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    Complement Deficiency

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    Zenia
    Complement deficiencies can cause recurrent bacterial infections or autoimmune disorders due to problems with the complement system's normal function. Specific deficiencies include C1 inhibitor deficiency, which causes hereditary angioedema, and C2 and C3 deficiencies, which increase infection risk and can cause SLE-like symptoms. Diagnosis involves testing complement protein levels and treatment focuses on preventing and quickly treating infections.

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    Complement Deficiency

    Uploaded by

    Zenia
    34 views5 pages
    Complement deficiencies can cause recurrent bacterial infections or autoimmune disorders due to problems with the complement system's normal function. Specific deficiencies include C1 inhibitor deficiency, which causes hereditary angioedema, and C2 and C3 deficiencies, which increase infection risk and can cause SLE-like symptoms. Diagnosis involves testing complement protein levels and treatment focuses on preventing and quickly treating infections.

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    Complement deficiencies can cause recurrent bacterial infections or autoimmune disorders due to problems with the complement system's normal function. Specific deficiencies include C1 inhibitor deficiency, which causes hereditary angioedema, and C2 and C3 deficiencies, which increase infection risk and can cause SLE-like symptoms. Diagnosis involves testing complement protein levels and treatment focuses on preventing and quickly treating infections.

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    © All Rights Reserved
    Download as PDF, TXT or read online from Scribd
    Download as pdf or txt
    34 views5 pages

    Complement Deficiency

    Uploaded by

    Zenia
    Complement deficiencies can cause recurrent bacterial infections or autoimmune disorders due to problems with the complement system's normal function. Specific deficiencies include C1 inhibitor deficiency, which causes hereditary angioedema, and C2 and C3 deficiencies, which increase infection risk and can cause SLE-like symptoms. Diagnosis involves testing complement protein levels and treatment focuses on preventing and quickly treating infections.

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    © All Rights Reserved
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    NOTES

    NOTES
    COMPLEMENT DEFICIENCIES

    GENERALLY, WHAT ARE THEY?


    ▪ Complement component serum levels
    PATHOLOGY & CAUSES ▫ Level ↓ correlates with specific protein
    deficiency
    ▪ Genetic diseases: a protein of the 30+ in
    ▫ Overactive pathway consumption
    complement system missing → abnormal
    → protein level ↓ (i.e. decreased C2/
    inflammatory/immune response-prone
    C4 ↓ indicates classical pathway
    individual
    overactivation—as in C1 inhibitor
    deficiency)
    SIGNS & SYMPTOMS
    TREATMENT
    ▪ Recurrent bacterial infection (i.e.
    pneumonia, tonsillitis, otitis), especially
    MEDICATIONS
    encapsulated bacteria
    ▪ Bacterial infection prevention: vaccination
    ▪ Rheumatologic/autoimmune disorders
    ▫ Meningococcal, pneumococcal,
    ▫ Can be systemic lupus erythematosus
    Haemophilus influenzae b (Hib) vaccines
    (SLE)-like (fever, rash, arthritis,
    (conjugated vaccines preferred for Hib
    glomerulonephritis)
    pneumococcal)
    ▪ Bacterial infection-suspicious symptoms →
    DIAGNOSIS swift antibiotic management

    LAB RESULTS
    ▪ Screening based on recurrent infection/
    autoimmune familial/individual history
    ▫ Genetic screening
    ▫ Total hemolytic complement (THC/
    CH50) testing < 11% (measures
    individual serum’s ability to lyse sheep
    red blood cells (RBCs) coated with anti-
    RBC rabbit antibody → activates serum
    complement proteins; AH50 alternative
    pathway evaluation test)

