasis
▪ embolized eggs lodge in small arterioles, producing acute
necrotizing arteriolitis and granuloma formation.
☛ eggs reach the lungs after the development of portosystemic
collateral circulation or via connections between the vesical and
systemic circulation.
☛ Subsequent fibrous tissue deposition leads to endarteritis
obliterans, pulmonary hypertension, and cor pulmonale.
☛ CNS schistosomiasis (Neuroschistosomiasis)
☛ Adult worms’ embolization to the spinal cord or cerebral
microcirculation, release eggs and cause intense inflammatory
reaction with local tissue destruction and scarring to that result
in cerebral disease or myelopathy. Hence, if
neuroschistosomiasis is confirmed or suspected but not proven,
corticosteroid therapy should be administered
☛ Epilepsy
▪ S. japonicum
▪ Migratory worms deposit eggs in the brain and induce a
granulomatous response
▪ transverse myelitis
▪ S. mansoni and S. haematobium
▪ due to eggs traveling to the venous plexus around the
spinal cord

Diagnosis
Microscopy
✓ Identification of schistosome eggs in a stool or urine sample via
microscopy is the gold standard for the diagnosis of
schistosomiasis.
✓ It can also be used for species identification and to measure the
parasite burden
✓ Eggs of S. mansoni, S. japonicum, S. haematobium, S. mekongi,
and S. intercalatum can be found in stool (although S.
haematobium is principally found in urine).
✓ In endemic settings, the Kato-Katz method is a common thick-
smear technique using 5 mg of stool examined with a low-power
microscope lens

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S. hematobium S. mansoni S. japonicum

Human schistosomiasis eggs: (A) S. mansoni. (B) S. hematobium. (C) S. intercalatum. (D) S. japonicum. (E) S.
mekongi.

cercarial dermatitis → History


Katayama fever
✓ high-level peripheral-blood eosinophilia, and
✓ a positive serologic assay for schistosomal antibodies
o FAST-ELISA and the confirmatory enzyme-linked immune
electrotransfer blot (EITB).
o Both tests are highly sensitive and 96% specific.
o In some instances, examination of stool or urine for ova
may yield positive results.
Established infection
✓ presence of schistosome ova in excreta
✓ Stool examination by the kato thick smear
✓ Urine examination by microscopy of sediment or by filtration of a
known volume through nuclepore filters.

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o Kato thick smear and nuclepore filtration Provide quantitative


data on the intensity of infection to assess the degree of
tissue damage and to monitor the effect of chemotherapy
✓ Rectal biopsies; other biopsy procedures (e.g, Liver biopsy) are
not needed, except in rare circumstances.

Treatment of Schistosomiasis
☛ Look at table below

❖ Cercarial dermatitis
o Antipruritic agents
❖ Acute schistosomiasis or Katayama fever
o Initial management: corticosteroids (prednisolone 20 - 40 mg
daily for 5 days).
o Praziquantel should be initiated only after acute symptoms
have resolved and should be administered concomitantly with
corticosteroids
❖ Neuroschistosomiasis
✓ prednisone 1 to 2 mg/kg for 2 weeks to six months → to prevent
irreversible tissue damage.
 In settings of long-term corticosteroid use strongyloidiasis
should be excluded.
✓ Praziquantel, 40 mg/kg stat, a few days after (to reduce
paradoxical worsening of neurologic symptoms) initiation of
corticosteroid treatment
✓ The two therapies (prednisolone and praziquantel) should be given
concomitantly.
❖ For all individuals with established infection, treatment to eradicate
the parasite should be administered (table below).
❖ Hepatomegaly and bladder lesions regress with early treatment but
established fibrosis persists

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Monitoring (follow up)

Follow-up after treatment includes:

Monitoring of clinical manifestations,


✓ Eosinophilia → initial elevations are likely. Eosinophilia
persisting for > 3 months after therapy may reflect insufficient
drop of parasite burden and/or an additional helminth infection.
Microscopy for eggs in stool or urine
✓ no sooner than 6 weeks in endemic areas following treatment
and 3 - 6 months after treatment in nonendemic areas.
✓ Persistence of viable eggs after 6 to 12 weeks after initial of
therapy warrants repeat treatment with praziquantel (40 to 60
mg/kg in two divided doses as in the initial therapy).
Medical imaging (abdominal ultrasound or MRI)
✓ to document long-term reversal of urinary tract lesions or
periportal liver disease after repeated mass treatment.

Prevention
Control strategies for Schistosomiasis endemic areas include:

☛ Water sanitation programs:


✓ safe water supplies with proper sewage control,
✓ Minimizing contact with fresh water or wearing protective
clothing and footwear in location of freshwater contact,
✓ Vigorous toweling of exposed skin and/or applying insect
repellent DEET (N,N-diethyl-mtoluamide) after exposure to fresh
water.
☛ Mass drug administration (MDA):
✓ praziquantel (nonpregnant and pregnant adults, and children ≥4
years: 40 mg/kg orally once; contraindicated in children <4 years).
✓ Annually repeated MDA is appropriate, but, more frequent
administration may induce resistance in endemic areas.
☛ no vaccine against schistosomiasis
☛ Skin topical agents
☛ Molluscicides – eg. Lemma toxin (Aklilu Lemma from endod)
☛ Follow up of exposed individuals

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Table -Treatment of common intestinal helminthic


parasitic infestations and blood flukes

Scientific name of the parasite/common Management


name/(aetiology);
✓ Mode of transmission and remarks
Ascariasis/round worm/ (Ascaris First line-options
lambricoids) ✓ Albendazole, 400mg P.O. stat,
▪ for children: 1 – 2 years, 200mg stat.
✓ Ingestion of the larvae of the parasite ✓ Mebendazole, 100mg P.O.BID for 3 days or 500mg, stat
together with food
✓ Presence of migrating larvae in the Alternative (pregnant women)
lungs can provoke pneumonia ✓ Pyrantel pamoate, 700mg P.O. stat
Hookworm (Necator americanus or First line-options
Ancylostoma duodenale) ✓ Albendazole, 400mg P.O. stat (preferred) OR
✓ Mebendazole, 100mg P.O. BID for 3 days or 500mg stat
✓ Penetration of the larvae of the parasite
through skin Alternatives:
✓ Pyrantel pamoate, 700mg P.O. stat
Taeniasis/tape worm/ (T. saginata, First line-Intestinal infestation
T.solium) ✓ Praziquantel P.O. 600mg or 10mg/Kg, stat
Alternative
✓ Ingestion of row meat or milk from ✓ Niclosamide, 2g, P.O. stat
cows and pork
✓ T. solium (pork tapeworm) may cause
fatal cysticercosis Treatment of neurocysticercosis
✓ T.saginata is known as beef tape worm ✓ Albendazole P.O. 15mg/kg/day for 8- 28 days or
✓ Praziquantel, 50–100mg/kg/day, TID, for 15–30 days.
▪ Longer courses are often needed in patients with
multiple subarachnoid cysticerci
PLUS
✓ High-dose glucocorticoids
✓ Anti-epileptics (if there is seizure)
Shistosomiasis / bilharziasis/ First line

For S.mansoni, S. hematobium, S. intercalatum


✓ Praziquantel, 40 mg/kg stat or in 2 divided doses 4-6
hours apart on 1 day
For S. japonicum, S. makongi
✓ Praziquantel, 60 mg/kg in 2 divided doses 4-6 hours
apart on 1 day.

☛ Repeated treatment is usually required in endemic areas


☛ Praziquantel is not effective against the larval - thus
treatment is most effective from 4-6 weeks after
exposure, as infection well established and worms fully
matured.

Alternatives
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For S. haematobium
✓ Metrifonate, 600 mg P.O., TID at 14 days interval.
For S. mansoni
✓ Oxamniquine, 1250 mg (30 mg/kg) P.O. stat.
☛ It is contraindicated in pregnancy and in general is
not as effective as praziquantel.
✓ Artemisinin derivatives may be used in very early infection
to disrupt the glucose metabolism of immature
schistosomes.

Considerations in special population

Pregnancy:

✓ Praziquantel is pregnancy category B. Praziquantel is


excreted in breast milk. Although no adverse effects
during lactation have reported, termination of breastfeeding
during treatment and for 72 hours thereafter or postponing
treatment until after breastfeeding might be considered.
✓ Oxamniquine is contraindicated in pregnancy.

Pediatrics:

✓ divided dosing is preferred than single dose in children


and infants (20 mg/kg/dose two to three times daily for 1
day)

Enterobiasis/pin worm/ First line-options


(Enterobius Vermicularis) ✓ Mebendazole, 100mg P.O. BID for 3 days, repeat in 2
weeks OR
✓ Ingestion of the eggs of the parasite ✓ Albendazole, 400mg P.O. stat, repeat in 2 weeks,
together with food
✓ Common in children and auto infection Alternative
may occur ✓ Piperazine, 4g po, stat.

☛ Simultaneous treatment of the entire household is


warranted due to high transmission possibilities

(A) Eggs of E. vermicularis in a cellulose-tape preparation,


(B) in a wet mount, (C) in an iodine-stained wet mount
from a formalin concentrate, (D) viewed under UV
microscopy.
Strongyloidiasis/Thread worm/ First line
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(Strongloidexs stercolaries) ✓ Ivermectin, 200µg/kg daily for 2 days.


✓ For disseminated strongyloidiasis, treatment with
✓ Penetration of the larvae of the parasite ivermectin should be extended for at least 5–7 days or
through skin until the parasites are eradicated.
✓ Larvae migrate to the lungs where they
cause tissue destruction and bleeding. Alternatives-options
✓ Treat concomitant anaemia if any ✓ Thiabendazole, 1500mg, P.O. BID, for 3 consecutive days
(comparable efficacy to ivermectin). OR
▪ for children: 25mg/kg p.o. for 3 consecutive days
✓ Albendazole 400mg P.O.BID for 3 consecutive days (less
effective than ivermectin).

Trichuriasis /whip worm/ (T.tricura) First line-options


✓ Mebendazole, 500mg P.O., stat (preferred over
✓ Heavy infestation leads to bloody Albendazole) OR
diarrhoea, bleeding & weakness ✓ Albendazole, 400mg, P.O. for 3 days

☛ oxantel pamoate 15 to 30 mg/kg (if available) plus


albendazole 400 mg on consecutive days is superior than
other therapies

(A) Egg of T. trichiura in an iodine-stained wet mount, (B)


unstained wet mount, (C) unstained wet mount,(D) Two
eggs of T. trichiura, showing the variability in size of the
species.
First line
Hymenolepis nana /dwarf tapeworm/ ✓ Praziquantel, 25mg/kg or 1800mg P.O. stat, followed by
repeat dose 10 days later

Alternatives
✓ Niclosamide, 2g P.O. on the first day followed by 1g daily
for 6 days

(A-D) Eggs of Hymenolepis nana. On the inner membrane


are two poles, from which four to eight polar filaments
spread out between the two membranes. The oncosphere
has six hooks.
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9.3. Dyspepsia, PUD and GERD (የጨጓራ ሕመም ፣


ቁስለትና አሲድ መብዛት)

9.3.1. Dyspepsia (የጨጓራ ሕመም፣ የምግብ አለመፈጨት ችግር)

 Dyspepsia is not a diagnosis by itself but it is a common symptom with an


extensive differential diagnosis and a heterogeneous pathophysiology

Etiology

 Approximately 25 % of patients with dyspepsia have an underlying organic


cause. However, most commonly (up to 75 % of patients) have functional
(idiopathic or non-ulcer) dyspepsia with no underlying cause on diagnostic
evaluation
 Although there are several organic causes for dyspepsia, the main causes are;
✓ PUD (peptic ulcer disease)
✓ GERD (gastroesophageal reflux disease),
✓ NSAID-induced dyspepsia, and
✓ Gastric malignancy
 Medication (other than NSAID) induced dyspepsia, biliary pain, chronic
abdominal wall pain and pancreatitis are other possible causes.

Clinical features
Dyspepsia describes a wide and common clinical entity which presents
in one of the three ways:
1. Epigastric pain/burning (epigastric pain syndrome)
2. Postprandial fullness
3. Early satiety

ALARM SIGNS (need to be further investigation for cancer)

☬ Advanced age (>55years)


☬ Previous gastric surgery
☬ Unintended weight loss
☬ Persistent vomiting
☬ Hematemesis
☬ Progressive dysphagia/Odynophagia
☬ Otherwise unexplained anemia
☬ Palpable abdominal mass
☬ Lymphadenopathy
☬ Jaundice
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Investigations

✓ H. Pylori test: IgG serology or stool antigen or 13C-urea test


 H. Pylori test needs to be done for the following patients
➢ Long standing dyspepsia
➢ Younger than 55 year
➢ No alarm symptoms
➢ No use of NSAID
➢ No features of GERD
 “Test and treat” for H. Pylori can be practiced in these group of
individuals
 For more about H. Pylori test, click here → 26.5.6 H. Pylori stool antigen
and serum Ab test
✓ Hemoglobin/hematocrit
✓ Stool for occult blood → when indicated
✓ Upper GI endoscopy
☛ Indication
▪ Clinically significant weight loss (> 5% within 6 to 12 months)
▪ Overt GI bleeding
▪ > 1 alarm features
▪ Rapidly progressive alarm features

Treatment

Non pharmacologic; recommend the following for patients with mild


symptoms and no alarm signs
Life style modification
o Dietary recommendations
▪ Avoid offending foods/drinks → Dietary selection should not be
forced or recommended universally unless patients identify the
specific food item as triggering factor (e.g. coffee/caffeine/,
spicy foods, food with high fat content, carbonated beverages/
coca cola, mirinda, pepsi/, and chocolate).
▪ Avoiding meals 2 -3 hours before bed is also advisable.
▪ Eat small amount of food frequently instead of eating much
amount less frequently (e.g small amount of food 5 times daily


instead of much amount 3 times daily)
Eat slowly during each feeding time
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o Weight loss in overweight and obsess patients.


o Use pillows or head elevations to 15-20 cm during sleep.
o Decrease or avoid alcohol
o Stop smoking (for smokers)

Pharmacologic

I. H. Pylori negative
First line→ PPI
✓ Omeprazole, 20mg P.O., BID for 4-8 weeks
✓ Esomeprazole, 40mg P.O., daily for 4-8 weeks
✓ Pantoprazole, 40mg P.O., BID for 4-8 weeks
Alternatives → H2 receptor blockers
✓ Cimetidine, 400mg P.O., BID for 4-8 weeks
✓ Ranitidine, 150mg P.O. BID for 4-8 weeks
✓ Famotidine, 20-40mg P.O. daily for 4-8 weeks

II. H. Pylori positive: H. pylori eradication therapy


First line therapy → All drugs for 7-14 days
✓ Amoxicillin, 1gm, P.O. BID PLUS
✓ Clarithromycin, 500mg, P. O., BID PLUS
✓ PPI
Alternative (for penicillin allergic patients)→ All drugs for 7-14 days
 This regimen has a higher failure rate.
✓ Clarithromycin, 500mg P.O. BID PLUS
✓ Metronidazole, 500mg, P.O. BID PLUS
✓ PPI

➢ For failure of triple therapy, some physicians recommend


quadruple therapy with bismuth added to the triple regimen →
look at the algorism below
o Amoxicillin, 1gm, P.O. BID PLUS
o Clarithromycin, 500mg, P. O, BID PLUS
o PPI PLUS
o Bismuth, 2tab, PO, QID
➢ Serology tests for H. pylori shouldn’t be used as a test of cure
or eradication since they could remain positive for long period of
time.

III. Antacids → for Symptomatic relief


➢ Antacids react with hydrochloric acid in the stomach to form salt
and water which inhibits peptic activity by raising the Ph
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➢ Magnesium antacids tend to be the best buffer


➢ Maalox antacid syrup is available in most setups of Ethiopia →
contains Magnesium hydroxide and Aluminum hydroxide

✓ Magnesium trisilicate + Aluminum hydroxide, 10-30ml, PO, PRN OR


✓ Magnesium hydroxide + Aluminum hydroxide, 10-30ml P.O. OR
✓ Magnesium trisilicate, 100-200mg, P.O. between meals PRN OR
✓ Magnesium hydroxide, 10-30ml or 600+622mg to 1200+1244mg, P.O
between meals PRN

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Algorism; approach to a patient with dyspepsia

* Gastric mucosal biopsies should be obtained at the


time of upper gastrointestinal endoscopy to rule out
infection with H. pylori.
¶ Additional evaluation may be required based on
symptoms (eg, abdominal imaging in patients with
concurrent jaundice or pain suggestive of a
biliary/pancreatic source).
Δ Refer to UpToDate topic reviews.
◊ Patients with continued symptoms of dyspepsia for
three months with symptom onset at least six months
before diagnosis and no evidence of structural disease to
explain the symptoms should be diagnosed and treated
as functional dyspepsia.
§ Eradication of H. pylori infection can be confirmed with
a urea breath test, stool antigen testing, or upper
endoscopy-based testing performed 4 weeks after
completion of antibiotic therapy. The choice of test
depends on the need for an upper endoscopy (eg,
follow-up of bleeding peptic ulcer) and local availability.
H. pylori serology should not be used to confirm
eradication of H. pylori. Refer to UpToDate topic on
diagnostic tests for H. pylori.
¥ Allow 8 to 12 weeks before reassessing symptomatic
response.
‡ For patients with a partial clinical response to a proton

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as combination therapy with a proton pump inhibitor.

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9.3.2. Peptic ulcer disease (PUD)/የጨጓራ ቁስለት/

➢ Peptic ulcers are focal defects in the gastric or duodenal mucosa that extend
into the submucosa or deeper.
➢ The natural history of PUD ranges from resolution without intervention to the
development of complications like bleeding, perforation & GOO (Gastric outlet
obstruction).
➢ N.B anterior duodenal ulcer perforates and posterior duodenal ulcer bleeds.
Perforation is more common in males (M:F ratio = 8-10:1)
➢ PUD needs both medical and surgical evaluation

Pathophysiology
➢ PUD occurs due to imbalance between offending factors/risk factors/ and
mucosal defense mechanisms. Any factor and stimuli that can compromise the
protective mechanisms and/or intensify the damaging forces can result in
mucosal injury and inflammation

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Clinical features

➢ Burning epigastric pain (> 90%)


✓ Patients with duodenal ulcer often experience pain 2 to 3 hours after a
meal and at night, in which 2/3rd of patients with duodenal ulcers will
complain of pain that awakens them from sleep.
✓ The pain of gastric ulcer more commonly occurs during eating .
➢ Associated symptoms
✓ Nausea, bloating
✓ Hematemesis/Melena

Investigations
1. H.pylori tests (Stool antigen, Serum antibody)
2. Upper GI endoscopy has both diagnostic & therapeutic importance → to look
for ulcers, protruding mass or any active bleeding. Gastric mucosal biopsies should be
obtained at the time of endoscopy to rule out infection with H. pylori.
3. Barium meal → It demonstrates barium within the ulcer crater.
4. ECG
☛ ECG should be done in elderly patients & patients with co-morbid illness
like DM, Hypertension & dyslipidemia who present with dyspeptic
symptoms.
☛ This will help you to rule out the life-threatening condition, acute coronary
syndrome.
☛ The rationale behind this workup is the consideration of the dyspepsia
symptom in such patients could be an angina equivalent.
5. Serum gastrin level

Management of PUD
✓ Medical management is the same as Dyspepsia which is discussed above
✓ Surgical treatment for PUD is indicated for:
▪ Perforation
▪ Hemorrhage
▪ Obstruction
▪ Intractable ulcer

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9.3.3. Gastroesophageal reflux disease (GERD)

Some degree of brief reflux occurs physiologically; usually after a meal


or during sleep.
Gastro oesophageal reflux disease (GERD) refers to return of stomach
contents in to the esophagus which is a pathologic reflux associated
with symptoms and complications.
GERD is a common in primary care practice. Due to its symptoms it
can also be misdiagnosed.
Based on the endoscopic appearance GERD is classified in to two
types: Erosive and non-erosive.
✓ Erosive GERD (Erosive esophagitis) is diagnosed when there are
endoscopically visible breaks in the esophageal mucosa while non-
erosive GERD shows no visible mucosal injury on endoscopy.
GERD is associated with significant esophageal or extraesophageal
complications.
o Esophageal complications
 Barrett's esophagus: a precancerous change in the
esophageal mucosa (from squamous epithelium to columnar
epithelium)
 Esophageal stricture: which manifests with solid food
dysphagia and intermittent food impaction.
o Extraesophageal complications
 Triggering Asthma
 Laryngeal and pharyngeal reflux: which manifests with
chronic cough, repetitive throat cleaning, hoarseness of
voice

Clinical manifestations

Symptoms
The two major symptoms of GERD which are considered classic
(typical) are heartburn and regurgitation.
o Heartburn is a commonly described by patients as a burning
sensation behind the sternum (retrosternal area).
o Regurgitation is defined as back flow of gastric contests in to
the mouth or pharynx. Patients feel an acidic (sour) content
coming to the mouth mixed with small amounts of undigested
food.

Other symptoms
o Chest pain: GERD associated chest pain can mimic angina
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o Hoarsens of voice
o Persistent cough
o Nausea
o Sensation of a lump in the throat (Globus sensation)
o Increased salivation (Water brash)

Diagnosis and investigations


Diagnosis
In patients with typical symptoms (i.e. heartburn or regurgitation), the
diagnosis of GERD can be considered on clinical grounds without
additional investigations, if there are no alarm signs. In such cases
empiric therapy should be started.

Investigations
Upper GI (gastrointestinal) endoscopy
o Endoscopy is not necessary to make a diagnosis of GERD but it
is indicated in patients with alarm features to see evaluate for
possible malignancy.
o The alarm features are
 weight loss
 age above 60 years
 iron deficiency anemia
 dysphagia
 persistent vomiting
 family history of cancer in parents or siblings.
o If GERD symptoms have been there for more than 5-10 years,
endoscopy can be considered to look for evidence of Barrett's
esophagus.

Treatment

Non-pharmacologic treatment

1. Life style modifications → look at above from Dyspepsia


2. Surgery
Surgical intervention (usually fundoplication) in GERD patients is
rarely indicated in the following circumstances:
o Large hiatal hernia causing the reflux symptoms
o Evidence of aspiration
o Esophagitis refractory to medical therapy
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o Persistent symptoms documented as being caused by


refractory GERD: after checking compliance to PPI and
optimizing PPI use.

Pharmacologic treatment

First line:
PPIs → No major difference in between the available PPIs
➢ Omeprazole 40mg PO daily for 8 -12 weeks OR
➢ Esomeprazole 40mg PO daily for 8-12 weeks OR
➢ Pantoprazole 40mg PO daily for 8-12 weeks
Stop therapy on symptom resolution to assess response
After the first 8 -12 weeks, resume therapy as needed → Intermittent
OR On demand

Alternatives:
H2 blockers → If PPIs are not available and the symptoms are mild
➢ Cimetidine 400mg BID for 8 weeks OR
➢ Ranitidine 150mg BID for 8 weeks OR
➢ Famotidine 20mg BID for 8 weeks

9.4. GI bleeding

 Gastrointestinal (GI) Bleeding refers to any bleeding that occurs from the
mouth to the anus.
 Anatomically GI bleeding is divided in to upper and lower.
 The ligament of Treitz is used as the anatomic reference to differentiate
lower and upper GI bleeding.

9.4.1. Upper GI bleeding

❖ Upper GI bleeding refers to gastrointestinal blood loss originating from


the GIT is proximal to the ligament of Treitz at the duodenojejunal
junction.
❖ It can be overt or occult bleeding.

1. Overt upper GI bleeding can manifest in the following ways:


➢ Hematemesis: vomiting of frank red blood or a “coffee-grounds”
material.
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➢ Hematochezia: passage of bright red or maroon (dark red) blood


from the rectum. Upper GI bleeding causes hematochezia rarely,
when it is massive and very acute.
2. Occult upper GI bleeding present with symptoms anemia such as
lightheadedness, or a positive fecal occult blood test on routine
testing.

Causes of Upper GI bleeding

❖ The two major causes that should be considered in every patient with
overt upper GI bleeding are peptic ulcer disease and esophageal
varices.

1. Peptic ulcer disease


2. Esophageal varices
3. Gastroduodenal erosions
4. Mallory-Weiss tears (esophageal mucosal tear due to vomiting or
retching)
5. Esophagitis
6. Vascular malformations,
7. Neoplasm
8. Coagulopathy
9. Obscure upper GI bleeding: often from small intestinal lesions

Clinical features
Symptoms
 Nausea
 Vomiting of bright red blood or coffee-ground matter
 Melena
 Hematochezia: rare in upper GI bleeding but can occur in massive acute
bleeding.
 Symptoms related to the underlying cause
✓ Medication history: antiplatelet (aspirin, clopidogrel), NSAID or
anticoagulants
✓ Symptoms of portal hypertension or liver cirrhosis in patients with
variceal bleeding e.g. ascites, fatigue.
✓ The bleeding in varices is generally bright red, painless, brisk, and
voluminous.
✓ Long standing epigastric pain: Suggestive of PUD
✓ Preceding forceful vomiting or retching suggests Mallory-Weiss tears 1090
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✓ Weight loss: may indicate neoplasm

Signs
☬ Signs suggesting the hemodynamic status of the patient and the degree
of anemia
✓ Orthostatic hypotension
✓ Resting tachycardia
✓ Degree of pallor
☬ Signs of the underlying cause of the upper GI bleeding
✓ Signs of CLD or portal hypertension indicating the possibility of
bleeding varices: Ascites, splenomegaly, encephalopathy.
✓ Other site bleeding: platelet related disorders or coagulopathies

Diagnosis and investigations


Diagnosis
The diagnosis is clinical→ a history of hematemesis or melena
The next step in the diagnosis is trying to establish the cause of the
upper GI bleeding.
Upper GI endoscopy → has both diagnostic and therapeutic value.

Investigations
CBC
Serial hemoglobin/hematocrit every 8 hour→ the initial
hemoglobin/hematocrit may be normal as the loss is whole blood (both
plasma and cells)
Coagulation profile: PT (INR) and PPTT
Urea and Creatinine
Liver enzymes
Upper GI endoscopy

Risk stratification

There are a few risk stratification tools which are useful to assess the
likelihood of a person with upper GI bleeding to need further
interventions like endoscopic treatment and transfusion.

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The Glasgow-Blatchford bleeding score (GBS) is one of the scores. It is


simple risk stratification tool which does not require endoscopy. We
recommend using the score
Table.: Glasgow-Blatchford bleeding score (GBS)

Risk marker Value Score


38 - 46 2
Urea (blood urea) (mg/dl) 47 - 57 3
58 - 146 4
>147 6
12 - 13 1
10 - 12 3
males < 10 6
Hemoglobin (g/dl) females 10 - 12 1
< 10 6

100 - 109 1
Systolic BP (mmHg) 99 - 90 2
< 90 3
Pulse ≥100 (per min) 1
Presentation with melena 1
Presentation with syncope 2
Hepatic disease 2
Heart failure 2
Interpretation of the score
✓ 0 → low risk
✓ 1-7 → high risk, keep in hospital as the patient is
likely to require transfusion or endoscopic intervention
✓ ≥ 8 → requires ICU admission

Treatment

1. Hemodynamic stabilization

Monitor airway, BP and PR.


Keep NPO
Secure double IV line (considering transfusion and fluid mgt)
Treat hypotension initially with rapid, bolus infusions of isotonic
crystalloid
Provide transfusion if either of the following is present
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✓ Hemoglobin <9 mg/dL in high-risk patients (e.g. elderly, coronary


artery disease)
✓ Hemoglobin <7 mg/dL in low-risk patients

2. IV PPI for all patients


✓ Omeprazole 80mg IV loading followed by 40mg IV BID OR
✓ Esomeprazole 40 mg IV BID OR
✓ Pantoprazole 40 mg IV BID

3. Arresting bleeding
Endoscopic therapy is the main stay of therapy to arrest bleeding
After hemodynamic stabilization.
Balloon tamponade may be performed as a temporizing measure for
patients with uncontrollable hemorrhage after tracheal intubation.

4. Open surgery

Indications for surgery


✓ Hemodynamic instability despite vigorous resuscitation (> 3 units
three of transfusion)
✓ Shock associated with recurrent hemorrhage
✓ Perforated PUD along with bleeding
✓ Failed endoscopic therapy for bleeding PUD
✓ No access to endoscopy therapy with ongoing bleeding
✓ Relative indications: difficult crossmatch, refusal of transfusion, shock
on presentation,

5. Treating the underlying cause

Patients with H. Pylori associated ulcer bleeding should receive


eradication therapy.
In NSAID or Aspirin associated bleeding ulcers: stop the drug and
re-evaluate the need.
Anticoagulants: stop and re-evaluate for continued need, dose
adjustment if continued
Variceal bleeding: band ligation and non-selective beta-blocker
therapy (propranolol)
Idiopathic (non-H. pylori, non-NSAID) ulcers: long-term PPI is
recommended

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9.4.2. Lower GI bleeding


❖ The incidence of lower GI bleeding is higher in older age groups,
particularly in those taking anti-platelet agents like aspirin, NSAID’s or
anticoagulants.
❖ Lower GI bleeding can be overt or occult.
o Overt lower GI bleeding presents with either frank red bleeding
(hematochezia) or dark, tarry stool (melena).
o Occult GI bleeding presents with evidence of iron deficiency anemia
but no hematochezia or melena.
❖ Lower GI bleeding is labeled to be massive when it is associated with
hemodynamic instability.

Causes of lower GI bleeding

1. Vascular causes
o Hemorrhoids
o Ischemic bowel
o Vascular dysplasia (angiodysplasia)
o Post procedure (post polypectomy)
2. Neoplastic causes
o Colon cancer
o Polyps
3. Anatomic causes
✓ Diverticulosis
4. Inflammatory causes
✓ IBD
✓ Infectious colitis

Clinical manifestations
Symptoms

 Hematochezia: passage of bright red or dark red (maroon) blood or


clots per rectum.

✓ Bleeding from the left colon tends to be bright red in color while
bleeding from the right colon appears to be dark or maroon colored
and may be mixed with stool.
✓ Bleeding from the right colon might rarely cause melena (the stool
itself is dark)
 Symptoms of anemia or hemodynamic compromise: fatigue, postural
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Signs

 Signs of hemodynamic compromise:


✓ Hypotension (supine or postural)
✓ Resting tachycardia.
 Signs of anemia
✓ Pallor
✓ Tachycardia
✓ Ejection systolic murmur

Diagnosis and investigations


Diagnosis
1. Identifying whether the bleeding is upper or lower GI in origin.
✓ Massive upper GI bleeding can cause hematochezia; hence,
differentiating Upper from lower GI bleeding is necessary.
✓ The presence of hemodynamic instability favors upper GI bleeding
✓ The presence of clots suggests lower GI bleeding
✓ When there is suspicion of upper GI source: insert NG tube and do
gastric lavage with normal saline
 Gastric lavage with coffee-ground material or bright red blood=
upper GI bleeding
 Gastric lavage is bilious = lower GI bleeding
 If the gastric lavage is neither of the above = indeterminate (it
can be either of the two)
2. Identifying possible causes or precipitants of the bleeding.
✓ The history should focus on the following

➢ Medications: Antiplatelets (e.g. Aspirin or clopidogrel), NSAID’s (e.g.


Diclofenac, indomethacin, ibuprofen), anticoagulants
➢ Prior history of bleeding
➢ Significant abdominal pain: suggests inflammatory or ischemic bowel
disease or perforation
➢ Significant weight loss: suggests malignancy

✓ DRE
3. Localization of the bleeding and definitive diagnosis
✓ All patients with a clinical diagnosis of lower GI bleeding require
colonoscopic examination to identify the cause of bleeding, arrest
the bleeding if identifiable.

Investigations

☬ Baseline IX
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✓ CBC: in massive acute bleeding the hemoglobin may appear


normal.
✓ Serial hemoglobin; every 8 hours
✓ Coagulation studies: INR (PT) and PTT
✓ Liver enzymes
✓ BUN and creatinine
☬ Colonoscopy: when the clinical diagnosis is lower GI bleeding
☬ Upper GI endoscopy: when the clinical diagnosis is upper GI bleeding.

Treatment
1. Hemodynamic status evaluation and resuscitation
o In patients with hemodynamic compromise secure two wide bore IV
cannula and resuscitate with crystalloids.
o While crystalloids are being given, blood should be requested for
transfusion.
✓ Do not depend on the initial hemoglobin or hematocrit to for
transfusion, as it is apparently (“falsely”) normal.
2. Discontinue antiplatelets, NSAID’s or anticoagulants
3. Correct coagulopathies
o E.g. If INR is high or patients has been on warfarin, give fresh
frozen plasma and/or vitamin K
4. Surgical consultation
o In patients who continue to bleed massively and who are unstable to
do colonoscopy or if colorectal cancer is suspected

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9.5. IBD (inflammatory Bowel Disease)


➢ IBD is a chronic idiopathic inflammatory disease of the GIT caused by a
dysregulated immune response to host intestinal microflora
➢ The two major types of IBD are
o Ulcerative colitis (UC) and
o Crohn’s disease (CD)
➢ These disorders have both distinct and overlapping pathologic and
clinical characteristics
➢ There is a genetic predisposition for IBD and patients with this condition
are more prone to the development of malignancy

Epidemiology of IBD

➢ The incidence of IBD varies within different geographic areas


➢ Highest incidence is seen in Europe, the United Kingdom, and North
America
➢ Peak incidence of UC and CD is in the 2nd to 4th decades (15-30 years)
o A second modest rise in incidence occurs between the 7th and 9th
decades of life (60-80 years)
➢ Pediatric IBD (patients <17 years old) composes ∼20–25% of all IBD
patients, and ∼5% of all IBD patients are <10 years old
➢ Urban areas have a higher prevalence of IBD than rural areas, and high
socioeconomic classes have a higher prevalence than lower
socioeconomic classes
➢ Smoking is an important risk factor in IBD with opposite effects on UC
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➢ IBD is a familial disease in 5–10% of patients, and the strongest risk


factor for the development of IBD is a first-degree relative with the
disease
➢ Children of mothers and fathers with UC have an approximately fourfold
increased risk of UC, and the children of mothers and fathers with CD
have an almost eightfold increased risk of CD

UC CD
causes ulceration and inflammation CD can affect any part of the GI
of the inner lining of the colon and tract from the mouth to the anus
rectum
Affects only the mucosa Transmural inflammation
No skip lesions Segmental with skip lesions
Almost always involves the rectum Rectum is often spared in CD.

Broad areas of ulceration “Cobblestone” appearance


Smoking is protective Smoking is Risk factor

ULCERATIVE COLITIS (UC)

UC is a mucosal disease that usually involves the rectum and


extends proximally to involve all or part of the colon.
o About 40–50% of patients have disease limited to the rectum
and rectosigmoid
o 30– 40% have disease extending beyond the sigmoid but not
involving the whole colon, and
o 20% have a pancolitis.
▪ 10-20% of patients may develop backwash ileitis (UC
involving terminal ileum)
UC, almost always involves the rectum
Proximal spread occurs in continuity without areas of uninvolved
mucosa

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FIGURE 326-3 (Harrison 21st edition) Ulcerative colitis. Diffuse (nonsegmental) mucosal
disease, with broad areas of ulceration. The bowel wall is not thickened, and there
is no cobble stoning

Clinical presentation of UC
The major symptoms of UC are;
o Diarrhea → usually nocturnal or postprandial
o Rectal bleeding
o Tenesmus
o Passage of mucus, and
o Crampy abdominal pain.
Can have acute or subacute to chronic presentation
The severity of symptoms correlates with the extent of disease
Occasionally, diarrhea and bleeding are so intermittent and mild that
the patient does not seek medical attention
When the disease extends beyond the rectum, blood is usually
mixed with stool or grossly bloody diarrhea may be noted
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Constipation is commonly seen in patients with proctitis, while


disease beyond rectum is associated with diarrhea
Severe cramping and abdominal pain can occur with severe attacks
of the disease
Other symptoms in moderate to severe disease include anorexia,
nausea, vomiting, fever, and weight loss
Physical signs include
o Tender anal canal
o Direct tenderness on palpation of the colon
o Blood on rectal examination
o Hepatic tympany in patients with megacolon
o Signs of peritonitis in patients with perforation

Table; Clinical Severity of UC


Mild Moderate Severe Fulminant
Bowel movement <4 >6 >10
Blood in stool Intermittent Frequent Continuous
Temperature Normal >37.5° >37.5°
Pulse Normal >90 bpm >90 bpm
Intermediate
Hemoglobin Normal <75% normal rate Transfusion required
ESR <30 mm/hour >30 mm/hour >30 mm/hour
Abdominal Abdominal distension
Clinical signs
tenderness and tenderness

Complications of UC

➢ Toxic megacolon
➢ Toxic colitis
➢ Massive hemorrhage
➢ Perforation
➢ Strictures
➢ Malignancy

Diagnosis of UC

Laboratory features
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o Raised ESR, CRP and platelet count


o Decreased hemoglobin
o hypoalbuminemia
o Fecal lactoferrin and calprotectin levels
o +ve Fecal occult blood test
o Active inflammation, predict relapses, and detect pouchitis
o Leukocytosis
o Negative stool examination for bacteria, C. difficile toxin, and
ova and parasite
Sigmoidoscopy
o Should be done before initiation of treatment
o Used to assess disease activity and severity
Barium enema
o Fine mucosal granularity
o Mucosal thickening
o Ulcerations
o Loss of haustration
o Shortened and narrowed colon
o Postinflammatory polyps (pseudopolyps)
CT- scan

CROHN’S DISEASE (CD)

➢ CD can affect any part of the GI tract from the mouth to the anus.
o Some 30–40% of patients have small-bowel disease alone
o 40–55% have disease involving both the small and large intestines,
and
o 15–25% have colitis alone.
➢ In the 75% of patients with small-intestinal disease, the terminal ileum is
involved in 90%.
➢ Unlike UC, which almost always involves the rectum, the rectum is often
spared in CD.
➢ CD is often segmental with skip areas throughout the diseased intestine
➢ Unlike UC, CD is a transmural process
➢ “Cobblestone” appearance is characteristic of CD, both endoscopically
and by barium radiography

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FIGURE 326-5 (Harrison 21st edition) Crohn’s disease of the colon. showing thickening
of the wall, with stenosis, linear serpiginous ulcers, and cobble stoning of the
mucosa

Clinical presentation of CD

Can present with one of the two patterns of the disease:


o A fibrostenotic obstructing pattern or
o A penetrating fistulous pattern
The site of disease influences the clinical manifestations
o Ileocolitis
o Jejunoileitis
o Gastroduodenal disease
o Colitis and perianal disease

Ileocolitis
o The most common site of inflammation is the terminal ileum
o Right lower quadrant pain and mass- mimicking acute
appendicitis
o Diarrhea
o Weight loss due to diarrhea, anorexia, and fear of eating
o Features of bowel obstruction and postprandial pain
o Fistula formation to adjacent bowel, the skin, or the urinary
bladder
▪ Dysuria, pneumaturia, fecaluria, or recurrent bladder
infection
Jejunoileitis
o Loss of digestive and absorptive surface
▪ Malabsorption and steatorrhea
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o Diarrhea due to:


▪ Bacterial overgrowth in obstructive stasis or fistulization
▪ Bile acid malabsorption due to a diseased or resected
terminal ileum
▪ Intestinal inflammation with decreased water absorption
and increased secretion of electrolytes
Gastoduodenal disease
o Nausea, vomiting, and epigatric pain
o H. Pylori-negative gastritis
o Fistulas
o Chronic gastric outlet obstruction (GOO)
Colitis and perianal disease
o Low-grade fever and malaise
o Diarrhea
o Crampy abdominal pain
o Hematochezia
o Strictures
o Fistula formation into stomach or duodenum
o Perianal disease
▪ Incontinence
▪ Large hemorrhoidal tags
▪ Strictures
▪ Anorectal fistulae
▪ Perirectal abscess

Complications of CD
Fistula formation
Bowel perforation
Intraabdominal and pelvic abscess
Intestinal obstruction
Massive hemorrhage
Malabsorption
Severe perianal disease

Diagnosis of CD
➢ Laboratory features
o Elevated ESR and CRP
o Hypoalbuminemia
o Anemia
o Leukocytosis
➢ Endoscopic features
o Rectal sparing
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o Aphthous ulcerations
o Fistulas
o Skip lesions
o Can be both diagnostic and interventional
➢ CT enterography and pelvic MRI

Extraintestinal manifestations
Up to 1⁄3 of IBD patients have at least one extraintestinal disease
manifestation
Dermatologic
o Erythema nodosum
o Pyoderma gangrenosum

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Rheumatologic
o Peripheral arthritis
o Ankylosing spondylitis
o Sacroiliitis
Ocular
o Conjunctivitis
o Anterior uveitis/iritis
Hepatobiliary
o Fatty liver
o Cholelithiasis
o Primary sclerosing cholangitis
Urologic
o Nephrolithiasis
o Ureteral obstruction
o Ileal bladder fistula
Metabolic bone disorders
Thromboembolic disorders

Treatment of IBD
➢ Includes medical and surgical interventions
➢ Goals of therapy
o Remission induction and
o Prevention of disease flares (maintenance)
➢ Nutritional therapies
o Dietary antigens may stimulate the mucosal immune response
o Patients with active CD respond to bowel rest, along with TPN
o Liquid or pre-digested formula for enteral feeding reduces inflammation in
CD patients
o Multivitamin supplementation

Medical therapies
5-ASA agents
o Are the mainstay of therapy for mild to moderate UC
o Effective at inducing and maintaining remission in UC
o Include sulfasalazine and mesalamine
o Can be administered orally or as enemas
o Side effects include allergic reactions, headache, nausea, and
vomiting
Glucocorticoids
o For moderate to severe disease
o Effective only for remission induction
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o Prednisone 40-60 mg/day- starting dose, Then gradual tapering


o Side effects- fluid retention, abdominal striae, fat redistribution,
hyperglycemia, osteoporosis, myopathy, emotional disturbances,
withdrawal symptoms etc
Antibiotics
o Metronidazole and ciprofloxacin are effective in active inflammatory,
fistulous, and perianal CD
o Antibiotics have no role in the treatment of active or quiescent UC,
except in those with pouchitis
Azathioprine and 6-mercaptopurine
o CD, remission maintenance or reduction of steroid use:
▪ Azathioprine, 2 to 3 mg/kg, Po, daily
▪ Mercaptopurine, 1 to 1.5 mg/kg, Po, daily
o UC:
▪ Azathioprine, 1.5 to 2.5 mg/kg, Po, daily
• UC, remission maintenance or reduction of steroid use
▪ Mercaptopurine
• Initial: 50 mg once daily; titrate dose up if clinical remission
not achieved or down if leukopenia occurs
• Maintenance: 1 to 1.5 mg/Kg, Po, daily
o Commonly used in the management of glucocorticoid-dependent IBD
o Glucocorticoid-sparing agents
o Azathioprine is effective for postoperative prophylaxis of CD
o Are associated with four-fold increased risk of lymphoma
Methotrexate
o Inhibits dihydrofolate reductase resulting in impaired DNA synthesis
o Effective in inducing remission and reducing glucocorticoid dosage
o Side effects include leukopenia and hepatic fibrosis
Cyclosporine
o Inhibits both cellular and humoral immunity
o Used in patients with glucocorticoid-resistant IBD
Tacrolimus
o A macrolide antibiotic with immunomodulatory properties
o For refractory IBD

Biological therapies
➢ Anti-TNF therapy
o Infliximab
o Adalimumab
o Cetrolizumab
o Golimumab
➢ Anti-integrins
o Natalizumab
o Vedolizumab
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FIGURE 326-12 (Harrison 21st edition) Medical management of inflammatory bowel


disease. 5-ASA, 5-aminosalicylic acid; CD, Crohn’s disease; UC, ulcerative colitis.

Surgical therapies
Indications for Surgery

TABLE 326-10 (Harrison 21st edition) Indications for Surgery 1107


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9.6. Constipation
➢ Constipation is difficult to define. In general, it may be defined as
infrequent passage of stool.
➢ It may be caused by either organic or functional disorders.
➢ A new onset of constipation should be taken as an alarm sign for
possible colorectal malignancy; hence investigation for the underlying
cause should be performed before resorting to symptomatic treatment.

Clinical features

➢ Complaint of persistent, difficult, or infrequent, or seemingly incomplete


defecation.
➢ Diagnosis is mainly clinical

Non pharmacologic

➢ Removal of the underlying cause


➢ More fiber diet intake
➢ High residue diet intake
➢ Increased fluid intak

Pharmacologic

➢ Short term relief of severe constipation


o Magnesium sulfate, 10-20mg, PO, in a glass of water, preferably
before breakfast.
➢ For chronic constipation
o Treating constipation with laxatives of any type for long period of
time is not advisable.
o All patients with more than acute constipation should be evaluated
for colonic cancer.
o The presence of weight loss, anemia, and anorexia are strong
indicators of malignancy.

First line

o Bisacodyl, 5 - 10mg, P.O. at night OR 10mg rectally in the morning

Alternatives
o Glycerin rectally at night after moistening with water
o Liquid paraffin, 10ml, P.O. every 8-12 hours as required
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Chapter 10; UTI (የሽንት ቧንቧ


ልክፍት/ኢንፌክሽን/)

➢ UTI (urinary tract infection) refers to the presence of microorganisms in


higher numbers to cause invasion of the urinary tract (UT) epithelium and
inflammation that cannot be accounted for contamination.

Classification of UTI
➢ UTI is classified in different ways that have implication to treatment and
outcome
1. According to anatomic site of involvement:
✓ Lower UTI: cystitis, urethritis, prostatitis
✓ Upper UTI: pyelonephritis, involving the kidney

2. According to the presence of structural urinary tract problems

✓ Uncomplicated UTI:
☛ occurs in individuals who lack structural or functional
abnormalities in the UT that interfere with the normal flow of
urine.
☛ Mostly in healthy females of childbearing age.
✓ Complicated UTI:
☛ occurs in individuals with structural or functional abnormalities in
the UT that can interfere with normal flow of urine such as
▪ congenital distortion of the UT
▪ a stone
▪ an indwelling catheter or the use of intermittent bladder
catheterization
▪ vesicoureteral reflux or other functional abnormalities
▪ BPH
▪ Obstruction
▪ neurological deficit.
☛ UTI in men and pregnant women can be classified as complicated.
☛ RF risks for serious infections
▪ Recent urinary tract instrumentation
▪ peri-and postoperative UTI
▪ CKD and transplantation
▪ poorly controlled diabetes mellitus
▪ immunosuppression (such as neutropenia or advanced HIV
infection).
➢ In addition, patients should also be carefully evaluated for high risk of
resistant infections
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Recurrent UTI
❖ Multiple symptomatic UTIs with asymptomatic periods in between.
❖ Significant when there a r e ≥ 2 symptomatic episodes per year or it
interferes with patient’s quality of life.
❖ It is usually a reinfection than a relapse.
▪ Relapse: Infection with same organism within 14 days of stopping
antibiotics for previous UTI
▪ Reinfection: a completely different organism; most common cause
of recurrent cystitis

Bacteriuria
❖ Asymptomatic bacteriuria:
✓ Bacteriuria > 105 bacteria/ml of urine without symptoms.
✓ It is very common in elderly women and men.
✓ Use of antibiotics for asymptomatic bacteriuria can drive antibiotic
resistance and increase the risk for subsequent symptomatic UTI.
✓ Asymptomatic bacteriuria should be treated in pregnant women and
in men undergoing urological procedures. The benefits of therapy in
other groups were questionable.
❖ Symptomatic abacteriuria:
✓ Symptoms of urinary frequency and dysuria in the absence of
significant bacteriuria

Etiologies
➔ The vast majority of acute symptomatic infections occur in young
women.
➔ E. coli cause approxmatley 80% of acute infections in patients without
catheters, stone or other urologic abnormalities. On the other hand,
organisms like klebsiella, enterobacteria, proteus, serratia and
psuedomonas assume greater importance in complicated and nosocomial
UTIS.

Clinical features
❖ The range of possible symptoms caused by UTI is extremely broad,
from no symptoms to symptoms referable to the lower urinary tract
(e.g. dysuria and frequency), to symptoms indicative of an upper UTI
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full-blown urosepsis.

❖ Lower UTI (Cystitis)


▪ Commonly dysuria, frequent urination and urgency;
Occasionally, gross hematuria, Suprapubic pain
▪ Elderly people may have nonspecific symptoms only (like
chronic dysuria or urinary incontinence, mental status changes,
abdominal pain and decreased eating or drinking)
▪ Chronic nocturia or chronic incontinence, general malaise, and
cloudy or malodorous urine are nonspecific features that should
not routinely swift for cystitis evaluation and treatment.

❖ Upper UTI (pyelonephritis)


▪ dysuria, frequent urination and urgency, hematuria
▪ Systemic symptoms like fever, chills, rigors, and marked fatigue
or malaise beyond baseline, nausea, vomiting
▪ Suprapubic pain
▪ Costovertebral angle tenderness; flank pain
▪ Pelvic or perineal pain (in men),
▪ Elevated WBC
▪ Elderly people may have nonspecific symptoms only (like
mental status changes, abdominal pain and decreased eating
or drinking)

Investigations and diagnosis

➢ Clinical
☛ signs and symptoms and urinalysis are the common
diagnostic methods
☛ Digital rectal examination (DRE): For men with symptoms of
pelvic or perineal pain, DRE might be warranted to evaluate a
tender or edematous prostate, suggesting acute prostatitis.

➢ Urine analysis
☛ pyuria (WBC > 10 cells/mm3)
present in almost all patients with UTI.
Hence, its absence suggests alternative diagnosis
particularly in patients with nonspecific symptoms.
☛ bacteriuria → >102 CFU/ml is diagnostic.
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in clean catch specimen.


In women with symptomatic UTI a lower bacterial count
should be used as 1/3 of symptomatic women have <105
CFU/ml. (e.g. 100 CFU/ml will have higher positive
predictive value)
☛ Cloudiness
☛ Red blood cells
☛ Nitrite positive (E. coli, Proteus, Klebsiella),
☛ Leukocyte esterase positive,
☛ Casts (if pyelonephritis)
fever and flank pain, even in absence of typical
symptoms of cystitis may suggestive for pyelonephritis.

➢ Urine gram stain and culture


☛ Blood cultures → +ve in 20% of patients with upper UTI
☛ Indication for blood culture
complicated UTI
recurrent UTI
Pyelonephritis
urosepsis.

➢ Imaging:
☛ e.g. Abdominal U/S (kidneys and urinary tract)- indicated in
complicated UTIs (suspected obstruction, severely ill)
poor responders and recurrent UTIs.
☛ Radiology helps to see calculus or obstruction or abscess

Treatment

Non pharmacologic

❖ Postcoital voiding and liberal fluid intake for women with recurrent
UTI
❖ Manage underling anatomical or functional urinary obstruction or
abnormality.
☛ Antimicrobials alone might not be effective unless correcting
such underlying conditions.
☛ Patients with neurogenic bladder, indwelling bladder catheters,
nephrostomy tubes, and urethral stents may require additional
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urinary flow, exchange or removal of a catheter, or


urologic/gynecologic consultation.

Pharmacologic

A. Acute uncomplicated lower UTI (cystitis)


First line

✓ Ciprofloxacin 250- 500mg PO, BID for 3 days or


✓ Norfloxacin, 400mg PO., BID, for 3 days. or
✓ Cotrimoxazole (TMP-SMO) 960mg (160/800mg) P.O, BID for 3 days or
✓ Nitrofurantoin 50mg P.O., QID for 7 days (effective if available)
Alternative

✓ Fosfomycin 3g single dose OR


✓ Cefpodoxime100mg PO, BID for 5 days OR
✓ Amoxicillin-clavulanate 500/125mg TID for 5 days

B. Mild to moderate upper UTI (Pyelonephritis)

☛ like pyelonephritis, known comorbidities and with immunosuppression


☛ able to take orally with no vomiting, no dehydration, no evidence of
sepsis

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First line

✓ Ciprofloxacin, 500mg P.O., BID, oral for 7-10 days.

NB: for the following indications

✓ For patients requiring temporary emergency admission


✓ in a community with local flurorquinolone resistance >10%
(may be true for certain settings in Ethiopia)
✓ patients intolerant to fluoroquinolone

use the following

✓ single dose ceftriaxone (1 gram IV or IM) initially or


✓ Ertapenem (if available) 1 gram IV or IM or
✓ gentamicin 5 mg per kg IV or IM, once)

can be administered along with or followed by an oral


fluoroquinolone (if no tolerance issue)
Among the available fluoroquinolones, moxifloxacin attains lower
urinary levels than others and should not be used for UTI

Alternative

✓ Cotrimoxazole, 960mg P.O, BID for 14 days. Or


✓ Cefpodoxime proxetil, 200mg P.O., BID for 10 days (β-Lactam for 10–14
days; less effective than first two options)

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C. Severe acute upper UTI (Pyelonephritis)

(e.g. pyelonephritis) (high grade fever, vomiting, dehydration, or


evidence of sepsis) without risk of resistant infections → start IV

First line

✓ Ciprofloxacin, 400mg, I.V, BID or


✓ ceftriaxone, 2gm, I.V, daily or 1gm, I.V, BID
till patient improves (usually at 48 - 72 hours) and then continue
✓ Ciprofloxacin 500mg, PO, BID to complete 10-14 days course, on
discharge.

Alternative

✓ Ceftriaxone or cefotaxime co-prescribed with gentamycin/ amikacin

D. Severe pyelonephritis with the either of following


three risk factors for of resistant pathogens in the
last 3 months

1. Multidrug-resistant urinary isolate


2. Inpatient stay at a health care facility
3. Use of a broad-spectrum antibiotic (fluoroquinolone, 3rd or later generation
cephalosporin trimethoprim-sulfamethoxazole)

First line

✓ Meropenem 1gm IV TID OR


✓ Imipenem 500mg IV QID

Alternative

✓ Ceftazidime 2 gm IV TID or
✓ Cefepime 2 gm IV TID
✓ Piperacillin-tazobactam 3.375 gm IV QID
o piperacillin-tazobactam may be used as an initial agent due to
its advantage of covering gram positive cocci (staphylococci and
enterococci) infections.

Addition of aminoglycoside: Gentamycin 3-5mg/Kg, IV, daily can be


considered
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Vancomycin may be added based on the potential for MRSA (e.g.


previous MRSA isolate from the patient)

E. Recurrent UTI

✓ Antibiotic prophylaxis is recommended for


▪ women who experience ≥ 2 symptomatic UTIs within 6
months or ≥ 3 over 12 months.
▪ Recurrent pyelonephritis.
✓ Any prophylaxis should be given after current active infection is
treated.
✓ Recurrent infections might be a relapse or reinfection
❖ Relapse: assess pharmacologic reason for treatment failure.
Use longer treatment courses (for 2 - 6 weeks, depending on
length of initial course)
❖ Reinfection: reassess need for continuous prophylactic
antibiotics every 6 - 12 months.
1) If patient has ≤ 2 UTIs in 1 year, use therapy for symptomatic
episodes only (3-day treatment regimens).
2) If patient has ≥ 3 UTIs in 1 year and they are temporally related to
sexual activity
☛ use post-intercourse prophylaxis with
• cotrimoxazole single strength or
• cephalexin 250 mg or
• nitrofurantoin 50 - 100 mg and
☛ counsel on voiding after intercourse. Postcoital voiding and
liberal fluid intake is also recommended.
3) If patient has ≥ 3 UTIs in 1 year that are not related to sexual
activity
☛ The antibiotic prophylaxis options
o Trimethoprim-sulfamethoxazole 40 mg/200 mg once daily or 3
times per week
o Nitrofurantoin 50 mg or 100mg once daily
o Cephalexin 125 mg -250mg once daily
o Norfloxacin 200 mg once daily
o Ciprofloxacin 125 mg once daily
o Cefaclor 250 mg once daily
Usually duration of antibiotics is for six months followed by
observation.
If recurrent UTI comes again the prophylaxis can be prolonged for
1-2years.

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F. Prostatitis

Considered in men presenting with cystitis symptoms that are


recurrent or are accompanied by pelvic or perineal pain.
Primarily caused by gram-negative organisms.

1. Acute bacterial Prostatitis:


Fluroquinolones or cotrimoxazole for 4 weeks is first line agents.
2. Chronic bacterial prostatitis:
Difficult to treat
similar antibiotics to acute bacterial Prostatitis are used but for
a duration of 1 - 4 months.

G. Epididymitis

a. In patients older than 35 years


enteric organisms are the most probable causes.
Fluroquinolones or cotrimoxazole for 10 days to 4 weeks
b. In patients younger than 35 years
gonococcal or chlamydial infections are more probably causes.
ceftriaxone 250 mg IM once plus doxycycline 100 mg BID for
10 days.

Special population considerations

Pregnancy

pregnant women should be screened for bacteriuria and treated, even


if asymptomatic.
Antibiotic options recommended for
❖ uncomplicated UTI in pregnant women were:
✓ Augmentin for 3-5 days
✓ Cephalexin or cefpodoxime for 3-5 days
✓ Cefpodoxime for 3-5 days
✓ Nitrofurantoin (avoid at term if other options available) for 5
days.
❖ For sever or complicated scenarios
✓ 3rd generation cephalosporin’s (cefotaxime or ceftriaxone).
❖ In the presence of a risk for resistant infections the following can be
used as indicated for sever acute pyelonephritis.
✓ piperacillin-tazobactam or
✓ cefepime or
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✓ ceftazidime

☛ Antibiotics to be avoided for pregnant are


➔ Fluoroquinolones
➔ aminoglycosides and
➔ cotrimoxazole (used frequently but avoid especially during the
late 3rd trimester).

Paediatrics
Lower uncomplicated UTI (acute cystitis)
First line agents:
✓ Cotrimoxazole, 48mg/kg/day, PO, BID for 3- 5 days (available
syrup preparation 240mg/5ml)
o not recommended in the first 6 weeks of life.
Alternatives
✓ Augmentin 50-80mg/kg/day, PO, TID for 3-5 days (available syrup
preparation 400mg/5ml or 200mg/5ml) or
✓ Amoxicillin 50-80mg/kg/day, PO, TID for 3-5 days (available syrup
preparation 250mg/5ml, or 125mg/5ml)

❖ Fluoroquinolones are not recommended in paediatrics unless for


sever complicated conditions in the absence of other alternatives
(if no alternative Ciprofloxacin 10 mg/kg/dose, BID or TID, for 3
days).

Upper uncomplicated UTI (Acute pyelonephritis)


First line agents:
✓ Ceftriaxone 50-80 mg/kg IV daily
✓ Following initial response to parenteral therapy: Consider
changing to: Cefixime 16 mg/kg the first day then 8 mg/kg/day,
po, daily or BID to complete 10 days
Alternatives
✓ Ampicillin 50mg/kg/dose QID plus
✓ Gentamycin 7.5mg/kg daily

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Chapter 11; Acute febrile illness (AFI)

11.1. Malaria (ወባ)

➢ Malaria is a parasitic infectious disease caused by protozoan


parasites of the genus Plasmodium and is transmitted by
mosquitoes.
➢ It is characterized by recurrent symptoms of chills, fever and
generalized body pain.
➢ Aetiology: five Species of the genus plasmodia
– P. Falciparum
– P. Vivax
– P. Ovale
– P. Malariae
– P. Knowlesi
The commonest causes of Malaria in Ethiopia are P. Falciparum & P.
vivax
They are prevalent in all malaria endemic areas in the country with P.
falciparum representing about 81% (HMIS 2021) of the total reported malaria
cases.
The erythrocytic cycle, which is responsible for clinical paroxysms, takes about
o 48 hours in P. falciparum, P. vivax, and P. ovale infections (tertian
cycle)
o 72 hours with P. malariae infection (quartan cycle).

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Mode of transmission
➢ There are three modes of malaria transmission:
o The bite of an infected female anopheline mosquito (the main
method of transmission);
o Accidental transmission via blood transfusion or needle stick injury;
and
o Congenital transmission from mother to child during pregnancy or
parturition.

Epidemiology
❖ Malaria is a major public health problem in Ethiopia. About 75% of the total
area of the country is considered malarious and about 52% of the
population living in these areas is at risk of malaria.
❖ Majority of malaria cases have been due to P. falciparum, with the
remainder caused by P. vivax.
❖ Principal determinants of the epidemiology of malaria
1. Number, Density, human – biting habit and longevity of the
vector. Eg. Anopheles gambae is long-lived, breed readily, high
density in the tropics, preferably bites humans to other animals
2. Entomologic inoculation rate; Sporozoite + ve mosquitoes/Person
/Yr (>300 in tropical Africa)

❖ Endemicity of malaria is determined by parasitaemic rates or palpable


spleen
rates in children 2-9 yrs of age
✓ Hypo endemic - <10%
✓ Meso endemic - 11-50%
✓ Hyperendemic - 51-75%
✓ Holoendemic - > 75%

Life cycle of plasmodia

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Figure: Life cycle of malaria parasite

1. Plasmodium-infected Anopheles mosquito bites a human and transmits sporozoites into the
bloodstream.
2. Sporozoites migrate through the blood to the liver where they invade hepatocytes and divide to

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form
multinucleated schizonts (pre-erythrocytic stage).
3. Hypnozoites are a quiescent stage in the liver that exist only in the setting of P. vivax and P.
ovale infection. This liver stage does not cause clinical symptoms, but with reactivation and release

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into the circulation, late onset or relapsed disease can occur up to many months after initial
infection.
4. The schizonts rupture and release merozoites into the circulation where they invade red blood cells.
Within red cells, merozoites mature from ring forms to trophozoites to multinucleated schizonts
(erythrocytic stage).
5. Some merozoites differentiate into male or female gametocytes. These cells are ingested by the
Anopheles
mosquito and mature in the midgut, where sporozoites develop and migrate to the salivary glands
of the mosquito. The mosquito completes the cycle of transmission by biting another host.

Malaria Transmission pattern

1. Stable malaria transmission


Transmission throughout the year
Fairly uniform intensity of transmission with little variation over the
years
Long- living and frequently biting mosquitoes present
High immunity in the community due to intense transmission
Young children and pregnant women are susceptible groups
Eradication of malaria is very difficult
2. Unstable Malaria transmission
Uneven, erratic, less intense transmission
Liable to flare-up into dramatic epidemics
Short lived and less frequently biting mosquitoes present
Low immunity status of the community
All age groups are frequently affected
Eradication of malaria is much easier than stable malaria

Pathogenesis
The disease in humans is caused by the direct effects of RBC invasion
and destruction by the asexual parasite and the host’s reaction
NB: Almost all deaths are caused by falciparum malaria

Pathogenesis of falciparum malaria


✓ RBC membrane changes result in cytoadherence and rosette formation
→ sequestration of red cells containing mature form of the parasite in
vital organs (particularly the brain) → interfere with microcirculatory flow
& metabolism
✓ Splenic immunologic and filtration clearance functions → accelerated
removal of both parasitized and uninfected RBCs
✓ Both humoral and cell mediated immunity are necessary for protection.
Immune individuals have a polyclonal increase in serum levels of IgM, IgG
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and IgA,
although much of this antibody is unrelated to protection.

Host Factors: -
Geographic distribution of sickle cell disease, thalassemia and G6PD Deficiency
closely resemble that of malaria before introduction of control measures

Sickle cell disease - low O2 tension -  parasite growth


–  Severity of malaria (MR)

Factors retarding development of (cellular) immunity to malaria

Absence of MHC-Ags on infected RBCs Surface


Malaria Ag- Specific immune unresponsiveness
Strain- Diversity of malarial parasites
Expression of changing immunodominant Ags on RBC surface

Clinical features of Uncomplicated Malaria


Non-complicated malaria is symptomatic malaria with parasitemia without
signs of severity or evidence of vital organ dysfunction.
The main manifestation of uncomplicated malaria is fever.
Other symptoms are
o Chills, rigors
o headaches and body pains
o malaise,
o nausea, vomiting,
o joint weakness→ Arthralgia, myalgia
o NB - the classical malaria paroxysms of fever spikes, chills and
rigors occurring at regular interval (relatively unusual) signify infection
with P. vivax or P. ovale
Physical examination may reveal
o Fever, Tachycardia, Postural hypotension, Delirium
o Pallor
o Hepatosplenomegaly.
o Mild Jaundice

clinical diagnosis
❖ A patient from malaria endemic area has fever or history of fever in the
last 48 hours or a patient from non-malaria endemic area has fever or
history of fever in the last 48 hours and has a history of travel to malaria
endemic areas within the last 30 days and spending at least one night.
❖ Making the diagnosis of malaria on clinical features alone is not
recommended, as this often has low specificity and increases the chances
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❖ Malaria treatment based on clinical diagnosis must be the last option when
there is no availability of RDTs or microscopy.
❖ The health worker examining a suspected malaria case should look for
other causes of fever (e.g. pneumonia, pyelonephritis, meningitis,
tonsillitis/ATP/, typhoid fever, relapsing fever, VL/visceral leishmaniasis/) and
manage the case accordingly

Laboratory diagnosis
Parasitological diagnosis is required for confirmation of the diagnosis of
malaria.
The two main methods in routine use for parasitological confirmation of
malaria are light microscopy and rapid diagnostic tests (RDTs).
For the management of a new fever episode, quality-assured microscopy
and RDTs are equivalent in terms of performance for the diagnosis of
uncomplicated malaria.
Microscopy→ Demonstration of the parasite by peripheral blood smear
o Thick and thin blood smear (100 - 200 thick field exam).
o Light microscopy using thick blood films can be very sensitive, detecting
as few as 5 parasites/µl of blood.
o Thin blood film stained with Giemsa is helpful for identifying the malaria
parasite species and has a sensitivity of 20 parasites/µl.
o RDTs have a sensitivity to detect malaria parasites above 100
parasites/µl.
o Determination of parasitemia (8000 wbc/µl assumption)

* Identification of a schizont with >12 merozoites in the peripheral circulation is an important diagnostic clue for
P. vivax. In general, schizonts of P. falciparum are very rarely seen in blood films; they are generally absent
from the peripheral circulation except in cases of severe infection with overwhelming parasitemia.
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Ab-based diagnostic stick /card test /RDT/ → if microscopy is unavailable


o Detect P. falciparum specific histidine rich protein-2 (PfHRP-2) or
lactate dehydrogenase antigen
o Remain positive for weeks after infection

Immage; Rapid malaria test; T1 Positive → Positive result for P. falciparum (P.f.), T2 Positive → Positive result
for P. vivax (P.v.) or P. malariae (P.m.) or P. ovale (P.o.) In some cases the appearance of only the T2 Line
may indicate a mixed infection with two or more of P.v., P.m., and P.o., T1 + T2 Positive → Positive result for 1125
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P. falciparum (P.f.) In some cases the appearance of both the T1 and T2 Lines may indicate a mixed infection
of P.f. with another species, No T1 or T2 Lines → Negative result (no malaria antigens were detected)

For more about rapid malaria test, click here → 26.5.3 Rapid malaria test

Treatment of uncomplicated Malaria

P. falciparum
Coartem (Artemether (120mg) - Lumefantrine (20mg)) combined
tablets 4 tabs po bid for 3 days.
AL and single dose primaquine is the recommended first-line drug

So, the usual dosage of coartem for adults is → Coartem,4 tabs, po, BID, for
3 days
To reduce the transmission of P. falciparum infection, give a single dose of
0.25 mg/kg primaquine with AL (except pregnant women, infants aged < 6
months and women breastfeeding infants aged <6 months. and testing for
G6PD deficiency is not required during primaquine treatment

P. Vivax /P. Ovalle


Chloroquine 150 mg base or chloroquine syrup 50 mg base/5ml;
✓ 1g (4 tablets) at 0 and 24 hours. It is followed by 500mg (2
tablets) at 48 hrs.
o The usual order note is Chloroquine 4,4,2
0r
✓ 1 g (4 tablets) initially, then 500mg (2tablets) in 6 hours, it is
then followed by 500mg (2ablets), PO, daily for 2 days. or
✓ 10 mg base/kg/day, PO, TID, 1st and 2nd days, and 5mg
base/kg/day, PO, TID, on 3rd day for 3 days (for a total dose of 25
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mg chloroquine base/kg with a maximum total of 1,500 mg


chloroquine base /= maximum of 2,500 mg chloroquine phosphate
salt/).
✓ A tablet of 250 mg chloroquine phosphate (“salt”) is the same as
chloroquine 150 mg base.
PLUS
primaquine 15mg po/d (0.25mg/kg /day) for 14 days for hepatic hypnozoite
clearance.
❖ N.B. Coartem (AL) may be used to treat P. vivax infection when chloroquine
is not available.

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Chloroquine treatment schedule:


Chloroquine is available as tablet (250mg, which is equal to 150mg base) or
as syrup (50mg base per 5 ml). The dose is 25 mg/kg which is given in divided doses over three days
Age Weight (Kg) Chloroquine Drug Dose
Tablet Syrup
< 4 months 5-6 ½ tab on day 1 and ¼ tab on 5 ml syrup daily on day 1 and
days 2 and 3 2, and 2.5 ml on day 3
4-11 months 7-10 ½ tab daily for 3 days 7.5 ml syrup daily for 2 days
and 5 ml for 3rd day
st
1-2 years 11-14 1 tab on 1 day and ½ tab daily 12.5 ml syrup daily for 2 days
for next two days and 7.5 ml for 3rd day
3-4 years 15-18 1 tab daily for 3 days 15 ml syrup daily for 3 days
5-7 years 19-24 1 ½ tab on day 1 & 2, and 1 25 ml syrup daily for 2 days
tab on third day and 15 ml for third day
8-11 years 25-35 2 ½ tab day 1, 2 tabs day 2, 1
tab on day 3
12-14 years 36-50 3 tabs on days 1, and 2 tabs
daily on 2nd and 3rd days
15 years + adults 51+ 4 tabs on days 1 and 2, and 2
tabs on third day
(1g at 0 and 24 hrs followed by
0.5g at 48 hrs PO)
Contraindications of Chloroquine:
➢ persons with known hypersensitivity
➢ persons with a history of epilepsy
➢ persons suffering from psoriasis

Primaquine phosphate dose:


0.25 mg base per Kg or 15mg base PO QD for 14 days for adults (administer single dose for P.falciparum or for
14 days for P.vavax)
Age Weight (Kg) Primaquine Drug Dose
7.5mg Tablet 15mg Tablet
7 months to 4 years 8-18 ½ -
5-7 years 19-24 ¾ -
8-10 years 25-35 1 ½
11-13 years 36-50 1½ ¾ or 1
14+ years 50+ 2 1 ½ or 1
Contraindications of Primaquine:
➢ Pregnancy
➢ Women breast feeding infants < 6 months of age
➢ Infants ≤ 6 months of age

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P. falciparum and P. vivax (mixed infection):


The recommended first-line treatment for mixed infection is Coartem (AL)
and primaquine radical cure for 14 days.
The second line treatment for both P. falciparum and P. vivax is
Dihydro artemisinin-piperaquine (DHA-PPQ) instead of oral quinine.
Note: do not treat a patient with confirmed mixed infection with both AL
and chloroquine.

Alternative treatment for uncomplicated malaria:


AL for 03 days and primaquine for 14 days may be used to treat
P. vivax infection when chloroquine is not available.
If all chloroquine, AL and Dihydro artemisinin - piperaquine are not
available for P. vivax infection, use oral quinine.
If AL is not available for P. falciparum or mixed malaria infections,
use oral quinine with single dose premaquine.
✓ 10 mg/kg quinine sulphate salt (= 8.3 mg base/kg), TID, for
7 days. (The maximum adult dose is 600mg quinine
sulphate (salt), PO, TID, for 7 days.)
The second line treatment for both P. falciparum and P. vivax is
Dihydro artemisinin-piperaquine (DHA-PPQ) instead of oral quinine.

Dihydroartemisinin + piperaquine (DHA-PPQ) dose


Body weight (kg) Dihydroartemisinin + piperaquine dose
(mg) given daily for 3 days
5 to < 8 20 + 160
8 to < 11 30 + 240
11 to < 17 40 + 320
17 to < 25 60 + 480
25 to < 36 80 + 640
36 to < 60 120 + 960
60 < 80 160 + 1280
>80 200 + 1600

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Quinine treatment schedule:


Quinine dose is 8.3 mg base/Kg (=10mg quinine sulphate salt/Kg) three times daily for seven days. (The max
adult dose is 600 mg TID for 7 days)

Age Weight (Kg) quinine Drug Dose


200 mg salt 300 mg salt
2 to 4 months 4-6 ¼ -
4-12 months 6-10 1/3 ¼
1-2 years 10-12 ½ 1/3
2-3 years 12-14 ¾ ½
3-4 years 14-19 ¾ ½
5-7 years 20-24 1 ¾
8-10 years 25-35 1½ 1
11-13 years 36-50 2 1½
14+ 50+ 3 2

Supportive treatment:
If patients, especially children present fever of ≥37.50 C, treat with
antipyretics and, if necessary, fanning and tepid sponging.
✓ Paracetamol (acetaminophen) 15 mg/kg every 4 hours is widely
used; it is safe and well tolerated, given orally or as a
suppository

N.B

Though the prevalence of G6PD deficiency is very low in Ethiopia,


closely follow-up patients started on primaquine for haemolysis by
informing the patient the symptoms of hemolytic anemia like weakness,
dizziness, lightheadedness, dark urine color or directly observing the
treatment, doing serial haemoglobin test and checking for darkening of
urine.
Discontinue primaquine and come back to the health facility if there is
any side effect.
If there is evidence of haemolysis, primaquine should be discontinued
and should not be given to the patient in the future.

Clinical malaria
➢ If the result of the multi-species RDT is negative for all malaria species,
malaria is unlikely. Other causes of fever should be investigated.
➢ A negative Blood Film test DOES NOT rule out malaria.
➢ Where multi-species RDT is not available, and the patient fulfills clinical
criteria of malaria, AL should be given.
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Severe Falciparum Malaria

Manifestations (Danger signs) of severe malaria


In the presence of positive BF for asexual form P. falciparum

Clinical features
Unarousable coma/cerebral malaria
o A GCS < 11 in adults or a Blantyre coma score < 3 in children
o Altered consciousness (e.g. sleepiness, confusion, drowsiness, coma)
Prostration, i.e. generalized weakness so that the patient is
unable to sit, stand or walk without assistance.
Unable to eat or drink
Repeated vomiting, resulting in inability to retain oral medication
Severe dehydration
Multiple convulsions: More than two episodes within 24 h
Haemoglobinuria (cola coloured urine)
Respiratory distress (acidotic breathing/deep breathing or in-drawing
of chest wall) → acidaemia/acidosis
Severe anaemia (normochromic, normocytic) → paleness of palms is most
reliable symptom in children
Renal failure → No urine output in the last 24 hours
Pulmonary oedema: Radiologically confirmed or oxygen saturation < 92% on
room air with a respiratory rate > 30/ min, often with chest indrawing and
crepitations on auscultation
Shock: Compensated shock is defined as capillary refill ≥ 3 s or
temperature gradient on leg (mid to proximal limb), but no hypotension.
Decompensated shock is defined as systolic blood pressure < 70 mm Hg in
children or < 80 mmHg in adults, with evidence of impaired perfusion (cool
peripheries or prolonged capillary refill).
Significant bleeding: Including recurrent or prolonged bleeding from the
nose, gums or venepuncture sites; haematemesis or melaena

Laboratory findings
Severe malarial anaemia: Haemoglobin concentration ≤ 5 g/ dL or a
haematocrit of ≤ 15% in children < 12 years of age (< 7 g/dL and < 20%,
respectively, in adults) with a parasite count > 10 000/µL
Hypoglycemia (< 40 mg/dL)
Acidosis (bicarbonate <15 mmol/L)
Hyperlactatemia (>5 mmol/L)
Hyperparasitaemia: P. falciparum parasitaemia > 2%
Renal impairment (creatinine >3mg/dl) or blood urea > 20 mmol/L 1131
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Jaundice (yellowish discoloration of the eyes): Plasma or serum bilirubin >


50 µmol/L (3 mg/dL) with a parasite count > 100 000/ µL

*Severe vivax and knowlesi malaria: defined as for falciparum malaria but with no parasite
density thresholds.

Any patient, who fulfills clinical criteria of malaria, presenting with any of the
above-mentioned danger signs, regardless of whether the RDT/BF result is
negative or positive, should be managed for severe malaria

➢ Put on Artesunate and anti-meningeal dose of ceftriaxone in our setup


➢ REMEMBER: A delay in management could cause unnecessary death of the patient.

Essential laboratory tests for severe malaria


The diagnosis of severe malaria is based on clinical features and confirmed with
laboratory testing. While confirmation of the diagnosis is necessary treatment must
be started promptly and not withheld while confirming the diagnosis

Parasitological test (microscopy), If not use RDT


RBS
CBC, if not HgB and HCT
Blood grouping and cross-matching
BUN and creatinine
Lumbar puncture to exclude meningitis or cover with appropriate antibiotics.

Factors known to influence the severity of disease in a malaria infection

➢ The species of parasite. P. falciparum causes almost all cases of severe


malaria. However, P. vivax is being increasingly recognized as a cause of
severe malaria;
➢ The immunity of the individual. Adults who have lived all their life in an
endemic area are less susceptible to severe disease than Adults who visit
an endemic area for the first time
➢ Young children living in the same endemic area
➢ Pregnancy
➢ The availability and efficacy of antimalarial medicines;
➢ The degree of parasite drug-resistance that prevails locally;
➢ HIV/AIDS, especially in pregnant women and those with advanced immune
deficiency;
➢ Some genetically inherited conditions in the human host, e.g. sickle-cell
trait, s-thalassemia, and probably G6PD deficiency have a protective effect;

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Differential diagnosis of severe malaria


Decreased Level of Consciousness

•Viral encephalitis
• Bacterial meningoencephalitis
• Cerebral typhoid
• Cerebro-vascular event (stroke)
• Complicated typhus, relapsing fever
• Febrile illness with hypoglycaemia
• Sepsis
• Convulsion in a patient with fever

Renal failure

• Glomerulonephritis (AGN)
• Acute tubular necrosis (ATN) due to hypovolemia or hypotension

Jaundice associated with fever

• Viral hepatitis
• Yellow fever
• Acute cholecystitis
• Choledocholithiasis

Treatment of severe malaria


If clinical features strongly suggest severe P. falciparum malaria, treatment maybe
started even though results are negative (Note: This should be a VERY rare
circumstance).

Admit the patient


Position semi-prone or on side
Make rapid clinical assessment and Maintain ABC of life
Exclude or treat hypoglycemia (more so in pregnant women)
Insert NG tube for feeding and medication and urinary catheter/glove
catheter for UOP determination
Ensure nutrition and nursing care
Take blood while establishing an IV line for IX
If fever exceeds 39°C, remove patient's clothes, use tepid sponge,
Consider other infections and broad-spectrum antibiotics.
Consider need for anti-convulsant treatment
Consider the need for blood transfusion. The most common indication for blood
transfusion is severe anemia (Hb < 5g/dl).
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Consider antibiotics if there is a suspicion of concomitant bacterial infections.


o Patients diagnosed with concomitant infections like pneumonia, UTI,
meningitis
o Patients suspected to have infections (shock which is not responding
to fluid management, metabolic acidosis with hypotension especially if
not responding to fluid management, comatous patients when CSF
analysis is not possible)

Pharmacologic mgt

Treatment for severe malaria is either:

First line

➢ Artesunate, IV or IM

Alternative

➢ Artemether, IM

If artesunate or artemether are not available

➢ Quinine infusion, IV or
➢ Quinine, IM

1. Artesunate

Artesunate, 2.4 mg/kg (for Children weighing < 20 kg, 3 mg/kg/dose) IV


or IM given on admission (time = 0), then at 12 h and 24 h, then once
a day for 5 days or until the patient tolerates PO medication.
o Dosage regimen: Give 3 parenteral doses of injection artesunate in
the first 24 hours
o First dose on admission (time zero),
o Second dose 12 hours after the first dose and
o Third dose at 24 hours after the first dose.
o Thereafter every 24 hours until patient is able to tolerate oral
medication to complete the treatment with in three days
o Once a patient has received at least 24h of parenteral therapy and
can tolerate oral therapy, complete treatment with full (3days) course
of second line drug (Dihydro artemisinin piperaquine (DHA-PPQ)
▪ If DHA-PPQ not available, artemether + lumefantrine (AL), for
03 days.
o If AL is contraindicated, continue treatment with quinine tablets.
o Artesunate can be continued for 5 to 7 days
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Alternative

2. Artemether
Artemether is the alternative parenteral treatment when parenteral artusnate is
not available for severe malaria.
Dosage for Adults and children → 3.2 mg/kg/day, IM, daily on 1st day, then
1.6 mg/kg/day on 2nd and 3rd day
Administration: IM (NEVER ADMINISTER BY IV ROUTE)
Note: anterior thigh is preferred site for providing IM injection Frequency of
administration
once daily Duration of treatment
o It can be provided up to a total of 3 days.
o It can be discontinued if the patient tolerates oral treatment after 48
hours (two doses) Then, will be followed by full dose AL
A full course of oral AL therapy should be started to complete the treatment,
Additionally, a single-dose primaquine will be added for P. falciparum cases.
A 14-day primaquine should be given for P. vivax cases

3. quinine Infusion
If Artesunate and artemether both are not available, give quinine
Infusion
✓ Start IV quinine 20mg/kg in 500ml D5 or NS to run over 4 hrs
loading then Maintenance dose should be given 12 hours after the
start of the loading dose at a dose of 10 mg/Kg in 500ml D5 or NS
to run over 4hrs, TID, for at least 48hrs
✓  dosage by 1/3rd to half, if required to treat with IV quinine after
48 hours (6 doses including the loading dose). It is unusual to
continue IV infusions of quinine for more than 4-5 days;
✓ Rapid administration of quinine is not safe and may cause sudden
death due to arrhythmia or refractory hypotension. The infusion
rate should not exceed 5 mg salt/kg/hr
✓ If for any reason quinine cannot be administered by IV infusion,
quinine dihydrochloride can be given in the same dosages by IM
injection in the anterior thigh (not in the buttock). The dose of
quinine should be divided between two sites – half the dose in
each anterior thigh. If possible, for IM use, quinine should be
diluted in normal saline to a concentration of 60 - 100mg salt/ml;
✓ A loading dose of quinine should not be used if (i) the patient
received quinine within the preceding 24 hours; (ii) mefloquine
within the preceding 24 hours; or (iii) mefloquine within the
preceding seven days;
✓ Quinine is not given by subcutaneous injection;
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✓ Quinine is safe in pregnancy and in anaemic patients, if the


doses are carefully calculated by body weight.
✓ The parenteral treatment should be changed to P.O. only after 24 hours
and as soon as the patient’s condition improves and if there is no
vomiting.
✓ Oral treatment should be given with Artemether + Lumefantrine.
However, if a patient has a history of intake of Artemether +
Lumefantrine before complications developed, give Quinine tablets 10
mg salt/kg TID to complete 7 days treatment.
❖ Re-check malaria blood smear by microscopy after 48 hours to assess
effects of anti-malarial treatment on blood parasite density;

1.1 Cerebral Malaria


In repeated malarial attack if the last attack is ≥ 10 years, no risk of
cerebral malaria (i.e. for cerebral malaria, the last attack should be <
10 years)

Clinical features

Have nuchal rigidity, fever and headache


Cmn in endemic area
LOC for > 30 minutes
✓ Repeated seizure without gaining consciousness
✓ Cerebral malaria is unlikely in fully awake patients

Management

Ensure ABC of life, coma care, feeding, bladder and bowel care,
detection and treatment of other complications like aspiration
Start artesunate immediately
Broad spectrum antibiotic to cover other DDX like meningitis (if possible
do LP before initiating antibiotic)

1.2 Hypoglycemia
Give 50% dextrose (0.5gm/Kg) followed by infusion of 10% dextrose (0.1
gm/kg/hr)
Correct hypoglycaemia (< 40 mg/dl) if present by infusing dextrose over a
period of 3-5 minutes. This can consist of any one of the following:
✓ 1 ml/kg of 50% dextrose diluted with an equal volume of NS (1ml/kg) IV
slowly over several minutes OR
✓ 5 ml/kg of 10% dextrose by slow IV infusion OR
✓ For other strengths of dextrose, calculate accordingly.
This should be followed by intravenous infusion of 10% dextrose) given slowly;
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Re-check blood glucose every 2-4 hours during the course of treatment,
particularly in the pregnant or comatose patient because hypoglycemia can
recur even after an IV bolus of glucose.

1.3 Seizure
Do RBS to R/O hypoglycaemia, if there correct as mentioned above
Diazepam 0.15 mg/kg maximum 10mg IV stat then phenytoin 20mg/kg followed
by 5 mg/kg/day
The IV diazepam can also be given intra-rectally using a rectal tube or NG
tube (0.5-1.0 mg/kg) if injection is not possible.
Diazepam can cause respiratory depression. Therefore, an Ambu bag and
resuscitation equipment should be at hand when used.

1.4 Severe Anaemia


➢ Anemia associated with malaria is partly due to the destruction of red cells
that contain parasites (hemolysis). Several other mechanisms may accelerate
the development of anemia:
➢ non-parasitized red cells are destroyed more quickly than normal cells during
malarial illness, and the bone marrow does not function adequately.
➢ Anemia is worsened if there is abnormal bleeding, intravascular hemolysis or
renal failure

Note:

❖ Co-infection with other parasitic diseases (e.g. Schistosomiasis, Visceral


Leishmaniasis, soil transmitted helminths) may further increase anemia.
❖ Only about 1/3rd of patients with mild anemia show pallor and patients may
have moderate anemia without showing pallor. To confirm that anemia is
present, Hb levels should be measured.
❖ Patients with severe anemia may present with palpitation, dyspnoea or
tachypnoea. Severe or rapidly developing anemia may contribute to both
cerebral signs (e.g. confusion, restlessness, coma /altered consciousness and
retinal hemorrhages) and cardiac failure.

Management

The most common indication for blood transfusion is severe anaemia.


Assess the patient’s clinical condition rather than relying on the haematocrit
and/or Hb level.
As a rule of thumb: Indication for transfusion
➢ If the haematocrit is <15%
➢ Anomia-associated acidosis, shock or the parasitaemia is so high that
you can predict a critical drop
➢ Spontaneous bleeding 1137
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1.5 Acute pulmonary oedema and ARDS


Pulmonary edema is a grave complication of severe malaria and has a high
mortality rate. It may appear several days after chemotherapy has been started
and at a time when the patient’s general condition is improving and peripheral
parasitemia is diminishing.
It must be differentiated from iatrogenically produced pulmonary edema
resulting from fluid overload (caused by poor management of the intravenous
infusion).
ARDS appears to be due to the direct effect of parasites sequestered in the
lungs, possibly through release of cytokines. It is indistinguishable for
pulmonary
edema but both of these complications are unusual in children.

Clinical presentation:
Hyperventilation (rapid breathing) is the initial manifestation
Crackles are present on auscultation, and pink frothy sputum (severe
cases).

Management

Semi-erect positioning
Intra nasal O2
Fluid restriction and
Diuretics for overhydration, e.g. furosemide 40 mg IV. If no response increase
dose progressively to maximum 6mg/kg/day
Intubation and mechanical ventilation including positive end expiratory pressure
(PEEP), perform regular suction (via endo tracheal tube or oral/ naso
pharangeal airway) for ARDS

1.6 Algid malaria


Severe malaria complicated by circulatory shock is known as algid
malaria. Which is characterized by hemodynamic disorders as shock with
pronounced metabolic changes and hypothermia.
Algid is a rare complication (0.37% of cases).

Management
large-volume fluid resuscitation and hemodynamic optimization
o The optimal resuscitation strategy for algid malaria is unknown,
and volume restriction has been advocated as a means to
prevent life-threatening cerebral and pulmonary oedema.
Early antimalarial agents and
broad-spectrum antibiotics. 1138
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1.7 Acute renal failure


Acute renal failure – acute tubular necrosis – is a common complication in
adults, but is rarely seen in children.
It is worsened by hypovolemia and hypotension.
It is highly preventable if fluid balance and BP is maintained. If a patient has
oliguria, first correct fluid deficit and try to correct BP
However, if there is persistent oliguria (<17 ml/hour in adults: 0.3 ml/kg/hour in
children) despite adequate correction of dehydration or hypotension, renal
failure is present or imminent. Hiccup may be an indicator of advanced renal
failure.

