V EN O

DEEP
OM BO S I S
TH R
DVT

By Dr Mohammad Musa (Shafaqe)

 Definition

Deep vein thrombosis is the

formation of a blood clot in one
of the deep veins of the body,
usually in the leg
 ETIOLOGY

 DVT ususally originates in the lower extremity

venous level ,starting at the calf vein level and
progressing proximally to involve
popliteal ,femoral ,or iliac system. .80 -90 %
pulmonary emboli originates here .
 Virchow tried
 More than 100 years ago, Virchow described a triad of factors

Venous stasis
Endothelial damage
Hypercoagulable state
 1- Venous stasis

 prolonged bed rest (4 days or more)

A cast on the leg
 Limb paralysis from stroke or spinal cord
injury
 extended travel in a vehicle
2- Hypercoagulability

 Surgery and trauma responsible for up to 40%

of all thromboembolic disease
 Malignancy
 Increased estrogen (due to a fall in protein ‘S)
Increased estrogen occurs during
 all stages of pregnancy—
 the first three months postpartum,
 after elective abortion, and
 during treatment with oral contraceptive pills
Inherited disorders of
coagulation


deficiencies of protein
‘S,
 ’ protein ‘C,’ and
 antithrombin III.
Acquired disorders of coagulation
 Nephroticsyndrome results in urinary loss of
antithrombin III, this diagnosis should be
considered in children presenting with
thromboembolic disease
 Antiphospholipidantibodies accelerate
coagulation and include the lupus
anticoagulant and anticardiolipin antibodies.
Inflammatory processes, such as
• systemic lupus erythematosus (SLE),
• sickle cell disease, and
•inflammatory bowel disease (IBD),

also predispose to thrombosis,

presumably due to hypercoagulability
 3-Endothelial Injury
 Trauma,
 surgery,
 invasive procedure may disrupt venous integrity
 Iatrogenic causes of venous thrombosis are increasing due to the
widespread use of central venous catheters, particularly subclavian and
internal jugular lines. These lines are an important cause of upper
extremity DVT, particularly in children.
Clinical Pathophysiology

 The nidus for a clot is often an intimal defect

 When a clot forms on an intimal defect, the
coagulation cascade promotes clot growth
proximally. Thrombus can extend from the
superficial veins into the deep system from which
it can embolize to the lungs.
 Opposing the coagulation cascade is the
endogenous fibrinolytic system. After the clot
organizes or dissolves, most veins will recanalize
in several weeks. Residual clots retract as
fibroblasts and capillary development lead to
intimal thickening.
 Venous hypertension and residual clot may
destroy valves, leading to the postphlebitic
syndrome, which develops within 5-10 years
 Edema, sclerosis, and ulceration
characterize this syndrome, which
develops in 40-80% of patients with
DVT.
 patients also can suffer exacerbations
of swelling and pain, probably as a
result of venous dilatation and
hypertension
 Pulmonary embolism (PE) is a serious
complication of DVT. Many episodes of
pulmonary embolism go unrecognized,
and at least 40% of patients with DVT
have clinically silent PE on VQ scanning
 Clinical Presentation

 Calf pain or tenderness, or both

 Swelling with pitting edema
 Swelling below knee in distal deep vein
thrombosis and up to groin in proximal
deep vein thrombosis
 Increased skin temperature
 Superficial venous dilatation
 Cyanosis can occur with severe obstruction
Contin…

 Palpate distal pulses and evaluate capillary refill

to assess limb perfusion.
 Move and palpate all joints to detect acute
arthritis or other joint pathology.
 Neurologic evaluation may detect nerve root
irritation; sensory, motor, and reflex deficits
should be noted
 Homans'’ sign: pain in the posterior calf or knee
with forced dorsiflexion of the foot
 Search for stigmata of PE such as tachycardia
(common), tachypnea or chest findings (rare), and
 exam for signs suggestive of underlying
predisposing factors.
Wells Clinical Prediction
Guide
 The Wells clinical prediction guide
incorporates risk factors, clinical
signs, and the presence or absence
of alternative diagnoses
 . Wells Clinical Prediction Guide
for DVTClinical ParameterScore
 Active cancer (treatment ongoing, or
within 6 months or palliative)1
 Paralysis or recent plaster
immobilization 1
 Recently bedridden for >3 days or
major surgery <4 weeks1
 Localized tenderness along the
distribution of the deep venous system1
 Entire leg swelling1
 Calf swelling >3 cm compared to the
asymptomatic leg 1
 Pitting edema (greater in the
symptomatic leg)1
 Collateral superficial veins (nonvaricose)1
 Alternative diagnosis (as likely or > that
of DVT)
 Total of Above Score