    190 OSMOSIS.ORG
    Chapter 31 Complement Deficiencies

    C1 ESTERASE
    INHIBITOR DEFICIENCY
    osms.it/complement_deficiency

    PATHOLOGY & CAUSES DIAGNOSIS


    ▪ Autosomal dominant disorder: C1 inhibitor LAB RESULTS
    protein missing → clinical hereditary ▪ Low C1 esterase inhibitor, C4 levels
    angioedema (HAE) syndrome
    ▪ C1 esterase inhibitor role: inhibits C1
    OTHER DIAGNOSTICS
    protein cleavage in complement cascade
    ▫ C1 esterase inhibitor deficiency → History
    overactive C1 cleavage → ↑ classical ▪ Recurrent, self-resolving angioedema
    complement pathway activation → episodes with/without colicky, abdominal
    proinflammatory, ↑ immune responsive pain
    state → ↑ downstream anaphylatoxin ▪ No concurrent angiotensin-converting
    production (C2a, C4a) enzyme (ACE) inhibitors/nonsteroidal anti-
    ▪ C1 esterase inhibitor also mediates inflammatory drug (NSAIDs) use
    bradykinin production → hereditary ▪ Positive angioedema family history
    angioedema (HAE)
    ▫ C1 esterase inhibitor absence → ↑ Physical examination
    kallikrein, factor XII → unchecked ▪ Nondependent (i.e. head/neck), non-pitting
    bradykinin production → vasodilation → edema areas without urticaria/pruritis
    severe angioedema

    TREATMENT
    SIGNS & SYMPTOMS
    MEDICATIONS
    Angioedema episodes ▪ Therapies: purified C1 inhibitor concentrate,
    ▪ Commonly last 24–72 hours, without kallikrein inhibitor, bradykinin-B2-receptor
    urticaria/pruritis antagonist
    ▫ Frequent prodromal symptoms: fatigue, ▪ If above targeted therapy interventions
    nausea, gastrointestinal (GI) symptoms, unavailable → fresh frozen plasma
    myalgias present ▪ Avoid angiotensin-converting-enzyme
    ▫ Individuals may report stress (physical/ (ACE) inhibitors
    mental) as episode triggers

    Edematous episodes SURGERY


    ▪ Nondependent areas, non-pitting ▪ Acute episodes → intubation for airway
    ▫ Most common locations: upper management
    respiratory/GI tract skin/mucosal tissue
    ▫ GI bowel edema → nonspecific GI
    distress symptoms (abdominal pain,
    colic)
    ▫ Laryngeal edema most feared → closed
    airway → asphyxiation

    OSMOSIS.ORG 191
    C2 DEFICIENCY
    osms.it/complement_deficiency

    PATHOLOGY & CAUSES DIAGNOSIS


    ▪ Autosomal recessive disorder: involves C2 LAB RESULTS
    protein absence in classical complement ▪ Recurrent SLE-like episodes: CH50 testing
    cascade
    ▫ Most common complement deficiency
    OTHER DIAGNOSTICS
    disorder
    ▪ Clinical/family recurrent, bacterial infection
    ▫ Symptoms commonly present in early
    history
    childhood
    ▪ Associated with IgG deficiency
    TREATMENT
    SIGNS & SYMPTOMS MEDICATIONS
    ▪ Bacterial infection vigilance: prompt
    ▪ Individuals sometimes present with SLE-
    antibiotic therapy
    like symptoms
    ▪ SLE-like episodes: corticosteroids, other
    ▫ Fever, rash, arthritis, glomerulonephritis
    immunosuppressants
    ▪ ↑ infection risk from encapsulated bacteria
    ▫ Streptococcus pneumoniae,
    Haemophilus influenza type b, Neisseria
    meningitidis

    C3 DEFICIENCY
    osms.it/complement_deficiency
    → type III hypersensitivity reaction
    PATHOLOGY & CAUSES ▫ Inability to opsonize underlies frequently
    encountered sinopulmonary diseases
    ▪ Autosomal recessive disorder: involving (see bacterial infections below)
    protein C3 (vital protein connecting three
    ▪ Inability to form C5 convertase → deficient
    complement activation pathways—
    membrane attack complex (MAC) formation
    classical, alternative, lectin—to final,
    common pathway) ▫ Inability to complete complement
    cascade underlies (primarily meningitis-
    ▫ Presents with severe infections shortly
    related) septic presentation
    after birth
    ▪ Abnormal C3 protein levels → abnormal
    ▫ Rarest complement deficiency disorder
    three complement pathway activation
    ▪ Cleavage product: C3b (major opsonin) → abnormal pathway byproduct
    ▫ Inability to effectively opsonize without concentrations (i.e. anaphylatoxins C2a,
    C3b → antigen-antibody complex C4a) → abnormal immune cell response
    unable to be phagocytosed → excess to immune insult → abnormal neutrophil
    immune complex formation, deposition response → abscess formation