Management

Correct rehydration
decrease IV quinine dose by 30-50 % after 2 days of Rx
Avoid nephrotoxic drugs
Follow input-output and serum cr
Haemodialysis when cr > 3mg/dl

1.8 Hemoglobinuria:
➢ Hemoglobinuria results from the rapid breakdown of red blood cells
(massive
intravascular hemolysis) in the circulation.

Clinical presentation:
➢ The urine is dark, and tests strongly positive for blood (Hb) but contains no
red
cells on microscopy.
➢ The plasma may also be dark because of the hemoglobin released from
the red
cells.

Management:
➢ Maintain hematocrit above 15%
➢ monitor JVP to avoid fluid overload and hypovolaemia
➢ If oliguria develops and BUN & cr levels rise, consider peritoneal dialysis or
hemodialysis
➢ continue anti-malarial therapy.

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1.9 Jaundice:
Jaundice is more common in adults than in children and is due partly to
hemolysis and partly to liver dysfunction.

Clinical presentation:
Yellowish discoloration of the sclerae of the eyes or the frenulum of the
tongue is quite commonly seen in severe P. falciparum malaria in adults,
but is uncommon in children.
Signs of hepatic failure are rare.
Jaundice in malaria occurs at the same time as fever, unlike jaundice due
to hepatitis.
If jaundice is present, look for other complications.

1.10 Bleeding tendency:

❖ In P. falciparum malaria, the platelet count is typically reduced.


Nevertheless,
spontaneous bleeding is rare in both children and adults. When it develops,
it results from DIC.

Management:
❖ Check bleeding time of the patient, crossmatch blood, give whole fresh
blood or
platelet infusion as needed to correct blood loss and bleeding.

Treatments contra-indicated in the patient with severe


malaria

The following treatment should not be administered to patients with severe


malaria:

✓ Corticosteroids and NSAID (ibuprofen, aspirin);


✓ Other agents given for cerebral edema (urea, mannitol);
✓ Low molecular weight dextran;
✓ Epinephrine (adrenaline);
✓ Heparin;
✓ Epoprostenol (prostacyclin);
✓ Pentoxifylline (oxpentifylline);
✓ Hyperbaric oxygen;
✓ Cyclosporine (cyclosporin A.).

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Chronic Complications of Malaria

1. Hyper reactive malarial splenomegaly (HMS)

Pathogenesis
Abnormal immune response to repeated malarial infection
RES hyperplasia and  clearance

Presentation
Massive splenomegaly + peri splenitis
Hepatomegaly
Anaemia (NCNC) + pancytopenia
Prone to skin + respiratory infection, sepsis
 Serum titre of IgM and malarial Antibodies
Hepatic sinusoidal lymphocytosis
Peripheral B-Cell lymphocytosis
Hypergammaglobulinemia
At risk of malignant lymphoproliferative disorder

Major criteria include


Gross splenomegaly (≥ 10 cm) below the costal margin in adults for which
no other cause can be found
Elevated serum IgM level ≥ 2 standard deviations above the local mean
Clinical and immunologic responses to antimalarial therapy
Regression of splenomegaly by 40% by 6 months after start of therapy
High antibody levels of Plasmodium species (≥1:800)

Minor criteria include the following:


Hepatic sinusoidal lymphocytosis
Normal cellular and humoral responses to antigenic challenge, including
a normal Phyto hemagglutination response
Hypersplenism
Lymphocytic proliferation
Familial occurrence

Treatment
Chloroquine 500mg (2tab), PO, weekly for 6 months.
o Weekly and daily dosing’s are said to be equally effective
o Follow up every 3 months (with CBC and spleen size…
abdominal U/S) 1141
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2. Quartan Malarial nephropathy

Repeated P. malariae infection → soluble immune complex deposition


in glomerular BM → Nephrotic syndrome (FSGS)
Treatment: Poorly responsive to antimalarial or steroid + cytotoxic drugs

3. Burkitt’s lymphoma + EBV infection


High prevalence in malarious areas of Africa
Malaria induced immuno suppression may provoke EBV infection

Prevention of Malaria
Early detection and prompt treatment of cases
Personal protection measures: Using permethrin impregnated bed nets
/Mosquito repellents
Chemoprophylaxis: 1wk before departure and for 4 wks after leaving
the endemic area. Drug options:
✓ Mefloquine 228mg of base (250mg of salt) or 5 mg/kg po/week
✓ Doxycycline 100mg once a day
✓ Chloroquine 300mg of base orally, once\wk
✓ Proguanil 200mg orally, once \day, in combination with weekly
chloroquine

Special population considerations

Pregnancy
Maternal effect

High level parasitaemia


in low-transmission areas, the risk of development of severe malaria
is high.
Common complications: Anaemia, hypoglycaemia and acute
pulmonary
oedema

Fetal effects

Fetal distress, Premature labor, Still birth, LBW


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Congenital malaria in new born

Treatment of Malaria in Pregnancy


➢ Pregnant women living in areas of low or unstable malaria transmission (like
many malarious areas in Ethiopia) have little or no immunity to malaria, and
are at higher risk of developing severe malaria than are non-pregnant adults
living in the same area.
➢ In these areas, malaria is a major cause of maternal anaemia, spontaneous
abortion, stillbirth, premature delivery, low birth weight (birth weight < 2.5kg),
neonatal death and maternal death. In non-immune women, severe malaria
symptoms (hypoglycaemia, cerebral malaria, and pulmonary oedema being
particular problems) are more common in pregnancy.
➢ In stable transmission settings, the deleterious impact of malaria is particularly
apparent in first and second pregnancies.

Treatment of uncomplicated malaria in pregnancy

➢ There is insufficient information on the safety and efficacy of most antimalarial


medicines in pregnancy, particularly for exposure in the first trimester, and
treatment recommendations differ from those for non-pregnant adults.
➢ In all trimesters, give Artemether-lumefantrine (AL) For the treatment of
Falciparum malaria in pregnancy
➢ Chloroquine, which is the treatment of choice for P. vivax (chloroquine-
sensitive), P. ovale and P. malaria, is safe in pregnancy.
➢ Primaquine is contraindicated during pregnancy and up to 6 month of delivery
(breast feeding)
➢ Provide weekly chloroquine prophylaxis until after delivery and breastfeeding for
6 months

Treatment of severe malaria in pregnancy

➢ A pregnant woman with severe malaria should be given a parenteral


antimalarial medicine in full doses without delay.
➢ Parenteral artesunate is more effective than parenteral quinine in reducing the
risk of death from severe malaria.
➢ Although safety data on the use of artemisinins in the first trimester are
limited, saving the mother’s life is the primary objective.
➢ Therefore artesunate (IV or IM) is the preferred drug for all severe forms of
malaria in all trimesters of pregnancy.
➢ IM Artemether is the second option while Quinine (IV or IM) may be
considered as the last option.
➢ After 24 hours of parenteral drug administration, treatment should be completed
with full dose of AL including the first trimester
➢ The amount of antimalarial drugs passed into breast milk and consumed by
the breast feeding infant is very small, so the treatment is the same as the
non-pregnant adults except primaquine should be avoided. 1143
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➢ Intermittent preventive treatment (IPTp) with SP is not recommended in


Ethiopia.

Paediatrics
➢ AL is currently recommended for the treatment of uncomplicated malaria
in infants under 5 kg as the same dose as 5 kg
➢ Chloroquine is a safe drug that can be used in all children with only P. vivax
infection
➢ Available drugs for infants and children
✓ Chloroquine syrup and tablets for children syrup → see from
uncomplicated malaria management above
✓ Coartem tablets based on Kg → see from uncomplicated
malaria management above
✓ Artemether syrup
Age Dosage (PO, BID, for 3 days)
1 - 6 months 5 ml
7months - 3yr 10 ml
4 - 8 yr 15 ml
9 - 12 yr 20 ml

✓ Cotexin syrup /dihydro artemisinin/, 160mg/80ml, 4 mg/kg/day,


PO, BID for 4 days or 4 mg/kg/day, PO, BID in the 1st day
followed by 2 mg/kg/day PO, BID for the next 6 days (used for
all malaria subtypes) or you can use the following table for
dihydro artemisinin syrup
Weight in Day1 (ml, PO, BID) Day 2 to day 7
kg (ml, PO, BID)
< 5 5 2.5
5 – 10 10 5
10 – 15 15 7.5
16 – 20 20 10
> 20 Tablet is recommended

For severe malaria in children

➢ Artesunate 2.4 mg/kg/dose (for Children weighing > 20 kg); or 3


mg/kg/dose (for Children weighing < 20 kg), IV or IM given on
admission (time = 0), then at 12 h and 24 h, then once a day for 5
days or until the patient tolerates PO medication. If the patient
tolerates after 24 h, the medication can be changed to PO AL for
the next 3 days. 1144
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➢ under six years of age, treat with a single dose of rectal artesunate
(10mg/Kg) and immediately go to appropriate further care. Do not use
rectal artesunate in older children and adults.

☛ For More Refer Updated National paediatric malarial infection guideline

Antimalarial drugs (Dose and special considerations)

A. Coartem (AL)

Contraindications:

✓ Persons with a previous history of reaction after using the drug;


✓ Persons with severe and complicated malaria should not be treated with
oral medications.

B. ORAL QUININE TREATMENT SCHEDULE


Oral quinine dosage is 8.3 mg base/kg (=10 mg quinine sulphate salt/kg),
TID, for 7 days. (The maximum adult dose is 600mg quinine sulphate
(salt), TID, for 7 days.)

C. Artesunate Injection for severe malaria

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D. Artemether injection
Artemether injection is given at a loading dose of 3.2 mg/kg on the first
day followed by 1.6 mg/kg daily for two days. Then if the condition of the
patient improves, will be followed by full dose AL
Administration: IM (NEVER ADMINISTER BY IV ROUTE)
Injectable artemether contains 80 mg in 1 ml ampoule (80 mg/ml), oily
solution for IM injection only.
When the dose required is less than 1 ml, use a 1 ml syringe graduated in
0.01 ml.
Note: anterior thigh is preferred site for providing IM injection Frequency of
administration

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11.2. Typhoid fever (ታይፎይድ)

Salmonellosis
❖ Caused by the genus Salmonella → Non spore-forming gram -ve
bacilli
❖ Enteric fever
o Clinically the most important form
o Caused by:
Salmonella enterica serotype Typhi (formerly S. typhi) –
Causes typhoid fever
Salmonella enterica serotypes Paratyphi A, B and C
(formerly S. paratyphi A, B and C) – Cause paratyphoid
fever

Typhoid fever
Typhoid fever is an acute febrile illness caused mainly by Salmonella
typhi. The mode of transmission is via contaminated food or water.
Clinically the term includes the milder paratyphoid fever
Common in countries with poor access to sanitation

Pathogenesis:

Ingestion of contaminated food or drink → penetration of gut mucosa


→ infection of lymphoid tissues → lymphatic/hematogenous
dissemination and colonization of RES → infection of body parts/ re-
infection of intestine

Clinical presentation

✓ IP: 3 to 21 days
Fever and abdominal pain
Diarrhoea (children, HIV infected, malnourished patients) or
constipation (adults)
Skin rashes (rose spots)
Hepatosplenomegaly
Delirium, coma

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Rose spots are small (1 to 5 mm), erythematous, blanchable, nontender papules, which begin early during the
acute febrile period of typhoid fever. Crops of lesions (10 to 20) appear at irregular intervals for approximately 10
to 14 days, typically distributed on the abdomen, chest, and back. Rarely, vesicular or hemorrhagic lesions
appear. The lesions persist for two to three days.

Clinical features based on onset of illness


➢ 1st week
o Stepp ladder fever, chills and rigor
o Malaise
o Headache
o Joint pain
➢ 2 week
nd

o Abdominal pain
o Diarrhoea or constipation
o Skin rashes (rose spots)
➢ 3 week
rd

o Hepatosplenomegaly
o GI bleeding
o Intestinal perforation (severe abdominal pain)

N.B these features are not always present. But fever is always there the
name so called typhoid fever

Complications

Intestinal perforation/ bleeding


Hepatic/ splenic abscesses
Meningoencephalitis, nephritis, arthritis, osteomyelitis

❖ Relapse rate after Rx is 10%


❖ Chronic carriers: asymptomatic individuals who shed the organisms
(in
urine or stool) for more than 1 year
✓ Mainly: women, patients with biliary stones or tumors, GI
malignancy
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Diagnosis

❖ Diagnostic gold standard: Mnemonic → culture from BUS (Blood, BM,


urine or stool)
samples
Blood culture ---best in the 1st week (90% Sensitivity); less so
in the 3rd week (50% Sensitivity)
BM culture – especially in those who took antibiotics for < 5
days
Stool and urine cultures – best in the 3rd week in untreated
patients
❖ Serological examination, such as the Widal test may be used as an
adjunt to diagnosis in the proper clinical setup particularly in children
< 10 years old and travellers from nonendemic areas. The Widal test
is, however, characterized by false positive results. But we are using
it currently in our set up
✓ The Widal test detects anti-S. Typhi antibodies, and the minimal
titers defined as positive for the O (surface polysaccharide)
antigens for active infection and H (flagellar) antigens in past
infection or in immunized person.

Limitation of widal test


False positive reactions
▪ Due to past infection
▪ Cross reaction (malaria, relapsing fever, non-typhoidal
salmonella)

False negative reaction

▪ Early typhoid cases


▪ Poor antigen preparation
▪ Poor transport of reagents &storage.

Widal test; rapid slide test

o For more about widal test click here → 26.5.4 widal test
❖ CBC
✓ Patients with enteric fever frequently have anemia and either
leukopenia or leukocytosis 1149
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✓ leukopenia with left shift is typically seen in adults, while


leukocytosis is more common in children.
✓ leucocytosis in the 3rd week of illness, should prompt suspicion of
intestinal perforation.
❖ Deranged OFTs

Management
Symptomatic treatment:
Use of antipyretics, e.g. paracetamol to control fever.

Uncomplicated Typhoid fever


First line

✓ Ciprofloxacin, 500mg P.O., BID for 7 to 10 days

Alternative

✓ Azithromycin,1g, PO, daily for 5 to 7 days


✓ Cefixime, 400mg, PO, daily for 7 to 14 days

N.B local studies in Ambo and Mekelle, showed that 50-100% of


isolates were resistance to previously recommended antibiotics like
amoxicillin, cotrimoxazole, erythromycin, Nitrofurantoin, streptomycin and
doxycycline, and 20% for chloramphenicol.
☛ Thus, the main options are fluoroquinolones, 3rd generation
cephalosporins, and azithromycin.

Complicated/ severe Typhoid fever


For patients who have severe disease (e.g. systemic toxicity, depressed
consciousness, prolonged fever, organ system dysfunction, or other
feature that prompts hospitalization) and complication, initial therapy with
a parenteral agent is appropriate.

First line

✓ Ceftriaxone 1g, IV/IM, daily or in 2 divided doses, for 10 - 14


days

Alternative
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✓ Only if no alternative: IV Ciprofloxacin: 20 mg/kg/day BID (maximum 800


mg/day) then, Oral: 30 mg/kg/day, BID (maximum 1000 mg per day)
✓ Cefotaxime, 1 - 2 g, IV, TID, for 10 - 14 days

Adjunct Corticosteroid treatment:


This is recommended only for patients with evidences of CNS
involvement (delirium, obtundation, stupor, coma) or shock

First line

✓ Dexamethasone, 3mg/kg IV initially, followed by 1mg/kg IV QID,


for 48hrs total (This is preferred in patients with severe disease)

Alternative

✓ Prednisolone, 20-40mg P.O., (or equivalent) once daily for the first
3 days of antibiotic treatment.

Special population considerations

Paediatrics:

▪ fluoroquinolone use is not justified in paediatrics <18 years old due


to arthropathy and cartilage toxicity in immature animal studies.
☛ Hence only recommended for sever enteric fever if and only if
there are no other alternatives (use Ciprofloxacin 15mg /kg
/dose, BID, for 7-10 days).

First line (3rd Generation Cephalosporin)

✓ Cefixime, 15 to 20 mg/kg/day (max; 400 mg/day), PO, BID, for 7


to 14 days; (available syrups 100mg/5ml, 200mg/5ml, 500mg/5ml) OR
✓ Ceftriaxone, 80 mg/kg/day, IV, daily for 7 to 14 days OR
✓ Cefotaxime, 150 - 200 mg/kg/day in 3 to 4 divided doses (max:
12 g daily), IM/IV, for 7days
o For fluoroquinolone resistant: 80 mg/kg/day in 3 to 4 divided
doses (max: 12 g daily)

Alternatives (not effective)

✓ ??? Azithromycin (syrup 200mg/5ml), 20 mg/kg/day, PO, daily for 5 to 7


days
✓ ??? Cefaclor, 20 to 40 mg/kg/day, BID or TID, for 7 days
✓ ??? Cephalexin (syrup 125mg/5ml, 250mg/5ml), 50mg/Kg/day, BID for 7days
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Pregnant women:

▪ Fluoroquinolone are contraindicated in pregnant mothers.


▪ Third generation cephalosporins should be used in pregnant mothers
in place of fluoroquinolone or azithromycin.

First line

✓ Ceftriaxone 1g, IV/IM, daily or in 2 divided doses, for 7


days

Alternative

✓ Cefotaxime, 1g, IV, TID, for 7 days

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11.3. Typhus (ታይፈስ)

Typhus is a disease Caused by Rickettsiae


Commonly there are two types of epidemiologically distinct typhus.

Epidemic typhus Endemic typhus


Another name louse-borne typhus flea-borne typhus
Caused by R.prowazekii R.typhi
Transmitted by body louse Tick
Vectors Pediculus humanus corporis Fleas
Reservoirs --- Rats

Other strains of rickettisia are also present in Ethiopia.

1. Epidemic Typhus

Epidemiology:

Currently prevalent in mountainous areas of Africa, South America


and
Asia
Persist and common in the rugged, mountainous areas of Ethiopia
Particularly high during the rainy seasons from July to September
and December.
It is related to poverty, war and disasters and common among a
crowded, cold, and unhygienic environments (e.g. rural communities,
day laborers, and homeless people). Hence, typhus is probably
common across the country.
Lice acquire the organism when they ingest a blood meal from a
rickettsemic patient

Transmission

Rickettsiae multiply in the mid-gut of lice


Infected lice defecate during blood meal, and the patient auto
inoculates the organisms by scratching

❖ Brill-Zinser disease is a recrudescent, mild form of epidemic typhus


occurring years after the acute disease, probably as a result of
immunosuppression or old age
❖ Potential agent of bioterrorism
• high case fatality rate
• difficult to diagnose 1153
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• inhalation of aerosols is highly infectious

2. Endemic Typhus

Transmission:

✓ Fleas acquire R. typhi from rickettsemic rats and humans are infected
when rickettsia-laden flea feces are “scratched” into pruritic bite
lesions
and infrequently by direct flea bite
✓ Inhalation of aerosolized flea feces can transmit the infection

Clinical Manifestations of typhus


The clinical presentation of both types is similar and cause an AFI
characterized by:

✓ IP: 1 to 2 weeks
✓ Prodromal symptoms: headache, myalgia, arthralgia, nausea and
malaise
Followed by abrupt onset of fever (>38°C), chills,
maculopapular rash
Rash
▪ Usually starts on the 5th day
▪ Macular, maculopapular, petechial
▪ Initially on the trunk -> then becomes generalized
▪ Spares face, palms and soles
✓ Pulmonary involvement is frequently prominent
o Dry cough, bibasilar rales
o CXR: interstitial pneumonia, pulmonary edema, pleural effusion
Tachycardia
Hypotension
Less commonly: abdominal pain, Eye pain, confusion, stupor,
seizures, ataxia,
coma, photophobia, jaundice, conjunctival injection, Splenomegaly

CXN of typhus
➢ Vasculitis resulting in gangrene and cerebral thrombosis is among the
more serious complications of typhus.
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➢ Skin necrosis and gangrene of the digits


✓ Respiratory failure
✓ Hematemesis
✓ Cerebral hemorrhage
✓ Greater severity is associated with old age, underlying disease and
treatment with sulfa drugs
✓ Case fatality rate in untreated patients: 1%, may reach up to 40%

Diagnosis of typhus
The Weil Felix serology test with demonstration of a rising/high titer.
o For more about Weil Felix serology test click here → 26.5.5
Weil-Felix slide agglutination test
IFA (Micro immunofluorescent) and plate microagglutination tests have
high sensitivities for typhus
Immunohistology of skin biopsy
PCR

Treatment of typhus

Non pharmacologic

✓ Delousing:
➢ Regularly washing clothes and body plus long-acting insecticides
should be used.
➢ Pyrethroid permethrin is the delousing agent of choice. It can be
applied as a dust or spray to clothing or bedding.

Pharmacologic

☛ Identification of the etiology is highly challenging. Hence, empiric therapy


for this AFI should carefully consider the patient clinical presentation, the
local typhus epidemiology, and the population group seeking care (e.g.
homeless, poor hygienic ore recent travels to rural areas where louse
born case are dominant).

First line

✓ Doxycycline, 100mg, PO, BID (200mg, P.O., daily) for 7-10 days OR
✓ Tetracycline, 250mg, PO, QID for 7-10 days 1155
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Alternatives

✓ Chloramphenicol, 500mg P.O., QID for 7 days


▪ for children: 25mg/kg
▪ used in
o Patients allergic to Tetracyclines
o Pregnant women, and
o Children < 8 years of age who require prolonged or repeated
courses of therapy
o Reduced renal function

Prevention

➢ Delousing:
➢ Antibiotic prophylaxis:
▪ Doxycycline 200mg PO stat.
▪ For travelers to endemic areas a weekly single dose for the
duration of stays and continued for one week after leaving the
area can be used.
➢ Environmental control: Areas where flying squirrels are common like
in campgrounds, roof joists, etc. should be sealed with metal
screening to prevent squirrels from nesting in inside homes or around
human residency areas.
➢ No specific vaccine is on use currently.

Special population considerations

Pediatrics:

✓ Tetracyclines should not be used in children less than 8 years.


✓ CDC recommends “doxycycline as first line choice for children of all
ages with suspected tickborne rickettsial disease.
✓ In premature and full-term neonates CAF will result in “gray baby
syndrome" characterized by cyanosis, abdominal distention, vasomotor
collapse, and death due to poor metabolism potential of the infants.

Pregnant women:

✓ Chloramphenicol, 500mg P.O., QID for 7 days

Caution! Tetracyclines should not be used in pregnant mothers (it is CAT X


drug).

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11.4. Relapsing fever

❖ An acute febrile illness caused by spirochetes of the genus Borrelia


❖ Episodes of fever that accompany spirochetemia
❖ Arthropod-borne infection with two forms:
Tick-borne relapsing fever (TBRF)
• Caused by B. hermsii, B. turicatae (New World species) or
B. duttonii (Old World species)
• Sporadic cases or small outbreaks
Louse-borne relapsing fever (LBRF)
• Caused by B. recurrentis
• Mainly in developing countries
• In Ethiopia the endemic form is a louse-borne disease
(LBRF)
• Typically occurs in an epidemic form
❖ Borrelia are:
o Spirochetes morphologically different from gram positive and
gram negative organisms
❖ Other spirochetal diseases
o Syphilis
o Leptospirosis
o Lyme disease

Tick borne relapsing fever (TBRF)

➢ Less common in the tropics


➢ Soft ticks (Ornithodoros spp.) transmit the infection via saliva or
excretory fluid when feeding

Louse borne relapsing fever (LBRF)

➢ Common in the highlands of Ethiopia


➢ Human lice transmit the disease
➢ Outbreaks during cold seasons
➢ Also seen: during wars, famine; among refugees and homeless
people
➢ Infected lice contain organism in their hemolymph -> infect
humans when lice are crushed and fluid contaminates mucous
membranes or skin abrasions

❖ After infection spirochetes enter the blood and are spread to different
sites: liver, spleen, CNS, bone marrow, etc.
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❖ Severity of illness depends on the density of spirochetes in the blood

Clinical manifestations

❖ LBRF and TBRF are similar in their manifestations


❖ IP: 3 to 12 days
❖ High grade recurrent fever is the typical feature
❖ Others:
▪ nausea, vomiting, chills, rigors, sweating, headache, arthralgia,
myalgia
❖ Neurologic manifestations:
▪ delirium, stupor, coma, focal neurologic deficit
❖ Cardiopulmonary:
▪ myocarditis, cough, respiratory distress
❖ Hematologic: bleeding

Physical examination:

❖ hepatosplenomegaly, cranial nerve palsies, petechiae, etc.

Diagnosis

Relapsing fever should be considered if two of the following criteria fulfilled

i. The presence of relapsing fevers, especially if the recurrent fevers


are accompanied by the crisis phenomenon (rigors, further elevation
of temperature, pulse and blood pressure before fever ends, for 15-
30 minutes).
ii. History of exposure to, body lice in areas where louse-borne
relapsing fever (LBRF) or cattle ticks in localities where tick-borne
relapsing fever (TBRF) is common.

Confirm suspicion by:


▪ Blood film -> Giemsa or Wright stain -> look for
extracellular Borrelia
▪ PCR: done when BF is negative
CSF analysis → If neurologic involvement suspected (meningitis or
meningoencephalitis)
In complicated cases: CBC, Liver function tests, ECG
Culture and serology mostly not applicable

Management

Non pharmacologic

❖ Delousing
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Pharmacologic

First line

✓ Procaine penicillin, 400,000-600,000-unit I.M. stat.


▪ For children: 200,000-400,000 units.
Check blood film after 12 hours of treatment.
➢ If negative → give tetracycline 250 mg TID for 3 consecutive
days.
➢ If the blood film remains positive → repeat the same dose of
procaine penicillin and continue with tetracycline later as
described above.

Alternative

✓ Tetracycline hydrochloride, 250 - 500mg P.O. daily for 2 days. OR


✓ Erythromycin, 500mg P.O., stat. OR
✓ Doxycycline 100 - 200mg mg, P.O stat

Prevention

Reducing louse and tick exposure:


Good personal hygiene, reduced crowding, access to fresh water
and washing facilities.
Post exposure antibiotic prophylaxis:
➢ doxycycline 200mg on the first day, then 100 mg/day for 4
days (1st line).
➢ Tetracycline 500 mg QID for 4 days (alternative).
No effective vaccine for relapsing fever.

Special population considerations

Pediatrics:

✓ Tetracyclines are contraindicated in children less than 8 years.


✓ In premature and full-term neonates CAF will result in “gray baby
syndrome" characterized by cyanosis, abdominal distention, vasomotor
collapse, and death due to poor metabolism potential of the infants.
Hence, penicillin, macrolides and cephalosporins can be used.
Pregnant women:

✓ Tetracyclines should not be used in pregnant mothers.


✓ Penicillin, macrolides and cephalosporins can be used in pregnant
and nursing mothers. 1159
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N.B.
1. Jarish-Herxheimer reaction:

❖ Some patients may develop Jarisch-Herxheimer


reaction and is believed to be due to a rapid clearance of the
spirochetes.
❖ The first dose of appropriate antibiotic causes transient worsening of
clinical
symptoms/signs. This mostly happens within the first two hours after
antibiotic
administration.
❖ This reaction is very common occurring in 35-100% and is
associated with increased mortality.
❖ In its classic form, it occurs in two
distinct phases:
✓ Chills phase → which consists of a rise in BP, pulse, and
respiratory
rate; and
✓ flush phase → which is associated with dramatic fall of BP.
❖ The reaction should be actively anticipated and managed aggressively
with fluid resuscitation and cardiovascular support

2. In patients who remain febrile after treatment, consider other concomitant


infections like typhus.

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Chapter 12; MSS Related disorders and infections

12.1. Rheumatologic Disorders


12.1.1 Gout (ሪህ)
Gout is a common inflammatory arthritis resulting from deposition of
crystals of urate in the joint space and tissues around the joint.
Urate crystals are formed as a consequence of long term elevation of
serum uric acid levels in a predisposed individual.
Uric acid is a byproduct of purine metabolism. Most of the purine is
produced endogenously by the liver and a lesser part comes from
consumption of purine rich food.
Recurrent gout attack can cause joint damage, additionally it can result
in:
❖ Tophus (pleural form, Tophi): accumulation of urate crystals in
subcutaneous tissue, cartilage and soft tissue areas.
❖ Kidney stones: formation of urate stones in the kidneys and
urinary tract
❖ Urate Nephropathy
Although the prevalence of gout is not studied in Ethiopia, it is one of
the commonest causes of inflammatory arthritis observed in clinical
practice.

Risk factors for Gout


➢ Obesity
➢ Hypertension
➢ DM
➢ Metabolic syndrome
➢ CKD
➢ Alcoholism

Males are much more commonly affected than females. It is rare to find
gout in reproductive age woman, after menopause the difference
between men and women narrows.
Even though hyperuricemia is the cause gout, only 10-15% of patients
with hyperuricemia develop gout.

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Most patients with hyperuricemia don’t develop clinical Gout in their life
time. Due to this fact hyperuricemia should not be considered equivalent
to Gout.

Clinical features

The clinical manifestations of Gout are classified in to three


1. Acute attacks (flares)
2. Inter critical gout (periods between flares)
3. Chronic Gout (Chronic Gouty arthropathy) with or without tophi

A. Acute attacks (flares)

Symptoms
 Severe (excruciating) pain over a joint associated with swelling, redness,
and hotness.
 The pain is acute in onset and reaches to its maximum within 6-
12hours, not exceeding 24hours.
 Initial attacks involve a single joint. Rarely multiple joints may be
involved.
 The majority of the first attacks involve the base of the great toe
(known as podagra) or knee.
 Flares usually subside within several days without treatment and few
days with treatment.
 Patients might perceive the initial attack as an unnoticed trauma.
 The course of gout after the first attack is variable. Some might have
no recurrence while other might have frequent or occasional recurrences.
 Multiple joint involvement and upper extremity involvement at initial
presentation should prompt investigation for other causes of polyarthritis.
 Most patients do not have any symptoms in the period between flares.

Signs
 A swollen, tender, erythematous joint and evidence of joint effusion.

B. Inter critical gout (periods between flares)

❖ Even after a severe flare most patients enter in to a completely


asymptomatic period.
❖ The presence of a completely asymptomatic period is unusual in
other causes of arthritis, hence helps for diagnosis. 1162
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C. Chronic Gouty arthropathy/ Tophaceous gout

Symptoms

 Chronic joint pain of variable severity involving few or many joints


 Acute flares of variable frequency on top of chronic joint pain
 Deformity of joints with limitation of movement

Signs

 Joint deformity and swelling


 Tophi
o Painless (non-tender), visible and palpable swelling usually present
around the joints, tendons or the ears.
o When tophi stretch the skin their white to yellow color might be
visible

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Investigation and diagnosis

Diagnosis of gout flare

 Clinical dx

clinical diagnostic rule

1. Male sex (2 points)


2. Previous patient-reported arthritis flare (2 points)
3. Onset within one day (0.5 points)
4. Joint redness (1 point)
5. First metatarsal phalangeal joint involvement (2.5 points)
6. Hypertension or at least one cardiovascular disease (1.5 points)
7. Serum urate level > 5.88 mg/dL (3.5 points)

Based upon the total score, patients can be identified as having probability of gout as;
➢ low (≤4 points),
➢ intermediate (>4 to <8 points)
➢ high (≥8 points)

 Demonstration of urate crystals from aspirated joint fluid using polarized


light microscope → Gold standard

 Joint fluid aspiration and analysis is mandatory if septic arthritis is


considered.

 Serum uric acid level


o Normal or low uric acid is common during acute attacks (it can
be high, normal or low).
 In acute attacks imaging (like X-ray) has limited role
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Diagnosis of inter critical and chronic gout


 The diagnosis of inter critical and chronic gout depends on clinical,
serum uric acid and imaging findings
o The presence of recurrent flares and asymptomatic period
o Presence of tophi
o Elevated serum uric acid level
o X-ray:

✓ punched out lesion


✓ intra-osseous lesions
✓ sclerotic overhanging edges
✓ joint space is preserved and narrowing occurs late.
✓ Calcified tophi on soft tissue and joint area

o Ultrasound of joint/s:

 Evaluation of associate risk factors→ All patients with gout need to be


screened for cardiovascular risk factors:

✓ FBS and/or HbA1c,


✓ lipid profile
✓ BUN & creatinine.
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NSAIDs Dosage Duration Precautions


Indomethacin Oral: 50mg, TID (Max,200mg/day) Total duration x PPI prophylaxis should
Rectal suppository: 100mg/day 7 days be given for prevention
Diclofenac Oral: The initial high of GI bleeding in the

 Neutrophilic leukocytosis and/or elevation of ESR or CRP are common


in gout flares, but their presence in other acute arthritides generally
makes these findings of little diagnostic value.

Treatment of gout

Pharmacologic management

1. Treatment of acute attacks (flares)

First line treatment for acute attacks

A. In individuals with normal kidney function: NSAIDS

NSAIDS should be avoided in patients with impaired kidney function,


active PUD and cardiovascular disease.
Full anti-inflammatory dose needed
There is no evidence to show one NSAID is clearly superior to another.

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Immediate release 50mg, TID dose can be following group


Extended release 75mg, BID reduced after 2- ❖ Age >60
Maximum dose: 150mg/day 3 days ❖ Dyspepsia history in
Rectal suppository: 100mg/day any age group
Intramuscular: 75mg, IM, BID ❖ Concurrent use of
Ibuprofen 800mg PO TID (Max;3,200mg/day) Aspirin, anticoagulant
Meoxicam 15mg/day, PO (Max;15mg/day) or steroid

B. In individual with impaired kidney function: short course steroids are first
line
Prednisolone, 30mg per day, to be tapered over 10-14 days.
▪ Typical prescription: 30mg x3days, 20mg x3days, 10mg
x3days, 5mg x3days
Intramuscular steroid/Intra-articular steroid: If oral prednisolone is not
tolerated
Triamcinolone acetonide 40-60mg, IM, stat.
▪ For intra-articular 40mg for large joints and 20mg for small
joints.
Methylprednisolone 40-80mg, IM, stat.
▪ For intra-articular 40mg for large joints and 20mg for small
joints, intra-articular, once
C. In patients with diabetes; worsening of hyperglycemia should be
anticipated and doses of diabetes medication needs to be adjusted
accordingly.

2. Second line treatment for acute attacks

In normal kidney function: Colchicine


▪ Colchicine: Initial dose of 1.2 mg, after one hour 0.6 mg, a
total dose in the first day
✓ Subsequent dose: 0.5 to 0.6mg daily to twice daily
✓ Duration: Until symptoms subside

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3. Urate lowering therapy:

for prevention of recurrence, joint damage and renal


complication
Indications for starting urate lowering therapy: Any one of the
following
✓ Recurrent acute flares (> 2 flares in one year)
✓ Presence of tophi
✓ Chronic joint damage: Clinical or radiologic
✓ Renal stones in patients with hyperuricemia
✓ First attack in patients who need continuation of diuretics
Allopurinol is the first line urate lowering therapy
❖ Dose in patient’s normal kidney function
✓ Start after two weeks of flare
 Starting dose: Allopurinol 100mg/day
✓ Dose should be escalated every 2-4 weeks, until target uric
acid level is achieved.
✓ Increase by 100mg every month until target serum uric acid
level is achieved to a maximum dose of 800mg/day.
✓ Most patients require about 300mg/day or above.
✓ Once target serum uric acid level is achieved: follow up can
be done every 4-6 months
❖ Dose in patients with significantly impaired kidney function
✓ Starting dose
 eGFR 5–15ml/min: 50 mg twice weekly
 eGFR 16–39ml/min: 50 mg every 2 days
 eGFR 31–45ml/min: 50 mg daily
✓ Maximum dose for patients with eGFR<30m/min 300mg/day

Precautions with Allopurinol


Allopurinol is generally well tolerated; however, severe cutaneous drug
reactions can rarely happen and be fatal.
Hence, all patients taking the drug need to be informed to stop
the drug immediately and seek medical attention, if they notice
rash or have itching.

Target serum uric acid level


❖ Non tophaceous Gout: < 6mg/dl
❖ Tophaceous gout: < 5mg/dl
Prophylaxis for flares during urate lowering therapy
❖ During initiation and dose escalation of Allopurinol gout flares are
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❖ Prevention of flares is needed during the first 06 months of


Allopurinol therapy.
❖ For patients with normal kidney function
First line
✓ Colchicine 0.5 to 1mg/day

Alternative (if cardiovascular risk is low)


✓ low dose NSAIDs with PPI (e.g. Diclofenac 50mg -75mg/day,
Ibuprofen 200-400mg BID)
B) In situations when colchicine or NSAIDs are not tolerated/not available/
contraindicated: Prednisolone 5 to10mg/day

❖ For patients with impaired kidney function:


First line
✓ Prednisolone 5 to10mg/day

Non pharmacologic management of Gout

Non- pharmacologic management is essential in all patients with


gout. The non-pharmacologic management includes the following
three elements:
❖ Dietary management
❖ Life style management and screening for cardiovascular risk
factors
❖ Education

1. Dietary management
Dietary management alone is insufficient to control gout but it is
an important adjunct.
Excessive focus on dietary management without using effective
urate-lowering therapy should be avoided.

Foods which need to be Remark


restricted
Meat There is no difference among the red meat
types (beef, lamb, goat meat or mutton)
Alcoholic drinks including beer Red wine in moderation has the lowest risk
High sugar containing drinks
and foods
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Foods should encouraged or not restricted Remark


Milk and dairy products Encourage
Fruits and vegetables Encourage
Egg Encourage
Bean, peas, chickpea Safe and can be taken safely

2. Life style management and cardiovascular risk screening


Weight reduction should be encouraged in overweight and
obese individuals.
All patients with gout should be screened for hypertension,
diabetes, and dyslipidemia.

3. Education
All patients with gout should be educated on flare management, the
purpose and the lifelong nature of urate lowering therapy, adherence,
dietary and life style management
Educate patients and their families on the common misconceptions on
the dietary management of gout.

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12.1.2. Systemic lupus erythematosus (SLE) (lupus)

SLE is a multi-system autoimmune disease with chronic, relapsing-


remitting course and variable manifestations.
Manifestations could range from a mild one to a life-threatening.
The diagnosis of the disease could be challenging as it might have
unpredictable course and mimic many other systemic diseases.
SLE can affect any organ including the musculoskeletal, skin,
hematologic, renal, neuropsychiatric, cardiovascular, and respiratory
system.
Not all manifestations appear simultaneously. Interval between the
different manifestations could be months or years.
Constitutional (especially fatigue), mucocutaneous and musculoskeletal
symptoms tend to occur early.
Females are much more commonly affected than males (F:M ratio =
9:1).
The age of onset also ranges childhood to old age. The common age
of onset is third to 3rd to 5th decade.
Renal disease is the commonest organ/life threatening involvement.
Lupus is associated with increased risk of thrombosis and accelerated
atherosclerosis
Pregnancy increases the risk of flare and should be avoided unless the
lupus in remission for more than six months.

Clinical features

Symptoms

➢ Constitutional symptoms: Fatigue, fever, weight loss


➢ Mucocutaneous: Increased hair loss, photosensitivity, acute or
subcutaneous/subacute and chronic skin lesions
➢ Musculoskeletal: Joint pain/swelling, morning stiffness, deformities can
also happen
➢ Pulmonary: Cough, shortness of breath, pleuritic chest pain
➢ Cardiovascular: chest pain
➢ Renal: body swelling, decrement in urine amount, reddish urine, foaming
of urine
➢ Neurologic: headache, seizures, decreased cognition, changes in mental
status, weakness of extremities, features of painful peripheral neuropathy
➢ Psychiatric: behavioral changes
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Signs

➢ Mucocutaneous: malar rash (butterfly shaped rash), maculopapular or


bullous lesions, scaring discoid rash, painless oral ulcers, non-scaring
alopecia
➢ Musculoskeletal: joint swelling, tenderness and decreased mobility
➢ Pulmonary: signs of pleural effusion, pleural friction rub, crackles
➢ Cardiovascular: signs of pericardial effusion, pericardial friction rub
➢ Renal: edematous state
➢ Neurologic: focal neurologic deficit, low score on mine mental test
➢ Psychiatric: behavioral changes

Picture; Malar rash (butterfly shaped rash)

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Investigation and diagnosis

Investigations

Autoantibodies
o ANA
o Anti-dsDNA
o Anti-Smith
o Anti-phospholipid antibodies: Lupus anticoagulant, anti-cardiolipin,
beta-2 glycoprotein
Investigations for systemic involvement
o CBC → anemia, thrombocytopenia, leukopenia
o U/A → proteinuria, hematuria
o 24hour urine protein >500mg
o Creatinine and urea
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o Echo
o MRI and MRA

Diagnosis

The diagnosis of SLE is based on a constellation of clinical laboratory


and autoantibody tests.
The presence of cutaneous, musculoskeletal symptoms associated with
constitutional symptoms in young or middle aged women unless
explained by another obvious diagnosis should suspected to be SLE
A high index of suspicion is needed.
Classification criteria
o The two widely used classification criteria for SLE clinical diagnosis
are the 2012 SLICC and 2019 EULAR/ACR
o Both have good sensitivity and specificity (83.7% to 96.7%); hence, it
is advised to use either of them for the purpose of diagnosis in
patients with clinical features suggestive of SLE.

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Table: The 2012 SLICC criteria for SLE classification


Ref.: Arthritis Rheum 2012; 64:2677-2686.
➢ Diagnosis requires fulfillment of at least four criteria, with at least one clinical
criterion AND one immunologic criterion OR
➢ Lupus nephritis as the sole clinical criterion in the presence of ANA or anti-
dsDNA antibodies
Clinical Criteria Immunological Criteria
➢ Acute cutaneous lupus ➢ ANA above laboratory
➢ Chronic cutaneous lupus reference range
➢ Oral ulcers: palate ➢ Anti-dsDNA above
➢ Nonscarring alopecia (diffuse thinning or hair laboratory reference range,
fragility with visible broken hairs) except ELISA: twice above
➢ Synovitis involving two or more joints, laboratory
characterized by swelling or effusion OR ➢ Anti-Sm
tenderness in two or more joints and thirty ➢ Antiphospholipid antibody:
minutes or more of morning stiffness. any of the following
➢ Serositis ➢ Low complement
➢ Renal ➢ Direct Coombs test in the
➢ Neurologic absence of hemolytic
➢ Hemolytic anemia anemia
➢ Leukopenia (< 4000/mm3 at least once)
➢ Thrombocytopenia (<100,000/mm3) at least
once

Treatment

Non-pharmacologic treatment
Exercise
Minimization of sun exposure: hat, umbrella
Stress management

Pharmacologic management

NSAIDS: for arthralgia and mild arthritis


Corticosteroids: For multiple indications
o Pulse steroid: for acute life or organ threatening
▪ Methylprednisolone 250 - 1000mg IV for 3 days
o High dose steroid: for severe organ/life threatening for 4-8 weeks
with tapering after that
▪ prednisolone 0.5-1mg/kg/day or equivalent
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o Low dose steroid (maintenance): ≤ 10mg

Antimalarial: all patients with SLE in the absence of contraindication


o Chloroquine phosphate 250mg/day or 250mg PO 5 times per week
o Baseline and annual ophthalmologic screening is needed, for possible
retinopathy.
Other immunosuppressive:
o For life/organ threatening indication or as steroid sparing
o They should be prescribed by specialists who have experience in
using them
▪ Azathioprine
▪ Methotrexate
▪ Mycophenolate Mofetil
▪ Cyclophosphamide
➢ Patients with SLE with renal, neurologic involvement should be consulted
for the specialist urgently.

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12.1.3 Rheumatoid arthritis (RA) /ቁርጥማት/

➢ RA is a chronic systemic inflammatory disease mainly characterized by


symmetrical polyarthritis of the small joins of hand and feet with
progressive damage of joints.
➢ In addition to joints, it affects the lung (ILD, Pleurisy, PAH), blood
(cytopenia and Felty’s syndrome), skin (erythema nodosum and a variety
of vasculitic lesions) and less commonly other organs.
➢ It more common in women than men.
➢ Although the onset can be at any age, the peak is 50-60 year in
women and >70 year in men.

Clinical features
Symptoms

Joints symptoms
o The most typical symptomatic presentation of RA is that of a
symmetric polyarthritis (defined as involving > 5 joints), involving
small joints of the hands, wrists, and/or feet.
o Joint pain
o Joint swelling
o Early Morning stiffness: usually lasts > 02 hours
o Limitation of joint mobility (difficulty of using the joint)
Constitutional symptoms
o Fatigue
o Generalized musculoskeletal pain
o Weight loss
Symptoms from other organ-system involvement (extra-articular
symptoms)
o Occasionally patients may also present with other organ involvements:
o Cough, shortness of breath, chest pain: Lung involvement
o Dryness of the eyes, red and/or painful eyes: Eye involvement
o Swellings(nodules), red/dark lesions, ulcers on the skin : Skin/vascular
involvement
o Numbness or pain over the extremities: Peripheral nerve involvement

Signs

Joint
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o Swelling (bogy swelling from effusion or subtle swelling from


thickening)
o Tenderness
o Deformities (swan neck deformity of fingers, ulnar deviation of MCP
joints, Boutonniere deformity of thumb…)
Other organ-systems (extra-articular signs):
o Depending on the systems involved e.g. subcutaneous nodules,
enlarged lymph nodes, signs of pleural/pericardial effusion,
splenomegaly

Investigations and diagnosis


➢ RA should be strongly suspected in any patient who present with
multiple joint pain, swelling and morning stiffness for few weeks.
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➢ Hand, wrist, and foot joints are the most commonly involved; however,
any joint can be involved.
➢ Distal interphalangeal (DIP) joints are usually spared in RA.
➢ The spine (the back), apart from the atlantoaxial joint, is not directly
involved by inflammation but may be affected by osteoporosis and
mechanical imbalance due to involvement of the weight bearing joints.
➢ There is no single test, imaging finding or clinical finding which is
diagnostic of RA. A strong clinical suspicion is needed in any patient
when with polyarthritis for few weeks.
➢ The classification criteria for RA is designed for the purposes in
researches, but it is a good clinical guide to make a diagnosis with a
reasonable sensitivity
➢ Rheumatoid factors (RFs)
✓ Sensitivity: About 70% of patients are positive at diagnosis.
✓ False positivity: other CTD like SLE and some infectious diseases
like malaria and hepatitis C
✓ False negativity: Nearly one third of patients with RA are negative
RFs results
➢ Anti-CCP (Anticyclic-citrullinated peptide) antibody test
✓ Sensitivity: Similar to rheumatoid factors
✓ Specificity: > 95%.
➢ Other investigations
✓ ESR or CRP: Moderately increased ESR (usually not >50ml/min) or
CRP. ESR and CRP may be normal in about one-third of patients.
✓ CBC: Norma WBC, mild anemia (due to chronic inflammation), or
thrombocytosis (due to chronic inflammation)
✓ Imaging (X-ray): in early disease X-ray is usually normal, as the
disease advances X-ray shows decreased bone density, bone
erosion, joint space narrowing, and deformities.

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ACR/EULAR 2010 Classification Criteria for Rheumatoid Arthritis

These criteria should be restricted to persons with at least one clinically detectable
swollen joint in the absence of a more likely diagnosis
A score of ≥6 points is classified as definite RA. In each domain, consider only the
category with most points.
Joint involvement and distribution (0-5 points)
➢ Any swollen or tender joint on physical examination
➢ Large joints: Shoulders, elbows, hips, knees, and ankles
➢ Small joints: Metacarpophalangeal, proximal interphalangeal, second through fifth
metatarsophalangeal, thumb interphalangeal, and wrists
✓ 1 large joint → 0 point
✓ 2–10 large joints → 1 point
✓ 1–3 small joints → 2 points
✓ 4–10 small joints → 3 points
✓ > 10 joints (and at least 1 small joint) → 5 poin

Serology (0-3 points)


✓ Low-positive results are > 1 to 3 times the upper limit of normal of the assay
used.
✓ High-positive results are > 3 times the upper limit of normal of the assay used
✓ Negative RF and negative ACCP → 0 point
✓ Low-positive RF or low-positive ACCP → 2 points
✓ High-positive RF or high-positive ACCP → 3 points

C. Acute-phase reactants (0-1 point)


✓ Normal CRP and normal ESR → 0 points
✓ Abnormal CRP or abnormal ESR →1 point
D. Duration of symptoms (0-1 point)
➢ Patient's self-report on the maximum duration of symptoms of any joint clinically
involved at the time of assessment
✓ < 6 wk → 0 point
✓ ≥6 wk →1 point

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Treatment

Pharmacologic treatment

Disease-modifying antirheumatic drugs (DMARDS)


❖ All patients with RA should be started with DMARDS without any
delay
❖ If DMARDs are not available or you don’t have the experience of
using them, the patient should be referred.

1) First line DMARD: Methotrexate (MTX) 7.5 - 25mg/once per week

➢ Investigation before initiation of MTX: CBC, liver enzymes, screening


HBV and HCV, BUN and Creatinine, Chest X-ray.
➢ Starting dose: 7.5mg - 10mg per week, PO or Sc
➢ The MTX dose needs to be escalated by 2.5mg-5mg, at intervals no
more frequent than every month until disease activity is well controlled
or maximum tolerated dose is achieved.
➢ Maximum dose: 25mg/week
➢ All patients on MTX should be given Folic acid to prevent the
hematologic and other side effects.
✓ Folic acid 1mg tab, po/day or 5mg tab, po/2-3 times per week
➢ Major adverse effects: Liver toxicity, Bone marrow suppression
(pancytopenia), lung toxicity and increased susceptibility to infection
➢ Monitoring: All patients need to have CBC and LFT monthly for the first
3 months, then every 03 months.
➢ Contraindications to MTX:
✓ Pregnancy
✓ CKD / Significant impairment in kidney function (eGFR<30ml/min),
✓ CLD
✓ Active/uncontrolled infection.

2) Additional or alternative DMARDS

➢ Chloroquine: Chloroquine phosphate 250mg/day


✓ As additional agent: Add Chloroquine in patients who are having
poor disease control while taking maximally tolerated dose or
>15mg of MTX/week.
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✓ As an alternative to MTX: In patients for whom MTX is


contraindicated or have mild disease Chloroquine can be used as
an alternative.
✓ Dosing in adults: Chloroquine phosphate 250mg tab (equivalent to
chloroquine base 150mg), 01 tablet 5 times per week
➢ Disease activity not well controlled by a combination of maximum/
maximally tolerated dose Methotrexate and chloroquine:
✓ Add low dose steroid (<10mg/day) as part of the DMARD and
Consult specialist
➢ Relieving acute inflammatory pain
First line: NSAIDS or short course corticosteroids
➢ NSAID options
✓ Ibuprofen, 400-800mg, P.O, TID with meals.
✓ Diclofenac, 150mg/day, P.O, in 2-4 divided doses. Rectal
suppository 100mg/day
✓ Indomethacin, 25-50mg P.O.TID; maximum dose: 200mg/day. Rectal
suppository, insert 100mg, BID or once.
✓ Meloxicam, 7.5 - 15mg/day. Maximum dose 15mg/day
✓ Piroxicam, 10-20mg/day. Maximum dose 20mg/day
➢ Precautions with NSAIDS
✓ Avoid NSAIDS in patients with impaired kidney function
✓ Offer PPIs for those at high risk of NSAIDs associated peptic ulcer
bleeding: patients with history of peptic ulcer symptoms, on
Aspirin/anticoagulant /steroid

3) Corticosteroids: Indications

➢ As a bridge to DMARDS at diagnosis


✓ Prednisolone
▪ Starting dose: 20mg/day. Do not exceed 30mg/day.
▪ Tapering: taper by 5-10mg every 2 weeks, keep it <10mg/day
for 3-6 months until DMARDs take over.
✓ Flare management
▪ Prednisolone 15 -20mg/day taper to baseline dose or stop in
2 weeks
✓ Chronic therapy
▪ Corticosteroids are not generally regarded as DMARDS
▪ Long term therapy is not recommended
▪ In some patients where disease activity is poorly controlled
while a combination maximum/maximum tolerated dose
DMARDs low dose steroid may be needed
▪ Prednisolone 5-10mg/day achieved

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Diagnosis of
RA made

Start Methotrexate 7.5- 10mg/week


Start Predisolone 30-40mg/day
+ as bridge therapy
Folic acid 5mg, 2-3 x/week Taper by 5-10mg every 2 weks

Increase the dose of Methotrexate by


2.5-5mg/month - Predinsolone 5-10mg/day for 3- 6
-until remission or low disease activity is months only
achieved
- Maximum dose 25mg/week

If remission is not achieved


Add Chloroquine phosphate 250mg/day

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12.1.4 Osteoarthritis (የአጥንት እና አንጓ ብግነት)

➢ Osteoarthritis (OA) is a joint disease which results from an active


pathology involving the whole joint structure including cartilage damage,
low grade joint inflammation, bone remodeling, and osteophyte formation.
➢ It was previously thought that OA is a degenerative disease; however, it
is now understood that it is the result of active biochemical and cellular
pathologic process.
➢ Joint pain and progressive loss of joint function result from the
pathologic process.
➢ The knee, hip and hand joints are the most commonly affected sites.
➢ OA is considered to be the leading cause of join related disability in old
adults.

Risk factors for OA

✓ Old age
✓ Overweight/obesity
✓ Female sex
✓ Occupation
✓ Injury/trauma.

Clinical features
Symptoms

➢ Joint pain
✓ Pain in OA is generally activity related and relived by rest. It is
more intense at the start of activity.
✓ It is worse in the afternoon and evening.
➢ Joint stiffness
✓ The morning stiffness in OA is shorter (<30 minutes) compared to
rheumatoid arthritis and other inflammatory arthritis.
➢ Symptoms of “crepitus”
✓ Clicking, grinding or popping feelings
➢ Instability of joint:
✓ Buckling or giving away feeling, lacking the confidence to use
weight bearing joints
➢ Limitation of movement
➢ Deformity
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Signs

➢ Distribution of joint involvement:


✓ Single joint OA: knees, hips, thumb, interphalangeal joints, cervical
or lumbar spine
✓ Generalized (Polyarticular) OA
▪ More than two joint regions are involved.
▪ Symptoms usually starts in the hands around middle age and
subsequently affect the knees and other joints over several
years
▪ The main clinical sign is the presence of multiple Heberden's
nodes (hard/bony swelling in the DIP joints) or Bouchard’s
nodules (hard/bony swellings in PIP joints)

Investigations and diagnosis

➢ The diagnosis of osteoarthritis is clinical


➢ The presence of following three makes the diagnosis of OA highly likely:
✓ Age ≥45 years
✓ Joint pain in only one or few joints
✓ Morning stiffness duration ≤ 30 minutes
➢ The presence of other clinical features e.g. Heberden’s node, joint
instability and crepitus makes the diagnosis of OA more certain.
➢ x-ray of the involved joint → support the diagnosis
➢ ESR or CRP: Generally normal in patients with OA.
➢ Investigations to exclude other differential diagnoses
✓ Psoriatic Arthritis has to be ruled out in polyarticular OA
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✓ Rheumatoid factor/anti-CCP antibody if rheumatoid arthritis is


suspected
✓ Joint fluid aspiration may be needed

Treatment

Pharmacologic treatment

➢ Pain management:

First line

✓ NSAID’s are first line:


▪ Topical NSAIDS: For knee and other joints as well OA
▪ Systemic NSAIDS (oral or rectal suppository): For all types of
OA including
• For patients with high risk for GI bleeding use with PPI
• NSAIDS are contraindicated in patients with history of
upper GI bleeding and CKD

Second line → If NSAIDS are contraindicated or ineffective

✓ Duloxetine: Initial dose 30mg/day, increase t0 60mg/day after at


least one week. Maximum dose 120mg/day
✓ Acetaminophen (Paracetamol): 1g TID to QID, Max;4g/day.
✓ Tramadol: Dose for immediate release: 50mg/day and increase to
50mg BID. Gradually increase to 50mg QID. Max; 300mg/day

Drugs which are not recommended for the management of OA

➢ Non-tramadol opioids
➢ Systemic steroids
➢ Colchicine
➢ Bisphosphonates
➢ Methotrexate

Intra-articular steroids can be used for Pain management in knee or hip


(for hip it should only be image guided) which can be given by specialist
who have experience.

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➢ Exercise:
✓ Both aerobic (e.g. walking) and local muscle strengthening are
useful
✓ Tai Chi (a form of Chinese martial art practice along with
meditation) and Yoga
➢ Weight loss: For overweight individuals with knee or hip OA
➢ Patient education: including self-management
➢ Cane or walking stick /for knee or hip OA/, braces/ tibiofemoral knee
braces for knee OA / and orthosis / Hand orthosis for first
carpometacarpal joint
➢ Surgical treatment
✓ Total joint replacement hip or knee) can be considered in patients
with end-stage OA (i.e. severe persistent symptoms and marked
functional impairment). Patients should be referred to specialized
hospitals or centers.

The following surgical interventions are not recommended

➢ Arthroscopic debridement
➢ Abrasion arthroplasty (involving burring and drilling of sclerotic bone)
➢ Synovectomy

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12.2. MSS infections

12.2.1. Pyogenic Osteomyelitis


➢ Pyogenic Osteomyelitis is an acute infection of the bone and its structures
caused by bacteria.
➢ Osteomyelitis occurs as a result of hematogenous spread, contiguous spread
from adjacent soft tissues or direct infection from trauma or surgery.

Aetiology

➢ Hematogenous osteomyelitis is usually monomicrobial, while osteomyelitis due


to contiguous spread or direct inoculation is usually polymicrobial.
➢ S. aureus is the most common causative organism.
➢ Coagulase- negative staphylococci and aerobic gram-negative bacilli are also
common causes.
➢ Streptococci, enterococci and anaerobes are also implicated.

Clinical features
➢ Gradual onset varying from few days to weeks of local bone pain, swelling,
low grade fever, malaise and weight loss.

Investigations
➢ Usually Clinical Dx
➢ CBC
➢ ESR & CRP
➢ X-ray of the affected bone
➢ Culture of pus/sequester (if debridement is done)

Treatment
Non pharmacologic
➢ Rest/immobilization
➢ Surgical debridement (Drainage by surgeon/orthopedic surgeon)
➢ N.B. Osteomyelitis frequently requires both surgical therapy for debridement of
necrotic material together with antimicrobial therapy for eradication of infection.
The debrided necrotic material should be sent for culture.
Pharmacologic
➢ Empiric antibiotic
✓ Empiric treatment with activity against S. aureus (especially MRSA) and
gram-negative organisms is required.
First line
✓ Vancomycin, 30mg/kg/day, IV, BID (initially 20 mg/kg loading dose, not to
exceed 2 g/dose) → usual adult dose 1gm, IV, BID
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PLUS
✓ Ceftriaxone 2 g IV daily OR
✓ Ciprofloxacin, 400mg, IV, BID or 750mg, P.O., BID
Alternative
✓ Cloxacillin, 2gm, I.V. QID PLUS
✓ Ciprofloxacin, 400mg, IV, BID or 750mg, P.O., BID
Specific antimicrobials: Once susceptibility results were available, specific drugs
should be used.

Duration of therapy
✓ Duration of antibiotics is for at least 6 weeks from the last debridement.
✓ For patients with residual infected bone that is not amenable to complete
removal should be treated at least for 6 weeks duration after the last
debridement (optimal duration is uncertain).
✓ For patients who undergo amputation or complete removal of all involved
bone warrant a 5 days course of antibiotic therapy after complete
debridement. If there is evidence of soft tissue infection at the operative
side pathogen-directed 10 to 14 days parenteral or highly bioavailable oral
agent can be used.
✓ In the presence of orthopedic hardware, 6 weeks parenteral therapy
following debridement is used. Thereafter, long-term antibiotic suppression
with an oral agent, guided by antimicrobial susceptibility data is
recommended. Suppressive therapy is warranted only for individuals with
retained hardware and/or necrotic bone not amenable to complete
debridement. Oral suppression antibiotics should be continued at least
until fractures are united (demonstrated radiographically).

N.B. Further treatment is guided by culture sensitivity tests

For pain and fever


✓ Analgesic/antipyretic e.g. Paracetamol, 500mg -1g P.O. PRN (4- 6 times
daily) can be given.
Monitoring For patients on parenteral antimicrobials:
✓ Weekly CBC and chemistries should be performed.
✓ In addition, ESR & CRP should be obtained at the beginning and end of
parenteral treatment (at any time in between if clinical suspicion for
treatment failure) and at the time of transition to oral suppressive therapy
(if used).
✓ If inflammatory markers persistently elevated two weeks after completion
of antibiotic therapy (in the absence of alternative explanation) possibility
of persistent osteomyelitis be considered.
✓ If a patient has associated symptoms, evaluate completeness of the
debridement, review microbiologic diagnosis and susceptibility data and
thus may warrant repeated debridement and additional antimicrobial


therapy.
If no clinical signs consistent with persistent infection, clinical observation
is reasonable.
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✓ For patients on oral suppressive antibiotic therapy:


✓ CBC, creatinine, and ALT at 2, 4, 8, and 12 weeks and then every 6 to
12 months thereafter.

12.2.2. Septic Arthritis


➢ The term septic arthritis refers to bacterial infection of a joint.
➢ Septic arthritis is dangerous and destructive to the joint.
➢ It may occur secondary to hematogenous spread (80-90%), contiguous spread
(10-15%), and direct penetration of microorganisms secondary to trauma,
surgery or injection.
➢ Old age, DM, skin infection, alcoholism, intra-articular injections are some of
the common risk factors.
➢ S. aureus is the most common cause.
➢ Streptococci and other gram positive are also frequent causes.
➢ Gram-negative bacilli are found as causes in specific situations such as
trauma, immunosuppression and very elderly.

Clinical features
➢ Septic arthritis presents acutely and mostly with a single swollen and painful
joint.

Investigations
➢ CBC
➢ ESR/CRP
➢ Synovial fluid analysis → cell count (WBC count) with differentials, Gram stain,
AFB, culture (two sets), and assessment for crystals.
➢ X-ray of the affected joint

Diagnosis
➢ Septic arthritis should be suspected in patients with acute onset of at least one
swollen, painful joint.
➢ Septic arthritis diagnosis should be established based on synovial fluid analysis
and culture.
➢ Septic arthritis could be definitively established if positive synovial fluid gram
stain and/or culture are obtained.
➢ In patients with purulent synovial fluid (leukocyte count of 50,000 to 150,000
cells/µl, mostly neutrophils) but negative synovial fluid cultures, a presumptive
diagnosis septic arthritis may be made.
➢ If synovial fluid culture is negative and no purulent fluid, alternative diagnosis
should be considered.

Treatment
➢ In general, management of acute bacterial arthritis involves joint drainage
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Non pharmacologic
➢ Aspiration/drainage: needle aspiration, arthroscopy, or arthrotomy (open surgical
drainage)
➢ Splintage, but early immobilization if joints are mobile.
➢ The joint must be splinted with a POP slab or skin traction to relieve pain and
prevent contractures

Pharmacologic → Empiric antibiotics


➢ Prior to antibiotics administration, sent synovial fluid analysis

First line
✓ Vancomycin, 30mg/kg/day, IV, BID, (usual adult dose 1gm, IV, BID) not to
exceed 2g/day for 4-6 weeks
PLUS
✓ Ceftriaxone, 2gm, I.V, daily for 4-6 weeks or
✓ cefotaxime 2 g IV TID

Alternatives
✓ Cloxacillin, 2g, IV, QID for 4-6 weeks
plus
✓ Ceftriaxone 2gm, IV, daily or
✓ cefotaxime 2 g IV TID

➢ NB: For suspected septic arthritis (in the above regimens) due to MRSA
Vancomycin is a suitable. Alternatives include clindamycin, Cotrimoxazole,
doxycycline, linezolid, and rifampin in combination with either ciprofloxacin or
fusidic acid.
➢ For suspected septic arthritis due to MSSA suitable choices include Cloxacillin,
dicloxacillin (500 mg, PO, QID), flucloxacillin (500 mg, PO, QID), or cephalexin
(500 mg, PO, QID).
➢ Patients who are allergic to penicillin can be treated with clindamycin (600 mg,
PO, TID).

Synovial fluid analysis (gram stain) and Empiric therapy choice


(until susceptibility results are available):

➢ If synovial fluid gram stain shows gram positive cocci → use vancomycin with
the above dose as first line and Cloxacillin as alternative.
➢ If synovial fluid grams stain shows gram negative bacilli -use third-generation
cephalosporin (use ceftriaxone with the above dose) as first line.
➢ If the initial Gram stain of synovial fluid is negative but synovial fluid cell count
is consistent with septic arthritis (purulent fluid of 50,000 to 150,000 cells,
mostly neutrophils), the approach depends on individual clinical circumstances.
✓ For immunocompetent patients without confounding factors (such as
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✓ For immunocompetent patients with traumatic bacterial arthritis, use


vancomycin plus a third-generation cephalosporin.
✓ For immunocompromised patients and injection drug users, use
vancomycin plus a third-generation cephalosporin (ceftriaxone).
✓ Ceftazidime (2 g IV TID) or cefepime (2 g IV TID to QID) should be used
in place of ceftriaxone if there is a high risk for Pseudomonas infection.
✓ Consequently, antibiotic therapy should be adjusted to culture and
susceptibility data once available.

Duration of therapy
➢ Duration of antibiotic treatment is 4-6 weeks (optimal duration is uncertain).
➢ At least the first 2 weeks of antibiotics should be through IV route.
➢ For susceptible pathogens durations may be shorter than indicated (e.g.
fluoroquinolone susceptible pathogens can be treated for 5 to 7 days of
parenteral, followed by 14 to 21 days of oral fluoroquinolone with careful
monitoring of the compliance and response).
➢ For staphylococcus bacteremia (in the absence of endocarditis) 4 weeks
parenteral treatment is recommended.
➢ If no staphylococcus bacteremia 1 to 2 weeks oral therapy can be used after
1 to 2 weeks of parenteral therapy.
➢ For patients with septic arthritis with endocarditis, treat for duration required for
endocarditis.
➢ Patients with septic arthritis and contiguous osteomyelitis require a long (4-6
weeks) course of antibiotics.

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Chapter 13; Hematologic Disorders

13.1. Anaemia (የደም ማነስ)

➢ Anemia is not a disease by itself but a manifestation of different disease


entities (causes)
➢ Anemia is functionally defined as reduction in RBC mass, accompanied
by a decrease in oxygen carrying capacity.
➢ Laboratory wise anemia is defined as a reduction in one or more of the
three RBC measurements in the CBC: Hgb, hematocrit (HCT), or RBC
count. For practical purposes, hemoglobin or hematocrit are commonly
used.
➢ WHO criteria for diagnosing anemia in men and women are hemoglobin
values <13 and <12 g/dl, respectively.
➢ Anemia is not a single disease entity; it is rather a manifestation of
several pathologies.

Classification of anemia
➢ Designed for systematic approach of different causes of anemia
➢ There are two approaches of classification
I. Kinetic approach→ Based on the mechanisms responsible for the
anemia
II. Morphologic approach → Based on the size of RBCs and the
reticulocyte response

1. Kinetic approach
A) Anaemia due to decreased RBC production
✓ Also known as ineffective erythropoiesis
✓ Causes include
▪ Lack of nutrients- iron, folate, or B12
▪ Bone marrow disorders- aplastic anemia, MDS, tumour
infiltration
▪ Bone marrow suppression- drugs, irradiation
▪ Anemia of chronic disease/inflammation
B) Anemia due to increased RBC destruction
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✓ Haemolytic anemias
C) Anemia due to blood loss
✓ Obvious or occult bleeding

Morphologic approach

➢ Size → as measured by mean corpuscular volume (MCV)


✓ The normal RBC has a volume (MCV) of 80-100 femtoliters (fL),
equal to that of the nucleus of a small lymphocyte
✓ RBCs larger than the nucleus of a small lymphocyte on a
peripheral smear are considered macrocytic, while those that appear
smaller are considered microcytic

➢ Chromicity
✓ Normochromic → MCH = 27-33 or central pallor of RBCS < 1/3rd of
the size of RBC
✓ Hypochromic → MCH <27 or central pallor >1/3rd of the size of
RBC

b. Macrocytic normochromic anemia


✓ MCV >100fL
✓ Causes include
▪ Folate deficiency
▪ Vit.B12 (Cobalamin) deficiency
▪ Any condition causing marked reticulocytosis
▪ Alcohol abuse
▪ Hypothyroidism
▪ Drugs- zidovudine, methotrexate, and hydroxyurea
✓ Megaloblastic anemia
▪ Due to folate and cobalamin deficiency
▪ Characterized by hypersegmented neutrophils
c. Microcytic hypochromic anemia
✓ MCV<80 fl
✓ Causes include;
▪ Iron deficiency anaemia
▪ Lead poisoning
▪ Sideroblastic anemia
▪ Thalassemia
▪ Anemia of chronic illness (30% of the cases)
d. Normocytic normochromic anemia
✓ MCV 80-100 fl
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✓ Causes include;
▪ Anemia of chronic illness (70% of the cases)
▪ CKD
▪ Early iron deficiency anemia
▪ Acute blood loss

Table; Classification of anemia based on hemoglobin level or severity; WHO


2015
Population Hemoglobin level (in g/dl)
Non-anemia Anemia
(Normal) Mild Moderate Severe
Children 6-59 months of age ≥ 11 10-10.9 7-9.9 <7
Children 5-11 years of age ≥ 11.5 11-11.4
Children 12-14 years of age ≥ 12 11-11.9
Men ≥ 15 years of age 13.3 - 16.2 11-12.9 8-10.9 < 8
women ≥ 15 years Non pregnant 12.0 - 15.8 11-11.9
of age Pregnant ≥ 11 10-10.9 7-9.9 < 7

Clinical features
Symptoms
➢ Fatigue, dyspnea, palpitation, syncope
➢ Headache, lightheadedness, tinnitus, vertigo, difficulty of concentration
➢ Anorexia, nausea, indigestion
➢ Symptoms s of the underlying disease e.g. melena in GI bleeding,
heavy menstrual bleeding, generalized body swelling in CKD,

Signs
➢ Pallor, tachycardia, wide pulse pressure /ejection systolic murmur.
➢ Signs of Heart Failure (raised JVP, S3, hepatomegaly, edema)
➢ Signs of the underlying disease-causing anemia: lymphadenopathy,
splenomegaly, angular chelitis, tumors (abdominal/ pelvic mass) etc.
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Investigation and diagnosis

1) CBC with RBC indices


2) Peripheral blood smear
3) Reticulocyte count and index

Picture; High-power view of a normal peripheral blood smear. Several platelets (arrows) and a normal lymphocyte
(arrowhead) can also be seen. The red cells are of relatively uniform size and shape. The diameter of the
normal red cell should approximate that of the nucleus of the small lymphocyte; central pallor (dashed arrow)
should equal one-third of its diameter.

Picture; peripheral blood smear from a patient with iron deficiency is shown at two different magnifications. Small
(microcytic) red blood cells are shown, many of which have a thin rim of pink hemoglobin (hypochromia).
Occasional "pencil"-shaped cells are also present. A small lymphocyte is shown for size comparison (arrow).
Normal red blood cells are similar in size to the nucleus of a small lymphocyte (arrow), and central pallor in
normal red blood cells should equal approximately one-third of the cell diameter.

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This photo(left) shows two anticoagulated blood-filled Wintrobe hematocrit tubes following high speed
centrifugation. The tube on the left is from a normal subject, with a hematocrit of 38 percent (blue arrow). The
tube on the right is from a 19-year-old female with essential thrombocytosis, a normal white blood cell count, and
a platelet count of 5,000,000/microL. The extreme degree of thrombocytosis can be appreciated by the presence
of a marked increase in the size of the "buffy coat" (white arrow). When the Wintrobe tube is filled to near
capacity (upper arrows), and the white blood cell count is not markedly elevated, the platelet count can be
estimated by the thickness of this layer, with each mm being equivalent to one million platelets/microL. In normal
subjects, the buffy coat, which is comprised of white blood cells and platelets, is only minimally visible.

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4) Further investigations: depends on the suspected cause/s of anemia


based on the above tests, the history and physical examination findings.
➢ Suspected iron deficiency anemia:
✓ Serum ferritin
✓ Total iron binding capacity (TIBC)
𝐒𝐞𝐫𝐮𝐦 𝐈𝐫𝐨𝐧
✓ Transferrin saturation = 𝑋 100 %, TIBC = Total Iron binding
𝐓𝐈𝐁𝐂
capacity
Once iron deficiency is diagnosed:
✓ Stool for occult blood
✓ Stool microscopy for hookworm infestation
✓ Upper GI endoscopy or colonoscopy may be needed based on the
clinical suspicion.
➢ Suspected megaloblastic anemia:
✓ serum vitamin B12 level
✓ serum folate
➢ Suspected hemolytic anemia:
✓ Reticulocyte count or percentage bilirubin (indirect
hyperalbuminemia)
✓ LDH
✓ Coomb’s test

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Treatment
Non pharmacologic

➢ Transfusion of packed RBC:


➢ Indications for transfusion
✓ Hemoglobin < 7g/dl → for most hospitalized patients
▪ For ambulatory patients with chronic anemia transfusion may
not be needed even at hemoglobin is <7g/dl, unless the
patients have severe symptoms e.g. heart failure
✓ Hemoglobin < 8g/dl → for those with pre-existing chronic cardiac
disease, undergoing orthopedic or cardiac surgery
✓ In trauma or acutely bleeding patients
▪ Do not use hemoglobin or hematocrit for transfusion decision
as they are falsely elevated
▪ Hemodynamic status and ongoing nature of bleeding should
be used
▪ Whole blood is preferable if there is acute or ongoing
bleeding
✓ For the following patient’s higher hemoglobin target might be aimed
▪ Acute coronary syndrome
▪ Severe thrombocytopenia in hematology/hematology patients
➢ Nutritional support

Pharmacologic
➢ Depends on the underlying cause of anemia.
➢ Patients with anemia suspected due to primary bone marrow disease,
malignancy, autoimmune disease, GI bleeding, and unknown/unclear
cause should get further management at referral hospital level.

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13.1.1. Iron deficiency anemia (IDA)


➢ IDA is a common cause of anemia worldwide.
➢ The major causes of IDA are
✓ nutritional deficiency
✓ impaired absorption from the GI tract
✓ chronic blood loss from the GI or genitourinary tract caused by:
▪ hook worm infestation
▪ colonic cancer
▪ bleeding peptic ulcer or gastric cancer
▪ prolonged or excessive menstrual bleeding
▪ gynecologic malignancies etc.

Clinical features

➢ In addition to the general clinical features anemia (mentioned above),


chronic IDA might show unique clinical features.
✓ Pica: desire (craving) to eat unusual substances like soil, ice.
✓ Koilonychia: Thin, brittle nail with depressed (concave or spoon)
distal half.
✓ Cheilosis (also called angular cheilitis), Glossitis or angular
stomatitis: the tongue and angel the mouth inflamed and sore,
✓ Atrophic glossitis with loss of tongue papillae, which may be accompanied
by tongue pain or dry mouth
✓ Alopecia (rare) in especially severe cases
✓ Chlorosis (pale, faintly green complexion; extremely rare)
✓ Esophageal web, which may be accompanied by dysphagia (e.g.
Plummer-Vinson or Patterson-Kelly syndrome; rare)
✓ Restless legs syndrome (RLS), also called Willis-Ekbom disease
(WED)

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Investigations specific for IDA

➢ CBC: low Hg and hematocrit, low MCV, low MCH, and increased RDW.
➢ PM; microcystic hypochromic anemia (look at images above)
➢ Iron studies
✓ Serum Ferritin → usually low (it could be high in patients with
chronic inflammation or CKD in spite of iron deficiency)
✓ Serum iron → may be low or normal
✓ Total iron binding capacity (TIBC)→ usually high
𝐒𝐞𝐫𝐮𝐦 𝐈𝐫𝐨𝐧
✓ Transferrin saturation (TSAT) = 𝒙 𝟏𝟎𝟎 %; low (<20%)
𝐓𝐈𝐁𝐂
➢ Clinical evaluation and investigation to identify the possible cause of
bleeding
✓ Stool for ova of parasites
✓ Digital rectal examination
✓ Gynecologic examination
✓ Upper GI endoscopy and/or colonoscopy.

Treatment of IDA

➢ Treatment of the underlying cause


✓ The cause of the iron deficiency state should be identified and
treated.
➢ Oral iron (tablet): For at least 3 months following correction of the
anemia
✓ Ferrous sulfate, 325mg (has 65mg elemental iron), PO, TID. OR
✓ Ferrous fumarate, 325mg, (has 107 elemental iron), PO, BID. OR
✓ Ferrous gluconate, 325mg P.O. (39mg elemental iron), 1-2tabs, TID
➢ Oral iron (solutions/syrup): if the tablets are not tolerated or patient
preference
✓ Iron hydroxide polymaltose syrup (50mg/5ml of elemental iron), 10ml
PO, BID to TID. OR
✓ Ferrous gluconate syrup (24mg/5ml of elemental iron),15ml, PO TID.
OR
✓ Ferric ammonium citrate syrup (32.8mg/15ml of elemental iron), give
30ml, TID.

How to instruct oral iron intake?


➢ Preferably to be taken 2 hours before or 4 hours after meal.
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➢ If separating from food is difficult due to gastrointestinal side effects,


foods which significantly interfere with iron absorption should be avoided
when the iron is given e.g. milk, eggs, tea, and coffee.
➢ GI side effects are very common with oral iron administration. These
include epigastric pain, nausea or vomiting, constipation or diarrhea,
metallic taste.
➢ For patients who do not tolerate, they may be advised to take it with
meals, or to take a smaller dose, solutions or elixir forms.

Intravenous (IV) iron


➢ Indications for IV iron therapy
✓ Intolerance to oral iron therapy.
✓ Anemia secondary to CKD with a requirement for erythropoietin.
✓ No improvement in hemoglobin after 4 weeks of oral iron.
✓ Existence of conditions that interfere with absorption of iron from
the GI tract e.g. atrophic gastritis, gastrectomy, inflammatory bowel
disease
✓ Blood loss difficult to cope with oral iron therapy e.g. heavy
menstrual bleeding, bleeding telangiectasia
✓ Severe anemia during late 2nd or 3rd trimester of pregnancy

➢ IV iron administration
✓ For patients not on hemodialysis:
▪ Iron sucrose 200mg, IV, administer over 5 minutes, every 3
days for a total of 5 doses (a total of 1g).
• This dose is usually sufficient but if hemoglobin is not
corrected, additional doses can be given.
OR
▪ Iron sucrose 200mg diluted in 100ml NS; administer over 30
minutes.
✓ For patients on hemodialysis
▪ Iron sucrose 100mg, IV, over 2-5 minutes, given early during
dialysis sessions (within the first hour) until iron deficiency is
corrected. It needs to be given again, if iron deficiency
persists or recurs.

N.B Patients with iron deficiency anemia due to GI bleeding or unknown


cause or those with known reversible cause but refractory to iron therapy
should get further management at referral hospital level.
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13.1.2. Megaloblastic anemia


➢ Megaloblastic anemia is a morphologic term that describes abnormal red
blood cells with maturation defects; the red blood cells tend to be large.
➢ The major causes of megaloblastic anemia are vitamin B12 (Cobalamin)
and folate deficiency or a combination of both
➢ The pathologic process which results in megaloblastic anemia can also
result in leukopenia and thrombocytopenia. In case of Vitamin B12
deficiency the nervous system can be affected.

Causes of megaloblastic anemia

➢ Major causes of vitamin B12 deficiency


✓ Gastric origin (pernicious anemia, chronic atrophic gastritis)
✓ Small intestine malabsorption (chronic diarrhea from small
bowel/ileal pathologies)
✓ Strict vegetarians.
➢ Major causes of folate deficiency
✓ Poor nutritional status
✓ Increased demand during pregnancy and lactation
✓ Alcoholism
✓ Drugs: anti-epileptic drugs (phenytoin, phenobarbitone) or drugs
which affect Folate metabolism (Methotrexate, cotrimoxazole)
✓ Malabsorption
✓ Critical illness.

Clinical features

➢ In addition to the clinical features of anemia due to any other cause,


some clinical manifestations may suggest megaloblastic anemia.
✓ Glossitis (pain over the tongue with smooth, beefy red tongue)
✓ Angular cheilitis
✓ Jaundice
✓ Neurologic or neuropsychiatric manifestation: specific to vitamin B12
deficiency, but not folate deficiency
▪ Neuropathic pain in the lower limbs
▪ Decreased position sensation and gait disturbance
▪ Weakness of the lower extremities
▪ Irritability, depression, disorientation, dementia, frank psychosis
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Investigations for megaloblastic anemia


➢ CBC
✓ Anemia with high MCV (>100fl). When there is concomitant iron
deficiency, the MCV can be normal or low.
✓ Leukopenia and thrombocytopenia may also be found.
✓ Peripheral morphology: hyper segmentation of neutrophils, large
RBCs (macro-ovalocytes) → look at image above
✓ Hyper segmentation of neutrophils is defined as >5% of neutrophils
with 5 or more lobes.
➢ Bilirubin: Indirect hyperbilirubinemia
➢ Determination of the levels of vitamin B12 and Folate
✓ Serum vitamin B12 level
✓ Serum folate level
✓ RBC folate level: to be requested if serum folate level is normal
➢ Bone marrow aspiration: indications
✓ If the serum vitamin B12 and folate levels are normal but there is
strong clinical suspicion.
✓ When there is need to exclude other causes.
➢ Determining the cause of the deficiency: if the cause is not clinically
obvious, further wok up will be needed to identify the underlying cause.

Treatment

Treatment of vitamin B12 (Cobalamin) deficiency

➢ Cyanocobalamin (Vitamin B12) 1000µg (1mg), IM, to be given according


to the following schedule
✓ Every day for one week
✓ Every week for four weeks. If hemoglobin has not normalized,
continue weekly until it gets normal.
✓ If the underlying disorder persists, 1mg every month for the rest of
the patient's life.

Treatment of folate deficiency

➢ Folic acid, 1 to 5mg P.O., daily for 1-4 months, or until complete
hematologic recovery.
✓ Vitamin B12 level should be checked before giving folic acid alone;
as treatment with folic acid alone might worsen neurologic
manifestation of vitamin B12 deficiency.
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✓ If vitamin B12 can’t be checked, both Folic acid and vitamin B12
should be started at the same time.

Follow up of treatment response


✓ Symptomatic improvement
✓ Hemoglobin level

Patients with the following conditions need special care with hematology
and gastroenterology services
✓ If the underlying cause is not clinically obvious.
✓ If other causes of anemia/cytopenia cannot be excluded.
✓ Lack of response to the treatment provided.

13.2. Blood Transfusion


Indications for blood transfusion

Table; Thresholds for red blood cell transfusion in adults


Condition Hemoglobin threshold
for transfusion
Symptomatic patient (eg, myocardial ischemia) 10 g/dL
Hospitalized Preexisting coronary artery 8 g/dl
patient disease
Acute coronary syndromes 8 to 10 g/dL
ICU (hemodynamically stable) 7 g/dl
GI bleeding (hemodynamically 7 g/dL
stable)
Cardiac surgery 7.5 g/dL
Non-cardiac surgery 8 g/dL
Ambulatory Oncology patient in treatment 7 to 8 g/dl
outpatient Palliative care setting As needed for
symptoms; hospice
benefits may vary

➢ for Acute blood loss;


✓ Do not use hemoglobin or hematocrit for transfusion decision as they are
falsely elevated.
✓ Hemodynamic status and ongoing nature of bleeding should be used
✓ Whole blood is preferable if there is acute or ongoing bleeding

Practical points about transfusion


Nurses)
(especially for medical interns and ward
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➢ Consent → Informed consent for RBC transfusion should be obtained from the
intended recipient before all non-emergent administration of blood components.
According to AABB standards, elements of consent should include: a
description of the risks, benefits, and treatment alternatives; the opportunity for
the intended recipient to ask questions; and the right of the patient to accept
or refuse transfusion.
➢ After determining patient M.HCT, 1st send blood sample for cross match (if BG
&Rh is unknown, request ''BG& Rh with cross match'', if BG is known, write
pt's BG and Rh on request paper and request cross match)
➢ During transfusion, keep the Patient NPO, discontinue any medication (either
Parenteral or oral) until transfusion is finished
➢ Check the blood unit bag about expire date, major/minor reaction, compare the
bag number with the number written on transfusion request paper
➢ For patients who require blood that is warmed (e.g. those at risk of
hypothermia or autoimmune cold-induced hemolysis), put the blood out of the
cold box keep covered with clothes at the bedside, that raise the temperature
closer to body temperature are used. Avoid heating of the blood cells above
40°C, which will cause hemolysis
➢ Use Green IV cannula for transfusion
➢ Transfusion one unit should be completed within 3 hours but not less than one
hour (faster rate may be needed in acute blood loss)
✓ Infusion rate →Suggested rates for adults are 20 to 40 drops per minute
for the first 15 minutes and then as rapidly as tolerated;
✓ The complete infusion should not exceed 4 hours. However, slower rates
of infusion (possibly combined with administration of a smaller unit to
comply with the four-hour infusion requirement) and/or the administration
of diuretics may be indicated for patients who are predisposed to
circulatory overload.
✓ the dose of transfusion for Neonates is 20ml/kg, less than 7 days old
over 3hr (Acute blood loss - Whole blood 20ml/kg less than 7 days old
over 1 hour.)
➢ follow with transfusion follow up sheet
➢ finally, document ‘’transfusion completed without complication at ''X'' DLT/NLT’’
➢ Blood transfusion follow up sheet (include blood component E.g. Whole blood
transfussion follow up sheet)

Blood transfusion follow up sheet


Date time BP PR RR T0 SaO2 JVP S3 Liver Basal itching rash Input output sign
gallop size rales

Doctor Following the patient Nurse following the patient


Name………………………….
Sign……………………………
Date………………………….
Name……………………….
Sign…………………………
Date………………………….
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➢ Check post transfusion M.HCT of last transfusion (the usual trend in our set
up is after 8hour)
✓ UpToDate 2018 says ‘’The post-transfusion hemoglobin level may be
accurately measured as early as 15 minutes following transfusion, as long
as the patient is not actively bleeding. This practice is based on studies
showing a high degree of concordance between values measured 15
minutes after the transfusion versus longer intervals’’.
✓ Each unit of packed red blood cells (RBCs) contains approximately 200
mL of red cells and, in an adult, will raise the hematocrit by roughly 3 %
points unless there is continued bleeding.
➢ Within one day, it is better not to transfuse more than 3 units of blood unless
there is life threating condition (e.g. massive bleeding, active and uncontrolled
Upper GI bleeding)
➢ Observation following transfusion
✓ In addition to observing the patient during transfusion, continue observing
for 15 to 30 minutes post-transfusion.

Complications of Transfusion

Complications from a single transfusion

➢ ABO incompatibility
✓ Clinical presentation=hematuria, bilateral flank pain, fever, chills, rigor,
oliguria (ATN)
✓ Rx=stop blood transfusion. send it to blood bank & recheck
▪ Repeat coagulation profile
▪ Iv fluids, monitor UOP, U/A for Hgb
▪ Diuretic- furosemide
➢ Minor incompatibility reaction
✓ Due to extra vascular hemolysis (mild, occur in 2-21days)
✓ Clinical presentation-fever, malaise & jaundice
✓ Rx-supportive
➢ Febrile reaction
✓ Due to sensitization to WBCs or platelets
✓ increase temperature but no hemolysis
✓ Use of 20-40mm filter or leukocyte depleted blood avoids it.
➢ Allergic reaction
✓ Due to allergy to plasma products
✓ Clinical presentation - chills, rigor & rash
✓ Rx- antihistamines
➢ Embolism
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✓ Although air embolism has been reported as a complication, healthy


individuals can tolerate large amounts of air injected intravenously at a
rapid rate.
✓ The normal adult can tolerate an embolism of 200 mL of air.
✓ Smaller amounts, however, can cause alarming signs.
✓ Manifestations of venous air embolism include a rise in venous pressure,
cyanosis, a "mill wheel murmur", tachycardia, hypotension, and syncope.
✓ Treatment - consist of placing the patient on the left side in a head down
position with the feet up.
✓ Arterial air embolism may be visible in the retinal vessels or as blood
flows from transected vessels.
✓ Plastic tubes used for transfusion can break off within a vein and
embolize into the right atrium or pulmonary artery.
✓ Embolized catheters have been successfully removed.