High probability: Score ³3

Moderate probability: Score = 1 or 2
Low probability: Score £0
 Adapted from Anand SS, et al. JAMA. 1998; 279
[14];1094
Diagnostic Studies

 Clinical examination alone is able to

confirm only 20-30% of cases of DVT
 Blood Tests
 the D-dimer
 INR.
 Current D-dimer assays have
predictive value for DVT, and the
 INR is useful for guiding the
management of patients with known
DVT who are on warfarin (Coumadin)
D-dimer

 D-dimer is a specific degradation product of cross-

linked fibrin. Because concurrent production and
breakdown of clot characterize thrombosis,
patients with thromboembolic disease have
elevated levels of D-dimer
 three major approaches for measuring D-dimer
 ELISA
 latex agglutination
 blood agglutination test (SimpliRED
 False-positive D-dimers occur in patients with
 recent (within 10 days) surgery or trauma,
 recent myocardial infarction or stroke,
 acute infection,
 disseminated intravascular coagulation,
 pregnancy or recent delivery,
 active collagen vascular disease, or metastatic
cancer
Imaging Studies

 Invasive
 venography,
 radiolabeled fibrinogen and.
 noninvasive
 ultrasound,
 plethysmography,
 MRI techniques
venography

 gold standard” modality for the diagnosis of DVT

 Advantages
 Venography is also useful if the patient has a high
clinical probability of thrombosis and a negative
ultrasound,
 it is also valuable in symptomatic patients with a
history of prior thrombosis in whom the
ultrasound is non-diagnostic.
side effects

 phlebitis
 anaphylaxis
Nuclear Medicine Studies

 Because the radioactive isotope incorporates into

a growing thrombus, this test can distinguish new
clot from an old clot
Plethysmography

 Plethysmography measures change in lower

extremity volume in response to certain stimuli.
Ultrasonography

 color-flow Duplex scanning is the imaging test of

choice for patients with suspected DVT
 inexpensive,
 noninvasive,
 widely available
 Ultrasound can also distinguish other causes of
leg swelling, such as tumor, popliteal cyst,
abscess, aneurysm, or hematoma.
clinical limitations

 expensive
 reader dependent
 Duplex scans are less likely to detect non-
occluding thrombi.
 During the second half of pregnancy, ultrasound
becomes less specific, because the gravid uterus
compresses the inferior vena cava, thereby
changing Doppler flow in the lower extremities
Magnetic Resonance
Imaging

 It detects leg, pelvis, and pulmonary thrombi and

is 97% sensitive and 95% specific for DVT.
 It distinguishes a mature from an immature clot.
 MRI is safe in all stages of pregnancy.
DIFFERENTIAL DIAGNOSIS

o Cellulitis
Thrombophlebitis
o Arthritis
Asymmetric peripheral edema
secondary to CHF, liver disease,
renal failure, or nephrotic syndrome
lymphangitis
Extrinsic compression of iliac vein
secondary to tumor, hematoma, or
abscess
Hematoma
Lymphedema
 Muscle or soft tissue injury
Neurogenic pain
Postphlebitic syndrome
Prolonged immobilization or limb paralysis
Ruptured Baker cyst
Stress fractures or other bony lesions
Superficial thrombophlebitis
Varicose veins
Management

 Using the pretest probability score calculated

from the Wells Clinical Prediction rule, patients
are stratified into 3 risk groups—high, moderate,
or low.
 The results from duplex ultrasound are
incorporated as follows:
 If the patient is high or moderate risk and the
duplex ultrasound study is positive, treat for DVT.
 If the duplex study is negative and the patient is low risk, DVT has
been ruled out.