    192 OSMOSIS.ORG
    Chapter 31 Complement Deficiencies

    SIGNS & SYMPTOMS TREATMENT


    ▪ Severe, recurrent encapsulated bacterial MEDICATIONS
    infections shortly after birth ▪ Bacterial infection vigilance: prompt
    ▫ Particularly Streptococcus pneumoniae antibiotic therapy
    ▪ Children who survive severe infections ▪ Bacterial infection prophylaxis: vaccination
    develop problems secondary to immune ▫ Pneumococcal vaccination
    complex deposition, reaction ▫ Meningococcal vaccination (for resulting
    ▫ Especially membranoproliferative dysfunctional C5–C9 MAC formation)
    glomerulonephritis

    DIAGNOSIS
    LAB RESULTS
    ▪ Clinical/family history of recurrent, bacterial
    infections (especially Streptococcus
    pneumoniae) → CH50 testing

    C5-C9 DEFICIENCY
    osms.it/complement_deficiency

    PATHOLOGY & CAUSES DIAGNOSIS


    ▪ Autosomal recessive disorder group: LAB RESULTS
    involving any protein (C5–C9) involved ▪ Clinical recurrent, bacterial infection history
    in MAC formation (part of final, common (especially Neisseria species) → CH50
    complement pathway) testing
    ▪ MAC-forming inability: precludes ability to
    create osmotic gradient for cellular lysis
    TREATMENT
    SIGNS & SYMPTOMS MEDICATIONS
    ▪ Bacterial infection vigilance: prompt
    ▪ Frequent, recurrent bacterial infection antibiotic therapy
    ▫ Propensity for Neisseria gonorrhoeae, ▪ Severe bacterial infection mitigation:
    meningitidis infections (thin cell walls meningococcal vaccination
    → especially complement destruction-
    vulnerable)

    OSMOSIS.ORG 193
    PAROXYSMAL NOCTURNAL
    HEMOGLOBINURIA (PNH)
    osms.it/pnh

    ▪ Splenomegaly may present in severe


    PATHOLOGY & CAUSES hemolysis setting
    ▪ Venous, arterial thrombosis
    ▪ Acquired genetic disorder: hematopoietic
    stem cells produce cells that lack cell-
    membrane protein CD55 (AKA decay- DIAGNOSIS
    accelerating factor (DAF)) or CD59 that
    predispose cells to complement-mediated
    LAB RESULTS
    lysis
    ▪ Normochromic, normocytic anemia;
    ▫ Involved gene (on X chromosome)
    pancytopenia; ↑ lactate dehydrogenase
    is phosphatidylinositol glycan
    (LDH) tests
    complementation group A (PIGA)
    ▫ Biologically-male individuals in early 20s Sugar water test
    (most common) ▪ Serum mixed in sucrose (isotonic solution,
    ▪ CD59: anchor protein for low ionic strength) → predisposes to
    glycosylphosphatidylinositol (GPI), a complement-mediated lysis → CD55/59-
    marker of ‘self’ antigenicity on erythrocytes, deficient cells hemolyze
    leukocytes
    ▫ CD59 deficiency → cells sensitive Acid hemolysis test (Ham test)
    to complement-mediated lysis → ▪ Alternative complement cascade triggered
    intravascular hemolysis in acidified serum conditions → CD55/59-
    ▫ Nocturnal: relative hypoventilation deficient cells hemolyze
    during sleep → slightly ↑ serum CD55/59 protein flow cytometry
    CO2 → slightly acidic serum pH → ↑
    ▪ Most sensitive, specific test
    complement activity → ↑ nighttime
    hemolysis
    TREATMENT
    COMPLICATIONS
    ▪ Potentially fatal venous (Budd–Chiari MEDICATIONS
    syndrome), arterial thrombosis ▪ Glucocorticoids (prednisone; typically poor
    ▪ Aplastic anemia, myelodysplasia, response)
    myelofibrosis, acute leukemia evolution ▪ Eculizumab: monoclonal antibody binds
    C5 cleavage → prevents MAC formation,
    complement-mediated cell lysis
    SIGNS & SYMPTOMS
    ▪ Episodic crises triggers include infection,
    SURGERY
    dietary iron supplementation, menstruation ▪ Bone marrow transplantation
    ▪ Nocturnal hemoglobinuria (upon waking)
    ▪ Lumbar, abdominal, general
    musculoskeletal pain

    194 OSMOSIS.ORG

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