➢ Thrombophlebitis
✓ Prolonged infusions into a peripheral vein are associated with venous
thrombosis.
✓ Intravenous infusions that last more than 8 hours are more likely to be
followed by thrombophlebitis, with an increased incidence in the lower
limbs.
✓ Treatment consists of discontinuation of the infusion and the application
locally of warm moist compresses.
✓ Embolization from superficial thrombophlebitis or venous thrombosis is
extremely rare.
➢ Over transfusion and Pulmonary Edema
✓ Volume overload is typically a concern in the elderly, small children, and
those with compromised cardiac function.
✓ Overloading the circulation is an avoidable complication.
✓ It can occur with rapid infusion of blood, plasma expanders, and other
fluids, particularly in patients with heart disease.
✓ To prevent the complication, the central venous pressure should be
measured whenever large amounts of fluid are administered.
✓ Circulatory overload is manifested by a rise in venous pressure, dyspnea,
and cough.
✓ Rales can generally be heard at the lung bases.
✓ Treatment consists of diuresis, placing the patient in a sitting position,
and, occasionally, venesection.

➢ TRALI (transfusion-related acute lung injury)


✓ It is sometimes seen after transfusion and is characterized as mild to life-
threatening.
✓ Noncardiogenic pulmonary edema is often accompanied by fever, rigors,
and a "white out" chest x-ray.
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✓ Treatment is discontinuation of any transfusion, notification of the


transfusion service, and intensive pulmonary support, sometimes including
intubation.
✓ This type of pulmonary edema does not respond to diuretics and is
thought to be caused by infused donor antigranulocyte or anticlass I or II
MHC antibodies.
➢ Infection
✓ Bacterial infection
▪ contamination of infused blood is rare and can be acquired from
contaminated collection bags or poor cleaning of the donor's skin.
▪ Gram-negative organisms, especially coliform and Pseudomonas
species, which are capable of growth at 40C (39.20F), are the most
common cause.
▪ Clinical manifestations include
• fever, chills, abdominal cramps, vomiting, and diarrhea.
• There may be hemorrhagic manifestations and increased
bleeding.
▪ If the diagnosis is suspected, the transfusion should be
discontinued and the blood cultured.
▪ Emergency treatment includes oxygen, adrenergic blocking agents,
and antibiotics.
✓ Hepatitis, HIV, malaria, syphilis.
▪ It is mandatory to screen the blood for these diseases before
transfusion.

Complications from massive transfusion


➢ Massive transfusion, historically defined as the replacement by transfusion of
10 units of red cells in 24 hours, is a response to massive and uncontrolled
hemorrhage. With more rapid and effective therapy, alternative definitions such
as 3 units over 1 hour are more sensitive in identifying patients needing rapid
issue of blood products for serious injuries because of uncontrolled hemorrhage
➢ Such transfusion episodes are associated with a number of hemostatic and
metabolic complications.
➢ Massive transfusion involves the selection of the appropriate amounts and
types of blood components to be administered, and requires consideration of a
number of issues including volume status, tissue oxygenation, management of
bleeding and coagulation abnormalities, as well as changes in ionized calcium,
potassium, and acid-base balance.

Complications include;
➢ Allergic and immune transfusion reactions can occur in any patient, and are
more common in multiply-transfused patients. including TRALI
➢ Coagulopathy
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➢ Hyperkalaemia/ Hypokalaemia
✓ Hyperkalemia from potassium released from RBCs during blood bank
storage is primarily a concern in massive transfusion, impaired renal
function, and infants/newborns.
➢ Hypothermia
➢ Iron overload
✓ Iron overload becomes a concern after a large number of transfusions for
chronic anemia.
✓ Each transfused unit of RBCs contains 250 mg of elemental iron

Blood components
➢ Banked Whole Blood
✓ With the new preservatives, the shelf life has been extended to 40 ± 5
days.
✓ At least 70% of the transfused erythrocytes remain in the circulation for
24 hours after transfusion and are viable.
✓ The hemolysis that occurs during storage is insignificant.
✓ Preferred for anemia with volume depletion

➢ Fresh Whole Blood


✓ Refers to blood that is administered within 24 hours of its donation and is
rarely indicated.
✓ Because of the time required for testing for infectious disease, it must be
administered untested.
✓ One unit of platelet concentrate has more viable platelets than 1 unit of
fresh blood.
✓ Fresh whole blood is a poor source of platelets and factor VIII.
✓ Preferred for neonates

➢ Packed RBC (Red Blood Cells)


✓ The major difference between packed RBCs and whole blood is the
volume of plasma present in the unit of blood.
✓ Patients with chronic anemia should be transfused with Packed RBC
since volume replacement is not required.
✓ Furthermore, since the patient already has an expanded blood volume to
compensate for the anemia, circulatory overload may be a risk if plasma
is also given.
✓ Cells are spun down and concentrated.
✓ Each unit = 330 ml (Hct=50 - 70%)
✓ Packed RBCs are stored in a SAG-M solution (saline–adenine–
glucose–mannitol) to increase shelf-life to 5 weeks at 2 - 60C. 1213
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➢ Fresh-frozen plasma (FFP)


✓ It is rich in coagulation factors & removed from fresh blood and stored at
-40 to -500C with a 2 years shelf-life.
✓ It is the first-line therapy in the treatment of coagulopathic hemorrhage.

➢ Platelet
✓ Pooled platelet concentrate containing about 250 x109 cells/L.
✓ Platelets are stored on a special agitator at 20 - 24 0C and have a shelf-
life of only 5 days.
➢ Cryoprecipitate
✓ It is precipitate of FFP
✓ Rich in factor VIII and fibrinogen
✓ Stored at -300C with a 2-year shelf-life
✓ Given in low-fibrinogen states or in factor VIII deficiency

➢ Prothrombin complex concentrate


✓ Contain factors II, IX and X (factor VII may be included)
✓ Indicated for the emergency reversal of anti-coagulant (warfarin) therapy in
uncontrolled haemorrhage

13.3. Thrombocytopenia
13.3.1. Thrombocytopenia in hospitalized patients

➢ Thrombocytopenia is defined as a platelet count less than 150 × 103


per μl.
➢ The degree of thrombocytopenia can be divided from mild to severe.
However, these numbers should be interpreted cautiously as severity
definitions may vary.
✓ Mild = 100,000 to 150,000/ μl
✓ Moderate = 50,000 to 99,000/ μl
✓ Severe <50,000/ μl
➢ The safest platelet count at which bleeding is unlikely to occur is not
precisely known. It also varies significantly with the underlying cause.
✓ Surgical bleeding risk is high when platelet counts <50,000/ μl.
(<100,000/ μl for neurosurgery or major cardiac or orthopedic
surgery).
✓ Severe spontaneous bleeding: the risk is high when platelet counts
<20,000 - 30,000/ μl
➢ Thrombocytopenia is not only a risk for bleeding but it can also be a
manifestation of life threatening thrombotic disorders.
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✓ Common clinical disorders which can cause thrombosis and


thrombocytopenia at same time
▪ DIC (disseminated intravascular coagulation)
▪ HIT (Heparin induced thrombocytopenia)
▪ TTP/HUS (thrombotic thrombocytopenic purpura/hemolytic
uremic syndrome
▪ APS (antiphospholipid antibody syndrome)
➢ Thrombocytopenia is a common in hospitalized patients. The risk is even
much higher in critically ill patients.
➢ The causes of thrombocytopenia in hospitalized patients are numerous
causing diagnostic challenges.

The major causes thrombocytopenia in hospitalized patients


➢ Spurious thrombocytopenia (Pseudothrombocytopenia)
➢ Hemodilution: massive transfusion or crystalloid resuscitation
➢ Sepsis
➢ Malaria
➢ DIC
➢ Heparin induced thrombocytopenia (HIT)
➢ Drug induced thrombocytopenia
➢ Pregnancy complications: gestational thrombocytopenia, preeclampsia,
HELLP syndrome, acute fatty liver of pregnancy, DIC
➢ Chronic liver disease and hypersplenism.
➢ Alcohol or nutritional deficiencies (Vitamin B12 and/or folate deficiency)
➢ Thrombotic microangiopathies (TMA): TTP/HUS (Thrombotic
thrombocytopenic purpura/Hemolytic uremic syndrome), catastrophic APS
➢ Autoimmune (Rheumatologic) diseases: SLE
➢ Post transfusion purpura
➢ Viral infections: HIV, Hepatitis C

Clinical evaluation of thrombocytopenia in acutely ill hospitalized


patients
➢ Confirmation of the thrombocytopenia:
✓ Platelet clumping is a laboratory artifact than cause spurious
thrombocytopenia.
✓ Repeat CBC
✓ Using EDTA-free tubes (e.g. heparin or citrate tubes)
✓ Do peripheral morphology to see if the thrombocytopenia is genuine
or not.
➢ Detailed clinical history and physical examination: Evaluate if the
underlying disease (e.g. sepsis) is a possible cause
➢ Evaluating for life threatening causes
✓ Several malaria; peripheral blood smear ( thin and thick)
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✓ HIT: History of heparin administration, date of administration, the


presence of thrombosis, the degree of decrease in platelet count
from baseline in percentage.
✓ TTP/HUS: Peripheral morphology for fragmented RBCS, serum LDH,
BUN and serum creatinine, urinalysis
✓ Acute leukemia: other cell line, peripheral smear and bone marrow
aspiration
✓ DIC: determine PT(INR) and PTT, peripheral smear
✓ Transfusion history: transfusion associated pupura
➢ Detailed drug history
➢ Evaluate for other common causes
✓ Liver disease: clinical evaluation and liver function tests
✓ Viral causes: HIV and HCV screening
✓ Alcohol intake
✓ Nutritional status: Peripheral blood smear to see evidence of
megaloblastic anemia.

Treatment

➢ Treatment of the underlying cause: is the main stay of management in


acutely ill hospitalized patients with thrombocytopenia.
➢ Platelet transfusion: Indications
✓ Active bleeding: If there is active bleeding and the platelet count
<50,000/ μl.
✓ Prophylactic platelet transfusion: In patients without active bleeding
prophylactic platelet transfusion should be avoided unless the
platelets count < 10,000/ μl.
➢ Hold antiplatelet agents and anticoagulants: if platelets count < 30,000/
μl.

13.3.2. Immune/Idiopathic Thrombocytopenic Purpura


(ITP)

➢ ITP is an acquired autoimmune disorder characterized by a low platelet


count resulting from platelet destruction
➢ Other conditions which can cause immune related thrombocytopenia
should be excluded before the diagnosis ITP such as;
✓ HIV
✓ HCV infection
✓ H. Pylori infection
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✓ SLE
✓ CLL
➢ Hence, ITP is a diagnosis of exclusion.
➢ Patients with other associated conditions (e.g. other autoimmune
diseases) are described as having secondary immune thrombocytopenia.
➢ The incidence of ITP is higher in children than adults. Preceding viral
infections are common precipitants of ITP in children.
➢ Classification of ITP based on the duration of the disease
✓ Newly diagnosed ITP: ITP duration of less than 3 months
✓ Persistent ITP: ITP duration of 3-12 months
✓ Chronic ITP: ITP duration of more than12 months

Clinical features
➢ Asymptomatic: The vast majority of patients with ITP are not
symptomatic, unless the platelet is very low.
➢ Bleeding mucocutaneous bleeding also called ―Platelet-type‖ bleeding )
✓ Petechiae, purpura, and easy brusing.
✓ Epistaxis, gingival bleeding, menorrhagia, gross hematuria
✓ Gastrointestinal bleeding: bloody vomitus, bleeding peer rectum
✓ Intracranial bleeding: headache, change in mental status or focal
neurologic deficit
✓ Signs of anemia: Pallor, tachycardia, low blood pressure or postural
drop in blood pressure (if massive bleeding)

Pictures; Petechiae in a man with immune thrombocytopenia (ITP).


(A) Dense, cutaneous petechiae on the foot and ankle. There are no petechiae on the
sole of his foot, a site at which the vessels are protected by the strong subcutaneous
tissue.
(B) Occasional petechiae on the patient's face and large, bullous hemorrhages on the
buccal mucosa, which are related to the lack of vessel protection by the submucosal
tissue. Similar petechiae and hemorrhagic bullae can be seen in patients with
thrombocytopenia of any cause.

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Investigations and diagnosis


➢ The diagnosis of ITP is made based on clinical grounds after exclusion
of other causes of thrombocytopenia.
➢ A platelet count of < 100,000/µl is needed for consideration of the
diagnosis.
➢ Peripheral blood smear: is required to exclude other causes of
thrombocytopenia and to confirm the presence of true thrombocytopenia.
➢ Serologies: HIV and HCV (hepatitis C Virus) serology tests are needed
in all patients
➢ H. Pyolri test: is indicated in all patients.
➢ ANA might be needed is there is a clinical evidence of SLE.
➢ TSH: autoimmune thyroid diseases are common in patients with ITP.
➢ Bone marrow aspiration/biopsy:
✓ It is not generally indicated for the diagnosis of ITP
✓ It is indicated in individuals with atypical features such as B-
symptoms, lymphadenopathy, splenomegaly, unexplained leukocyte
abnormalities or unexplained anemia, and age > 60 years.
✓ It is also indicated before splenectomy

Treatment

➢ Increase the platelet count to a safe level to prevent major bleeding.


Safe level of platelet is >30,000/µl. N.B.: The aim of ITP treatment is
not to bring the platelet to normal levels

Non pharmacologic

➢ Emergency platelet transfusion


✓ Generally, platelet transfusion should be avoided.
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✓ Indication for platelet transfusion: life-threatening bleeding only.


✓ If platelet transfusion is indicated, intravenous steroids should be
started immediately.
➢ Splenectomy: is an option of treatment for patients who have
corticosteroid refractory or dependent disease.

Pharmacologic

➢ Not all patients with ITP need treatment. Those with no indications to
treatment should be followed with CBC and clinical assessment of
bleeding. The patients should be given enough information about
bleeding.
➢ Indications for treatment
✓ Platelet count < 30,000/µl, irrespective of bleeding status.
✓ Platelet count > 30,000/µl and significant bleeding (other than minor
mucocutaneous bleeding)
➢ First line: Corticosteroids
✓ Dexamethasone, 40mg, oral or IV, daily for 04 consecutive days
with no tapering. Repeat this 4 day cycles every 2-4 weeks for 4-6
cycles.
OR
✓ Prednisolone, 1mg/kg for 1-2 weeks, if there is response taper over
a period of six weeks or less.
▪ Typical tapering regimen: After response, reduce by 10
mg/week until 0.5 mg/kg is reached; then taper by 5mg/week.
➢ Treatment response
✓ Response: is defined if there is a platelet count >30,000/µl and at
least doubling from the baseline both must be fulfilled).
✓ Durable response: if there is response persisting up to 6 months.
✓ Remission: is defined if platelet count is >100,000//µl for >12
months
✓ Steroid dependent: Ongoing need for continuous prednisolone > 5
mg/d (or equivalent) or frequent courses of corticosteroids needed
to keep a platelet count >30,000/µl
➢ Alternative treatments:
✓ Intravenous immunoglobulin (IVIg)
✓ Anti-D
✓ Rituximab
✓ Splenectomy Note: alternative treatments are indicated for steroid
resistance or dependent, special population with specific indications
and these treatments should only be provided by hematologist or
specialist who has experience in using these agents.

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13.4. VTE (DVT and PTE)


Dr. Mulualem. G, Dr. Robel. D

Venous thromboembolic disease (VTE) refers thrombosis (blood clot) that occurs in
the deep veins, called deep vein thrombosis (DVT), or embolization in to
pulmonary arterial circulation called pulmonary embolism (PE).
One of the common sites for thrombus formation in the deep veins of the legs or
pelvis. This is known as deep vein thrombosis, or DVT.
The thrombus can dislodge and travel in the blood, particularly to the pulmonary
arteries. This is known as pulmonary embolism, or PE.
The term 'VTE' includes both DVT and PE.
VTE covers a spectrum ranging from asymptomatic calf vein thrombosis to
symptomatic DVT or PE.
Pulmonary thromboembolism (PE) is occlusion of pulmonary arteries by embolus
dislodged from thrombus at a distant site, mostly deep vein of the lower limb.
Massive PE is with a SBP of <90 mm Hg for >15 minutes, or <100 mm Hg in a
patient with a history of hypertension, or a >40% reduction in baseline SBP.
Sub massive PE is characterized by a normal or near-normal BP with right
ventricular dysfunction or myocardial necrosis
Pulmonary embolism can fatal, if it is not detected and treated early.
Non-fatal VTE can cause serious long-term complications

Risk factors for VTE

◼ Immobility
◼ Previous VTE
◼ Major surgery, e.g. orthopedic, abdominal and pelvic surgery
◼ Trauma → especially involving the pelvis and lower limbs
◼ Pregnancy and postpartum state
◼ Contraceptive pill use, hormone replacement therapy (HRT)
◼ Cancer
◼ Obesity
◼ Medical conditions such as;
A. Heart Failure
B. Nephrotic syndrome or CKD
C. HTN
D. COPD
E. SLE
F. IBD
◼ Inherited disorders causing hypercoagulability

Pathogenesis
A major theory described the pathogenesis of VTE is called Virchow's triad, which
occurs as a result of: mnemonic → EBC
❖ Endothelial Injury
❖ Blood flow alterations (Stasis)
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❖ Coagulopathy → Alterations in the Constituents of Blood

Clinical features
◼ VTE mimics other illnesses, and PE is known as "the Great Masquerader,"
making diagnosis difficult.
◼ Occult PE is especially hard to detect when it occurs concomitantly with overt
Heart Failure or Pneumonia.
◼ In evaluating patients with possible VTE, the initial task is to decide on the
clinical likelihood of the disorder.
◼ VTE can cause death from PE or, among survivors, Chronic Thromboembolic
Pulmonary Hypertension and Post thrombotic Syndrome/chronic venous
insufficiency/may occur.

DVT

For patients who have DVT, the most common history is


❖ A cramp in the lower calf that persists for several days and becomes more
uncomfortable as time progresses.
Physical findings, if present at all, may consist only of mild palpation discomfort in
the lower calf.
Massive DVT is much easier to recognize.
❖ The patient presents with marked thigh swelling and tenderness during palpation
of the common femoral vein.
❖ In extreme cases, patients are unable to walk or may require a cane, crutches,
or a walker.

PE

For patients who have PE, the most common history is unexplained
breathlessness.
❖ Dyspnea is the most common symptom of PE, and Tachypnea is the most
common sign.
Dyspnea, Syncope, Hypotension, or Cyanosis indicates a Massive PE, Whereas
Pleuritic Pain, Cough, or Hemoptysis often suggests a Small Embolism situated
distally near the pleura.
On physical examination,
❖ Young and previously healthy individuals may appear anxious
❖ But otherwise seem well, even with an anatomically large PE.
The presence of pulmonary infarction usually indicates a small PE
❖ But one that is exquisitely painful because it lodges peripherally, near the
innervation of pleural nerves.

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Pleuritic Chest Pain is more common with small, peripheral emboli. However,
larger, more central PEs can occur concomitantly with peripheral pulmonary
infarction.
They may have dyspnea only with moderate exertion.
They often lack "classic" signs such as
❖ Tachycardia, Low-grade Fever, Neck Vein Distention, and an Accentuated
Pulmonic Component of S2.
Sometimes paradoxical bradycardia occurs.

Investigations and diagnosis of DVT


◼ Routine laboratory tests for baseline (e.g. CBC, LFT, coagulation studies)
A. But they are not useful diagnostically.
◼ Imaging Modalities include:
A. Compressive Ultrasonography (with Doppler)
Diagnostic test of choice
Sensitivity and specificity of > 95% for the diagnosis of DVT.
However, about 50% of patients with PE have no imaging evidence
of DVT on U/
Features of venous thrombosis on Compressive U/S:
A) Lack of Compressibility
B) Direct thrombus visualization
C) Abnormal Doppler flow
B. MR Venography (contrast enhanced)
C. Chest CT(CTPA)
◼ Supportive Investigative modalities include;
A. Cardiac biomarkers
B. CXR
C. ECG.
D. Echo
E. D- dimers
D dimers are a breakdown of Fibrin by Plasmin. The normal level is
< 500(negative result).
Elevation of D-dimer indicates endogenous although often clinically
Ineffective thrombolysis.
The Sensitivity of the D-dimer is >80% for DVT (Including Isolated
Calf DVT) and >95% for PE
But are not specific are more applicable for ‘ruling out’ VTE.

Investigations and diagnosis of PTE

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➢ CXR - normal or can have unilateral basilar atelectasis, Pleural based opacity
(Hampton’s hump), dilated pulmonary artery (Pala’s sign), unilateral lung
oligemia (Westermark’s sign)
➢ ECG: tachycardia, non-specific ST and T wave changes in the anterior leads
(V1-V4), S1Q3T3 pattern, P Pulmonale and incomplete or complete right
bundle branch block.
➢ Echo: Severely dilated RV with severely reduced systolic function, akinesia of
the mid free wall but normal motion at the apex of the right ventricle,
Paradoxical RV septal systolic motion, Pulmonary artery systolic pressure >30
mmHg, Dilated IVC with lack of respiratory collapse, visualization of clot etc…
➢ Spiral CT: is diagnostic in 98 percent of patients with PE.
➢ Doppler ultrasound: to look for DVT as supportive evidence

Classification

◼ Patients with Massive PE present with


A. Systemic Arterial Hypotension and
B. Usually have anatomically widespread thromboembolism.
◼ Those with Sub massive PE have
A. RV hypokinesis on Echocardiography but
B. Normal Systemic Arterial Pressure.
◼ Patients with Low risk PE have both
A. Normal right heart function and
B. Normal systemic arterial pressure.
They have an excellent prognosis with adequate anticoagulation.

Modified Wells score


◼ In evaluating patients with possible VTE, the initial task is to decide the
clinical likelihood of the condition.
◼ There are different clinical criteria to determine the probability of VTE (Pretest
Probability) of which Wells Score is commonly used.
◼ The modified Wells score classifies patients suspected of having VTE into two
levels as ‘Likely’ and ‘Unlikely’

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Interpretations and actions to be done in Wells score (for best setup, not applicable in
our setup)

DVT likely (Wells score ≥ 2 points):


do a proximal leg vein ultrasound scan, with the result available within 4 hours if possible
If scan is positive, start mx for DVT.
If initial scan is negative or if it’s impossible to get scan results in 4 hours, do a D-dimer test and
start interim therapeutic anticoagulation.
If scan is negative and D dimer is positive, stop interim anticoagulation and offer a repeat scan at
6-8 days
If both scan and D dimer are negative, look for other potential ddx
If the scan is positive, continue anticoagulation

DVT is unlikely (Wells score ≤ 1 point), offer a D dimer test.


◼ If the D-dimer test result is negative, think about other differentials
◼ If the D-dimer test result is positive, offer a proximal leg vein ultrasound scan, with the result
available within 4 hours if possible or interim therapeutic anticoagulation, and a proximal leg
vein ultrasound scan with the result available within 24 hours.
◼ If the proximal leg vein ultrasound scan is positive, continue management for DVT
◼ If the proximal leg vein ultrasound scan is negative, look for other differentials.

PE Likely (Wells score > 4 points):


◼ offer a computed tomography pulmonary angiogram (CTPA) immediately
◼ If CTPA is positive, start anticoagulation
◼ If CTPA is negative but DVT is still suspected, do CUS
◼ If CTPA is negative and DVT is not suspected, look for another differential

PE Unlikely (Wells score ≤ 4 points):


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◼ offer a D-dimer test with the result available within 4 hours if possible
◼ if the D-dimer test result cannot be obtained within 4 hours, offer interim therapeutic
anticoagulation while awaiting the result
◼ If the D-dimer test result is positive, continue mx for PE
◼ If the D dimer result is negative stop interim therapeutic anticoagulation think about alternative
diagnoses.

Management of VTE
◼ The management of VTE is done in three different phases:
A. Initial Management
B. Primary Treatment
C. Secondary prevention

Initial management (first 5-21days)

◼ aim is to prevent thrombus extension, embolization and bleeding.


◼ The main modality of mgt is anticoagulation.
◼ Choice of agents:
A. LMWH
B. Fondaparinux
C. Direct Oral Anticoagulants (rivaroxaban, apixaban)
D. UFH

Primary treatment (3-6 months)

◼ refers to the minimal length of time initial venous thromboembolism should be


treated.

Secondary prevention (Indefinite)

◼ long term anticoagulation with the intent to prevent VTE recurrence.

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Non pharmacologic management


◼ Elastic compression stockings after anticoagulation
◼ Early ambulation after proper anticoagulation

Pharmacologic
I. Acute treatment

First line

✓ UFH, 5000 Units, IV, bolus; then 250 Units/Kg/dose, Sc, BID or 17,500 Units
SC, BID (for an average adult) until two consecutive INR values become
therapeutic (2-3) or
✓ Enoxaparin 1mg/kg, SC, BID, until two consecutive INR values become
therapeutic (2-3)
o Enoxaparin dose should be reduced or it should be avoided in
patients with advanced CKD (GFR<30ml/min)
PLUS
✓ Warfarin (starting simultaneously with heparin)
o Starting dose: 5 mg, P.O., daily with regular dose adjustment and
monitoring of INR until target of 2 - 3 is attained.
o Add warfarin 5mg, PO, on day 1 or 2 of UFH, daily for 2 days, check
INR after 2 days and adjust based on the result
o Overlap warfarin and UFH for at least 5 days until desired INR/INR=2-
3/ maintained for 24hr then discontinue UFH.

N.B
➢ The full effect of warfarin requires at least 5 days, even if the prothrombin
time, used for monitoring, becomes elevated more rapidly.
➢ If warfarin is initiated as monotherapy during an acute thrombotic illness, a
paradoxical exacerbation of hypercoagulability increases the likelihood of
thrombosis.
➢ Overlapping UFH or LMWH with warfarin for at least 5 days will nullify the
early procoagulant effect of warfarin.

Alternatives

✓ Rivaroxaban 15mg PO BID X 3 weeks


o Rivaroxaban should be avoided in patients with advanced CKD
(GFR<30ml/min)

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Management of warfarin-associated bleeding or


supratherapeutic INR
(See the table below)

At least half of the bleeding complications with warfarin occur When the INR
exceeds the therapeutic range (which is 2 to 3).

INR >9 without bleeding


◼ warfarin therapy should be held and give oral vitamin K, 2.5 to 5 mg
◼ Nonbleeding patients should not be given PCC or FFP solely to correct a
supratherapeutic INR, as these products have associated risks.
◼ The INR is monitored daily or every other day, and warfarin is resumed at a
lower dose once the INR in the therapeutic range.

INR 5 to 9 without bleeding


◼ warfarin is held temporarily (e.g. one or two doses) with or without
administration of a small dose of oral vitamin K (e.g. 1 to 2.5 mg).
◼ Warfarin generally is resumed at a lower dose once the INR is in the
therapeutic range.

INR <5 without bleeding


◼ One or more doses of warfarin may be omitted and/or the dose is reduced
slightly.
◼ If the INR elevation is minimal and/or expected to be transient, no dose
reduction may be necessary.
◼ Additional therapies such as vitamin K are not indicated in this setting.

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HAS-BLED bleeding risk score, in patients with atrial fibrillation receiving


warfarin

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II. Chronic treatment


◼ Warfarin, dose adjusted to achieve target INR of 2 -3 OR
◼ Rivaroxaban 20mg po, daily.

III. Duration of anticoagulation


◼ Patients with VTE due to a reversible/time-limited risk factor (e.g. surgery): 3-
6 months.
◼ Patients with first episode of idiopathic/unprovoked VTE: 3-6 months
◼ Most patients with advanced malignancy should be treated indefinitely or until
the cancer resolve
◼ Patients with recurrent idiopathic/unprovoked VTE: indefinitely

Management of VTE in special population

1. Pregnancy:

◼ Adjusted-dose subcutaneous LMW heparin is the preferred agent for initial


and long-term anticoagulation in pregnant women with acute DVT.
◼ UFH is alternatives to LMW heparin.
◼ Warfarin can cause embryopathy when administered between 6 and 12
weeks.

A. Cancer:

◼ Treatment of DVT is associated with higher morbidity, due to higher than


usual rates of both recurrent thrombosis and anticoagulant-associated
bleeding.
◼ LMWHs are the preferred agents for the anticoagulation in those with
preserved renal function.

Management of PTE
➢ Risk factor assessment: clinical assessment using modified Wells criteria (PE likely if
score > 4)
Principle of management
➢ Patients usually die from cardio respiratory failure Early detection of nonspecific
management and addressing hypoxia and hemodynamic instability is mandatory
Restricted fluid challenge for patients with PE and early initiation of
vasopressors (preferably Norepinephrine) for those with no response.
➢ Early anticoagulation should be initiated as soon as possible and thrombolytics
should be initialed for those with massive PE and without contraindication
➢ Administer oxygen for hypoxaemia
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➢ Empiric anticoagulation:
➢ Mechanical ventilator

13.4.1. VTE prophylaxis


◼ VTE is a major cause of death and mortality among patients admitted for
both surgery and acute medical care.
◼ The major risk factors that predispose patients for the development of VTE
are well known.
◼ Provision of prophylaxis for hospitalized patients who are at high risk of VTE
is an established strategy which decreases death and morbidity.
◼ The major risk of pharmacologic prophylaxis with anticoagulants or
antiplatelets is increased risk of bleeding; hence, the risk of bleeding should
also be assessed along with assessment for the risk of VTE.

VTE prophylaxis in surgical patients

◼ Risk assessment for VTE in surgical patients mainly depends on the type of
surgery and the bleeding risk associated with the procedure.

Type of surgery Need for VTE Recommended thromboprophylaxis Duration


prophylaxis
Major orthopedic surgery Yes First line 2-4 weeks
Enoxaparin 40mg, Sc, daily Or Starting 12 hours
Rivaroxaban 10mg, po/day after surgery
Second line
UFH, 5,000 IU SC, BID
Major general surgery Yes Enoxaparin (same dose as above) Or 2-4 weeks
UFH (same dose as above)
Major neurosurgery No
Laparoscopic No
cholecystectomy
Transurethral No
prostatectomy or radical
prostatectomy
Cardiac or vascular Yes Enoxaparin (same dose as above) Or
surgery UFH (same dose as above)
Major trauma Yes
Major gynecologic Yes

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VTE prophylaxis in medical patients

◼ The major risk factors for VTE among medical patients hospitalized for acute
care
A. ICU admission (critical care),
B. Stroke with lower limb paralysis
C. Active cancer
D. Known thrombophilia (inherited or acquired)
E. Prolonged immobilization ≥ 3days
F. Heart failure
G. Acute respiratory failure
H. Sepsis
I. Chronic inflammatory diseases.
◼ The presence of one or more risk factors puts the patient at increased risk.
◼ The higher the number of the risk factors, the higher the risk of developing
VTE.
◼ Although not widely validated, there are a few risk assessment models
designed to help clinicians make a better risk assessment and decide on the
provision of prophylaxis.
◼ We the use of one of the risk assessments tools: IMPROVE-VTE risk
assessment model (see the table below).
◼ Before starting prophylactic anticoagulation assessment of the risk of bleeding
is as important as assessing the risk of VTE. Use the IMPROVE-VTE
bleeding risk assessment tool given below.
◼ The major contraindications for pharmacologic prophylaxis
A. Active bleeding
B. Intracranial hemorrhage of any cause
C. Thrombocytopenia (<50,000 or <100,000 with additional risk factor)
D. Major surgery planned in the coming 12 hours.
◼ If a patient has a high risk of bleeding based on clinical evaluation or using
the IMPROVE VTE bleeding risk assessment, prophylactic anticoagulation
should be avoided.
◼ Options for pharmacologic prophylaxis
A. Enoxaparin 40mg, SC, daily for the time of hospitalization during acute illness
OR
B. UFH, 5,000 IU, SC, BID for the time of hospitalization during acute illness 3 -
4 weeks

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Table. IMPROVE VTE risk assessment model


No. Risk factors at admission Points
Known thrombophilia 3
Previous VTE 3
Malignancy (Active or treated in the last 6 months) 1
Current lower limb paralysis 2
Immobility > 7 days 1
Age >60 years 1
ICU stay 1
Score 0-1 = low risk, no need for prophylaxis
Score 2 -3 = moderate risk, needs prophylaxis
Score > 4 = High risk, needs prophylaxis
Any score 2 or above = Needs for prophylaxis

Table: IMPROVE VTE Bleeding risk assessment


No. Risk factor Score
Active GI bleeding 4.5
Bleeding in the past three months before admission 4
Platelet count <50,000 4
Age > 85 3.5
Hepatic failure (INR>1.5) 2.5
Severe Renal Failure (GFR <30ml/min) 2.5
Liver failure (INR>1.5) 2.5
Any ICU admission 2.5
Central venous catheter 2
Rheumatic disease 2
Active cancer 2
Age 40-84 1
Male 1
Moderate renal failure (GFR 30-59ml/min) 1
A score >7 is considered high risk for bleeding

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Chapter 14; Fluid and electrolyte disturbance

14.1. Fluid, Maintenance Fluid (MF) calculation


Composition of body fluids

Total Body Water (TBW)


➢ 60% in an average young adult male & 50% in young adult female
➢ The highest percentage of TBW is found in newborns, with approximately 80%
of their total body weight.

Fluid Balance
➢ Fluid and electrolyte homeostasis is maintained in the body
➢ Neutral balance: input = output
➢ Positive balance: input > output
➢ Negative balance: input < output
➢ Na+ is the major extracellular cation & K+ major intracellular cation
➢ Fluid balance is made through vasopressin, water ingestion & renal
water transport to keep osmolality 280-295 mosm/kg

Types of crystalloids
➢ RL (ringer lactate)
✓ Slightly hypotonic in that it contains 130 mEq of lactate.
✓ It is ideal for the replacement of existing fluid deficits when serum
electrolyte concentrations are normal. Because Lactate is used rather than
bicarbonate because it is more stable in IV fluids during storage. It is
converted into bicarbonate (used to buffer acid base imbalance) by the
liver after infusion, even in the face of hemorrhagic shock.
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➢ NS (normal saline /Sodium chloride (0.9%))


✓ It is mildly hypertonic, containing 154 mEq of sodium that is balanced by
154 mEq of chloride
✓ The high chloride concentration imposes a significant chloride load on the
kidneys and may lead to a hyperchloremic metabolic acidosis.
✓ So, it is an ideal solution, for correcting volume deficits associated with
hyponatremia, hypochloremia, and metabolic alkaloids
➢ D5W (5% dextrose)
✓ 50 g of dextrose per liter--supplies 200 kcal/L
✓ Dextrose is always added to solutions containing <0.45% sodium chloride
(hypotonic) to maintain osmolality and thus prevent the lysis of RBCs that
may occur with rapid infusion of hypotonic fluids. The addition of
potassium is useful once adequate renal function and urine output are
established.

➢ 0.45% sodium chloride


✓ useful for replacement of ongoing GI losses as well
✓ This solution provides sufficient free water for insensible losses and
enough sodium to aid the kidneys in adjustment of serum sodium levels.
✓ This hypotonic solution causes lysis of RBCs--to prevent this add 5%
dextrose (50 g of dextrose per liter)

➢ DNS → contains 5% dextrose and NS, important for transition phase of


DKA mgt

Alternative Resuscitative Fluids


➢ Hypertonic saline
✓ Hypertonic saline solutions (3.5% and 5%) → used for correction of
severe sodium deficits
✓ Hypertonic saline (7.5%)

colloids
➢ Four major types of colloids are available
✓ Albumin
✓ Dextrans
✓ hetastarch, and
✓ Gelatin

Disorders Fluid of choice


Diarrhea RL
Vomiting NS
DKA
Sepsis Crystalloid

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Maintenance Fluid (MF) calculation


➢ It is the usual daily requirement. It to replace basal fluid requirement i.e
the sensible and insensible losses
➢ Calculation of MF replacement doesn’t include replacement of either
preexisting deficits or ongoing additional losses

Maintenance fluid calculation


Weight in kg Amount of fluid /kg/day
0-10 kg 100 ml/kg/day
11-20 kg 1000ml (100 X the 1st 10 kg) + 50 ml/kg/day for
the next kg
>20 kg 1500ml (100 X the 1st 10 kg + 50 x the 2nd 10kg)
+ 20 ml/kg/day for the remaining kg

➢ E.g. MF for 70kg pt (10kgX100ml +10kgX50ml+50kgX20ml) = 2500ml per day


(i.e 2500 ml over 24hrs)
➢ To run over 8hours divide the total MF for 3 (since 24hr ፥ 3 = 8hrs). So, for
this pt, 2500ml /3 = 833 ml over 8hrs
✓ 1ml=20drops through IV line
✓ 8hrs=8X60min=480 min
➢ If we want 833ml over 480min (meaning 8 hrs), we have to adjust by
calculating the drop as follows
833ml x 20 drops 16,660 drops
MF = = = 35 drops per minute
8ℎ𝑟𝑠 𝑥 60𝑚𝑖𝑛 480 𝑚𝑖𝑛
➢ What are the fluid components for MF?
✓ 1/3rd of total MF is NS and 2/3rd D10
✓ D10 = 85% of D5 + 15 % of D40
➢ For the above patient
✓ 1/3rd of 833ml = 278ml of NS, 2/3rd of 833ml = 555 ml of D10
✓ 85% of 555ml D10 = 472ml D5, 15 % of 555ml D10 = 83ml D40
➢ So, your order could be like this
✓ Put on MF (278ml of NS + 472ml D5 + 83ml D40) to run over 8
hrs at a rate of 35 dpm
✓ This numbers may be difficult to give practically. So, the order can
be modified as Put on MF (280ml of NS + 470ml D5 + 80ml D40)
to run over 8 hrs at a rate of 35 dpm
✓ The usual trend of MF, for adult, in our setup is; 3 vials of D40 in
1L of NS to run over 8hr (@40 dpm) → please don’t practice like
this
➢ How do we know that, D10 = 85% of D5 + 15 % of D40?

Fluid preparation
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➢ Fluid is available in the form of 5% DW, 40% DW, 9% NS, or RL, but there is
no readily prepared fluid 10% DW (D10) in most setups of Ethiopia.
➢ We have to prepare fluid using what is available. To prepare fluid, use
following formula. We need to prepare x% DW from a% DW and b% DW
( a − x ) x Tv. ( X − b ) x Tv.
Vb = (a – x ) + ( x – b)
, Va = (a – x ) + ( x – b)
(Where x = conc. of DW wanted, a = highest conc. of DW , b =
lowest conc. of DW, Va = volume of a, Vb = volume of b, Tv =
total volume needed = Vb + Va )
➢ For example: How to prepare Total volume (Tv) of 10%DW from 40%DW &
5% DW.
✓ Given x = 10%, a = 40, b = 5% , Va = volume of 40%, Vb = Volume
of 5%, Tv = total volume needed = ( Vb + Va)
( 40− 10 ) x Tv. ( 10 – 5 ) x Tv.
✓ Vb = (40 – 10 )+ ( 10 – 5)
, Va = (40 – 10 )+ ( 10 – 5)
30 x Tv. 5 x Tv.
✓ Vb = 35
, Va = 35
✓ Vb (D5W) = 0.85 (meaning 85%) x Tv (D10), Va (D40) = 0.15
(meaning 15%) x Tv (D10)

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14.2. Electrolyte disturbance

14.2.1 Hypokalaemia

Hypokalemia is defined as serum potassium level < 3.5mmo/l.

Potassium Value (in mmol/L or meq/l)


Normal 3.5 - 5.0
Mild hypokalemia 3.0 - 3.5
Moderate hypokalemia 2.5 - 3.0
severe hypokalemia < 2.5

Causes of Hypokalemia
Hypokalemia is either caused by loss from the body or entrance (shift) of
the plasma potassium in to the cell (intracellular compartment)
Causes due to potassium loss
✓ Renal loss:
▪ Diuretics, DKA, resolving AKI/obstructive uropathy, prolonged
vomiting or NG tube drainage
▪ Hypomagnesemia, renal tubular disorders due to drugs like
aminoglycosides, amphotericin, tenofovir, inherited tubular
diseases
▪ Hyperaldosteronism
✓ GI loss: diarrhea
Causes due to redistribution/shift into intracellular space
✓ Medicines: Insulin, beta-2 agonists
✓ Metabolic alkalosis

Clinical features
Unless it is severe, Mild to moderate hypokalemia is generally
asymptomatic.
If there are symptoms attributable to hypokalemia, it is considered to be
severe.
Symptoms of muscle weakness:
✓ Weakness of extremities
✓ Abdominal distention
Neuromuscular
✓ Generalized fatigue and malaise
✓ Muscle cramps, paresthesia
✓ Severe weakness (K <2.5 mEq/L)
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✓ Paralysis if K <2.0 mEq/L and rapid development


CVS: ventricular or atrial arrythmia: the most feared manifestation of
hypokalemia is ventricular arrhythmia, as it is sudden onset there might not
be any signs during evaluation, cardiac arrest
GIT: Constipation, ileus, Gaseous abdominal distention with decreased to
absent bowel sounds and failure to pass feces due to paralytic ileus
GUS: Polyuria (hypokalemic nephropathy)
Rarely features of rhabdomyolysis: muscle weakness, pain and dark
urine
life-threatening complications are arrhythmias and paralysis

Investigations and diagnosis


Diagnosis
The diagnosis is made based of serum potassium determination.
ECG is needed to assess the severity

Investigations
Electrolytes → Serum potassium, Serum magnesium, serum Ca
ECG → for ECG features of Hypokalemia read from Chapter 22; Basics of
ECG and ECG interpretation or click here → Electrolyte disturbances (i.e.
hyperkalemia, hypokalemia)
Further investigations to determine the underlying cause might be needed if
the cause is not obvious like Cr and BUN, serum osmolality, urine PH,
Urine K

Treatment

Total body deficit is 200-300 mEq per 1 mEq/L decrement in serum


K+ level
Rate and route dependent on presence of symptoms, severity of
hypokalemia, and comorbidities
Complete replacement over several days
Oral potassium preferable to IV therapy whenever possible

Non pharmacologic treatment


Encourage foods rich in potassium e.g. Peanut butter, avocado, bananas,
orange juice, papaya.
Avoid exercise in patients with moderate to severe hypokalemia

Pharmacologic treatment
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Severe hypokalemia
Potassium chloride (KCl) IV infusion. 40-60 meq of elemental potassium, in
1000ml Normal saline, to run every 6-8 hours.
✓ Use non dextrose containing fluids
✓ Maximum concentration of potassium is 60meq in one liter of fluid.
✓ Maximum rate of infusion (in the presence of perfuser machine) is
10meq/hour
✓ Recommended if neuromuscular symptoms, cardiac arrhythmias, ongoing
GI loss or severe hypokalemia
✓ KCL 15-20 mEq/L in NS via peripheral vein. If > 40meq/L Kcl required,
central vein needed
PLUS
Potassium chloride (KCl) tablet, 600mg (equivalent to 8meq of potassium),
2-3tabs, PO, TID to QID.

Mild to moderate hypokalemia


Potassium chloride (KCl) tablet, 600mg (equivalent to 8meq of potassium),
2-3tabs, PO, TID to QID.
Potassium citrate, Potassium gluconate → Use in acidotic patient
For Hypokalemia due chronic loop diuretics: Spironolactone-see doses in
each indication (Heart Failure, liver cirrhosis)

Treatment of the cause


Some causes of hypokalemia may be treated pharmacologically. See the
examples below.
✓ Vomiting - anti-emetics
✓ Hypomagnesemia - magnesium sulfate
✓ Hyperaldosteronism (Aldosteronism) – spironolactone
✓ Potassium wasting tubulopathies - spironolactone or NSAIDS.
Patients with chronic hypokalemia, the cause of which is not established
need to be evaluated by nephrologist.

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14.2.2 Hyperkalemia

Hyperkalemia is defined as a serum potassium level of > 5.5mmol/l.


It is considered severe if the serum potassium is >6.5 mmo/l or there is
ECG or clinical manifestation associated with the hyperkalemia.

Potassium Value (in mmol/L or meq/l)


Normal 3.5 - 5.0
Mild hyperkalemia 5.5 - 6.0
Moderate hyperkalemia 6 - 6.5
severe hyperkalemia > 6.5

Causes of hyperkalemia
I) Low renal excretion: AKI or CKD, spironolactone, ACE
inhibitors/ARBS, NASAIDS, adrenal insufficiency
* A decrease in renal K+ excretion due to AKI or CKD is the most
common underlying cause.
II) Excess intake: potassium tablets, potassium rich diet in patients
with AKI/CKD
III) Release from intracellular space: tumor lysis, rhabdomyolysis,
hemolysis
IV) Shift from intracellular space: acidosis, digoxin, adrenergic
blockers
V) Pseudo hyperkalemia (In-vitro cell death): tight tourniquet,
thrombocytosis, erythrocytosis, marked leukocytosis

Clinical features
Mild hyperkalemia is generally asymptomatic
Severe hyperkalemia results in muscle weakness or paralysis, Dyspnea,
Chest pain, palpitation or syncope, cardiac conduction abnormalities and
cardiac arrhythmias.

Investigations and diagnosis


Diagnosis
The diagnosis is made based of serum potassium determination.
If there is no obvious cause, pseudo hyperkalemia needs to be excluded
ECG is needed to assess the severity. Refer short case of nitsbin for ECG
features of Hyperkalemia (click here → 22.6.5 Electrolyte abnormality)

Investigations
RBS
Serum potassium
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Serum creatinine and urea


ECG → for ECG features of Hypokalemia read from Chapter 22; Basics of
ECG and ECG interpretation or click here → Electrolyte disturbances (i.e.
hyperkalemia, hypokalemia)
Investigations for causes e.g. if adrenal insufficiency is suspected basal
serum cortisol level will be needed for screening purpose.

Treatment

Non pharmacologic treatment


Decrease food rich in potassium → see section on hypokalemia
Discontinue medicines which increase potassium→ ACE- I, ARBs,
Spironolactone, NSAIDs
Dialysis: in refractory hyperkalemia due to AKI or CKD/ESRD

Pharmacologic treatment principles (For moderate to severe


hyperkalemia)
✓ Mild hyperkalemia may actually protect against tachyarrhythmias.

Calcium gluconate, 10ml of a 10% solution, IV, over 2-3 minutes,


with constant cardiac monitoring. The dose can be repeated after 5
minutes, if the ECG changes of hyperkalemia persist or recur PLUS
Regular Insulin, 10 units IV, followed immediately by 60-80ml ml of
40% dextrose (25g of glucose), every 4-6 hours) PLUS
Furosemide, 40 - 120mg, IV, dose should depend on previous
response, degree of kidney function impairment. The dose can be
repeated according to response. PLUS
Salbutamol, 10 to 20mg in 4 mL of saline by nebulization over 10
minutes or MDI (100µg/puff), 8 - 10 puffs every 20-30 minutes.
Sodium bicarbonate, 1- 2mEq/kg, IV, bolus over 1-2 min; repeat as
needed to improve cardiotoxic manifestations

Patients in whom the cause of potassium disorder is not clear need to be


evaluated by nephrologist.

Treatment based on clinical feature and underlying cause

➢ shift potassium intracellularly.


✓ Insulin + glucose. (10Iu RI + 50ml of 50% dextrose)
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✓ IV sodium bicarbonate:1-3 amps (44mEq per amp) IV over 20-30


min
✓ Inhaled albuterol: 10-20mg nebulized over 10 min
➢ K+ > 6.0 without ECG Change → Enhance excretion of potassium with
✓ Calcium or sodium polystyrene sulfonate (Kayexalate, 0.5 g/kg po
(0.3–0.6 g/kg PO) in 2 mL/kg 70% sorbitol
✓ Diuretics
➢ Hyperkalemia with EKG Changes, or cardiac arrest
✓ Antagonize potassium-mediated Cardiotoxicity with Ca-gluconate,
CaCl2 or NaHCO3
➢ Renal failure:
✓ Hemodialysis effective at removing potassium
✓ Furosemide: Effective in absence of oliguric renal failure, Causes
potassium-losing diuresis
➢ Mineralocorticoid deficiency:
✓ Hydrocortisone, fludrocortisones
➢ Treat the underlying cause

14.2.3 Hyponatremia

➢ Normal serum sodium level is 135 - 145 mmol/L


➢ Hyponatremia is defined as a plasma sodium concentration of <
135mmol/L.
➢ Severe hyponatremia is defined as a plasma sodium concentration of
<115 mmol/L
➢ Acute hyponatremia is development of hyponatremia in < 48 hours
➢ Chronic hyponatremia if duration known to be >48 hrs
➢ Hyponatremia can be due to a loss of sodium in excess of water, a
gain of water in excess of sodium or both. Hyponatremia is a water
problem, not a Na+ problem. i.e. water intake > water excretion
➢ Causes of hyponatremia → classified based on the volume status
of the patient
✓ Hypovolemic hyponatremia → diarrhea, vomiting, burn, polyuria
✓ Euvolemic hyponatremia → syndrome of inappropriate ADH secretion
(SIADH), hypothyroidism, low dietary solute intake
✓ Hypervolemic hyponatremia → CHF, CKD, CLD, nephrotic syndrome.

Clinical features
➢ The symptoms directly attributable to hyponatremia primarily occur with
acute and marked reductions in the serum sodium concentration and 1242
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reflect neurologic dysfunction induced by cerebral edema, and possibly


adaptive responses of brain cells to osmotic swelling. In this setting, the
associated fall in serum osmolality creates an osmolal gradient that
favors water movement into the cells, leading to brain edema.
➢ Acute hyponatremia (duration known to be <48 hr.)
✓ Early: nausea, malaise, headache, muscle twitching, lethargy
✓ Late/Severe: obtundation Confusion and disorientation, seizures,
coma, Respiratory distress or arrest
➢ Chronic hyponatremia (duration known to be >48 hr.)
✓ Frequently mild or no symptoms

Investigations and diagnosis


Diagnosis
➢ The diagnosis of hyponatremia is made based on the serum sodium
level.
➢ Clinical evaluation is needed to classify the volume status of the patient
and the more specific cause.

Investigation
➢ RBS
➢ Serum electrolytes
➢ Creatinine and BUN
➢ Serum osmolality to R/o pseudohyponatremia
𝐺𝑙𝑢𝑐𝑜𝑠𝑒 𝐵𝑈𝑁
✓ Plasma osmolality = (2 x plasma Na+) + +
18 2.8
✓ Patients with hyponatremia have low osmolality (<275mosm/kg)
➢ CXR → If pulmonary pathologies (pneumonia, lung cancer) suspected.
➢ Urine Na
➢ Urine osmolality
➢ TFT → In euvolemic hyponatremia
➢ Serum cortisol → basal or random (in critical patients)
➢ Investigation directed to the suspected underlying cause

Treatment

Non pharmacologic treatment


➢ Free water restriction – for euvolemic and hypervolemic causes
➢ Encourage table salt intake-if not hypervolemic
➢ Discontinue thiazide diuretics
➢ Management of the underlying cause
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Pharmacologic treatment
➢ Hypovolemic hyponatremia
✓ Normal saline, IV infusion-volume depending on the estimated fluid
deficit
➢ Hypervolemia hyponatremia
✓ Furosemide, dose depending on the underlying disease and
previous response.
➢ Euvolemic hyponatremia: if it is severe/symptomatic acute hyponatremia
✓ 3% NaCl (513mmol of Na/L), IV, 1-2 ml/kg/hour
✓ Should elevate the serum Na approximately 1-2mmol per hour
✓ Raising the serum Na 4-6mmol/L over 2-3 hours is enough to
prevent serious neurologic complications
✓ Subsequently, the rate of correction should be less than 10mmol/L
per 24 hours.
➢ Osmotic demyelination syndrome
✓ To prevent Osmotic demyelination syndrome Rapid correction of
hyponatremia should be avoided

➢ As hypertonic saline is not commonly available, some practitioners advise


patients to take more salt or an arbitrary amount of salt. This practice
could be dangerous as it might result in overcorrection.
➢ The following could serve as an improvised guidance on preparing 3%
NaCl oral solution
✓ 1 tea spoon (tsp) of table salt = 6 g salt ≈ 2,400 mg sodium = 104
mmol sodium
✓ A 500ml of standard 3% saline (3% hypertonic saline) contains
256.5mmol of sodium
✓ To prepare as 500ml of 3% sodium chloride solution, add 2 and a
½ tsp (tea spoon of salt in 500ml of water.
✓ Example of administration: For a 70kg male adult with an aim to
increase serum sodium by 8mmmol/24 hour, give 35ml of the about
solution every hour. (This should be given by measuring the amount
using a syringe)

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14.2.4 Hypernatremia

➢ Hypernatremia is defined as plasma sodium concentration of >145mmol/l.


➢ Severe hypernatremia is plasma sodium value of >160 mmol/L.
➢ Hypernatremia can be due to loss of water, gain of sodium, or both.
Loss of water is the more common denominator.
➢ Individuals who can get and take water are unlikely to develop
hypernatremia. Hence, the majority of patients who develop severe
hypernatremia are patients who cannot get water by themselves e.g.
patients with depressed mental status, stroke, on mechanical ventilator,
the very elderly…

Causes of hypernatremia
➢ Hypovolemic hypernatremia
✓ Renal water loss
▪ Loop diuretics
▪ post obstructive dieresis
▪ osmotic diuresis → glucosuria
▪ Hypercalcemia
▪ Hypokalemia
▪ Drugs like lithium
✓ Extra renal water loss:
▪ Burns
▪ GI Losses → Diarrhea, vomiting, etc.
▪ Insensible Loss (skin or lungs)
• Fever
• Hot Room
• Hyperventilation
o In association with deficit in water intake (coma,
stroke, immobility)
o Small volume hyperosmolar > 600mosm urine:
insensible loss
➢ Euvolemic hypernatremia: Diabetes insipidus, hypodipsia
➢ Hypervolemic hypernatremia: Iatrogenic (sodium bicarbonate, hypertonic
saline), Salt poisoning in infants, Sea water ingestion

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Clinical features
➢ Hypernatremia is basically a mirror image of hyponatremia. A rise in the serum
sodium concentration and osmolality causes water movement out of the brain
which leads to shrinkage of brain cell volume and secondary neurological
symptom
➢ Mild and chronic hypernatremia is usually asymptomatic
➢ If conscious most patients with hypernatremia will have excessive thirst
➢ Severe acute hypernatremia causes CNS symptoms-irritability, lethargy,
seizure and coma.

Manifestations of acute hypernatremia


➢ With acute hypernatremia defined as hypernatremia developing within hours,
the rapid decrease in brain volume can cause rupture of the cerebral veins,
leading to focal ICH and SAH and possibly irreversible neurologic damage.
➢ Acute hypernatremia can also result in demyelinating brain lesions similar to
those associated with overly rapid correction of chronic hyponatremia.
➢ The clinical manifestations of acute hypernatremia begin with lethargy,
weakness, and irritability, and can progress to twitching, seizures, and coma.
➢ Severe symptoms usually require an acute elevation in the serum sodium
concentration to above 158 mEq/L.
➢ Values above 180 mEq/L are associated with a high mortality rate, particularly
in adults

Manifestations of chronic hypernatremia


➢ Chronic hypernatremia, which is defined as hypernatremia that has been
present for more than a day, is much less likely to induce neurologic
symptoms.
➢ Assessment of symptoms attributable to hypernatremia is often difficult because
most affected adults have underlying neurologic disease. The latter is required
to diminish the protective thirst mechanism that normally prevents the
development of hypernatremia, even in patients with diabetes insipidus.
➢ Like hyponatremia, hypernatremia, even if mild, is associated with increased
morbidity and mortality.

Investigations and diagnosis


Diagnosis
➢ Diagnosis is made based on serum sodium determination
Investigation
➢ Serum electrolytes
➢ Creatinine and BUN
➢ Urine specific gravity/osmolality
➢ Blood sugar
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➢ If diabetes insipidus is suspected refer to next level of care after


management of the acute state.

Treatment

Non pharmacologic treatment


➢ Avoid rapid correction.
➢ Encourage free water intake for thirst. This is the preferred route of
correcting water deficit in conscious patients with intact thirst.

Pharmacologic treatment
➢ The main stay of treatment for hypernatremia is water (free water) given
orally (preferred) or intravenously as 5%DW but the patients volume
status depends on the severity of hypernatremia and the patient’s
volume state.
➢ Hypovolemic Hypernatremia:
✓ Ringer’s lactate, IV, until hypovolemia improves.
✓ Once the hypovolemia improves shift the fluid to 5%DW after
calculating the water deficit.
➢ Euvolemic Hypernatremia:
✓ Correct water deficit using either oral free water or 5%DW
✓ Replace ongoing losses
✓ Consult specialist if Diabetes Insipidus is suspected.
➢ Hypervolemic Hypernatremia:
✓ Thiazide diuretics are preferred if the volume overload is mild
Alternative
✓ Furosemide IV or P.O., dose and route depending on severity of
hypervolemia.

Rate of correction of hypernatremia


➢ In acute hypernatremia (developing within hours) immediate reduction of
serum Na is recommended but at a rate not exceeding 0.5mmol/hour
over 48-72 hours
➢ Correction should not exceed 10mmol/day.
➢ Correction of chronic hypernatremia must occur slowly to prevent rapid fluid
movement into the brain and cerebral edema, changes that can lead to
seizures and coma

Calculation of water deficit


➢ Water deficit = CBW x ⌊
𝒔𝒆𝒓𝒖𝒎 𝑵𝒂
𝟏𝟒𝟎

➢ CBW refers to estimated current body water
𝟏⌋
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➢ CBW = 60% and 50% of body weight in younger men and women,
respectively
➢ CBW= 50% and 45% in elderly men and women, respectively.

Patients suspected of having diabetes insipidus (with polyuria, polydipsia,


dilute urine and no diabetes mellitus) should be evaluated by
endocrinologist or internist.

14.2.5. Hypocalcemia

➢ Normal serum calcium level is 8.7 - 10.2 mg/dL (2.2 - 2.6 mmol/L) and
ionized serum calcium level is 4.5 - 5.3 mg/dL (1.12 - 1.32 mmol/L)
➢ Total calcium should always be corrected for serum albumin.
➢ Corrected calcium = measured calcium + [ 0.8 x (4.0- serum albumin)]
➢ Hypocalcemia is defined as a corrected total serum calcium level < 8.5
mg/dl (<2.12 mmol/l) or ionized serum calcium level < 4.5 mg/dL
(<1.13mmol/l)
➢ Hypocalcemia is a common problem in clinical practice, both in
ambulatory care and in hospitalized patients. More than 80% critically ill
patients develop hypocalcemia.
➢ The major factors that influence serum calcium concentration are
parathyroid hormone (PTH), vitamin D activity and their action on the
kidneys and the intestine.
➢ Hypocalcemia is mainly caused by disorders related the level or activity
of parathyroid hormone and/or vitamin D.
➢ The clinical presentation of hypocalcemia could vary from asymptomatic
(incidental finding) to a life threatening one depending on the rapidity of
development and severity.

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Major causes of hypocalcemia

➢ Hypocalcemia with inadequate PTH (low or inappropriately normal PTH)


✓ Surgical removal (commonly post thyroidectomy or
parathyroidectomy)
✓ Neck radiation
✓ Autoimmune destruction
✓ Idiopathic hyperparathyroidism

➢ Hypocalcemia with high PTH


✓ CKD
✓ PTH resistance: pseudohypoparathyroidism, hypomagnesemia
✓ Vitamin D deficiency: Nutritional or malabsorption
✓ Vitamin D resistant: Vitamin-D dependent or resistant rickets

➢ Miscellaneous
✓ “Hungry bone syndrome” following parathyroidectomy
✓ Extravascular deposition of calcium: hyperphosphatemia,
pancreatitis, tumor lysis syndrome
✓ Critical illness
✓ Drugs: IV bisphosphonate therapy

Clinical features
➢ Chronic hypocalcemia is generally asymptomatic or cause mild
symptoms.
➢ The hallmark of hypocalcemia is an irritable neuromuscular system which
shows spontaneous or induced hyperexcitability, called tetany.
➢ Mild symptoms: perioral numbness, paresthesia of the hands and feet,
muscle cramps, fatigue
➢ Severe clinical manifestations
✓ Tetany:
▪ Spams of hands and/or feet (carpopedal spasm): forced
inward movement (adduction) of the thumb, flexion of
metatarsophalangeal joints and wrists
▪ Laryngeal spams: stridor or change in voice, air hunger
▪ Induced tetany
• Trousseau’s sign: Carpal spasm induced but inflating
sphygmomanometer 20mmHg above the systolic BP and
keeping it for 3 minutes.
• Chvostek’s sign: elicited by tapping the facial nerve about
2cm in front of the ear (tragus) and observing contraction
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of the facial muscles. Chvostek’s sign can also be seen in


normal individuals. It has poor sensitivity and specificity.
✓ CNS manifestations: Focal or generalized seizures, confusion,
delirium, papilledema
✓ Cardiac manifestations: hypotension, features of heart failure,
prolonged QT on ECG
✓ GI manifestations; abdominal cramps, biliary colic
➢ Clinical features related to the underlying disease
✓ Chronic hypoparathyroidism:
✓ cataracts, poor dentition, dry skin, brittle nails, coarse hair, basal
ganglia calcifications
✓ Vitamin D deficiency in adults: diffuse bone pain and muscle
weakness

Investigations and diagnosis

➢ ECG: look for prolonged QT interval


➢ If the cause of hypocalcemia is obvious e.g. post-thyroidectomy or post-
parathyroidectomy, advanced chronic disease, or tumor lysis, further
investigation might not be needed.
➢ The most important investigations need for identifying the possible cause
of hypocalcemia are the following
✓ Creatinine and BUN
✓ Serum magnesium and phosphorus
✓ Serum PTH (preferably intact PTH)
✓ vitamin D level (25(OH)vitamin D)

Treatment

Non-pharmacologic
➢ Increase diet rich in calcium and vitamin D.

Pharmacologic
➢ Hypocalcemia with severe symptoms (tetany, seizure, change in mental
status, prolonged QT) or acute (postoperative) <7.5mg/dl: IV calcium
➢ Calcium gluconate (10%) 01 ampoule (10ml) IV over at least 10min
(rule of 10)
✓ If symptoms persist, repeat the above. Don’t repeat more than two
times.
✓ Give a continuous infusion (drip) of calcium in the following way 1250
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▪ Add 06 ampoules of 10% calcium gluconate in 1L of 5%DW


run 12 hours (80ml/hr or 28 drops/minute).
▪ This equivalent to 540mg of elemental calcium in 1000ml =
0.54mg/ml preparation running at about 45mg/hour)
✓ Do serum calcium every 12 hour and continue infusion until calcium
reaches 8mg/dl
✓ Start oral calcium (see below) as soon as the patient is able to
take orally, overlap with the intravenous infusion.
➢ Severe hypocalcemia in the presence of hypomagnesemia: correct the
magnesium first
✓ IV magnesium sulfate: see hypomagnesemia treatment
✓ Give also calcium gluconate as above.
➢ Long-term calcium replacement therapy: for mild hypocalcemia and after
IV calcium in sever hypocalcemia.
✓ Give elemental calcium 1500 to 2000mg/day, BID or TID
▪ Calcium carbonate 1000mg (equivalent to 400mg elemental
calcium), 2tabs, PO, BID or TID
✓ Target serum calcium is to keep it between 8-9mg/dl. Don’t go
beyond 9mg/dl.
➢ Vitamin D supplementation or correction of deficiency (if confirmed)
✓ Vitamin D3 or D2: If deficiency confirmed (50,000IU weekly for 6-
8weeks), if not yet confirmed, give 800IU/day empirically.

14.2.6. Hypercalcemia

➢ Hypercalcemia is defined as a total serum calcium >10.3mg/dl or an


ionized calcium >5.2mg/dl (2.6mmol/l)

Hypercalcemia total serum calcium level (in mg/dl)


Mild 10.3 - 12
Moderate 12 -14
Severe >14

➢ The most important denominator in the causation of hypercalcemia is


increased bone resorption. The contribution of increased oral absorption
is modest.
➢ The two most common causes of hypercalcemia are primary
hyperparathyroidism and malignancy accounting 90 % of cases.
➢ The work up of hypercalcemia is focused on differentiating the two
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➢ Other less common causes include


✓ Increased vitamin D activity: excess ingestion, overproduction in
granulomatous diseases (tuberculosis, sarcoidosis)
✓ Decreased renal excretion: Familial hypocalciuric hypercalcemia
✓ Tertiary hyperparathyroidism: in advanced CKD
✓ Endocrinopathies: hyperthyroidism, adrenal insufficiency
✓ Drugs: thiazide diuretics, Lithium
✓ Excess calcium intake

Clinical features

➢ Mild hypercalcemia is generally asymptomatic


➢ Symptom develop if severe hypercalcemia develops over a shorter
period of time
➢ Symptoms are remembered as “Stones, bones, moans and groans”.
➢ Bone pain
➢ Fatigue, muscle weakness
➢ Polyuria, polydipsia, kidney stones
➢ Constipation, anorexia, nausea, vomiting, constipation, pancreatitis
➢ High blood pressure
➢ Anxiety, depression, cognitive dysfunction
➢ Confusion and coma

Investigation and diagnosis

Diagnosis
➢ Once hypercalcemia is confirmed from serum total calcium or ionized
calcium, the next step important investigation is determination of serum
PTH.
➢ Low PTH: very likely hypercalcemia due to malignancy or vitamin D
related causes
➢ High or normal PTH: Hyperparathyroidism
➢ If serum PTH can’t be done and the patient has overt malignancy,
consider the hypercalcemia to be due to the malignancy.

Investigations
➢ Other investigation for patients with low serum PTH
✓ Investigate for malignancy based on clinical clues e.g. screening for
multiple myeloma
✓ Serum 25(OH) and 1,25(OH)Vitamin D
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➢ Phosphorous: low in primary hyperparathyroidism, elevated in Vitamin D


related causes
➢ ECG: short QT interval
➢ X-rays: osteoporotic changes in cortical bone, typically in the wrist,
bone cysts (osteitis cystica fibrosa) in the long bones
➢ Ultrasound: Renal stones or evidence of nephrolithiasis

Treatment

Non-pharmacologic treatment
➢ If the patient has severe hypercalcemia (>14mg/dl) or has severe
symptoms (features of dehydration, change mental status) urgent
admission is needed.
➢ Discontinue drugs which can cause hypercalcemia: thiazide, lithium
➢ Surgical management: in primary hyperparathyroidism, if there are
indications.
➢ Management at referral hospital level is strongly recommended.

Pharmacologic treatment

Severe hypercalcemia
➢ Aggressive hydration with normal saline for few days
✓ 4-6 liters of NS over 24 hours (1 liter over 4-6 hours), close monitoring
for fluid overload and fluid balance.
✓ Do not routinely use Furosemide unless the patient is fluid
overloaded (pulmonary crackles, raised JVP).
✓ If Fluid overloaded, Furosemide, 20-40mg IV, when needed. Similar
doses of can be repeated if fluid overload persists.
➢ Intravenous bisphosphonate
✓ Zoledronic acid, 4mg, diluted in 100ml of NS or D5W, given as infusion
over 15-30minutes.
➢ Corticosteroids
✓ Dexamethasone 4mg IV BID OR
✓ Hydrocortisone 100mg IV, BID OR
✓ Prednisolone 30-40mg/day.

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14.2.7 Hypomagnesemia

➢ The major dietary sources of magnesium are green vegetables (such as


spinach), nuts and whole grains (cereals).
➢ Units of serum magnesium measurement and normal values:
✓ Serum magnesium can be reported in any of the three units: mmol/l,
mEq/l or mg/dl.
✓ The molecular weight of magnesium is 24.3 and its valence is 2 (+2).
Hence. the relationship between the units is as follows

➢ mEq/l = mmol/L x 2 OR mmol/l= mEq/l ÷ 2


➢ mg/dl = 2.43 x mmol/l OR mg/dl= 1.21 x mEq/l

➢ The normal range for serum magnesium is 1.7 to 2.1 mg/dl= 1.4 to
1.7 mEq/l= 0.70 to 0.85 mmol/L.
➢ Hypomagnesemia is defined as serum magnesium <1.6mg/dl or < 0.66
mmol/L (<1.3mEq/L).

Hypomagnesemia serum magnesium level (in mg/dl)


Mild 1.2 - 1.6
Moderate 1.2 - 1.5
Severe <1.2

➢ Clinically significant symptoms and signs do not commonly occur until


the level falls below 1.2 mg/dL.
➢ Hypomagnesemia is common in hospitalized patients, particularly critically
ill patients.
➢ The mechanisms of hypomagnesemia development are renal losses, GI
losses or poor intake, redistribution (shift or sequestration) or a
combination.

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Table. Causes of hypomagnesemia


Mechanisms Causes
➢ Medications
✓ Loop or thiazide diuretics (Not potassium
sparing diuretics)
✓ Nephrotoxic medications: aminoglycosides,
Renal loss
amphotericin B, Cisplatin and Cyclosporine
➢ Polyureic states
✓ Postobstructive diuresis
✓ polyureic phase of recovering AKI (ATN)
✓ DKA
➢ Extracellular fluid expansion (hyperfiltration)
✓ Aggressive saline infusion
➢ Hypercalcemia
➢ Inherited renal tubular disorders: Gitelman or
Barrter syndrome
Gastrointestinal causes ➢ Diarrhea
➢ Prolonged NG tube suction or prolonged vomiting
➢ Prolonged PPI use
➢ Malabsorption
➢ Small bowel resection
➢ Severe malnutrition
➢ Chronic alcohol dependence
Redistribution (shifting in to the ➢ Correction of DKA
intracellular space) ➢ Refeeding syndrome
or sequestration ➢ Hungry bone syndrome: after parathyroidectomy
or thyroidectomy
➢ Acute pancreatitis

Clinical features

➢ Asymptotic: Mild hypomagnesemia developing slowly is usually asymptomatic.


➢ Symptomatic: The major manifestations are neuromuscular, cardiovascular, and
refractory electrolyte abnormalities.
➢ Neuromuscular: Neuromuscular hyperexcitability
✓ Positive Chvostek’s and Trousseau’s signs
✓ Tetany
✓ Tremor, fasciculation
✓ Seizure
✓ Confusion
➢ Cardiovascular: ECG abnormalities or life-threatening ventricular arrhythmias
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✓ Early ECG abnormalities: Wide QRS, peaked T-wave


✓ Late ECG abnormalities: Progressive widening of QRS, prolonged PR
interval and diminished T-wave
✓ Arrhythmias: Torsade’s de pointes, a repetitive polymorphic ventricular
tachycardia with QT prolongation
✓ Increase risk of digoxin toxicity
➢ Electrolyte abnormalities
✓ Hypokalemia: refractory to potassium replacement alone
✓ Hypocalcemia: refractory to calcium and vitamin D treatment alone
➢ Normal serum magnesium with magnesium depletion
✓ Patients with refractory hypokalemia and hypocalcemia should be
suspected to have magnesium depletion despite normal serum
magnesium. This is particularly true for patients with risk factors (e.g.
chronic diarrhea, alcohol abuse, long term diuretic use)

Diagnosis and investigation

Diagnosis
➢ Whom to screen for hypomagnesemia?
✓ Critically ill patients admitted to ICU
✓ All patients with hypokalemia or hypocalcemia
✓ Patients with clinical manifestations suspicious of hypomagnesemia
✓ Patients with potential causes for hypomagnesemia: chronic diuretic use,
nephrotoxic medication, prolonged PPI use, polyuric patients, chronic
diarrhea, alcohol dependence, post parathyroidectomy/thyroidectomy
➢ Confirming hypomagnesemia: serum magnesium level (watch the unit)
➢ Identifying the cause of hypomagnesemia
✓ Hx of drug use, history of diarrhea, alcohol use, and nutritional
assessment.
✓ If the cause is not obvious determine 24hour urine magnesium. A 24hour
urine magnesium excretion >10mg should be considered renal wasting
and <10mg suggests GI loss or transcellular shift.

Investigation: additional investigations needed


➢ Serum potassium
➢ Serum calcium
➢ ECG
➢ Serum creatinine: To help decide the rate of treatment

Treatment
Non-pharmacologic treatment
➢ Correction of the underlying cause: e.g. discontinuation of diuretics, nephrotoxic
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➢ Increase dietary intake of magnesium: Food rich in magnesium: Green leafy


vegetables, nuts or peanuts, legumes (e.g. beans), soy milk, and whole grains

Pharmacologic treatment
Treatment of severe (<1.2mg/dl) and symptomatic
hypomagnesemia
➢ Life threatening (arrhythmia)
✓ IV Magnesium sulfate1- 2g, IV push over 3-5 minutes, Followed by
continuous infusion
➢ Emergent: No arrhythmia but severe symptoms (e.g. neuromuscular
manifestations)
✓ IV Magnesium sulfate, 1 to 2g diluted in 100mL D5W, run 15-30minutes,
Followed by continuous infusion.
➢ Non-emergent repletion in patients with severe hypomagnesemia
✓ Start with continuous infusion. Avoid the initial bolus.
✓ How to give continuous infusion?
▪ 4 - 6 g magnesium sulfate diluted in 1-2 liters of D5W to run over
12 to 24 hours. E.g. 3g magnesium sulfate in 1000ml D5W runs
over 12 hours.
✓ Duration of continuous infusion
▪ Continuous infusion should continue for two more additional days
after correction of the serum magnesium.

➢ Patients with significantly impaired kidney function (eGFR<30ml/min):


✓ Because of the risk for severe hypermagnesemia, 50% of the magnesium
sulfate dose described above should be given.
➢ Monitoring serum magnesium
✓ Serum magnesium should be determined 1-2 times per day
➢ Major adverse effect
✓ The major adverse effect of IV magnesium sulfate is iatrogenic
hypermagnesemia, which almost exclusively occurs in patients with
impaired kidney function.
✓ Monitor for depressed/absent DTR, bradycardia and low BP, which are
the major manifestations of hypermagnesemia.

Moderate hypomagnesemia (1.2- 1.5mg/dl) in inpatient setting


✓ IV magnesium sulfate 2gm in 1000ml D5W to run 12-24 hours.

Continue Potassium or Calcium infusions


➢ In patients with severe hypokalemia or hypocalcemia associated with
hypomagnesemia, IV infusions of potassium or calcium should be continued as
correction of magnesium takes long periods of time (a few to several days)
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Oral magnesium
➢ Oral magnesium should be started along with or after IV magnesium sulfate.
➢ Most oral magnesium preparations are poorly absorbed and poorly tolerated
(due to diarrhea)
➢ 240 - 1000mg of elemental magnesium is needed in 24 hours.
➢ The most commonly available oral magnesium preparation available is
magnesium hydroxide.
✓ Magnesium hydroxide (liquid form), 400mg/5ml (168mg elemental Mg5ml)
give 10ml BID-TID.
✓ If it is combined with Aluminum, avoid prolonged use.

Pharmacologic treatment of renal potassium loss (wastage):


➢ Potassium sparing diuretics also spare magnesium.
➢ In situations where is continued renal loss of magnesium, give magnesium
alone fails to correct the hypomagnesemia.
➢ These situations include: continued need to use diuretics, nephrotoxic
medications until tubular injury recovers (Cisplatin, Amphotericin B,
Aminoglycosides), inherited tubulopathies (Gitelman or Barrter syndrome).
➢ Spironolactone starting dose 25-50mg/day or 2 divided doses, maximum
400mg/day or in two divided doses

14.2.8 Hypermagnesemia

➢ Hypermagnesemia is defined as a serum magnesium level > 2.5mg/dL


(>1.1mmo/L or > 2.2mEq/L). However clinical symptoms do not generally occur
unless serum magnesium is >5mg/dL
➢ Hypermagnesemia is relatively uncommon in clinical practice and symptomatic
hypomagnesemia is much less common. This is due to the kidney’s
tremendous capacity to excrete excess body magnesium.
➢ Hypermagnesemia occurs in three clinical settings
✓ Marked impairment in kidney function (acute or chronic)
✓ Iatrogenic or accidental excess infusion or ingestion of magnesium:
typically, in the setting of treatment for preeclampsia or eclampsia with IV
magnesium sulfate
✓ Excess release from the intracellular compartment (generally with impaired
kidney function): Tumor lysis syndrome, rhabdomyolysis.

Clinical features
➢ Asymptomatic: serum magnesium level 2.5 -5mg/dL, though defined as
hypermagnesemia, is generally asymptomatic unless there is a concomitant
hypocalcemia.
➢ Symptomatic: The major symptoms and signs of hypermagnesemia are related
to neuromuscular or cardiovascular system.
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➢ Neuromuscular: characterized by depressed neuromuscular conduction(activity)


✓ Mild: Nausea, vomiting, constipation, facial flushing, dizziness, depressed
deep tendon reflexes.
✓ Moderate: Absent deep tendon reflexes, drowsiness, paralytic ileus, urinary
retention, blurred vision, and hypotension.
✓ Severe (life threatening): flaccid paralysis, respiratory depression, coma,
apnea.
➢ Cardiovascular: characterized by delayed(depressed) cardiac conduction
✓ ECG abnormalities (every conduction is delayed): prolonged PR interval,
AV block, prolonged QRS duration, prolonged QT interval.
✓ Severe (Life threatening): bradycardia advanced AV-block, cardiac
arrest/asystole.
✓ Hypocalcemia: hypermagnesemia suppresses PTH secretion

Table. Correlation between serum magnesium level and clinical


manifestations
Serum magnesium level Symptoms/signs
5-7mg/dl Nausea, vomiting, constipation
Facial flushing
Dizziness
7-12mg/dl Urinary retention, ileus,
Blurred vision, confusion, lethargy
Loss of deep tendon reflexes
Prolonged PR interval, wide QRS, prolonged QT
Hypotension
>12mg/dl Flaccid paralysis
Respiratory depression
Coma
Advanced AV-block/bradycardia
Cardiac arrest

Diagnosis and investigations

➢ A serum magnesium level >2.5mg/dl confirms the presence of


hypermagnesemia.
➢ Additional important investigations needed in those with confirmed
hypermagnesemia
✓ RFT: creatinine and Egfr
✓ Serum calcium, phosphorous and potassium
✓ ECG
➢ Monitoring serum magnesium level: patients receiving parenteral magnesium
sulfate need baseline RFT, ECG, close follow up of serum magnesium, DTR
and mental status.
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➢ Additional history: history of excess magnesium ingestion (antacids or


magnesium-based laxatives).

Treatment
Non-pharmacologic
➢ Stop magnesium infusion or oral magnesium containing drugs.
➢ Hemodialysis: In symptomatic hypermagnesemia with impaired kidney function

Pharmacologic
➢ Symptomatic hypermagnesemia:
✓ Intravenous calcium
▪ Calcium gluconate 10%, 10ml, diluted in 100ml D5W to run over 5-
10 minutes.
▪ In patients with cardiac arrest, give undiluted over 2-3 minutes.
▪ Repeat the dose, if symptoms persist.
✓ Forced diuresis
▪ Normal saline 200ml/hour for 6 -12 hours, if the patient does not
have volume overload (edema, pulmonary congestion, and
hepatomegaly).
▪ Give Furosemide 40mg, IV, stat, in the middle of the NS infusion.

✓ Hemodialysis
▪ In patients with significantly impaired kidney function
(eGFR<30ml/min) and symptomatic hypermagnesemia, excretion of
the magnesium is unlikely to happen; hence urgent hemodialysis is
needed after giving.
➢ Asymptomatic hypermagnesemia
✓ No need for pharmacologic treatment.
✓ Stopping magnesium containing medications or magnesium sulfate
infusion, if being given, will suffice.

Prevention
➢ During parenteral magnesium sulfate administration
✓ Determine baseline serum creatinine and continuously monitor urine output
✓ Monitor serum magnesium regularly every 6 hours
✓ If possible, have ECG monitoring (bedside monitor)
➢ Avoid prolonged use of magnesium containing medications in patients with
impaired kidney function medications (antacids or magnesium containing
laxatives)

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Chapter 15; Dyslipidemia and metabolic syndrome

15.1. Metabolic syndrome

➢ The metabolic syndrome is defined as the co-occurrence of risk factors


for atherosclerotic cardiovascular disease (ASCVD) and future
development of type 2 diabetes.
➢ Abdominal obesity and the associated insulin resistance are considered
to be main pathogenic mechanism behind the metabolic syndrome.
➢ The most important clinical implication of diagnosing metabolic syndrome
is intensification of life style and pharmacologic based ASCVD risk
reduction.

15.2. Dyslipidemia

➢ Dyslipidemias are disorders of lipoprotein metabolism that may result in


the following abnormalities: High total cholesterol (TC), high low-density
lipoprotein cholesterol (LDL-C), high non-high-density lipoprotein
cholesterol (HDL-C), high triglycerides (TG), or low HDL-C.
➢ Serum cholesterol and its lipoprotein carriers (LDL, and VLDL) are
known to be related to atherosclerotic cardiovascular disease (ASCVD).
➢ LDL-cholesterol is the dominant form of atherogenic cholesterol.
➢ HDL-cholesterol is not atherogenic.
➢ Although LDL-Cholesterol is a primary cause of atherosclerosis, other
major cardiovascular risk factors contribute a lot.
➢ The major cardiovascular risk factors include cigarette smoking,
hypertension, diabetes, other non-LDL abnormalities and old age
➢ LDL-C is calculated with the formula: LDL= Total-cholesterol–
(triglycerides/5) – HDL. When triglyceride level is above 400mg/dl, this
equation is sufficiently accurate.

Atherosclerotic cardiovascular disease (ASCVD) risk calculation


and prevention
➢ Coronary artery disease, ischemic stroke, and peripheral arterial disease
the major atherosclerotic cardiovascular diseases (ASCVD)
➢ Primary prevention of ASCVD is a preventive strategy implemented in
individuals at increased risk before the development of the ASCVD.
➢ Secondary prevention is a preventive strategy implemented in individuals
who have past or current ASCVD.
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➢ ASCVD risk calculation tools are validated tools of predicating the


probability of developing these diseases in the future, generally
expressed as the percentage probability in the coming 10 years
➢ Decision on treatment and intensity of treatment of dyslipidemia for
primary prevention should be based on the calculated ASCVD risk.

Clinical features
➢ Central obesity
➢ High blood pressure
➢ Xanthelasmas and xanthomas
➢ If ASCVD has already developed: angina pain, intermittent claudication,
transient ischemic attacks

Diagnosis and Investigations

➢ The diagnosis of metabolic syndrome is based on the presence of three


of the following five risk factors;

Table: criteria for the diagnosis of metabolic syndrome


No Risk factor Defining level
1. Waist circumference Men >102 cm Women > 88 cm
2. Triglycerides >150 mg/dl
3. HDL cholesterol Men <40 mg/dl Women <50mg/dl
4. Blood pressure 130/85 mm Hg
5. Fasting glucose >100 mg/dl

➢ For calculation of ASCVD risk use the AHA/ACC 2013 ASCVD Risk Calculator
which available as freely downloadable tools for smartphones or online use.
✓ Or you can search from UpToDate like this

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Picture; Calculator: Cardiovascular risk assessment in adults (10-year, ACC/AHA


2013). ACC: American College of Cardiology; AHA: American Heart Association; HDL: high density
lipoprotein; ASCVD: atherosclerotic cardiovascular disease; CHD: coronary heart disease.
✓ This calculator helps predict the 10-year risk of the following hard ASCVD events:
▪ First occurrence of nonfatal myocardial infarction
▪ CHD death
▪ Fatal or nonfatal stroke
✓ This calculator may overestimate risk (see Lancet reference) and a discussion with the patient needs
to ensue if there are any questions.
✓ Risk estimates were developed from cohorts primarily comprising White and African-American subjects.
Risk may be underestimated in American Indians, Asian Americans of South Asian ancestry, and
Puerto Ricans. Risk may be overestimated in Asian Americans of East Asian ancestry and some
Mexican Americans.
✓ This calculator has only been validated for ages 40 to 79 years.

➢ After calculating the 10yr ASCVD, categorize individuals in the age 40-75year
in to the following risk categories.
✓ <5% = LOW RISK
✓ 5 to < 7.5% = BORDERLINE
✓ 7.5 to< 20% = INTERMEDIATE
✓ >20% = HIGH
➢ The presence of CKD, metabolic syndrome, inflammatory diseases like
rheumatoid arthritis and HIV, premature menopause, family history of premature
ASCVD increase the risk and are considered das risk modifiers.
➢ Additional investigations
✓ FBS and HbA1C
✓ Urinary protein/albumin
✓ Creatinine and urea/eGFR

For more about CVD risk assessment refer from Long case of Nitsbin
Under Chapter 1 (click here→WHO risk based CVD (Cardiovascular disease)
Management in Ethiopia)

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Treatment
Non- pharmacologic management

➢ Life-style modification
✓ Diet
▪ Diet that emphasizes intake of vegetables, fruits, whole grains,
legumes
▪ Healthy protein sources (low-fat milk products), low-fat chicken
(without the skin), and fish
▪ Limits intake of sweets, sugar-sweetened beverages, and red
meats
✓ Weight Control
✓ Physical Activity
▪ At least 150 minutes per week (e.g., At least ½ hour 5-7x/wk) of
moderateintensity physical activity or 75 minutes of vigorous
intensity.
▪ Moderate intensity physical activity: typical example brisk walking
▪ Vigorous intensity physical activity: typical example Jogging, running
or biking

Pharmacologic treatment
➢ Statin therapy
✓ The intensity of statin therapy is divided into 3 categories 160 1. High-
intensity statin = lowers LDL-C levels by ≥50% 2. Moderate-intensity statin
= lowers LDL-C levels by 30% to 49%, 3. Low-intensity statin therapy =
lowers LDL-C levels by <30%
✓ Low-intensity statin therapy = lowers LDL-C levels by <30%

Table. Intensity of statin therapy


High intensity Moderate intensity Low
intensity
Atorvastatin 40-80mg 10-20mg -
(commonly used 40mg) ( commonly used 20mg)
Rosuvastatin 20-40mg 5-10mg -
(commonly used 20mg) (commonly used 10mg)
Simvastatin - 20-40mg 10mg
Lovastatin - 40mg 20mg

Table. Indications of statin therapy


High intensity statin Moderate intensity Low intensity

➢ Anyone with LDL-C ➢ Anyone with DM + age 40-75yr ➢ Age 40-75yr,


>190mg/dl ➢ No DM + Age 40-75 + ASCVD Borderline risk (5-
➢ Secondary prevention RISK 7.5-20% + risk enhancers 7.5%) + multiple
➢ Age 40-75yr and ASCVD ➢ Age 20-39yr, LDL>160mg/dl and risk enhancers
risk >20% family history of premature ➢ If moderate intensity
➢ DM, age 40-75yr +risk
enhancers
ASCVD
➢ If high intensity therapy is not
tolerated
therapy is not
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➢ Statin safety
✓ Statin therapy is usually well tolerated and safe.
✓ Some side effects are seen occasionally.
✓ The most common side effect a statin-associated muscle symptom.
Myalgia is more common than genuine myositis, or the very rare
rhabdomyolysis.
✓ If muscle symptoms are mild, another statin can be rechallenged
with a lower intensity.
✓ Statins increase the risk of new onset diabetes modestly but it
should not be reason not to start or withdraw statins.
➢ Other pharmacologic treatments in metabolic syndrome
✓ Hypertension and diabetes should be treated as per the standard
treatment guideline.

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Chapter 16; STI (የአባላዘር በሽታ)


➢ Sexually Transmitted infections (STI’s) are serious and common
problems worldwide.
➢ There are more than 20 types. Many of these are curable with
effective treatment, but continue to be a major health problem for an
individual and the community at large.
➢ With the emergence of HIV/AIDS the management of STIs makes more
serious issue and calls for early screening, effective and urgent
management.
➢ There are two basic approaches in the management of STIs namely
etiologic diagnosis using laboratory tests and syndromic approach. Both
classic approaches present with a number of problems.
1. Etiologic diagnosis approach is often regarded as the ideal way of
diagnosing disease
2. The syndromic approach is the choice of resort when there are no
laboratory facilities. The syndromic case management has the following
key features:
➢ It enables all trained first line health care providers to diagnose STI
syndromes and treat patients on the spot, without waiting for
laboratory results.
➢ It will help to offer treatment on the initial visit which is an important
step to stop the spread of the disease.
➢ It is problem oriented (it responds to the patient’s smx’s).
➢ It is highly sensitive and does not miss mixed infections.
➢ Uses flow charts that guide the health worker through logical steps.
✓ Each flowchart is made up of a series of steps:
▪ The clinical problem- the patient’s presenting symptoms at
the top; this is the starting point
▪ A decision to make, usually by answering “yes” or “no” to a
question
▪ An action to take: what you need to do
➢ Provides opportunity and time for education and counseling.

NB: A number of different organisms that cause STIs give rise to only a
limited number of syndromes.
➢ The aim of syndromic STI management is to identify one of the 7
syndromes and manage accordingly. These are
1) Vaginal discharge
2) Urethral discharges
3) genital ulcer 1266
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4) lower abdominal pain


5) scrotal swelling
6) inguinal bubo
7) neonatal conjunctivitis.