• When discordance exists between the pretest probability and the

duplex study result, further evaluation is required.
 If the patient is high risk but the ultrasound study was negative,
the patient still has a significant probability of DVT
 a venogram to rule out a calf vein DVT
 surveillance with repeat clinical evaluation and
ultrasound in 1 week.
 results of a D-dimer assay to guide management
 If the patient is low risk but the ultrasound study
is positive, some authors recommend a second
confirmatory study such as a venogram before
treating for DVT
EMERGENCY
DEPARTMANT CARE
 The primary objectives of the treatment of DVT
are to
 prevent pulmonary embolism,
 reduce morbidity, and
 prevent or minimize the risk of developing the
postphlebitic syndrome.
 Anticoagulation
 Thrombolytic therapy for DVT
 Surgery for DVT
 Filters for DVT
 Compression stockings
Anticoagulation

 Heparin prevents extension of the thrombus

 Heparin's anticoagulant effect is related directly
to its activation of antithrombin III. Antithrombin
III, the body's primary anticoagulant, inactivates
thrombin and inhibits the activity of activated
factor X in the coagulation process.
 Heparin is a heterogeneous mixture of
polysaccharide fragments with varying
molecular weights but with similar
biological activity. The larger fragments
primarily interact with antithrombin III to
inhibit thrombin.
 The low molecular weight fragments
exert their anticoagulant effect by
inhibiting the activity of activated factor
X. The hemorrhagic complications
attributed to heparin are thought to
arise from the larger higher molecular
weight fragments.
 The optimal regimen for the treatment of DVT is
anticoagulation with heparin or an LMWH followed
by full anticoagulation with oral warfarin for 3-6
months
 Warfarin therapy is overlapped with heparin for 4-
5 days until the INR is therapeutically elevated to
between 2-3.
 After
an initial bolus of 80 U/kg, a constant
maintenance infusion of 18 U/kg is initiated.
The aPTT is checked 6 hours after the bolus
and adjusted accordingly. .
 The aPTT is repeated every 6 hours until 2
successive aPTTs are therapeutic. Thereafter,
the aPTT is monitored every 24 hours as well
as the hematocrit and platelet count.
Advantages of Low-Molecular-Weight
Heparin Over
Standard Unfractionated Heparin
 Superior bioavailability
 Superior or equivalent safety and efficacy
 Subcutaneous once- or twice-daily dosing
 No laboratory monitoring*
 Less phlebotomy (no monitoring/no intravenous
line)
 Less thrombocytopenia
 Earlier/facilitated
 At the present time, 3 LMWH
preparations,
Enoxaparin,
Dalteparin, and
Ardeparin
 warfarin
 Interferes with hepatic synthesis of vitamin K-
dependent coagulation factors
 Dose must be individualized and adjusted to
maintain INR between 2-3
 2-10 mg/d PO
 caution in active tuberculosis or diabetes;
patients with protein C or S deficiency are at
risk of developing skin necrosis
 Thrombolytic therapy for
DVT
 Advantages include
 prompt resolution of symptoms,
 prevention of pulmonary embolism,
 restoration of normal venous circulation,
 preservation of venous valvular function,
 and prevention of postphlebitic syndrome.
 Thrombolytic therapy does not prevent
 clot propagation,
 rethrombosis, or
 subsequent embolization.
 Heparin therapy and oral anticoagulant
therapy always must follow a course of
thrombolysis.
 Thrombolytictherapy is also not effective
once the thrombus is adherent and
begins to organize
 The hemorrhagic complications of
thrombolytic therapy are formidable
(about 3 times higher), including the
small but potentially fatal risk of
intracerebral hemorrhage.
The uncertainty regarding thrombolytic
therapy likely will continue
 Surgery for DVT
 indications
 when anticoagulant therapy is ineffective
 unsafe,
 contraindicated.
 The major surgical procedures for DVT are clot
removal and partial interruption of the inferior
vena cava to prevent pulmonary embolism.
 These pulmonary emboli removed at autopsy
look like casts of the deep veins of the leg
where they originated.