16.1. Vaginal Discharge Syndrome/VDS/


➢ Abnormal vaginal discharge in terms of quantity, color or odor could be
most commonly as a result of vaginal infections.
➢ It is a poor indicator of cervicitis, especially in young girls because a
large proportion of them are asymptomatic.
Etiology
➢ Bacterial vaginosis (Gardnerella vaginalis) is the leading cause of vaginal
discharge in Ethiopia
➢ The following are most common causes of vaginal discharge listed
based on decreasing order of frequency in Ethiopia
✓ Gardnerella vaginalis (Polymicrobial)
endogenous infections
✓ Candida albicans.
✓ Trichomonas vaginalis
✓ Neisseria gonorrhoeae sexually acquired
✓ Chlamydia trachomatis

Risk Assessment

➢ Major risk factor for cervicitis using vaginal discharge as an entry point
to manage cervical infection is far from ideal.
➢ While vaginal discharge is highly indicative of vaginal infection, it is
poorly predictive of cervical infection with gonorrhea and/or chlamydia.
➢ The flowchart may become more predictive of cervical infection if a
number of risk factors indicative of cervical infection are included
➢ N.B. One or more of the following are risk factors for STI related
cevicitis in Ethiopia
✓ Multiple sexual partners in the last 3months.
✓ New sexual partner in the last 3 months
✓ Ever traded sex
✓ Age below 25 years
NB: The presences of one or more risk factor suggest cervicitis.

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Figure; The algorithm of syndromic case management of vaginal discharge

Treatment

➢ Vaginal discharge syndrome can cause devastating complications if left


untreated.
➢ Hence any woman with vaginal discharge syndrome must be treated
promptly.
➢ Look at table below

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16.2. Lower Abdominal Pain/Pelvic inflammatory


disease/(PID)
➢ All sexually active women presenting with lower abdominal pain should
be carefully evaluated for the presence of upper genital tract infections
(tube, uterus, ovaries, and pelvic cavity).
➢ In addition, all women with presumptive STI should undergo thorough
bimanual and abdominal examination because some of the women with
PID may not complain of lower abdominal pain.
➢ Other suggestive symptoms include pain during intercourse, vaginal
discharge, abnormal vaginal bleeding (inter-menstrual), painful urination,
pain during menstruation, fever and sometimes nausea and vomiting.
➢ PID is difficult to diagnose because the clinical manifestations widely
vary.
➢ PID becomes highly probable when one or more of the above symptoms
are seen in a woman with adnexal tenderness, vaginal discharge and
cervical motion tenderness.

Indications for hospital admission with acute PID

➢ The diagnosis is uncertain


➢ Surgical emergencies such as appendicitis and ectopic pregnancy cannot
be excluded
➢ A pelvic mass is suspected
➢ Severe illness precludes management on an outpatient basis
➢ PID in pregnancy
➢ The patient is unable to follow or tolerate an outpatient regimen
➢ Failed to respond to outpatient treatment

N.B. Many experts recommend that all patients with PID should be
admitted to hospital for treatment.

Etiology

➢ The most common causative agents responsible for this syndrome


include N.gonorrhae, C.trachomatis, and anaerobic bacteria.
➢ Facultative Gram-negative rods and Mycoplasma hominis are also
implicated sometimes.
➢ As it is difficult to differentiate between these clinically, and a precise
microbiological diagnosis is nearly impossible in most clinical set ups,
hence the treatment regimen must be effective against the incriminated
microorganisms. 1269
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Figure; The algorithm of syndromic case management of lower abdominal pain

Treatment

➢ Look at table below

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16.3. Urethral Discharge Syndrome (UDS)


➢ Urethral discharge is the presence of abnormal secretions from the distal
part of the urethra and it is the characteristic manifestation of urethritis.
➢ Urethritis is usually due to STI’s although UTI may produce similar
symptoms.
➢ Urethral discharge is one of the commonest STI among men in our
country.

Cause or Etiology of UDS

➢ Urethral discharge can be caused by many different causative micro-


organisms (either single or polymicrobial).
➢ The two most common causative agents of the syndrome are Neisseria
gonorrhea and Chlamydia trachomatis (81% and 36.8% respectively).
➢ Most of the time urethral discharge is due to mixed infection of
Neisseria gonorrhea and Chlamydia trachomatis
➢ Some of the other causative micro-organisms are mycoplasma
genitalium, Trichomonas vaginalis, and Ureaplasma urealyticum.
➢ In some rare cases it can be also the result of non-infectious causes.
➢ Due to these reasons urethral discharge is a syndrome of many causes
rather than a single disease to be dealt with and it needs to be dealt
with as a syndrome while it is being managed.

Clinical manifestations of UDS


➢ The common signs and symptoms of UDS are
✓ Burning sensation (dysuria) during micturition
✓ Increased urgency and frequency of urination
✓ Itching sensation of the urethra.
➢ Urethral discharge:
✓ The amount and nature of the discharge vary according to the
causative agents and other factors like prior treatments with
antibiotics.
✓ The appearance of the discharge can be purulent or mucoid, clear,
white, or yellowish, green.
✓ Sometimes it can be associated with scrotal swelling and pain
which tends to be unilateral.
✓ The urethritis caused by N. gonorrhea has usually an acute onset
with profuse and purulent discharge and the one caused by C.
trachomatis has sub-acute onset with scant mucopurulent discharge. 1271
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Complications of UDS
➢ Common acute complications
✓ Disseminated gonococci syndrome
✓ Perihepatitis
✓ Acute epididymoorchitis
➢ Common chronic complications
✓ Urethral stricture
✓ Infertility
✓ Reiter’s syndrome (the most common type of inflammatory
polyarthritis in young men)

Figure; The algorithm of syndromic case management of urethral discharge syndrome

Treatment of UDS
➢ UDS needs to be treated ASAP because if it is not treated on time it
can cause serious complication.
➢ Treatment should target gonorrhea and chlamydial infections.
➢ Look at the table below

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16.3.1. Persistent/Recurrent Urethral Discharge

➢ Some patients may complain of persistent or recurrent burning sensation


or dysuria on urination, with or without discharge, due to various
reasons.
✓ Inadequate treatment or poor compliance and/or
✓ Re-infection (partner/s not managed)
✓ Persistent urethritis after Doxycycline based treatment might be
caused by doxycycline resistant M. genitalium
✓ T. vaginalis is also known to cause Urethritis in men, hence the
index patient should be treated for this.
✓ Infection by drug-resistant organisms (N. gonorrhea)

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Figure: The algorithm of syndromic case management of persistent or recurrent urethral


discharge syndrome in men

Treatment of Persistent/Recurrent Urethritis Syndrome

➢ Look at table below

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16.4. Genital Ulcer Syndrome (GUS)

➢ Genital ulcer is an open sore or a break in the continuity of the skin or


mucous membrane of the genitalia as a result of sexually acquired
infections.
➢ Genital ulcer facilitates transmission of HIV more than other STI
because it disrupts continuity of skins and mucous membranes
significantly.
➢ The relative prevalence of causative organisms for GUD varies from
place to place; hence clinical differential diagnosis of genital ulcers is
inaccurate in places where there are several etiologies.

Etiology of Genital Ulcer Syndrome


➢ HSV (HSV-1 and HSV-2)
➢ Treponema pallidum
➢ Haemophilius ducreyi (Chancroid)
➢ Chlamydia trachomatis serovar L1, L2 & L3 (LGV)
➢ Klebsiella granulomatis

➢ Most cases of genital herpes are caused by HSV-2 in both males and
females constituting 44% and 76% of the cases respectively.Moreover,
dual infection with other genital ulcer pathogens is 52% of males and
78% of females.

Clinical presentations
➢ Clinical manifestation and patterns of GUS may vary with presence of
HIV infection.
➢ Genital ulcer has different kinds of clinical manifestations due to different
causatives.
➢ Common clinical manifestations of genital ulcer are:
✓ Constitutional symptoms such as fever, headache, malaise and
muscular pain
✓ Recurrent painful vesicles and irritations
✓ Shallow and non-indurated tender ulcers
✓ Common sites in male are glance penis, prepuce and penile shaft
✓ Common sites in women are vulva, perineum, vagina and cervix
and can cause occasionally severe vulvo-vaginitis and necrotizing
cervicitis
✓ Painless indurated ulcer (Chancre)
✓ Regional lymph adenopathy 1275
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Common causes of GUS

➢ Genital herpes:
✓ HSV is the most common causes of genital ulcer worldwide.
✓ It produces lifelong infection after the primary infection (latency).
✓ The lesions are painful, erythematous macules which progressively
form vesicles, pustules, ulcer and crusts.
➢ Chancroid (ከርክር)
✓ Chancroid is also the common cause of genital ulcer in developing
countries.
✓ The lesion started as painful papules and pustules which ulcerate
with dirty base and soft edge.
✓ Inguinal fluctuant adenopathy (buboes) may occur following ulcer.
➢ Syphilis:
✓ Clinically has three stages (primary, secondary, tertiary).
✓ The ulcer starts during the primary stage of the disease as papules
& rapidly ulcerate.
✓ The ulcer is typically painless, clean base and raised boarder.
➢ Lymphogranuloma veneurum (LGV):
✓ The disease starts as painless papules that develops an ulcer.
✓ After a few days painful regional LAP develop and associated
systemic symptoms may occur.
➢ Granuloma inguinale (Donovanosis):
✓ It is chronically progressive ulcerative disease without systemic
symptoms.
✓ Presents with non-suppurative painless genital ulcer and beefy-red
appearance

Complications of genital ulcer syndrome


➢ Locally destructive granulomatous lesions (Gummas) occur on the skin,
liver, bones, or other organs
➢ Tabes dorsalis and dementia, often with paranoid features
➢ Latent meningovascular parenchymatous
➢ Optic atrophy
➢ General paresis
➢ Aortic aneurysm and aortic valve insufficiency
➢ Asymptomatic aortitis
➢ Angina pectoris
➢ Recurrent disease
➢ Aseptic meningitis
➢ Encephalitis
➢ Phimosis in men
➢ Destruction of the penis or auto amputation 1276
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➢ Extra genital lesions

Figure: The algorithm of syndromic case management of genital ulcer syndrome

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Treatment of genital ulcer syndrome


➢ To avoid the complications, some of which are life threatening as
mentioned above, the syndrome must be treated aggressively and
promptly.

Non-pharmacologic

➢ Prevent secondary infection by local cleaning

Pharmacologic

➢ Look at table below

16.5. Scrotal Swelling

➢ Inflammation of the epididymis usually manifests with acute onset of


unilateral testicular swelling, often with tenderness of the epididymis and
vas deferens, and occasionally with erythema and edema of the
overlying skin.
➢ When it occurs in young male (<35 years old) accompanied with
urethral discharge it is usually due to gonococcal or chlamydial
infections.
➢ In older people the etiologic agent may be non-STIs such as E. coli,
Klebsiella spp. or Pseudomonas.
➢ TB orchitis is generally accompanied by an epididymitis

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Figure: The algorithm of syndromic case management of Scrotal Swelling

Treatment
➢ If quick and effective therapy is not given, the complications (Destruction
and scarring of testicular tissues, infertility, impotence, and prostatitis)
may occur.
➢ The treatment of scrotal swelling suspected of STI origin is similar to
that of urethral discharge
➢ In addition, analgesia and scrotal support may be indicated as required.

Non-pharmacologic:

➢ Scrotal support

Pharmacologic

➢ Look at table below


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16.4. Inguinal Bubo

➢ It is a painful, fluctuant, swelling of the lymph nodes in the inguinal


region (groin).
➢ Buboes are usually caused by either chancroid or LGV.
➢ In many cases of chancroid, but not all, an associated ulcer is visible.
➢ Infection of the lower limb and other non-STIs like TB can also cause
swelling of the inguinal lymph nodes.

Etiology → common causes of inguinal and femoral bubo are

➢ Chlamydia trachomatis (L1, L2 and L3) (causes LGV)


➢ Klebsiella granulomatis (donovanosis)
➢ Treponema pallidum (causes syphilis)
➢ Haemophilius ducreyia (causes chancroid)

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Figure: The algorithm of syndromic case management of urethral discharge syndrome

Treatment
Non pharmacologic:

➢ Keep the lesion clean and dry

Pharmacologic

➢ Look at table below

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16.5. Neonatal conjunctivitis.


Refer updated NICU guideline

Syphilis (ቂጥኝ)
➢ Syphilis is caused by the bacterium Treponema pallidum.
➢ During initial stage of infection, the organism spreads widely, setting the
point for consecutive manifestations.
➢ Syphilis is important health concern for women, especially HIV-infected
women.
➢ Adverse pregnancy outcomes such as miscarriage or stillbirth, congenital
syphilis in the new born and progression of latent syphilis in the mother
are anticipated complications if the mother is left untreated.
➢ Thus, RPR test should be routinely done on pregnant mothers in their
first trimester and treatment should be instituted if the rapid plasma
regain (RPR) test is reactive.

Staging and clinical manifestations


➢ Each stage of syphilis has characteristic clinical presentations not altered
by pregnancy

i. Early syphilis

A. Primary syphilis: chancre (ከርክር)


✓ Typically involves of a solitary painless chancre at site of
inoculation, complemented by local adenopathy.

B. Secondary syphilis:
✓ A systemic illness often including a rash (The rash is classically a
diffuse, symmetric macular or papular eruption involving the entire
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trunk and extremities including the palms and soles), malaise, fever,
and other symptoms such as pharyngitis, mucous patches, hepatitis,
condyloma lata, alopecia.

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C. Early latent:

✓ Period infection with T. pallidum as demonstrated by serologic


testing, but no symptoms. Occurs within first year of initial infection.

ii. Late syphilis

➢ Approximately 25 to 40% of patients with untreated syphilis can develop


late disease.
➢ The clinical events may appear at any time from 1 to 30 years after
primary infection.
➢ It is not necessary for individuals to have experienced clinically
symptomatic primary or secondary syphilis prior to developing late
syphilis
➢ The most common manifestations of late syphilis include:
✓ Cardiovascular syphilis (especially aortitis)
✓ Gummatous syphilis (granulomatous, nodular lesions which are rare,
can occur in a variety of organs, usually skin and bones)
✓ CNS involvement (particularly general paresis and tabes dorsalis)

D. Tertiary syphilis:
➢ Late syphilis with symptomatic manifestations involving the CVS or
gummatous disease (granulomatous disease of skin and subcutaneous
tissues, viscera, or bones).

E. Late latent syphilis:


➢ Period of infection with T. pallidum as demonstrated by serologic testing,
but no symptoms. Occurs after one year after initial infection, but if
timing of infection is not known, late latent syphilis is presumed.
Neurosyphilis

➢ May happen at any time in the course of infection. 1284


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a. Early neurosyphilis:
➢ may have asymptomatic meningitis; symptomatic meningitis; or less
commonly meningovascular disease (ie, meningitis and stroke).
➢ Vision or hearing loss with or without concomitant meningitis may also
be present, and ocular/otologic syphilis is treated as neurosyphilis.

b. Late neurosyphilis:
➢ The most common forms involve brain and spinal cord (dementia -
general paresis and tabes dorsalis).

Complications of syphilis
➢ If untreated, Syphilis have a number of significant late manifestations or
complications, including cardiovascular, gummatous, and neurologic cxn.

Investigations (screening and diagnosis)


➢ Diagnostic testing should be made for all patients with signs and
symptoms of syphilis.
➢ Asymptomatic patients had better be screened for syphilis if at high risk
for acquired disease or for transmitting infection to others (eg,
pregnancy).

DIAGNOSTIC TESTS

➢ Serologic tests
✓ Serologic tests provide a presumptive diagnosis of syphilis. 1285
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✓ There are two types of serologic tests for syphilis: nontreponemal


tests and treponemal-specific tests.
➢ Nontreponemal tests include:
✓ Rapid plasma reagin (RPR)
✓ Venereal Disease Research Laboratory (VDRL)
✓ Toluidine Red Unheated Serum Test (TRUST)
➢ Specific treponemal tests include:
✓ Fluorescent treponemal antibody absorption (FTA-ABS)
✓ Micro hemagglutination test for antibodies to T. pallidum (MHA-TP)
✓ T. pallidum particle agglutination assay (TPPA)
✓ T. pallidum enzyme immunoassay (TP-EIA)
✓ Chemiluminescence immunoassay (CIA)
➢ Direct methods for diagnosis
✓ Direct methods can be used to provide a definitive diagnosis of
syphilis.
✓ Since T. pallidum cannot be cultured in the laboratory, the organism
must be identified through direct visualization or detection in clinical
specimens.
i. Darkfield microscopy and direct fluorescent antibody (DFA) testing can be
used to detect the organism;
✓ However, neither of these tests are routinely available in clinical
settings because these methods require special equipment to
perform the test, as well as considerable experience and expertise
to properly interpret the results.

ii. PCR

Diagnosis and interpretation of results

➢ Diagnostic evaluation for syphilis is the same in pregnant and


nonpregnant women.
➢ A diagnosis of syphilis is made using serologic testing of blood
specimens (presumptive diagnosis than definitive).
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➢ A diagnosis is made when both nontreponemal and treponemal tests are


reactive.
➢ Nevertheless, either test can be used as the initial screening test. But
due to high possibility of false positive screening test results,
confirmatory testing is necessary.
➢ If neurosyphilis considered, additional CSF analysis should be performed.
➢ Appropriate interpretation of serologic testing (depends on clinical
disease presence or absence, patient's prior syphilis history, and
individual's immune status):
✓ If no prior syphilis history: diagnosis made if both nontreponemal &
treponemal tests are reactive.
✓ If has history of treated syphilis: a positive nontreponemal test may
suggest a new infection, evolving response to recent therapy,
treatment failure, or presence of a serofast state.
➢ False positive and false negative results
✓ A positive nontreponemal test followed by a negative treponemal
test: generally considered a false positive result.
✓ An initial treponemal-specific screening may have a positive
treponemal test followed by a negative nontreponemal test. This is
usually seen for previously treated syphilis. Also, in very early
syphilis (occasional), or in late syphilis when nontreponemal tests
become nonreactive over time.
✓ Patient with clinical signs and symptoms of early syphilis (eg, ulcer,
rash) may have false negative result for initial nontreponemal test,
classically due to testing prior to antibody formation or secondary to
a prozone effect.
➢ Latent syphilis: diagnosed if no clinical signs or symptoms of syphilis but
has serologic evidence of infection. Early or late latent depending upon
duration of infection- if duration unknown considers it as late syphilis.
➢ All diagnosed cases of new syphilis should be treated, tested for HIV
and other STD.

Screening

➢ Pregnant women should be screened for syphilis.


✓ False-positive screening tests may be more common in the setting
of pregnancy. Thus, confirmatory testing must be performed
(algorithm)
➢ asymptomatic patients should be screened for syphilis if they are at high
risk for having acquired disease or for transmitting disease to others.

Pre-treatment evaluation
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➢ A nontreponemal titer should be obtained just before starting therapy


(preferably, on the first day of therapy) since titers can increase
significantly over a few days between diagnosis of syphilis and treatment
initiation.

Treatment

➢ Penicillin remains the gold standard treatment for syphilis in both


pregnant and nonpregnant patients appropriate for their stage of
infection.
➢ Parenteral (IM or IV) penicillin G is the only therapy with recognized
efficacy and safety for both mother and fetus during pregnancy. It is
effective for treating maternal disease, preventing transmission to the
fetus, and treating established fetal disease.
➢ Alternatives are not as safe for pregnant woman or fetus or not as
effective for prevention of congenital syphilis. Hence, if possible,
desensitize allergic patients and treat with IV penicillin.

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Table: Treatment of syphilis for pregnant and non-


pregnant adults with normal renal function

Stage of syphilis* Treatment

N.B If possible, desensitize allergic patients and treat with IV penicillin


Non-pregnant adults Pregnant adults
Early syphilis Firs line: ➢ Benzathine Penicillin G (Bicillin L-A)
(Primary/secondary/early ➢ Benzathine Penicillin G 2.4 million 2.4 million units(MU) IM Stat
latent) < 2 years units IM stat (administer as 1.2 MU in each
duration Alternatives: buttock)
➢ Ceftriaxone 1 - 2g IV/IM daily for If serologic failure on follow-up:
10 to 14 days or ➢ additional follow-up not assured,
➢ Erythromycin 500 mg PO QID Prompt CSF and retreating as late
for 14 days or syphilis is recommended.
➢ Doxycycline 100 mg PO BID for 14
days or
➢ Tetracycline 500 mg po QID for 14
days or
➢ Amoxicillin 3 g plus probenecid 500
mg, both given PO BID for 14 days
Late syphilis (Late Firs line: ➢ Benzathine Penicillin G (Bicillin L-A)
latent/tertiary/unknown ➢ Benzathine Penicillin G 2.4 million 2.4 million units IM once weekly
duration) > 2 years units IM once weekly for 3wks (administer as 1.2 MU in each
duration Alternatives buttock) for 3 weeks (7.2 million
➢ Ceftriaxone 2g IV/IM daily for 10 to units total dose)
14 days or If a dose is missed for > 14 days,
➢ Erythromycin 500 mg PO QID ➢ restart the full 3 dose course of
for 30 days or therapy.
➢ Doxycycline 100 mg PO BID for 4
weeks

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Neurosyphilis (including First line: ➢ Aqueous crystalline penicillin G 3 to


ocular syphilis) ➢ Aqueous penicillin G 3 to 4 million 4 Million Units IV every 4 hours or
units IV every four hours (or 18 to as a continuous infusion over 24
24 million units continuous IV hours (18 to 24 MU/day) for 10 to
infusion) for 10 to 14 days or 14 days OR
➢ Penicillin G procaine 2.4 million ➢ Penicillin G procaine 2.4 million
units IM daily plus probenecid 500 units IM once daily (usually
mg PO QID, both for 10 to 14 administered as 1.2 MU in each
days buttock) plus probenecid 500 mg
➢ If possible, desensitize allergic PO QID, both for 10 to 14 days
patients and treated with IV
penicillin

Alternatives:
➢ Ceftriaxone 2 g IV daily for 10 to
14 days OR
➢ doxycycline 200 mg PO BID for 21
to 28 days (If no ceftriaxone or
allergic to it)
➢ After IV treatment completion, single dose of 2.4 million Units Benzathine
Penicillin G (for non-pregnant) and once/week for 3 weeks (pregnant) can be
used
Post-exposure See discussion below ➢ Penicillin G benzathine (Bicillin L-A)
prophylaxis 2.4 million units IM stat (administer
as 1.2 MU in each buttock)
*The National STI Guideline (2015) consider and manage a history of non-reactive RPR test within the
past 2 years as early syphilis and infections more than two years ago or no prior history of non-reactive
RPR test (unknown duration) as late syphilis.

Complications of treatment among pregnants


➢ Jarisch-Herxheimer reaction:
✓ this may precipitate uterine contractions, preterm labor, and/or no
reassuring fetal heart rate (NRFHR) tracing in pregnant women
treated in the 2nd TM of pregnancy.
✓ Provide supportive care of maternal distress and standard obstetric
management of pregnancy complications.

Follow-up
➢ Monitor clinically and with serologic testing after treatment to ensure
response.
➢ Frequency of follow up and interpretation of nontreponemal titers;
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➢ Frequency of serologic monitoring depends on stage of disease &


existence of HIV:
✓ In HIV-uninfected with early syphilis: test at 6 and 12-months
following treatment and at any time if clinical symptoms recur. In
general, such patients experience adequate response by 12 months.
✓ HIV-uninfected with late syphilis: follow-up serologic testing at 6, 12,
and 24 months. Some with late syphilis may not have adequate
response for up to 2 years after treatment.
✓ HIV co-infected: should be monitored more frequently.
✓ Neurosyphilis: Monitored at same frequency as without
neurosyphilis. Additional, monitoring of CSF abnormalities is
necessary.
✓ Pregnant women; follow-up frequency is the same to non pregnants
and depends on stage of disease and HIV coinfection.

➢ The same test, preferably RPR, should be done each time and at the
same laboratory.
➢ A 4 times increase in nontreponemal titer after treatment is always
abnormal.
➢ A 4 times decrease in titer, equivalent to a change of two dilutions
(such as from 1:16 to 1:4 or 1:32 to 1:8), is considered as acceptable
response to therapy; but this may take months to attain.
➢ For pregnant a fall in maternal titers does not guarantee that fetal
treatment has been adequate.
➢ Over time, most successfully treated syphilis patients experience
seroreversion; but some may remain serofast.

Handling treatment failure


➢ Suspect failure if nontreponemal titers do not decline ≥ 4 times, or if 4
times increase after an initial decline.
➢ If no adequate response to treatment, determine if reinfected,
experiencing a slow response to treatment, or has failed treatment.
➢ Treatment failure is likely due to poor adherence, alternative agent use,
immunosuppressed status, or unrecognized CNS disease.

Treatment after an exposure

Sexually partners:

➢ Should be evaluated clinically and serologically for evidence of infection.


➢ Empiric treatment requirement depends primarily upon when the
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Vertical transmission (VT)

➢ Frequency is higher with early than late stage syphilis.


➢ Among women who acquire syphilis during pregnancy, the risk of VT
increases with increasing gestational age at acquisition of maternal
infection.
➢ Fetal infection should be suspected if there are characteristic findings on
ultrasound examination after 20 weeks of gestation in a woman with
untreated or inadequately treated syphilis.
➢ Hepatomegaly and placentomegaly are early findings suggestive of
congenital syphilis. Anemia, ascites and hydrops occur later in course of
fetal infection. An abnormal ultrasound is not diagnostic and the normal
also does not exclude fetal infection.

Fetal treatment

➢ Maternal penicillin treatment is curative for fetal infection in most cases.


➢ A maternal treatment ≤ 30 day before delivery is a risk factor for
congenital infection.
➢ A maternal treatment with non-penicillin agents is also a risk factor.
➢ Aqueous crystalline penicillin G 50, 000 units/kg IV TID for 10-15 days
OR procaine penicillin G 50,000 units/kg IM daily for 10 -15 days for
prevention (at risk cases) and treatment of congenital syphilis.

Gonorrhea (ጨብጥ)
➢ Gonorrhea is an infection with the gram-negative coccus Neisseria
gonorrhoeae
➢ Gonorrhea is a major cause of urethritis in men and cervicitis in women;
the latter can result in PID, infertility, ectopic pregnancy, and chronic
pelvic pain.
➢ Gonococcal infections, including urethritis, cervicitis, epididymitis, and
proctitis, are a significant cause of morbidity among sexually active men
and women worldwide.
➢ Urogenital, anogenital, pharyngeal, and ocular gonococcal infections that
are not associated with bacteremia or ascending spread of the pathogen
to other organs are considered uncomplicated.
➢ Extragenital infections of the pharynx and rectum are prevalent in certain
groups, such as men who have sex with men (MSM).
➢ Invasive infections with N. gonorrhoeae, including disseminated
gonococcal infection, endocarditis, and meningitis, are uncommon but
can result in serious morbidity (complicated) 1292
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DIAGNOSTIC APPROACH
➢ Clinical syndrome approach (preferred in our setup) → which can
manifest as VDS, UDS, PID, conjunctivitis…
➢ nucleic acid amplification testing (NAAT) is the test of choice for the
initial microbiologic diagnosis of N. gonorrhoeae infection, although
culture remains an important diagnostic tool when antibiotic resistance is
suspected.
➢ If NAAT methods are unavailable, microscopy (for men), culture, antigen
detection, and genetic probe methods can be used with endocervical or
urethral swabs.

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Management
A. Syndromic approach is recommended (refer mgt of VDS, UDS, PID)
B. Mgt based on specific diagnosis
i. Uncomplicated gonorrhea: Cervicitis, proctitis, urethritis, pharyngitis:

First line
✓ Ceftriaxone 250mg IM stat plus
✓ azithromycin 1g po stat

Alternatives
Patients with severe cephalosporin allergy
✓ azithromycin 2 g PO stat
plus
✓ gentamicin 240mg IM stat or
✓ Gemifloxacin 320mg PO stat

If ceftriaxone unavailable
✓ Cefixime, 400 mg as a single dose in combination with oral
azithromycin
▪ Not recommended due to limited efficacy

ii. Conjunctivitis

✓ Ceftriaxone 1 g IM stat plus


✓ Azithromycin 1 g PO stat

additionally, consider a one-time saline lavage of the infected eye for


conjunctivitis.

iii. Disseminated gonococcal infection (arthritis and arthritis-dermatitis


syndrome)

✓ Ceftriaxone 1g IV/IM daily


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▪ Duration; for 24 to 48 hours after clinical improvement, then


may switch to an oral agent guided by antimicrobial
susceptibility to complete a total of at least 7 days of therapy
plus
✓ Azithromycin 1 g PO stat

iv. Gonococcal Endocarditis

✓ Ceftriaxone 1 to 2 g daily or BID for at least 28 days plus


✓ Azithromycin 1 g PO stat

v. Gonococcal Meningitis:

✓ Ceftriaxone 1 to 2 g daily or BID for 10 to 14 days plus


✓ Azithromycin 1 g PO stat

Gonococcal infection, expedited partner therapy

✓ Ceftriaxone 250mg IM stat plus


✓ azithromycin 1g po stat

Note:
➢ To be used only for heterosexual partners with gonorrhea if health
department partner-management strategies are impractical/unavailable
and there is concern by the provider for the prompt evaluation and
treatment of the partner
➢ Provide written materials to educate partners about their exposure to
gonorrhea, importance of therapy, and when to seek clinical evaluation
for adverse reactions/complications

Treatment failure
➢ Note: Reinfections are more likely to occur than actual treatment
failures,
➢ Re-treatment with preferred dual-therapy regimen is recommended for re-
infection.
➢ Choice of agent (e.g. ceftriaxone, Gemifloxacin, or gentamicin) to
combine with azithromycin following treatment failure varies considerably
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depending on the failed initial dual-therapy regimen, susceptibilities of


isolate, and geographic location

Management of Treatment failure

➢ Treatment failure following single-therapy regimen or other non-preferred


treatment regimens:
✓ Ceftriaxone 250mg IM stat plus
✓ azithromycin 1g po stat
➢ Treatment failure following initial therapy of an alternative dual therapy
regimen (cefixime and azithromycin):
✓ Ceftriaxone 250mg IM stat plus
✓ azithromycin 2g po stat
➢ Treatment failure following initial therapy of the preferred dual-therapy
regimen (ceftriaxone and azithromycin):
✓ Ceftriaxone 500mg IM stat plus
✓ azithromycin 2g po stat

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Table; Pharmacologic Treatment of STI

Treatment
N.B For all STI, in addition to treatment, educate the patient on
Type of STI ➢ Abstinence from sex and avoiding alcohol intake till all symptoms
resolve and management completed
➢ Sex Partner notification and management based on type of STI and
indication
➢ Importance of HIV testing
➢ Proper and consistent use of condom
➢ Risk reduction
➢ Treatment compliance
Risk assessment +ve Risk assessment -ve
➢ Ceftriaxone 250mg IM stat or ➢ Metronidazole 500
➢ Ciprofloxacin 500mg po stat or mg bid for 7 days
Vaginal Discharge
➢ Spectinomycin 2 gm IM stat If discharge is white
Syndrome
PLUS or curd-like add
➢ Azithromycin 1gm po stat or ➢ Clotrimazole vaginal
➢ Doxycycline 100 mg po bid for 7 days pessary 200 mg at
PLUS bed time for 3
➢ Metronidazole 500 mg bid for 7 days days OR
➢ Miconazole vaginal
If discharge is white or curd-like add > pessary 200mg at
Clotrimazole vaginal pessary 200 mg at bed time for 3
bed time for 3 days days.

Note: The preferred regimen is Ceftriaxone


250mg IM stat + Azithromycin 1gm po stat +
Metronidazole 500 mg bid for 7days
Sex Partners
➢ Examination and treatment usually not necessary if the risk
assessment is negative.
➢ However, treatment with an imidazole cream (e.g, miconazole,
clotrimazole) may be indicated in some cases of recurrent infection,
or if the partner has penile candidiasis (Balanitis).
Outpatients In patients

Lower Abdominal Pain

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➢ Ceftriaxone 250 mg IM stat or ➢ Ceftriaxone 250 mg IM/IV or


➢ Ciprofloxacin, 500mg po stat or ➢ Spectinomycin 2 gm IM BID
➢ Spectinomycin 2gm IM stat PLUS
PLUS ➢ Azithromycin 1gm po daily or
➢ Azithromycin 1gm po stat or ➢ Doxycycline 100 mg po BID
➢ Doxycycline 100 mg po BID for 14 for 14 days
days PLUS
PLUS ➢ Metronidazole 500 mg po BID
➢ Metronidazole 500 mg po BID for for 14 days
14 days
Note: The preferred regimen is Note: For inpatient PID,
➢ Ceftriaxone 250mg IM stat PLUS ceftriaxone, spectinomycin or
➢ Azithromycin 1gm po stat PLUS azithromycin should continue for
24hrs after the patient remain
➢ Metronidazole 500 mg bid for 14
clinically improved, after which
days doxycycline and metronidazole
should continue for a total of 14
Admit if there is no improvement days
within 72 hours
First line (preferred)
➢ Ceftriaxone 250mg IM stat plus
➢ Azithromycin 1gm po stat
Urethral Discharge Alternative
Syndrome ➢ Ciprofloxacin, 500mg PO stat or
➢ Spectinomycin 2 gm IM stat
PLUS
➢ Doxycycline 100 mg po bid for 7 days or
➢ Tetracycline 500 mg po QID for 7 days or
➢ Erythromycin 500 mg po QID for 7 days (in cases of
contraindications for Tetracycline. e.g. for children and pregnancy)

NB:
➢ Patients should be advised to return if symptoms persist for 7 days
after the initiation of treatment.
➢ Single dose treatment is encouraged as much as possible
➢ Re-treat with initial regimen
✓ If non-compliant or re-exposure occurs, re-treat with the initial
regimen with due emphasis on drug compliance and/or partner
management.
Persistent/Recurrent ✓ Cover M. genitalium and T. vaginalis
Urethral Discharge ➢ If compliant with initial regimen and re-exposure can be excluded, the
recommended drug for persistent or recurrent urethral discharge
syndrome in Ethiopia is:
✓ Metronidazole 2 gm po. Stat or
✓ Tinidazole 1gm po once for 3 days (Avoid Alcohol!)
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PLUS
✓ Azithromycin 1g PO, stat (only if not used during the initial
episode to address doxycycline resistant M.genitalium)
➢ Despite all these treatments, if symptoms still persist to require
treatment with a new antibiotic regimen and a sexually transmitted
agent is the suspected cause, all partners in the past 3 months
before the initial diagnosis and any interim partners should be
consulted to a gynecologist for evaluation and appropriate treatment
of treatment failure.
A. Treatment for non- vesicular genital ulcer
➢ Benzathine penicillin, 2.4 million units IM stat or
➢ Doxycycline (in penicillin allergy) 100mg bid for 14 days
Genital Ulcer PLUS
Syndrome (GUS) ➢ Ciprofloxacin 500mg PO bid for 3 days or
➢ Erythromycin 500mg PO QID for 7 days
PLUS
➢ Acyclovir 400mg PO, TID for 10 days (or 200 mg 5 times per day of
10 day)

B. Treatment for vesicular, multiple or recurrent genital ulcer


➢ Acyclovir 400 mg PO TID for 7 days or 200 mg 5 times per day for
10 days

N.B. There is no medically proven role for topical acyclovir, its use is
discouraged.

C. Treatment for recurrent infection episodes:


➢ Acyclovir 400 mg P.O. TID for 5 to 7 days,

Treatment should be initiated during prodrome or immediately after onset


of symptoms.
Local care: Keep affected area clean and dry

D. Suppressive treatment: recommended for patients with ≥ 6


recurrences per year
➢ Acyclovir, 400mg P.O. BID for 1 year
N.B. The need for continued suppressive therapy should be reassessed.
First line (preferred)
➢ Ceftriaxone 250mg IM stat plus
Scrotal Swelling ➢ Azithromycin 1gm po stat
Alternative
➢ Ciprofloxacin, 500mg PO stat or
➢ Spectinomycin 2 gm IM stat
PLUS
➢ Doxycycline 100mg po bid for 7 days or
➢ Tetracycline 500 mg po QID for 7 days or
➢ Erythromycin 500 mg po QID for 7 days (in cases of
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contraindications for Tetracycline e.g. for children and pregnancy)


First line
➢ Ciprofloxacin, 500mg P.O, BID for 3days
Inguinal Bubo PLUS
➢ Doxycycline, 100mg P.O, BID for 14days OR
➢ Erythromycin, 500mg, P.O, QID for 14days

If patient have genital ulcer, add


➢ Acyclovir 400mg PO TID for 10 days (or 200mg 5 times per day for
10 days)

➢ N.B. Fluctuant lymph nodes should be aspirated through healthy skin


but incision and drainage or excision of nodes may delay healing
and should not be attempted
➢ If there is doubt with diagnosis and/or treatment failure
✓ Do culture and sensitivity test, if available DNA PCR and treat
accordingly.

Prevention of STIs
➢ Comprehensive approach to STI prevention includes
✓ Risk assessment with counseling
✓ Vaccination
✓ Identification of infected individuals and effective treatment with
follow-up
✓ Evaluation and treatment of sexual partners.

➢ Accurate risk assessment, education and counseling of at-risk


individuals to avoid STIs
✓ Carefully obtain routine sexual histories for proper screening and
prevention counseling.
✓ Behavioral risk factors include:
▪ New or multiple sex partners
▪ sex partners with recent STI no or inconsistent condom use
outside a monogamous sexual partnership, Commercial sex
work for money or drugs
▪ Sex workers or sexual contact with them
✓ Careful evaluation of adolescents and pregnant is important for the
high risk for STI.
✓ All individuals evaluated for STI screening or diagnosis should be
tested for HIV infection.
✓ Patient-centered risk reduction counseling:
▪ assess patient's understanding of STI transmission risk
▪ discuss risk of patient's sexual behavior
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▪ assessing patient's willingness to change behaviour, have


shared goal for behavioral change, with clear & realistic
steps.
✓ Prevention may include abstinence, mutual monogamy, barrier
methods (Male and female condoms).
✓ Use of male condoms has been associated with a reduced risk for
HIV, chlamydia, gonorrhea, HSV, and HPV transmission.

Vaccination

➢ Pre-exposure vaccinations of at-risk individuals for vaccine-preventable


infections avoid several sexually transmitted or associated infections:
✓ Hepatitis A virus (HAV) vaccine→ individuals with CLD, and those
with risk factors for HAV infection (like illicit drug use).
✓ Hepatitis B virus (HBV) vaccine → for nonimmune individuals with
STI risk factors, comprising injection drug users and HIV-infected
ones.
✓ Human papillomavirus (HPV) vaccine→ Gardasil have recently been
developed to prevent HPV type 16 and 18 infections which are
associated with 80% of cervical cancer. It is offered to all girls who
are age 14 in Ethiopia.
✓ Meningococcal vaccine→ for persons exposed to outbreaks, HIV-
infected ones, among others.
➢ Identification of both asymptomatic and symptomatic individuals with STIs
can avoid unrecognized transmission.
➢ Effective diagnosis, treatment, counseling, and follow-up of infected
individuals is also critical component of STI prevention.
➢ Sex partners of infected individuals should also be evaluated, treated,
and counseled to prevent persistent infection transmission.

Other prevention methods:


➢ Male circumcision: may reduce HIV acquisition; also decrease risk of
HSV and HPV infection.
➢ Antimicrobial-based prevention may include:
✓ antiretroviral treatment (preexposure prophylaxis, and post-exposure
prophylaxis, to prevent HIV infection)
✓ Suppressive antiviral therapy for genital herpes simplex virus (HSV)
can prevent transmission.

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Chapter 17; Sepsis


Sepsis is life-threatening organ dysfunction caused by a dysregulated
host response to infection.
Sepsis and septic shock are the major causes of morbidity and mortality
worldwide.
The morbidity and mortality seems higher among extreme age groups
(neonates and elderly) than adults.

Cause
✓ Sepsis is caused by an immune response triggered by an infection.
✓ The infection is most commonly bacterial. Fungi, viruses, or parasites
can also cause sepsis.
✓ The most common primary sources that leads to sepsis was respiratory
tract, brain, urinary tract, skin, and abdominal organ infections.
✓ RF for sepsis
▪ Young or old age
▪ a weakened immune system from conditions such as cancer or
diabetes
▪ major trauma or burns

Clinical presentations
Common signs and symptoms of include
✓ Fever,
✓ Tachycardia
✓ Tachypnoea
✓ confusion.
✓ There may also be symptoms related to a specific infection, such as
a cough with pneumonia, or painful urination with a kidney infection.
✓ In the very young, old, and immunocompromised patients, symptoms
of a specific infection may not present and the body temperature
may be low or normal rather than high.

Investigation and diagnosis


The diagnosis of sepsis depends on
▪ Age
▪ clinical presentation
▪ types of infection and other factors.
Different screening tools were available for Sepsis. This may include
1. SIRS (Systemic Inflammatory Response Syndrome) → no more
used
2. SOFA (sequential Organ Failure Assessment)
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3. quick SOFA (qSOFA).

❖ However, they may need validation to the local contexts as they were
developed based on western patient data.

Quick SOFA (qSOFA) score.

❖ Given the limitations an adult patient with suspected infection can be


quickly screened for likelihood of having poor outcomes if they have at
least 2 of the following 3 clinical criteria (qSOFA):
1. RR ≥ 22 BPM
2. SBP ≤ 100 mmHg
3. Altered mentation.
❖ This simple bedside risk stratification tool (qSOFA) is best used to
identify patients at risk of sepsis in out of-hospital, emergency
department and general hospital ward settings (less useful for ICU
patients, SOFA is better predictive for ICU).
❖ Sepsis diagnosis also includes identification of a specific source or
anatomic site of infection for an emergent source control.

SOFA Score

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❖ Old Definition of sepsis


✓ Sepsis = SIRS + Infection
▪ SIRS = 2 out of the following 4 abnormalities
1. Fever or hypothermia
2. Tachycardia
3. Tachypnea
4. Leucocytosis or leucopenia
▪ Infection → either of the following (i.e. confirmed or
suspected infection)
☛ Bacteraemia (or viraemia /fungaemia/protozoan)
☛ Septic focus (abscess / cavity / tissue mass)
✓ Severe sepsis = Sepsis + Organ Dysfunction
✓ Septic Shock = Severe sepsis + Hypotension

New sepsis definition


❖ Sepsis:
✓ Suspected or documented infection and
✓ Acute increase of ≥2 SOFA points /a proxy for organ
dysfunction/ (use ≥2 qSOFA points for emergency, non ICU
case)
❖ Septic Shock: Sepsis and
✓ Vasopressor therapy needed to elevate MAP ≥65
mm Hg and
✓ Lactate >2 mmol/L (18 mg/dL) despite adequate
fluid resuscitation
❖ Septic shock is defined as a subset of sepsis in which underlying
circulatory, cellular and metabolic abnormalities are associated with a
greater risk of mortality than sepsis alone
❖ Severe Sepsis → No longer used

❖ Infection related organ dysfunction:


▪ all patients with infection should be carefully evaluated for
organ failure. Conversely, any unexplained acute organ
dysfunction should also raise the possibility of an underlying
infection.
▪ Along with routine and organ specific investigations, the
following are the key diagnostic recommendations for sepsis
✓ Early recognition and triage
✓ Measure lactate level and re-measure lactate if initial
lactate is elevated (> 2 mmol/L or 18 mg/dl).
✓ Obtain blood cultures 1304
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☛ at least two sets of blood cultures (aerobic and


anaerobic) from different sites
☛ Should always be withdrawn prior to antibiotic
administration as long as it does not cause a delay in
administration.
☛ Samples from all indwelling vascular access devices
and cultures from easily accessible sites (eg, sputum,
urine) are also important
✓ Imaging of suspected sources.
✓ Organ specific investigations
✓ Physical examination
☛ BP
☛ RR
☛ Capillary refill

Treatment

Treatment approaches in sepsis

❖ Sepsis and septic shock are medical emergencies that require an


immediate treatment and resuscitation.
❖ One of the Golden methods recommended by the surviving sepsis
international guideline is a one-hour bundle (group of procedures and
treatments to be carried within one hour). These are:

Earl measures

The following treatment stapes had better be implemented ASAP:


1) Securing the airway and correcting hypoxemia ASAP as indicated
2) Secure IV line (within 15 minutes) for the early administration of
fluids and antibiotics
3) Rapid (or bolus) administration of 30mL/kg IV crystalloid for
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✓ RL or NS are preferred. Should be started within 30-60 minutes


of sepsis recognition and completed within first 3 hours.
✓ Can be repeated (up to 2-3 liters) until BP and tissue perfusion
are acceptable, pulmonary edema follows, or there is no further
response.
✓ Adequacy of fluid administration can be guided by hemodynamic
parameters:
✓ Clinical targets including MAP of 60 - 70 mmHg and UOP ≥
0.5 mL/kg/hour.
✓ Dynamic measures of fluid responsiveness (eg, respiratory
changes in the radial artery pulse pressure) are preferred,
✓ Static measures (eg, CVP 8 - 12 mmHg or central venous
oxygen saturation ≥70 %).
✓ Initially elevated serum lactate should be followed (eg, every
6 hours), till normalization as a marker of tissue hypo-
perfusion.
4) Initiation of broad-spectrum antibiotic within 60 minutes if possible,
after blood sample withdrawal (Table 1)
o IV empiric broad spectrum (gram +ve and -ve coverage).
o 3rd generation cephalosporin’s alone or in combination with other
antibiotics can be used as first line agents in undifferentiated
sepsis
o Select an appropriate agent based on patient's history,
comorbidities, immune status, suspected site of infection, presence
of invasive devices, Gram stain data, and local prevalence and
resistance patterns if available.
o Antimicrobial therapy in septic patients should always be initiated
with a full, high end-loading dose of each agent used.
o Antibiotics can be administered for a total of 10 days in most
cases. However, shorter or longer courses may be used based on
the patient response, clinical condition, immunity status, specific
source of septicemia, type of pathogen, etc.
o If suspected, add coverage against viruses and fungi (e.g. in
neutropenic patients)
o Empiric antimicrobial therapy should be narrowed once pathogen
identification and sensitivities are established and/or adequate
clinical improvement is noted (look antibiotic stewardship below)

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Table 1: Antibiotic selection options for sepsis


(Community acquired with no healthcare admission in previous 90 days) and immune-competent patients.

Community acquired AND First choice antibiotic regimen Second line antibiotic
Immune-competent
Undifferentiated (no Ceftriaxone,1 - 2g IV daily (usual dose is 1g, IV, Ampicillin, 2-4g, IV, QID plus
obvious source identified) BID) Gentamicin, 5 mg/kg, IV, daily
Pneumonia Ceftriaxone,1 - 2g IV daily + Ceftriaxone + Doxycycline
Azithromycin, 500mg, po, daily for 3 days

add Vancomycin,1g, IV, BID if necrotizing


pneumonia or high risk of MRSA suspected (if
normal renal function)
UTI Ciprofloxacin,500-600mg, po, BID or 400mg IV, BID Ampicillin + Gentamycin

Intra-abdominal Infection Ceftriaxone,1 - 2g IV daily + Metronidazole, 500mg, Augmentin or Ampicillin-Sulbactam


IV, TID
Skin/Skin Structure Cefazolin, 1 - 2g, IV, TID Anti-staphylococcal penicillin’s (e.g
Infection – Pure cellulitis Add Vancomycin if necrotizing abscesses or high cloxacillin)
risk of MRSA
Skin/Skin Structure Piperacillin-Tazobactam, 4.5g, IV, TID Ampicillin-Sulbactam
Infection with Special Add Vancomycin if necrotizing abscesses or high
Risks risk of MRSA
(Special Risks: immersion
injuries, animal bites,
diabetic foot ulcer)
Bacterial Meningitis – Ceftriaxone,2g, IV, BID Ampicillin or benzyl penicillin alone
“Spontaneous” Add Vancomycin if gram positive cocci seen in (if microorganism identified) or with
CSF gram stain gentamycin
Add Ampicillin for age < 1 month and > 50
years/immune-compromised

Consecutive measures

5) Peripheral (norepinephrine) or central inotrope infusion therapy for fluid


refractory septic shock during or after resuscitation.
✓ Refractory are those who remain hypotensive despite adequate fluid
resuscitation (eg, 3L in first three hours)
✓ If indicated administered ASAP to maintain MAP ≥ 65 mm Hg.

✓ Norepinephrine (noradrenaline) is the preferred first choice agent


✓ Initial dose: 0.1 - 0.15 µg/kg/min (8 - 12 µg/min); 1307
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❖ a lower initial dose of 5 µg/minute may be used, eg, in


older adults.
❖ Norepinephrine must be diluted; eg, a usual
concentration is 4 mg in 250 mL of D5W or NS (16
µg/mL)

✓ Maintenance dose: 0.025 - 0.05 µg/kg/min (2 - 4 µg/min)


✓ Maximum dose rage in refractory shock: 0.5 - 0.75 µg/kg/min
(35 - 100 µg/min);
✓ If refractory to IV fluid and vasopressor

☛ Glucocorticoids
☛ inotropics and
☛ blood transfusions (consider RBCs if hemoglobin <7 g/dl), can
be administered on an individual basis.

6) Regular monitoring and stabilization


o Be cautious with consecutive fluid administration volume in
patients with CHF, ESRD and cirrhosis.
o If the patient respond, rate of fluid administration can be reduced
or stopped, vasopressors weaned, and diuretics administered (if
required)
o If non responsive (or failed after initial response), reinvestigate
including the following considerations: removal of devices that may
be infected, adequacy of antibiotic regimen, nosocomial super
infections etc.
o Fluids may be unhelpful or harmful when the circulation is no
longer fluid responsive. Hence, frequent monitoring is essential for
early recognition of cardiogenic and noncardiogenic pulmonary
edema (ie, acute respiratory distress syndrome [ARDS]).
7) Source control (emergently or at leases within 6 to 12 hours)
o Consider in all patients with sepsis, if the source is not identified
and addressed in the initial evaluation (Table 2).
o Remove of intravascular access devices promptly if it is a possible
source of sepsis or septic shock after other vascular access
established.

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Table 2: Source control methods for common ICU infections


Source Interventions
Pneumonia Chest physiotherapy, suctioning
Urinary tract Drainage of abscesses, relief of obstruction, removal or changing of
infected catheters
Catheter-related Removal of catheter
bacteremia
Peritonitis Resection, repair, or diversion of ongoing sources of contamination,
drainage of abscesses, debridement of necrotic tissue
Pancreatic infection Drainage or debridement
Soft tissue infection Debridement of necrotic tissue and drainage of discrete abscesses
Septic arthritis Joint drainage and debridement
Endocarditis Valve replacement
Prosthetic device Device removal
infection
Empyema Drainage, decortication
Sinusitis Surgical decompression of the sinuses
Cholangitis Bile duct decompression

8. Antibiotic stewardship.

o Sorting out the source of infection (preferably identifying the


specific pathogen) and optimizing antibiotic use is critical.
o De-escalation should be planned within 72 hours based on the
culture report and other criteria’s. Procalcitonin may help to guide
the de-escalation and deciding on the duration.

Prevention
o Vaccination
o Proper hand washing and other peculiar precautions
o Maintaining a clean environment
o Preventing aspiration etc.

Special population considerations

Pregnant:

✓ Same principles as outlined in this topic can be used while aware of


hemodynamics alterations during pregnancy. Readers are also
encouraged to consult other up-to-date recommendations.
Elderly:

✓ elderly patients are more likely to have an altered clinical


presentation. In addition, the severity of the disease, sensitivity to
treatment and mortality is high in them, practitioners are encouraged
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to have more frequent monitoring schedules for this group of


population.

Additional considerations

Adequate antibiotic dosing and sepsis

✓ Loading dose is warranted for antibiotics with low volume of distribution


(teicoplanin, vancomycin, colistin) in all critically ill patients to rapidly
achieve target drug concentrations. For sepsis and septic shock, an IV
loading dose of 25–30 mg/kg (based on actual body weight) is
suggested to rapidly achieve the target trough drug concentration. In
septic patients loading doses are also important for β-lactams
administered as continuous or extended infusions. Loading dose of any
antimicrobial agent can be safely administered in an altered renal
function, although this may affect frequency of administration and/or
total daily dose. Hence appropriate dose adjustment should be
performed for kidney failure with a particular attention for nephrotoxic
antibiotics like vancomycin and gentamycin.
✓ In addition antibiotic dosing should be carefully considered based on
the nature of the drug for septic patients. For instance for time
dependent drugs like piperacillin/tazobactam 3.375 g every 6 hours
doing schedule is better than 4.5 g every 8 hours for at least achieving
a higher T > MIC. On the contrary drugs like floroquinolones and
aminoglycosides will be good if given at higher doses.
✓ Please consult the principles of antimicrobial therapy for drugs
selections and considerations for allergic reactions.

Vasopressors for sepsis

✓ Vasopressor infusions are high-risk medications requiring caution to


prevent a medication error and patient harm. Centers should have
available protocols that include steps on how to prepare and administer
vasopressor infusions using a limited number of standardized
concentrations. For further details and alternative vasopressors look for
the management of shock under the emergency conditions

Corticosteroids for sepsis

✓ No septic patient should be on corticosteroids unless there is a


refractory shock. IV hydrocortisone alone can be used to treat septic
shock patients if adequate fluid resuscitation and vasopressor therapy
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are unable to restore hemodynamic stability. 200mg/day IV


hydrocortisone can be initiated and tapered after shock reversal was
noted.

other aspects of care for patients with sepsis and septic shock like

✓ the use of blood products


✓ mechanical ventilation
✓ sedation and analgesia
✓ glucose control
✓ renal replacement therapy
✓ venous thromboembolism prophylaxis
✓ stress ulcer prophylaxis
✓ nutrition.

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Chapter 18; Thyroid Hormone Disorders

18.1. Thyrotoxicosis and Thyroid storm (የሚረጭ እንቅርት)

18.1.1. Thyrotoxicosis

Thyrotoxicosis and hyperthyroidism are two different pathogenetic


mechanisms which can be distinguished by the findings on the 24-hour
radioactive iodine uptake (RAIU).
✓ Thyrotoxicosis → Biochemical/physiological manifestation of excessive
quantities thyroid hormone
✓ Hyperthyroidism → Overproduction of thyroid hormone by thyroid
gland
Thyrotoxicosis is a condition resulting from an excess of thyroid hormones.
If left untreated, significant weight loss and cardiac complications, including
Heart Failure, may occur.
Causes
✓ Grave’s disease (autoimmune, common in females)
✓ Toxic multinodular goiter
✓ Toxic adenoma
✓ Thyroiditis (causes transient thyrotoxicosis which progresses to normal or
hypothyroid state later)
✓ Iatrogenic causes (side effect of medications containing iodine e.g.
amidarone)

Clinical features
Symptoms
Weight loss despite increased appetite
Excessive sweating
Heat intolerance
Palpitations
Nervousness and irritability
Menstrual irregularity, mainly oligomenorrhea
Increased hair loss
In thyroiditis there could be neck pain and

Signs
Tachycardia with or without irregularity: Sinus tachycardia or atrial fibrillation
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Goiter often present but not always


Smooth and diffuse goiter in Grave's disease
Irregular goiter in toxic multi-nodular goiter
Single thyroid nodule in toxic adenoma
Thyroiditis: there could be tenderness
Tremors and brisk deep tendon reflexes
Moist palms
Exophthalmos (Staring or protruding eye, lid lad/retraction in Grave’s disease)

Investigations and diagnosis

TFT
✓ 1st determine TSH, then free T4 if TSH is abnormal
✓ TSH is the best initial diagnostic test. If the TSH is low, it suggests
hyperthyroidism
✓ A low TSH result should be followed by Free T4 and total T3
determinations. Rarely Free T3 determination may be needed.
o TSH normal = excludes hyperthyroidism
o TSH is low and high Free T4 or T3 = Primary hyperthyroidism
o If TSH is low, Free T4 and T3 normal= subclinical hyperthyroidism
ECG
Thyroid imaging and cytology are not generally necessary in the
work up of hyperthyroidism.

Algorism; Diagnosis of Hyperthyroidism

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Algorism; Laboratory tests in the differential diagnosis of hyperthyroidism

Treatment

✓ Avoid stimulants e.g. Caffeine

Hyperthyroidism treatment includes;


❖ Ablative therapy
❖ Surgery → Partial thyroidectomy; should only be done after a state of euthyroid
state is achieved with medical therapy
❖ Radioactive iodine
❖ Medical therapy
❖ Antithyroid drugs (Thionamides)

Anti-thyroid drugs (thionamide)

First line38
✓ Propylthiouracil (PTU)

38
according to UpToDate 2018, PTU is favored over methimazole because of PTU's effect to decrease T4-
to-T3 conversion. 2021 STG for general hospitals of Ethiopia, consider Carbimazole as first line and PTU as an
alternative.
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o Initial dose: 100 - 150mg, PO, TID


o Max; 300mg, PO, TID
o Maintenance dose: Variable but commonly 100-200mg/day

Second line /alternative


✓ Carbimazole
o Initial dose 30-40mg/day divided in 2-3 doses
o Maximum dose 60mg/day
o Maintenance dose: variable but commonly 5-15mg/day
o Titrated down the dose based on thyroid function tests:
▪ In the initial few months based on Free T4 levels and T3
▪ After the first few months follow up is based on TSH

❖ Duration of treatment with anti-thyroid drugs


✓ Depends on the specific cause of the hyperthyroidism
▪ In Grave’s disease: hyperthyroidism generally resolves in 1.5
- 2 years; hence, if euthyroid state is achieved the anti-
thyroid drug needs to be discontinued in 1.5 to 2 years.
▪ In toxic multinodular goiter39 or toxic adenoma: treatment
should continue until thyroidectomy or radioiodine therapy is
done

Adjunct pharmacologic treatment

Beta blockers: for symptom control until euthyroid state is achieved.


✓ Propranolol, 20-40mg, PO, BID or TID OR
✓ Atenolol 25-100mg, PO, daily OR
✓ Metoprolol 25-100mg, PO, daily or in two divided doses

N.B
 Propranolol has additional effects of blocking peripheral conversion
of T4 to T3
 Betablockers are absolutely contraindicated in patients with;
o Asthma or COPD
o Severe peripheral vascular disease
o Bradycardia
o 2nd or 3rd degree heart block

39
if thyrotoxicosis is associated with goiter (e.g. toxic multinodular goiter) or if you
suspect thyroid malignancy, consult or link to surgery.
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o Hypoglycemia-prone diabetics in whom the early warning


symptoms of hypoglycemia may be masked and
o Raynaud phenomenon
 In the absence of contraindications, beta blockers can be
administered as soon as the diagnosis of hyperthyroidism is made,
even before obtaining a definitive diagnosis as to the etiology of the
thyrotoxicosis.

18.1.2. Thyroid storm / thyrotoxic crisis


It is a Severe and life-threatening thyrotoxicosis with an exaggeration of the
usual symptoms of hyperthyroidism
An endocrine emergency with mortality rate of, as high as, 10 to 30%
despite treatment.
Usually occurs as a result of previously unrecognized or poorly treated
hyperthyroidism
Thyroid hormone levels do not help to differentiate between uncomplicated
hyperthyroidism and thyroid storm. i.e. the degree of hyperthyroidism is not
a criterion for diagnosing thyroid storm.

Precipitants

◼ Infection
◼ Trauma
◼ DKA
◼ MI
◼ CVA
◼ PE
◼ Surgery
◼ Labor
◼ Withdrawal of thyroid medication
◼ Iodine administration
◼ Palpation of thyroid gland
◼ Ingestion of thyroid hormone
◼ Unknown etiology (20-25%)

Clinical features

Exaggeration of the usual symptoms of hyperthyroidism


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The most common signs are fever, tachycardia out of proportion to the
fever, altered mental status, and diaphoresis
Clues include a history of hyperthyroidism, exophthalmoses, widened pulse
pressure and a palpable goiter
Cardiovascular features include;
❖ Tachycardia (>140 beats/minute) and/or atrial fibrillation → in >60 % of
cases
❖ CHF features.
❖ Hypotension
❖ Cardiac arrhythmia
❖ Sudden cardiac death may occur
Common GI symptoms include diarrhea and hyper defecation
CNS manifestations include; Agitation, anxiety, delirium, psychosis, stupor,
or coma
Apathetic thyrotoxicosis is a distinct presentation seen in the elderly
❖ Characteristic symptoms include lethargy, slowed mentation, and apathetic
facies
❖ Goiter, weight loss, and proximal muscle weakness also present

Diagnosis

◼ Thyroid storm is a clinical diagnosis based upon the presence of


severe and life-threatening symptoms (hyperpyrexia, cardiovascular
dysfunction, altered mentation) in a patient with biochemical evidence of
hyperthyroidism (elevation of free T4 and/or T3 and suppression of
TSH). And treated empirically
◼ There are no universally accepted criteria or validated clinical tools for
diagnosing thyroid storm
◼ Scoring system for thyroid storm → In 1993, Burch and Wartofsky
introduced a scoring system using precise clinical criteria for the
identification of thyroid storm (table below)
A. A score of ≥ 45 or more is highly suggestive of thyroid storm
B. a score < 25 makes thyroid storm unlikely.
C. A score of 25 to 44 is suggestive of impending storm.
D. While this scoring system is likely sensitive, it is not very specific.

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Chapter 11; Acute febrile illness (AFI)

Table; Burch and Wartofsky’s Diagnostic Parameters and Scoring points for
thyroid storm*
Clinical Features Score
37.2 to 37.7 5
37.8 to 38.2 10
Temperature (0C) 38.3 to 38.8 15
38.9 to 39.4 20
39.5 to 39.9 25
>40.0 30
CNS effects Mild → Agitation 10
Moderate → Delirium, Psychosis, Extreme lethargy 20
Severe → seizure, coma 30
Gastrointestinal-hepatic Moderate → Diarrhea, Nausea/vomiting, Abdominal pain 10
dysfunction Severe → Unexplained jaundice 20
99 to 109 5
110 to 119 10
Tachycardia 120 to 129 15
130 to 139 20
CVS dysfunction ≥140 25
Atrial fibrillation 10
Heart failure Mild → Pedal edema 5
Moderate → Bibasilar rales 10
Severe → Pulmonary edema 15
Precipitant history Negative 0
Positive 10
* A score of 45 or more is highly suggestive of thyroid storm, a score of 25 to 44 supports the
diagnosis, and a score below 25 makes thyroid storm unlikely.

Laboratory findings

TFT

◼ All patients with overt primary hyperthyroidism have low TSH and high
free T4 and/or T3
◼ TSH should be assessed in all patients in whom there is A clinical
suspicion of thyroid storm;
A. hyperpyrexia with temperature > 39.4°C
B. Goiter
C. Cardiovascular dysfunction
D. Altered mentation
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E. Atrial fibrillation
F. History of antithyroid drug therapy for hyperthyroidism
G. Recent thyroid or nonthyroidal surgery
H. Recent exposure to iodine-containing contrast.
◼ If the TSH is below normal, free T4 and T3 should be measured.
◼ The degree of hyperthyroidism (elevation of T4 and/or T3 and
suppression of TSH) in patients with thyroid storm is, in general,
comparable with that in patients with uncomplicated overt
hyperthyroidism. Thus, the degree of hyperthyroidism is not a criterion
for diagnosing thyroid storm.
➢ Other nonspecific laboratory findings may include;
➢ Mild hyperglycemia → secondary to a catecholamine-induced inhibition of
insulin release and increased glycogenolysis
➢ Mild hypercalcemia → may occur due to hemoconcentration and
enhanced bone resorption
➢ Abnormal LFT → elevated transaminase and elevated bilirubin
➢ Leukocytosis, or leukopenia.
➢ ECG features of arrythmia
➢ Radioiodine uptake is not necessary for the diagnosis of thyroid storm,
and treatment should not be delayed for scanning in patients with
clinical manifestations of thyroid storm.

Management of thyroid storm

Needs ICU care!!


Treatment can then be divided into 5 areas:
Principles of treatment
✓ General supportive care
✓ Beta blocker → to control the symptoms and signs induced by
increased adrenergic tone
✓ Thionamide (PTU, Methimazole) → to block new hormone
synthesis
✓ Iodine solution → to block the release of thyroid hormone
▪ The administration of iodine should be delayed for at least
one hour after thionamide administration to prevent the iodine
from being used as substrate for new hormone synthesis.
✓ Glucocorticoids → to reduce T4-to-T3 conversion, promote
vasomotor stability, and possibly treat an associated relative adrenal
insufficiency
✓ Identification and treatment of precipitating events
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◼ Iodinated radiocontrast agent (if available) → to inhibit the peripheral


conversion of T4 to T3
◼ Bile acid sequestrants → may also be of benefit in severe cases to
decrease enterohepatic recycling of thyroid hormones
A. Cholestyramine, 4 g, PO, QID

A) General supportive care


◼ ABC of life (airway protection, oxygenation, fluids and cardiac
monitoring)
◼ Proper fluid, electrolyte, and nutritional support.
❖ Many patients require substantial amounts of fluid, while others may
require diuresis because of CHF
◼ Antipyretics
❖ Cooling blanket
❖ PCM, 1g, PO, TID/QID
❖ Avoid Aspirin (Salicylates)!! → because it can increase serum free
T4 and T3 concentrations by interfering with their protein binding
(i.e. displace T4 from TBG /Thyroid binding globulin/)
◼ ± Phenobarbital (sedation)…↑peripheral metabolism; inactivation of T4, T3.
◼ Prevent peripheral effects:
B-Blocker
A) Propranolol, 60 - 80 mg, PO, every 4 - 6 hours, with appropriate
adjustment for heart rate and blood pressure. OR
✓ IV: 0.5 to 1 mg administered over 10 minutes followed by 1
to 3 mg over 10 to 15 minutes every several hours with
continuous cardiac monitoring; when transitioning to oral
therapy, IV therapy may need to be continued until the effects
of oral therapy are achieved
B) Atenolol, 25 to 100 mg, PO, once or twice daily; up to 200 mg/day OR
C) Metoprolol; Immediate release (metoprolol tartrate): 25 to 50 mg, PO,
BID or TID OR
✓ may also consider administering once-daily extended-release
formulation (metoprolol succinate)
D) Esmolol (IV), 500 µg/kg IV bolus, then 50-200 µg/kg/min maintenance

N.B
◼ Propranolol has the additional effects of blocking peripheral conversion
of T4 to T3. But, this effect of propranolol is slow, occurring over 7 to
10 days, and contributes little to the therapeutic effects of the drug
◼ Look at contraindications of betablockers from thyrotoxicosis section
above.
➢ Decrease de novo synthesis:
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Chapter 11; Acute febrile illness (AFI)

 PTU, 600-1000mg PO Loading, followed by 200-250 mg, PO, q4


hrs OR
 Methimazole, 40 mg, PO Loading, followed by 20 mg PO, every 4
- 6 hours

◼ PTU is favored over methimazole because of PTU's effect to


decrease T4-to-T3 conversion
➢ Iodine solutions to prevent release of hormone → One hour after the first dose
of thionamide is taken.
✓ Lugol solution (Potassium iodide and iodine), 8 - 10 drops (1ml =
20drops), PO, TID/QID or
✓ Saturated solution of Potassium iodide (SSKI), 5 drops PO, QID or

➢ Glucocorticoids
✓ Hydrocortisone, 100 mg, IV, TID or
✓ Dexamethasone, 2 mg, IV, QID

➢ Identification and treatment of precipitating events


✓ Diuretics and digitalis for heart failure
✓ Broad spectrum antibiotics for infection
✓ Others → look at precipitant factors above

 If the patient continues to deteriorate despite appropriate therapy


circulating thyroid hormone may be removed by plasma transfusion,
plasmapheresis, charcoal plasma perfusion

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Chapter 11; Acute febrile illness (AFI)

18.2. Hypothyroidism
❖ The body requires thyroid hormones for normal metabolism and growth.
❖ Hypothyroidism is a condition in which there is a reduction in thyroid hormone
production.
❖ In adults, it may be the cause of a slow metabolic rate, systemic problems
and dementia.
❖ The most common reason is decreased production by thyroid glands (called
primary hypothyroidism), rarely it could be caused by pituitary abnormalities
(secondary)
❖ Antibody-related thyroid gland destruction, surgical removal of the thyroid,
pituitary lesions or surgery, congenital, severe iodine deficiency are the major
causes.
❖ Myxedema coma describes the most severe state of hypothyroidism and is a
medical emergency.

Types of Hypothyroidism
Primary hypothyroidism
❖ From thyroid destruction
Central or secondary hypothyroidism
❖ From deficient TSH secretion, generally due to sellar lesions such as pituitary
tumor or craniopharyngioma
❖ Infrequently is congenital
Tertiary hypothyroidism
❖ From deficient TSH stimulation above level of pituitary→ i.e. lesions of
pituitary stalk or hypothalamus
❖ Is much less common than secondary hypothyroidism

Clinical features

Symptoms
❖ Patients could remain asymptomatic for several years or they might not
recognize the symptoms themselves.
❖ Intolerance to cold environments, constipation, weight gain, hair loss, dry skin
❖ Hoarse voice, lethargy, memory loss, depressed reflexes, dementia
❖ Abnormal menstrual periods and sub-fertility (in adult females)

Signs
❖ Puffy face, pallor, slow pulse (usually <60 per minute)
❖ Goiter may be present

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Investigation and Diagnosis

◼ TSH
◼ Free T4

The diagnosis of hypothyroidism is usually delayed due to lack of recognition.


A very high index of suspicion should be maintained in any adult woman who
presented with fatigue or non-specific symptoms.
TSH is the best screening test
❖ TSH >20 micro unit/ml: highly suggestive primary hypothyroidism
❖ Normal TSH: excludes primary hypothyroidism
❖ Mildly elevated TSH (<20 microunits/ml): needs freeT4 determination
❖ Mildly elevated TSH with normal free T4: subclinical hypothyroidism

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Chapter 11; Acute febrile illness (AFI)

Treatment

Levothyroxine
❖ Starting dose → for patients with no cardiovascular disease
 for patients with no cardiovascular disease
o Young patients → 100 µg/day
o Elderly patients → 50 µg/day
 Patients with established cardiac disease → 25-50 µg/day
❖ Dose adjustment
 Dose adjustment should be made after at least 2-3 months of therapy
 Dose increments by 25-50 µg/day in 2- 3months
 Achieving TSH is the target of treatments
 After normalization of TSH, annual follow up of TSH suffices

Myxedema Coma

◼ Myxedema is a rare life-threatening decompensation of hypothyroidism


◼ Usually in individuals with long-standing hypothyroidism
◼ Most often seen in the winter months
◼ It is an endocrine emergency with Mortality rate of > 50%
◼ Occurs in patients (esp. Elderly women) who have severe, untreated
hypothyroidism, and although it may be spontaneous

Precipitating factors

◼ Infection
◼ Surgery or trauma
◼ Myocardial infarction
◼ Stroke
◼ exposure to cold
◼ drugs → use of sedatives or opiates, Lithium, Amiodarone

Clinical features

◼ Onset is insidious, with progressive stupor culminating in coma.


◼ In addition to the clinical features of hypothyroidism patients may present with
A. Hypothermia
B. Seizures
C. Altered metal status → Coma, delusions, and psychosis (myxedema maddness)
D. Hyponatremia → Dilutional secondary to decreased free-water clearance
E. Hypoglycemia → Secondary to impaired gluconeogenesis
F. Hypotension
G. Bradycardia
H. Respiratory Failure → Secondary to decreased strength of respiratory muscle,
Hypercapnia and hypoxia is common
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Chapter 11; Acute febrile illness (AFI)

Investigations and Diagnosis

High clinical suspicion, commonly has Hx. of hypothyroidism


RBS → Hypoglycemia
CBC → Anemia, leukocytosis suggests underlying infection as precipitant
Serum electrolyte → Hyponatremia
Liver enzymes → ↑ Transaminases
ECG → Sinus Bradycardia, Prolonged QT interval, Low voltage, Flattened
or inverted T waves
Others → ↑ CPK, ↑ LDH, ↓Po2 and ↑PCo2 on ABG’s

Treatment

◼ Admit to ICU for ventilatory support and for intravenous medications.


◼ Supportive measures
ABC of life
Passive rewarming (heating blanket)
Correction of hyponatremia → Hyponatremia typically responds to fluid
restrictions. Severe cases may require hypertonic saline with Lasix
Dextrose-containing IV fluids if there is hypoglycemia
Vasopressors are usually ineffective and should only be used in
severe hypotension
Empiric antibiotics for infection.
Avoid exposure to potent sedative or analgesic agents that may
exacerbate altered mental status
◼ Parenteral thyroxine:
A. Levothyroxine 300-500 µg, IV, slowly followed by 50-100 µg daily

Alternative
B. L-triiodothyronine 25 µg IV/PO, TID (12.5 µg in patients with
cardiovascular disease)
◼ Glucocorticoids → if there is concomitant adrenal insufficiency
Hydrocortisone 100 mg IV, TID
◼ Precipitating causes should be sought and treated

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Chapter 19; Poisoning, Drug Overdose, and Envenomation

Chapter 19; Poisoning, Drug


Overdose, and Envenomation
Dr. Mulualem. G

19.1. Poisoning and over dose(መመረዝ)

➢ Poisoning is an exposure to an amount of substance that is likely to produce


untoward effects in an individual.
➢ Poisoning represents the harmful effects of accidental or intentional exposure to
toxic amounts of any substance. The exposure can be by ingestion, inhalation,
injection, or through skin.
➢ The effects may occur immediately or several hours or even days after the
exposure.
➢ The damage could be local or systemic.
➢ Poisoning can be from
✓ Household substances (e.g. bleach),
✓ Industrial (e.g. methanol)
✓ Pesticides (e.g. organophosphates)
✓ Therapeutic medicine overdose (e.g. phenobarbitone, Amitriptyline)
✓ Toxic plants (e.g. poisonous mushrooms, toxic herbal medications)
✓ Bites and stings of venomous animals (e.g. snakes, bees).

EPIDEMIOLOGY

➢ Studies have shown that acute poisoning has been identified as a


significant global public health problem
➢ Poisoning is a common reason for emergency departments visit and
hospitalization worldwide with major morbidity and mortality in many
countries.
➢ It is the 3rd most common emergencies of pediatrics leading to
increased childhood morbidity and mortality. Childhood poisoning is
usually accidental and tends to be associated with a low morbidity and
mortality
➢ WHO estimated 0.3 million people die every year due to various
poisoning agents.
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Chapter 19; Poisoning, Drug Overdose, and Envenomation

poisoning is an important problem.


➢ According to a Study done at TASH, Household cleansing agents were
the leading causes (43.1%) followed by organophosphates (21.6%) and
phenobarbitone (10.3%). Females outnumbered males and mean age was 21
years, most being (96.5%) intentional self-harm poisonings
➢ Another study done in Gondar University teaching hospital indicates that
acute poisoning accounts for 0.45% of emergency admissions.
Organophosphates, rat poison and alcohol were implicated in majority of
the cases for suicidal as well as parasuicidal intentions.
➢ In Ethiopia, Organophosphates and household cleansing agents are the
predominant agents of acute poisoning.

Clinical features

➢ Clinical presentation is variable depending on the type of poison/medicine,


route and dose.
➢ Many of the manifestation are nonspecific.
➢ Toxidromes are sets of clinical findings which could help in guiding the
possible class of the poison/medicine
➢ It is very helpful to have a sample of the substance or the container in which
it was stored as only few poisons can be identified instantly

Table; Toxidromes
Examples of
Toxidrome Mental status Pupil Vital signs Other toxic agents
Confusion Coma Miosis Bradycardia Salivation, urinary & fecal Organophosphate and
Cholinergic
Hypertension or incontinence, diarrhea, carbamate insecticides, nerve
Hypotension vomiting, lacrimation, agents,
bronchoconstriction,
fasciculations, weakness,
seizures
Agitation, Mydriasis Hyperthermia, Dry skin & mucous Antihistamines, tricyclic
Anticholinergic
hallucinations, membranes, decreased antidepressants, antiparkinson
delirium with tachycardia, bowel sounds, urinary agents, antispasmodics,
mumbling speech, hypertension, retention, myoclonus, phenothiazines, atropine
coma tachypnea choreoathetosis

Confusion, Mydriasis Hyperthermia, Seizures, myoclonus, Amitriptyline,


Tricyclic
agitation, coma tachycardia, choreoathetosis, cardiac nortriptyline, imipramine,
antidepressant hypertension then arrhythmias
hypotension
CNS depression, Miosis Hypothermia, Hyporeflexia Benzodiazepines,
Sedative- hypnotic
stupor, coma bradycardia, barbiturates, alcohols,
hypotension,
hypoventilation
CNS depression, Miosis Hypothermia, Hyporeflexia pulmonary Opiates (eg, heroin, morphine,
Opioid
coma bradycardia, edema, needle marks methadone, oxycodone)
hypotension,
hypoventilation

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Hyperalert, Mydriasis Hyperthermia, Diaphoresis, tremors, Cocaine, amphetamines,


Sympathomimetic
agitation, tachycardia, hyperreflexia, seizures ephedrine, pseudoephedrine,
hallucinations, hypertension, phenylpropanolamine,
paranoia widened pulse theophylline, caffeine
pressure, tachypnea,

Investigations

✓ RBS
✓ CBC
✓ U/A
✓ Electrolytes
✓ BUN and creatinine
✓ LFT
✓ Urine HCG → Routine urine pregnancy testing is strongly recommended in all women of
childbearing age
✓ ECG
✓ CXR → for possible aspiration pneumonia
✓ Toxicological analysis of identified substance (e.g. Gastric aspirate) or from serum → if
available

General Management for poisoning and overdose

Mgt principle
➢ Supportive care
o Identify the substance
▪ Obtaining the original toxic substance
▪ Containers found near or on patient
▪ Through accurate history
o ABC of life
o Left lateral positioning
o Oxygen, monitors, IV access (determine RBS and draw sample for other investigation
while securing IV line)
o Treatment of seizures
o Correction of temperature abnormalities and metabolic derangements
o Drugs: Consider universal antidotes (Thiamine, Oxygen, Naloxone, Glucose)
➢ Decontamination
➢ Specific antidotes and other supportive care
➢ Psychiatric Evaluation

Pharmacologic and other cares


☛ Prevention of further poison absorption
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o Gastric lavage
o Decontamination of eye
o Skin decontamination
o Activated charcoal
☛ Enhancement of elimination
o Multiple-dose activated charcoal
o Haemodialysis
o Urinary pH alkalization
o Hyperbaric oxygenation
☛ Administration of anti-dotes
o Neutralization by antibodies
o Metabolic antagonism
o Physiologic antagonism
☛ Prevention of re-exposure
o Child-proofing
o Psychiatric referral
☛ For Comatose pts…
o Search for Hypoxia, Opioid intoxication, hypoglycaemia, and Wernicke’s encephalopathy.
o ‘Coma cocktail’
o DONT (stands for Dextrose, Oxygen, Naloxone, and Thiamine)
o It applies in case of uknown poisoning with unconsciousness and coma
o Treat hypoglycemia with 30ml of D50W, IV dextrose (glucose).
o Patients at risk of Wernicke’s encephalopathy also require 100mg of
thiamine, but do not require that it be administered before the dextrose.
o Altered mental status, when hypoglycemia cannot be excluded, is an
indication for IV dextrose.
o Supplemental oxygen, thiamine, glucose, and naloxone are often
administered empirically as a cocktail in cases of altered mental status.

Initial management

1. Hypoglycemia
o 40% Dextrose, IV, 40-60ml over 1-3 minutes PLUS
2. Hypotension
o N S, 1000ml, IV fast then according to response
3. Seizure management and medicine-associated agitated behavior

o Diazepam 10mg, IV, stat repeat doses as needed→ CAUTION-respiratory depression

Activated charcoal
Catharsis
o
electrolyte abnormalities and osmotic diuresis.
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Chapter 19; Poisoning, Drug Overdose, and Envenomation 1330

o Magnesium sulphate, 250mg/kg or


o Sodium sulfate, 250mg/kg
Alkalization of urine

Decontamination

Skin decontamination
Remove contaminated clothing and flush exposed areas with copious quantities of tepid
(lukewarm) water or saline. Wash carefully behind ears, under nails, and in skin folds.
Use soap and shampoo for oily substances.
Always wear PPE to prevent secondary contamination to yourselves

Eye decontamination
Irrigate with copious amounts of water or saline for 10 – 15 minutes
Ophthalmologic consultation is indicated for all ocular alkali injuries

GI Decontamination Principles

A. Activated charcoal
B. Ipecac syrup
C. Gastric (Orogastric) lavage
D. Whole bowel irrigation
E. Urine alkalinisation

A. Activated Charcoal

Activated charcoal, 50 - 100g (1- 1.5g/kg), P.O., or via NG tube, diluted in 400–800ml
water stat
✓ Activated charcoal may reduce systemic absorption of a variety of substances
(especially from GIT).
✓ The greatest benefit (indication) is achieved if activated charcoal is given within 1
hour after ingestion.
✓ Charcoal administration has become the decontamination strategy of choice to prevent
poisoning after toxicant ingestion
✓ When mixing, add a small amount of water to charcoal in a container cap and shake
container to make a slurry and then dilute further.
Complication: no systemic effects, but may induce vomiting, constipation, diarrhoea, Bowel

1330
perforation or obstruction following multidose charcoal administration, aspiration of the
activated charcoal and impaired absorption of orally administered antidotes.

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Chapter 19; Poisoning, Drug Overdose, and Envenomation 1331

Avoid (no value): strong acids, alkali, corrosives, heavy metals, cyanides, lithium,
hydrocarbons (paraffin), methanol and ethylene glycol.
Contraindications:
✓ Known or suspected GI perforation
✓ GCS <8 (LOC) or declining rapidly (risk of aspiration)
✓ Unprotected airway.
✓ Known ingestion of substance that charcoal does NOT adsorb.

Multiple Dose activated Charcoal

❖ Dose: initial dose of 50 to 100 g (1 -1.5g/kg), PO or via NG tube, followed by 50g PO


every 4hrs (in case of intolerance 25 g every 2 hours) /0.5 - 1g/kg/, until clinical
conditions and lab parameters improves
❖ Multiple doses can enhance elimination of drugs already absorbed into the body by
interrupting enterohepatic circulation of drugs excreted into the bile.
❖ Indication: ingestion of large doses of Carbamazepine, dapsone, phenobarbitone,
quinine, theophylline, Salicylates, sustained release formulations.
❖ Contraindications: diminished bowel sounds, proven ileus or small bowel obstruction.

B. Syrup of Ipecac → Induction of vomiting

Dose; Ipecac syrup (7%), 15-30ml, PO, stat


☛ May repeat once with 15ml if vomiting doesn’t occur 20-30min
☛ If vomiting doesn’t occur within 30-45min after second dose, perform gastric lavage
☛ Ipecac is no longer recommended for poisoning; Activated charcoal is treatment of choice

Indications

✓ Very recent ingestion (<1hr)


✓ Toxin known not to cause decreased LOC
✓ Toxin known not to fit through OG tube

Contraindications
✓ Ingestion > 1 hr ago
✓ Toxin known to cause decreased LOC/seizure
✓ Caustics, hydrocarbons, TCAs

C. Gastric lavage (Orogastric Lavage)

Indicated for ingestion of large amounts of tablets and capsules with a high inherent
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toxicity within 2 hrs.


Procedure:
✓ Place patient head tilted 20 degrees downward and in left lateral decubitus position
✓ Intubate patient, if they can’t protect their airway
✓ Insert a large bore orogastric tube (32-40 F)
✓ Aspirate fluid from stomach prior to fluid lavage
✓ Install warm tape water or saline into stomach: 200-300ml (10 mL/kg in children)
✓ Aspirate fluid back & repeat till aspirate clears
✓ Consider administration of activated charcoal via orogastric tube before removal.

Risks: pulmonary aspiration, epistaxis, laryngospasm, hypoxia, sinus bradycardia &


mechanical injury
Contraindications:
✓ Patients with LOC
✓ Unprotected airway
✓ Ingestion of corrosives, volatile substances, hydrocarbons,
✓ Patients at risk of GI haemorrhage.

D. Whole Bowel Irrigation

Instillation of large volumes of laxative agent such as polyethylene glycol in osmotically


balanced electrolyte solutions
Promotes rapid, mechanical elimination of ingested toxins
Not recommended for routine use in the poisoned patient
1332
May be considered for substantial ingestions of iron, sustained release products, enteric
coated products and symptomatic acute lead toxicity with known lead particles in the
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gastrointestinal tract. It has been used for other metal ingestions (e.g., lead), overdoses of
sustained-release medications (e.g., lithium, theophylline), ingested pharmaceutical patches,
and ingestions of vials or packages of illicit drugs.
It might also be useful in particularly massive and/or late-presenting overdoses for which
the efficacy of gastric emptying and/or charcoal is expected to be suboptimal.
The technique may be used by mouth in cooperative patients or by NG tube;
The usual recommended dosing is 2 L /hour in adolescents and adults (500 mL /hour
(25ml/kg/hr, maximum 2L/h) in children)
Contraindication: In ileus, bowel obstruction or perforation, and in patients with
hemodynamic instability, Unprotected airway, hemorrhage, Intractable vomiting
Complications: Nausea, vomiting, Pulmonary aspiration, Time consuming; possible delay
instituting other definitive care

E. Urinary Alkalinisation

Infusion of sodium bicarbonate to raise urinary pH to enhance clearance of toxins


excreted by kidneys
Sodium bicarbonate (NaHCO3), IV, 8.4%,
✓ Bolus of 1-2ampules, IV, 50–100mEq (1-2 mEq/kg) in 1 L sodium chloride 0.45%.
Administer 250–500mL over 1–2 hours.
✓ Maintenance rate with 3 ampules of NaHCO3 in 1L of D5W at 1.5 X maintenance fluid
rate for at least 4-6hrs
✓ Target → continue treatment until
☛ urinary pH 7.5-8.5 or
☛ BP improves
✓ Monitor electrolytes→ Pronounced hypokalemia may result from this technique. Thus,
serum potassium must remain above 4 mEq/L to reliably achieve continuous urinary
alkalinization.
✓ Urinary pH should be monitored frequently (every 15 to 30 minutes) until the urine pH
is 7.5 to 8.5.
✓ Urinary alkalinization is sustained by either intermittent bolus or continuous infusion of
bicarbonate.
✓ Serum pH should not be allowed to rise above 7.5 to 7.55.
✓ This is a high-risk procedure and should only be performed in consultation with a
specialist. Risks associated with urinary alkalinization include volume overload (heart
failure and pulmonary edema), pH shifts, and hypokalemia. Therefore, contraindications
to this procedure include patients who cannot tolerate the volume or sodium load,
hypokalemic, or have renal insufficiency.
✓ May be of benefit in salicylate, lithium, barbiturate and, TCA poisoning.

Sodium bicarbonate (NaHCO3),: Oral:


o Initial: 48 mEq (4 g), then 12 to 24 mEq (1 to 2 g) every 4 hours
o dose should be titrated to desired urinary Ph
o maximum doses up to 16 g/day (200 mEq) in patients <60 years and 8 g (100
mEq) in patients >60 years.
o Administration of 48 mEq (4 g) every 8 hours for a total daily dose of 144 mEq 1333
(12 g) has also been shown to achieve a urinary pH of at least 7 after a period of
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10 hours
o Note: Intravenous administration is preferred in specific overdoses (eg, salicylate)
with a target urinary pH of 7.5 to 8.5

Universal Antidotes -→ DONT


➢ Dextrose (Glucose)
➢ Oxygen
➢ Naloxone
➢ Thiamine

Table; Common antidotes

Poison Antidote(s) Dose for adults


Carbon monoxide Oxygen high-flow oxygen by tight-fitting facemask or ventilator

Benzodiazepines Flumazenil Initial dose: 0.1-0.2mg IV over 30-60 sec, repeat 0.1-0.2mg
IV every minute up to 1mg

Acetaminophen N-acetylcysteine Initial oral dose: 140mg/kg, then


70mg/kg q 4h x 17 doses

Heparin Protamine sulfate 1 mg neutralizes 90-115 U heparin;


Initial dose: 1 mg/min to total dose 200mg in 2 h
Isoniazid Pyridoxine Initial dose: 1 gm pyridoxine for every gm INH ingested or
(Vitamin B6) empiric 5gm IV over 10 min if amount ingested unknown

Opiates Naloxone Initial dose: 0.1-2.0mg IV push (opioid dependent patients


should receive 0.1 mg IV every 30-60 sec until clinical
response)
Ticyclic antidepressants Sodium Initial dose: 1-2 ampules (50-100mEq) IV push, then IV infusion
bicarbonate to maintain blood pH 7.45-7.55 (Preparation: 3 amps 50mEq of
NaHCO3 in 1liter D5W infused at 200-250 mL/h)

Organophosphates Atropine Initial dose: 0.5-2.0mg IV; repeat q 3-5


Carbamates Nerve agents min until sweat and secretions clear
Pralidoxime Initial dose: 1 gm IV over 15 min, then
IV infusion of 3-4mg/kg/h for 24-72 hrs

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19.2. Specific poisons


19.2.1 Organophosphates and Carbamates poisoning (ጸረ
ተባይ፣ ተባይ ማጥፊያ፣ ማላታይን /በተለምዶ/)
☛ Organophosphates and carbamates also known as cholinesterase inhibitors are widely used
as pesticides that may cause human poisonings after accidental or intentional exposure.
☛ Poisonings are particularly common in rural areas where more potent agents are widely
available as agricultural insecticides and home use
☛ They can be absorbed via inhalation, ingestion, and skin contact.
☛ Examples:
✓ Organophosphorus – malathion, parathion, TEPP, mevinphos (Phosdrin)
✓ Carbamates- methiocarb, carbaryl, Sarin, soman, tabun.
☛ Patients present with muscarinic and nicotinic manifestations of intoxication.

Clinical features

➢ Clinical features of organophosphate poisoning can be classified into


o Acute organophosphate poisoning
o Intermediate syndrome
o Chronic toxicity

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1. 1) Acute organophosphate poisoning

➢ Signs and symptoms of acute organophosphate poisoning usually occur within 1–2 hours of
exposure but may be delayed up to several hours, especially after skin exposure.
➢ The severity of poisoning has been graded as mild, moderate and severe.

Table; Grading Severity of Organophosphate Poisoning


Features MILD MODERATE SEVERE
GA Walks and talks Cannot walk Unconscious, no papillary
reflex.
Symptoms ➢ Headache ➢ Soft voice ➢ Muscle twitching
➢ Dizzy ➢ muscle ➢ Flaccid paralysis
➢ Nausea twitching ➢ Increased bronchial
➢ Vomiting (fasciculations) secretions.
➢ Abdominal pain ➢ Anxiety ➢ Dyspnoea crackles /
➢ Sweating ➢ Restlessness wheeze.
➢ Salivation ➢ Small pupils ➢ Possible convulsions
➢ Rhinorrhoea (miosis) ➢ Respiratory failure
Serum 1.6-4.0 u/l 0.8-2.0 u/l < 0.8 u/l
acetylcholinesterase
enzyme (AChe)
Results:

➢ Clinical manifestations may be classified into muscarinic, nicotinic, and CNS effects.
➢ In ddition, chemical pneumonitis may occur if a product containing a hydrocarbon solvent is
aspirated into the lungs.
Mnemonic for clinical features of Muscarinic
A. Muscarinic overstimulation causes overstimulation → DUMB BELL’S

✓ Excessive salivation and sweating ✓ Diarrhoea


o Severe diaphoresis can actually lead to ✓ Urination
dehydration with systemic hypovolemia ✓ Miosis
✓ Lacrimation ✓ Bronchorrhea
✓ Vomiting
✓ Diarrhea ✓ Bronchospasm
✓ Bronchorrhea or bronchospasm. ✓ Emesis (Vomiting)
✓ Abdominal cramping ✓ Lacrimation
✓ Miosis ✓ Low or high HR (brady/tachycardia)
✓ Bradycardia or tachycardia ✓ Salivation and sweating

☛ The killer signs are the 3B’s:


✓ Bradycardia
✓ Bronchospasm
✓ Bronchorrhea
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B. Nicotinic overstimulation causes


✓ Muscle fasciculations
✓ Paresis or paralysis.
✓ Death is usually caused by respiratory muscle paralysis.
✓ HTN and Tachycardia because of nicotinic effects or decreased because of muscarinic
effects.

A. CNS poisoning may cause agitation, seizures, and coma.


B. Some organophosphates may cause a delayed, often permanent peripheral
neuropathy.

Investigations

➢ Clinical → There may be a solvent odor; some have a strong garlicky odor.
➢ RBS
➢ BUN, Creatinine
➢ LFT
➢ Electrolytes
➢ CXR (if pulmonary edema or aspiration of hydrocarbon solvent is suspected).
➢ ECG monitoring
➢ ABG
➢ Toxicological analysis

Treatment
➢ The main stay of therapy includes;
o Supportive measures
o Resuscitation
o Decontamination and
o Specific antidote

A. Emergency and supportive measures.


o ABC’s of life comes first→ Pay careful attention to respiratory muscle weakness; sudden
respiratory arrest may occur.
o Give coma cocktail (Naloxone, thiamine, dextrose and oxygen),
o Treat hydrocarbon pneumonitis, seizures, and coma if they occur.
o Observe patients for at least 6–8 hours to rule out delayed-onset symptoms
resulting from skin absorption

Resuscitation
➢ Give 500 - 1000 ml of normal saline (10-20 ml/kg) over 10-20 min to compensate 1337
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fluid loss due to sweating, diarrhoea and cholinergic hyper-secretion

Decontamination → Gastric lavage, activated charcoal


Specific drugs and antidotes.
➢ Specific treatment includes the antimuscarinic agent atropine and the enzyme
reactivator pralidoxime.
➢ After decontamination, antidotal therapy begins with the administration of
atropine sulfate given:

➢ Atropine, 2 - 5 mg (0.05 to 0.1 mg/kg to children), IV, doubled every 5 min


as needed to obtain and maintain full atropinization, which is indicated by an end
point of clearing bronchial secretions and pulmonary rales.
✓ Do not stop atropine therapy abruptly. Wean the rate of administration slowly.
✓ During weaning monitor the patient for possible worsening.
✓ Our goal in atropinazation is chest clearance and not tachycardia. i.e Clearance
of chest of secretions and maintenance of BP has been given more
importance in the target point than size of pupil and heart rate.
✓ Therapy is continued until all absorbed organophosphate has been metabolized and
may require 2 mg to more than 2g of atropine over the course of a few hours to
several days. Avoid atropine toxicity
✓ The most clinically important indication for continued atropine administration is
persistent wheezing or bronchorrhea.
✓ Note: Atropine will reverse muscarinic but not nicotinic effects.

➢ Duration of maintenance atropine therapy:


o This depends on the severity and response to therapy.
o Usually it is maintained for 24- 48 hrs or longer in severe cases, and
gradually withdrawn over 3-5 days
➢ Target end points for atropine therapy
o Clear chest on auscultation with no wheeze
o PR > 80 beats/min
o SBP > 80 mm of hg
o Pupil no longer pin point
o Dry axilla
➢ Since patients usually die from respiratory or circulatory failure, air entry on chest
auscultation, heart rate and blood pressure were given more importance than
dilatation of pupil, rise in body temperature, dryness of mouth/skin

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Atropinization
➢ 1 ampule (1mg/ml) = 1ml
➢ Start with 2mg
➢ Escalate every 5min by doubling the dose (i.e. 2mg →4mg → 8mg → 16mg)
➢ Maximum until chest is clear
➢ If the chest is clear give 10 to 20% of the last dose as follows
✓ every 2hrs for 6hrs then
✓ every 4hrs for 24 to 48 hrs then
✓ QID → TID → BID →stop

➢ Atropine toxicity which are;


o Absent bowel sounds (ileus)
o Hyperthermia/Fever/ → hyperthermia is a serious complication in hot wards
which needs prevention
o Tachycardia
o Delirium
o Confusion
o Agitation
➢ If atropine toxicity happens
o Discontinuation of the atropine infusion, followed by
frequent observation.
o When they settle down the infusion is to be started at 70- 80 % of the
previous rate
➢ Drug options if Atropine is not available
o Diphenhydramine can be an alternate centrally acting anticholinergic agent if atropine is not
available
o Glycopyrrolate
▪ Is recommended as an adjunct to atropine to control secretions or
▪ When atropine toxicity is confused with Organophosphate toxicity or
▪ When atropine is not available
▪ Ampoules of 7.5 mg of glycopyrolate in 200ml of saline is started as
infusion and is titrated to the desired effects of dry mucus membranes.
▪ It has also been given at a dose of 0.2mg Im stat and repeated 6hrly
if required.
➢ After atropinization has been instituted, severe poisonings should be treated with
the addition of pralidoxime.
➢ This drug is particularly useful in poisonings characterized by profound weakness
and muscle twitching.
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➢ Pralidoxime (after atropinisation); 1- 2g (25 - 50 mg/kg for children), IV,


administered in 100 mL of saline by infusion over approximately 30 minutes; then IV
infusion of 8-10mg/kg/h40 for 24-72 hrs
✓ In life-threatening situations, 50% of the initial pralidoxime dose may be infused
over 2 minutes, followed by the remainder of the dose over 30 minutes.
✓ After loading, a 1% concentration may be infused continuously at the rate of 500
mg/hr in adolescents and adults, or approximately 10 mg/kg/hr in children, and can
be titrated to clinical effect.
✓ Occasionally, patients may require more than 48 hours of therapy; the end point
should be persistent relief of neurologic and cholinergic signs.
✓ It is most effective if started within the first 24 hours of the exposure before
irreversible phosphorylation of the enzyme, but may still be effective if given late,
particularly after exposure to highly lipid soluble compounds
✓ Pralidoxime (2-PAM, Protopam) is a specific antidote for organophosphate toxicity,
that acts to regenerate the enzyme activity at all affected sites (muscarinic,
nicotinic, and probably CNS; however, it does not reactivate plasma cholinesterase).
✓ Pralidoxime should be given immediately to reverse muscular weakness and
fasciculations: •
✓ Pralidoxime is not generally recommended for carbamate intoxication, because in
such cases the cholinesterase inhibition is spontaneously reversible and short-lived.
However, if the exact agent is not identified and the patient has significant toxicity,
pralidoxime should be given empirically.
✓ Alternative; Obidoxime
➢ Note: Organophosphates are usually dissolved in hydrocarbon bases; thus, prepare to treat
hydrocarbon pneumonitis if it develops. Also, bronchopneumonia that complicates the
pulmonary edema has been observed in acute poisonings.
➢ Because the organophosphates cause elevated levels of acetylcholine in the plasma,
compounds that affect the uptake of acetylcholine and/or its release should be avoided in
the management of these patients. Specifically, aminophylline and phenothiazines are
contraindicated.
➢ Decontamination → activated charcoal, gastric lavage… Do not induce vomiting because of
the risk of abrupt onset of toxicity
➢ Observe patients for at least 6–8 hours to rule out delayed-onset symptoms resulting from
skin absorption.

40
Some references say 3-4 mg/kg/hr until clinical recovery or 7 days have elapsed whichever is later
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➢ Other mgt options


o Ventilation
o Furosemide: - It is recommended if pulmonary oedema persists,
even after full atropinisation
o Hydrocarbon Aspiration: - In case of ingestion of liquid concentrates of OP,
hydrocarbon solvent aspiration causes chemical pneumonitis. These cases are
to be managed as a case of Acute Respiratory Distress Syndrome.
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o Antibiotics:- Broad spectrum antibiotics are to be instituted as per antibiotics

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policy of the institution, considering the risk of infection due to frequent and
multiple interventions.
o Agitation/Convulsion → Diazepam
➢ Contraindications:
o Drugs like morphine, succinylcholine, theophylline, phenothiazine and reserpine
are contraindicated.

Order sheet example for organophosphate poisoning in our setup


- secure IV line
- keep NPO
- Irrigate the GI (Gastric lavage) (if pt come to emergency within 1hr)
- Put the pt in left lateral position
- Resuscitate with 1 to 2 L of NS
- Atropine 2mg, IV, double the dose Q 5min, till atropinization (until chest is
clear)
- Cimetidine, 400mg, IV, Loading followed by 200mg, IV, daily to BID (if there
is feature of GI irritation)
- Ceftriaxone 1g, IV, BID if only there is aspiration pneumonia
- Metronidazole, 500mg, IV, TID
- Keep at EOPD

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2) Intermediate syndrome
➢ An “intermediate syndrome”, characterized by recurrent muscle weakness occurring
within several days (usually 1 to 5) of the exposure.
➢ Seen in around 40 % of patients following ingestion. It may be associated with
inadequate pralidoxime therapy.
➢ Severe intoxications may also cause a toxic psychosis that resembles alcoholism.

Clinical features:

➢ Paralysis of neck flexor muscles, muscles inner-vated by the cranial nerves,


proximal limb muscles, and respiratory muscles; respiratory support may be needed.
➢ Symptoms or signs of cholinergic excess are absent in this syndrome.
➢ Electromyography may assist in making the diagnosis.
➢ Aggressive, early antidote therapy and supportive measures may prevent or
ameliorate the severity of this syndrome.
➢ Symptoms usually resolve within 7 days.

3) Chronic toxicity
➢ Chronic toxicity is seen primarily in agricultural workers with daily exposure,
manifesting as symmetrical sensorimotor axonopathy.
➢ This mixed sensor motor syndrome may begin with leg cramps and progress to
weakness and paralysis, mimicking features of the Guillain-Barré Syndrome.

19.2.2. Caustics Corrosives (በአሲድ ወይም ቤዝ መመረዝ)

❖ Corrosives are chemicals primarily acids and alkali that cause tissue injury to a burn.
❖ Acids cause coagulation necrosis with eschar formation that limits penetration and depth
of injury.
❖ Alkali cause liquefaction necrosis and penetrate more deeply. Alkali burns more common
and worse than acid.
❖ Some corrosives can cause severe systemic toxicity and profound electrolyte disturbance.

Clinical features
After ingestion of corrosive, hyper salivation, lethargy, polydipsia, vomiting, abdominal pain,
dysphagia, pharyngeal edema, oral pain, drooling, and oral, esophageal, and/or gastric
ulceration could occur.
Inhalation of corrosive gases may cause upper respiratory tract injury, with strider,
hoarseness, wheezing, and noncardiogenic pulmonary edema.
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Eye or skin exposure to corrosive causes instant pain and redness, followed by blistering.
Conjunctivitis and lacrimation are common. Serious full-thickness burns and blindness can
occur.
Significant injury: airway compromise or gastrointestinal perforation complicated by
peritonitis, mediastinitis, sepsis and shock.

Diagnosis
Is based on history of exposure to a corrosive agent and Characteristic findings of skin,
eye, or mucosal irritation and the presence of injury to the GIT.
Endoscopy: indicated within 24 - 48 hrs of severe or deliberate ingestions. Endoscopy for
all patients regardless of symptoms may be necessary.
CXR, and upright abdominal x-ray; will show impacted button batteries,
pneumomediastinum from esophageal perforation or free abdominal air from gastric
perforation.
Other IX: RBS, CBC, electrolytes, arterial blood gases,

Management
➢ Inhalation:
▪ Give oxygen, and
▪ Follow closely for signs of airway obstruction or for non-cardiogenic pulmonary
edema.
➢ Chemical ingestion:
▪ Pre-hospital: immediately give water or milk to drink.
▪ Gastric lavage & induction of vomiting are contraindicated.
▪ Give activated charcoal if the ingested agent can cause significant systemic
toxicity.
▪ If there is esophageal perforation, avoid giving water as it may also enter to the
mediastinum.
▪ If esophageal or gastric perforation is suspected surgical consultation and repair
immediately.
➢ Chemical eye and skin burn:
▪ Remove all clothing, wash skin, and irrigate eyes with copious water or saline.
➢ Button batteries:
▪ Immediately lodged endoscopy guided removal should be done immediately.
➢ Antacids are used for subsequent ulcer treatment
➢ use of steroids & antibiotics has no benefit.
➢ For most agents, there is no specific antidote.

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19.2.3. Herbicides (ጸረ አረም፣ የአረም ማጥፊያ መርዝ)


poisoning

Herbicides are used as a weed killer which can cause human toxicity.

19.2.3.1 ChlorophenoxyHerbicides
The most common agent in this group are
✓ 2,4-dichlorophenoxyacetic acid (2,4-D)→ locally available also as Sura
✓ 2,4,5-trichlorophenoxyacetic acid (2,4,5-T);
✓ 4-chloro-2 Methyl chlorophenoxyacetic acid;
Human toxicity can occur after dermal contact, inhalation or ingestion.
Muscle is the primary target
Minimum Toxic dose: 40-50 mg/Kg or 3-4 gm

Clinical feature
Eye and mucosal irritation after direct contact
Nausea, vomiting and diarrhoea after ingestion
Dyspnea, tachypnea and pulmonary edema after inhalational exposure
Systemic toxicity (If large exposure) result in:
✓ Neurologic toxicity (Mental status changes and seizures)
✓ Cardiac toxicity (hypotension, tachycardia, and dysrhythmias);
✓ Skeletal toxicity (muscle tenderness, fasciculation, rhabdomyolysis)

Diagnosis

Made by exposure history, no specific tests for its detection;


Baseline;
✓ U/A → occult heme test positive in the presence of myoglobin)
✓ ECG and monitoring
✓ Creatinine phosphokinase (CPK)

Treatment
Supportive → Decontamination measures
✓ Administer activated charcoal, then Perform gastric lavage
✓ After lavage, give a dose of charcoal
✓ Skin decontamination if exposed
✓ Urinary alkalinization is recommended for severely poisoned patients,
✓ Hemodialysis can also be used
Respiratory support for myopathic-related respiratory failure,
No specific antidote
Patients should be monitored for rhabdomyolysis and treated as necessary.
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Asymptomatic or minimally symptomatic discharged after 4 to 6 hours of observation;


Patients with muscle effects need Admission for Close observation and monitoring.

19.2.3.2 Bipyridyl Herbicides (Paraquat and Diquat)

Includes Paraquat and Diquat which are nonselective contact herbicides.

❖ Paraquat (1, 1-dimethyl-4, 4’-bipyridylium chloride)

Available as a liquid concentrate (20%), as granules (2.5-10%), or an aerosol (0.2%)


Fast-acting, nonselective herbicide, used for killing grass and weeds
Plasma concentration peaks within minutes to 2 hours after ingestion, then distributed to most
organs, with the highest concentrations found in the kidneys and lungs;
In the lung paraquat accumulates and the high local oxygen tension generates a high levels
of toxic oxygen species and subsequent damage
In the kidney paraquat is concentrated during excretion, often leading to acute tubular
necrosis, which may occur soon after ingestion (within 24 hours)
Paraquat-induced renal dysfunction may decrease paraquat excretion, thereby enhancing
overall toxicity
A lethal oral dose of the 20% concentrate paraquat solution is about 10 to 20 mL in an adult
and 4 to 5 mL in a child;
Ingestion is responsible for the majority of paraquat deaths
Inhalation exposure to sprays can be very irritating to conjunctiva and the airway but are
unlikely to cause systemic toxicity

❖ Diquat
Has similar structure, mechanism and lethal dose as paraquat
Fewer occurrences of pulmonary injury and fibrosis because of diquat’s lower affinity for
pulmonary tissue
Caustic to the skin and GI tract, and exposure can result in renal and liver necrosis.

Clinical feature Bipyridyl poisoning (Paraquat) → depend on route of exposure

GI tract_ Ulceration of the lips, tongue, and pharynx within one to two days of ingestion,
esophageal ulceration may proceed to esophageal perforation
Skin —skin rashes (particularly on scrotal and intergluteal areas), cracked nails, and epistaxis
Lungs — Inhalation may cause local toxic effects on bronchi, possibly resulting in cough,
dyspnea, chest pain, pulmonary edema, epistaxis, and hemoptysis;
Eyes —corneal exposure can cause ulceration and scarring
Systemic toxicity
✓ Multisystem effects include acute renal failure, cardiac failure, hepatic failure, and
extensive pulmonary injury,
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✓ Evident within a few hours following large ingestions, but more typical manifestations of
renal failure and hepatocellular necrosis develop between the second and fifth days,
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with progressive pulmonary fibrosis leading to refractory hypoxemia 5 days to several


weeks later
✓ Metabolic (lactic) acidosis is common as a result of pulmonary effects (hypoxemia) and
multisystem failure;

Diagnosis
Exposure history
U/A
Organ function test
serum electrolyte
CXR → may show pneumomediastinum/pneumothorax due to corrosive rupture of the
esophagus
Paraquat test in urine/ blood
Serial pulmonary function test
Arterial blood gas determinations
Upper GI endoscopy if indicated

Treatment
Admit any patient with Paraquat poisoning even if asymptomatic,
Supportive care:
✓ ABC of life
✓ Antipain
✓ Treatment of renal failure and complications
✓ Treatment of infection,
Do not administer supplemental oxygen unless the patient is severely hypoxic, because
added oxygen stimulates superoxide radical formation and promotes oxidative stress
Maintain intravascular volume and urine output to prevent pre-renal kidney injury,
Decontamination
✓ Remove clothing for splash
✓ Skin washing with mild detergent for dermal contact
✓ Irrigate eyes with saline/ copious water if conjunctivae exposure,
✓ Lavage not routinely recommended unless patient present early and for ingested
✓ Activated charcoal (1gm/kg up to 100 gm), and repeat dose in 1–2 hours
✓ Prolonged Hemoperfusion or Hemodialysis two to three weeks, 4-6 hours daily,
Repeated pulse doses of glucocorticoids and cyclophosphamide may improve survival in
severe cases
Treatment for diquat poisoning is similar to that for paraquat.

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19.2.3.2. Organophosphate herbicides


In addition to their use as insecticides, some organophosphate compounds are effective
herbicides.
Butiphos is used commonly as a cotton defoliant before mechanical harvesting.
Treatment is identical to that for organophosphate insecticides.

19.2.4. Rodenticides Poisoning (የአይጥ መርዝ እና የነቀዝ መድሃኒት)


መመረዝ
Are chemicals used for extermination of rodents like rat and mouse; sometimes used as a
grain preservative by destroying insects;
Classified based on whether the agent has anticoagulant or non-anticoagulant effect,

A. Non-anticoagulant Rodenticides (Metalophosphate) Poisoning

includes: Zinc/ Aluminum Phosphide, Arsenic, Barium carbonate/ hydroxide/ chloride/sulfide,


Phosphorus (elemental/ yellow), sodium fluroacetate, Strychnine, Tetramine, Thallium Sulfate ,
ANTU, Bromethalin, Dicaboximide, Vacor.

Aluminum phosphide (የነቀዝ መድሃኒት) and Zinc Phosphide (የአይጥ


መርዝ)
Metal phosphides have been used as a means of killing rodents and are considered single
dose fast acting rodenticides (death occurs commonly within 1 - 3 days after single bait
ingestion).
A bait consisting of food and a phosphide (usually zinc phosphide) is left where the rodents
can eat it, are used to preserve grain, especially wheat, and to kill rats.
Grain preservative is usually sold as tablets, and rat killer is sold as pellets.
Examples of locally available poisons include: Celphos (Al Phosphide) 56%, Commando (Zn
Phosphide) 80%, No Rat (Zn Phosphide).
Cause Cellular toxicity and necrosis to the GI tract, kidney, and liver if ingested and to the
lungs if inhaled;

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Toxic dose;
✓ The LD50 zinc phosphide,
▪ lowest reported lethal dose in humans is 4 g;
✓ Aluminum phosphide
▪ Ingestion of as little as 500mg aluminum phosphide has caused death in an
adult
▪ It has high mortality rate (30 to 100%)
▪ Survival is unlikely if > 1.5g is ingested. Since 1 tab is 3 gram and patients
have taken at least one tablet, mortality is 100% in our setup

Picture; Aluminum phosphide tablets

Clinical feature
The onset of symptoms is usually rapid, although delayed onset of pulmonary edema has
been described;
If ingested; Immediate nausea, vomiting, epigastric pain, phosphorous or fishy breath, black
vomitus, and GI irritation or ulceration
Inhalation of phosphine gas is associated with cough, dyspnea, headache, dizziness, and
vomiting
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Myocardial toxicity, shock unresponsive to Vassopressers, and acute lung injury, agitation,
coma, seizures, hepato-renal injury, metabolic acidosis, hypocalcaemia tetany in both
exposures has been observed;

Diagnosis
Is based on a history of exposure to the agent
IX;
✓ RBS
✓ BUN & Cr
✓ Electrolytes
✓ liver transaminases
✓ CXR
✓ ABG or oximetry

Treatment
Emergency and Supportive care
Decontamination → Gastric lavage with potassium permanganate or combination coconut oil
and 3- 5%sodium bicarbonate (Reduce stomach acid and resulting production of phosphine
gas);
No specific antidote
✓ Magnesium sulphate IV with low dose of dopamine may be beneficial
✓ Consider acetylcysteine
Admit and observe for 48 - 72 hours for delayed onset of pulmonary edema
See the algorism below

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Management of Metalophosphate Poisoning


Primary survey → ABCD of life
Gastric Lavage with Potassium permanganate (1:1000) unless contraindicated
Activated charcoal 30 - 100mg if available and not contraindicated

Then

If BP < 90/60mmHg and PR ≥ 100 BPM


If BP < 90/60mmHg and PR < 100 BPM
→ Start Dopamine 5 µg/KG/min infusion → Start Adrenaline 0.1 µg/KG/min infusion
Or through perfuser
through perfuser

And

-Hydrocortisone, 200mg, IV, QID for 48 hr’s


-Calcium gluconate 10% (10ml) with 10ml of NS to run over 5-10 minutes (slowly) QID
for 48hr’s
-Magnesium sulphate, 1gm (2ml of 50% solution) with 5 ml of NS, IV Push over 2
minutes. 0.5 gm(1ml) with 1ml Lidocaine, IM, on each Buttock and 3 gm(6ml), with
300ml of NS to run over 3 hrs LOADING

Then

1gm with 100ml of NS IV, TID for 48 hrs Maintenance

N.B

Before and after administration of MgSo4 see; PR, RR, Patellar reflex and UOP
If possible, follow with serum magnesium Level

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B. Anti-coagulant rodenticides
First generation rodenticidal anticoagulants
✓ They are less toxic than second generation agents.
✓ E.g. Warfarin (Coumadin) is used therapeutically and as rodenticides;
Second generation agents
✓ They are far more toxic than first generation.
✓ Lethal after a single ingestion of bait thus, they are sometimes referred to as "super
warfarin’s"
✓ Examples of Super warfarin: Brodifacoum, Diphacinone, Bromadiolone,
Chlorophacinone, Difenacoum, Pindone, and Valone;
✓ Have profound and prolonged anticoagulant effects.
✓ Locally available brands include Zara.

Toxic dose: most warfarin-based rodenticides produce little effect after a single dose (10-
20mg); While a single dose of super warfarin (as low as 1 mg) produce a significant clinical
effect,

Clinical feature

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Seen as early as 8-12 hrs but mostly delayed by 1-2 days after ingestion and continue for
days, weeks or months after super warfarin ingestion

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Sign and symptom of bleeding diathesis such as ecchymoses, subconjunctival hemorrhage,


bleeding gums, or evidence of internal hemorrhage (eg, hematemesis, melena, or hematuria)
the most immediately life-threatening complications are massive GI bleeding and ICH.

Diagnosis
Based on exposure history
Coagulation profile → Elevated levels of PT (INR) from admission level suggest poisoning
and a normal PT level after 48 hrs of exposure rules out significant exposure
CBC → Platelet count which may be used to rule out other causes of bleeding
BG &RH and cross-match

Treatment
Emergency and supportive treatment
✓ Treat hypovolemia/ shock with crystalloids,
✓ Transfusion with whole blood or FFP
✓ Consult neurosurgeon if intracranial bleeding suspected
✓ Minimize or avoid invasive procedures like NGT insertion or endotracheal intubation if
possible
✓ Avoid drug, which may decrease metabolism of warfarin like cimetidine, sulfonamides,
NSAID;
Antidote → Vitamin K (phytonadione), effectively restores the production of clotting factors
✓ 5-10mg very slowly IV/SC, max; 200 mg/d
✓ Repeated may be required, especially in super warfarin product ingestion
✓ Titrate Vit. K dose based on PTT level,
✓ May require FFP/ whole blood transfusion for active bleeding as Vit. K take effect (6-
24hr later).
Decontamination: Activated charcoal can be used.
Enhanced elimination has no role.

19.2.5. Ethanol (ከልክ ያለፈ ስካር፣ በአልኮል መመረዝ)


Ethanol (CH3CH2OH) is the most common alcohol ingested as a recreation or used with other
chemical or drugs intentionally as suicidal means.
Its principal effects are GI irritation and intoxication; and it doesn’t by itself produce metabolic
acidosis.
Toxicity most commonly occurs from ingestion, but ethanol may also be absorbed via
inhalation or percutaneous exposure.
A standard alcoholic beverage, such as 12 oz (355 mL) of beer (2% to 6% ethanol by
volume), 5 oz (148 mL) of wine (10% to 20% ethanol by volume), or 1.5 oz (44 mL) of 80-
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Ethanol may be found in high concentrations in many other common household products
such as mouthwash (may contain up to 75% ethanol by volume), colognes and perfumes (up
to 40% to 60%), and as a diluent or solvent for medications (concentration varies widely
between 0.4% and 65%), hand sanitizers ( Up to 60 -70%)
Some ethanol is broken down in the stomach by gastric alcohol dehydrogenase, which lowers
the amount available for absorption by producing acetaldehyde. This enzyme is present at
higher levels in men than in women, which may account for the fact that women usually
develop a higher blood ethanol level than men after consuming the same dose per kilogram
of body weight.
Ethanol is a CNS depressant.

Clinical features
The hallmark of ethanol toxicity is clinical inebriation.
Behavioural disinhibition may initially appear as euphoria or agitation and combativeness.
As intoxication becomes more severe, slurred speech, nystagmus, ataxia, and decreased
motor coordination develop.
Severe intoxication may cause respiratory depression and coma.
Nausea and vomiting
Peripheral vasodilation promoting hypothermia and flushed, warm skin may also lead to
orthostatic hypotension (usually mild) and reflex tachycardia.
Hypoglycaemia
Lactic ketoacidosis.
Alcohol withdrawal syndrome
Signs
Look evidence of infections and traumatic injuries
Depressed mental status

Diagnosis
RBS
serum alcohol levels in patients with altered mental status of unclear cause.

Treatment
Management is observation until sobriety.
Treat hypoglycaemia with IV glucose 0.5 to 1 grams/kg
long-term drinkers are sometimes treated with IV fluids containing magnesium, folate,
thiamine, and multivitamins, termed a banana bag because of the yellow color imparted by
the multivitamin mixture.
Wernicke’s encephalopathy (characterized by abnormal mental status, ataxia, and nystagmus)
requires daily treatment with thiamine, 100 mg, until normal diet is resumed.
Prior to discharge, reassess for an underlying mental health disorder, such as suicidal or
homicidal ideation, that requires further care or hospital admission.
Clinical judgment, rather than a serum ethanol level, determines the appropriateness of
discharge.
Discharge the patient in the care of a responsible companion.
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19.2.6. Household Products

19.2.6.1. Detergents (መንጽህ)


Detergents are synthetic surface-active agents containing chemical products used at home.
Most products contain bleaching (chlorine-releasing), bacteriostatic (having a low concentration
of quaternary ammonium compound), or enzymatic agents.
Detergents may cause skin irritation and have sensitizing properties.
Mortality and serious morbidity are rare.

Clinical presentation
Nausea, vomiting, and diarrhoea, hematemesis may occur and as a result secondary
dehydration and electrolyte imbalance may develop.
Mild ocular irritation is possible.
Dermal contact generally causes a mild erythema or rash

Diagnosis:
Based on history of exposure.
IX; RBS, Electrolytes, glucose, calcium and Phosphate (after ingestion of phosphate-containing
products, Methaemoglobin (Cationic detergents)

Treatment
In patients with protracted vomiting or diarrhea, administer IV fluids to correct dehydration and
electrolyte imbalance.
If corrosive injury, use the management guideline for corrosive ingestion.
If hypocalcaemia occurs after ingestion of a phosphate-containing product, give IV calcium.
Decontamination:
✓ dilute orally with small amounts of water or milk.
✓ Do not induce vomiting because of the risk for corrosive injury.
✓ Consider gastric lavage only for massive ingestions.
✓ Activated charcoal is not effective.
✓ In severe cases anti-emetics may be required (e.g., metoclopramide, 1omg /0.2–0.4
mg/kg/, PO, SC, or IM, QID based).
Eyes and skin exposure→ irrigate with copious amounts of tepid water or saline. Consult an
ophthalmologist if eye pain persists or if there is significant corneal injury.

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19.2.6.2. Sodium Hypochlorite /Bleach/(በረኪና)


Sodium hypochlorite is a chemical commonly found in bleach, water purifiers, and cleaning
products.
Sodium hypochlorite is a green/yellow liquid with the characteristic smell of chlorine and it is
commonly known as bleach (berekina).
Household bleach usually contains approximately 5 % sodium hypochlorite, although some
may contain up to 10 %...
Chlorine gas produces a corrosive effect on contact with moist tissues such as the eyes and
upper respiratory tract.

Clinical presentation
HEENT: exposure to the fumes can cause burning in the eyes, ears, and nose, pain in the
mouth, and pain in the throat
RS; chest tightness, coughing and difficulty of breathing. In more severe cases increased
breathing rate, wheezing, swelling of the airways and respiratory failure may occur, the onset
of which may take up to 36 h.
Skin: irritation of the exposed area. Burns and blistering have been reported.
GIT: abdominal pain, vomiting
CVS: Rare cases of cardiovascular collapse and shock are presumed to consider secondary
to severe local injury.
Nervous system: Lethargy, delirium and coma can occur in patients with severe respiratory
effects.

laboratory studies
For ingestion → CBC, electrolytes, and chest and abdominal x-rays to look for mediastinal or
intraabdominal air, which suggests perforation.
For inhalation, arterial blood gases and pulse oximetry.

Treatment
Emergency and supportive measures
o Inhalation of chlorine gas:
✓ Immediately remove victim from exposure
✓ Give humidified supplemental oxygen.
✓ Observe for upper airway obstruction, and intubate if necessary.
✓ Use bronchodilators for wheezing and treat non-cardiogenic pulmonary edema if it
occurs.

o Ingestion of hypochlorite solution:


✓ if a solution of 10% or greater has been ingested, or if there are any symptoms of

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corrosive injury (dysphagia, drooling, or pain), flexible endoscopy is recommended to
evaluate for serious esophageal or gastric injury.

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Decontamination: for oral exposures, emesis and activated charcoal are contraindicated.
Instead, immediately give water by mouth. Do not induce vomiting.
Skin and eyes: remove contaminated clothing, and flush exposed skin immediately with
copious water. Irrigate exposed eyes with water or saline. Bathing with mild shampoo and
thorough rinsing for significant dermal exposures is recommended.

19.2.6.3 Dettol (ዲቶል)

Dettol is a commonly available household disinfectant. It contains Isopropyl alcohol (12%),


Chlorxylenol (4.8%), and Pine oil (9%).

Clinical presentation:
It causes CNS depression, corrosion of oral mucosa and gastrointestinal tract (upper GI
hemorrhage), laryngeal edema, upper airway obstruction, bronchospasm, nephrotoxicity,
hepatitis and cardiac arrhythmias.
The main risk of poisoning is aspiration with subsequent development of acute respiratory
distress syndrome (ARDS), pneumonia and sudden cardio-respiratory arrest.
Micro-aspiration has been hypothesized to be the reason for delayed upper airway obstruction
that may occur in totally asymptomatic patients up to 48 h after admission.

Treatment:
The mainstay of dettol poisoning is supportive management along with close observation in
hospital for stridor.
Emesis and gastric lavage should not normally be attempted. The only indication for gastric
lavage in the acute setting is a patient who has consumed other poison along with Dettol.
Patient should be started on IV fluids with regular monitoring of electrolytes.
Adolescents and adults who have consumed more than 200 to 300 ml and children who
have consumed lesser amounts should be kept NPO and watched carefully for signs and
symptoms of nephrotoxicity and CNS depression.
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In case of severe poisoning or any evidence of hematuria or azotemia, do forced alkaline


diuresis
Exchange transfusion, and early dialysis for isopropyl alcohol can be attempted in rare
patients who are deteriorating steadily despite adequate supportive measures.
Even patients who arrive comatose to the ED frequently demonstrate a rapid and complete
recovery. It is, however, important to monitor closely in hospital for strider for a minimum of
48 hours after admission.

19.2.7. Hydrocarbon (ጋዝ፤ቤንዚን፤ኪሮሲን) poisoning


Hydrocarbons, or petroleum distillates, are widely used in the petroleum, plastic, agricultural,
and chemical industries as solvents, degreasers, fuels, and pesticides.

CLASSES OF HYDROCARBONS

The four structural classes of hydrocarbons are:


✓ Aromatic hydrocarbons
✓ Aliphatic hydrocarbons
✓ Halogenated hydrocarbons
✓ Terpene hydrocarbons
Aromatic hydrocarbons
✓ Are cyclic compounds containing a benzene ring (eg, benzene, toluene, and
xylene).
✓ They are used primarily in solvents, glues, nail polishes, paints, and paint
removers.
Aliphatic hydrocarbons
✓ Are petroleum distillates such as gasoline, kerosene, and naphtha.
✓ They are found in furniture polishes, lamp oil, and lighter fluid.
Halogenated hydrocarbons are fluorinated, chlorinated, or brominated (eg, methylene
chloride, chloroform, carbon tetrachloride, trichloroethylene, tetrachloroethylene).
The terpenes include turpentine and pine oil.

HYDROCARBON TOXICITY

Hydrocarbons also can be classified according to their potential for toxicity:


✓ Low toxicity (unless complicated by gross aspiration) – Examples include
asphalt, tars, mineral oil, petroleum jelly, motor oil, and axle grease.

✓ Aspiration hazard – Clinical effects are typically limited to direct pulmonary


damage and subsequent inflammation. Examples include turpentine, gasoline,
kerosene, mineral seal oil (furniture polish), charcoal lighter fluid, mineral spirits,
or outdoor torch and cigarette lighter fluids.

✓ Systemic toxicity
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▪ Halogenated and aromatic hydrocarbons are absorbed readily through the


gastrointestinal and/or respiratory systems.
▪ Systemic effects include cardiac arrhythmias secondary to myocardial
sensitization and CNS depression.
▪ Systemic toxicity also occurs after ingestion of compounds that combine
aliphatic hydrocarbons with toxic additives (eg, organophosphates, heavy
metals, camphor

Toxicity Caused by direct injury from pulmonary aspiration or systemic intoxication after
ingestion, inhalation, or skin absorption.
Aspiration leads to a necrotizing, potentially fatal chemical pneumonitis.
CNS toxicity is manifested as alterations in mental status, including narcosis, inebriation, and
frank coma.
In addition to these toxicities, the solvents possess additional toxicities, including the risk of
bone marrow injury (in the case of benzene → long term risk factor for hematologic
malignancy).
Aliphatic hydrocarbons and simple petroleum distillates such as lighter fluid, kerosene,
furniture polish, and gasoline are poorly absorbed from the gastrointestinal tract and do not
pose a significant risk of systemic toxicity after ingestion, as long as they are not aspirated.
In contrast, many aromatic and halogenated hydrocarbons, alcohols, ethers, ketones, and
other substituted or complex hydrocarbons are capable of causing serious systemic toxicity,
such as coma, seizures, and cardiac arrhythmias.
Inhalation of any hydrocarbon vapors in an enclosed space may cause intoxication as a
result of systemic absorption or by displacing oxygen from the atmosphere.
Dermal absorption can be significant for some agents but is insignificant for most of the
simple, aliphatic compounds.

Clinical Presentation:
Pulmonary presents as coughing, gagging, or choking. This may progress within a few hours’
to tachypnea, wheezing, and severe chemical pneumonitis.
Death may ensue from secondary bacterial infection and other respiratory complications.
Ingestion often causes abrupt nausea and vomiting, occasionally with hemorrhagic
gastroenteritis.
Some compounds may be absorbed and produce systemic toxicity which includes confusion,
ataxia, lethargy, and headache.
With significant exposure, syncope, coma, and respiratory arrest may occur.
Cardiac arrhythmias may occur owing to myocardial sensitization (with chlorinated and
fluorinated compounds

Diagnosis: →based on history of exposure and typical findings.

Aspiration pneumonitis: 1359


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✓ If symptoms are not present within 6 h of exposure, it is very unlikely that chemical
pneumonitis will occur.
✓ Chest x-ray and arterial blood gases or oximetry may assist in the diagnosis.
Systemic intoxication:
✓ diagnosis is based on history of ingestion or inhalation, accompanied by the
appropriate systemic clinical manifestations.

Other useful laboratory studies:


✓ RBS
✓ electrolytes BUN, creatinine, liver transaminases
✓ chest x-ray
➢ If the patient has any respiratory symptoms upon arrival to the ED, CXR should be
obtained immediately. Symptoms occur as soon as 30 min after aspiration or may be
delayed for several hours. Lung radiographic changes usually occur within 2-8 h,
peaking in 48-72 h. aspiration pneumonia features, Pneumatoceles and pleural
effusions may occur.
✓ ECG monitoring for suspected significant inhalation or ingestion.
➢ Cardiac dysrhythmias may occur and may be exacerbated by hypoxia and acid-base
or electrolyte disturbances.
✓ ABG

Treatment
Treatment is generally supportive, consisting of oxygen, fluids, and ventilatory support as
necessary.
Because most hydrocarbons cause clinical toxicity only when aspirated, the mainstay of
treatment is to leave ingested compounds in the gut (when possible) and to prevent emesis
or reflux.
Gastric emptying is generally reserved only for those compounds with the potential for
systemic toxic effects. Gastric emptying is always contraindicated in other cases.
The mnemonic CHAMP refers collectively to the following hydrocarbons:
Camphor
Halogenated carbons, Patients who ingest these compounds in volumes >30 mL,
Aromatic hydrocarbons such as might occur with intentional overdose, may benefit
Metals and from gastric emptying. This is still a high-risk procedure that
Pesticides. can result in further aspiration.

Antibiotics should not be used prophylactically but should be reserved for specific infections if
they develop.
The use of corticosteroids in the treatment of aspiration is not recommended.
In the event of hypotension or bronchospasm, epinephrine and other catecholamine containing
vasopressors, (Dopamine and Norepinephrine) are contraindicated because hydrocarbons are
known to cause ventricular irritability and predispose to fibrillation, an effect that is
exacerbated by catecholamines.
Decontamination
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✓ Skin and eyes: remove contaminated clothing and wash exposed skin with water and
soap. Irrigate exposed eyes with copious tepid water or saline and perform fluorescein
examination for corneal injury.
✓ Ingestion: for agents with no known systemic toxicity, gut decontamination is neither
necessary nor desirable because any gut-emptying procedure may increase the risk of
aspiration.

19.2.8. Carbon monoxide poisoning (በጭስ መመረዝ)


CO is an odourless, tasteless, colourless, non-irritating gas formed by the incomplete
combustion of any carbon-containing material (e.g., wood, coal).
Common sources of human exposure include smoke inhalation in fires, faulty or poorly
ventilated charcoal, kerosene or gas.
CO binds to hemoglobin with an affinity 200 to 300 times greater than that of oxygen
resulting in reduced oxyhemoglobin saturation and decreased blood oxygen-carrying
capacity.

Clinical features
☛ High index of clinical suspicion is important
☛ Acute carbon monoxide poisoning:
o Mild levels: headache, dizziness, weakness, nausea, malaise
o Moderate: confusion, lethargy, syncope, nystagmus, ataxia
o Severe: coma, convulsions, pulmonary edema, myocardial infarction, cardiac arrest.
Acute renal failure and rhabdomyolysis have also been reported with severe toxicity
☛ Sub-acute clinical squeal of CO poisoning:
o Persistent neurologic dysfunction is the most common long term sequealae of carbon
monoxide poisoning.
o Onset occurs between several days and several weeks or even months following
exposure.
o Decreased cognitive function, personality changes, dementia, Parkinson and decelerate
rigidity.
o Exposure during pregnancy may result in fetal death.

Investigations

☛ Clinical: Dx is based on a compatible Hx and physical exam in addition with an elevated


carboxyhaemoglobin level measure by co oximetry of a blood gas sample.
☛ Other laboratory studies are helpful in evaluating the extent to the toxicity and include CBC,
electrolytes, glucose, BUN, creatinine and CPK.

Treatment
Non pharmacologic
☛ Supportive treatment
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☛ Take the patient out to open air.

Pharmacologic
☛ The most important interventions in the management are removal from the CO source &
administer 100% oxygen by face mask
☛ Comatose patients should be intubated & mechanically ventilated using 100% oxygen.
☛ Hyperbaric oxygen

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19.3. Snake bite (የእባብ ንክሻ)


The majority of snakebites are non–poisonous; only few species are venomous (poisonous).
Most common venomous snakes are the pit vipers (vasculotoxic) and the elapidae and
hydrphidae (primarily neurotoxic).
Children, because of their smaller body size, are far more likely to have severe
envenomation.

Clinical features
Local signs and symptoms

There will be an immediate pain.


Local bruises and persistent bleeding from fang puncture.
Swelling begins within 10-20 minutes. It may become extensive after viper and spitting
cobras, involving whole limb or adjacent trunk or whole body in children.
Draining lymph nodes may become enlarged, painful and tender within 30-60 minutes.

Figure: Moderately severe envenomation. Note edema and early ecchymosis 2 h after a bite to the finger

Blisters, may appear near the fang marks in 12-24 hours.


Demarcated pigmentation or depigmentation with anesthesia and a distinctive smell of
putrefaction are sign of necrosis. This progresses to frank necrosis with sloughing of dead
tissue.
Increasing myalgia, blisters advances to tissue necrosis and gangrene will develop.

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Figure: left) Severe envenomation. Note extensive ecchymosis 5 days after a bite to the ankle. Right) Early
stages of severe, full-thickness necrosis 5 days after a viper bite

Figure; Severe necrosis 10 days after a pit viper bite in a young child

Systemic signs and symptoms


Bleeding and clotting disorder:
o There is local bleeding from wound, fang puncture and venepuncture site and
systemic bleeding from coagulation abnormality and impaired platelets.
o Spontaneous systemic bleeding (e.gs from gum and nose, hematemesis, rectal
bleeding, hemoptysis, hematuria, retroperitoneal, intracranial bleeding and in pregnant
woman ante-partum hemorrhage).
Shock (hypotension): could be anaphylaxis or bleeding related or cardiotoxic effect.
Progressive descending paralysis starting with dropping eyelids (ptosis) and pupillary
abnormality, paralysis of eye movement causing diplopia(ophthalmoplegia),; paralysis of facial
muscle, jaw, tongue, neck flexors causing “broken neck” sign, and other cranial palsies,
difficulty of producing speech(dysphonia), difficulty of handling secretions(drooling) finally
respiratory muscle and total flaccid paralysis.
Acute renal failure may ensue because of hypotension or rhabdomyolysis.

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Severity of envenomation:

None ("dry bite"): fang marks only


Mild: local findings only. e.g., pain, local ecchymosis, non-progressive swelling
Moderate: swelling (clearly progressing, systemic signs or symptoms, and/or laboratory
abnormalities
Severe: Respiratory distress, Neurologic dysfunction, and/or Cardiovascular instability/shock

Investigations
CBC
BG & RH
Urinalysis for presence myoglobin or blood
BUN and Creatinine
LFT
PT/ PTT /INR
Electrolytes
Whole blood clotting test (leave 2-5ml of blood in dried test tube. Failure to clot after 20
minutes implies incoagulable blood)

N.B. Avoid venepuncture in state of generalized bleeding

Treatment

Non pharmacologic
First Aid
☛ A significant proportion of snake bites do not result in envenomation……observe if no
clinical features of local/systemic sign and/ or symptoms;
☛ Move patient to a safe area
☛ Remove anything tight around the bitten area (ankle bracelets, Rings)
☛ Splint the limb below the level of the heart to reduce movement and absorption of
venom if the limb is the affected organ; apply a firm bandage to affected limb from
fingers or toes to proximal site of bite.
☛ Do not move the limb
o Carry the person on a stretcher and tie the limb to a straight piece of wood.
o C lean the wound and reassure the patient.

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At the hospital

☛ Bed rest, reassure, keep warm


☛ Assess patient's airway, breathing and circulation (ABC of resuscitation)
o Give NS infusion (bolus of 20–40 mL/kg) if the patient is hypotensive; if hypotension
persists, consider anti-venom. Only after aggressive volume resuscitation and
antivenom administration; if the shock unresponsive, vasopressors (e.g., adrenaline,
dopamine) should be added.
o With any evidence of difficulty swallowing or breathing, proceed with endotracheal
intubation and ventilatory support (may be required for days or weeks).
o Paralysis of respiratory muscles can last for days and requires intubation and
mechanical ventilation or manual ventilation;
☛ For probable venomous bites:
o Measures applied in the field (such as constriction bands) should be removed once IV
access has been obtained
o Clean site of bite with antiseptic lotion or soap and water
o Do not attempt to suck or make any incisions at the site of the bite
o Leave wound open; punctured wounds are especially likely to be infected.
o Avoid intramuscular injections
o In acute renal failure dialysis (peritoneal or hemodialysis), usually reversible
o If the snake is identified as non-poisonous or there is absence of swelling or systemic
signs after 6 hours reassure the patient
o Surgical debridement when required

Pharmacologic
If any evidence of neurologic dysfunction (e.g., any cranial nerve abnormalities such as ptosis
or inability to maintain upward gaze):
o Pre-treat with atropine: 0.6 mg IV (children, 0.02 mg/kg; min. of 0.1 mg) Followed by a
trial of anticholinesterase inhibitors
▪ Neostigmine: 1.5–2.0 mg IM (children, 0.025–0.08 mg/kg)
▪ If objective improvement is evident at 5 min, continue neostigmine at a dose of 0.5 mg
(children, 0.01 mg/kg) IV or SC every 30 min as needed, with continued administration of
atropine by continuous infusion of 0.6 mg over 8 h (children, 0.02 mg/kg over 8 h).
Prophylactic antibiotics are unnecessary unless prehospital care included incisions or mouth
suction.
If there is secondary infection:
First line
o Amoxicillin/clavulanic acid, 500/125mg, (i.e. Augmentin, 625mg), PO, T ID for 5-7
days.
o Immunization, primary or booster:
Tetanus toxoid vaccine, IM, 0.5mL immediately.
o
Analgesia
For mild pain:
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o Paracetamol, 1g, P.O, 4-6 hourly when required to a maximum of 4 doses per 24
hours.
For severe pain: ADD
☛ Tramadol, 50-100mg, 2-3X per day

N.B. The use of an NSAID is not recommended due to the potential danger of AKI in
a hypotensive patient.

Polyvalent antivenom

Indications for polyvalent antivenom:


o Worsening of local injury (e.g., pain, ecchymosis, or swelling)
o Abnormal results on laboratory tests (e.g., worsening platelet count, prolonged
coagulation times)
o Systemic manifestations (e.g., unstable vital signs or abnormal mental status).
o All patients with confirmed mamba bites before symptom onset
o Patients with confirmed puff adder or Gaboon adder bites should receive antivenom
at the onset of any symptoms

N.B.
☛ In most cases patients do not need and should not be given antivenom.
☛ The dose of antivenom is the same for adults and children.
☛ Serum sickness is a relatively common adverse event.
☛ Even after the administration of antivenom, patients with neurotoxic snakebites may need
ventilation.

Polyvalent snake antivenom

Slow IV infusion. Dilute 100 mL in 300ml of NS. Administer slowly for the first 15
minutes, as most allergic reactions will occur within this period. Increase the flow rate
gradually to complete the infusion within one hour.
o Prepare IM epinephrine (adrenaline) and IV chlorpheniramine, be ready if allergic
reaction occurs when antivenum given.
o Before giving the anti-venom, perform skin test with 0.02 to 0.03 ml in 1:10 dilution,
subcutaneous, to test for anaphylaxis. If itching/urticarial rash, restlessness, fever,
cough or difficult breathing develop, then stop anti-venom and give epinephrine
(adrenaline).
o Start giving the antivenom with minimal dose for mild cases with a minimal dose of
22-40 ml and give a maximum of 200-400 ml. Blood transfusion should not be
required if anti-venom is given.
o Continue to observe for progression of edema and systemic signs of envenomation
during and after antivenom infusion.
✓ Measure limb circumference at several sites above and below the bite
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✓ Outline the advancing border of edema with a pen every 30 minutes.


✓ These measures serve as an index of the progression as well as a guide for
antivenom administration.
o More anti-venom should be given after 1–2 hr if the patient is continuing to bleed
briskly or has deteriorating neurotoxic or cardiovascular signs.
o Repeat laboratory determinations every 4 hours or after each course of antivenom
therapy, whichever is more frequent. Repeat if there is no clinical improvement after
the infusion.
o Clotting function returns to normal only after clotting factors are produced by the liver.
o Response of abnormal neurological signs to anti-venom is more variable and depends
on type of venom
o Neurotoxicity from elapid bites (cobra and mamba) may be harder to reverse with
antivenom. Once neurotoxicity is established and endotracheal intubation is required,
further doses of antivenom are unlikely to be beneficial. In such cases, the victim
must be maintained on mechanical ventilation until recovery, which may take days or
weeks.
o Mild hypersensitivity reactions should not be a reason not to give polyvalent.
o If acute reaction to antivenom develops and depending on severity of reaction:
▪ Stop infusion.
▪ Treat with standard doses of epinephrine (IM or IV; IV route only in the setting
of severe hypotension)
▪ Antihistamines (IV) e.g., Diphenhydramine, 1 mg/kg to a max. 100 mg, plus
Cimetidine, 5–10 mg/kg to a maximum of 300 mg
▪ IV glucocorticoids
▪ When reaction is controlled, restart antivenom ASAP if still indicated (may
further dilute in a larger volume of NS).

Surgical Management
Seek surgical opinion if there is severe swelling in a limb, it is pulseless or painful or there
is local necrosis
Surgical care will include:
o Intact serum-filled vesicles or hemorrhagic blebs should be left undisturbed. If ruptured,
they should be debrided with sterile technique.
o Excision of dead tissue from wound
o Incision of fascial membranes to relieve pressure in limb compartments, if necessary
o Skin grafting, if extensive necrosis
Antibiotic treatment is not required unless there is tissue necrosis at wound site
Tracheostomy (or endotracheal intubation) if paralysis of muscles involved in swallowing
occurs
Bite in the hand, fore-arm or leg may be complicated by muscle-compartment syndrome If
there are signs of compartment syndrome
✓ Elevate the leg
✓ Consider additional dosing of the infusion
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✓ Consider fasciotomy if there is no response for conservative management.

Monitoring
Monitor very closely immediately after admission, then hourly for at least 24 hours as
envenomination can develop.
Any patient with signs of envenomation should be observed in the hospital for at least 24 h,
Patients whose condition is not stable should be admitted to an intensive care setting
Measure/record circumferences of the bitten extremity every 15 min until swelling has
stabilized; while monitoring, the extremity should be positioned at approximately heart level.
Admit to hospital. (If no evidence of envenomation, monitor for 8 h before discharge.)
Institute monitoring (cardiac and pulse oximetry)
Vital signs, cardiac rhythm, oxygen saturation, urine output.
At discharge, victims of venomous snakebite should be warned about possible recurrent
coagulopathy, signs and symptoms of wound infection, antivenom-related serum sickness

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19.4. Specific Drug Overdoses (እጅግ ከመጠን በላይ


የሆነ መድሃኒት በመውሰድ መመረዝ)

19.4.1. Acetaminophen/Paracetamol/ overdose

✓ Acetaminophen or Paracetamol having many brand names is a widely used drug found in
many over the counter and prescription analgesics and cold remedies.
✓ Paracetamol overdose can cause Hepatotoxicity, Renal damage, Fetal death and spontaneous
abortion:
✓ Toxic dose; Acute ingestion of > 6–7 g (>150–200 mg/kg in children) or in adults’ is
potentially hepatotoxic.
✓ Chronic toxicity may happen after daily consumption of high therapeutic doses (4–6 g/day)
for 24hr or more by alcoholic patients. Children have developed toxicity after receiving as
little as 60– 150 mg/kg/day for 2–8 days.
✓ High-risk patients for toxicity include; If the patient is alcoholic, malnourished, or fasting, or
taking drugs that induce P-450 activity (e.g., anticonvulsants, INH)

Clinical Presentation
✓ Clinical manifestations depend on the time after ingestion.
✓ Early:
o usually no symptoms other than anorexia, nausea, or vomiting. Rarely, a massive
overdose may cause altered mental status and metabolic acidosis.
✓ After 24–48 hrs
o when AST and ALT level rise, hepatic necrosis becomes evident.
o If acute fulminant hepatic failure occurs, encephalopathy and death may ensue.
o Encephalopathy, metabolic acidosis, hypoglycaemia, and progressive rise in the
prothrombin time are indications of severe liver injury and has poor prognosis.
o Acute renal failure occasionally occurs, with or without concomitant liver failure.

Investigation
✓ RBS
✓ Electrolytes
✓ BUN and creatinine → the renal injury manifested after 2-3 days
✓ Liver enzymes
✓ PT, INR
✓ Urine HCG→ because acetaminophen cross placenta by 14 weeks. So, antidote should be
considered in pregnancy ASAP.
✓ ECG → to exclude the presence of co-ingested cardiotoxic substances.
✓ Abdominal U/S → may reveal hepatic enlargement, renal abnormality, and inflammatory
changes.
✓ CT→ to see cerebral edema and encephalopathy in For patients with altered mental status
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✓ Interpretation of serum acetaminophen level lab result is based on Rumack-Matthew


nomogram (refer Poisoning and Drug Overdose Management Training for Health Care Professionals, FMOH, Ethiopia, 2020)

Treatment
A. Emergency and supportive measures:

✓ Antiemetic (metoclopramide or ondansetron) for Spontaneous vomiting


✓ Provide general supportive care for hepatic or renal failure if it occurs.
✓ Treatment for acetaminophen-induced fulminant hepatic failure includes
o N-Acetylcysteine (NAC) therapy
o Correction of coagulopathy and acidosis
o Monitoring for and aggressive treatment of cerebral edema, and
o Early patient referral to a liver specialty/transplant centre if available.

B. Decontamination:

✓ Prehospital. →
o Activated charcoal, if available.
o Ipecac-induced vomiting may be useful for initial treatment of children at home if it can
be given within 30 min of exposure.
✓ Hospital.
o Activated charcoal. It should be given before po NAC. This is because activated charcoal
will adsorb the po NAC
o Gastric emptying is not necessary if charcoal can be given promptly.

C. Specific drugs and antidotes:

NAC (N-Acetylcysteine)

✓ Indication to Consider giving NAC


o If the patient is at increased risk for toxicity (if patient falls within a high-risk group)
o Multiple or subacute overdoses
o Time of ingestion is uncertain or unreliable.
o In chronic acetaminophen ingestions, NAC treatment is advised
➢ If the amount ingested was more than 150–200 mg/kg or 6–7 g within a 24-hour
period
➢ If liver enzymes are elevated
✓ NAC ORAL; loading dose of 140 mg/kg PO, followed by 70 mg/kg every 4 h for 17 more
doses over 72 h (a total of 18 doses).
o If stat serum levels of acetaminophen are not immediately available, initiate antidote
therapy with NAC
o Maximal benefit, if it is started within 8– 10 h and of diminishing value after12–16 h.
However, treatment should not be withheld, even if the client comes as late as 48 h post
ingestion
o If the patient vomits, repeat the dose.
o If vomiting interferes with oral acetylcysteine administration, give it by gastric tube and
use antiemetic or give the NAC iv if necessary.
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✓ IV NAC;
o It is recommended if there is altered mental status or severe vomiting. However, mostly
oral NAC has bad odour and unpleasant test.
o Continuous IV infusion is recommended for acute ingestion, as follows:
➢ Loading dose: 150 mg/kg IV; mix in 200 mL of D5W and infuse over 1 hr.
➢ Dose 2: 50 mg/kg IV in 500 mL D5W over 4 hrs
➢ Dose 3: 100 mg/kg IV in 1000 mL D5W over 16 hrs.
o Intermittent iv infusion may be considered for late-presenting or chronic ingestion.
➢ A loading dose of 140 mg/kg iv (diluted in 500 mL D5W), infused over 1 hr.
➢ Maintenance doses of 70 mg/kg IV, given every 4 hours for at least 12 doses (dilute
each dose in 250 mL of D5W and infuse over a minimum of 1 hr.)
o The duration of IV NAC is for only 20 hrs.
✓ Once the standard treatment duration has elapsed, only discontinue therapy if the serum
acetaminophen level is below the limits of detection, liver transaminase levels are normal,
and the patient is asymptomatic. If there is evidence of hepatic toxicity, then NAC should be
continued until this has resolved.
✓ Treatment may be stopped 36 h after the last dose of acetaminophen if the liver enzymes
are normal.

✓ All patients requiring acetylcysteine therapy should be admitted to the hospital until the
completion of the therapy. In general, admission to a hospital bed is adequate unless the
co-ingestant is of concern, hepatotoxicity is severe, or the patient is suicidal, and 24-hour
direct observation cannot be arranged.
✓ Patients who are not at risk for developing acetaminophen-induced hepatotoxicity (e.g.,
acetaminophen concentration below the nomogram or unmeasurable acetaminophen
concentration with normal hepatic transaminase concentrations) should be observed in the
ED for 4-6 hours to exclude potentially toxic coingestants before disposition.

19.4.2. NSAIDs Overdose


✓ NSAIDs and are widely used for control of pain and inflammation.
✓ Overdose by most NSAID usually produces only mild GI upset.
✓ CNS, hemodynamic, pulmonary, and hepatic dysfunction also occur with some NSAD’s.
✓ Significant symptoms occur after ingestion of more than 5-10 times the usual therapeutic
dose.

Clinical presentation
✓ Generally, Asymptomatic or have mild GI upset (nausea, vomiting, abdominal pain, and
sometimes hematemesis).
✓ Occasionally, patients exhibit drowsiness, lethargy, ataxia, nystagmus, tinnitus, and
disorientation.
✓ With the more toxic agents and with massive ibuprofen overdose, seizure, coma, renal failure,
and cardiorespiratory arrest may occur.
✓ Rarely Hepatic dysfunction, hypoprothrombinaemia, and metabolic acidosis.
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Investigation
✓ RBS
✓ U/A
✓ CBC
✓ Electrolytes
✓ BUN & creatinine
✓ liver transaminases
✓ PT, aPTT

Treatment
✓ Emergency and supportive measures:
o Maintain an open airway and assist ventilation if necessary
o Administer supplemental oxygen.
o Treat seizure, coma, and hypotension if they occur
o Antacids may be used for mild GI upset.
o Replace fluid losses with IV crystalloid solutions.
✓ Decontamination:
o Prehospital: consider activated charcoal if available and the patient is alert
o Hospital: consider activated charcoal. Gastric emptying is not necessary for most
ingestion if activated charcoal can be given promptly. Consider gastric lavage for massive
overdoses
✓ There is no antidote. Vitamin K may be used for patients with elevated PT caused by
hypoprothrombinaemia.

19.4.3. Cardiac glycosides (digoxin and digitoxin) overdose


✓ Cardiac glycosides are used therapeutically as digoxin and digitoxin.
✓ Toxic dose; Healthy adults may develop symptoms after ingestions of more than 2-3 mg of
digoxin but rarely develop severe toxicity with ingestions less than 5mg.Toxic effects in
children are likely with ingestions of more than 0.1mg/kg of digoxin and ingestions of 4 mg
can be fatal.

Clinical presentation
✓ Intoxication may occur after acute accidental or suicidal ingestion or with chronic therapy.
✓ Signs and symptoms depend on chronicity of the intoxication.
✓ With acute over dose:
o vomiting, hyperkalaemia, sinus bradycardia, sinoatrial arrest, and 2nd or 3rd degree AV
block are common.
o Ventricular tachycardia or fibrillation may occur.
o Hyperkalaemia is a marker of severe acute toxicity and serum potassium is the best
predictor of cardiac glycoside toxicity after an acute overdose.
✓ With chronic intoxication:
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o visual disturbances, weakness, sinus bradycardia, atrial fibrillation with slowed ventricular

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response rate or junctional escape rhythm, and ventricular arrhythmias (ventricular


bigeminy or trigeminy, ventricular tachycardia, bidirectional tachycardia, and ventricular
fibrillation) are common.
o Accelerated junctional tachycardia and paroxysmal atrial tachycardia with block are
frequently seen.
o Hypokalemia and hypomagnesemia from chronic diuretic use may be evident and appear
to worsen the tachyarrhythmias.

Complications
✓ Hypoxic seizure
✓ Encephalopathy
✓ Ischemic stroke
✓ MI
✓ ATN

Investigation
✓ Electrolytes → Serum potassium levels higher than 5.5 meq/L are associated with severe
poisoning, serum magnesium
✓ BUN & creatinine
✓ ECG monitoring
✓ Ix based on cxn (if there)
✓ Specific levels: stat serum digoxin or digitoxin levels are recommended, although they may
not correlate accurately with severity of intoxication. Therapeutic levels of digoxin are 0.5-2
ng/mL; of digitoxin, 10-30 ng/mL.

Treatment
✓ Emergency and supportive measures:
o ABC of life
o Monitor the patient closely for at least 12–24 h after significant ingestion because of
delayed tissue distribution.
✓ Decontamination:
o Prehospital: activated charcoal, if there is no contraindication
o Hospital: activated charcoal. Gastric emptying is not necessary if activated charcoal can
be given promptly. Repeat-dose activated charcoal maybe useful for Digitoxin toxicity and
in patients with severe renal insufficiency, in which clearance of digoxin is markedly
diminished.

✓ Treat hyperkalemia (refer under short case of Nitsbin. click here →



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✓ 14.2.2 Hyperkalemia)
✓ Treat bradycardia or heart block:
o Atropine is usually the drug of choice in this circumstance.
➢ For adults, give 0.5-1mg iv. For children, give 0.02 mg/kg iv up to a maximum of
0.5 mg and 1 mg in adolescents. Repeat as needed.
➢ Note that 3 mg is a fully vagolytic dose in adults. If response is not achieved at 3
mg, the patient is unlikely to benefit from further treatment unless bradycardia is
caused by excessive cholinergic effects (e.g., carbamate or organophosphate
overdose).
o A temporary pacemaker may be needed for persistent symptomatic bradycardia.
✓ Treat Ventricular tachyarrhythmias:
o May respond to lidocaine.
➢ Administer 1-1.5 mg/kg (usual adult dose 50-100 mg; children, 1 mg/kg) iv bolus at
a rate of 25-50 mg/min, followed by infusion of 1-4 mg/min (20-50 mcg/kg/min) to
maintain serum concentrations of 1.5-5 mg/L.
➢ If significant ectopy persists after the initial bolus, repeat doses of 0.5 mg/kg iv can
be given if needed at 10-min intervals (to a maximum 300 mg or 3 mg/kg total
dose; children may be given repeat 1 mg/kg doses every 5-10 min to a maximum of
5 mg/kg).
o In patients with congestive heart failure or liver disease, use half the recommended
maintenance infusion dose of lidocaine or use phenytoin (a loading dose of 15–20
mg/kg iv slowly at a rate not to exceed 50-100 mg/min or 1 mg/kg/min in children) or to
correction of low potassium or magnesium.
o Avoid quinidine, procainamide, and bretylium.
✓ Specific drugs and antidotes:
o Digi bind (Fab fragments of digoxin-specific antibodies)
➢ They are indicated for
• (Acute) significant poisoning (e.g., severe hyperkalaemia i.e. K>6.0mEq/L,
symptomatic arrhythmias not responsive to drugs described above)
• Chronic toxicity with any life-threatening dysrhythmia
• Possibly for prophylactic treatment in a massive oral overdose with high
serum levels.
➢ Digi bind rapidly binds to digoxin and, to a lesser extent, digitoxin and other cardiac
glycosides.
➢ The inactive complex that is formed is rapidly excreted in the urine.
➢ A full neutralizing dose of digoxin-Fab is based on an estimation of the total-body
load of digoxin, which can be calculated from either the dose ingested or a steady-
state serum digoxin level.
➢ In an acute poisoning, each vial of digoxin-Fab reverses approximately 0.5 milligram
of ingested digoxin.
➢ In hemodynamically stable patients, half the calculated full neutralizing
dose is infused, and the other half is given if an adequate clinical response is not
seen in 1 to 2 h. 1375
➢ A total of 200 to 480 mg of digoxin-Fab (5 to 12 vials) is required to effectively treat
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severely digoxin-toxic patients.


➢ When the ingested dose is unknown and serum level is unavailable, 10 vials are
recommended as initial treatment in life-threatening situations.
➢ Digoxin-Fab are administered iv through a 0.22-mm filter over 30 min, except in
cardiac arrest, when the dose is given as an IV bolus.

19.4.4. Opiates and opioids overdose


✓ This group includes naturally occurring opiates (e.g., morphine, heroin, codeine, and
hydrocodone) as well as synthetic opiate analogues (e.g., fentanyl, pethidine/ meperidine, and
methadone.
✓ Dextromethorphan is an opioid derivative with potent antitussive but no analgesic or addictive
properties.
✓ Tramadol is a newer analgesic that is unrelated chemically to the opiates but acts on mu (μ)
opioid receptors.
✓ Some newer fentanyl derivatives have potency for toxicity up to 2000 times that of morphine.

Clinical presentation
✓ With mild or moderate overdose:
o Lethargy is common.
o The pupils are usually small, often “pinpoint” size.
o Hypotension and bradycardia
o Diminished bowel sounds
o The muscles are usually flaccid.
✓ With higher doses:
o In general, opioids have effect in the CNS, causing coma (sedation) and respiratory
depression.
o Death results from respiratory failure, usually because of apnea or pulmonary aspiration
of gastric contents.
o In addition, acute noncardiogenic pulmonary edema may occur by unknown mechanisms,
often after resuscitation and administration of the opiate antagonist naloxone.
✓ Seizures occur occasionally with certain compounds
✓ Cardiotoxicity•
✓ Opioid withdrawal syndrome can cause anxiety, piloerection (goose bumps), abdominal
cramps, diarrhoea, and insomnia.
✓ Typical manifestations of opiate intoxication are pinpoint pupils, respiratory and CNS
depression, and the patient quickly awakens after administration of naloxone.
✓ Signs of iv drug abuse (e.g., needle track marks) may be present.

Investigation 1376
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✓ RBS
✓ Electrolytes
✓ CXR
✓ Arterial blood gases or oximetry

Treatment
✓ Emergency and supportive measures:
o ABC of life
o Administer supplemental oxygen.
o Treat coma, seizure, hypotension and non-cardiogenic pulmonary edema if they occur.
✓ Decontamination:
o Prehospital:
▪ Provide general supportive care.
▪ Activated charcoal is generally not indicated because of the risk of aspiration.
▪ Do not induce vomiting because of the potential for developing lethargy and
coma.
o Hospital:
▪ Administer activated charcoal if a patient presents soon after ingestion and is
not manifesting signs of toxicity. It is not recommended in patients showing
signs of toxicity because of the risk of aspiration.
▪ Gastric emptying is not necessary if activated charcoal can be given promptly.

✓ Specific drugs and antidotes:


o Naloxone, 0.4–2 mg, IV, repeat doses every 2–3 min, if there is no response, up to a
total dose of 10–20 mg
▪ It is a specific opioid antagonist
▪ Large doses may be given safely.
▪ As little as 0.2–0.4 mg is usually effective for heroin overdose.
▪ Caution: the duration of effect of naloxone (1–2 h) is shorter than that of many
opioids. Therefore, do not release the patient who has awakened after naloxone
treatment until at least 3–4 h have passed since the last dose of naloxone.
▪ In general, if naloxone was required to reverse opioid-induced coma, it is safer
to admit the patient for at least 6– 12 h of observation.
o Sodium bicarbonate may be effective for QRS interval prolongation or hypotension
associated with propoxyphene poisoning.

19.4.5. Phenothiazines and other antipsychotic drug overdose

✓ Phenothiazines, butyrophenones, and other related drugs are widely used to treat psychosis
and agitated depression.
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✓ In addition, some of these drugs (e.g., prochlorperazine, promethazine, and triperidol) are
used as antiemetic agents.
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✓ Suicidal overdoses are common, but because of the high toxic-therapeutic ratio, acute
overdose seldom results in death.

Clinical presentation
✓ Major toxicity is manifested in the cardiovascular and CNS.
o CVS toxicity: tachycardia, orthostatic hypotension.
o CNS toxicity: CNS depression, small pupils, Extrapyramidal dystonic reactions, disturbed,
Temperature regulation resulting in poikilothermia
✓ Mild intoxication:
o Causes sedation, small pupils, and orthostatic hypotension.
o Anticholinergic manifestations include dry mouth, absence of sweating, tachycardia, and
urinary retention. Paradoxically, clozapine causes hypersalivation through an unknown
mechanism.
✓ Severe intoxication:
o May cause coma, seizures, and respiratory arrest.
o Hypothermia or hyperthermia may occur.
o Clozapine can cause a prolonged confusion state and rarely cardiac toxicity.
✓ Extrapyramidal dystonic side effects of therapeutic doses include torticollis, jaw muscle spasm,
oculogyric crisis, rigidity, bradykinesia, and pill-rolling tremor.
✓ Patients on chronic antipsychotic medication may develop the neuroleptic malignant
syndrome characterized by rigidity, hyperthermia, sweating, lactic acidosis, and
rhabdomyolysis.
✓ Clozapine use has been associated with agranulocytosis

Investigation
✓ RBS
✓ Electrolytes
✓ BUN &creatinine
✓ CPK
✓ Arterial blood gases or oximetry
✓ Abdominal x-ray → to look for radiopaque pills, Phenothiazines are occasionally visible on
plain abdominal x-rays
✓ Chest x-ray
✓ ECG → usually shows QT interval prolongation and occasionally QRS prolongation
(particularly with thioridazine and Risperidone).

Treatment
✓ Emergency and supportive measures:
o ABC life and supplemental oxygen.
o Treat coma, seizures, hypotension, and hyperthermia if they occur.
o Monitor vital signs and ECG for at least 6 h and admit the patient for at least 24 h if
there are signs of significant intoxication.
✓ Decontamination:
o
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Prehospital: general supportive measures. Administer activated charcoal if there is no
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contra indication. Do not induce vomiting.


o Hospital: consider activated charcoal. Gastric emptying is not necessary if activated
charcoal can be given promptly
✓ There is no specific antidote.
✓ Dystonic reactions: give diphenhydramine, 0.5–1 mg/kg IV/IM or benztropine.
✓ QRS interval prolongation: treat quinidine-like cardiotoxic effects with bicarbonate, 1-2 mEq/kg
IV.

19.4.6. Benzodiazepines (BDZ) Toxicity


✓ BDZ’s to varying degrees, have in common 6 major pharmacologic effects:
Sedative, hypnotic, anxiolytic, amnestic, anticonvulsant and muscle relaxant.
✓ BDZ’s are commonly used for the short-term treatment of anxiety, insomnia, seizures, and
alcohol and sedative-hypnotic withdrawal.
✓ Examples of BDZ’s include; diazepam, lorazepam, midazolam, alprazolam, temazepam,
triazolam, clonazepam…
✓ Isolated benzodiazepine overdose has no significant morbidity and mortality. Most serious
toxicity will occur in the setting of co-ingestion of other agents or with parenteral
administration.
✓ Death due solely to benzodiazepine overdose is rare in otherwise healthy individuals.
✓ Deaths in seemingly isolated overdoses are more likely with short-acting derivatives such as
alprazolam, temazepam, and triazolam.

Clinical Features
✓ nonspecific
✓ The predominant manifestations are neurologic and are characterized by somnolence,
dizziness, slurred speech, confusion, ataxia, incoordination, and general impairment of
intellectual function.
✓ Coma, particularly if prolonged, is atypical and should prompt suspicion of intoxication with
other agents or a non-toxin–related medical condition.
✓ In the elderly, infants and children, protein-deficient persons, and those with hepatic disease,
the neurologic effects of benzodiazepines may be prolonged or enhanced.
✓ Paradoxical reactions, including excitement, anxiety, aggression, hostile behavior, rage, and
delirium, are quite uncommon.
✓ Other effects that have unclear aetiologies include headache, nausea, vomiting, chest pain,
joint pain, diarrhea, and incontinence.
✓ Some benzodiazepines may cause short-term anterograde amnesia.
✓ Uncommonly, respiratory depression and hypotension may occur
✓ Extrapyramidal reactions.
✓ Various allergic, hepatotoxic, and hematologic reactions are infrequent.
✓ In general, benzodiazepines have no long-term organ-system toxicity other than that which
can be ascribed to indirect effects from neurologic or cardiorespiratory depression.
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Investigations
✓ RBS →.to rule out hypoglycemia as the cause of chane in mentation.
✓ CBC
✓ RFT
✓ LFT with Liver enzymes
✓ Pregnancy test in women of childbearing age
✓ ECG → to rule out conduction system poisoning by drugs that effect the QRS or QTc
interval
✓ Arterial blood gas analysis

Management
✓ Initial treatment
o ABC of life → Endotracheal intubation if needed. Oxygen, secure IV line, continuous
cardiac monitoring.
o Check RBS immediately
o Vast majority of benzodiazepine overdoses can be managed expectantly.
o Activated charcoal is generally not beneficial in overdose.
✓ Antidote → Flumazenil
o The initial adult dose of flumazenil is 0.2 mg (In children, 0.01 mg/kg, up to 0.2 mg), IV
over 30 seconds.
o A second dose of 0.3 mg may be given, followed by 0.5-mg doses at 1-minute intervals,
to a total of 3 mg.
o Most patients respond within 3 mg.
o Because the duration of action of flumazenil is short (0.7–1.3 hours), re sedation occurs
in up to 65% of patients and requires either re dosing or continuous infusion (0.25–1.0
mg/hr)
o Flumazenil is a nonspecific competitive antagonist of the benzodiazepine receptor, can
reverse benzodiazepine-induced sedation after general anesthesia, procedural sedation,
and overdose, but is not recommended for the reversal of benzodiazepine overdose in
the ED.
o Seizures and cardiac dysrhythmias can occur with flumazenil administration, and fatal

Flumazenil
Indication Contraindications
Absolute Relative
✓ Isolated ✓ Known or suspected co-ingestant that lowers seizure ✓ Chronic
benzodiazepine threshold benzodiazepine user,
overdose in no ✓ TCA, cocaine, lithium, methylxanthines, isoniazid, not taking for control
habituated user propoxyphene, monoamine oxidase inhibitors, of life-threatening
(e.g., accidental bupropion, diphenhydramine, carbamazepine, condition
pediatric cyclosporine, chloral hydrate ✓ Known seizure
exposure)
✓ Reversal of
conscious
✓ Patient taking benzodiazepine for control of a
potentially life-threatening condition (e.g., seizures)
✓ Concurrent sedative-hypnotic withdrawal
with
benzodiazepines
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sedation ✓ Seizure activity or myoclonus ✓ Head injury


✓ Hypersensitivity to flumazenil or benzodiazepines ✓ Panic attacks
✓ Patient with neuromuscular blockade ✓ Chronic alcoholism

✓ Disposition
o Patients remaining asymptomatic after 4 to 6 hours of ED observation may be medically
cleared.
o For cases of deliberate overdose, appropriate psychiatric consultation should be obtained
o Indications for observation or hospital admission include significant alterations in mental
status, respiratory depression, and hypotension.
o If mental status depression persists or is profound, other agents or conditions must be
considered.

19.4.7. Anticonvulsants poisoning

19.4.7.1 Phenytoin and fos phenytoin poisoning


✓ Phenytoin is a primary anticonvulsant for partial and generalized tonic clonic seizures.
✓ Serious complications are extremely rare after intentional phenytoin overdose if supportive
care is provided.
✓ Most phenytoin-related deaths have been caused by rapid IV administration or hypersensitivity
reactions.
✓ Phenytoin is extensively (about 90%) bound to plasma proteins, especially albumin.
✓ The free, unbound form is responsible for the drug’s clinical effect and toxicity.
✓ The unbound fraction of the drug is greater in neonates, the elderly, pregnant women,
renal failure, hypoalbuminemia (cirrhosis, nephrosis, malnutrition, burns, trauma), and
hyperbilirubinemia.
✓ Drugs that displace phenytoin from binding sites (salicylate, valproate, phenylbutazone,
tolbutamide, and sulfisoxazole) also result in an increased unbound fraction.
✓ Fosphenytoin (a disodium phosphate ester of phenytoin) is a prodrug that is converted to
phenytoin by phosphatases in the body

Clinical manifestations
✓ CNS Toxicity
o Nystagmus → The initial sign of toxicity, which is seen first on forced lateral gaze and
later becomes spontaneous. Vertical, bidirectional, or alternating nystagmus may occur
with severe intoxication. But, absence of nystagmus does not exclude severe phenytoin
toxicity.
o lethargy, ataxic gait, and dysarthria.
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o confusion, coma, and even apnea in a large overdose.


o complete ophthalmoplegia and loss of corneal reflexes.
o Paradoxically, very high levels of phenytoin may be associated with seizures, although
this is a rare occurrence, and such phenytoin-induced seizures are usually brief and
generalized and almost always are preceded by other signs of toxicity, especially in acute
overdose.
o Dystonias and movement disorders, such as opisthotonos and choreoathetosis.
o Hyperactive deep tendon reflexes, clonus, and extensor toe responses also may be
elicited.
o Chronic neurologic toxicity includes peripheral neuropathy and cerebellar degeneration
with ataxia.

✓ CVS Toxicity
o CVS CXN have been almost entirely limited to cases of IV administration, or in rare
cases of chronic oral toxicity.
o CVS toxicity is more common in the elderly, those with underlying cardiac
disease, and the critically ill patients.
o hypotension
o bradycardia
✓ Vascular and Soft Tissue Toxicity
o IM injection of phenytoin may result in hematoma, sterile abscess, and myonecrosis at
the injection site.
o IV extravasation may produce skin and soft tissue necrosis, compartment syndrome, and
limb gangrene.
o Delayed bluish discoloration of the affected extremity (“purple glove syndrome”) followed
by erythema, edema, vesicles, bullae, and local tissue ischemia

✓ Hypersensitivity Reactions
o Hypersensitivity reactions usually occur within 1 to 6 weeks of beginning phenytoin
therapy and can present as a febrile illness with skin changes (erythema multiforme, toxic
epidermal necrolysis or Stevens-Johnson syndrome) and internal organ involvement
(hepatitis, rhabdomyolysis, acute interstitial pneumonitis, renal failure, LAP, leukopenia
and/or DIC).
o Patients with a history of previous hypersensitivity reactions should not receive phenytoin
✓ Miscellaneous Effects
o Gingival hyperplasia is relatively common and is associated with poor dental hygiene
gingivitis and dental plaques.

Investigation
✓ RBS - To r/o hypoglycemia as the cause of any alteration in mental status.
✓ CBC- may have leucocytosis, eosinophilia
✓ Elevated liver enzymes.
✓ Serum albumin level- hypoalbuminemia patients with a therapeutic or mildly elevated
phenytoin concentration may exhibit significant toxicity.
✓ Pregnancy test- should be done in women of childbearing age.
✓ Serum Phenytoin level- The therapeutic phenytoin serum level is 10 to 20 µg/mL which
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generally corresponds to a free phenytoin level of 1 to 2 µg/mL.


✓ ECG -reveals increased PR interval, widened QRS interval, and altered ST
segments and T waves, arrhythmias, ventricular tachycardia, primary ventricular fibrillation,
atrioventricular block, or sinus arrest with junctional or ventricular escape that may occur after
intravenous (or very rarely oral) exposure

Management
✓ ABC of life
o Endotracheal intubation if indicated
o Treat Hypotension with IV boluses of isotonic saline. Atropine, epinephrine, and dopamine
remain first line medical treatment for symptomatic brady dysrhythmias.
✓ Decontamination
o Activated charcoal (AC) may be useful in the setting of a recent ingestion.
o Multiple dose AC may remove some unbound phenytoin undergoing enterohepatic
circulation, even if the phenytoin was administered IV. It is not routinely use multiple
doses of activated charcoal.
✓ Seizures from phenytoin toxicity should be treated with benzodiazepines and barbiturates as
needed.
✓ There is no specific treatment or antidote for phenytoin toxicity
✓ Disposition and Follow-Up
o The decision to discharge or medically clear a patient for psychiatric evaluation should be
clinically, cannot be based on one serum level.
o After acute ingestions, serum level should be measured every few hours.
o Patients with serious complications after an oral ingestion (seizures, coma, altered mental
status, or significant ataxia) should be admitted for further evaluation and treatment.
o Those with only mild symptoms may be observed in the ED and discharged once their
levels of phenytoin are declining.
o Mental health or psychiatric evaluation should be obtained, as indicated, in cases of
intentional overdose.

19.4.7.2 Carbamazepine poisoning


✓ Carbamazepine is a primary anticonvulsant used in the treatment of partial and tonic clonic
seizures. Other uses include trigeminal neuralgia, chronic pain disorders, manic
disorder, and bipolar disorder.

Clinical manifestations
✓ Neurologic and possibly some CVS effects characterize acute carbamazepine toxicity.
✓ CNS effects;
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o The initial neurologic disturbances include nystagmus, ataxia, and dysarthria. In patients
with large overdoses, fluctuations in level of consciousness and coma occur.
o Carbamazepine toxicity may cause seizures in both in epileptic and nonepileptic patients
by unknown mechanism.
o Chronic carbamazepine overdose can result in headaches, diplopia, or ataxia.
Idiosyncratic adverse events are common.
✓ Cardiovascular effects
o include sinus tachycardia, hypotension with myocardial depression, and cardiac conduction
abnormalities.
o These abnormalities can be delayed for as long as 20 hours and may occur with chronic
therapy but are not associated with life-threatening dysrhythmias or permanent sequelae.

Investigation
✓ RBS
✓ U/A
✓ CBC
✓ Liver enzymes → elevated in acute toxicity
✓ serum electrolyte → hyponatremia
✓ Pregnancy test- should be done in women of childbearing age.
✓ ECG
o Carbamazepine can cause QRS prolongation and arrhythmia
o Sinus tachycardia is the most frequently observed cardiac effect of carbamazepine
o Other effects include; bradycardia, AV block, premature ventricular contractions, ventricular
tachycardia, and junctional escape rhythms
✓ Serum carbamazepine level
o should be followed serially in an acute overdose.
o Serum concentrations may not peak for over 96 hours; levels should be obtained every
four to six hours until there is a definite downward trend and the patient is improving
clinically.
o Therapeutic concentrations of carbamazepine range from 4 to 12 µg/mL.
o Carbamazepine concentrations above 40 mg/mL correlate with an increased risk for
apnea, dystonia, hypotension, and coma

Management
✓ ABC of life
✓ Gastrointestinal decontamination
o Activated charcoal remains the most common method for acute carbamazepine poisoning
o Multidose activated charcoal may be used in cases of severe carbamazepine poisoning
✓ Extracorporeal elimination
o In patients with severe toxicity and multiorgan dysfunction, haemodialysis, hemoperfusion,
or hemodiafiltration is effective.
✓ QRS prolongation is treated with sodium bicarbonate. give boluses of 100 to 150 meq of
sodium bicarbonate IV for QRS intervals longer than 110 milliseconds, particularly in patients
with hypotension.
✓ Seizures caused by carbamazepine overdose should be treated with GABA agonists, such as
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benzodiazepines (eg, lorazepam). Propofol administered as a continuous infusion for the


sedation of intubated patients also functions as an effective anticonvulsant. There is no role
for phenytoin in the management of drug-induced seizures.
✓ ECG monitoring may be necessary in some patients
✓ Patients can be medically cleared from the ED if at least two carbamazepine measurements
obtained a few hours apart show decreasing levels (preferably below 15 µg/mL) and the
patient is awake, ambulatory, and free of cardiac conduction abnormalities.

19.4.7.3 Valproate (valproic acid/VPA/) poisoning


✓ Valproate (or valproic acid) is used to treat tonic-clonic seizures, absence seizures, partial
complex seizures, and post-traumatic epilepsy.
✓ Valproate is also used in migraine headache prophylaxis, to control manic episodes in bipolar
disorder, and to treat neuropathic pain.