This patient underwent a thrombectomy. The thrombus has
been laid over the approximate location in the leg veins
where it developed.
Filters for DVT

 Indications for insertion of an inferior vena

cava filter
 Pulmonary embolism with contraindication to
anticoagulation
 Recurrent pulmonary embolism despite adequate
anticoagulation
 Controversial indications:
 Deep vein thrombosis with contraindication to
anticoagulation
 Deep vein thrombosis in patients with pre-existing
pulmonary hypertension
 Free floating thrombus in proximal vein
 Failure of existing filter device
 Post pulmonary embolectomy
 Inferior vena cava filters reduce the rate of
pulmonary embolism but have no effect on the
other complications of deep vein thrombosis.
Thrombolysis should be considered in patients
with major proximal vein thrombosis and
threatened venous infarction
Compression stockings
(routinely
recommended
Further Inpatient Care

 Most patients with confirmed proximal vein

DVT may be treated safely on an outpatient
basis. Exclusion criteria for outpatient
management are as follows:
 Suspected or proven concomitant pulmonary
embolism
 Significant cardiovascular or pulmonary
comorbidity
 Morbid obesity
 Renal failure
 Unavailable or unable to arrange close
follow-up care
 Patients are treated with a low molecular weight heparin and instructed to
initiate therapy with warfarin 5 mg PO the next day. Low molecular weight
heparin and warfarin are overlapped for about 5 days until the
international normalized ratio (INR) is therapeutic.
 If inpatient treatment is necessary, low molecular weight heparin is
effective and obviates the need for IV infusions or serial monitoring of the
PTT.
 With the introduction of low molecular weight heparin, selected patients
qualify for outpatient treatment only if adequate home care and close
medical follow-up care can be arranged.
 Platelets
also should be monitored and
heparin discontinued if platelets fall below
75,000.
 Whileon warfarin, the prothrombin time
(PT) must be monitored daily until target
achieved, then weekly for several weeks.
When the patient is stable, monitor
monthly.
 Significant
bleeding (ie, hematemesis,
hematuria, gastrointestinal hemorrhage)
should be investigated thoroughly since
anticoagulant therapy may unmask a
preexisting disease (eg, cancer, peptic
ulcer disease, arteriovenous malformation).
Duration of
anticoagulation in patients
with deep vein thrombosis
 Transient cause and no other risk
factors: 3 months
 Idiopathic: 3-6 months
 Ongoing risk for example, malignancy:
6 -12 months
 Recurrent pulmonary embolism or deep
vein thrombosis: 6-12 months
 Patients with high risk of recurrent
thrombosis exceeding risk of
anticoagulation: indefinite duration
(subject to review)
 Further Outpatient
Care:
 Patients with suspected or diagnosed
isolated calf vein DVT may be discharged
safely on a nonsteroidal anti-inflammatory
drug (NSAID) or aspirin with close follow-up
care and repeat diagnostic studies in 3-7
days to detect proximal extension.
 At certain centers, patients with isolated
calf vein DVT are admitted for full
anticoagulant therapy.
 Patientswith suspected DVT but negative
noninvasive studies need to be reassessed by
their primary care provider within 3-7 days.
 Patients
with ongoing risk factors may need to
be restudied at that time to detect proximal
extension because of the limited accuracy of
noninvasive tests for calf vein DVT.
 Complications

 Acute pulmonary embolism

 Hemorrhagic complications
 Chronic venous insufficiency
 Prognosis:
All patients with proximal vein DVT
are at long-term risk of developing
chronic venous insufficiency.
About 20% of untreated proximal
(above the calf) DVTs progress to
pulmonary emboli, and 10-20% of
these are fatal. With aggressive
anticoagulant therapy, the mortality
is decreased 5- to 10-fold.
DVT confined to the calf virtually
never causes clinically significant
emboli and thus does not require
 Patient Education:
 Advise
women taking estrogen of the risks and
common symptoms of thromboembolic disease.
 Discourage prolonged immobility, particularly
on plane rides and long car trips
 PROPHYLAXIS
 Ideidentify any patiant who is at risk.
 Prevent dehydration.
 During operation avoid prolonged calf
compression.
 Passive leg exercises should be encourged
whilst patient on bed.
 Foot of bed should be elevated to increase
venous return.
 Early mobilization should be rule for all
surgical patients.