Clinical features
✓ After acute toxicity, the most frequent sign is CNS depression, ranging from drowsiness to
coma.
✓ Other findings include respiratory depression, hypotension, hypoglycaemia, and electrolyte
disturbances that may persist for days.
✓ Anion gap metabolic acidosis following overdose is a poor prognostic sign.
✓ Bone marrow suppression occurs 3–5 days following acute massive overdoses of VPA and
is characterized by pancytopenia. These hematopoietic disturbances usually resolve
spontaneously within a few days.
✓ Hepatotoxicity → Valproate-induced hepatotoxicity may be either intrinsic and benign
(reversible, reproducible, and dose dependent) or idiosyncratic and fatal (unpredictable, not
dose dependent, with a long latent period).
✓ Pancreatitis may occur, and thrombocytopenia may be clinically significant and severe.
✓ Cerebral edema has been seen in acute overdose.

Investigations
✓ RBS → hypoglycaemia as cxn of toxicity or to rule out hypoglycaemia as the cause of any
alteration in mental status
✓ U/A-Valproate is eliminated partly as ketone bodies and may cause a positive test result for
ketones in the urine or blood.
✓ Urine HCG -in women of childbearing age
✓ CBC- as a baseline and to see complication of VPA toxicity (Pancytopenia, thrombocytopenia)
✓ Serum electrolyte-hypernatremia, hypocalcaemia, hypophosphatemia, and anion gap metabolic
acidosis can be complication of valproate poisoning
✓ LFT and Enzyme tests- To see hepatotoxicity (elevated serum levels of aminotransferases,
ammonia, and lactate)
✓ ECG- to rule out conduction system impairment by drugs that prolong the QRS or QTc
intervals
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✓ Lipase and amylase- To assess Acute pancreatitis


✓ Serum ammonia level → Hyperammonaemia in the absence of liver failure during long-term
therapy.
✓ Arterial blood gas analysis- To See anion gab metabolic acidosis and treat accordingly
✓ Serum acetaminophen and Salicylates level-to rule out these common congestions
✓ Serum valproic acid concentration
o Therapeutic valproate concentrations are 50 to 100 µg/mL.
o Although serum concentration does not correlate well with either seizure control or
toxicity, adverse side effects increase as concentrations rise above 150 µg /mL, and
coma may occur with levels above 800 µg /mL.
o A consistent analytic methodology should be used when monitoring treatment.

Treatment
✓ Single-dose activated charcoal alone is sufficient for the vast majority of patients with a
valproate overdose.
✓ Consider multidose activated charcoal and/or whole-bowel irrigation after ingestion of
enteric coated, delayed-release preparations to prevent the ongoing absorption that may occur
from delayed capsule or tablet dissolution.
✓ Because of delayed peak serum levels after an overdose, serial concentrations should be
measured.
✓ high-dose naloxone to reverse valproate-induced neurologic depression, But naloxone
is unlikely to be helpful in the management of a comatose patient after valproate overdose.
✓ Hemoperfusion and hemodiafiltration have been used to treat severe valproate overdose.
✓ Disposition and follow up
o Patients with signs or symptoms (eg, somnolence) of severe VPA poisoning are admitted
to an ICU.
o In addition, adult patients who ingest > 200 mg/kg of VPA and/or have plasma
concentrations > 180 µg/mL (1260 µmol/L) usually develop some degree of CNS
depression and warrant admission to a closely monitored setting.
o Asymptomatic patients who ingest immediate-release preparations should be observed
closely for 6 hours.
o If the VPA level is low and the patient remains asymptomatic, further clinical deterioration
is highly unlikely.
o Patients who ingest sustained-release preparations should be observed for at least 12
hours.

19.4.8. Barbiturates (Commonly phenobarbitone/PB/)


✓ Barbiturates are from the group of ‘sedative – hypnotics’ that lower excitement & induce
sleep.
✓ Barbiturates are addictive, producing physical dependence and a withdrawal syndrome that
can be life-threatening.

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✓ While tolerance to the mood-altering effects of barbiturates develops rapidly with repeated
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increases with continued use.


✓ The main action of barbiturates is to depress activity in the nervous and musculoskeletal
systems.
✓ Barbiturates act directly on the medulla to produce respiratory depression.

Clinical features

☛ Mild barbiturate toxicity mimics ethanol intoxication, presenting with drowsiness, slurred
speech, ataxia, unsteady gait, nystagmus, emotional liability, and impaired cognition.
☛ In severe acute intoxication, CNS depression progresses from stupor to deep coma and
respiratory arrest.
☛ The life threat of severe barbiturate toxicity is respiratory depression
☛ A characteristic of a barbiturate overdose is the persistence of the pupillary light reflex even
with stage IV coma. Although pupils are usually normal or small and reactive, concomitant
hypoxia can cause pupils to be fixed and dilated.
☛ Corneal and gag reflexes may be diminished or absent
☛ muscle tone flaccid, and DTR diminished or absent.
☛ Flexor (decorticate) and extensor (decerebrate) posturing can occur in patients comatose.
☛ These neurologic signs are variable and do not always correlate with severity of intoxication
or depth of coma.
☛ A fluctuating level of consciousness is commonly seen.
☛ Bullous skin lesions often occur over the hands, buttocks and knees.
☛ Barbiturate overdose has been associated with non-cardiogenic pulmonary edema.
☛ Other Common complications include hypoglycaemia (perhaps due to starvation), aspiration
pneumonia, and acute lung injury.
☛ Most common vital sign abnormalities are:
– Hypothermia
– Respiratory depression
– Hypotension

Investigations

Routine lab. Investigations


o RBS
o CBC
o RFT, LFT, serum electrolyte
o Arterial blood gas (if indicated)
Imaging
o CXR→ can detect noncardiogenic pulmonary edema or pneumonia.
o CT of the head → should be obtained in comatose patients with evidence of trauma,
focal neurologic signs, papilledema, or uncertain diagnosis
EEG → Since the electroencephalogram may be silent as a result of barbiturate
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therapeutic levels or greater.


Toxicology screen
☛ Barbiturate serum levels:
o Useful for the diagnosis of a comatose patient; however, acute treatment decisions
should be
clinically based.
o The therapeutic level of phenobarbital is 15 to 40 μg/mL (65–172 μmol/L).
o A serum level > 50 μg/mL can be associated with coma, especially in a patient who is
not a
chronic user. Levels greater than 80 μg/mL are potentially fatal.

Treatment

1. ABCDE Assessment and Initial Stabilization •

☛ Mechanical ventilation and intubation in severe overdose before GI decontamination.


☛ Volume expansion, by rapid infusion of 1-2 L of isotonic fluid, is the mainstay of circulatory
support in the absence of cardiac failure. If fluid resuscitation fails to correct hypotension,
vasopressors such as dopamine and norepinephrine should be initiated.
☛ Check hypoglycaemia and treat
☛ Hypothermia between 30°C (86°F) and 36°C (96.8°F) is common and should be treated with
rewarming measures.

2. Decontamination
☛ With very large overdoses, antecedent gastric lavage may be considered.
☛ A single dose of activated charcoal should be given to cooperative, clinically stable patients
who present with in 1 hour of acute oral overdose. For patients who have a compromised
airway, endotracheal intubation is advised prior to giving charcoal
☛ Multi-dose activated charcoal is consider if a patient has ingested a life-threatening amount of
phenobarbital.
☛ monitor the airway is to decrease the risk of aspiration or bowel obstruction.

3. Urinary Alkalinization → It is not considered a first-line treatment for phenobarbital poisoning


and it is not effective for shorter-acting barbiturates.

4. Extracorporeal Elimination
☛ Haemodialysis, hemoperfusion, and hemodiafiltration have all been used to enhance
elimination of phenobarbital; however, they are reserved for patients who are deteriorating
despite aggressive supportive care.
☛ These modalities are not useful for poisoning from barbiturates other than phenobarbital.
☛ Exchange transfusion has also been reported useful in neonatal phenobarbital toxicity 1388
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Disposition and Follow-Up


☛ Mild to moderate barbiturate intoxication responds well to general supportive care, including a
single dose of activated charcoal, if appropriate.
☛ Improvement in neurologic status and vital signs over 6 to 8 hours signals eventual patient
discharge or transfer.
☛ When indicated, assessment by mental health services should be performed or arranged.
☛ For phenobarbital, a long-acting agent, serial serum levels should be obtained during the
initial 6 hours after an overdose before concluding the patient can be safely discharged or
transferred.
☛ Evidence of toxicity after 6 hours will require hospital admission, and patients with severe
toxicity should go to the intensive care unit.

19.4.9. TCA (Tricyclic antidepressant) Poisoning

✓ TCA consists of: amitriptyline, clomipramine, desipramine, imipramine, amoxapine and


maprotiline.
✓ Life-threatening ingestion at >10mg/kg, and fatalities at >1gm for adults (therapeutic dose
5-10mg/kg/day).
✓ Prolonged GI absorption due to anticholinergic effects.

Clinical features:

✓ Mild to moderate overdose/ toxicity, anti-muscarinic effect predominates and presentation


includes:
o Central effect: agitation, confusion, hallucination, seizure, ataxia, drowsiness, sedation,
coma
o Peripheral: dry skin and mucosa, mydriasis, tachycardia, mild hypertension, hyperthermia,
Urinary retention, ileus, tremor, myoclonus, hyperreflexia
✓ Severe toxicity: usually occurs within 6 hours if ingestion, consist of: Coma, cardiac
conduction delays, supraventricular and ventricular tachycardia, hypotension, Respiratory
depression, seizure.
✓ In summary TCA poisoning may produce any of the three major toxic syndromes:
anticholinergic effects, cardiovascular effects and seizure disorder.
✓ Secondary complications include, Aspiration pneumonia, pulmonary edema, anoxic
encephalopathy, hyperthermia, rhabdomyolysis can contribute to morbidity and mortality.
✓ Death from TCA overdose may result from ventricular fibrillation, intractable cardiac shock, or
status epileptics and from secondary complications.

ECG Features

✓ The classic ECG with TCA toxicity shows


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o sinus tachycardia, right axis deviation, and prolongation of the PR, QRS, and QT
intervals
o less commonly aBrugada pattern (incomplete RBBB with ST elevation in V1-3 leads) and
various block type.
o ECG abnormalities develop within 6 hours of ingestion and typically resolve over 36 to
48 hours.
✓ The following signs suggest cardio toxicity:
o Prolongation of the QRS >100 msec
o Abnormal morphology of the QRS (eg, deep, slurred S wave in leads I and AVL)
o Abnormal size and ratio of the R and S waves in lead AVR: R wave in AVR >3 mm; R
to S ratio in AVR >0.7

Management of TCA overdoses

ABCs and supportive management


✓ Secure double IV line
✓ Monitored setting, full set of vital signs,
✓ serial ECG
✓ Airway equipment available
✓ Intubate if low LOC or respiratory depression
✓ Hyperventilate to pH of 7.50-7.55
✓ Provide high-flow oxygen
✓ If hypotensive (shock)
o give NS, IV boluses in increments of 10 mL/kg to a maximum of 30 mL/kg.
o Hypotension that does not improve with appropriate fluid challenges should
be treated with sodium bicarbonate (regardless of QRS complex duration).
o Vasopressors (Norepinephrine and epinephrine) should be used when
hypotension is unresponsive to fluids and sodium bicarbonate therapy
o Vasopressin can be tried if there is no response to norepinephrine or
epinephrine.
o Dopamine is less effective than norepinephrine
✓ Do NOT treat hypertension
✓ Urinary catheterization to prevent urinary retention, and a nasogastric tube may be
needed if ileus is present.
Universal antidotes → “TONG”, Thiamine, Oxygen, Naloxone (opioid antagonist), Glucose
GI Decontamination → After the ABC’s have been secured and If pt comes within 1hr of
ingestion but also later if severe toxicity
✓ Activated charcoal
✓ Gastric lavage (in intubated patient) → if ingested >20mg/Kg
✓ Don’t induce emesis
Treat seizures with:
• IV diazepam 5-10mg
• May use phenobarbital, propofol
• Avoid phenytoin (Na+-channel blocker)
Alkalinisation and Na loading for dysrhythmia by
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✓ Sodium bicarbonate → also Used to treat cardiac conduction abnormalities (the
above ECG features)
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✓ Hypertonic NACI (3%,7%)

Disposition
Patients with an alteration in mental status, hypotension, cardiac conduction abnormalities,
or seizures should be admitted to ICU.
Patients with mild symptoms, such as an isolated tachycardia without evidence of
conduction abnormalities (i.e., QRS <100 msec), could conceivably be admitted to a
monitored bed/ setting.
Asymptomatic patients who have no conduction abnormalities on ECG, may deteriorate
rapidly and should be monitored for at least 6 hours in an acute care setting can be
safely discharged or transferred to a psychiatric service for evaluation.
Hospitalized patients can be cleared medically after 24 hours if they are asymptomatic,
with a normal or baseline ECG, normal mental status, and resolution of all antimuscarinic
symptoms.

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Chapter 20; Miscellaneous

20.1. Tetanus (መንጋጋ ቆልፍ)


Dr. Mulualem. G, Dr. Robel. D

➢ Tetanus is a toxin-mediated disease of the nervous system characterized by muscle spasms.


➢ Caused by Clostridium tetani: - anerobic spore-forming bacilli found in the soil
➢ Usually follows trauma.
➢ Four forms:
✓ Generalized (the most common)
✓ Local
✓ Cephalic
✓ Neonatal
➢ C. tetani does not grow in healthy tissues
➢ Factors that increase chance of tetanus disease are:
✓ Penetrating injuries
✓ Superinfection by other bacteria
✓ Devitalized tissue
✓ Foreign body presence
✓ Tissue ischemia
➢ Clinical situations that may also predispose for tetanus:
✓ Infected umbilical stump in neonates
✓ Septic abortion
✓ Unhygienic circumcision
✓ Dental infections
✓ Infected diabetic foot ulcers
➢ In 10% of tetanus patients site of entry is not identified

Clinical Features
➢ Incubation period:
✓ Ranges from a few days to a few weeks with an average of a week
✓ A short incubation period (time from injury to first symptom) of ≤4 days generally
indicates severe disease.
✓ The period between the first symptom and the development of muscular spasms is 1392
termed the period of onset. Shorter periods of onset, particularly <48hrs, are again
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associated with more severe forms of tetanus


✓ Shorter in neonatal tetanus and with injuries close to the CNS
➢ Recovery from tetanus takes 4-6 weeks
➢ Generalized tetanus
✓ The commonest form
✓ The most common and important clinical features include trismus (lockjaw) localized
or generalized muscular rigidity and spasm.
✓ Lockjaw (or trismus) the cardinal symptom is characterized by: intense, painful
spasms of the masseter muscles, and an inability to open the mouth
✓ Other symptoms: stiff neck, opisthotonos, risus sardonicus, board abdomen, apnea
during spasms, dysphagia, sweating, arrhythmia, fever, labile BP
✓ Consciousness is not impaired in tetanus patients
✓ The presence of arrhythmia, extreme oscillation in blood pressure, diaphoresis,
laryngeal spasm and urinary retention may suggest autonomic dysfunction.
➢ Local tetanus
✓ Rare
✓ Signs/ symptoms limited to one part of the body
✓ Difficult to diagnose early
✓ Less severe
✓ Often evolves to generalized form
➢ Cephalic tetanus
✓ Head and neck area
✓ Often evolves to generalized form
✓ Dysphagia, trismus, focal cranial neuropathies
✓ CN-VII is commonly affected, but others (CN – III, IV, VI and XII) may be affected
alone or in combination
➢ Neonatal tetanus
✓ Neonates of unimmunized or poorly immunized mothers
✓ Follows unclean management of the umbilical stump
✓ Intense cry, refusal to feed, poor sucking, difficulty opening mouth due to trismus,
facial muscle spasms, rigid body parts

Investigations

➢ Clinical, based on the history and examination findings.

Severity Scoring
➢ There are several severity scores used but the Ablett classification has been used most
commonly.

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Table; Ablett classification of severity of Tetanus


Grading Clinical features
I- Mild Mild to moderate trismus; general spasticity; no respiratory
embarrassment; no spasm; little or no dysphagia
II- Moderate Moderate trismus; well-marked rigidity; mild to moderate but short
spasms; moderate respiratory embarrasement with RR greater than 30;
mild dysphagia
III-Severe Severe trismus; generalized spasticity; reflex prolonged spasms;
increased RR greater than 40; apnoeic spells; severe dysphagia;
tachycardia greater than 120.
IV-Very Grade III and violent autonomic disturbances involving the
Severe cardiovascular system. Severe hypertension and tachycardia alternating
with relative hypotension and bradycardia, either of which may be
persistent.

Treatment

Non pharmacologic

➢ Admit patients to a quiet place, and in severe cases, to an ICU if possible for continuous
cardio-pulmonary monitoring.
➢ Wound care which includes thorough cleansing and debridement.
➢ Intubation or tracheostomy, and mechanical ventilation in severe cases.
➢ Adequate hydration and feeding should be given attention

Pharmacologic

➢ Patients with severe tetanus should be managed in the intensive care setting where
mechanical ventilator and appropriate medication are available. This may necessitate
referral of most patients to specialized centers.

A. Control of spasm

➢ Diazepam, 10 mg I.V. every 4 hourly


✓ the dose being titrated depending on the response.
✓ Large doses as much as 250mg d a i l y could be used.
✓ NB: Heavy sedation with higher doses of diazepam has a potential to cause
respiratory depression and should only be used while the patient is mechanically
ventilated.
PLUS
➢ Chlorpromazine, 25-50mg I.M. QID alternated with diazepam
PLUS
➢ Magnesium sulphate, loading dose of 40mg/kg IV over 30 min, followed by IV infusion of
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2g/h for patients over 45kg and 1.5g/h for patients 45kg or under.
✓ Magnesium is used in patients with severe tetanus for whom tracheostomy has been
done; it helps in reducing the need for other muscle spasm controlling drugs and
may reduce muscle spasms and well-studied in reducing autonomic instabilities)

B. Neuromuscular blockade

➢ Neuromuscular blocking agents are used when sedation alone is inadequate.


✓ Suxamethonium, 20-100mg I.V. depending on the effect with mechanical ventilation
may be employed in patients with severe laryngeal spasm
✓ Halting toxin production and neutralizing circulating toxins
✓ Wound debridement to eradicate spores and necrotic tissue is recommended for all
patients with tetanus. This avoids ideal conditions for germination.

C. Antimicrobial treatment

➢ Metronidazole, 500mg I.V/PO TID or QID for 7-10 days


✓ Has some benefit. In addition, antimicrobials will fail to eradicate C. tetani unless
adequate wound debridement is carried.
alternative
✓ Penicillin G 2 to 4 million units IV every 4 to 6 hours for 7 to 10 days.

Metronidazole reduces the requirement for muscle relaxants and sedatives than penicillin’s
and cephalosporins.

D. Neutralization of circulating (unbound) toxin

➢ Human Tetanus immunoglobulin (HTIG), 500 IU I.M. stat (at a different site to the vaccine)
✓ the use of passive immunization to neutralize unbound toxin (bound toxin is irreversible)
is considered as the standard care as it is associated with improved survival.
✓ Give immediately after the diagnosis, with part of the dose infiltrated around the wound.
➢ Intravenous immune globulin may be administered as an alternative if HTIG is not available.

E. Active immunization
➢ Tetanus Antitoxin (TAT) 10,000 IU IM. after a skin test:
✓ All patients with tetanus, particularly in those never immunized previously, full series of
active immunization with appropriate booster doses is recommended immediately upon
diagnosis, because tetanus infection do not confer immunity.
✓ Administer vaccines at a different site than tetanus immune globulin.
F. Control of Autonomic dysfunction
➢ Hypertension and supra-ventricular tachycardia can be treated with combined alpha and
Beta- blockers.
✓ Labetalol is widely used first line option.
✓ Beta blockers alone (e.g. propranolol had caused a sudden death) are not
recommended.
✓ Morphine (0.5-1.0mg/kg per hour) can also be used to control the sympathetic
hyperactivity.
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Table; summary of Drugs for Tetanus management


Drug name dose Comment
Control of spasm
Diazepam 10 mg I.V. should be given Be cautious with
every 4 hourly, the dose respiratory depression at
being titrated depending on high dose, if not
the response. mechanically ventilated.
Neuromuscular blockade
Suxamethonium 20-100mg I.V. May be employed in
patients with severe
laryngeal spasm.
Control of autonomic dysfunction
Magnesium sulphate Load 40mg/kg IV over 30 well-studied in reducing
min, then IV infusion of autonomic instabilities;
2g/h for > 45kg & 1.5g/h help to reduce spasms
for ≤45kg
Labetolol 0.25-1.0mg/min IV infusion Alpha and beta blocker,
avoid beta blockers alone
Morphine 0.5-1.0mg/kg per hour
Halting toxin production and neutralizing circulating toxins
Wound debridement to Initially and as necessary Halt bacteria germination
eradicate spores and and related toxin
necrotic tissue production
Human Tetanus 500 IU I.M. single dose Start immediately. Help
immunoglobulin (HTG) to neutralize unbound
circulating toxins
Tetanus Antitoxin (TAT) 10,000 IU IM. Start immediately. after a
skin test or history taking

Airway and other supportive measures

➢ If ICU services are not available, acute respiratory failure is a principal cause of death from
tetanus.
➢ In the absence of an ICU
✓ A separate ward or room should be designated for patients with tetanus, and
✓ Keep sensory stimuli to a minimum because loud noises, physical contact, and light can
trigger tetanic spasms. Eye shades and ear plugs can also be used to reduce stimuli.
✓ Nondepolarizing neuromuscular blockers (e.g. vecuronium and pancuronium) are not safe
in the absence of ventilatory support. Yet, benzodiazepines and baclofen can be used
with careful doses titration to avoid respiratory depression. Magnesium sulfate can be
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➢ Supportive care is the basic treatment for tetanus because the tetanus toxin once bound to
neurons cannot be displaced from the nervous system. Hence patients with severe cases will
remain immobile for a long (for weeks), most of them in mechanical ventilation. As a result,
they are predisposed to decubitus ulcers, nosocomial infections, thromboembolic disease,
tracheal stenosis, and gastrointestinal hemorrhage.
➢ Bed sore prevention measures are important
➢ Early nutritional support may be required, enteral feeding is preferred, to meet the increasing
energy demands of tetanus patients.
➢ Prophylactic acid blockers or sucralfate may prevent gastroesophageal hemorrhage from
stress ulcer.
➢ Thromboembolism prophylaxis with heparin, or low molecular weight heparin should be
administered early.
➢ Physical therapy should be started as soon as spasms have ceased, to avoid disability from
prolonged muscle wasting and contractures.

Prevention
➢ Appropriate tetanus prophylaxis (human tetanus immune globulin and/or vaccine (e.g. TT))
should be administered ASAP following a wound as well as up one to two weeks of injury
for previously vaccinated (not fully vaccinated or vaccinated before 5-10 years) and up to 21
days of injury for previously unvaccinated late care seekers.
➢ This is because the incubation period is quite variable; most cases occur within 8 days, but
the incubation period can be as short as 3 days or as long as 21 days.
➢ For previously unvaccinated or partially vaccinated a human tetanus immune globulin is
concurrently (with the vaccine) recommended unlike the full vaccinated individuals.
➢ Immunization of pregnant or childbearing age women reduces neonatal tetanus mortality by
more than 90 %.
➢ Improving hygiene during home births is also help to prevent neonatal tetanus.

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20.2. Leprosy (የስጋ ደዌ በሽታ ፣ ቁምጥና)


Dr. Asmare. W

Leprosy (Hansen’s disease)


➢ A Chronic, granulomatous infection and its sequelae caused by Mycobacterium leprae,
principally affecting the Skin & peripheral nerves.
✓ But also the Eyes, Testes, the mucosa of the upper respiratory tract, Lymph nodes,
small muscles & bones of face, hands, & feet are affected. (but capable of affecting any
tissue or organ.)
✓ Acute inflammatory episodes called leprosy reactions occur at any time during which
Nerve Damage occurs.
➢ The major disability is due to Nerve Damage to Autonomic, Sensory and Motor fibers of the
peripheral nerves of hands & feet.
➢ Blindness and facial disfigurement results from direct involvement of eyes, face by the bacilli
and/or secondary to cranial nerves.
➢ Prompt diagnosis and treatment helps to avoid most complications of leprosy.
➢ Leprosy can cause permanent, and progressive psychological, and physical impairment.
➢ serious social and economic consequences result from
✓ Distress, anxiety and functional difficulties during daily living.
✓ social ostracism due to leprosy stigma
✓ 4 - 5 million people are disabled by leprosy world wide.

Etiology
➢ In 1873 Gerhard Armauer Hansen – identified M. leprae.
➢ Earliest description - from India

Microbiology
➢ M. leprae → acid-fast bacillus .
➢ A member of the family Mycobacteriacae.
➢ straight or slightly curved rod-shaped organism.
➢ Multiplies very slowly → generation time 14 days.
➢ An obligate intracellular parasite.
➢ It grows best at 27ºC to 33ºC→ predilection for affecting cooler areas of the body
✓ the skin, nerve segments close to the skin, and the mucous membranes of
the upper respiratory tract ……..
➢ M. leprae has never been cultured in artificial media.
➢ Grows in armadillos extensively
➢ Armadillo and foot pad of mouse → core body temperature of 34ºC. ( M. leprae grows best
at 30-33ºC)
➢ It is a disease virtually confined to humans.
➢ Leprosy is found in wild armadillos in the south, central United States and in Chimpanzee,
Sooty Mangabey Monkeys, in Africa

Epidemiology of leprosy Ethiopia


➢ M ‫׃‬F 2:1 in case of lepromatous leprosy.
➢ Affects predominantly young, 15-44yrs of age.
➢ Long Incubation period
✓ Tuberculoid :2-5 years
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✓ Lepromatous :8-12 years (~30years)


➢ WHO’s goal of elimination is Prevalence of less than 1 case per 10,000 Population.
➢ In Ethiopia the average prevalence is 0.6 - 0.7
➢ Areas of higher prevalence have also been reported

Transmission
➢ uncertain.
➢ Nasal droplets from lepromatous patients. (believed to be the mode of transmission by most
authorities)
➢ skin-to-skin contact – not considered as an important route.
➢ Requirements for the spread of leprosy;Contagious patient (lepromatous patient),Susceptible
individual (genetic, poverty …)and Close or intimate contact.
➢ Contact with a tuberculoid case carries a very low risk.

Pathogenesis
➢ a little is known

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➢ A predominantly Th1 response is seen in tuberculoid leprosy patient → IL-2, IFN- γ & TNF-β
→ granuloma formation, mild form of the disease.

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➢ Th2 response is seen in lepromatous patient → IL-4, IL-5, IL-10 → suppress macrophage
activity and allow strong humoral response, unrestricted proliferation of M. leprae.

Classification of leprosy

➢ The Aim of Classification of Leprosy


✓ Guide the treatment.
✓ follow the disease progress and predict outcome
✓ Assess the likelihood of complications.
✓ Plan control measures.
✓ Aid for communication between experts.
✓ Research e.g. clinical trials.
1, WHO’s classification
2, Ridley-Jopling’s classification

WHO’s classification
➢ Based on the number of skin lesions present, number of peripheral nerves involved &
presence or absence of bacilli on smears.
➢ Paucibacillary disease
✓ one to five skin lesions and no bacilli on smear testing.
✓ if only one nerve is involved, & nerve biopsy smear is negative (in case of pure neural
leprosy)
➢ Multibacillary disease
✓ six or more skin lesions with or without bacilli
✓ Less than six skin lesions, which have a positive slit skin smear result.
✓ if ≥ 2 nerves are involved or if one or more nerve involved with positive smear (in case
of pure neural leprosy)

Ridley-Jopling’s classification.
➢ Used to differentiate types of leprosy.
➢ helps in determining prognosis.
➢ It is based on clinical picture, histology, sometimes bacillary load.
➢ The granulomatous spectrum of disease described by Ridley&Jopling;
✓ Polar tuberculoid (TT)
✓ Border line tuberculoid (BT)
✓ Mid borderline (borderline) (BB)
✓ Borderline lepromatous (BL)
✓ Lepromatous leprosy (LLp)
✓ Polar tuberculoid leprosy ( TT )
➢ Immunity is strong.
➢ Solitary plaque having annular configuration, both border is sharply marginated, indurated,
erythematous, scaly, hypo pigmented hypesthetic, anhidrotic.
➢ Size is often less than 10cm.

Borderline Tuberculoid leprosy (BT)


➢ Immunity is strong to restrain infection.
➢ Somewhat unstable (upgrade or downgrade).
✓ Primary lesions could be papules or plaques.
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✓ Plaques may have sharply marginated satellite papules.


✓ Lesions larger >10cm.
✓ Multiple, asymmetric lesions are common.
✓ Impaired sensation.
➢ Nerve trunk involvement, enlargement or palsies involving
✓ Commonly not more than two nerves.

Borderline leprosy (BB)


➢ represents mid-zone of the granulomatous spectrum.
➢ it is the most unstable form.
➢ patients quickly down grade or uprgrade
➢ annular lesion with sharply mariginated interior and poorly mariginated exterior marigns.
➢ Large plaque with islands of normal appearing skin.
➢ Patient are rarely seen due to the unstable nature of this form.
➢ Classic ‘Diamorphic’ lesion.

Borderline lepromatous (BL)

➢ Resistance
✓ Is too low to restrain bacillary proliferation but still sufficient to induce tissue destructive
inflammation (nerve damage) thus, patients with BL have the worst of both worlds.
➢ Highly variable in its clinical presentation.
➢ Diamorphic lesion can be seen in in 1/3rd of patients.
➢ Punched out lesions can also be seen
➢ Lesions range from solitary to wide spread.
➢ Poorly defined papules & nodules.
➢ Annular & plaque lesions are often asymmetric.
➢ Lepromatous like nodules are symmetric if numerous.
➢ Nerve trunk palsies have highest prevalence.

Lepromatous leprosy (LL)


➢ Lack of CMI → unrestricted proliferation & widely disseminated multiorgan disease.
➢ Poorly defined nodules are most common lesion (~2cm) with Symmetrical distribution.
➢ Diffuse dermal infiltration
➢ Thickening of ear lobes, widening of nasal root, fusiform swelling of digits, loss of lateral 1/3rd
eye brows (madarosis), leonine facies.

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CLINICAL MANIFESTATIONS AND DIAGNOSIS

➢ Leprosy should be considered in the setting of skin lesions that are chronic and not
responding to standard treatment for more common conditions or when
➢ sensory loss is observed within lesions or in extremities.
➢ Additional clues include presentation of cuts or burns in the absence of pain and travel
history including residence in endemic countries (foreign birth, military experience, etc).
➢ 90% history of numbness first→ sometimes years before the skin lesions appear
➢ Sensory loss: Temperature → light touch → pain → deep pressure.
➢ The skin lesions appear later during the course of the disease.
➢ Borderline patients may present in reaction with nerve pain, sudden palsy, multiple new skin
lesions, pain in the eye, or a systemic febrile illness.
➢ Patients commonly present with
✓ skin lesions
✓ weakness or numbness due to a peripheral nerve lesion
✓ a burn or ulcer in an an aesthetic hand or foot.
➢ Assess for physical signs in 3 general areas:
✓ For cutaneous lesions.
✓ Neuropathies.
✓ Eye damage.
➢ For cutaneous lesions
✓ Assess the number, distribution, morphology, symmetry of skin lesions.
✓ Always look at the face, ears, trunk, buttock and lateral aspect of the limbs for
cutaneous lesions.
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✓ A hypo pigmented macule/plaque with a raised border is often the first cutaneous lesion.

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✓ Lesions may or may not be hypo esthetic.


➢ Neuropathies
✓ Assess for areas of hypoesthesia (light touch, pinprick, temperature) & anhidrosis
especially of peripheral nerve trunks and cutaneous nerves.
✓ commonly affected nerves include posterior tibial nerve, ulnar, median, lateral popliteal,
and facial nerves. (assess for enlargement, tenderness, consistency, irregularities)
✓ sensory loss, motor loss, and autonomic loss should be assessed.
✓ Nerves commonly involved include
▪ the ulnar and median (claw hand)
▪ the common peroneal (foot drop)
▪ the posterior tibial (claw toes and plantar insensitivity)
▪ Facial, radial cutaneous,great auricular.
➢ Eye damage is most often seen with facial lesions.
✓ Lagophthalmos (inability to close the eye) due to involvement of facial nerve.
✓ a late finding in LL
▪ reduced corneal reflex→ leaving dry eyes and reduced blinking are due to
ophthalmic division of trigeminal nerve involvement. ( corneal ulceration, scarring,
blindness)
▪ Extraocular findings include madarosis , leonine facies..

Table: Case definitions in Leprosy

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Diagnosis
➢ the cardinal signs of leprosy
➢ The diagnosis of leprosy is primarily clinical.
➢ Diagnosis is based on one or more of 3 signs:
✓ Hypo pigmented or reddish patches with definite loss of sensation.
✓ Thickened peripheral nerves with loss of sensation & or weakness of muscles supplied.
✓ Acid-fast bacilli on skin smears or biopsy material.
➢ Lab… Slit skin smear
✓ Lesions and cooler areas of the skin, such as the fore head, earlobes, chin, elbows,
knees, buttock and trunk are preferred sites for smear.
✓ An incision 5 mm long and 3 mm deep is made and blade is turned at right angles to
cut, and to take fluid, and pulp from the dermis.
✓ M. leprae are detected by modified Zeihl-Nelson staining.
➢ Skin biopsy
✓ To assess the extent and type of infiltrate and involvement of dermal nerves, a full-
thickness skin biopsy should be taken from the most active margin of the most active
lesion, entirely within a lesion.
✓ Skin smears, in which a small incision is made (on the ears, elbows, and/or knees) to
collect a dermal fluid sample, are no longer widely used.

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✓ Mycobacterial culture should be performed on biopsies from skin lesions to exclude
cutaneous infections due to M. tuberculosis and nontuberculous mycobacteria.

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➢ Polymerase chain reaction


✓ PCR is available for detection of M. leprae DNA in tissue.
✓ PCR is more useful as an identification tool (eg, when clinical or histologic features are
inconclusive) than as a detection tool.
✓ In one study, PCR on biopsies from patients with lepromatous disease had sensitivity
and specificity of >90 percent and 100 percent; PCR on biopsies from patients with
tuberculoid disease had sensitivity and specificity of 34 and 80 percent, respectively.
✓ PCR is not commercially available but can be performed by the NHDP Center.

Management
Goals
➢ Bacteriological cure.
➢ Detect and treat reactions.
➢ Prevent nerve damage and disabilities.
➢ Treat complications of nerve damage.
➢ Rehabilitation
✓ Physical
✓ Mental and
✓ Social

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Multi drug therapy (MDT)


Table; MDT Regimen

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Reactional states
➢ Immunologically driven distinctive tissue destructive inflammatory processes that appear
suddenly in any form of leprosy.
➢ Precipitating factors
✓ MDT, Pregnancy, Inter current infections, BCG etc
➢ Usually occur as complications during treatment but they may occur before treatment or after
➢ Treatment.
✓ Two types of reactional states are known;
▪ Type-1 (Reversal).
▪ Type-2 (Erythema nodosum leprosum, ENL).

Management of Type I (RR)


➢ General principle
✓ Lab investigation
✓ Grading severity of reaction into mild and sever
➢ Mild
✓ inflammation of skin lesions without nerve involvement
➢ Severe
✓ Reactional lesion overlying major nerves
✓ Nerve involvement
✓ Edema of hand and feet
✓ Mild RR persisting over 4 weeks
➢ Specific treatment
✓ Prednisone tapering dose starting 40 to 60 mg, depending on severity of reaction
✓ Other drugs: azathopurine, cyclosporine
✓ Nerve abscess: surgical release
✓ Prevention of secondary disabilities by health education (eye, hand & foot care)

Type II (Erythema Nodosum Leprosum)


➢ Immune complex reaction due to excess production of antibody to M. leprae antigens
➢ Common in lepromatous spectrum (BB, BL & LL)
➢ Panniculitis and vasculitis (tender subcutaneous nodules)
➢ Mild to moderate inflammation of nerves
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Treatment of ENL
➢ General
➢ Lab investigation
➢ Grading of severity
➢ Mild
✓ Skin eruption without nerve tenderness or loss of function
➢ Severe
✓ Multiple and ulcerating lesion
✓ Iritis, orchitis, nephritis or hepatitis
✓ Nerve tenderness and loss of function

➢ What is a relapse?
✓ Return of active disease after completion of prescribed treatment
✓ When the BI at any site increases by at least 2+
✓ Detection of active disease 2 years after completion of treatment
✓ Relapse rate mono therapy era 20 -27%
✓ Relapse with combination treatment 4-20%
✓ Relapse after MDT less than 1% with the 2 years of MDT/ MB
✓ Relapse after 1year MDT/MB not yet known
➢ How to recognize relapse
✓ Active lesion
✓ Increase in BI
✓ New lesion
✓ Erythema
✓ Neuritis
✓ Deterioration of nerve functions
➢ Clinical features
✓ New lesions
✓ Extension of existing lesions
✓ Change in morphology of lesions
✓ Increase in number of lesions
✓ Erythema of lesions
✓ Neuritis
✓ New nerve function loss
✓ Eye symptoms e.g iritis
➢ Management of relapse
✓ Distinguish misclassified cases and defaulter
✓ Treat all relapses with full WHO/MDT regimen

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20.3. Anthrax (ቁርባ)

➢ Anthrax is an infection caused by a bacterium called B. anthracis, that exists in the


environment as a spore and can remain viable in the soil for decades.
➢ Spores ingested by grazing herbivores germinate within the animal to produce the
virulent vegetative forms that replicate and eventually kill the host.
➢ Products (e.g., meat or hides) from infected animals serve as a reservoir for human
disease.
➢ B. anthracis can invade the human body by transcutaneous, GI, and pulmonary
routes
➢ Infection can lead to localized or systemic disease:
✓ Cutaneous anthrax: when spores enter cutaneous, they become vegetative,
multiply, locally spread, and produces toxins which cause extensive edema and
tissue necrosis.
✓ Gastrointestinal anthrax; follows ingestion of contaminated and undercooked meat.
✓ Inhalational anthrax: spores enter alveoli, cause hemorrhagic mediastinitis. Left
untreated it is universally fatal.

Clinical features
➢ Cutaneous anthrax: eschar with extensive surrounding edema is the hallmark
✓ Most common form
✓ Lesions occur in exposed areas: face, neck, arms, and hands.
✓ Starts as small, painless, pruritic papule
✓ A ring of vesicles develops around the papule.
✓ Vesicular fluid may be exuded
✓ The original papule ulcerates with a necrotic a black, depressed eschar (dead
tissue)
✓ Extensive edema of the surrounding tissues
✓ Regional lymphadenopathy and lymphedema
✓ Edema with face or neck infection may produce airway compromise.

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➢ Gastrointestinal anthrax
✓ Initial symptoms: headache, low-grade fevers, and conjunctival injection.
✓ Oropharyngeal: sore throat, dysphagia and painful regional lymphadenopathy.
Extensive swelling of the neck and chest wall.
✓ Gastrointestinal: Abdominal pain, nausea/vomiting, less frequently diarrhea.
Progressive ascites and hypotension.

➢ Inhalational anthrax
✓ Initial phase (4-5 days): myalgia, fever, and malaise, hemoptysis, dyspnea,
odynophagia, or chest pain
✓ Fulminant bacteremic phase: progressive severe dyspnea, hypoxia, and shock.

➢ Meningitis:
✓ Can occur in association with any of the other forms of anthrax.
✓ Typically hemorrhagic meningitis: hemorrhagic CSF confusing with traumatic LP.
✓ Delirium or coma, seizures, cranial nerve palsies, myoclonus

Investigations and diagnosis


➢ A high index of suspicion is needed in those who have exposure to animals.
➢ Specimen for gram stain and culture
✓ Swab from cutaneous lesion: unruptured vesicles, base of ulcer, eschar (elevate
the edge and swab the base)
✓ Oropharyngeal lesion
✓ Pleural fluid, ascitic fluid should be sampled if present
✓ In GI anthrax: stool, rectal swab
✓ Blood culture
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✓ All patients with suspected systemic anthrax or meningitis should have lumbar
puncture unless contraindicated.

Treatment
Non pharmacologic

➢ Apply contact isolation precautions for patients with draining anthrax lesions.
➢ Drain pleural fluid: Chest tube drainage, improves survival by decreasing toxin level
➢ Drain ascites: drain as much as possible (continuous or frequent intermittent drainage)
➢ Standard sepsis care: IV fluids for patients with systemic anthrax.
➢ Other supportive cares

Pharmacologic
➢ Antimicrobial therapy

Table: Antimicrobial therapy for anthrax


First line Alternative Duration
Anthrax with ➢ Ciprofloxacin 400 mg IV If Meropenem or other ➢ At least 2 weeks or
meningitis TID carbapenems are not until the patient is
OR PLUS available, replace it with clinically stable,
Systemic ➢ Meropenem 2g IV TID ➢ Penicillin G 4million whichever is longer.
anthrax when PLUS IU Q4hr ➢ Complete a 60-day
meningitis is ➢ Clindamycin 900mg IV OR course with either of
not ruled out TID ➢ Ampicillin 3gm QID the following two oral
by CSF If clindamycin is not agents
analysis available replace it with ✓ Ciprofloxacin
either 500mg BID
➢ Rifampicin 600mg OR
BID ✓ Doxycycline
OR 100mg BID
➢ Chloramphenicol
1gm, QID
Systemic ➢ Ciprofloxacin 400 mg IV If clindamycin is not Similar to meningitis:
anthrax when TID available replace it with see above
meningitis is PLUS either
excluded ➢ Clindamycin 900mg IV ➢ Doxycycline 200mg
TID loading, then 100mg
BID
OR
➢ Chloramphenicol 1gm
QID
Cutaneous ➢ Ciprofloxacin 500mg PO ➢ Clindamycin 600mg PO 7-10 days
anthrax with
no systemic
BID
OR
TID
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involvement ➢ Doxycycline 100mg PO BID

Considerations for special population


➢ All the considerations above are applicable for pregnant, lactating, and postpartum women.
However, ciprofloxacin is strongly preferred when single agent is used.

➢ Corticosteroids: Hydrocortisone or Dexamethasone IV


✓ Indications:
▪ Meningitis
▪ Extension head and neck edema in cutaneous anthrax
▪ Vasopressor refractor shock
➢ Antitoxin therapy:
✓ Is recommended for patients with systemic anthrax.
✓ Anthrax immunoglobin derived from human plasma can be used for this purpose.
➢ Prevention
✓ Annual vaccination of livestock is the major means of preventing naturally
occurring epizootics of anthrax.
✓ Pre-exposure vaccination with anthrax vaccine adsorbed (AVA) for likely
occupational exposure to aerosolized Bacillus anthracis spores.
✓ Post-exposure prophylaxis (PEP) for documented or suspected inhalational
anthrax with oral single antimicrobial agent (ciprofloxacin preferred) (doxycycline
can be used for non-pregnants‘) for 42 to 60 days plus vaccination.
✓ For naturally occurring gastrointestinal or cutaneous antimicrobial prophylaxis a 7-
to 14-day ciprofloxacin may be considered but no vaccination is recommended

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20.4. Rabies (የእብድ ውሻ በሽታ)

➢ Rabies is a fatal viral disease that can affect almost all mammals.
➢ The causative agent is Rabies virus from class Rhabdoviridae, genus Lyssavirus and
species Serotype 1.
➢ The virus is transmitted through inoculation of saliva, usually from the bite of an
infected animal.
➢ More than 95% of the deaths are due to exposure to dogs, which are the major
reservoir and transmitter of rabies, but transmission by wild animals such as bats,
foxes, and wolves is also possible.
➢ The incubation period is relatively long (3 weeks to 3 months) but can be as long as
several years in rare cases.
➢ The closer the inoculation site is to the CNS, the shorter the incubation period.

Clinical features

➢ Prodrome (2-10 days):


✓ Paresthesias (pins and needles sensation) around bite: very suggestive of rabies.
✓ Fever, headache, malaise, muscle pain, nausea, vomiting, and cough.

➢ Encephalitic rabies: Acute neurologic phase (2-7 days):


✓ Confusion, delirium, altered mentation, agitation, hallucinations.
✓ Spasms in response to touch, noise, visual, or olfactory stimuli.
✓ Phobic spasms: hydrophobia (fear of water) and aerophobia (fear of air): strong
evidence for rabies.
✓ Autonomic system dysfunction: enlarged pupils, increased production of saliva,
tears, perspiration
✓ Generalized arousal or hyperexcitability associated with disorientation, fluctuating
consciousness, restlessness, agitation, and visual or auditory hallucinations.
✓ Coma, death (0-14days)
▪ Occurs after several days to 1 week. Once Neurologic features develop
death is 100% with in 7 to 10 days
▪ Hypoventilation, loss of temperature control, heart dysfunction can lead to
death.

➢ Paralytic rabies (Ascending paralysis)


✓ Similar to Guillain-Barré syndrome, occurs in some cases and makes diagnosis
more difficult.
✓ This can also occur during post-exposure rabies treatment. 1413
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Investigations and diagnosis


➢ Diagnosis rests on history of exposure and typical neurological findings.
➢ CSF: increased white cells (lymphocytes), mildly increased protein.
➢ Laboratory confirmation is usually postmortem

Treatment
➢ There is no effective treatment against rabies.
➢ It is almost always fatal.
➢ Supportive management is important.
➢ Recovery is exceedingly rare and has only occurred in cases where intensive
respiratory and cardiac supports were available.
➢ Apparently healthy dogs and cats at the origin of the exposure should be kept under
observation for 10 days.
➢ Dogs and cats that are suspected of being rabid, as well as wild animals, should be
humanely killed and their tissues examined in the appropriate laboratory.

Non pharmacologic

➢ Supportive treatment of a paralyzed patient mostly focused on nursing care and


providing comfort to the patient.

Pharmacologic
Palliative care
➢ The short clinical course of rabies entails much suffering.
➢ Patients remain conscious, are often aware of the nature of their illness and very
agitated.
➢ Provide adequate sedation and comfort with emotional and physical support.
➢ IV morphine: relieve severe agitation and phobic spasms. Sedation with barbiturates
can be added.
➢ Avoid intubation and other life support measures when the diagnosis is certain.

Health worker safety

➢ It is theoretically possible for person-to-person rabies though this has not been
described.
➢ As a precaution staff must wear mask, gloves, and goggles.
➢ Post-exposure prophylaxis is required if a percutaneous, mucous membrane, or
nonintact skin exposure to patient‘s body fluids or tissue occurred. 1414
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Rabies post exposure prophylaxis (PEP)


Rabies post-exposure vaccination after animal bites
➢ Wound care
✓ The cornerstone of rabies prevention is wound care: potentially reduces the risk
of rabies by 90%.
▪ Immediately scrub with soap and water, and flush with water for 15
minutes
▪ Irrigate with Povidone-iodine
➢ Vaccination
✓ Decide on post-exposure vaccination and immunoglobulin use depending on the
type of contact with the rabid animal.

Table; Postexposure prophylaxis (PEP)


Category of Description PEP
exposure
Category I Touching or feeding animals, licks on No PEP is required. Wash
the skin, contact of intact skin with exposed skin Surfaces.
secretions or excretions of rabid
animal or person.
Category II Nibbling of uncovered skin, minor Wound washing and
scratches or abrasions without immediate vaccination
bleeding
Category III Single or multiple transdermal bites Wound washing and
or scratches, licks on broken skin, Immediate vaccination and
contamination of mucous membrane administration of rabies
with saliva from licks; exposure to immunoglobulin
bat bites or scratches

Vaccination:
➢ IM doses of 1ml or 0.5ml given as 4 - 5 doses over 4 weeks.
➢ One dose of the vaccine should be administered on days 0, 3, 7, 14, and 30.
✓ RX; Antirabies vaccine. 1ml, IM, @ 0, 3, 7, 14, and 30 days.
➢ Abbreviated multisite schedule: 2-1-1 regimen: 1 dose is given in the right arm, 1
dose in the left arm at day 0, and 1 dose applied in the deltoid muscle on days 7 &
21
➢ All intramuscular injections must be given into the deltoid region.
➢ The vaccine should never be administered in the gluteal region.

If prior pre-or post-exposure vaccination:


➢ 2 IM doses separated by 3 days are sufficient. 1415
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➢ Rabies immunoglobulin treatment is not indicated in such cases.

Intradermal vaccination:
➢ Smaller doses of cell-derived vaccines are also used.
➢ Less effective than IM vaccine
➢ The schedules are different than IM schedules.
✓ Antirabies vaccine, 5ml, SC, daily for 14 days followed by every 10 days for 3
doses

Immunoglobulin:
➢ Human rabies immune globulin 20 IU/kg OR
➢ Equine rabies immunoglobulin 40 IU/kg

Pre-exposure vaccination
➢ Pre-exposure vaccination is recommended for those in rabies diagnostic and research
laboratories and veterinarians, individuals at high risk of exposure such as stray dog
handlers, park officials, or bat handlers.
➢ Pre-exposure vaccination is administered as;
✓ 1 full dose vaccine given 3 times, IM or
✓ 0.1 ml intradermal, on days 0, 7, and 21 or 28.

Antibiotics
➢ Augmentin is better than cloxacillin for Animal bite.
➢ Clean the wound but Don’t cover it.
➢ If suturing is necessary, delayed wound closure after wound care.

N.B

Once patients develop antirabies features (like photophobia…), it is 100% lethal within 3
to 7 days and no need of vaccination

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20.5. Filariasis, Lymphatic (Elephantiasis)/ዝሆኔ/

➢ The term filariasis refers generally to disease caused by the lymphatic-dwelling filarial
worms Wucheria bancrofti, Brugia malayi, and Brugia timori.
➢ Wuchereria bancrofti is the most common cause of lymphatic filariasis in the Tropics
including Ethiopia.
➢ The infection is transmitted by mosquitoes.
✓ Filarial parasites exhibit a daily periodicity in the concentration of microfilariae in
the peripheral blood.
➢ The main clinical presentation (lymphedema) is also the main feature of podoconiosis
("non-filarial elephantiasis").
✓ Podoconiosis, a non- infectious disease, is a geochemical disease occurring in
individuals exposed to red clay soil of volcanic origin.
➢ Lymphatic filariasis is found in several districts of SNNP, Oromiya, Amhara,
Benishangul Gumuz, and Gambella.
➢ Podoconiosis is also widespread in six regional states in the country (Amhara,
Benishangul Gumuz, Oromia, SNNPR, Somali and Tigray)

Clinical Features
➢ Progressive filariasis: In progressive filariasis, the clinical features depend on the
clinical stage.
✓ Asymptomatic amicrofilariaemic stage: No clinical symptom
✓ Asymptomatic microfilariaemic stage: No clinical symptoms but microfilariae
detectable
✓ Stage of acute manifestations:
▪ Filarial fever (ADL-DLA)
▪ Acute adenolymphangitis (ADL): high fever, lymphatic enlargement, local
edema, tenderness and redness of overlying skin. Ulceration can occur.
▪ Dermatolymphangioadenitis (DLA): high fever, chills, muscle aches, and
headache with inflammatory skin changes in the area of infection.
✓ Lymphangitis
✓ Lymphadenitis
✓ Epididimorchitis
➢ Stage of obstructive (chronic) lesions: 5-15 years
✓ Leg lymphedemas or hydrocele (see the table below for staging of lymphedema)
✓ Chyluria: milky urine. Lymph being intermittently discharged in the urine. This can
lead to malnutrition

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Table: Stages of lymphedema in chronic lymphatic filariasis


Swelling Skin folds Apearance
Stage I Reversible at night Absent Smooth, normal
Stage II Not reversible at night Absent Smooth, normal
Stage III Not reversible at night Shallow Smooth, normal
Stage IV Not reversible at night Shallow Irregular, occasional knobs or
nodules
Stage V Not reversible at night Deep Smooth or irregular
Stage VI Not reversible at night Shallow or deep Wart-like lesions on foot or toes
Stage VII Not reversible at night Deep Irregular; needs help with daily
activities; dependent

➢ Occult or cryptic filariasis, presenting as tropical pulmonary eosinophilic (TPE)


syndrome:
✓ Occult filariasis results from hyper-responsiveness to filarial antigens.
✓ Classic manifestations are: paroxysmal cough and wheeze, scanty sputum,
occasional hemoptysis, adenopathy, chronic interstitial lung disease, recurrent
lowgrade fever, and weight loss.

Investigations and diagnosis


➢ Lymphatic filariasis should be suspected in individuals living in districts known to have
the disease who present with typical acute manifestations (see above) or chronic
manifestations (lymphedema, chyluria, hydrocele).
➢ Definitive diagnosis is established by either of the following
✓ Blood film:
▪ Demonstration of microfilariae in peripheral blood film (Giemsa or wright
stain):
▪ Due to the nocturnal periodicity; the greatest number of microfilariae can
be found in blood between 10:00 PM and 2:00 AM.
✓ Detection of circulating filarial antigen
➢ CBC: extremely high eosinophil count.
➢ Imaging
✓ Ultrasonography: adult worms may be visualized in the lymphatics of the female
breast or male scrotum

Treatment
Non pharmacologic

➢ Supportive treatment and prevention of acute ADL attacks:


✓ Hydration and rest 1418
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✓ Antipyretics and analgesics


✓ Treatment and prevention of lymphedema: Hygiene measures for the affected
limb:
✓ Wash twice daily with soap and clean water and dry well
✓ Keep nails short and clean
✓ Elevate the affected limb at night
✓ Wear comfortable footwear
✓ Prevent and treat entry lesions
✓ Frequent exercise of the affected limb to promote lymph flow
✓ Standing on toes, flexing and circling ankles while sitting • Use of antibiotic or
antifungal agents:
✓ antiseptic, antibiotic, and antifungal creams for small wounds and abrasions
✓ systemic antibiotics or antifungals in severe cases • Surgical treatment of
hydrocele

Pharmacologic

➢ Recommended regimen for lymphatic filariasis in clinical settings:


✓ Diethylcarbamazine citrate (DEC), 6mg/kg P.O. daily for 12 days
OR
✓ Diethylcarbamazine citrate, 6 mg/kg. P.O. PLUS Albendazole 400mg P.O., Stat.

✓ DEC should not be used in patients with onchocerciasis, due to possible severe
adverse reactions (fatal encephalopathy).
✓ Patients should be examined for co-infection before using DEC.
▪ In co-infected patients, the following alternative regimen should be used:
• Ivermectin, 200-400micrograms/kg P.O.
Plus
• Albendazole 400mg P.O. as single dose
✓ N.B. Ivermectin should not be used in patients with loiasis.

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Table: Treatment of lymphatic filariasis among adults


Infection status Clinical condition Treatment
Lymphatic lymphatic filariasis with single-dose DEC (6 mg/kg), ± doxycycline
filariasis clinical symptoms or not (200 mg/day for 4 to 6 weeks)
(Mono- has tropical pulmonary 14 to 21 days of DEC (6 mg/kg/day) ±
infection) eosinophilia due to W. doxycycline (200 mg/day for 4 to 6 weeks)
bancrofti
Concomitant Without ocular DEC is contraindicated with
infection: involvement Onchocerciasis; Thus, first ivermectin
lymphatic (150 mcg/kg single dose) followed by
filariasis with DEC treatment as above (after 1 month of
Onchocerciasis ivrmectin)
with ocular involvement doxycycline 200 mg orally once daily for 4
to 6 weeks) followed by ivermectin 150
mcg/kg orally single dose
Concomitant <2500 Loa loa DEC standard regimen for loiasis (8 to 10
infection: microfilariae/mL of mg/kg/day for 21 days)
lymphatic blood
filariasis with 2500 to 8000 L.loa ivermectin pretreatment, followed by DEC
Loiasis microfilariae/mL of
blood
> 8000 L.loa doxycycline (200 mg/day once orally for 4
microfilariae/mL of to 6 weeks) or Albendazole (200 to 400
blood mg BID for 21 days, with fatty meal)

Prevention
➢ Mass drug administration (MDA)
✓ Annual single dose of DEC 6mg/kg
PLUS
✓ Albendazole 400 mg, yearly for 4-6 years in areas where onchocerciasis is not
co-endemic with filariasis.
▪ In areas where onchocerciasis is present but loiasis is absent:
• Annual single dose of Ivermectin 200-400 µgs/kg
PLUS
• Albendazole 400 mg, yearly for 4- 6years.
➢ Vector control

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20.6. COVID -19


➢ Covid -19 is RNA virus that belongs to the family of CORONA (Latin Crown, from the
structure of the virus under electron microscope)
➢ The name Covid -19 stands for;
✓ CO – Corona
✓ VI – Virus
✓ D - Disease
✓ 19 – First identified in December 2019 G.C
➢ The new CORONA virus identified as the cause of the acute respiratory disease in
humans since the end of December 2019 (2019-nCoV)
➢ Later labeled as SARS-CoV2 by WHO is a different strain of CORONA virus from
SARS and MERS CORONA viruses.
➢ The difference is not limited to genetic make-up only but also in the clinical
presentations, case fatality and the rate of spread across the globe.
➢ The disease caused by this virus is known as COVID-19.
➢ First seen in Wuhan, China, the disease has been recognized as global public health
emergency by WHO after cases had started to be seen outside china in less than
two-month period.
➢ Transmission
✓ Physical contact and respiratory routs are the two most important well-established
routs of transmission of the virus.
✓ Poor hand hygiene practice, overcrowding, and close physical contacts like hand
shaking contributes for the fast spread of the
virus with in very short period of time

Case definitions for COVID-19


1. Suspected case
A person presenting with fever (>38℃) or history of fever and symptoms of
respiratory tract illness e.g. cough, difficulty in breathing AND a history of travel to or
residence in a country/area or territory reporting local transmission of COVID-19
disease during the 14 days prior to symptom onset.
OR
A person with fever (>38℃) or history of fever and symptoms of respiratory tract
illness e.g. cough, difficulty in breathing AND in the last 14 days before symptom
onset, close contact with a person who is under investigation or confirmed for
COVID-19
OR
A person with fever (>38℃) or history of fever and symptoms of respiratory tract
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illness e.g. cough, difficulty in breathing; And requiring hospitalization) And in the
absence of alternative diagnoses that fully explains the clinical situation
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2. Probable case:

Suspect case for which testing for COVID-19 is inconclusive


OR
A suspect case for whom testing could not be performed for any reason

3. Confirmed case:

A person with laboratory confirmation of COVID-19 infection, irrespective of clinical


signs and symptoms.

General principle of clinical management for COVID-19


➢ Specimens for detecting COVID-19 can be obtained from
✓ Nasopharyngeal (NP) swabs
✓ Oropharyngeal (OP) swabs
✓ Deep expectorated sputum (if produced) or
✓ Bronchoalveolar lavage in specialized conditions.
➢ Give supplemental oxygen if SPO2 if < 90% in non-pregnant adults and < 92% in
pregnant mothers and children
✓ SPO2 has to be >94% For children with emergency signs such as
▪ Airway obstruction
▪ Shock
▪ Severe respiratory distress
▪ Convulsion and
▪ Resuscitation

Specific treatments
➢ Immuno-modulators
✓ No proven anti-viral therapy so far
✓ Use Chloroquine and/or Azithromycin as immune-modulators
▪ For patients with moderate to severe infection and
▪ In patients with milder symptoms if they are elderly and/or with underlying
diseases.
✓ Dose:
▪ Chloroquine phosphate 1g (4tabs) stat, then 500mg (2 tabs) after 12 hours
then 500mg (2 tab) bid for 5 days and
▪ Azithromycin 500mg PO daily for 3 days.
✓ Baseline EKG and CBC/comprehensive metabolic panel (CMP).
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▪ If therapy is extended beyond 3 days, obtain a CBC/CMP on day 3 and day 7.

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1. Mild illness
Clinical features

➢ Patients with uncomplicated upper respiratory tract viral infection, may have non-
specific symptoms such as fever, cough, sore throat, nasal congestion, malaise,
headache, muscle pain
➢ Atypical symptoms in elderly, immunocompromised and infants
➢ These patients may not have any signs of dehydration, sepsis or shortness of breath.

Management
➢ Maintain standard Infection prevention and control procedures
➢ Minimize contact with household members and ask patient to wear a surgical mask if
contact is necessary
➢ Close monitoring for signs of clinical deterioration such as respiratory failure, sepsis/
septic shock has to be done for early management of such complications.
➢ Advise patients to keep hydrated, but not to take too much fluid as this can worsen
oxygenation
➢ Paracetamol 1gm, PO, TID to QID, maximum 4g/ 24hr
➢ Tramadol 50–100 mg PO/IV every 4–6 hours, maximum 400 mg/day
✓ Can be given alternatively or combined with paracetamol.
➢ Avoid Ibuprofen, and Aspirin use

2. COVID-19 patients with pneumonia (mild or moderate)

Clinical features

➢ Patient with above symptom and pneumonia with no signs of severity.

Management

➢ Management as in the mild illness +empiric oral antibiotics


✓ Amoxicillin 500mg po TID or
✓ Augmentin, 625mg, PO, TID or 1gm PO BID for 5-7days

3. COVID-19 Patients with severe Pneumonia or who developed SARI


Clinical feature
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Assess severity using CURB-65 criteria.


✓ Confusion
✓ Urea > 7mmol/L or abnormal Creatinine value
✓ RR >30
✓ BP <90/60
✓ Age >65
▪ For all patients, the CURB-65 score should be interpreted in
conjunction with clinical judgment.
▪ Patients with a CURB-65 score of >2 should be admitted

Management:
Provide oxygen supplementation → Target SpO2 ≥ 90% (for pregnant mother,
children, patient in shock SpO2 > 92-94%)
Conservative IV fluid management should be instituted except when patient is in
shock
In COVID 19 superimposed bacterial infection is common and to treat all likely
pathogens antibiotics administration is common depending on the treating physician
judgment
Empiric antimicrobials should be started after taking specimen for culture and
sensitivity (preferably broader spectrum antibiotics).
✓ Don’t delay antibiotics intake if culture service isn‘t available
In patients with who are critical, hospitalized, immune-compromised or previous
structural lung disorder:
✓ Ceftazidime/Cefepime *2g iv Tid +or +/- Vancomycin 1 gm IV
BID.
✓ Ceftriaxone 1gm IV bid is alternative to ceftazidime/Cefepime but nowadays it is
not routinely used in severe pneumonia or sepsis because of high rate of
resistance.
If there is no response with the above antibiotics or culture and sensitivity result
suggests it
✓ Meropenem (or other available carbapenemes) 1g IV,TID +/- vancomycin 1g IV,
BID.
When patients improve and are able to take PO → Augmentin, 625mg, PO, TID

Management of patients with hypoxemic respiratory failure and


ARDS
➢ Some patients fail to maintain oxygen saturation despite standard oxygen flow
administration.
✓ Such condition is usually due to intrapulmonary ventilation-perfusion
mismatch with hypoxemic respiratory failure.
➢ Clinical features of acute hypoxemic respiratory failure:
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✓ Dyspnea
✓ Cyanosis
✓ Tachycardia
✓ Tachypnea
✓ Use of accessory muscles
✓ Nasal flaring
✓ Intercostal and subcostal retraction and
✓ patients may develop altered mental status.
➢ Patients with COVID-19 develop acute respiratory failure 20 to ARDS
ARDS is characterized by:
✓ Onset: new/worsening respiratory symptoms within one week
✓ Chest imaging: bilateral opacities not fully explained by other features like
effusions, lobar opacity, lung collapse or nodules
✓ Origin of edema: respiratory failure not fully explained by cardiac failure or fluid
overload
✓ Oxygenation: severe hypoxemia regardless high oxygen input
✓ Impaired oxygenation
➢ Kigali‘s definition may be used to assess oxygenation: - when SpO2/
FiO2 ≤ 315 it suggests ARDS.

Management of acute hypoxemic respiratory failure 20 to ARDS


➢ Oxygen via face mask with reservoir bag-flow rates 10-15l/min
✓ 2-HFNO/NIV should only be used in selected patients without comorbidities and
nonpregnant.
✓ Monitor closely for one hour and deliver invasive ventilation if acutely deteriorate
or no improvement
➢ Endotracheal intubation
➢ Mechanical ventilation
➢ If no improvement, consider prone ventilation except in pediatrics patient
➢ Management of septic shock (refer from short case of Nitsbin or click here → Chapter
3; Shock)

Invasive respiratory support for COVID 19


➢ Current data indicate that 5% of the COVID 19 affected patients are critically ill.
Hence, supporting the respiratory system with positive pressure is needed expansively

Mechanical Ventilator Management of COVID19 Patients


1. Setting on Mechanical Ventilator → Invasive Mechanical Ventilation (IMV) for ARDS

2: Treat underlying cause


3: Monitor and respond as per protocol

➢ Weaning from Mechanical Ventilator


➢ Conduct spontaneous breathing trial daily when
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✓ FIo2<= 0.4 and PEEP <=8 Or PEEP<=5 and FIO2<=0.5


✓ Patients has acceptable spontaneous breathing efforts (may decrease ventilator
support by 50% to see the effort)
✓ Systolic BP ≥ 90mmHg without vasopressor support
✓ No neuromuscular blocking agents or blockade

Prevention of Complication
➢ Reduce days on mechanical ventilation by assessing readiness for spontaneous
breathing (spontaneous breathing trial)
➢ Reduce Ventilator Associated Pneumonia
➢ Oral intubation preferred over nasal intubation in adolescents and adults
➢ Keep the head of patients up in 30-45O
➢ Use closed suctioning method to prevent contamination
✓ Use new clean breathing circuit if possible, for each patient, change the circuit
only if damaged and soiled
➢ Reduce incidence of venous thromboembolism
✓ LMW heparin or unfractionated heparin
✓ Intermittent pneumatic compression
➢ Turn patients every 2 hours to prevent pressure ulcer
➢ Initiate early enteral nutrition with in the 24-48hours of admission
➢ Start H2 blocker or PPI prophylaxis for GI bleeding

Discharge criteria for COVID-19 cases admitted to treatment center


➢ Patient diagnosed with COVID-19 pneumonia can be discharged when the symptoms
have subsided, patients get stable and able to feed, and the body temperature
remains at a normal range for at least 3 days without antipyretics, and two
consecutive laboratory tests are negative collected ≥24 hours apart.
➢ If laboratory tests are not available or significantly delayed decision should be based
on clinical judgment
➢ Patients can remain infectious for 2 weeks after symptoms have improved, thus
maintain isolation and IPC.
➢ Any person who has contact with confirmed COVID-19 case has to be followed for
14 days:
✓ If no symptoms develop within 14 days follow up, discharge the person from the
follow up.
✓ If symptoms develop during the 14 days follow up, admit the patient, treat and
follow the same protocols to discharge.

Further reading
➢ NATIONAL COMPREHENSIVE COVID19 MANAGEMENT HANDBOOK, FMOH, Ethiopia, 2020 1426
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Chapter 21; Interpretation of Chest X - Ray (የደረት ራጅ ማንበብ) 1427

Chapter 21; Interpretation of Chest X - Ray


(የደረት ራጅ ማንበብ)
Dr. Mulualem. G

A CXR is a two-dimensional representation of a three-dimensional structure. As a


result, the CXR includes many overlapping structures

Basic principles: Densities

The more X-rays reach an area of the film, the darker that area will be on the
radiograph. Therefore, if an object is very dense, less X-rays will reach the film
and consequently the image of the object will appear white on the radiograph.
If an object has little density, its image will appear black on the CXR because it
allows most of the X-ray beam to reach the film.
Difference in density and x ray attenuation…help outline anatomic
structures…allowing visualization of details

Image; Plain films have five basic radiographic densities in order of increasing brightness: 1 → Air (black),
2 → Fat (gray), 3 → Fluid (gray), 4 → Bone (white), 5 → Metal or x ray contrast agents (white).

Basic stapes for Interpretation of CXR

A. Quality Assessment (Technical Aspects)


➢ Is the film correctly labeled?
➢ Assessment of exposure quality
B. Assessment of Patient dependent factors
➢ Assessment of Centering / Symmetry of film:
➢ Assessment of adequacy of inspiratory effort
C. Review of important radiographic anatomy
➢ The soft tissues
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➢ The diaphragm → Elevation, flattening, costophrenic (C-P) angle, air under the
diaphragm
➢ The pleura:
➢ Trachea
➢ The Hilum
➢ The lung fissures
➢ The lungs
➢ The Heart and mediastinum

21.1. Step 1. Quality Assessment (Technical Aspects)

1.1 Is the film correctly labeled? Check the following:


Name, age and sex of the patient
Date of CXR is taken
Health facility’s name
The left & right-side markers
Projection of film
o P-A: commonly used
o A-P…. “ward film”
o Lateral
o Lateral decubitus

CXR Projections

A) P-A projection

Figure; PA CXR; Most CXRs are taken in a PA position; The x-ray beam passes through the patient from

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back to front (i.e. PA) onto the film. The heart and mediastinum are thus closest to the film and therefore
not magnified.

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B) A-P or supine film

Portable bedside CXR- “ward film”, Especially for critically ill / ICU pts
Important to;
o Look for new pathology after admission
o Assess C-P status & position of catheters, ETTs and other devices
o Detect complications related to these devices

Image; A-P CXR

Limitations:
o Often rotated films, poor quality
o Magnification of intra thoracic structures
▪ Widening of upper mediastinum…due to increase in venous return
▪ Cardiac diameter increased by 15-20%
▪ High position of diaphragm
▪ Small lung volumes, compression of lower lobes
o Difficult to detect small pleural effusions and pneumothorax

C. lateral view

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D. Lateral Decubitus

1.2 Assessment of exposure quality:

Is the film penetrated enough?


In Optimal exposure /good penetration
o Vertebrae are seen until T4 spine; below which it is covered by cardiac
shadow. T4 is at the level of sternal angle
o Visualization of vessels to at least 1/3rd of the lung periphery.

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A B
Picture; A) Over penetrated/ over exposed film (Dark film). Easy to see thoracic spines behind the heart
shadow; but pulmonary vessels peripherally are not clearly seen. B) Under penetrated film (The image too
white); Fail to see vertebrae above T4 (and also behind the heart). Accentuates pulmonary vascularity,
which may be mistaken for generalized infiltrates.

21.2. Step 2. Assessment of Patient dependent factors

2.1 Assessment of Centering / Symmetry of film:


Well centered CXR: medial / sternal ends of clavicles are equidistant from the mid
line (the vertebral spinous process)
o If distance on one side is > 1.5 cm, it is asymmetric
o Patient rotation to one side makes the side of lung darker.
If there is rotation, the side to which the patient is rotated is assessed by
comparing the densities of the two hemi-thoraces. The increase in blackness of
one hemi-thorax is always on the side to which the patient is rotated, irrespective
of whether the CXR has been taken PA or AP.
Rotation will also alter the relative appearance on the hila and can mimic hilar
asymmetry and the projection of the sternum over the hilum may be evident

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rotated film ( to the Left )


Picture; this patient (image over the right) is rotated to the left. Note the spinous process is close to the
right clavicle and the left lung is ‘darker’ than the right, due to the rotation.

2.2 Assessment of adequacy of inspiratory effort (i.e. does the patient has taken
adequate inspiratory effort?)
By counting visible anterior or posterior ribs

Picture; Optimal: 6 anterior or 10 posterior ribs are visible above the diaphragm

Poor inspiratory effort / Expiratory film:


CXR is taken on expiration

Hemidiaphragms are higher


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Heart appears large, crowding of basilar pulmonary vessels.


Breast shadows overlap the hemi diaphragms.
Expiratory film obtained after maximum expiration to RV
o To detect air trapping, small pneumothorax

Picture; < 6 anterior or < 10 posterior ribs visible

Limitations: Results in spurious findings like


o Enlarged cardiac silhouette
o Bilateral patchy basilar infiltrates
o Hilar or mediastinal abnormalities
Misinterpreted as cardiomegaly, basal pneumonia/interstitial lung diseases.

Poor inspiratory effort Vs full inspiration

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Picture; Two CXRs of the same patient taken on the same day. For the CXR on the left the patient has
made a poor inspiratory effort. Note the apparent bulkiness of the hila, increased density in the lower
zones and the enlarged cardiac silhouette. The CXR on the right taken in full inspiration demonstrates that
the patient’s CXR is normal and previous apparent abnormalities were due to poor inspiratory effort

If > 6 anterior or > 10 posterior ribs are visible above diaphragm, it implies
hyperexpanded lungs (eg. air trapping as in COPD with large lung volumes & flat
diaphragm)

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21.3. Step 3. Review of important radiographic anatomy

From the periphery to the center or vice versa.


Compare symmetrical sides of the film

Review areas:
o Apices
o Behind the heart
o CP angles
o Below the diaphragm
o Soft tissues (breast, surgical emphysema)
o Ribs & clavicle
o Vertebrae
Hidden areas: apices, mediastinum & hila, posterior sulcus

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Pictures; Normal lateral CXR, PCPA- post C_A angle

3.1 The soft tissues


Normal tissue shadowing on CXR -breast shadow, nipple shadow
Look for any subcutaneous emphysema, edema, or mass
The soft tissues lateral to the bony thorax should be smooth, symmetric
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Picture; Breast and nipple shadow

3.2 Bony structures


(Ribs, sternum, thoracic spine, clavicle, scapula)
look for any bone mass or lesion (lytic, sclerotic), fracture, deformity, rib spacing,
notching etc.

3.3 Diaphragm
Elevation, flattening, C-P angle, air under the diaphragm
Normally the Right is higher (by 1-1.5cm) than the Left. A difference of > 3cm is
abnormal
The highest point of the hemidiaphragm should be at least 1.5cm above a line
drawn from cardio phrenic to costophrenic angle (< 1.5 cm suggests flat
diaphragm)
Air in the gastric fundus is normally seen below Left hemidiaphragm but air under
Right hemidiaphragm is pathological (as in perforated PUD).

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Dome medially located with a sharp costophrenic angle

Picture; Air under the diaphragm, the normally air-filled gastric fundus lies beneath the diaphragm. If there
is free gas on the left, only the diaphragm, about 3–4 mm thick, separates the free gas from the lung.
Air in the gastric fundus is separated from the lung by the diaphragm and the gastric wall. Again, sharp
margins to the gas shadow increase the likelihood of free gas. If uncertainty remains, a lateral decubitus
AXR view should resolve the issue, as the free gas will travel to the least dependent area, i.e. the upper
most lateral margin of the abdomen.

Picture; Emphysema: see the flat diaphragm

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3.4 Pleura

Look for
Fluid or air in the pleural cavity; thickening, calcification
Normally the costophrenic angle is acute. Obliteration tells pleural
effusion/empyema
Meniscus sign (◡) is the typical obliteration of the costophrenic angle suggesting
fluid in the pleural cavity.
250ml fluid can be detected on a PA film; lateral decubitus film can detect 10 to
50 ml. The smallest amount visible on decubitus radiographs is 10 ml. With care,
as little as 175 mL of effusion can be detected on supine images.

Picture; Pleural effusions show homogeneous opacity without air bronchogram (as the pleura is extra
parenchymal). This helps to differentiate pleural fluid from consolidation.

In the supine position, a simple pleural effusion will accumulate posteriorly in the
chest and the above described meniscal effect is not seen.
On an upright PA film, fluid collects in the lateral costophrenic angle due to
gravity, giving it a blunted appearance. The posterior costophrenic angle is the
deepest, and fluid collects there first. This angle is hidden by the dome of the
diaphragm on a PA view. However, it is well seen on the lateral view. For this
reason, the upright lateral view is superior to the PA for demonstrating small
amounts of pleural fluid.
When in doubt of pleural effusion, order a decubitus view with the patient lying
down on the side of the suspected effusion. This will bring the fluid between the
lung and the chest wall where it is easy to see. Sometimes the parietal and
visceral pleura are stuck to each other (adhesion). In this situation, a pleural
effusion may not be able to move when the patient changes position. The fluid
may even be stuck in one of the fissures mimicking the appearance of a lung
mass (pseudo-tumor).
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Immobile pleural fluid is called a loculated effusion.

Pictures; B) Lateral CXR: fluid around the left lower lobe. C) Left lateral decubitus view: fluid between the
chest wall and the left lung. A free fluid separating the lung from chest wall by > 10 mm on lateral film is
an indication for therapeutic thoracentesis.

Pleural fluid 1st spill out to posterior C-P angle, then to lateral & eventually
anterior; with further accumulation, it spreads up wards. Appear as Homogenous
opacity obscuring the basal lung field, Obliteration of the costophrenic and cardio
phrenic angle, Elevation of the ipsilateral hemidiaphragm

a. Empyema

Presents as a complex pleural collection.


Fibrous bands may create loculations and the thicker fluid/pus may not be mobile,
therefore failing to collect in the dependent areas
Meniscal contour may not be seen

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Picture; Frontal CXR of an adult with a right sided empyema. Note the pleural based opacity with a
vertical (white arrows) rather than meniscal contour indicating a complex collection in this case including
pockets of air (black arrows). The presence of pleural opacity that fails to conform to the meniscal
appearance characteristic of a simple pleural effusion should alert the reader to the possibility of an
empyema, or pleural tumor. Extension of an empyema outside the chest wall may mimic an invasive soft
tissue mass

b. Pneumothorax

Best seen on expiratory films


In upright PA film, look for a black crescent over the apex of the lung.
o The visceral pleura is often seen as a thin white line under the black
crescent, since it is flanked by air on each side
o No lung tissue (branching white blood vessels) is seen peripheral to the
visceral pleura line

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Picture; A) Chest radiograph of a pneumothorax. The pleural line has lucency on either side, representing
air in the pleural space on one side of the line and air in the lung on the other. The line is sharply
demarcated and can be traced along its course (lower arrow). No blood vessels can be seen beyond the
superior (upper arrow) and lateral (middle arrow) extent of the line. B) Chest radiograph of a skinfold
(arrows) that could be mistaken for a pneumothorax. The border is more of an edge, with lucency on only
one side. The edge is poorly defined and cannot be followed continuously (lower arrow). Blood vessels
can be traced beyond the border of the fold (arrowhead). A skin-fold line often is relatively straight,
whereas a pleural line follows the curve of the inner aspect of the chest wall

Deep sulcus sign of pneumothorax

On a supine AP, the air rises to the anterior and lateral costophrenic angles
(sulci); since they are the highest region in the pleural cavity when pt is lying
down. This creates an abnormally dark and deep lateral sulcus (i.e. deep sulcus
sign).

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Picture; On P-A chest x-ray (A), the costophrenic angle is normally acute (arrow). In a supine patient, a
pneumothorax will often be anterior, medial, and basilar. On a subsequent supine film (B), the dark area
along the right cardiac border and lung base appeared larger (small arrows), and the costophrenic angle
much deeper and more acute than normal (large arrow). These findings were not recognized, and, as a
result, a tension pneumothorax developed in the same patient (C) with an extremely deep costophrenic
angle (large black arrow), an almost completely collapsed right lung (small white arrows), and shift of the
mediastinum to the left.

c. Tension pneumothorax

It is a medical emergency and pt may present with cardiorespiratory distress which


needs immediate intervention

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Picture; PA CXR demonstrating an abnormally black right hemithorax. The right lung has been pushed
medially. The mediastinum is shifted to the left

e. Hydropneumothorax

Presence of both gas & fluid in pleural space


o On erect CXR –air fluid level
o Loculated form - appear as single or multiple collection with air fluid level

Picture; Hydropneumothorax. When fluid and air are present in the pleural space on an upright chest x-
ray, a perfectly straight horizontal line will extend all the way from the spine to the edge of the pleural
cavity. In this patient, a loculated right basilar hydropneumothorax is present. The air/fluid interface is

1444
easily seen (arrows). If this were a lung abscess, the air/fluid level would be very unlikely to extend all the
way from the medial to the lateral aspect of the hemithorax

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3.5 Trachea
Normally mid line or slightly shifted to the right
Diameter is 25mm in male, 21mm in female
Look for:
o Any narrowing, widening
o Displacement: away from the side of a pneumothorax or effusion; towards in
fibrosis or collapse
o Carinal angle – site of bifurcation of trachea, located at T6. Normal angle
is 600 - 750. Angle increased in Left Atrial enlargement or LAP
o Right paratracheal stripe: Normally the Right wall of the trachea should be
clearly seen (uniformly smooth and < 4mm in width)
o Any thickening or nodularity

Picture; Rt paratracheal stripe thickening & bilateral hilar enlargement

The left lateral tracheal wall is surrounded by mediastinal vessels and fat is not
normally visible on CXR
The hilar point is formed by the outer margins of the upper lobe pulmonary veins
and the lower lobe pulmonary arteries as they cross. Note the left main pulmonary
artery loops over the left main bronchus therefore the left basal pulmonary artery
crosses the left upper lobe pulmonary vein higher on the left than on the right and
the hila point is also normally higher on the left.

3.6 Hilum

Formed by pulmonary vessels and adjacent airways


Normally LNs are not seen on a CXR
Equal density, size & concave lateral border
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Y shaped on its side appearance.


Left hilum is 1 - 2.5 cm higher than the right.
Hilar prominence occurs in: TB, sarcoidosis, lymphoma, fungal disease,
pneumoconiosis, lung ca & metastases, Pulmonary arterial hypertension

Picture; Sarcoidosis; Symmetrical hilar nodes, Paratracheal nodes, AP window nodes, Alveolar lung infiltrate

3.7 Lung fissures

Fissures are pleural reflections which separate the individual lobes.


The right lung has oblique (major) and horizontal (minor) fissures.
The left lung has an oblique fissure, separating it into upper and lower lobes.
Note: The horizontal fissure is seen on both frontal and lateral views as a fine
horizontal line. The oblique fissures are seen only on the lateral film as oblique
lines.

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Picture; Main Fissures; Right upper lobe (RUL) sits above horizontal fissure (HF), the Right lower lobe
(RLL) lies behind the oblique fissure (OF) and Right middle lobe (RML) is between the two. left lung has
an oblique fissure, separating it into left upper lobe (LUL) and left lower lobe (LLL).

Main Fissures. Separate lobes of lung

Oblique Fissure
o Commence at T4 or T5 & end at anterior CPA on the Right & 5 cm behind
from Rt CPA for the Lt.
Horizontal Fissure
o Extend from hilum to 6th rib at anterior axillary Line
All fissures seen on Lateral film.
Horizontal fissure can be visible on a PA film.

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3.8 Lung parenchyma

Lobar anatomy: Right lung has 3 lobes (upper, middle & lower), Left lung has 2
lobes (upper &lower lobes)
Causes of lung lucency
o Lung cysts & cavities
o Emphysema
o Bronchiectasis
o Pneumothorax
Causes of lung opacity
o Consolidation
o Atelectasis
o Infiltrations
o Nodule/ mass
o Fluid

i. Air space diseases

Consolidation
Filling of alveoli with liquid like substance which causes silhouetting of adjacent
structures.
Common etiologies: Pneumonia, pulmonary hemorrhage, ARDS, pulmonary edema,
aspiration, neoplasm
Air bronchograms: patent air ways filled with air; creating faint luceny with in the
consolidated lung. It tells that the opacity is intrapulmonary (not a pleural
pathology)

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Picture; Silhouette sign: Ill-defined heart border due to consolidation on the para cardiac area. The CXR
appearances reflect the loss of air, hence the increase in opacity.

Atelectasis / Collapse:

Loss of lung volume due to decreased aeration.


Direct signs are from lobar volume loss.
o Displacement of the fissures & vascular crowding.
Indirect signs are due to the effect of volume loss on adjacent structures.
o Elevation of the diaphragm
o Rib crowding on the side with volume loss
o Mediastinal shift to the side with volume loss
o Over inflation of adjacent or contralateral lobes
o Hilar displacement.

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ii. Mass

Interstitial infiltrates:

Nodular
Reticular/ Reticulonodular
Milliary: DDx- TB, Hemosiderosis, sarcoidosis, fungal, pneumoconiosis
Honeycomb pattern

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If the lesion measures less than 3 cm, it is called a nodule. If it is larger than 3
cm, it is called a mass.
A nodule/mass is caused by either a malignant (e.g. lung cancer, metastasis) or
benign process (e.g. hamartoma, granuloma).
Primary lung cancers tend to have ill-defined, speculated borders, and grow over
time. Metastases tend to produce multiple smooth round lung nodules, often of
variable size. Benign lesions tend to be small, well defined, smooth, round and
maybe calcified. They usually are stable in size when compared to prior films
A doubling of volume in less than 3 months is unlikely to be a neoplasm but
more likely an infective or inflammatory process.
Doubling times from 3 to 18 months are within the window for malignant lesions

Lung mass

Picture; CXR of an adult male with metastatic renal cell carcinoma. Note the multiple well defined “cannon
ball” metastases.

Lung ca: Tumors < 1 cm in diameter may not be visible on CXR. Cavitation is
most likely to be found in SCC (squamous cell carcinoma)

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Picture; left) Milliary pattern. Right) Honeycomb pattern representing lung scarring.

iii. Fibrosis

The CXR is an insensitive investigation for detecting pulmonary fibrosis.


HRCT can demonstrate mild to moderate degrees of fibrosis that are not detected
on CXR.
When fibrosis is apparent on CXR the cardinal feature is reticulation, a fine
network of lines, corresponding to fibrous thickening of the lung interstitium such
that it becomes visible on CXR
To make a diagnosis of fibrosis the other conditions that thicken the interstitium
such as interstitial edema in heart failure, lymphangitis carcinomatosis and alveolar
proteinosis, should be excluded or other evidence of fibrosis should be present.
The presence of volume loss in the region of reticulation and/or honeycomb
destruction supports a diagnosis of fibrosis.
Honeycomb destruction of the lung is primarily a feature of idiopathic pulmonary
fibrosis, is characteristically peripheral and basal in site and may be seen on CXR
if severe

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Picture; CXR of a pt with idiopathic pulmonary fibrosis. The magnified area demonstrates the interlacing
network of lines/ reticulation, which represent the visible pathologically thickened interstitium, in this case
due to fibrosis

iv. Lung opacity: Pulmonary edema

PA CXR: left) typical batwing distribution of air space disease. Right) 1. Vascular redistribution:
Cephalization (blood vessels in the upper lung zones become larger than the ones in lower lung zones
/the inverse of normal/), 2. Interstitial pattern and Kerly B lines, 3. Peribrochial cuffing (bronchi seen head
on are surrounded by fluid Blood diversion), 4. Pleural effusions, 5. Batwing pattern (symmetrical air space
disease in the lung adjacent to the hila)

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Picture; Kerley B lines (black arrow); Tiny horizontal lines seen at the periphery of the basal lung area,
perpendicular to the pleura…represent fluid in the interlobular septa

v. Cavity

Gas filled space surrounded by complete wall. It has a thick, irregular wall, often
with a solid mural component.
Solitary cavity: most likely infection or primary lung cancer, post traumatic
Multiple cavitary lesions are typically vascular or spread through the vascular
system. DDX are: Aspiration lung abscess, TB, Septic emboli, Vasculitis (Wagner’s
granulomatosis), metastases

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Pictures; left) Right upper lobe large cavity. Middle) Multiple cavity: Bilateral thin walled cavities…cancer.
Right) Lung abscess: air–fluid level
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Cavity location:
o TB: Upper zone
o Lung abscess: Right lower zone
o Amoebic lung abscess: Right basal lung
o Pulmonary infarction: Basal
Cavity wall:
o Thick- neoplasm, acute abscess, wegner’s granulomatosis
o Thin wall- Usually benign e.g. bullae, pneumatocele, hydatid cyst, Chronic
inactive TB, traumatic lung cyst
o Shaggy inner wall – abscess
o Irregular & nodular – cancer
o Presence of air fluid level – lung abscess, empyema, TB, cavitating ca
o Presence of ball inside cavity- Aspergilloma in an old cavity
Note: A cyst may be confused with cavity.

In general, thin-walled cavities (5 mm) tend to be infective and, when thick-walled


(10 mm), SCC of the lung enters into the DDX.
After a suspected aspiration, chest x-ray abnormalities typically appear within two
hours.

vi. Lung cyst

Cyst is an air-containing lucency with a thin, nearly imperceptible wall. usually due
to a primary airway abnormality (e.g. Emphysema, bronchiectasis)
DDx for a single cyst:
o Bulla: an air-filled cyst measuring >1 cm
o Bleb: an air-filled cystic structure contiguous with the pleura measuring <1
cm.
N.B Rupture of a bleb is commonest cause of spontaneous pneumothorax.
Pneumatocele: is an air-filled space caused by prior lung trauma or as a
sequela of pneumonia, typically from A long-term sequel of S. aureus or PCP.
Pneumatoceles almost always resolve
The appearance is similar to that of a cavity, but thin walled with no adjacent lung
parenchymal opacity to suggest active inflammation

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Picture; A pneumatocele in a patient who had a staphylococcal pneumonia as a child. Note the thin wall,
the entirety of which is visible (white arrows), unlike the wall of a bulla. NO adjacent parenchymal opacity
to suggest active inflammation

vii. Bullous emphysema

Bullous emphysema is characterized by bullae, which cause areas of absence or


paucity of lung markings. Only a proportion of the wall of the bulla is usually
visible creating thin curvilinear lines

Picture; CXR of a pt with bullous emphysema. Note the curvilinear lines (arrows) formed by the walls of
the bullae, but the entire wall is not visible.
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3.9. Heart and mediastinum

a. Heart

Central dense shadow


Cardiac shadow-2/3rd Left side, 1/3rd Right side
Cardiac silhouette: boundary is (look at picture below)
o Right border – IVC, RA, SVC
o Left border – Aortic arch, pulmonary bay, LV, LA appendage

Picture; Cardiac silhouette

Normal cardiothoracic ratio is 35 - 50 % (look at picture below)


o Draw a midline (vertical line) along the spinous processes. Take the
maximum distance formed by the cardiac silhouette on both sides (A & B
on the picture), add them and divide for total thoracic diameter (C on the
picture). Multiply by 100%
𝐀+𝐁
▪ Cardiothoracic ratio = 𝐱 𝟏𝟎𝟎 % = 35-50%, If > 50 % -
𝐂
cardiomegaly

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𝐀+𝐁
Picture; cardiothoracic ratio = 𝐱 𝟏𝟎𝟎 % = 35-50%, If > 50 % - cardiomegaly
𝐂

Heart size will vary with body habitus making absolute lower limits meaningless,
but reasonable upper limits for adults are 15.5 cm for females and 16 cm for
males.
Look for evidences of chamber enlargement
o LA – splaying of carina, straightening of Left heart border, double Right
heart border, posterior displacement of esophagus
o RA – lateral bulging & clear outline of Rt heart border
o LVH – left & downwards displacement of the apex
o RVH – Narrowing of the anterior retrosternal clear space on lateral CXR.
Round apex with upward and lateral displacement. Obliteration of pulmonary
bay b/c of pulmonary artery enlargement
o LA or RA enlargement & LVH can be seen on P-A CXR; RVH is seen on
lateral CXR (causes narrowing of the anterior retrosternal clear space)

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Picture: CXR of A pt with early left heart failure. The magnified view demonstrates the double heart
border, right atrial wall (white arrow) and left atrial wall (black arrow). Double right heart border: caused by
the projection of the right wall of the left atrium behind the silhouette of the right atrium

Pericardial effusion

Pericardial effusions are difficult to appreciate on CXR. The most obvious signs
are a change in the shape of the heart to a more rounded contour (the globular
heart) and a rapid increase in size of the cardiac silhouette.
If pericardial fluid is >250 ml, it may be seen on CXR
o “Flask shaped’’ or ‘’water bottle heart’’ on erect PA film
o Globular when supine film
Pericardial calcifications: appear as curvilinear calcification on the surface of the
heart.
Causes of pericardial calcification
Pericarditis (TB, rheumatic fever, viruses)
Post-traumatic

Picture; A water bottle heart

b. Mediastinum:

Encompasses midline thoracic structures that are delineated by mediastinal pleura,


the diaphragm, the sternum, the spine, and the thoracic inlet.
Divided into Anterior, Middle (visceral) and Posterior (paraspinal) compartments

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Picture; Components of the PA mediastinal shadow (A): SVC (1), Ascending aorta (2), RA (3), IVC (4),
aortic arch (5), pulmonary trunk (6), LA appendage (7) and, LV (8). Mediastinal compartments on the
lateral film (B) include: superior(S), anterior (A), middle (M) and posterior (P) compartments

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21.4. CXR features of common lung pathologies

Pneumonia

Lobar Pneumonia

Commences as localized infection of terminal air space


Uniform consolidation of all or part of a lobe
Homogenous opacity limited by the fissure
Normal lung volume
Air bronchogram seen

Pictures; Left) Frontal CXR of an adult male with pneumonia confined to the anterior segment of the right
upper lobe. Note the inferior demarcation by the minor fissure (white arrows). Right) Atypical pneumonia;
Poorly-defined nodular opacities in RLL zone in a pt with Mycoplasma pneumoniae pneumonia.

Broncho Pneumonia

Causes patchy consolidation


It Is a multifocal process which commences at terminal & respiratory
bronchioles; tend to spread segmentally

Acute hypersensitivity pneumonitis

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Picture; A frontal CXR of an adult female diagnosed with acute hypersensitivity pneumonitis. Note the
patchy ground grass opacity.

Pulmonary TB

Primary TB:

Consolidation, hilar LAP, effusion & milliary disease May occur in any lobe, but
most typical locations are the lower lobes or right middle lobe.
Classic imaging findings are not always seen, but include:
o Ghon focus: Initial focus of parenchymal infection, usually located in upper
part of lower lobe or lower part of upper lobe.
o Ranke complex: Ghon focus and LAP
Cavitation is rare

Picture; The Primary complex (Ghon focus & ipsilateral hilar LAP) … Right lower lobe peripheral air space
opacity & Right hilar adenopathy

Because most inspired air is distributed to the middle and lower lung zones, these
areas of the lungs are most commonly involved in primary TB

Reactivation TB
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Upper lobe consolidation with cavity ± fibrosis


Usually lacks LAP
May have Pleural effusion/empyema
It is usually localized to the apical and posterior segments of the upper lobes,
where the substantially higher mean oxygen tension (compared with that in the
lower zones) favors mycobacterial growth
Miliary TB: It can occur in primary or reactivation TB. diffuse random distribution of
tiny nodules seen in hematogenous disseminated TB
Healed TB appears as apical scarring, usually with upper lobe volume loss and
superior hilar retraction.
Calcified granulomas may be present as well, which indicate containment of the
initial infection by a delayed hypersensitivity response

Pictures; left) Right upper lobe large cavity. Right) Upper lobe consolidation with cavitation

Bronchiectasis

Bronchiectasis is defined by the presence of dilated bronchi with thickened walls.


CXR is insensitive for the detection of bronchiectasis with only severe disease
being identified with any certainty.
Bronchiectasis is descriptively divided into 3 types; cylindrical, varicose and cystic.
Chest CT is more specific for bronchiectasis and is the imaging modality of choice
for confirming the diagnosis.
CT findings include airway dilation (detected as parallel "tram tracks" or as the
"signet-ring sign"—a cross-sectional area of the airway with a diameter at least 1.5
times that of the adjacent vessel), lack of bronchial tapering (including the
presence of tubular structures within 1 cm from the pleural surface), bronchial wall
thickening in dilated airways, inspissated secretions (e.g., the "tree-in-bud" pattern),
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or cysts emanating from the bronchial wall (especially pronounced in cystic


bronchiectasis

Picture; CXR of a pt with cylindrical bronchiectasis, on the magnified image are ring shadows (white
arrows) and tram tracks or lines (black arrows), representing dilated bronchi end on and lengthways
respectively

Picture; Chest CT; Airway dilation (detected as parallel "tram tracks" or as the "signet-ring sign"—a cross-
sectional area of the airway)

COPD
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Emphysema

Pictures; A) Hyperlucent, Hyperinflated lungs, Avascular zones. Sometimes, ball-shaped collections of air
develop, which are called bullae. On the radiograph, there is an overall decrease in lung density (too
black). This makes sense since the fluid density alveolar walls are being destroyed and air is trapped in
the lungs. Also, because of tissue destruction, there are fewer visible blood vessels. Ones that are seen
sometimes take an abnormal curved course because they are going around destroyed lung. B) Lateral
CXR: flattened hemidiaphragms and barrel chest deformity.

PCP

CXR findings can be normal


Classic finding is bilateral perihilar (central) airspace opacities with peripheral
sparing.
There is a propensity to cause upper lobe pneumatoceles, which may predispose
to pneumothorax or pneumomediastinum.

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ILD: Silicosis

Picture; A pt with silicosis: variably sized, poorly defined nodules (arrows) predominating in the upper lobes

ARDS

Picture; AP CXR of ARDS that shows diffuse interstitial and alveolar infiltrates, that can be difficult to
distinguish from LV failure. BUT the heart size is normal

Pulmonary edema

Vascular redistribution: cephalization of the vessels


Interstitial edema, peri bronchial cuffing, and Kerley B and A lines. 1466
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o Kerley B lines: seen at the peripheral lung; due to thickened interlobular


septa.
o Kerley A lines radiate outward from the hila and may represent dilation of
lymphatic channels.
Alveolar edema
o Bilateral perihilar opacifications
o Bat wing/ butterfly appearance when severe
o Pleural effusions and cardiomegaly are often present.

Note: pulmonary edema is usually symmetric and dependent

Acute PTE

The CXR is often normal.


Sometimes a focal, black, wedge-shaped area is seen representing infarcted sub-
segmental areas of lung that may cavitate, as blood does not fill the blood
vessels after the embolism.
o Focal oligemia (Westermark's sign)… Paucity of vascular markings in the
region of the PE.
o A peripheral white wedge-shaped area of air space disease is seen due to
post-obstruction infarction (Hampton's hump).
An enlarged right descending pulmonary artery (Palla's sign).
Nonspecific signs include atelectasis and pleural effusion.
The development of pulmonary arterial hypertension may be evident with prominent
proximal pulmonary arteries

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Picture; Wedge shaped Pulmonary infarct

Pleural based mass

If the medial margin is visible, but the lateral margin is indistinct, the mass is
probably pleural based

picture; Left image demonstrates a pleural based mass, in this case mesothelioma. Note on the magnified
image the well-defined medial margin (white arrows) where the mass is adjacent to the lung and the
merging of the upper border with the chest wall (black arrow).

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Chapter 22; Basics of ECG and ECG


interpretation
Dr. Mulualem. G

22.1 ECG
❖ Electrocardiography (ECG/EKG) is the process of recording the electrical activity of
the heart over a period of time using electrodes placed on the skin through ECG
machine.
❖ The term Electrocardiography is derived from three Greek words. Electro = related
to electrical activity, Kardio = for heart and graph = to write
❖ The graph of voltage vs time produced by this noninvasive procedure is referred to
as electrocardiogram (ECG/EKG). That is a surface representation of the electrical
events of the cardiac cycle.
❖ The ECG is the most important test for interpretation of the cardiac rhythm,
conduction system abnormalities, and the detection of myocardial ischemia.

Fig; The Normal Conduction System

The sinoatrial (SA) and atrioventricular (AV) nodes generate a slow


action potential, mediated by calcium ions. In comparison, the tissues
of the atria, ventricles, and the His-Purkinje system generate a fast
action potential mediated by sodium ions. Sequential activation of
these structures results in the characteristic waveforms visible on the
surface electrocardiogram (ECG). The AV node and bundle of His are
small structures; as a result, no electrical activity is recorded on the
surface ECG during their activation.

Cardiac impulse
 Cardiac impulse originates in the SA node
 Traverses the atria simultaneously – no special conduction wires in atria – so the
delay
 Reaches AV node – the check post – so delay
 Enters bundle of His and branches – through specialized conducting wires called
Purkinje network - activates both ventricles – quick QRS
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 First the septum from L to R, then right ventricle and then the left ventricle and
finally the apex
 Then the ventricles recover for next impulse

Indication for ECG


❖ Detection of MI and evaluation of other types of Structural heart disease including
VHD, CMP, pericarditis, HHD...
❖ Cardiac dysrhythmia
❖ Pulmonary Embolism
❖ Electrolyte abnormalities like hyperkalemia
❖ To monitor drug treatment and toxicity (specifically antiarrhythmic therapy. e.g.
drug induced QT prolongation) and to detect metabolic disturbances.
❖ Monitoring for general anesthesia (pre op, intra op and post op monitoring)
❖ Old age with DM or HTN
❖ Cardiac stress testing
❖ Before CTA and MRA of the heart

22.2. ECG Leads and electrodes

Electrode is a conductive pad in contact with the body that makes an electrical circuit
with the ECG.
✓ On a standard 12-lead ECG there are 10 electrodes (RA, LA, RL, LL, V1-V6)
A lead is usually more abstract and is the source of measurement of vector.
✓ 12 lead ECG has 3 sets of leads
a. 3 standard limb leads (I, II, III)
b. 3 augmented limb leads (aVR, aVF, aVL),
c. 6 precordial (chest) leads (V1- V6)
✓ Cardiac Monitors→ usually limb leads
In clinical practice the term lead and electrode are used interchangeably, although
this is not technically correct.
(aVR = lead augmented vector right, aVL = lead augmented vector left, aVF = lead
augmented vector foot, RA = right arm, LA = left arm, RL = right leg, LL = left leg, V1-
V6 = vector 1 – vector 6)

ECG leads – Standard and augmented leads


❖ I -potential difference between Left hand electrode and right-hand electrode (lateral
LV)
❖ II- potential difference between Left foot electrode and right-hand electrode (inferior
LV)
❖ III- potential difference between Left hand electrode and left foot electrode (inferior
LV)
❖ aVR- Right hand electrode and center of heart
❖ aVL- Left hand electrode and center of heart(lateral)
❖ aVF- Left foot electrode and center of heart(inferior)
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Standard Limb Leads Augmented Limb Leads All Limb Leads

Placement of precordial leads over the chest

Fig; Precordial Leads


1. V1 (Red) → at 4th Right ICS, just right to the sternum
2. V2 (Yellow) → at 4th left ICS, just left to the sternum
3. V3 (Green) → Midway Between V2 and V4
4. V4 (Brown) → at 5th left ICS, along the MCL (place V4 before placing v3 to the
chest wall)
5. V5 (black) → at 5th left ICS, along the AAL or halfway between V4 and V6 if the
anterior axillary line is unclear.
6. V6 (violet) → at 5th left ICS, along the MAL 1471
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Placement of Limb leads


❖ Limb lead electrodes are placed on the arms and legs distal to the shoulders and
hips.
1. RL (black) → On the right leg, Avoid thick muscles
2. LL (Green) → On the left leg, in the same location where RL is placed
3. LA (Yellow) → On the left arm
4. RA (Red) → On the right arm in the same location where LA is placed

Tip → recognize the colors for fast placement


Majority of ECG machines available in our
setup have these colors (Europe form)

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Summary of Leads
Limb Leads Precordial Leads
Bipolar I, II, III (standard limb leads)
Unipolar aVR, aVL, aVF (augmented V1-V6
limb leads)
Category of leads
Category Leads Activity
Inferior II, III, aVF Look at electrical activity from the
leads inferior (diaphragmatic) surface of
heart. E.g. inferior MI
Lateral I, aVL, V5, V6 Look at electrical activity from the
leads lateral wall of LV. E.g. LVH
Septal V1, V2 Look at electrical activity from the
leads septal surface of heart
/interventricular septum/. E.g. septal
wall hypertrophy
Anterior V3, V4 Look at electrical activity from the
leads anterior wall of RV and LV
(sternocostal surface of the heart).
E.g anterior MI
Posterior V7, V8, V9 Acute posterior wall MI induces ST
leads elevations in leads placed over the
back of the heart

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Arrangement of Leads on the ECG Paper

22.3. ECG GRID

❖ ECG is a plot of voltage on the vertical axis against time on the horizontal axis.
❖ The ECG waves are recorded on special graph paper that is divided into 1 mm2 grid-
like boxes (figure 1).
❖ The ECG paper speed is ordinarily 25 mm/sec. As a result, each 1 mm (small)
horizontal box corresponds to 0.04 second (40 ms), with heavier lines forming larger
boxes that include five small boxes and hence represent 0.20 sec (200 ms) intervals.

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❖ On occasion, the paper speed is increased to 50 mm/sec to better define waveforms.
In this situation, there are only six leads per sheet of paper. Each large box is
therefore only 0.10 sec and each small box is only 0.02 sec. In addition, the heart
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rate appears to be one-half of what is recorded at 25 mm/sec paper speed, and all
of the ECG intervals are twice as long as normal. Other paper speeds are
occasionally used.
❖ Vertically, the ECG graph measures the height (amplitude) of a given wave or
deflection, as 10 mm (10 small boxes) equals 1 mV with standard calibration.
❖ On occasion, particularly when the waveforms are small, double standard is used (20
mm equals 1 mv).
❖ When the wave forms are very large, half standard may be used (5 mm equals 1
mv).
❖ Paper speed and voltage are usually printed on the bottom of the ECG.

Paper speed 25mm/sec

figure 1 1475
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Summary
▪ X-Axis represents time - Scale; X-Axis → 1 mm = 0.04 sec
▪ Y-Axis represents voltage - Scale; Y-Axis → 1 mm = 0.1 mV
▪ One big square on X-Axis = 0.2 sec (big box)
▪ Two big squares on Y-Axis = 1 milli volt (mV)
▪ Each small square is 0.04 sec (1 mm in size)
▪ Each big square on the ECG represents 5 small squares = 0.04 x 5 = 0.2 seconds
▪ 5 such big squares = 0.2 x 5 = 1sec = 25 mm
▪ One second is 25 mm or 5 big squares
▪ One minute is 5 x 60 = 300 big squares

22.4. ECG COMPLEXES AND INTERVALS

Table; ECG Complex


Wave or Description Duration Amplitude Some abnormality examples
Interval
P wave  The sequential activation of the right  <0.12 sec (3 small  <0.25 mv  Picked - >3mm shows right atria
and left atrium (atrial depolarization). boxes) (2.5 small enlargement
boxes)  Wide and bifid: > 0.12 sec
and bifid shows left atrial
enlargement
QRS  QRS complex shows Right and left  Normal duration of   Wide QRS Complex represent
complex ventricular depolarization QRS complex is o Bundle branch block
0.06 to 0.10 o Ventricular pre-excitation
seconds (1½ to o Ventricular pacing
2½ small boxes). o Ventricular tachycardia
 Doesn’t affected by o Hyperkalemia
heart rate  Wide QRS with normal rate →
Q wave  Septal  < 0.04 sec (1  < 3 mm (<3 bundle branch block
depolarization small box) small  Regular wide QRS with
boxes) tachycardia → Ventricular
tachycardia /hyperkalemia

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R wave  Ventricular   < 15 mm
contraction (<15 small  Wide QRS with increased voltage →
boxes) left or right ventricular
hypertrophy.
S wave  Complimentary to  
 A narrow QRS complex (<0.06 sec) →
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Chapter 22; Basics of ECG and ECG interpretation 1477

R supraventricular tachycardia
[SVT]).
 Prominent Q waves are a
characteristic finding in myocardial
infarction
ST  Electrical silence  Isoelectric  A normal  ST segment elevation > 2mm (>
segment  Measured from the end of QRS  0.08 to 0.12 sec ST segment 2 small square) above the
complex to the beginning of T wave (2-3 small boxes) is flat along baseline or Depression of >1
on the isoelectric line the mm (> 1 small square) below the
isoelectric baseline may be indicative of MI.
line
T wave  Ventricular repolarization  0.08 to 0.12 sec  amplitude is  Tall peaked T waves indicate
 Friend of ST (2-3 small boxes) variable. hyperkalemia.
 Inverted T waves are suggestive
of myocardial ischemia or a
ventricular conduction delay.
 T waves that are larger or
smaller than normal may indicate
and electrolyte imbalance.

U wave  A small rounded positive gradual or    Prominent U waves may be drug


abrupt slope after the T wave and related or indicate hypokalemia
occurs before the P wave.
 Not usually present on an ECG
unless the heart rate is slow.
 Represents Purkinge fiber
repolarization
TP  Ventricular relaxation  shortened in  
segment tachycardia
PR  Time interval from onset of atrial  0.12 to 0.20 sec   Long PR intervals are usually seen
interval depolarization to onset of ventricular (3-5 small boxes). in first degree AV block, Acute
depolarization.  The length of the Rheumatic Fever, Hyperkalemia
 It is measured from the beginning of PR interval but there may be other causes.
the P wave to the first part of the changes with heart  Short PR intervals are suggestive of
QRS complex (which may be a Q rate. Wolff-Parkinson-White syndrome
wave or R wave).
QT  Duration of ventricular depolarization  0.36-0.44 seconds   A prolonged QT interval may
INTERVAL and repolarization (<10 small boxes indicate prolonged ventricular
 Measured from the beginning of the or 2 large squares) repolarization and relative
Q wave to the end of the T wave refractory period. It can be
on the isoelectric line caused by some of the
o Cardiac drugs
o Hypocalcemia
o MI
o Myocarditis or pericarditis,
and
o LVH.
 A shortened QT may indicate
o Hypercalcemia or
o Be seen in patients taking
digitalis.
RR  Duration of ventricular cardiac cycle  0.80 sec (20 small  
interval  Used to check rhythm of cardiac boxes or 4 large
cycle squares)

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Figure; Formation of the major deflections on the ECG

The electrical impulse is initiated in the sinus node and then activates the
right and left atria, generating the P wave. Impulse conduction through the
atrioventricular (AV) node and bundle of His, which are small structures,
does not generate any ECG activity; this period of "electrical silence" is
the PR interval. The first part of the ventricle to be depolarized is the left
side of the interventricular septum, producing a small septal Q wave,
followed by depolarization of the remainder of the ventricular myocardium,
generating the full QRS complex. The T wave represents ventricular
repolarization. A U wave may be present, representing repolarization of
the His Purkinje system.

❖ ECG is composed of several different waveforms that represent electrical events


during each cardiac cycle in various parts of the heart (figure 2).
❖ ECG waves are labeled alphabetically starting with the P wave, followed by the QRS
complex and the ST-T-U complex (ST segment, T wave, and U wave).
❖ The J point is the junction between the end of the QRS and the beginning of the ST
segment (waveform 1).

Figure 2

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(waveform 1)

A. P wave

The P wave represents atrial depolarization.


The normal sinus P wave demonstrates depolarization from the right to left atrium
and is an initial low amplitude deflection preceding the QRS complex that is positive
in most leads.
The duration is generally <0.12 sec (3 small boxes) and the amplitude <0.25 mv (2.5
small boxes).
Since right atrial depolarization precedes that of the left atrium (as the sinus node is
in the high right atrium), the P wave is often notched in the limb leads and usually
biphasic in lead V1.
The initial positive deflection in V1 is due to right atrial depolarization that is directed
anteriorly, while the second negative deflection represents left atrial depolarization that
is directed posteriorly.
The atrial repolarization sequence (atrial ST and T wave phases) occurs just before,
simultaneously, and just after depolarization of the ventricular myocardium.
The atrial "T wave" itself is usually hidden by the QRS complex and not observed on
the routine ECG.
In addition, the amplitude of the atrial T wave is often too small to be observed at
standard gain.
Clinically, atrial repolarization (the atrial ST phase) is most evident during acute
pericarditis, in which one often sees PR segment elevation in lead aVR and PR
segment depression in the infero-lateral leads, reflecting an atrial current of injury.
The low amplitude atrial T wave may also be unmasked in certain cases of high
degree AV block, especially when the atria are enlarged.
Finally, alterations in the atrial ST segment and T wave may occur with other
pathologies, such as atrial infarction or atrial tumor invasion.
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B. QRS complex

✓ The QRS complex represents the time for ventricular depolarization.


✓ The entire QRS duration normally lasts for 0.06 to 0.10 seconds (1½ to 2½ small
boxes) and is not influenced by heart rate.
✓ If the initial deflection is negative, it is termed a Q wave.
✓ Small Q waves are often seen in leads I, aVL, and V4-V6 as a result of initial septal
depolarization and are considered normal.
✓ The first positive deflection of the QRS complex is called the R wave. It represents
depolarization of the left ventricular myocardium.
✓ Right ventricular depolarization is obscured because the left ventricular myocardial
mass is much greater than that of the right ventricle.
✓ The small R wave in lead V1 represents initial septal depolarization.
✓ The negative deflection following the R wave is the S wave, which represents
terminal depolarization of the high lateral wall.
✓ If there is a second positive deflection, it is known as an R'.
✓ Lower case letters (q, r, or s) are used for relatively small amplitude waves of less
than 0.5 mV (less than 5 mm with standard calibration).
✓ An entirely negative QRS complex is called a QS wave.
✓ The R wave should progress in size across the precordial leads V1-V6.
✓ Normally there is a small R wave in lead V1 with a deep S wave.
✓ The R wave amplitude should increase in size until V4-V6 while the S wave becomes
less deep. This is termed R wave progression across the precordium.

C. ST segment

❖ The ST segment occurs after ventricular depolarization has ended and before
repolarization has begun.
❖ It is a time of electrocardiographic silence.
❖ The intersection of the end of the QRS complex and the initial part of the ST
segment is termed the J point (waveform 1 above).
❖ Has a duration of 0.08 to 0.12 sec,
❖ The normal ST segment is usually flat along the isoelectric line (i.e. zero potential as
identified by the T-P segment) and has a slight upward concavity. However, it may
have other configurations depending upon associated disease states (e.g. ischemia,
acute MI, or pericarditis). In these situations, the ST segment may be flattened,
depressed (below the isoelectric line) with an upsloping, horizontal, or down sloping
morphology, or elevated in a concave or convex direction (above the isoelectric line).
❖ ST elevation of greater than 2mm (> 2 small square) above the baseline or
depression of greater than 1 mm (> 1 small square) below the baseline may be
indicative of an MI
❖ In some normal cases (as with sinus tachycardia) the J point is depressed and the
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ST segment is rapidly upsloping, becoming isoelectric within 0.08 seconds after the
end of the QRS complex.
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❖ For more Look at ECG CRITERIA FOR MYOCARDIAL ISCHEMIA/INFARCT below

D. T wave

The T wave represents the period of ventricular repolarization.


Since the rate of repolarization is slower than depolarization, the T wave is broad,
has a slow upstroke, and rapidly returns to the isoelectric line following its peak (i.e.
slow upstroke, rapid downstroke). Thus, the T wave is asymmetric and the amplitude
is variable.
In addition, the T wave is usually smooth up and down.
The duration is 0.08 to 0.12 sec (2-3 small boxes)
If there is any irregularity on the T wave (bump, notch, rippled, etc) a superimposed
P wave should be considered.
the T wave vector on the ECG normally is in the same direction as the major
deflection of the QRS Since depolarization begins at the endocardial surface and
spreads to the epicardium, while repolarization begins at the epicardial surface and
spreads to the endocardium, the direction of ventricular depolarization is opposite to
that of ventricular repolarization.
Tall peaked T waves indicate hyperkalemia. Inverted T waves are suggestive of
myocardial ischemia or a ventricular conduction delay. T waves that are larger or
smaller than normal may indicate and electrolyte imbalance.

E. PR interval

✓ The PR interval includes the P wave as well as the PR segment.


✓ It is measured from the beginning of the P wave to the first part of the QRS
complex (which may be a Q wave or R wave).
✓ It includes time for atrial depolarization (the P wave) and conduction through the AV
node and the His-Purkinje system (which constitute the PR segment).
✓ The length of the PR interval changes with heart rate, but is normally 0.12 to 0.20
sec (3 – 5 small boxes).
✓ The PR interval is shorter at faster heart rates due to sympathetically mediated
enhancement of atrioventricular (AV) nodal conduction; it is longer when the rate is
slowed as a consequence of slower AV nodal conduction resulting from withdrawal of
sympathetic tone or an increase in vagal inputs.

F. QT interval

❖ The QT interval consists of the QRS complex, the ST segment, and T wave. Thus,
the QT interval is primarily a measure of ventricular repolarization.
❖ The JT interval, which does not include the QRS complex, is a more accurate
measure of ventricular repolarization since it does not include ventricular
depolarization, but in most clinical situations, the QT interval is used.
❖ If the QRS complex duration is increased, this will lead to an increase in QT interval
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❖ A widened QRS, therefore, must be considered if a prolonged QT interval is being


evaluated.
❖ The time for ventricular repolarization and therefore the QT (or JT) interval is
dependent upon the heart rate; it is shorter at faster heart rates and longer when the
rate is slower.
❖ Thus, a QT interval that is corrected for heart rate (QTc) is often calculated as
follows (based on Bazett's formula):
𝐐𝐓 𝐢𝐧𝐭𝐞𝐫𝐯𝐚𝐥
QTc =
√𝐓𝐡𝐞 𝐑𝐑 𝐢𝐧𝐭𝐞𝐫𝐯𝐚𝐥 (𝐢𝐧 𝐬𝐞𝐜)
✓ Although this approach is simple, it is inaccurate at heart rate extremes and
results in overcorrecting at high rates and under correcting at low ones [1].
✓ The normal value for the QTc in men is ≤0.44 sec and in women is ≤0.45 to
0.46 sec.
✓ QTc values, however, are on a bell curve and normal patients may have longer
QTc values, while those with Long QT syndrome may have shorter QT values.
❖ Since the QRS widens in the setting of a bundle branch block, the QT interval will
widen.
❖ This increase in QT interval does not reflect an abnormality of ventricular
repolarization, since the increase is due to an abnormality of depolarization.

G. U wave

➢ U wave may be seen in some leads, especially the precordial leads V2 to V4.
➢ The exact cause of this wave is uncertain, though data suggest it may be from late
repolarization of the mid-myocardial M cells, due to a longer action potential duration
compared with the endocardium or epicardium, especially at slow heart rates.
➢ The amplitude of the U wave is typically less than 0.2 mV and is clearly separate
from the T wave. It is more evident in some circumstances such as hypokalemia and
bradycardia.
➢ The U wave may merge with the T wave when the QT interval is prolonged (a QT-U
wave), or may become very obvious when the QT or JT interval is shortened (eg,
with digoxin or hypercalcemia).

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22.5. APPROACH TO ECG INTERPRETATION

❖ A systematic approach to interpret an electrocardiogram (ECG) is essential for correct


diagnosis
✓ Step 1: Rate
✓ Step 2: Rhythm
✓ Step 3: Axis determination
✓ Step 4: Intervals
✓ Step 5: P wave
✓ Step 6: QRS complex
✓ Step 7: ST segment-T wave
✓ Step 8: Overall interpretation

22.5.1. Determining the Heart Rate


A rate of 60 to 100 is considered normal. A rate less than 60 is bradycardia, while a
rate over 100 is tachycardia
There are Three methods of determining heart rate
A. Rule of 300
B. Count Small Boxes
C. 10 Second Rule

A. Method 1; Rule of 300

❖ If the cardiac rhythm is regular, the interval between successive QRS complexes
determined from the ECG grid can be used to determine heart rate.
❖ The division of 300 by the number of large boxes calculates the heart rate/HR/.

𝟑𝟎𝟎
𝐇𝐑 =
𝐧𝐮𝐦𝐛𝐞𝐫 𝐨𝐟 𝐥𝐚𝐫𝐠𝐞 𝐛𝐨𝐱𝐞𝐬 (between successive QRS complexes)

For example;
interval between two successive heart rate
complexes
1 large box 300 ÷ 1 = 300 beats/min
2 large boxes 300 ÷ 2 = 150 beats/min
3 large boxes 300 ÷ 3 = 100 beats/min
4 large boxes etc 300 ÷ 4 = 75 beats/min

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❖ Alternatively, the time between QRS complexes can be measured in seconds. This
number can be divided into 60 to derive the heart rate.

𝟔𝟎
𝐇𝐑 =
𝐭𝐢𝐦𝐞(𝐢𝐧 𝐬𝐞𝐜) 𝐛𝐞𝐭𝐰𝐞𝐞𝐧 𝐐𝐑𝐒 𝐜𝐨𝐦𝐩𝐥𝐞𝐱𝐞𝐬

✓ For instance, if the time between 2 QRS complexes is 0.75 seconds, the heart
rate is 80 beats/min (60 seconds/minute ÷ 0.75 seconds/beat = 80 beats/min).

❖ Although fast, this method only works for regular rhythms.

Example 1

heart rate = 300 / 6 = 50 bpm

Example 2

heart rate = 300 / ~ 4 = ~ 75 bpm

Example 3

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heart rate = 300 / 1.5 = 200 bpm

B. Method 2; Count Small Boxes

➢ Sometimes it is necessary to count the number of small boxes between two R waves for fast
heart rates.
➢ That number is divided into 1500 to calculate bpm.
➢ Remember: 60 sec/min divided by 0.04 sec/small box = 1500 small boxes/min.
➢ Examples: If there are six small boxes between two R waves: 1500/6 = 250 bpm.
➢ If there are ten small boxes between two R waves: 1500/10 = 150 bpm.

C. Method 3; 10 Second Rule

If the rhythm is irregular, the simplest way to determine the rate is by counting the
number of complexes on the ECG and multiplying by six, since the standard ECG
displays 10 seconds of time (As most EKGs record 10 seconds of rhythm per page).
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✓ HR = 6 X total number of QRS complexes on the ECG

This method works well for irregular rhythms.

Examples

Using 6-sec ECG rhythm strip to calculate heart rate. Formula: 7 x 6 = 42 bpm
♥ Clinical Tip: If a rhythm is extremely irregular, it is best to count the number of R-R
intervals per 60 sec (1 min).

HR = 33 x 6 = 198 bpm

Regular rate abnormality examples

Sinus tachycardia occurs at rates of 100 to 180


Atrial tachycardia, AV nodal re-entrant tachycardia, or AV reciprocating tachycardia
occur at rates of 140 to 220
Atrial rates of 260 to 320 are seen with atrial flutter.

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Sinus tachycardia (HR = 300 ÷ 1.5 = 200 bpm)

Sinus bradycardia (HR = 300 ÷ 7 = 43 bpm)

22.5.2. Rhythm Analysis


✓ Calipers are extremely helpful for rhythm analysis.
❖ Step 1: Check the regularity of the QRS complexes
❖ Step 2: Locate the P wave
❖ Step 3: Establish the relationship between P waves and the QRS complex

Step 1: check the regularity of the QRS complexes

 Paper and Pencil Method


 Caliper Method

Do the QRS complexes occur with regular intervals or are they irregular?
If the complexes are irregular
✓ Is there a pattern to the irregularity? Is the rhythm regularly irregular (i.e. there
is a repeating pattern of irregularity) or is the rhythm irregularly irregular
without any pattern of irregularity?
✓ At least 5 supraventricular rhythms are irregularly irregular:
1. Sinus arrhythmia (in which there is only one P wave morphology and a
stable PR interval)
2. Sinus rhythm with premature atrial contractions
3. Sinus or other rhythm with variable AV block
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4. Multifocal atrial rhythm (wandering atrial pacemaker) when the rate is


<100 or multifocal atrial tachycardia with a rate >100 (in which there are
≥3 different P wave morphologies and PR intervals); or
5. Atrial fibrillation (in which there is no organized electrical activity).

Step 2: Locate the P wave

Are P waves visible? Are they regular?


✓ Absence of P waves may occur secondary to atrial fibrillation.
✓ Alternatively, P waves may be present but not visible if they are simultaneous with
and buried within the QRS complex as in a junctional rhythm or atrioventricular (AV)
nodal re-entrant tachycardia.
✓ In addition, they may be located within the ST segment as with an AV reciprocating
tachycardia or ventricular tachycardia.
✓ If a P wave is halfway between two QRS complexes, a second P wave is often
buried within the QRS complex.

Step 3: Establish the relationship between P waves and the QRS complex

Are the P waves associated with QRS complexes in a 1:1 fashion? Do the P waves
precede each QRS complex as is the case with most normal rhythms?
✓ If not, are there more or less P waves than QRS complexes and what are the
atrial and ventricular rates?
✓ If there are more P waves than QRS complexes, then some form of AV block
is present, which may be physiologic if there is a concomitant atrial tachycardia
or flutter.
✓ If there are more QRS complexes than P waves, then the rhythm is an
accelerated ventricular or junctional rhythm.
Do P waves occur after each QRS complex (i.e. retrograde P waves) What is the
morphology? Are they upright or inverted? Are they all the same in shape and size?
Are the irregular P waves associated with ectopic beats?
 upright and rounded in lead II the P Waves are usually originating from the SA
node, indicating a sinus rhythm.

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A. Regular rhythm

Normal Sinus Rhythm

Implies normal sequence of conduction, originating in the sinus node and proceeding
to the ventricles via the AV node and His-Purkinje system.
ECG Characteristics:
✓ Rate 60-100 bpm
✓ Regular narrow-complex rhythm
✓ Each QRS complex is proceeded by a P wave
✓ Narrow QRS complex
✓ P wave is upright in lead II & down going in lead aVR

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Rate: Normal (60–100 bpm)


Rhythm: Regular
P Waves: Normal (upright and uniform)
PR Interval: Normal (0.12–0.20 sec)
QRS: Normal (0.06–0.10 sec)
♥Clinical Tip: A normal ECG does not exclude heart disease.

Rate: Slow (50 bpm)


Rhythm: Regular
P Waves: Normal (upright and uniform)
PR Interval: Normal (0.12–0.20 sec)
QRS: Normal (0.06–0.10 sec)
♥ Clinical Tip: Sinus bradycardia is normal in athletes and during sleep. In acute MI, it may be
protective and beneficial or the slow rate may compromise cardiac output. Certain medications,
such as beta blockers, may also cause sinus bradycardia.

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Rate: Fast (200 bpm)


Rhythm: Regular
P Waves: Normal (upright and uniform)
PR Interval: Normal (0.12–0.20 sec)
QRS: Normal (0.06–0.10 sec)
♥ Clinical Tip: Sinus tachycardia may be caused by exercise, anxiety, fever, hypoxemia,
hypovolemia, or cardiac failure.

B. Irregular Rhythm

Rate: Usually normal (60–100 bpm); frequently increases with inspiration and decreases with
expiration
Rhythm: Irregular; varies with respiration
P Waves: Normal (upright and uniform)
PR Interval: Normal (0.12–0.20 sec)
QRS: Normal (0.06–0.10 sec) 1491
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♥ Clinical Tip: The pacing rate of the SA node varies with respiration, especially in children
and elderly people.

22.5.3. Axis determination

Axis
Axis is the electrical signal recorded on the ECG which contains information relative
to direction and magnitude of the various complexes.
The normal QRS electrical axis, as established in the frontal plane, is between -30
and 90º (directed downward or inferior and to the left) in adults. /figure 1/
An axis between -30º and -90º (directed superior and to the left) is termed left axis
deviation.
If the axis is between 90º and 180º (directed inferior and to the right), then right axis
deviation is present.
An axis between -90º and -180º (directed superior and to the right) is referred to as
extreme right or left axis.
If the QRS is equiphasic in all leads with no dominant QRS deflection, it is
indeterminate axis.

figure 1

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Axis Determination

The QRS axis can be determined by examining all of the limb leads, but the easiest
method involves looking at leads I, II, and aVF only (figure 2).
If the QRS complex is positive (upright) in both leads I and II, then the axis falls
between -30 and 90º, and the axis is normal.
If the QRS complex is positive in lead I but negative (down ward) in lead II, then the
axis is leftward (-30 to -90º).
If the complexes are negative in lead I and positive in aVF, then the axis is
rightward (90 to 180º).
If the complexes are negative in both I and aVF, then the axis is extreme (180 to -
90º).
❖ Another method of axis determination is to find the lead in which the complex is
most isoelectric; the axis is directed perpendicular to this lead. As an example, if the
QRS is isoelectric in lead III which is directed at 120º, then the electrical axis is
either 30º or -150º.
❖ A third method is to determine the frontal lead in which the QRS is of the greatest
positive amplitude. The axis is parallel to this lead.

Axis LI LII TIP


Normal Positive(upward) Positive(upward) Both Up
Right axis deviation (RAD) Negative(downward) Positive(upward) Meet
Left axis deviation (LAD) Positive(upward) Negative(downward) Leave
Extreme Right/Left Axis Negative(downward) Negative(downward) 1493
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deviation (ERAD)

figure 2

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Table; summary of axis determination


Mnemonics
 Leave criterion for LAD,
 The right thing is to meet each other (RAD)
Normal axis Right axis deviation (RAD) Left Axis Deviation (LAD)
 The QRS voltages are  The QRS voltages are  The QRS voltages are positive
positive and upright in Down ward and Negative and upright in leads L1 and
the leads - L1, L2, L3 in L1, but positive and aVL but Negative and down
and aVF upright in leads L2, L3 ward in L2, L3 and aVF
 L2, L3 and aVF tell and aVF.  L1, aVL tell that it is leftward
that it is downward  L2, L3 tell that it is  L2, L3, and aVF tell that it is
 L1, aVL tell that it is downward not down ward - instead it is
to the left  L1 tells that it is to right upward
 Downward and  Downward and rightward  Upward and Leftward is Left
leftward is Normal Axis is Right Axis Axis
 See the Right – Meet  See the Left - Leave each
criterion of QRS in L1 and other criterion of QRS in L1
L3. and L3.

Determine the axis of the following ECG


Question 1

Answer; Normal axis

Question 2

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Answer; Right axis deviation

Question 3

Answer; Left axis deviation

Causes of right axis deviation Causes for left axis deviation


✓ Normal variation (vertical heart with ✓ Normal variation (physiologic, often with age)
an axis of 90º) ✓ Mechanical shifts, such as expiration, high
✓ Mechanical shifts, such as diaphragm (pregnancy, ascites, abdominal tumor)
inspiration and emphysema ✓ LVH
✓ RVH ✓ Left BBB
✓ Right BBB ✓ Inferior wall myocardial infarction.
✓ Lateral wall myocardial infarction ✓ Left anterior fascicular block
✓ Dextrocardia ✓ CHD (primum ASD, endocardial cushion defect)
✓ Ventricular ectopic rhythms ✓ Emphysema
✓ Secundum ASD ✓ Hyperkalemia
✓ Left posterior fascicular block ✓ Ventricular ectopic rhythms
✓ Pre-excitation syndrome (Wolff- ✓ Pre-excitation syndromes (Wolff-Parkinson-White)
Parkinson-White)
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22.5.4. Intervals
PR interval
Normal PR interval: 0.12 to 0.20 s (3 - 5 small squares)
A normal PR interval indicates the electrical impulse originated from the SA node or
in the atrium.
Short PR intervals are suggestive of Wolff-Parkinson-White syndrome.
Long PR intervals are usually seen in first degree AV block, but there may be other
causes.

Picture; Prolonged PR Interval

QRS Complex
Wide QRS complex represents
o A bundle branch block
o Ventricular pre-excitation
o Ventricular pacing, or
o Ventricular tachycardia.

QT interval
Short and long QT intervals may be present.

22.5.5. P wave

See rhythm analysis above


The normal sinus P wave is generally upright in leads I, II, aVF, and V4-V6 and
negative in lead aVR. It may be negative or biphasic in leads III and V1.
A negative P wave in the inferior leads or lead I suggests an ectopic rhythm (low
atrial or left atrial respectively). Similarly, a completely positive P wave in V1 suggests
a left atrial location.

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22.5.6. QRS complex


➢ It is essential to analyze the QRS in all 12 leads to be sure that it is normal.

Look for
✓ QRS Axis
✓ Wide or narrow- duration normally lasts for 0.06 to 0.10 seconds (1½ to 2½ small
boxes)
✓ Pathological Q waves
✓ Left or right ventricular hypertrophy
❖ If the QRS complexes are of normal duration (<0.10 sec) and morphology, then the
rhythm is supraventricular.
❖ If the QRS is wide (i.e. >0.10 sec)
✓ The rhythm is either supraventricular with aberrant conduction, pre-excitation, or
ventricular pacing, or it is of ventricular origin.
✓ Wide QRS with normal rate → bundle branch block (examination of the
morphology can determine if there is left or right bundle branch block or pre-
excitation present)
✓ Regular wide QRS with tachycardia →Ventricular tachycardia /hyperkalemia
✓ Wide QRS with increased voltage may indicate left or right ventricular
hypertrophy.
❖ A narrow QRS complex (<0.06 sec) reflects rapid activation of the ventricles via the
normal His-Purkinje system, which in turn suggests that the arrhythmia originates
above or within the atrioventricular (AV) node (i.e., a supraventricular tachycardia
[SVT]).

Pathologic Q wave
✓ By definition, a Q wave is an initially negative deflection of the QRS complex
✓ 3 principles with respect to Q waves:
1. Not all Q waves are pathologic
2. Not all pathologic Q waves are due to myocardial infarction caused by fixed
coronary artery occlusion; and
3. There is no firm consensus on the criteria for the diagnosis of pathologic Q
waves
✓ Prominent Q waves are a characteristic finding in myocardial infarction, they can also
be seen in a number of Non infarct settings such as;
❖ Misplacement of chest lead electrodes
❖ Dextrocardia
❖ A rightward mediastinal shift in left pneumothorax
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❖ Pectus excavatum
❖ COPD
❖ Rarely, congenitally corrected transposition of the great vessels or congenital
absence of the left pericardium

Picture; QRS complex-wide like Ventricular tachycardia

Picture; Narrow QRS

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22.5.7. ST segment-T wave

Is there ST elevation or depression compared to the TP segment?


The TP segment, between the T wave of one beat and the P wave of the next
beat, should be used as the baseline.
Normal ST segment: No elevation or depression
ST segment has a duration of 0.08 to 0.12 sec,
ST elevation greater than 2mm (>2 small squares) above the baseline or
depression of greater than 1 mm (>1 small square) below the baseline may be
indicative of an MI.

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T wave
 Are the T waves inverted?
 High peaked T waves can be indicative of hyperkalemia.
 Inverted, elevated, or depressed T waves may indicate myocardial ischemia or
injury.
 Inverted T waves are suggestive of MI or a ventricular conduction delay.
 T wave inversions due to evolving or chronic ischemia are often associated with
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Causes of ST elevation Causes of ST Causes of tall


depression T waves
✓ Acute MI (e.g. Anterior, Inferior, Lateral). ✓ Subendocardial ✓ Hyperkalemia
✓ LBBB or LVH (V1-V2 or V3) MI ✓ Hyperacute
✓ Acute pericarditis ✓ Hypokalemia MI
✓ Normal variants (e.g. athletic heart) ✓ Digitalis ✓ LBBB
✓ Abnormal early repolarization syndromes toxicity
✓ Other
❖ Myocarditis (may look like MI or pericarditis)
❖ Massive pulmonary embolism (leads V1-V2 in
occasional cases)
❖ Brugada-type patterns (V1-V3 with right bundle
branch block-appearing morphology)
❖ Myocardial tumor
❖ Myocardial trauma
❖ Hyperkalemia (only leads V1 and V2)
❖ Hypothermia (J wave/Osborn wave)
❖ Hypercalcemia (rarely)
❖ Post-DC cardioversion (rarely)

22.5.8. Overall interpretation


Only after the prior steps have been completed should an overall description,
interpretation and possible diagnoses be determined.
This ensures assimilation of all information in the ECG and that no detail will be
overlooked.

Example 1
Interpret the following ECG

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Answer;
 Rate = 75 bpm
 Regular sinus rhythm
 No axis deviation
 PR interval of 0.14 sec (3.5 small squares)
 Normal QRS complex (0.10 sec)
 No ST segment elevation or
 Normal T wave (No T wave inversion or tall T wave)

Index = Normal ECG


Example 2

Answer;
 Rate = 55 bpm
 Regular sinus rhythm
 No axis deviation
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 PR interval of 0.12 sec (3 small squares)


 Loss of R waves in leads V1 to V3
 ST segment elevation in v2 to v4
 T wave inversion in leads I, aVL and V2 to V 5

Index = Anterior MI with sinus bradycardia

22.6. Common Disorders based on Pathologic finding from ECG

1. Myocardial ischemia and infarction


2. Pericarditis
3. Chamber hypertrophy
4. Arrhythmias
5. Electrolyte disturbances (i.e. hyperkalemia, hypokalemia)
6. Drug toxicity (i.e. digoxin and drugs which prolong the QT interval)

22.6.1 Myocardial Ischemia/infarction

Findings consistent with STEMI:


 ≥0.1 mV (1 mm) in all leads other than V2 and V3, where the following diagnostic
thresholds apply:
✓ ≥0.2 mV (2 mm) in men ≥ 40 years, ≥0.25 mV (2.5 mm) in men <40 years
✓ ≥0.15 mV (1.5 mm) in women.
Findings consistent with NSTEMI or unstable angina: → in two anatomically contiguous
leads
New horizontal or down-sloping ST depression ≥0.05 mV (0.5 mm) or T inversion
≥0.1 mV (1 mm) with prominent R wave or R/S ratio >1.
Contiguous leads are defined as pairs or groups of leads that reflect the different
walls of the heart. These are the inferior (II, III, aVF), lateral (I, aVL), and anterior
leads (V1 to V6).
.
Prior MI
The following are the criteria for ECG changes associated with prior MI (in the
absence of LVH or LBBB)
o Any Q wave in leads V2 to V3 ≥0.02 sec or QS complex in V2 and V3; or
Q wave ≥0.03 sec and ≥0.1 mV deep or QS complex in leads I, II, aVL,
aVF; or V4 to V6 in any two leads of a contiguous lead grouping (I, aVL;
V1 to V6; II, III, aVF).
o R wave ≥0.04 sec in V1 to V2 and R/S ≥1 with a concordant positive T
wave in the absence of a conduction defect.
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LOCATION OF ISCHEMIA OR INFARCTION

Image; blood supply and MI leads, LAD =left anterior descending coronary artery, RCA = right coronary artery, LCX = left circumflex
coronary artery

 The portion of the LV that is ischemic or infarcted may be predicted by which ECG
leads show ST-segment, T wave, or Q wave abnormalities.

A. Anterior, lateral, and apical MI


✓ ST-segment elevation or Q waves in one or more of the precordial leads (V1 to
V6) and leads I and aVL has traditionally been used to suggest anterior wall
ischemia or infarction (waveform 1A-B).
✓ Although characteristic ECG changes in leads V1 to V3 are considered typical of
anteroseptal ischemia, they may be more indicative of apical ischemia.

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waveform 1A-B

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B. Inferior and right ventricular MI


 ST-segment shifts or Q waves in leads II, III, and aVF suggest inferior wall ischemia
or infarction (waveform 2).
 If there is evidence of inferior wall ischemia, right-sided leads, especially V3R and
V4R, should be obtained to assess for a possible right ventricular ischemia/infarction
(waveform 2).

waveform 2

C. Posterior wall MI
 Acute posterior wall MI induces ST elevations in leads placed over the back of
the heart, eg, leads V7 to V9 (waveform 3 and figure 1).
 This is usually associated with reciprocal ST–segment depression in leads V1 to
V2 or V3.
 Similar ST changes can also be the primary ECG manifestation of anterior
subendocardial ischemia that may occur in combination with inferior infarction.
 Posterior inferior wall MI can usually be differentiated from anterior wall ischemia
by the presence of ST-segment elevation in the inferior leads (II, III, aVF) in
addition to posterior leads V7 to V9.
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 Relatively tall R waves may also appear in leads V1 to V3 (waveform 4),


corresponding to the appearance of pathologic Q waves (loss of depolarization
forces) in the posterior leads.

waveform 3

figure 1

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waveform 4

D. Multiple regions
 In some cases, ischemia affects more than one region of the myocardium.
 In this setting, the ECG should show the characteristic findings of involvement in
each region (waveform 5). However, partial normalization may result from
cancellation of opposing vectorial forces.

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waveform 5

Serial ECG changes of MI

IDENTIFICATION OF THE INFARCT-RELATED ARTERY


Blood supply of the heart

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✓ ECG may also provide information about the site or arterial occlusion in patients
with STEMI.

Inferior MI on the ECG

 An inferior wall MI generally have occlusion of either the right or the left
circumflex coronary artery.
 The presence of ST-segment elevation in lead III exceeding that in lead II,
particularly when combined with ST-depression in leads I and aVL, is a very
useful predictor of an occlusion in the proximal or mid portion of the right coronary
artery
 The presence of ST-segment elevation in lead II, which is equal to that of lead III,
especially when combined with ST-depression in leads V1 to V3 or ST-elevation in
leads I and aVL, is a useful but not absolute predictor of a left circumflex
coronary artery occlusion; these findings may also be seen in distal occlusion of a
dominant right coronary artery.
 Some patients with an inferior MI have right-sided ST-elevation in leads V1 and
V4R; this finding is indicative of acute right ventricular injury and correlates closely
with occlusion of the proximal right coronary artery.

Anterior MI on the ECG

 Anterior wall MI usually have occlusion of the left anterior descending coronary
artery (LAD).
 The presence of ST-elevation in lead aVR, complete right bundle branch block,
ST-depression in lead V5, and/or ST elevation in V1 greater than 2.5 mm strongly
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Complete normalization of the ECG following STEMI is uncommon but can occur,
particularly with smaller infarcts and when left ventricular ejection fraction and
regional wall motion improve.
Normalization is usually associated with spontaneous recanalization or good
collateral circulation.
In contrast, persistent Q waves and ST elevations several weeks or more after an
infarct correlate strongly with a severe underlying wall motion disorder (akinetic or
dyskinetic zone), although not necessarily a frank ventricular aneurysm (waveform
6).

waveform 6

22.6.2 Pericarditis

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22.6.3 Chamber enlargement and hypertrophy

The following criteria suggest left atrial enlargement/abnormality when correlated


with echocardiographic data:
❖ P wave duration >0.11 sec
❖ P wave/PR duration >1.6
❖ Negative phase of P in V1 >0.04 sec or >1 mm
❖ P-terminal force >0.04 mm/sec
❖ Notched P, interpeak interval >0.04 sec

RIGHT ATRIAL ABNORMALITY/ENLARGEMENT

❖ A relatively narrow P wave that is of increased amplitude (“P pulmonale”).


❖ The most common finding is a P wave >2.5 mm in lead II.
❖ In addition, a P wave >1.5 mm in V1 or V2 or a P wave that has a rightward
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❖ If the right atrium becomes sufficiently large, it may extend toward the left, causing
P waves in V1 to be inverted and giving the illusion of left atrial enlargement.
❖ In contrast to left atrial abnormality or interatrial block, the P wave duration is
usually normal.

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ECG criteria →There have been multiple ECG criteria proposed for diagnosing LVH. The
most popular include:
 Wide QRS
 Tall R waves in multiple leads
 Left Axis deviation
 Amplitude of S wave in lead V1 + amplitude of R wave in V5 or V6 (whichever is
the tallest) ≥35 mm.
 Amplitude of R wave in aVL + amplitude of S wave in V3 >28 mm for men, or
>20 mm for women.
 QRS voltage in all leads >175 to 225 mm.
 R wave in I + S in 3 more than 25 mm
 R in aVL more than 11 mm or >18 mm if left axis is present
 R in aVF more than 20 mm
 S in aVR more than 14 mm
 S in V1 or V2 + R in V5 or V6 more than 35 mm
 R in V5 or V6 more than 26 mm
 R + S in any V lead more than 45 mm

Clues to the diagnosis of right ventricular hypertrophy include:


 Right axis deviation (>+90)
 Tall R waves in V1 and V2
 R in V1 >6 mm
 R in V1 + S in V5 or V6 >10.5 mm
 R/S ratio in V1 >1
 S/R ratio in V6 >1



Late intrinsic deflection in V1 (>0.035 sec)
Incomplete right bundle branch block
ST-T wave abnormalities ("strain") in inferior leads
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 Right atrial hypertrophy/overload (“P pulmonale”)


 S>R in leads I, II, III, particularly in children (S1S2S3 pattern)

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22.6.4 Arrhythmia

Mechanisms of Arrhythmias
 Altered Automaticity (Increased or decreased Automaticity)
 Reentry from ectopic foci
 Triggered activity
 Conduction Block

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SVT = Supraventricular tachycardia, PVCs = premature ventricular contractions, AVNRT = Atrioventricular


node reentry tachycardia, AVRT = Atrioventricular reentrant tachycardia. VT = Ventricular Tachycardia

Tachyarrhythmias
 Supraventricular tachycardia (SVT)
 Atrial fibrillation
 Atrial flutter
 Ventricular tachycardia
✓ Monomorphic
✓ Polymorphic (Torsade’s de pointe)
 Ventricular fibrillation

Rhythms and arrhythmias of the sinus node

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Table; possible reversible causes of sinus bradycardia (the H &T s)


H’s T’s
 Hypoxia  Toxins (overdose)
 Hypovolemia  Trauma (esp. non-accidental)
 H+ (acidosis)  Tension pneumothorax
 Hypo/hyperkalemia  Tamponade (cardiac)
 Hypo/hyperglycemia  Thrombus (PE)
 Hypo/hyperthermia

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Rate: Normal to slow; determined by duration and frequency of sinus pause (arrest)
Rhythm: Irregular whenever a pause (arrest) occurs
P Waves: Normal (upright and uniform) except in areas of pause (arrest)
PR Interval: Normal (0.12–0.20 sec)
QRS: Normal (0.06–0.10 sec)
♥ Clinical Tip: Cardiac output may decrease, causing syncope or dizziness.

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22.6.4.1. Atrial and atrioventricular nodal (supraventricular) arrhythmias

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22.6.4.1.1 ATRIAL FIBRILLATION AND ATRIAL FLUTTER

Atrial Fibrillation is associated with the following changes on ECG


 Lack of discrete P waves.
 Fibrillatory or f waves are present at a rate that is generally between 350 and 600
beats/minute; the f waves vary continuously in amplitude, morphology, and
intervals.
 Ventricular response follows no repetitive pattern; the variability in the intervals
between QRS complexes is often termed “irregularly irregular.”
 The ventricular rate (especially in the absence of AV nodal blocking agents or
intrinsic conduction disease) usually ranges between 90 to 170 beats/min.
 The QRS complexes are narrow unless AV conduction through the His Purkinje
system is abnormal due to functional (rate-related) aberration, pre-existing bundle
branch or fascicular block, or ventricular preexcitation with conduction down the
accessory pathway.

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Image; AF

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22.6.4.2. Rhythms Produced by Conduction Block

AV Block (relatively common)


 1st degree AV block
 2nd degree AV block → type 1 and type 2
 3rd degree AV block
SA Block (relatively rare)

Atrioventricular block
Atrioventricular (AV) block may manifest as conduction delay in the AV node,
intermittent failure of conduction from the atria to the ventricles, or complete AV
block.

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First degree AV block, defined as a prolonged PR interval (>0.20 seconds), is not


a true block but is delayed or slowed AV conduction.
A partial list of causes of first-degree AV block include the following:
✓ Underlying structural abnormalities of the node
✓ An increase in vagal tone
✓ MI
✓ Infiltrative CMP and DCMP
✓ Drugs that impair or slow nodal conduction including digoxin, beta blockers,
and non-dihydropyridine CCB
✓ Certain muscular dystrophies

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SECOND DEGREE ATRIOVENTRICULAR BLOCK


Second degree atrioventricular (AV) block is defined as an occasional non-
conducted P wave, resulting in a long RR interval.
Second degree AV block may either be Mobitz type I (Wenckebach) or Mobitz
type II.

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22.6.4.3 Ventricular arrhythmias


 Ventricular arrhythmias are wide complex rhythms that may be regular or irregular.
 These may be normal rate, bradycardic, or tachycardic, and may occur as single
beats or sustained.
 Some ventricular arrhythmias may be present as sudden cardiac arrest.

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Torsade’s de pointes = "twisting of points"

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Intraventricular block
RIGHT BUNDLE BRANCH BLOCK
 Incomplete RBBB
 Complete RBBB
LEFT BUNDLE BRANCH BLOCK
 Incomplete LBBB
 Complete LBBB

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Ectopic Foci and Beats

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22.6.5 Electrolyte abnormalities

 Hyperkalemia
 Hypokalemia
 Hypocalcemia
 Hypercalcemia

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22.6.6 Drug toxicity

Digoxin and digitoxin toxicity


o ECG features of hyperkalaemia, sinus bradycardia, sinoatrial arrest, and 2nd or 3rd degree
AV block are common.

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Phenytoin toxicity
✓ ECG -reveals increased PR interval, widened QRS interval, and altered ST
segments and T waves, arrhythmias, ventricular tachycardia, primary ventricular fibrillation,
atrioventricular block, or sinus arrest with junctional or ventricular escape that may occur after
intravenous (or very rarely oral) exposure

Phenothiazine toxicity
✓ ECG → usually shows QT interval prolongation and occasionally QRS prolongation
(particularly with thioridazine and Risperidone).

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Chapter 23; Basics about rational use of antibiotics


Dr. Mulualem. G

WHO defines the rational use of antibiotics as the correct, proper and appropriate
use of antibiotics.
Rational use of antibiotics requires that the patient receives medications
appropriate to their clinical needs in doses that meet their own individual
requirements for an adequate period of time and lowest cost to them and their
community.
Antibiotics can be used as: Prophylaxis, Empirical or Definitive treatment

Dosing and common terminologies

❖ ‘’Stat’’ means given as a ‘’single dose’’ only and there is no any other repeat dose.
E.g. Albendazole, 400mg, PO, stat
❖ QD (lat. Quaque in die) = daily, once per day, every 24 hours (q 24hr)
 Don’t use the term ‘’QD’’, because the pharmacist may misinterpret as ‘’QID’’
❖ BID (lat. bis in die) = two times per day, every 12 hrs (2X/day or q12hr)
❖ TID (lat. ter in die) = three times per day, every 8 hrs (3X/day or q8hr)
❖ QID (lat. Quarter in die) = four times per day, every 6 hr (4X/day or q6hr)
❖ Dose more than 4x/day can be prescribed as → q4hr (6x/day), q3hr (8x/day), q1hr,
q5min….
❖ Suppository → drugs to be given per rectum. E.g. PCM suppository, bisacodyl
suppository
❖ Pessary → drugs to be inserted through vagina. E.g. clotrimazole vaginal pessary

Divided dose examples


❖ PTU, 300mg, PO, in 3 divided dose means 100mg, PO, TID = 300mg per day (but
it doesn’t mean 300mg TID)
❖ Ceftriaxone 2g, IV, in two divided doses = Ceftriaxone 1g, IV, BID

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Loading dose and maintenance dose


❖ Loading is the initial and highest dose to be given once, which is followed by
maintenance dose as daily, BID and the like.
❖ Example
 Cimetidine, 400mg, IV, Loading then 200mg, IV, BID
 Hydrocortisone, 200mg, IV, Loading then 100mg, IV, QID
 Aspirin (ASA), 325 mg, PO, loading followed by 81mg, Po, daily
 UFH, 5,000 IU, IV, loading then 250 IU/kg/dose, Sc, BID
 Mannitol Loading dose 1g/kg over 30-60min, followed by a maintenance dose of
0.5g/kg every 4-6hrs

Escalation and de-escalation


❖ Escalation is increasing the dose progressively with some form of scale until target
is achieved. The reverse is true for de-escalation
❖ Example
 Refer dopamine drip preparation from shock management (click here →
Chapter 3; Shock)
 Lisinopril 5 mg daily, escalate dose up to 40 mg Po daily if BP is uncontrolled.
Which means 5mg → 10 mg → 20mg → 25mg …. Maximum limit is 40 mg
 Amlodipine 5 mg daily, escalate to 10 mg if BP is uncontrolled.

Tapering dose

❖ Drugs to be tapered are those not to be stopped abruptly, rather you have to
discontinue the drug by decreasing the dose gradually. By how much to be tapered
depends on your target and patient’s clinical response
❖ Example
 Prednisone, 1-2 mg/kg/day, PO, daily or BID, for 4-6 wks, followed by gradual
tapering.

Maximum daily dose

❖ Drugs can be given or written in ranges. So, maximum daily dose is the highest
total dose to be given per day. Taking the drug above the maximum level may
cause toxicity or intolerable side effects.
❖ Example
 PCM, 500mg to 1g PRN; max 4g/day → in this case the patient can take a total of
up to 4g/day (i.e 500mg 8x/day or 1g 4x/day is the maximum limit)
 Enalapril for hypertension; Initial: 5 mg, PO, daily (2.5 mg, PO, daily in patients
taking diuretics); titrate upward, usually at 1- to 2-week intervals; usual dose range:
10 to 40 mg daily. Target dose: 20 mg daily in 1 or 2 divided doses. Maximum: 40
mg/day.
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Common scenarios in syrup and per body weight (per Kg) dosing

➢ If a drug is prescribed as per day form (‘’x’’mg/kg/day), you have to divide the
final calculated amount to the frequency of dose (i.e divide by 2 for BID dose,
divide by 3 for TID dose)
➢ But, if a drug is prescribed as per dose form (‘’x’’mg/kg/dose), you have to give
the total calculated amount per each dose (frequency of dose).
➢ Per dose and per day have no effect on once daily dosage forms

Examples
o Gentamycin, 5mg/kg/day, IV, TID, for 3 weeks is the same as gentamycin
5mg/kg/day, in three divided doses, IV, for 3 weeks
▪ For example, in 60 Kg pt, 5mg/kg/day = 5 x 60kg/day = 300mg/day.
300 ÷ 3 = 100mg. So, the final prescription is gentamycin, 100mg,
IV, TID
o But, metronidazole 7.5mg/kg/dose, IV, TID is quite different from
metronidazole 7.5mg/kg/day, IV, in three divided doses
▪ For example, in 1o Kg pt, 7.5mg/kg/dose = 7.5 x 10Kg/dose =
75mg/dose. So, the final prescription is metronidazole, 75mg, IV, TID

How to calculate and prescribe syrup?


Let’s see with amoxicillin syrup in 30 kg child

➢ Amoxicillin syrup is available as 250mg/5ml or 125mg/5ml


➢ If the dose of amoxicillin is 50mg/kg/day, TID, based on the above explanation
50mg/kg/day = 50mg x 30kg/day = 1500mg. since it is per day dose, we will
devide for 3 (i.e. for TID dose). 1500mg/day ÷ 3 = 500mg, TID
➢ Our target is how much ml does the child takes per each dose?
➢ In 250mg/5ml preparation, 250mg = 5ml
500mg = x
500𝑚𝑔 𝑥 5𝑚𝑙
➢ X = = 10ml
250𝑚𝑔
➢ So, the final prescription will be, Amoxicillin syrup (250mg/5ml), 10ml, po, TID for
7 days
➢ N.B one Tea spoon (tsp) = 5ml
➢ For final dispense of this dose (for pharmacist),
o This child needs 10ml, TID in each day which means S/he needs 10ml x 3
= 30 ml per day. The prescription is for 7 days, so 30ml/day for 7 days =
30ml x 7 = 210ml.
o If each bottle of amoxicillin syrup contains 100ml, for 210 ml, the pharmacist
should give 2 bottles of syrup (210ml ≅ 200ml).
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Recommendations to avoid Poor prescription writing


➢ generic name is preferred
➢ ".1" is easily misread as "1," a tenfold overdose
➢ "1.0 mg“ is easily misread as "10 mg," whereas "1 mg" is not
➢ The slash ("/") was traditionally used as a substitute for a decimal point. This
should be abandoned because it is too easily misread as the numeral "1.“
➢ "10U" is easily misread as "100"; the word "units" should always be written out.
➢ ‘’IU’’ to mean International unit easily misread as IV (intravenous)
➢ micrograms should always have this unit written

Lines of therapy
✓ Difference between 1st line, 2nd line, 3rd line and alternative
Treatment options can often be ranked or prioritized as 1st line, 2nd line, 3rd line and
so on.

1st line It is the first therapy that will be tried


Its priority over other options is usually due to
Recommended previously based on clinical trial on efficacy, safety
and tolerability
Chosen based on clinical experience of physicians (experts of the
subject)
Availability and cost effectiveness especially for low income countries
2nd line 2nd line therapy may be substituted or added to the treatment
regimen if 1st line therapy;
Fails to resolve the issue (i.e. if there is no clinical response to 1st
line treatment)
Produces intolerable side effects (including allergic reaction and
complications)
3rd line ➢ Reserved for microbiologic data proven resistance for 1st and 2nd
line options
➢ May be substituted or added over to 2nd line if clinical response is
not achieved. 2nd line therapy maybe totally substituted with 3rd line,
if intolerable side effect develops.
Alternative This are drugs which may be less effective than the preferred drug.
They are considered if the preferred drug is not available, route of
administration is unavailable, too costly for the patient, or allergy to
1st line drugs etc.

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Category of drugs for pregnancy

Picture; diagrammatic example on, how to search pregnancy risk factor of a specific drug from
UpToDate

Our (Authors) recommendation for pregnancy category drug prescription


 Category A and B → prescribe safely
 Category C → Give only if the potential benefits are more necessary than the
potential risk to the fetus. Otherwise, it is better to restrict these drugs during
pregnancy.
 Avoid category D and X → category D can be given if there is emergency condition
of the mother and the drug is lifesaving with lack of other safe drug options.
Category X is absolutely contra indicated
 Look at the description below

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Dose adjustment of antibiotics in renal impairment (AKI/CKD pt’) or


hepatic impairment (e.g CLD pt’)

Picture; diagrammatic example on, how to search, a specific drug dose adjustment for renal or
hepatic impairment, from UpToDate

Antibiotic sensitivity chart

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Classification of antibiotics
There are four major classes of antibiotics
o Cell wall Synthesis inhibitors
o Protein synthesis inhibitors
o Nucleic acid synthesis Inhibitors
▪ Folate antagonists
▪ Direct enzyme inhibitors
o Miscellaneous

Table; classes of antibiotics with common examples


Cell wall synthesis inhibitors
Examples# Antibacterial spectrum of coverage*
Beta Penicillin Natural Pen.G, Pen.V Streptococci, Pepto streptococcus,
lactam penicillin Intravenous Pen.G for N. Meningitidis
antibiotics Anti- Cloxacillin, Oxacillin, MSSA, CoNS
staphylococcal methicillin, naficillin
(penicillinase
resistant)
Amino Amoxicillin, Ampicillin Streptococci, E. coli, klebsiella, H.
penicillin’s influenza, Ampicillin (IV) for N.meningitidis,
Pepto streptococcus
Amino Amoxicillin + Streptococci, MSSA, G -ve bacilli except
penicillin’s clavulanic acid pseudomonas, Pepto streptococcus
with Beta (Augmentin), Ampicillin
lactamase + sulbactam
inhibitors
Extended Piperacillin Streptococci, MSSA, G -ve bacilli, N.
spectrum +tazobactam meningitidis, anaerobes except C. difficile
antibiotics
(Antipseudom
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Cephalospor 1st generation Cephalexin, cefazolin Streptococci except enterococci, MSSA, E.


ins coli, klebsiella, H. influenza, Pepto
streptococcus
2nd generation Cefuroxime, cefotetan Like 1st generation + gram - ve bacilli
except pseudomonas
3rd generation Ceftriaxone, cefixime, Streptococcus except enterococcus, MSSA,
Cefpodoxime, Cefdinir G -ve coccobacilli, G -ve bacilli except
pseudomonas, Pepto streptococcus
Ceftazidime G -ve bacilli, N. meningitidis
4th generation Cefepime Streptococcus except enterococcus, MSSA,
G -ve bacilli, N. Meningitidis,
Carbapenems Meropenem, Imipenem Streptococci, MSSA, G -ve bacilli, N.
Meningitides, and anaerobes except C.
difficile
Ertapenem Streptococci except enterococcus, MSSA, G
-ve bacilli except pseudomonas, and
anaerobes except C. difficile
Monobactams Aztreonam
Glycopeptides Vancomycin Gram +ve cocci including MRSA, Pepto
streptococcus and C. difficile from
anaerobes
Protein Synthesis Inhibitors
Bactericid Aminoglycosides Gentamycin, All G-ve bacilli, TB
al streptomycin,
neomycin, amikacin,
kanamycin
Bacteriost Tetracyclines Tetracycline (TTC), Streptococci except enterococci, MSSA, E.
atic doxycycline coli, klebsiella, H. influenza, pepto
streptococcus, Rickettsia, atypical’s
Chloramphenicol (CAF) Streptococci except enterococci, E. coli,
klebsiella, H. influenza,
Gram(-ve) coccobacilli, Pepto streptococcus
and Bacteroides from anaerobes
Macrolides Azithromycin Streptococci except enterococci, MSSA, E.
coli, klebsiella, H. influenza, N. Gonorrhea,
C. trachomatis from atypicals, Rickettsia
Erythromycin Streptococci except enterococci, MSSA,
atypical’s
Clarithromycin Streptococci except enterococci, MSSA, E.
coli, klebsiella, H. influenza, atypical’s
except C. trachomatis H. pylori,
Lincosamide Clindamycin Streptococci except enterococci, Staph
epidermidis (CoNS), MSSA, Pepto
streptococcus and Bacteroides from
anaerobes,
Nucleic acid synthesis Inhibitors
Direct Fluoroquinol 1st generation Nalidixic acid
enzyme
inhibitors
ones
2nd generation Ciprofloxacin,
Norfloxacin (bladder
All G-ve bacilli, N. Meningitidis 1567
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specific), ofloxacin
3rd generation Levofloxacin Streptococci except enterococci, G-ve bacilli
except pseudomonas, Pepto streptococcus,
4th generation Moxifloxacin
atypical’s except chlamydia, moxifloxacin is
active against bacteroids
Folate Sulfonamide Trimethoprim - Sulfamethoxazole MSSA, G-ve bacilli except pseudomonas,
synthesis Derivatives (cotrimoxazole, TMP - SMX) P.jirovecii (PCP)
inhibitors Pyrimethamine - Sulfadiazine
Pyrimethamine – Sulfasalazine
Miscellaneous
Nitroimidazole Metronidazole Anaerobes
Nitrofurantoin (just bladder infection) Enterococci, E. coli, klebsiella, H. influenza,
Rifampin Staph epidermidis (CoNS), MRSA and
MSSA,
*corelate with the antibiotic sensitivity chart above and with the table below
#
Drugs highlighted in bold letters are available in Ethiopia
MRSA = methicillin resistance staph aureus, MSSA = methicillin sensitive staph aureus
CoNS = Coagulase negative staphylococcus (staph epidermidis)

Group of common infectious bacteria

Table; Group of common infectious bacteria with their antibiotic options#


Group Bacteria Location Antibiotics active against the bacteria*
Gram +ve Streptococci S. pyogenes Brain, All penicillin’s except cloxacillin,
cocci (in chains) (GAS), S. respiratory cephalosporins except ceftazidime,
agalactiae (GBS), tract, oral, carbapenems, macrolides, Tetracyclines,
S. pneumoniae, heart, skin levofloxacin, clindamycin, chloramphenicol,
S. viridans vancomycin
Enterococci Intraabdominal, All penicillin’s except cloxacillin, Meropenem/
(Group D strep) urinary tract imipenem, vancomycin, nitrofurantoin
(bladder specific)
Staphylococci MSSA Bone/joint, Cloxacillin, Augmentin, piperacillin
(in clustors) respiratory tazobactam, cephalosporins except cefixime
tract, oral, and ceftazidime, carbapenems, macrolides,
heart, skin Tetracyclines, clindamycin, cotrimoxazole,
vancomycin, rifampin
MRSA vancomycin, rifampin
CoNS (Staph Skin, Cloxacillin, clindamycin, vancomycin, rifampin
epidermidis, S. prosthetics
saprophyticus) valves
Gram -ve
bacilli
Non-Beta
lactamase
E. coli, H.
influenza,
Brain,
respiratory
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Amoxicillin/ampicillin, Augmentin, piperacillin
tazobactam, cephalosporins, carbapenems,

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Chapter 23; Basics about rational use of antibiotics 1569

producing klebsiella tract, urinary clarithromycin, TTC, azithromycin and


pneumonia tract, doxycycline just H. influenza, fluroquinolones,
intraabdominal cotrimoxazole, chloramphenicol, nitrofurantoin
Beta Augmentin, piperacillin tazobactam, 2nd to 4th
lactamase generation cephalosporins, carbapenems,
producing fluroquinolones, cotrimoxazole,
chloramphenicol, nitrofurantoin
Extended E. coli, klebsiella piperacillin tazobactam,
spectrum pneumonia Meropenem/imipenem, fluroquinolones,
Beta cotrimoxazole, nitrofurantoin
lactamase
producing
SPACE Serratia, Proteus Augmentin, piperacillin tazobactam, 2nd to 4th
mirabilis, generation cephalosporins, carbapenems,
Actinobacterium fluroquinolones, cotrimoxazole
sp, Citrobacter
sp, Enterobacter
sp
Pseudomonas aeruginosa piperacillin tazobactam, ceftazidime,
cefepime, Meropenem/imipenem,
fluroquinolones except levofloxacin,
Gram -ve N. meningitidis Brain Pen. G (IV), Ampicillin (IV), piperacillin
coccobacilli tazobactam, 3rd and 4th generation
cephalosporins, Meropenem/imipenem, cipro
floxacillin, chloramphenicol, rifampin
N. Gonorrhea STI/PID Ceftriaxone, cefixime, azithromycin,
chloramphenicol
Anaerobes Pepto streptococcus Above the metronidazole, Penicillin’s except cloxacillin,
diaphragm cephalosporins except ceftazidime and
(oral, cefixime, Meropenem/imipenem/ ertapenem,
respiratory tetracyclines, levofloxacin/ moxifloxacin,
tract) clindamycin, vancomycin, chloramphenicol,
Bacteroides Below the metronidazole, piperacillin tazobactam,
diaphragm Cefoxitin/cefotetan,
(Intraabdominal, Meropenem/imipenem/ertapenem,
PID) moxifloxacin, clindamycin, chloramphenicol,
C. difficile Intraabdominal metronidazole, vancomycin
Atypical Mycoplasma pneumoniae, Respiratory Macrolides, Tetracyclines, levofloxacin/
bacteria Chlamydophila species tract moxifloxacin
Legionella pneumophilia Macrolides, Tetracyclines,
ciprofloxacin/levofloxacin/ moxifloxacin
Chlamydia trachomatis STI/PID Azithromycin, Erythromycin, Tetracyclines
Rickettsia R. prowazekii, R. typhi Typhus Doxycycline, TTC, Chloramphenicol,
Fluroquinolones,
Borrelia B. recurrentis, B. hermsii, B. Relapsing fever Procaine penicillin, TTC, Erythromycin,
turicatae (New World species), cephalosporins
B. duttonii (Old World species)
#
See the classification based on laboratory feature below
*correlate with the above table and sensitivity chart
GAS = Group A streptococcus, GBS = Group B streptococcus
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Chapter 24; Symptoms and signs in


Amharic (የበሽታ ምልክቶች አማርኛ
ትርጉም)
Dr. Mulualem. G

HEENT related sign and symptoms STI and Gynaecology related sign and
❖ Buldged fontanelle = የእርግብግቢት እብጠት symptoms
❖ Epistaxis = ነስር ✓ Dyspareunia = በግብረ ስጋ ግንኙነት ወቅት
❖ Icteric sclera = የዓይን ቢጫ መሆን ህመም መሰማት
❖ Increased head circumference = የእራስ ቅል ✓ Vaginal bleeding (abnormal uterine
መጨመር bleeding) = በማህጸን ደም መፍሰስ
✓ Menstrual irregularitie = የወር አበባ መዛባት
Respiratory system related sign and symptoms ☛ Dysmenorrhea = በወር አበባ ወቅት
➢ Chest pain = የደረት ህመም (ደረት ውጋት) ከፍተኛ የሆነ ህመም ስሜት
➢ Cough = ሳል ☛ Menorrhagia/ metrorrhagia = መጠኑ
➢ Fast breathing (Tachypnea) = ከላይ ከላይ መተንፈስ፣ ብዙ የሆነ የወር አበባ መፍሰስ/ ለብዙ
ቃታ መንሳት ጊዜ መፍሰስ
➢ Hemoptysis = ደም የቀላቀለ አክታ ☛ Amenorrhea (10, 20) = አደፍ ቅሪት
➢ Rhinorrhoea = የንፍጥ መብዛት (ማናፈጥ) ✓ Vaginal discharge = የማህጸን ፈሳሽ ፣
➢ SOB (Dyspnoea) = ትንፋሽ ማጠር የብልት ፈሳሽ
➢ Sputum = አክታ ✓ Urethral discharge = የብልት ፈሳሽ
➢ Stridor = ኩርርታ ✓ Genital ulcer with/without inguinal
➢ Wheeze = ማቃተት፣ የሚአፏጭ ድምጽ swelling = የብልት (ሀፍረተ ስጋ) ቁስል
✓ chancre = ከርክር
CVS related sign and symptoms
Edema = ውሃ አዘል ገላ Haematology related sign and symptoms
Fatigue (easy fatigability) = ድካም ▪ Bleeding = ደም መፍሰስ፣ መድማት
Intermittent claudication = አልፎ አልፎ በጉዞ ▪ Blurring of vision = የእይታ መደብዘዝ
ወቅት የሚከሰት የእግር ሕመም ▪ Epistaxis’s = ነስር
Leg swelling = የእግር እብጠት ▪ Light headedness = የራስ መቅለል
Orthopnoea = ተንጋሎ ትንፋሽ ማጠር ▪ Pallor = መገርጣት
Palpitation = የልብ መደንከር ▪ Tinnitus = ህውታ፣ በጩኸት የሚፈጠር የጆሮ
Tachycardia = ፈጣን የልብ ምት ህመም
PND = ድንገት በሚመጣ የትንፋሽ ማጠር ምክንያት
ከመኝታ ተነስቶ መስኮት ከፍቶ አየር ለማሰግባት MSS related sign and symptoms
መሞከር Deformity = አካለ ጎደሎነት
SOB (Dyspnoea) = ትንፋሽ ማጠር Fracture = ስብራት
Syncope = ራስን መሳት Instability = የሰውነት አለመረጋጋት

GI related sign and symptoms


Limping = ማነከስ 1571
Morning stiffness = የሰውነት ግትርነት (በጠዋት)
Nitsbin (ንጽቢን) Bedside oriented Internal medicine 2nd edition
Chapter 24; Symptoms and signs in Amharic (የበሽታ ምልክቶች አማርኛ ትርጉም) 1572

❖ Abdominal distension = የሆድ መነፋት Swelling = እብጠት


❖ Abdominal swelling = የሆድ እብጠት Weakness = ድካም
❖ Abdominal pain = የሆድ ህመም፣ የሆድ ቁርጠት
❖ Ascites = = ቅምጠ ውሃ ፣ ውሃ የቋጠረ ሆድ NS related sign and symptoms
❖ Constipation = ሆድ ድርቀት ☛ Body weakness (weakness of extremities)
❖ Diarrhoea = ተቅማጥ = የሰውነት መስነፍ
❖ Dyspepsia = የምግብ አለመፈጨት ችግር ☛ Cognitive disturbance = የመገንዘብ ችግር
❖ Dysphagia = የመዋጥ ችግር ☛ Disturbance in vision, hearing, swallowing
❖ Heart burn (Burning epigastric pain) = ቃር፣ = የማየት፣ የመስማት፣ የመዋጥ ችግር
የሚአቃጥል የደረት ህመም ☛ Disturbance of speech
❖ Hematemesis = ደም የቀላቀል ትውከት፣ ደም (dysphasia/aphasia) = የማውራት ችግር፣
ማስተፋት ማውራት አለመቻል
❖ Jaundice = የሰውነት ቢጫ መሆን፣ ወይቦ ☛ Headache = ራስ ምታት፣ ራስ ውጋት
❖ Melena = ደም የቀላቀለ ሰገራ ☛ LOC = ራስን መሳት ፣ እንደሞተ ሰው መሆን
❖ Nausea = ማቅለሽለሽ
☛ Neck stiffness = ማጅራት መገተር
❖ Odynophagia = ምግብ በመዋጥ ወቅት ህመም
☛ Seizure (Abnormal body movement) =
መሰማት
እንፍርፍሪት፣ የሚጥል ህመም
❖ Splenomegaly = የጣፊያ ማበጥ፣ ጓቋ/for VL
patient/
Miscellaneous
❖ Vomiting = ትውከት፣ ማስመለስ
→ Easy fatigability = ድካም
→ Fever = ትኩሳት
GUS related sign and symptoms
→ Increased appetite = የምግብ ፍላጎት
✓ Flank pain = የሽንጥ ህመም ፣ የጎን ህመም
መጨመር
✓ Hematuria = ደም መሽናት ፣ ደም የቀላቀል ሽንት
→ Loss of appetite = የምግብ ፍላጎት መጥፋት
✓ Oliguria or anuria = ሽንት ማነስ
(መቀነስ)
✓ Polyuria = ብዙ መሽናት
→ Lymphadenopathy = ፍርንቲት
✓ Urinary incontinence = ሽንት አለመቋጠር
→ Weight loss = ክብደት መቀነስ
✓ Lower urinary tract symptoms (LUTS):
 dribbling = የሽንት መንጠባጠብ፣
Others
 Dysuria (pain during urination) = ሽንት
→ Infection = ልክፍት
ማጥ
→ Inflammation = ብግነት
 frequency of micturition = በድግግሞሽ
→ Complication = ክፍ ምጪ
(አዘውትሮ) መሽናት
→ Risk factor = ለበሽታ አጋላጭ
 hesitancy = መሽናት እየፈለጉ ግን መሽናት
→ Side effect = የጎንዮሽ ጉዳት
አለመቻል፣
 reduced calibre and force of urinary
stream = የሽንት ሃይል መቀነስ፣
 straining to void = ማማጥ
 urgency = አጣዳፊ ሽንት

Vaccine Preventable disease (በክትባት ቅድመ መከላከል የሚቻሉ በሽታዎች)


Measles = ኩፍኝ ፣ አንከሊስ፣ ቋቋት
Mumps = ጆሮ ደግፍ
Rubella /German Measles/ = የጀርመን ኩፍኝ
Varicella (Chiken pox) = ጉድፍ
o Herepes zoster (shingles) = አልማዝ ባለጭራ
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Diphtheria = ዲፍቴሪያ፣ ተላላፊ የጉሮሮ በሽታ


Pertussis = ትክትክ
Tetanus = መንጋጋ ቆልፍ
Poliomyelitis (Polio) = ልምሻ ፣ ፖሊዮ

N.B vaccines
MMRV = Measles, mumps, rubella, and varicella virus vaccine
DPT = Diphtheria, tetanus toxoids, and acellular pertussis vaccine
Penta valent vaccine contains = DPT, HBV vaccine and Hib (Hemophilus influenza type b) vaccine

24.1. Amharic translation of Selected Dermatologic disorders (የተወሰኑ የቆዳ


በሽታዎች አማርኛ ትርጉም)
Acne Vulgaris = ብጉር
Bacterial infections of the skin and soft tissue
o Cellulitis = የቆዳ ብግነት
o Erysipelas =
o Carbuncle = ንፍርቅ እባጭ
o Furuncle(boil) = ቡግንጅ
o Impetigo = ፍንድሽ ቁስል
o Necrotizing fasciitis
Fungal Infections of the skin
o Mucocutaneous Candidiasis
o Balanoposthitis
o Candidal Intertrigo
o Candidal paronychia
o Vulvovaginitis = የሴት ብልት ብግነት
o Oral candidiasis (thrush) = የአፍ ፈንገስ ልክፍት
o T. capitis (ring wom) = ፎረፎር፣ ቆረቆር፣ አጓጉት
o Pityriasis Versicolor (PV) = ቋቁቻ
Viral skin disorders
o Herpes Simplex (HS) = ምች፣ ሽፍታ
o varicella-zoster (Chicken Pox) = ጉድፍ
o Herpes zoster (shingles) = አልማዝ ባለጭራ
o Molluscum Contagiosum
o Pityriasis rosea
lice: body and head lice = ቅማል
scabies = እከክ
o Itching = የማሳከክ ስሜት
Atopic Dermatitis (AD) = የቆዳ አስም
Contact dermatitis = በንክኪ የሚከሰት የቆዳ ብግነት/አለርጂ
Seborrhoeic dermatitis
Psoriasis = የሚያሳክክ የቆዳ በሽታ
Vitiligo
Albinism = ሻሾት
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Chapter 25; anatomical body parts in


Amharic (የሰውነት አካል ክፍሎች አማርኛ
ትርጉም)
Dr. Mulualem. G

HEENT (ከአንገት በላይ) Genitourinary System (ስርዓተ ሽንት)


Head = ራስ Kidney = ኩላሊት
o Hair = ጸጉር Ureter = ቦየ ፊኛ ፣ ፊኛ ኩልት ቱቦ
o SCALP = የራስ ቆዳ Bladder = ፊኛ
o Skull = ራስ ቅል፣ ጭንቅላት Urethra = ቦየ ሽንት ፣ ፊኛሽን ቱቦ
Eye = ዐይን Urethral meatus = ፊኛሽን ቀዳዳ
o Sclera = የዐይን ጽኑ ልባስ
o Conjunctiva = ልባሰ ዐይን Reproductive organs (አባለ ወሊድ ፣ የመራቢያ
o Pupil = ብሌን አካላት)
o Lens = ምስሪት ፣ ሌንስ Uterus = ማህጸን
o Eye lid = የዐይን ቆብ Uterine fundus = የማህጸን አናት
o Eye lash = ሽፋሽፍት፣ ሽፋል Fallopian tube = ፋሎኝ ፣ የማህጸን ቱቦ
o Eye brow = ቅንድብ Ovary = እንቁልጢ --› እንቁላል እጢ
Ear = ጆሮ Cervix = የማህጸን በር ፣ ህጽንተ አንገት
o External, middle and inner ear = ውጫዊ፣ Vulva = የሴት ብልት ከንፈር/ ቀዳዳ
መካከልኛ እና ውስጣዊ የጆሮ ክፍል Vagina = የሴት ብልት ፣ ከረቤዛ፣ እምስ /ጸያፍ
o Eustachian tube = እስታች ትቦ/ቦይ ቃል/፣ ማህጸን/በተለምዶ/
o Tympanic membrane/ear drum = የጆሮ Clitoris = ቂንጥር
ታምቡር Labia = ከናፍረ ከረቤዛ፣ ከናፍረ እምስ
Nose = አፍንጫ o Labia majora = ዐቢይ ከንፈረ ከረቤዛ
o Nostril = የአፍንጫ ቀዳዳ ፣ ዋንፍ o Labia minora = ንዑስ ከንፈረ ከረቤዛ
o Nasal septum = የአፍንጫ ግድግዳ Scrotum = ማህደረ ቆለጥ፣ የቆለጥ ከረጢት
o Nasal cavity = ሰርን Testes = ቆለጥ
Throat Prostate = ፍስ ውሃ እጢ ፣ ፕሮስቴት እጢ
Penis = ቁርዝ ፣ ቁላ/ጸያፍ ቃል/፣ እስኪት፣
Lymphoglandular System (ሥርዓተ ፍርንት/ሥርዓተ የወንድ ብልት
ሊንፍ/) Glans penis
Lymh node = ፍርንትት፣ ፍርንት እጢ/ሊንፍ እጢ
Lymphatic vessel = ፍርንት ስር Musculoskeletal System (ሥርዓተ አፅም እና
Lymhatic circulation = ፍርንት ዙረት/ዑደት ጡንቻ)
Skeleton = አፅም
Respiratory System (ሥርዓተ ትንፈሳ) Bone = አጥንት
Larynx = ማንቁርት o Vertebrae = አከርካሪ፣ ደንደስ
Vocal cord = ሀብለ ድምጽ፣ አውታረ ድምጽ o Vertebral bone = የጀርባ አጥንት
Trachea = ትንቧ ፣ የአየር ቧንቧ
Bronchi = ቀሳቢት
Bronchiole = ቀሳቢቴ፣ ደቂቅ ትንቧ
o Scapula = ብራኳ
o Humerus = አጽመ ወርች፣ የክንድ
የላይኛው ቅልጥም
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Lung = ሳንባ o Ulna = ክርን አጽም


Pleura = ልባሰ ሳንባ፣ አቃፌ ሳንባ፣ o Radius = የእጅ አጭሩ አጥንት
Pleural cavity = ሳንባ አኑር ወና o Pelvic bone = ዳሌ አጥንት
Diaphragm = ብራኔ ፣ ድልሺ /ከኦሮምኛ የተወሰደ/ o Pelvic cavity = ዳሌ ጎታ
Chest = ደረት o Femur = አጽመ ጭን፣ የጭን አጥንት
o Patella = የጉልበት ሎሚ
Cardiovascular System (ሥርዓተ ልብ እና ሸንዳ) o Tibia = አጽመ እግር፣ ውስጠ አጽመ ባት
Heart = ልብ o Fibula = ምርጊዝ ፣ ውጭ አጽመ ባት
o Left/Right ventricle = ግራ/ቀኝ ሰጭ ልበ ገንዳ ፣ Muscle = ጡንቻ
ከረርሰ ልብ Neck = አንገት
o Left Right auricle = ግራ/ቀኝ ተቀባይ ልበ ገንዳ Arm = ክንድ
o Myocardium /Cardiac muscle = የልብ ጡንቻ Fore arm = ክንድ
o Pericardium = ልብ ሰፋድል፣ ከባቤ ልብ Hand = እጅ
o Pericardial cavity = ልብ አኑር ወና Finger = ጣት
Vessel = የደም ስር Flank/ loin = ሽንጥ፣ ወገብ
o Artery = ደም ወሳጅ Buttock = ቂጥ፣ ዳሌ፣ መቀመጫ
▪ Aorta = ዐቢይ ደም ወሳጅ Thigh = ጭን፣ ታፋ
▪ Arteriole = ንዑስ/ደቂቅ ደም ወሳጅ Leg = እግር
▪ Capillary = ርቂት፣ ቀጭን የደም Calf = ባት
ቧንቧ Foot = ጫማ
▪ Capillary bed = መረበ ርቂት Toe = የእግር ጣት
o Vein = ደም መላሽ Joint = መገጣጠሚያ
▪ Vana cava = ዐቢይ ደም መላሽ o Shoulder joint = የትከሻ መገጣጠሚያ
▪ Venule = ንዑስ ደም መላሽ፣ o Elbow joint = የክርን መገጣጠሚያ
ደመላሺት o Wrist joint = የእጅ አንጓ መገጣጠሚያ
o Hip joint = የሽንጥ/የዳሌ መገጣጠሚያ
Gastrointestinal system (ስርዓተ እንሽርሽሪት) o Knee joint = የጉልበት መገጣጠሚያ
Mouth = አፍ o Ankle joint = የቁርጭምጭሚት
Palate = ላንቃ መገጣጠሚያ
Tonsil = አንቃር፣ ቶንሲል
Uvula = እንጥል Nervous System (ሥርዓተ ነርቭ)
Tongue = ምላስ Skull = ራስ ቅል፣ ጭንቅላት
Pharynx = ጉሮሮ o Frontal bone = ግምባር
Esophagus = ጉሮሮ o Temporal bone = ጆሮ ግንድ
Stomach = ጨጓራ፣ሆድ o Parietal bone = ጣባ
Small intestine = ቀጭን አንጀት o Occipital bone = ራስ ግርጌ
o Duodenum = ቀዳማይ ቀጭን አንጀት Brain = አንጎል
o Jejunum = ማእከላዊ ቀጭን አንጀት o Cerebrum = አንጎለ አእምረት
o Ileum = ዳህራይ ቀጭን አንጀት o Cerebral hemisphere = ገሚስ አንጎለ
Large intestine = ወፍራም አንጀት አእምረት
o Cecum = ጓዳ አንጀት o Cerebellum
o Colon = ትልቅ አንጀት o Medulla oblongata = ሰረሰርጌ አንጎል
o Sigmoid colon = ሲግማሰል ደንዳኔ Spinal cord = ህብለ ሰረሰር
o Rectum = ሬብ፣ ሽለላ አንጀት፣ ትልቅ አንጀት Nerve = ነርቭ
Peritoneum = መርመሬ
Anus = ፊንጢጣ፣ ቱሊ
Neuron = ሕዋስ ነርቭ
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Hepatic duct = ቦየ ጉበት


Hepatic portal vein = ጉበታዊ አቀባይ ደም መላሽ
Spleen = ጣፊያ
Pancreas = ቆሽት ፣ መረጭ፣ ጣፊያ/በተለምዶ/፣
ፓንክሪስ
Liver = ጉበት
Gall bladder = የሀሞት ከረጢት

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Chapter 26; Common Laboratory


Investigations with practical points and
procedures
Dr. Mulualem. G

Here we will discuss selected hematologic, chemistry, Hormone and Chemokine analysis,
serologic, and microbiological tests41

Basic hematologic tests include;


CBC (Complete blood count)
o M. HCT (Manual hematocrit)42
o Hgb (Rapid hemoglobin strip test)43
ESR (Erythrocyte sedimentation rate)
BF (Blood film)
PM (Peripheral morphology, peripheral blood smear)
Basic Immunohematology Tests
o BG & RH (Blood Group and RH determination), crossmatch

Basic Clinical chemistry tests


Serum Glucose level → RBS, FBS, OGTT, HbA1C (Glycated hemoglobin) test
LFT (Liver function tests) → Classified in 3 groups:
o Synthetic function: albumin, PT & aPTT
o Metabolic activity: bilirubin
o Cholestasis or biliary obstruction: ALP, Gamma Glutamyl Transferase (GGT)
Liver enzymes → indicate hepatocyte injury: AST (SGOT), ALT (SGPT)
RFT (Renal function test) → BUN and creatinine
Serum electrolyte tests → NA+, K+, Cl- Ca++, Mg++
Body fluid analysis → CSF analysis, pleural fluid analysis, ascitic fluid analysis, wound
discharge analysis44
Lipid profile tests → Triglyceride, CL (cholesterol), LDL, HDL
Coagulation profile → PT, aPTT, & INR
Serum Uric acid
Troponin and Creatine kinase
B-type natriuretic peptide (BNP)
Lactate dehydrogenase (LDH)

41
Sample for hematology and serology collected by CBC bottle, while sample for chemistry, hormone and chemokine analysis
collected by organ bottle.
42
Sample for M.HCT collected with capillary tube and at least 2/3rd of the tube should be filled for better out come
43

available. Hgb = 1/3rd of hematocrit


44
Samples from body fluids should be collected by sterile tubes (look at images in culture section below).
1577
If M.HCT is available no need of rapid Hgb test. It is used in peripheral setups where CBC machine or M.HCT are not

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Chapter 26; Common Laboratory Investigations with practical points and procedures 1578

Basic Hormonal analysis tests


✓ TFT (TSH, T4, T3)
✓ Calcitonin
✓ Erythropoietin
✓ FSH (Follicle stimulating hormone) and LH (luteinizing hormone)
✓ Serum HCG
✓ Progesterone
✓ Testosterone

Basic chemokine analysis tests


✓ PSA (prostate specific antigen)
✓ Alpha fetoprotein (AFP)
✓ CA 125, CA 19-9
✓ CEA (Carcinoembryonic antigen)
Basic clinical Serology tests include;
Urine HCG
Widal test
Weil-Felix reaction
PICT
Rapid malarial test
H. Pylori stool Ag and serum Ab test
HBsAg (Hepatitis B virus surface antigen) test
HCV ab (Hepatitis C virus antibody) test
RK- 39
VDRL (Venereal Disease Research Laboratory) and RPR
RF
ASO titer
Basic Microbiological tests
Gram stain
AFB (Aid fast bacilli)
Culture45

Practical points about sample collection [at bedside]46

Hematology
o Sample for hematology is taken by CBC bottle47. For ESR, collect adequate volume of
blood which is more than the volume of sample required for CBC. you can request
‘’CBC with ESR’’ in one request from one sample

45
Blood culture is collected with specific blood culture bottles following possible sterile techniques. Culture
from other samples (e.g, CSF, Ascitic fluid, stool and urine) can by collected with sterile tubes (sterile
urine cup for urine sample) → look at images in culture section below
46 1578
This topic is included in this text, considering most setups of Ethiopia where job description is not applied, and majority of
work load given for medical interns. The note is also very essential for medical laboratory and other health science students.
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o After taking sample mix gently and immediately to prevent coagulation


o ‘’CBC, BG & RH, Cross match’’ can be done from one sample of a patient. But, in
most setups CBC is done in hematology section of the laboratory while BG &RH done
at blood bank (or mini blood bank). So, the technician working in hematology may
discard the sample after doing CBC. To avoid this, request two papers like below
▪ Request #1 → ‘’CBC, please send sample to BG and RH’’
▪ Request #2 → ‘’BG & RH, Cross match’’
Chemistry
o Sample for chemistry is taken by Organ bottle
o Coagulation profile have its own bottle
o Don’t shake or mix the sample !!!
o During sample collection for serum electrolyte, after drawing venous blood, remove the
needle from the syringe then transfer sample from syringe into organ bottle. This is to
prevent hemolysis which significantly affect electrolyte determination
Sample for serology also collected by CBC bottle
For culture → look at specific topic below
Finally, unless you level the sample (at least by MRN and Pt’ name), all the above note will
be meaningless.

Picture; CBC bottles (EDTA blood tubes for Hematology test); These bottles are generally used for
haematology tests where whole blood is required for analysis. They have EDTA (Ethylene diamine tetra
acetic Acid) as an additive which Removes calcium, to prevent blood clotting.

Picture; Organ bottles (SST Tube with Gel and Clot Activator); SST Tube are used to collect blood for
clinical biochemistry and immunology. They can improve serum surface and prevent substance exchange

47
we use the term CBC bottle to say EDTA tube)
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between blood cell and serum. Guaranteeing biochemical character and chemical components of serum
unchanged evidently for a long time, which do not need to us special tool to transport serum. SST =
Serum separator tube

Picture; bottles for coagulation profile/PT, aPTT and INR/ sample collection (Blood PT Tube, Blood
Collection PPT Tube, Sodium Citrate Tube); these bottles have Sodium Citrate as an additive which Binds
and Forms calcium salts to remove calcium and finally prevent blood from clotting

26.1. Basic Hematology tests

26.1.1 BF (Blood film)

Blood film is done after preparing blood smear and staining with Giemsa stain
The term Giemsa stain originated from a name of German chemist and bacteriologist Gustav
Giemsa.
Reagents Required → Methanol, Giemsa powder, Glycerin, Water (Buffer)
Time of sample collection
o When the patients feels febrile
o Before anti-malaria drugs are given to the patients

Preparation of thick films


slides must be clean, free from dirt, grease and fingerprints
Mix the blood
Using an applicator stick, apply 4 drops of blood on to a microscope slide
Spread the blood without excessive stirring to form a smear approximately a cm 2, through which
newspaper print can be red. This should be approximately 5 red blood cells thick.
Allow to air dry horizontally (without using heat).
Label slides.
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preparation of thin blood smear


The microscope slides must be clean as for thick films otherwise the blood will not adhere
and the smear will be irregular.
Apply 1 drop of blood to the end of the slide, pace another slide at an angle of 45o and
bring it towards the drop of blood.
As soon as it touches it, the blood will disperse along the width of the slide.
Before it reaches the edges, pull the drop along the length of the slide.
the correct amount of blood in the drop the film will form a good tail before the end of the
slide. The film here should be 1 RBC thick. Make 2 slides for each test.
Air dry, Label slides

Diagrams; steps of thin Blood smear preparation

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Thick film considered “gold standard” for detection of parasites due to being able to use
larger volume (10µl of blood)
Thin film considered “gold standard” in species identification
Smear examinations should be under oil immersion
Negatives should not be reported until 200 oil immersion fields have been examined
Additional specimens should be examined at 12-hour intervals for a subsequent 36 hours.
Taking sample during febrile episodes of the patient increase positivity of the result
Mixed infections or low parasitemia usually difficult to diagnose.

Giemsa Preparation and staining procedure


Reagent
o Giemsa powder
o Buffered water, pH 7.1-7.2 or
o Buffered saline water, pH 7.1-7.2
10% solution for 10 minute staining
o Measure 45 ml of buffered water in 50 ml cylinder
o Add 5 ml of Giemsa stain to 50 ml mark
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o Mix gently
Gently immerse the slide into a methanol solution for proper fixation of the thin smear. But,
Do not fix thick films.
Allow to air dry.
Place the slides in a staining rod/rack
Cover the air-dried smear with a 1:10 diluted Giemsa using buffered distilled water at pH 7.2
(recommended for malaria parasites in order to stain schuffner’s granules) as a diluent
o 1:10 Giemsa =1 part of stock Giemsa + 9 parts buffered water
stain the slides as follows:
o 30 min if using 3% stain solution
o 10 min if using 10% stain solution
Wash the stain from the slide gently using clean water (not necessarily distilled water or
buffered water)
Wipe the back of each slide clean and place it in draining rack for the preparation to air dry.
Now observe the smear under a microscope.
o Focus on the film with the X10 objective.
o Examining the film first with 40x objective to select a well stained area
o Apply a drop of immersion oil on the slide and switch to the oil-immersion objective
(100).
o Examine at least 100 fields(100Xobjective)
o *P.malariae exam approximately 200 fields

☛ Note: Avoid drying of smear by an incubator or by heat, because it may fix the blood smear
onto the slide and results in lysis of RBCs.

* Identification of a schizont with >12 merozoites in the peripheral circulation is an important diagnostic clue for P. vivax. In general,

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schizonts of P. falciparum are very rarely seen in blood films; they are generally absent from the peripheral circulation except in
cases of severe infection with overwhelming parasitemia.

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Picture; Stages in humans

A negative test DOES NOT rule out malaria.

Blood smear and geimsa stain - Click on the link below and watch the video
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https://youtu.be/uVaYuq6Jzk4 2nd edition
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26.1.2 Manual hematocrit (M.HCT)

Sample for M.HCT, collected with capillary tube and at least 2/3rd of the tube should be filled
for better out come
Sample should be taken through the red/blue mark of Capillary tube which have coated
anticoagulant

Picture; capillary tubes

Pictures; Hematocrit determination after centrifugation. Left) centrifuge machine. Right) In this particular
picture, HCT measured with hematocrit scale is ≅ 50% (a) and ≅ 45% (b)

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This photo(left) shows two anticoagulated blood-filled Wintrobe hematocrit tubes following high speed centrifugation. The tube on the
left is from a normal subject, with a hematocrit of 38 percent (blue arrow). The tube on the right is from a 19-year-old female with
essential thrombocytosis, a normal white blood cell count, and a platelet count of 5,000,000/microL. The extreme degree of
thrombocytosis can be appreciated by the presence of a marked increase in the size of the "buffy coat" (white arrow). When the
Wintrobe tube is filled to near capacity (upper arrows), and the white blood cell count is not markedly elevated, the platelet count
can be estimated by the thickness of this layer, with each mm being equivalent to one million platelets/microL. In normal subjects,
the buffy coat, which is comprised of white blood cells and platelets, is only minimally visible.

26.1.3 Hemoglobin (Hgb) Determination

Picture; Hemoglobin test meters (equipment’s) or hemoglobin meters

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Picture; steps of Rapid hemoglobin determination using ‘’mission plus hemoglobin testing system’’

A) Insert 4 batteries into the battery compartment, close the battery cover and make sure
the snap is shut down
B) Insert the correct ‘’code chip’’ into the ‘’code chip slat’’ on the meter. Compare the code
number on the code chip with the code number printed on test strips canister or the
code device. Results will be inaccurate if the two numbers are not identical.
C) Turn on the meter. ‘’Setting up the Meter’’ before testing is necessary which includes;
correcting test number setup incase to test up to 999 tests with one memory of the
meter, setting 12h or 24h mode, time setup (the date, month and year), setting units
(g/dl, g/L or mmol/L) → download and watch the video from the link attached below
D) Insert the test strip into the test channel in the same direction as the arrows indicate
on the strip. Make sure that, the test strip is inserted all the way to the end of the
channel (insert the strip up to the encircled black line in the picture)
E) The ‘’blood drop symbol’’ will flash when the meter is ready for the specimen to be
applied
F) Collect capillary blood of 10 µl using a capillary transfer tube or pipette. The capillary
transfer tube will fill automatically
G) Make sure the blood covers the end of capillary transfer tube and never squeeze the
tube
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H) Apply the blood sample to the central region of specimen application area of the test
strip
I) Results will be displayed in about 15 seconds with Hgb and HCT values as shown in
the figure (Hgb = 12.9g/dl, HCT = 38%)

Mission Plus Hb Hemoglobin testing system - Click on the link below and watch the video
https://youtu.be/WO7HApAUSME

26.1.4 PM (Peripheral morphology)

Smear preparation for PM is the same as malarial thin smear preparation (look at
the section of BF above).
Review of the peripheral smear starts with choosing the best prepared and stained
slide for examination. Scanning the entire slide under low power enables selection
of an optimal area

Diagram; This schematic depicts a well-made peripheral blood smear. A drop of blood has been
placed on the left-hand side of a clean glass slide at point A, and has been pulled towards the right-
hand side using another glass slide, stopping at point B. The area near point A is too thick and too
darkly stained for interpretation, whereas the area at the very end of the smear, near point B (the
"feather edge") is too thin, distorting the morphology of all cells in that area. The optimal area for
viewing is just behind point B (shown by the asterisk), in an area where the red blood cells are just
touching and demonstrate central pallor.

There are various staining methods for PM, but most laboratories employ Wright-
Giemsa staining (look at BF section above)
For certain cases (e.g. Hematologic malignancy), pathologist evaluation of a well-
prepared smear is mandatory. Others (e.g anemia) can be evaluated by laboratory
technologist or experienced physicians.
Look at different morphologies of peripheral Blood smear from anemia section under
miscellaneous part of Nitsibin short cases. (click here →13.1. Anaemia (የደም ማነስ) )

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26.1.5 Blood group and RH (BG & RH) determination, cross match

Figure; Landsteiner’s Rule; Reciprocal antibodies are present in the sera of normal people
whose RBCs lack the corresponding antigen(s)

ABO phenotyping has two components:

Forward grouping → Direct (cell grouping)


o Testing of the red blood cells for the presence of ABO Antigens (or forward grouping).
Reverse grouping → Indirect (serum grouping)
o Testing of serum or plasma for the expected ABO Antibodies (or reverse grouping).

slide grouping
Specimen
o Patient’s serum
o Patient’s cells
Reagents and equipments:
o Anti- A and anti-B serum
o Group O serum (anti-AB)
o Antigen A and antigen B (20% known RBC suspension)
o Group AB serum (Control)
o Tile or slide

Interpretation
o Positive agglutination → antibodies specific for A/B antigen are present.
o Negative agglutination → no antibodies are present for antigens

Rh- typing
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o Administration of Rh +ve blood to Rh -ve may sensitize the person to form anti-D
antibody.
o Donation of Rh +ve blood to recipient having anti D could be
fatal.
RBCs (D-Ag) + Anti -D (antisera) → ± agglutination (ag- ab rxn)
This can be performed on slide test, saline tube test, modified tube test
Interpretation
o If there is agglutination of RBCs -------- positive for D- antigen
(Rh positive)
o If there is no agglutination of RBCs -------- the D- antigen is not
ex pressed. This can be Rh negative or Du variant.

Rh: Weak (Du) variant


➢ It is weak form of D antigen.
➢ Negative by direct (cell) typing, must be further tested for the presence of Du variants by
indirect antiglobulin test.
o Blood donor - as Rh positive
o Blood recipient – as Rh negative

Blood grouping on glass slide and Result interpretation

Picture; Reagents for blood grouping (Anti - A, Anti - B and Anti - D)

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Pictures; steps of blood grouping


A) Take blood sample from the bottle
B) Drop blood to the slide glass (4 blood sample drops are required for Anti - A, Anti - B,
Anti - D and control)
C) Add the reagents to each blood sample drop on slide
D) Mix the antibody reagents with blood using plastic sticks (as shown in the left upper
corner image), then rotate the slide gently to mix blood sample and reagent; caution not
to mix one sample drop with the other
E) Check agglutination and report the result
-
F) Final result of blood group ‘’B (B negative)’’; which is reactive for Anti - B only (no
reaction on Anti - A and Anti - D) → look at the chart below

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Picture; Blood group interpretation chart based on agglutination reaction

Click on the links below and watch the video


Blood grouping experiment - Amrita University
https://youtu.be/-jKzLLHjRfs

Blood Group test or Blood typing


https://youtu.be/Vp19SgV_BMA

Cross matching
➢ It is the last phase of pre transfusion testing
➢ It will detect ABO or Rh incompatibility
➢ There are two kinds of cross match.
1. Major cross match
2. Minor cross match

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Picture; Major vs Minor Crossmatch

Major cross match


❖ Detects antibodies in the recipient’s serum that may damage the cells of proposed serum.
❖ Recipient serum + Donor RBC → agglutination or hemolysis.
❖ Called major b/c the Abs in the recipient’s serum are most likely to destroy the donor’s RBC
❖ Result:
✓ Agglutination / hemolysis ----- incompatible
✓ No agglutination/ hemolysis ------compatible

Minor cross match

❖ Detect antibodies in donor’s serum capable of affecting the RBC of the recipient.
❖ It has minor importance.
❖ Involves testing/mixing the donor’s serum with recipient’s red cells.
✓ Donor serum + recipient RBC → agglutination/ hemolysis.
❖ Result can be interpreted like major cross match.
❖ Called minor because:
✓ Any Ab in the donor’s serum will be diluted by the large volume of the recipient’s
blood.
✓ The Ab may also be neutralized by ABH substances present in a recipient’s tissues,
so is unlikely to cause a serious reaction.
✓ The destructed RBCs of the patient may be compensated by the transfused RBC of
the donors

Table; Blood group compatibility for transfusion ( → compatible, x → incompatible)

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For more, refer under miscellaneous section of Nitsibin short case (click here → 13.2. Blood
Transfusion)

26.1.6 ESR (Erythrocyte Sedimentation Rate) (Macro and micro /µ/ ESR)

Sample should be collected with CBC bottle (ESR needs much volume of blood than CBC)
When whole blood is placed in a vertical tube, red cells will tend to fall toward the bottom.
The length of fall of erythrocyte in a given interval of time is called ESR
ESR is used to follow up patients and supportive for some disease diagnosis. But it has no
specific diagnostic value
Has 3 stages
1. Roulaex formation = 1st 10 minutes
2. Sedimentation = next 40 minutes
3. Packing of sediments = last 10 minutes

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Pictures; Diagrammatic view of ESR determination

Micro /µ/ ESR48

48
µESR is a routine investigation [especially for neonates} which can be done at bedside by any
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Pictures; µESR determination at bedside

Take sample through the red mark of capillary tube


Put the tube vertically and mark the end point (top level) of sample filled with blood
Check the result after 01 hour and measure the distance in which the blood sample falls
down from the initial maximum mark. For the picture in the right, µESR is
10mm/hr, 20mm/hr, 30mm/hr and 40mm/hr for samples of A, B, C and D
respectively.

26.2 RBS, FBS, OGTT, and HbA1c

RBS → determining serum glucose level irrespective of food intake or not (but they should
have taken food at most less than 8 hours before)
FBS → Fasting is defined as no caloric intake for at least 8 hours
OGTT→ test should be performed (as described by the WHO), using a glucose load
containing the equivalent of 75-gram anhydrous glucose dissolved in water. Then measure
glucose level after 2 hrs of taking 75-gram glucose (in our set up we use 9 vials of D40,
since 1vial of D40 is 8gram, which means 8 x 9 = 72gram)
HbA1c → determines glucose control level for the past 3 months, this is because of 3 month
life span of RBC

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Put one drop of capillary prick blood sample over the tip of the strip, and read the
result (automatic numbers as shown in the picture). If RBS is > 600mg/dl, glucometer
failed to interpret and it displays ‘’H’’ instead of numbers meaning ‘’High’’

Picture; glucometers

Picture; finger prick for RBS sample collection (also for manual hematocrit sample collection in
adults), then draw sample with capillary tube to send for laboratory (only few sample is needed,
if glucometer is available in the ward/OPD, you can take directly from fingertip to the test strip
and no need of capillary tube.)

Pictures; left) The areas of the foot of a baby or infant that are suitable for obtaining capillary blood.
Right) Heel Prick

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26.3. U/A (Urine analysis)


Urine examination includes the following

1. Gross /Macroscopic/ examination


2. Chemical Analysis (Urine Dipstick)
3. Microscopic Examination

1) Gross /Macroscopic/ examination of urine


Odor: normal urine has aromatic odor
Color: urine has different colors that can be associated with different pathological situations
o Watery to yellow → normal
o Deep yellow → concentrated urine
o Red, tea/ coca colored → hematuria
o Pussy → pyuria, infected urine
Turbidity: may indicate the presence of crystals, cells, protein
Transparency: freshly voided urine specimen is normally clear and transparent
Volume: The 24-hour urine voided by a healthy adult range from 600 to 2000ml
Oliguria: urine volume is less normal <400ml per 24 hours for prolonged period
Diuresis: temporal increment of urine due to excessive fluid intake
Polyuria: consistent elimination of an abnormally large volume of urine, over 2000ml/24hr.
Anuria: is the nearly complete absence of urine formation

i. Chemical Analysis (Urine Dipstick)

Procedure of urine dip stick

I. Immerse the reagent strip into the urine for up to 2 seconds then remove the
excess urine on the edge of the container
II. Compare the colors on the reagent area with corresponding color chart on the
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Urine dipstick interpretation


Parameter Image (report) Significance
Glucose ✓ DM
✓ renal glucosuria

Protein Proteinuria

✓ Nephrotic sxx
✓ Edema

Ketone ✓ DKA
✓ Starvation ketoacidosis

Blood Hematuria 2ry to


✓ Renal calculi
✓ Glomerulonephritis
✓ Primary or secondary Malignancy
from GUT

Bilirubin Jaundice (direct bilirubin) 2ry to


✓ CLD
✓ Biliary obstruction

Urobilinogen High → increased hepatic processing


of bilirubin
Low → bile obstruction
✓ CLD
✓ Hemolytic disorder

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Specific ✓ DI
gravity

Ph Acidic < 4.5


Alkaline > 8

✓ Respiratory or metabolic acidosis


✓ Urolithiasis

Nitrite Gram -ve bacteruria


✓ UTI
Leucocyte ✓ UTI
esterase ✓ Pyuria
✓ Urolithiasis

ii. Microscopic examination of urine


Urine preparation Procedure for microscopic examination

There are different types of specimens for urinalysis


❖ First Morning Specimen → the recommended specimen of choice. This is due to the fact that it
is generally more concentrated because of the amount of time it remained in the bladder.
❖ Random Specimen
❖ Postprandial specimen
❖ 24 hr urine
❖ Clean Catch Urine specimen
▪ Mid- stream Specimen
▪ Catheterization
❖ Once the sample of urine has been properly collected: Pour 10 to 15 ml of the well-mixed urine
in to a test tube and place it in the centrifuge (the test tube should always be balanced with a
second test tube filled with water/another urine sample) of equal volume
❖ Centrifuge the sample at low speeds of between 2,000 to 3,000 rounds per minute /RPM/ for
about 7 minutes
❖ Decant the supernate (to retain about 0.2- 0.5 ml inside the tube)
❖ Shake the tube to mix the sediment and supernate retained in the test tube
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❖ Using a pipette, collect and place a drop of the re-suspended sediment on to a microscopic
slide and place a cover slip over the drop for observation

❖ Note** If the urine sample is not analyzed within 2 hours after collection, it should be stored for
not more than 24 hours (refrigeration).

Microscopic examination and report

For urine analysis, the sediment should first be observed under low power field (LPF) when
observing for crystals, casts, squamous cells or other larger objects. When making a report, the
number of casts seen under the microscope is usually reported as the number of each type per
low power field. Moreover, low power allows for a wider view, which allows for clear observation
of the number of casts seen.

Note** - When observing the slide under low power, low light source should be used. This is
because of the fact that too much light would make it more difficult to see he cellular and
crystalline elements.
To observe and identify cells, crystals and bacteria, high power field (HPF) is used. In this case,
the types of cells will also be described as the number of each type found per the high-power
field.

Abnormal findings in urine microscopic examinations (for normal reference values click here →
Chapter 27; Reference Intervals for Laboratory Tests)

Per High Power Field (HPF) (400x)

➢ > 3 erythrocytes
➢ > 5 leukocytes
➢ > 2 renal tubular cells
➢ > 10 bacteria

Per Low Power Field (LPF) (200x)

➢ > 3 hyaline casts


➢ > 1 granular cast
➢ > 10 squamous cells (indicative of contaminated specimen)
➢ Any other cast (RBCs, WBCs)

Presence of:

➢ Fungal hyphae or yeast, parasite


➢ Pathological crystals (cystine, leucine, tyrosine)
➢ Large number of uric acid or calcium oxalate crystals

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26.4. S/E (stool examination)

For S/E, Collect the sample in a clean, water-tight dry urine free container with a tight lid.
In the case of neonates and Infants, collect from the diaper.

Saline and iodine Direct wet mount preparations:


1) Saline wet preparation:
Take one drop of 0.85% saline.
Take a small amount of stool and mix well.
The smear should be thin so that you can see the newsprint under the slide.
Put cover glass and see under the microscope 10x and 40x objective.
❖ This is best to see helminth eggs, larva, and trophozoites.

i. Iodine wet preparation → a.k.a wet preparation.

Prepare Lugol’s iodine solution


❖ Iodine solution consists of:
▪ Potassium iodide (KI) = 10 grams
▪ Iodine powder crystals = 5 grams
▪ Distilled water = 100 ml
❖ Procedure to make Lugol’s iodine solution:
▪ Dissolve KI in Distilled water.
▪ Slowly add iodine crystals.
▪ Shake the solution gently until they dissolve.
▪ Filter the solution before use, and this is the stock solution.
▪ Dilute the stock solution 1:5 with Distilled water. Make this working solution
before use.
▪ Too weak iodine solution; in that case, organisms will not stain properly.
▪ Too strong iodine solution will clump the stool.
❖ Take a drop of Lugol’s iodine solution.
❖ Take a small amount of stool and mix it well.
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❖ Make a thin smear.


❖ Put the cover glass on it and gently press it to get an evenly thin smear.
❖ See under 10x and 40x objective lenses.

Concentration methods

The main aim of the concentration method is to remove the debris. Also, when the parasite is
low in number
There are three methods used for the concentration of stool:
❖ Formalin-ethyl-acetate concentration method.
❖ Zinc-floatation method.
❖ Sheather sugar floatation method.

i. The formalin-ethyl-acetate concentration:

It is the most commonly used concentration method.


This method recovers the helminth eggs and larvae, to a lesser extent, trophozoites.
Principle → This is based on specific gravity. After centrifugation, the stool’s parasites are
heavier and settles down at the bottom as sediments. Debris is lighter and rises to the upper
layers.
Advantages are:
❖ It is easy to prepare the solution an also the procedure is easy to perform.
❖ Inexpensive
❖ There is a rare distortion of parasite forms (eggs).

The procedure of formalin-ethyl-acetate concentration:

The stool should be fixed in formalin for at least 30 minutes.


❖ Take 2 to 5 grams of the stool and mix thoroughly in the 10% formalin.
Filter the above stool in the formalin.
❖ This can be done by two layers of gauze or a wire screen and collect around 3 ml.
Add 10 to 12 mL of 0.85% saline and mix it well.
Centrifuge for 2 minutes at 2000 RPM (or2500 RPM).
Discard the supernatant and leave 1 to 1.5 mL of the sediment.
❖ If the supernatant is cloudy, then repeat the above steps of saline.
Add 9 mL of 10% formalin to the sediment.
Now add 3 mL of ethyl acetate.
Cap the test tube and shake well for 30 seconds.
Centrifuge the tubes for 1 minute at 2000 RPM
Four layers will form. The bottom is the sediment that is needed to prepare the smear.

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picture; stool formalin ethyl acetate after centrifugation


Remove the debris with a wooden applicator stick. Decant the upper three layers carefully and
leave the sediments in the test tube.
Clean the sides of the test tube with a swab.
❖ Giardia cyst may stick to the side of the test tube.
Add a few drops of the formalin and mix the sediment thoroughly. This will preserve the
sediment.
❖ Now, we can make the smears in saline and iodine wet preparation.
Examine under the microscope.

G) Zinc sulphate Floatation Method:

◼ Some authors believe it a superior method for concentration and identifying eggs and
protozoan cyst.
◼ The parasites are lighter and float on the surface, while the debris settles at the bottom.
◼ Look at the procedure in the diagram below

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Microscopic images of selected Intestinal parasites

Picture; Common nematode eggs and larvae easily recognized on microscopy (wet mount) include: (A)
Ascaris, (B) Trichuris /wet mount with iodine/, (C) hookworm (wet mount with iodine), (D) Enterobius
(pinworm), (E) Capillaria, (F) Strongyloides rhabditiform larvae.
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Ascaris eggs are large with rough surfaces and a dark dense center (A). Trichuris eggs have distinctive
mucus plugs at either end as well as a "tea tray" appearance (B). Hookworm eggs are optically clear at

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the edges with a dense center composed of one or more cells (C). Enterobius eggs have a distinctive
oval shape with slight concavity (D). Capillaria eggs are similar to Trichuris but are smaller with more
flattened ends (E). Strongyloides larva may be distinguished from hookworm larva by the presence of short
buccal cavity and primordial genitalia midway down the body (F).
The measurements given represent the range seen for the black bar lengths for each organism.

Picture; Common trematode eggs seen on easily recognized on microscopy (wet mount with iodine)
include: (A) Schistosoma mansoni, (B) Schistosoma haematobium, (C) Schistosoma japonicum, (D)
Clonorchis, (E) Fasciola, (F) Paragonimus
Schistosoma eggs are the largest of the helminths and can be distinguished by their spines which are
lateral (S. mansoni, A), terminal (S. haematobium and S. intercalatum, B), or vestigial (S. japonicum or S.
mekongi, C). Clonorchis and Opisthorchis eggs have an operculum and small remnant at the opposite end
(D). Fasciola and Fasciolopsis are also operculated but smooth (E). Paragonimus eggs are also
operculated but have a thick, almost pointed opposite end (F).
The measurements given represent the length of the eggs along the long axis for each organism.

Picture; Common cestode eggs recognized on wet mount include: (A) Taenia solium, (B) Taenia saginata,
(C) Hymenolepis nana, (D) Diphyllobothrium latum, (E) Hymenolepis diminuta, (F) Dipylidium caninum.
The eggs can be useful for diagnosis, although the primary diagnostic forms are the mature (gravid)
proglottids and the scolex. The eggs of Taenia are indistinguishable (A and B).

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Picture; Common protozoa easily recognized on microscopy include: (A) Entamoeba histolytica (trichrome
stain), (B) Giardia lamblia (wet mount), (C) Cryptosporidium (acid-fast stain), (D) Cystoisospora (wet mount
with exposure to ultraviolet light), (E) Cyclospora (wet mount), (F) Balantidium coli (wet mount with iodine).
E. histolytica may appear as a cyst form with chromatid bar (A). Giardia lamblia has distinctive flagella (B).
Cryptosporidium is small with acid-fast staining (C). Cystoisospora (formerly Isospora) has an oblong
shape, one or two nuclei, natural fluorescence, and acid-fast positivity (D). Cyclospora is similar to but
larger than Cryptosporidium, with natural fluorescence and acid-fast positivity (E). Balantidium coli is the
largest protozoan infecting humans and the only ciliate (F).
The measurements given represent the range seen for the black bar lengths for each organism.

For more images, look at investigation part of intestinal infection section of Nitsbin short cases
(click here → 9.1.1.2 Amoeba (አሜባ), 9.1.2.1 Giardia (ጃርዲያ), 9.2. Intestinal Helminthic Infestations
(የአንጀት ጥገኛ ተውሳክ ፣የአንጀት ትላትል) and blood flukes)

26.5. Serology and Rapid diagnostic tests /RDT/

26.5.1 Urine HCG49

Detect the presence of Human chorionic gonadotrophin (HCG) hormone, which is produced
by the trophoblastic tissue in the placenta
HCG has two sub units: The α sub unit & the β subunit
It has certain importance such as: To confirm pregnancy, to diagnose ectopic pregnancy and
GTD and trophoblastic tumors, testicular cancer in males.
Serum HCG reaches detectable level within 24 hours after implantation.

Methods of evaluation

49 1607
Urine HCG [strep test] is very simple test which can be performed at bedside (request ‘’urine HCG kit’’ and do it by yourself
instead of sending sample to lab, which decreases time wastage)
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2) Strip test → common in our set up


Principle:
o The test reaction is between the HCG in the urine and gold coated antibody on the
strip.
o A positive control is also impregnated on the strip so that interpretation will be very
easy.
o The preferential sample for HCG test is first morning urine
Steps and Result interpretation → look at the images below
➢ Immerse the strip on the urine sample up to the maximum line (horizontal blue
line)
➢ Lay the strip flat (you can put on the top of urine cup)
➢ Read the result within 5 minutes
▪ Double lines (control and test) → positive for HCG.
▪ Control line only → Negative for HCG
▪ Invalid result → without having any line or appearance of test line only.

The blue line indicates;


the maximum depth of
strip to be immersed on
urine

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Picures; Urine HCG strip test; A) negative urine HCG test in which only the control (C) line is visible; B)
shows positive urine HCG test in which both control (C) and test (T) line are visible. Picture taken, from two
patient samples, at private clinic in Ethiopia.

3) Direct agglutination slide test (direct latex slide test)

Principle:
o Latex reagent coated with anti-HCG antibodies + urine
o Presence of visible agglutination positive for HCG.
o No visible agglutination indicates Negative for HCG

4) Indirect agglutination slide test

Principle:
o Urine + anti-HCG antibody + latex HCG
o Presence of visible agglutination negative for HCG.
o No visible agglutination indicates positive for HCG

26.5.2 PICT

A rapid test which was previously known as provider-initiated counselling and testing (PICT).
Current recommendation is test and then counsel, so the name changed as provider-initiated
testing and counselling.
An antigen is coated on the strip with positive control.
up on addition of serum /plasma or whole blood depending on the test procedure, there will
be reaction between antigen and antibody if present in the sample.
Reactive results: two colored bars (one for the control & the other for the patient)
Non- reactive: single colored bar (positive control only)
Invalid result: without having any line.

For final result interpretation look at investigation section of RVI from long case of Nitsbin (click
here → Chapter 5; RVI (ኤችአይቪ ኤዲስ))
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26.5.3 Rapid malaria test

A 15-minute test which detects circulating malaria antigens in whole blood.


The only FDA cleared rapid malaria test.
Plasmodium falciparum → Sensitivity 95.3%, Specificity 94.2%
Plasmodium vivax → Sensitivity 68.9%, Specificity 99.8%
Note: Publications report P. ovale as being harder to detect as it only attacks young
erythrocytes
Histidine-rich protein II (HRP II) is specific to P. falciparum while aldolase is a pan-malarial
agent.
This Test has monoclonal antibodies directed against these proteins, which detects them in a
modified lateral flow format.

Procedure (steps)

Apply 15 µl of whole blood to the purple pad.


o Venous or capillary whole blood.
o EDTA collection tubes.
o Mylar-coated capillary tubes included in kit.
Apply 2 drops of Reagent to the white pad below where the blood is applied.
Apply 4 drops of Reagent to the pad located at the top of the left side of the test device.
Close the device and read in 15 minutes.

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Immage; Rapid malaria test;

A) T1 Positive → Positive result for P. falciparum (P.f.)


B) T2 Positive → Positive result for P. vivax (P.v.) or P. malariae (P.m.) or P. ovale (P.o.) In some cases
the appearance of only the T2 Line may indicate a mixed infection with two or more of P.v., P.m., and
P.o.
C) T1 + T2 Positive → Positive result for P. falciparum (P.f.) In some cases the appearance of both the
T1 and T2 Lines may indicate a mixed infection of P.f. with another species,
D) No T1 or T2 Lines → Negative result (no malaria antigens were detected)

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Pictures; RDT for malaria test; pf = P. Falciparum, pv = P. vivax, CON = control, S = place
for sample, A = place for buffer. Picture taken, from a patient sample, at private clinic in Ethiopia.

26.5.4 widal test

Measures agglutinating antibodies to O and H antigens of salmonella typhi from serum


The minimal titers defined as positive for the O (surface polysaccharide) antigens for active
infection and H (flagellar) antigens in past infection or in immunized person.
Steps;
➢ On clean slide, a drop of serum is placed (non-hemolyzed sample)
➢ Then a drop of antigen suspension is added
➢ Finally mix, look for agglutination
Widal test may be used as an adjunt to diagnosis in the proper clinical setup particularly in
children < 10 years old and travellers from nonendemic areas.
The Widal test is, however, characterized by false positive results. But we are using it
currently in our set up
Limitation of widal test
➢ False positive reactions
▪ Due to past infection
▪ Cross reaction (malaria, relapsing fever, non-typhoidal salmonella)
➢ False negative reaction
▪ Early typhoid cases
▪ Poor antigen preparation
▪ Poor transport of reagents &storage.

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Pictures; widal test reagents; +ve control, negative control, ‘’H’’ antigen and ‘’O’’ antigen. Picture
taken from a private clinic in Ethiopia.

Pictures; widal test; right) reactive widal test with clear agglutination. Picture taken, from two patient
samples, at private clinic in Ethiopia.

Widal test - Click on the link below and watch the video
https://youtu.be/dflOQ8hXUbA

N.B Salmonella typhi stool antigen test is very specific and sensitive (up to
99%) than widal test

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26.5.5 Weil-Felix slide agglutination test

A Weil-Felix reaction is a type of agglutination test in which patients’ serum is tested for
agglutinins to O antigen of certain non-motile Proteus and rickettsial strains (OX19, OX2,
OXK) to determine the presence and type of rickettsial infection
OX19, OX2 are strains of Proteus vulgaris. OXK is the strain of Proteus mirabilis.
The blood serum of a patient with suspected rickettsial disease is tested against certain
strains of (OX-2, OX-19, OX-K).
In 1915, Weil and Felix showed that serum of patients infected with any member of the
typhus group of diseases contains agglutinins for one or more strains of O X Proteus.
In cases of typhus, the reaction usually appears before the 6th day and reaches its height in
the second week.

Procedure

The Weil-Felix Test can be done as either a slide or a tube test. Here we are going to
discuss slide test
The antigens necessary (OX2, OX19, and OXK) can be obtained commercially.
On a solid surface (glass slide, tile, card), a small amount (50- 100 μL) of the patient’s
serum is placed.
A single drop of the desired antigen is added, and the resulting suspension is mixed and
then rotated for one minute.
Visible agglutination is indicative of a positive result, and corresponds roughly to a titre of
1:20.
Positive results can be further titrated using the tube method, which is more labour- intensive.

Pictures; reagents for Weil - Felix test (OX 19, OX2 and OX K)

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Pictures; Weil - Felix test procedure

Interpretation of the result

Look at Agglutination over the slide


Sera from endemic typhus agglutinate OX19, OX2.
Tick borne spotted fever agglutinate OX19, OX2.
Scrub Typhus agglutinate OXK strain
Test is negative in rickettsial pox, trench fever and Q-fever.
False positive reaction may occur in urinary or other Proteus infections Test may be negative
in 50 % scrub typhus

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Table; Interpretation of Weil - Felix result, RMSF = Rocky mountain spotted fever

Limitations of The Weil-Felix test


It suffers from poor sensitivity and specificity, with a recent study showing an overall
sensitivity as low as 33% and specificity of 46%. As a result, it has largely been supplanted
by other methods of serology, including indirect immunofluorescence antibody (IFA) testing,
which is the gold standard.
False negative reaction is common in scrub typhus.
False positive may occurs in Protues infection, Brucellosis, Borreliosis
However, in resource-limited settings (like in our set up), it still remains an important tool in
the diagnosis and identification of public health concerns, such as outbreaks of epidemic
typhus.

Weil Felix - a slide agglutination test for rickettsial disease


- Click on the link below and watch the video
https://youtu.be/ilqsQWDvggo

26.5.6 H. Pylori stool antigen and serum Ab test

Pictures; H. pylori stool antigen kits


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Diagram; steps of H. pylori antigen stool (fecal) test with kit; Detects directly the presence of H.
pylori antigen in a stool sample. A stool test can detect traces of H. pylori in the feces. This
test can be used to diagnose the infection and confirm that it has been cured after treatment.
One line = negative (control test), two line = positive, No line = invalid. The absence of the
control line, makes the result invalid. In this case, the sample must be retest.

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Diagram; H. pylori antigen stool (fecal) stripes test; Detects directly the presence of H. pylori
antigen in a stool sample. A stool test can detect traces of H. pylori in the feces. This test can
be used to diagnose the infection and confirm that it has been cured after treatment. One green
line = negative (control test), One green line AND one red line = positive, No line = invalid. The
absence of the control line, which is the upper green line, makes the result invalid. In this case,
the sample must be retest.

Picture; H. pylori serum antibody test cassette/kit/; H. pylori serum antibody test cassette or
strips detects antibodies to the bacteria and will not distinguish previous infection from a current
one. If test is negative, then it is unlikely that a person has H. pylori infection. If ordered and
positive, results should be confirmed using stool antigen or breath test. As a result, blood tests
cannot be used to see if the infection has been cured after treatment. Picture taken from a private clinic
in Ethiopia.

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Picture; H. pylori serum antibody test procedures

26.5.7 HBsAg (Hepatitis B virus surface antigen) test

Picture; HBsAg test kit

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HepBs Ag test procedure - Click on the link below and watch the video
https://youtu.be/h3iAL26d6SY

26.5.8 HCV Ab (Hepatitis C virus antibody) test

Picture; HCV antibody test kit

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Diagram; HCV antibody test procedure and result interpretation

Picture; HCV antibody positive test results

26.5.9 rk- 39 Rapid Diagnostic Test

rk- 39 (recombinant kinase 39) is a Serologic (antibody strip) test for VL


o rK39 is a 39-amino acid repeat of a kinesin-related protein cloned from Leishmania
chagasi and conserved in L. donovani complex.
it has 72% to 94 % sensitivity and 67 % to 98 % specificity
o More Specific and sensitive (reach up to 99%) in non-endemic area like south east
Asia (India)
o Not specific in endemic area like east Africa (Ethiopia, Sudan, Kenya)
Used for screening purpose
Common and available in Ethiopia.
Several brands of tests with rK39 antigen are available. The widely available rK39 test in the
market include Kalaazar Detect™ InBios, DiaMed-IT-Leish, etc.
So, always read the package inserted carefully and follow the manufacturer’s instructions.
Some brands can be used only with serum, while others can be used with whole blood
collected by finger prick
Procedure (see pictures below); In general, the test procedure is as follows;
o Remove the test strip from the pouch and place it on a flat surface.
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oPlace a specified amount of patient specimen (serum or finger-prick blood) on the


absorbent pad on the bottom of the strip.
o Add the specified amount of buffer provided.
o Read the result after 10 - 20 minutes according to the manufacturer’s instructions.
Some brands require a slightly different procedure, for example:
o Take a test tube or a U-bottom microtitre plate.
o Add a specified amount of buffer to the tube or well.
o Add a specified amount of specimen (blood or serum) to the tube or well and mix.
o Immerse the test strip into the buffer-specimen mixture.
o Read the result after 10 - 20 minutes according to the manufacturer’s instructions.

Interpretation of the test

Positive result: When both, control and test lines, appear, the sample tested has antibodies
against recombinant K39 antigen of Leishmania. Even a faint line should be considered
positive.
Negative result: When only the control line appears, there are no antibodies against
recombinant K39 antigen of Leishmania present in the patient’s sample.
Invalid result: When no control line appears, a fresh patient sample should be tested with a
new strip.

Advantages and disadvantages of the rK39 test

Advantages
o Simple to perform with minimal training.
o Does not require a laboratory.
o Can be performed with finger-prick whole blood, serum or plasma.
o Kits can be transported and stored at ambient temperature (up to 30 °C).
o Results are available within 10–20 minutes
Disadvantages
o Cannot distinguish between active cases and relapse in previously treated cases.
Therefore, interpretation must always be accompanied by clinical case definition.
o In patients with advanced HIV infection, a negative result does not rule out VL
diagnosis.

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26.5.10 RPR (Rapid reagain card test for syphilis)

Materials

The following are provided in the test kits:


Reagin antigen suspension
Reagin positive control serum
Reagin negative control serum
Reagin test card
Dispensing bottle and needle
Dropper tubes
Mixing sticks

Procedure

Let the reagents and specimens warm up to room temperature.


Dispense one drop of negative control serum on to one circle on the test card using a
disposable dropper tube.
Repeat step two with the positive control serum using a clean dropper tube.
Dispense on drop of each sample serum or plasma on to one circle on the card using a
clean dropper tube for each specimen.
Spread all the drops to cover the whole area of the circles using the mixing sticks.
Mix with reagain antigen suspension in the dispensing bottle. Hold the bottle vertically and
dispense one drop on to each test sample. Do not mix again.
Place the card on the rotor for 8 minutes at 100rpm.

Reading the results

Negative result:
o The carbon particles remain in an even suspension = Non reactive
Positive result:
o The carbon particles clump together = Reactive

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26.5.11 VDRL Slide Qualitative Test

Procedure:

Pipette 0.05ml or 1drop of inactivated serum into one ring of the ringed glass slide.
Add one-drop (1/60ml) antigen suspension onto each serum.
Rotate slide for 4 minutes. (If rotated by hand on a flat surface, this movement should
roughly circumscribed a 2 inch/5mm diameter circle).
Tests are read immediately after rotation microscopically with a 10x ocular and a 10x
objective.

Reading and reporting of results

Tests are read microscopically with low power objective at 10x magnification, which appears
short rod forms. Aggregation of these particles into large or small clumps is interpreted in
degrees of
Reporting system
o No clumping or very slight roughness: Non-reactive (NR)
o Small clumps: Weakly reactive (WR)
o Medium and large clumps: Reactive (R)

26.5.12 ASO latex slide agglutination test

Procedure: (Qualitative slide method)

Allow each component to reach room temperature.


Gently shake the latex reagent to disperse the particles.
Place a drop of undiluted serum on to the circle of the test slide using the disposable
pipettes provided.
Add one drop of the latex reagent next to the drop of serum.
Spread the latex reagent and serum sample over the entire area of the test circle.
See for agglutination by tilting the test slid for 2 min.

Interpretation

Agglutination indicates a positive result which 200IU/ml and no agglutination indicates a


negative result, which are 200IU/ml provided that the controls have given the expected
results.

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26.6. Basic microbiological tests


26.6.1 AFB

The detection of acid-fast bacilli (AFB) on microscopic examination of stained sputum smears
is the most rapid and inexpensive TB diagnostic tool.
A serious of at least 3 single specimens should be collected in 8 to 24 hours interval (with
at least one specimen obtained early in the morning) which should be submitted to the
laboratory for AFB smear and mycobacterial culture, although the diagnosis often can be
made with 2 specimens
o Spot - morning - spot examination (currently we are using spot - spot
examination only)
If pt present with dry cough, use induced sputum with BAL or hypertonic saline
method
Sputum AFB smears are relatively less sensitive (45 - 80%) than nucleic acid amplification
(NAA) or culture; approximately 10,000 bacilli per mL are needed for detection of bacteria in
AFB smear using light microscopy.
AFB sensitivity from Pleural fluid is 10 - 25%

Ziehl-Neelsen staining technique

The Ziehl-Neelsen staining technique is a differential staining technique that was initially
developed by Ziehl and modified later by Neelsen, hence the name Ziehl-Neelsen stain.
The Mycobacterial cell is difficult to stain by gram staining because they possess a
waxy envelope and a special method has to be used.
Besides being difficult to stain, once it is stained the organism is hard to decolorize.
Acid-fast bacteria can’t be affected by acid alcohol or 20% sulphuric acid, so named as acid
fast.
Required reagents → CAM
o Carbol-fuchsin → primary stain
o Acid-Alcohol → 20% sulphuric acid as Decolorizer
o Methylene blue/Malachite green → counterstain
Procedure
o Prepare the smear from the primary specimen and fix it by passing through the flame
and label clearly
o Place fixed slide on a staining rack and cover each slide with concentrated carbol
fuchsin solution.
o Heat the slide from underneath with sprit lamp until vapor rises (do not boil it) and wait
for 3-5 minutes.
o Wash off the stain with clean water.
o Cover the smear with 3% acid-alcohol solution until all color is removed (two minutes).
o Wash off the stain and cover the slide with 1% methylene
o Blue for one minute.
o
o
Wash off the stain with clean water and let it air-dry.
Examine the smear under the oil immersion objective to look for acid fast bacilli.
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Results and Interpretation


o Acid-fast bacteria retain the primary dye, carbol-fuschin, and stain pink or Red
o Non-acid fast bacteria take up the methylene blue dye and appear Dark blue or Blue.
Applications of Ziehl-Neelsen Staining
o Used for examination and identification of Mycobacterium species including M.
tuberculosis and M. leprae.
o Used to differentiate between acid-fast and non-acid fast bacilli
o Used for the identification of some fungal species such as Cryptosporidium.

Pictures; Acid-fast bacillus smear showing M. tuberculosis bacilli

How to do an acid fast- staining - Click on the link below and watch the video

https://youtu.be/faB_5STfZH8

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26.6.2 Gram stain

Gram stain is a special stain for the diagnosis of the gram-positive or gram-negative
organism in various samples like sputum, pus, CSF, urine, tissue, sample from infected ulcer
or wound etc.
Gram stain divides bacteria in to two physiologic groups, gram positive &gram
negative
The name comes from its inventor, Hans Christian Gram. He published a gram stain method in
1884.
Indication
✓ To differentiate between gram-positive and gram-negative organisms
✓ To diagnosis the presence of bacteria in sputum, pus, or any other tissue or fluids.
✓ CSF gram stain to diagnose bacterial meningitis.
✓ It can stain yeast and this needs to be reported.
Required reagents → Come In And Stain
o Crystal violet → Primary stain
o Gram’s Iodine → mordant
o Acetone-Alcohol → decolorizer
o Safranin O → counter stain, secondary stain
Procedure → look at the graphs below
o Prepare smear from specimen or culture.
o Allow the smear to air-dry.
o Rapidly pass slide three times through flame.
o Cover fixed smear with crystal violet for one minute and wash with tap water.
o Tip off the water and cover the smear with Gram’s iodine for one minute.
o Wash off iodine solution with tap water.
o Decolorize with acetone-alcohol for 30 seconds.
▪ N.B. A gram-negative bacterium has a high lipid content in outer cell
membrane which dissolves in the decolorization process, where the
complex will also be washed of, and stain with counter stain (next step)
▪ While in Gram-positive bacteria cell membrane remain intact and the stain
will not be washed off after alcohol treatment.
o Wash off the acetone-alcohol with clean water.
o Cover the smear with safranin for one minute.
▪ In gram, positive bacteria counterstain cannot enter so the bacteria are
purple.
▪ While in gram-negative bacteria safranin can enter and give pink color.
o Wash off the stain and wipe the back of the slide. Let the
o smear air-dry.
o Observe under microscope and report the result (Examine the stained smear
with oil immersion objective to look for bacteria).
▪ Gram positive bacteria → retain the primary stain, violet or deep
purple in color 1628
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▪ Gram negative bacteria → stain with counter stain, appear are pink,
magenta color.
▪ Yeast cells → Dark purple
▪ Nuclei of pus cell → Red
▪ Epithelia cells → Pale red

Table; Interpreting gram stain results*


Gram positive Gram negative (G-ve)
G +ve cocci G +ve bacilli (rods)
#
G -ve cocci G -ve bacilli
(rods)$
Clusters Chains

* Look at culture section, below for each bacterial differentiation with examples
#
Gram +ve bacilli can be large, medium, small or branching
$
G -ve bacilli can be Medium to long[plump], Medium to long [thin], Short to long [pleomorphic], Tiny, Curved

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Gram stain - Click on the link below and watch the video
https://youtu.be/ccMvyBcxvJc

26.6.3 Culture & biochemical tests

Culture is artificial cultivation of microorganisms in the laboratory


It is important for isolation and identification of microorganisms based on different
characteristics such as
o Colony characteristics
o Ability to produce pigments
o Hemolysis
o Ability to metabolize different nutrients
o Ability to produce gas

Practical points about sample collection for culture [at bedside]

i. Blood culture

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Picture; steps of blood culture collection in best setups


A) Mark the blood culture bottle at 10ml to take adequate sample; in addition, bottle should be
labeled with patients name, age, sex, date and time of collection, ward
B) Clean the cover area of the bottle
C) Clean and sanitize the sample taking site of the patient
D) Connect bottle to the adapter
E) Insert needle tip of the adapter to patients’ vein
F) Hold and wait until adequate sample is taken
G) Check that, correct volume was taken and send sample to lab immediately. Culture result
usually expected after 05 days of inoculation in culture media.

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Picture; steps of blood culture collection in our set up


A) → Mark the blood culture bottle at 10ml to take adequate sample; in addition, bottle should
be labeled with patients name, age, sex, date and time of collection, ward
B) → Clean the cover area of the bottle
C) → Clean and sanitize the sample taking site of the patient with possible aseptic techniques.
D) 1 → connect sterile IV set with 10cc syringe [as shown in the picture], then draw 10ml of
blood. This method avoids direct syringe contact with skin, which decreases contamination of
sample with skin normal flora

D2 → if D1 is not possible, draw blood directly from vein with 10 cc syringe, keeping possible
aseptic techniques to decreases contamination of sample with skin normal flora

E) Insert needle into a tube containing a culture medium and push the plunger into the barrel to
expel contents of the needle onto the side walls of the tube or directly into the liquid phase
of the medium (caution !!! → don’t open the cap /cover/ of culture bottle at any time of
sample collection). Check that, correct volume was taken and send sample to lab immediately
after filling the culture request slip. Culture result usually expected after 05 days of
inoculation in culture media.

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B) Urine culture

Sample
➢ Early morning clean catch mid-stream urine which is collected aseptically by sterile
urine cup OR Supra pubic aspirates. For neonates and children urine is collected
by sterile plastic bags
➢ Foley catheter
o Urine should be aspirated from the distal end of the catheter with sterile syringe
after disinfecting the area (avoid sample taking from the urine bag)
o Urine specimen should be obtained aseptically without opening the catheter
collection junction
Transport to the laboratory within 01 to 02 hours; if not, keep at 40C to avoid multiplication of
bacteria in urine
24hr urine cultures are not recommended

Pictures; sterile urine cup for urine culture sample collection

to 20 degrees cephalad. right) urine culture sample collection from foley catheter system; Ideally urine samples for 1633
Picture; left) suprapubic aspiration; The needle is inserted one to two centimeters above the pubic symphysis and angled 10

culture should be obtained by removing the indwelling catheter and obtaining a midstream specimen. If ongoing catheterization is

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Chapter 26; Common Laboratory Investigations with practical points and procedures 1634

needed, ideally the catheter should be replaced prior to collecting a urine sample for culture, to avoid culturing bacteria present in
the biofilm of the catheter but not in the bladder. Many systems have a "needleless" site that can be cleansed prior to specimen
collection. If a sample is being collected without catheter removal, urine should be obtained from the port in the drainage system. For
circumstances in which the above approaches are not possible, the culture should be obtained by separating the catheter from the
drainage system. Although this approach is associated with some risk of introducing microbes into the closed system, culture results
from urine collected from the drainage bag cannot be used to guide treatment.

C) Stool culture

◼ Stool sample for culture can be collected by a clean, water-tight dry urine free container
with a tight lid
◼ Then place some amount of stool, from the container into sterile culture tube using
applicator stick. The stick is available together with sterile tube
◼ Mix well with the buffer [all sterile tubes of stool culture have buffer inside] inside the tube
and level the tube before sending to laboratory.

A) CSF Culture

B) Culture from body fluids and wound discharge

Culture from stool, CSF and other body sites collected by sterile tubes
Sterile Swab is needed [usually available together with sterile tube] to collect stool into sterile
tube
Sterile swab also used to take sample from ulcer and wound discharge

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Pictures; sterile culture tubes

Pictures; sterile culture tubes with [cotton] swab stick

Culture media
A) Blood agar

Supports the growth of many bacterial pathogens (except H. influenzae).


Blood agar culture plates are also useful for observing hemolysis (the ability of bacterial colonies
to break down red blood cells).
Types of hemolysis — The presence of and type of hemolysis is useful for classifying
streptococcal species
❖ Alpha /𝜶/ hemolysis (incomplete or partial hemolysis) → is caused by bacterial production of
hydrogen peroxide, which in turn oxidizes hemoglobin (red) to methemoglobin (green). S.
pneumoniae and viridans streptococci display alpha hemolysis

❖ Beta/𝜷/ hemolysis (complete red cell lysis) → results in transparency in the normally red agar
media. This transparency is typically present around and under the colonies. Streptococcus

S. agalactiae and C. perfringens) may induce intense beta hemolysis when grown concurrently
with S. aureus.
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pyogenes and Listeria typically display beta hemolysis. Some weakly beta-hemolytic species (eg,

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❖ Gamma /𝜸/ hemolysis (no hemolysis) → results in no change in the agar color around and
under the colony. Enterococcus faecalis (formerly group D Streptococcus) displays gamma
hemolysis.
❖ Hemolytic streptococci are further categorized by Lancefield grouping (see below)

Chocolate agar → named for its brown color

MacConkey agar → selective medium designed to detect gram-


negative bacteria

Selective medias 1636


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Helps to detect specific pathogenic organisms growing concurrently with normal colonizing
bacteria in specimens collected from nonsterile sites.
Pathogens that may be identified with selective media include Bordetella pertussis, Salmonella
species, Shigella species, N. gonorrhoeae, and Legionella pneumophila

Biochemical tests (Bench tests)


Catalase test → used to distinguish staphylococci (catalase +ve) from streptococci (catalase -ve)
and enterococci.

Coagulase test → used to differentiate S. aureus from other staphylococci (CoNS /S.
epidermidis/)

Oxidase test 1637


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Used to differentiate gram-negative bacilli based on their production of certain cytochrome c


oxidases.
A positive result is indicated by a purple color change that is detectable within a few seconds.
Oxidase-positive organisms include → P. aeruginosa, Pasteurella multocida, Vibrio, and
Aeromonas species.
Oxidase-negative organisms include → Enterobacteriaceae (such as E. coli, K. pneumoniae,
Enterobacter cloacae, Serratia spp) and Acinetobacter species.

Lancefield grouping
Lancefield grouping of hemolytic streptococci groups are based on specific carbohydrates in the
bacterial cell wall that allow agglutination with particular antisera. Not all streptococci can be
grouped; some species such as S. pneumoniae do not express Lancefield antigens
usually used to identify beta-hemolytic streptococci but may also be used to help identify other
streptococci and enterococci. For example, Enterococcus species are usually group D; S.
anginosus group are frequently group F but may be groups A, C, or G.

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For antibiotics sensitivity and antibiotic coverage of each bacteria click here → Chapter 23;
Basics about rational use of antibiotics

Further reading → UpToDate 2018 (Approach to Gram stain and culture results in the
microbiology laboratory, culture section)

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Chapter 27; Reference Intervals for Laboratory Tests


Dr. Mulualem. G

Analyte SI unit Conventional units


Hematology
CBC (Complete blood count)
Leucocyte with Alkaline phosphatase 0.2–1.6 μkat/L 13–100 μ/L
Differential blood count (ALP)
WBC 3.54–9.06 × 109/L 3.54–9.06 ×
103/mm3
Neutrophils 0.40–0.70 40–70%
Relativ Bands 0.0–0.05 0–5%
e Lymphocytes 0.20–0.50 20–50%
counts: Monocytes 0.04–0.08 4–8%
Eosinophils 0.0–0.6 0–6%
Basophils 0.0–0.02 0–2%
Neutrophils 1.42–6.34 × 109/L 1420–6340/mm3
Bands 0–0.45 × 109/L 0–450/mm3
Absolu Lymphocytes 0.71–4.53 × 109/L 710–4530/mm3
te
counts Monocytes 0.14–0.72 × 109/L 140–720/mm3
: Eosinophils 0–0.54 × 109/L 0–540/mm3
Basophils 0–0.18 × 109/L 0–180/mm3
Erythrocyte count Adult males 4.30–5.60 × 109/L 4.30–5.60 ×
106/mm3
Adult females 4.00–5.20 × 1012/L 4.00–5.20 × 106/mm
Hematocrit Adult males 0.388–0.464 38.8–46.4
Adult females 0.354–0.444 35.4–44.4
Hemoglobin Plasma 6–50 mg/L 0.6–5.0 mg/dL
Whole Adult males 133–162 g/L 13.3–16.2 g/dL
blood: Adult 120–158 g/L 12.0–15.8 g/dl
females
Mean corpuscular hemoglobin (MCH) 26.7–31.9 pg/cell 26.7–31.9 pg/cell
Mean corpuscular hemoglobin concentration (MCHC) 323–359 g/L 32.3–35.9 g/dL
Mean corpuscular hemoglobin of reticulocytes (CH) 24–36 pg 24–36 pg
Mean corpuscular volume (MCV) 79–93.3 fL 79–93.3 μm3
Mean platelet volume (MPV) 9.00–12.95 fL 9.00–12.95
Platelet count 165–415 × 109/L 165–415 × 103/mm3
Platelet, mean volume 6.4–11 Fl 6.4–11.0 μm3
Reticulocyt Adult males 0.008–0.023 red 0.8–2.3% red cells
e count cells
Adult females 0.008–0.020 red
cells 1640
0.8–2.0% red cells

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ESR Females 0–20 mm/h 0–20 mm/h


Males 0–15 mm/h 0–15 mm/h
CRP <10 mg/L <10 mg/L
CRP, high Cardiac Low <1.0 mg/L <1.0 mg/L
sensitivity risk Average 1.0–3.0 mg/L 1.0–3.0 mg/L
High >3.0 mg/L >3.0 mg/L
D-dimer 220–740 ng/mL FEU 220–740 ng/mL FEU

Chemistry including Hormonal, Immunology and chemokine analysis

Electrolyte Sodium 136–146 mmol/L 136–146 meq/L


s Potassium 3.5–5.0 mmol/L 3.5–5.0 meq/L
Chloride 102–109 mmol/L 102–109 meq/L
Calcium 2.2–2.6 mmol/L 8.7–10.2 mg/dL
Calcium, ionized 1.12–1.32 mmol/L 4.5–5.3 mg/dL
Phosphorus, inorganic 0.81–1.4 mmol/L 2.5–4.3 mg/dL
Magnesium 0.62–0.95 mmol/L 1.5–2.3 mg/dL
Alanine aminotransferase (ALT, SGPT) 0.12–0.70 μkat/L 7–41 U/L
Liver Aspartate aminotransferase (AST, SGOT) 0.20–0.65 μkat/L 12–38 U/L
enzymes Gamma glutamyl transferase (GGT) 0.15–0.99 μkat/L 9–58 U/L
Phosphatase, alkaline (ALP) 0.56–1.63 μkat/L 33–96 U/L
ALP, bone Male ≤20 μg/L ≤20 ng/mL
Female Premenopausal ≤14 μg/L ≤14 ng/mL
Postmenopausal ≤22 μg/L ≤22 ng/mL
LFT Albumin 40–50 g/L 4.0–5.0 mg/dl
Protein, total 67–86 g/L 6.7–8.6 g/dL
Total 5.1–22 μmol/L 0.3–1.3 mg/dL
Bilirubin Direct 1.7–6.8 μmol/L 0.1–0.4 mg/dL
Indirect 3.4–15.2 μmol/L 0.2–0.9 mg/dL
RFT Female 44–80 μmol/L 0.5–0.9 mg/dL
Creatinine Male 53–106 μmol/L 0.6–1.2 mg/dL
Blood Urea nitrogen (BUN) 2.5–7.1 mmol/L 7–20 mg/dL

Urea = 2.14 X BUN (since 60 ⁄28 = 2.14)


MW of urea = 60, MW of BUN = 28
TFT TSH (thyrotropin) 0.34–4.25 mIU/L 0.34–4.25 μIU/mL
Thyroxine, free (fT4) 9.0–16 pmol/L 0.7–1.24 ng/dL
Thyroxine, total (T4) 70–151 nmol/L 5.4–11.7 μg/Dl
Triiodothyronine, free (fT3) 3.7–6.5 pmol/L 2.4–4.2 pg/mL
Triiodothyronine, total (T3) 1.2–2.1 nmol/L 77–135 ng/dL
Thyroglobulin 13–318 μg/L 1.3–31.8 ng/mL
Thyrotropin receptor antibody ≤1.75 IU/L ≤1.75 mIU/mL
Calcitonin Male 0–7.5 ng/L 0–7.5 pg/mL
Female 0–5.1 ng/L 0–5.1 pg/mL 1641
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Lipid Ranges depend on individual patient factors; see 2013 ACC/AHA Guideline on the
profile Treatment of Blood Cholesterol
Cholesterol Total Normal < 5.17 mmol/L <200 mg/dL
Borderline 5.17 - 6.18 mmol/L 200 - 239 mg/dL
High ≥ 6.21 mmol/L ≥ 240 mg/dL
HDL Normal ≥ 1.55 mmol/L ≥ 60 mg/dL
Lower < 1.03 mmol/L < 40 mg/dL
LDL 1.8 - 4.9 mmol/L 70 -190 mg/dL
Triglycerides Normal 0.34–1.69 mmol/L 30–149 mg/dL
(Triglycerides should Mildly elevated 1.7 - 5.6 mmol/L 150- 499 mg/dL
be measured after Moderately elevated 5.6 - 10.0 mmol/L 500 - 886 mg/dL
fasting for 12 to 14 Very high > 10.0 mmol/L > 886 mg/dL
hours)
Coagulatio The normal range varies by laboratory and reagent/instrument combination
n profile PT (Prothrombin time) 11–13 second
aPTT (Activated partial thromboplastin time) 25 - 35 seconds.
➢ For heparin monitoring, it is recommended
that each laboratory establish the therapeutic
range by determining the aPTT range that
corresponds to 0.2 to 0.4 units/mL by
protamine titration or 0.3 to 0.7 anti-factor Xa
units/mL.
INR (international normalized ratio) Therapeutic range 2-3 (dimensionless)
𝐏𝐚𝐭𝐢𝐞𝐧𝐭 𝐏𝐓 ISI
INR = [ ]
𝐂𝐨𝐧𝐭𝐫𝐨𝐥 𝐏𝐓
ISI = international sensitivity index
TT (thrombin time) 14 to 19 seconds
Bleeding time Bleeding usually stops within 4-8 min
Troponin I (99th percentile of a healthy population) Method-dependent Method-dependent
Troponin T (99th percentile of a healthy population) 0–14 ng/L 0–14 ng/L
Rheumatoid factor <15 kIU/L <15 IU/mL
Anti CCP (Cyclic Citrullinated peptide) < 5 IU/mL
Uric acid Females 0.15–0.33 mmol/L 2.5–5.6 mg/dL
Males 0.18–0.41 mmol/L 3.1–7.0 mg/dL
Antinuclear antibody (ANA) Not applicable Negative at 1:40
Quantitative 0 – 40 AU/mL
B-type natriuretic peptide (BNP) Age and gender <100 ng/L <100 pg/mL
specific:
Creatine kinase (total) Females 0.66–4.0 μkat/L 39–238 U/L
Males 0.87−5.0 μkat/L 51–294 U/L
Creatine kinase-MB Mass 0.0–5.5 μg/L 0.0–5.5 ng/mL
Fraction of total activity 0–0.04 0–4.0%
(by electrophoresis)
Anti-thyroglobulin antibody <40 KIU/mL <40 IU/mL
Anti-Smith antibody Not applicable <1.0 U
Anti-smooth muscle antibody Not applicable 1.0 U
Adrenocorticotropin (ACTH)
Erythropoietin
1.3–16.7 pmol/L
4–27 U/L
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6.0–76.0 pg/mL
4–27 U/L
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Ferritin Female 10–150 μg/L 10–150 ng/mL


Male 29−248 μg/L 29–248 ng/mL
Iron 7–25 μmol/L 41–141 μg/dL
Iron-binding capacity 45–73 μmol/L 251–406 μg/dL
Serum Vitamin B12 Level 200 – 1100 pg/ml
Serum folate level 2.5 – 20 ng/ml
Chemokin Alpha fetoprotein/AFP/ (adult) 0–8.5 μg/L 0–8.5 ng/ml
es Prostate-specific antigen (PSA) 0.0–4.0 μg/L 0.0–4.0 ng/mL
Prostate-specific antigen, free >0.25 decreased risk >25% decreased risk
With total PSA between 4 and 10 μg/L and of prostate cancer. of prostate cancer
when the free PSA is:
<0.10 increased risk <10% increased risk
of prostate cancer of prostate cancer
Lactate dehydrogenase (LDH) 2.0–3.8 μkat/L 115–221 U/L
CA 125 <35 kU/L <35 U/mL
CA 19-9 <37 kU/L <37 U/mL
CA 15-3 <33 kU/L <33 U/mL
CA 27-29 0–40 kU/L 0–40 U/mL
Carcinoembryonic Nonsmokers 0.0–3.0 μg/L 0.0–3.0 ng/mL
antigen (CEA) Smokers 0.0–5.0 μg/L 0.0–5.0 ng/mL
Femal Menstrua Follicular 3.0–20.0 IU/L 3.0–20.0 mIU/mL
FSH e ting phase
Ovulatory 9.0–26.0 IU/L 9.0–26.0 mIU/mL
phase
Luteal phase 1.0–12.0 IU/L 1.0–12.0 mIU/mL
Postmenopausal 18.0–153.0 IU/L 18.0–153.0 mIU/mL
Male 1.0–12.0 IU/L 1.0–12.0 mIU/mL
LH Femal Menstrua Follicular 2.0–15.0 U/L 2.0–15.0 mIU/mL
e ting phase
Ovulatory 22.0–105.0 U/L 22.0–105.0 mIU/mL
phase
Luteal phase 0.6–19.0 U/L 0.6–19.0 mIU/mL
Postmenopausal 16.0–64.0 U/L 16.0–64.0 mIU/mL
Male 2.0–12.0 U/L 2.0–12.0 mIU/mL
Serum HCG Nonpregnant female <5 IU/L <5 mIU/mL
1–2 weeks postconception 9–130 IU/L 9–130 mIU/mL
2–3 weeks postconception 75–2600 IU/L 75–2600 mIU/mL
3–4 weeks postconception 850–20,800 IU/L 850–20,800 mIU/mL
4–5 weeks postconception 4000–100,200 IU/L 4000–100,200
mIU/mL
5–10 weeks postconception 11,500–289,000 IU/L 11,500–
289,000mIU/mL
10–14 weeks postconception 18,300–137,000 IU/L 18,300–

Second trimester 1400–53,000 IU/L


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137,000mIU/mL
1400–53,000
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mIU/mL
Third trimester 940–60,000 IU/L 940–60,000 mIU/mL
Progesterone Femal Follicular <3.18 nmol/L <1.0 ng/mL
e: Midluteal 9.54–63.6 nmol/L 3–20 ng/mL
Male <3.18 nmol/L <1.0 ng/mL

17- Hydroxy Male <4.17 nmol/L <139 ng/dl


progesterone (adult) Femal Follicular phase 0.45–2.1 nmol/L 15–70 ng/dL
e: Luteal phase 1.05–8.7 nmol/L 35–290 ng/dL
Testosterone, free Female, adult 10.4–65.9 pmol/L 3–19 pg/mL
Male, adult 312–1041 pmol/L 90–300 pg/mL
Testosterone, total, Female 0.21–2.98 nmol/L 6–86 ng/dL
Male 9.36–37.10 nmol/L 270–1070 ng/dL
Prolactin Male 53–360 mg/L 2.5–17 ng/mL
Female 40–530 mg/L 1.9–25 ng/mL
Lamellar body count (LBC) Immature <15,000/μL 15,000–50,000/μL
Indeterminate 15,000-50,000/μL 15,000-50,000/μL
Mature >50,000/μL >50,000/μL
Lecithin/sphingomyelin (L/S) Immature ≤1.5 ≤1.5
ratio Transitional 1.5–1.9 1.5–1.9
Mature 2.0–2.5 or greater 2.0–2.5 or greater
Cortisol Fasting, 8 a.m.–12 noon 138–690 nmol/L 5–25 μg/dL
12 noon–8 p.m. 138–414 nmol/L 5–15 μg/dL
8 p.m.–8 a.m. 0–276 nmol/L 0–10 μg/dL
Alpha1 antitrypsin (AAT) 1.0–2.0 g/L 100–200 mg/dL
Ammonia, as NH3 11–35 μmol/L 19–60 μg/dL
Amylase (method dependent) 0.34–1.6 μkat/L 20–96 U/L
Insulin 14.35–143.5 pmol/L 2–20 μU/mL
Glucagon 40–130 ng/L 40–130 pg/mL
Glucose 3.6–5.3 mmol/L 65–95 mg/dL
Glucose Normal 4.2–5.6 mmol/L 75–100 mg/dL
(fasting)/FB Increased risk for diabetes (Impaired 5.6–6.9 mmol/L 100–125 mg/dL
S/ Glucose level)
Diabetes mellitus FBS ≥7.0 mmol/L FBS ≥126 mg/dL
OGTT ≥11.1 mmol/L OGTT ≥200 mg/dL
RBS ≥11.1 mmol/L in RBS ≥200 mg/dL in
symptomatic pt symptomatic pt
Hemoglobin Alc Normal 0.04–0.06 Hgb 4.0–5.6%
fraction
Prediabetes 0.057–0.064 Hgb 5.7–6.4%
fraction
Diabetes mellitus HBA1c level ≥ 0.065 HBA1c level of
Hgb fraction as ≥6.5% as suggested
suggested by the
ADA
by the ADA
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C peptide 0.27–1.19 nmol/L 0.8–3.5 ng/mL


Gastrin <100 ng/L <100 pg/mL
Growth hormone 0–5 μg/L 0–5 ng/mL
Somatostatin <25 ng/L <25 pg/mL
β-Hydroxybutyrate 60–170 μmol/L 0.6–1.8 mg/dL
Ketone (acetone) Negative Negative
Lactate Arterial 0.5–1.6 mmol/L 4.5–14.4 mg/dL
Venous 0.5–2.2 mmol/L 4.5–19.8 mg/dL
Protein C Total antigen 0.70–1.40 70–140%
Functional 0.70–1.30 70–130%
Protein S Total antigen 0.70–1.40 70–140%
Functional 0.65–1.40 65–140%
Free antigen 0.70–1.40 70–140%
U/A (urine analysis)
Sediment Red blood cells 0–2/high-power field
White blood cells 0–2/high-power field
Hyaline casts 0–5/low-power field
Bacteria
Crystals
Bladder cells
Squamous cells
Tubular cells
Broad casts None
Epithelial cell casts
Granular casts
Red blood cell casts
Waxy casts
White cell casts
Ph 5.0–9.0 5.0–9.0
Specific gravity: After 12-h fluid >1.025 >1.025
restriction
After 12-h deliberate ≤1.003 ≤1.003
water intake
Protein <0.15 g/d <150 mg/dl (+2 or
less)
Protein/creatinine ratio Male: 15–68 mg/g 15–68 mg/g
Female: 10–107 mg/g 10–107 mg/g
Microalbumin Normal 0.0–0.03 g/d 0–30 mg/d
Microalbuminuria 0.03–0.30 g/d 30–300 mg/d
Clinical albuminuria >0.3 g/d >300 mg/d
Microalbumin/creatinine ratio Normal 0–3.4 g/mol creatinine 0–30 μg/mg creatinine
Microalbuminuria 3.4–34 g/mol 30–300 μg/mg
creatinine creatinine
Clinical albuminuria >34 g/mol creatinine >300 μg/mg creatinine
24hr urine protein 15 – 150 mg/24hr
Ketone (acetone)
Glucose (glucose oxidase method)
Negative
0.3–1.7 mmol/d
Negative 1645
50–300 mg/dl (+1 or
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Chapter 27; Reference Intervals for Laboratory Tests 1646

less)
Oxalate Male 80–500 μmol/d 7–44 mg/d
Female 45–350 μmol/d 4–31 mg/d
Osmolality 100–800 mosm/kg 100–800 mosm/kg
Phosphate (phosphorus) (varies with intake) 12.9–42.0 mmol/d 400–1300 mg/d
Urea nitrogen 214–607 mmol/d 6–17 g/d
Uric acid (normal diet) 1.49–4.76 mmol/d 250–800 mg/d
Vanillylmandelic acid (VMA) <30 μmol/d <6 mg/d
Acidity, titratable 20–40 mmol/d 20–40 meq/d
Glomerular filtration rate (GFR) >60 mL/min/1.73 m2 >60 mL/min/1.73 m2
(For African Americans, (For African Americans,
multiply the result by multiply the result by
1.21) 1.21)
Arterial blood gas analysis Arterial blood gas analysis
(HCO3-) 22–30 mmol/L 22–30 meq/L
Pco2 (Sea Level, Fio2 0.21) 4.7–6.0 kPa 35–45 mmHg
Po2 (Sea Level, Fio2 0.21, age related) 8.9–13.8 kPa 67–104 mmHg
Ph 7.35–7.45 7.35–7.45
Carboxyhemoglobin and methemoglobin at pH 7.40 and 37°C ≤0.01 ≤1%

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Nitsbin (ንጽቢን) Bedside oriented Internal medicine 2nd edition
Reading assignment 1647

Reading assignment50

1. Respiratory system
o Upper respiratory tract infections
o Acute Bronchitis

2. GI system
o Hepatocellular carcinoma
o Diseases of the small intestine (malabsorption syndrome)
o Dysphagia and esophagitis

3. NS
o Brain abscess
o Headache
o Movement Disorders
o NMJ disorders
o Peripheral neuropathies

4. Hematology
o Hemostasis and bleeding disorders

5. Endocrinology and Metabolic disorders


o Disorders of the thyroid gland
o Cushing syndrome
o Hyper aldosteronism
o Pheochromocytoma
o Disorders of pituitary gland
o Acid base disorders

6. Infectious disease
o Staphylococcal and Streptococcal Infections
o Clostridium Difficile Infection
o Shigellosis
o Brucellosis
o Virology → HSV, Influenza viruses, Ebola virus/ኢቦላ/
o Viral AFI → Dengue fever/ደንጉ/, Yellow fever/ቢጫ ወባ/, Chikungunya/ችጉንጉንያ/

50 rd
We will try to address in 3 edition
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Nitsbin (ንጽቢን) Bedside oriented Internal medicine 2nd edition
References (ዋቢ መጽሐፍት) 1648

References (ዋቢ መጽሐፍት)

1) Harrison’s principle of internal medicine 21st edition


2) UpToDate, © 2018, version 2.0
3) ADA (American diabetic association), Standards of medical care in diabetes, 2023
4) IWGDF (The International Working Group on the Diabetic Foot) Guideline on
the classification of diabetic foot ulcers, 2019.
o Free PDF download accessible here → www.iwgdfguidelines.org
5) GOLD (Global initiative for Chronic obstructive Lung disease), COPD diagnosis,
management and prevention, 2021
o Free PDF download accessible here → http://www.goldcopd.org
6) WHO GUIDELINE for the treatment of visceral leishmaniasis in HIV co-infected patients in
East Africa and South-East Asia, 2022
7) Bates’ Guide to Physical Examination and History Taking, 12th edition
8) ECG NOTES, Interpretation and management Guide, Shirley A Jones, 2005
9) Standard treatment guideline for general hospitals in Ethiopia, FMOH, 4th edition, 2021
10) National Comprehensive HIV Prevention, Care and Treatment Training for Health care
Providers, March, 2020, FMOH, Ethiopia
11) National malaria guideline, 4th edition, 2018, MOH, Ethiopia
12) Malaria Case Management Training Manual for Health Professionals in Ethiopia, January
2022, FMOH
13) Guidelines for Clinical and Programmatic Management of TB, TB/HIV, DR-TB and Leprosy
in Ethiopia, 7th edition, 2021, FMOH, Ethiopia
14) National Programmatic management of Drug resistant TB in Ethiopia, FMOH, December
2019
15) Guideline for diagnosis, treatment and prevention of leishmaniasis in Ethiopia, 2nd edition,
2013, MOH, Ethiopia
16) Poisoning and Drug Overdose Management Training for Health Care Professionals, 2020,
MOH, Ethiopia
17) NATIONAL NONCOMMUNICABLE DISEASES MANAGEMENT PROTOCOLS, November
2021, FMOH, Ethiopia
18) CRITICAL CARE POCKET GUIDE 2022, FMOH, Ethiopia
19) National Training on DM for Health Care Workers, Participant’s Manual (Draft Revised
Version) Addis Ababa January 2021
20) NATIONAL TRAINING ON HYPERTENSIONFOR HEALTH CARE WORKERS IN
ETHIOPIA: Participant’s Manual October, 2021, Addis Ababa, Ethiopia
21) NATIONAL TRAINING ON RHEUMATIC HEART DISEASE PREVENTION & CONTROL
FOR HEALTH CARE WORKERS IN ETHIOPIA: Participant’s Manual October 2021 Addis
Ababa
22) NATIONAL COMPREHENSIVE COVID - 19 MANAGEMENT HANDBOOK, 2020, FMOH,
Ethiopia
23) National Guideline for CHOLERA SURVEILLANCE AND OUTBREAK RESPONSE 3rd
edition, 2022 GC.
24) Cardiology handbook, university of Gondar hospital, management guidelines, 2014

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25) Abilo Physical Examination and Clinical History Taking for Health Science Students, Abilo
Tadesse, MD, Assistant professor of Internal medicine, University of Gondar

Nitsbin (ንጽቢን) Bedside oriented Internal medicine 2nd edition


References (ዋቢ መጽሐፍት) 1649

26) Bedside and Round notes from UOG


27) Class Lecture notes from UOG and AAU/TASH
28) Internal medicine long and short case notes, Mulualem. G (ኦሪት), MED IV, December
2010

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Nitsbin (ንጽቢን) Bedside oriented Internal medicine 2nd edition
References (ዋቢ መጽሐፍት) 1

END
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Nitsbin (ንጽቢን) Bedside oriented Internal medicine 2nd edition 1

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