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Cryoglobulinemia

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Cryoglobulinemia Andrew J Avery A.M. Report 08/19/09 – PowerPoint PPT presentation

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Title: Cryoglobulinemia


1
Cryoglobulinemia
  • Andrew J Avery
  • A.M. Report
  • 08/19/09

2
Introduction
  • Precipitation of blood proteins at temperatures
    lower than 37ºC is referred to as
    cryoprecipitation
  • Cryoglobulins are either immunoglobulins or a
    mixture of immunoglobulins and complement
    components that precipitate from both serum and
    plasma (if just plasma, then called
    cryofibrinogen)

3
Introduction
  • Wintrobe and Buell are credited with the first
    description of the cryoprecipitation phenomenon.
    In 1933, they described a patient with signs and
    symptoms of hyperviscosity associated with
    multiple myeloma

4
Cryoglobulins
5
Prevalence
  • The prevalence of clinically-significant
    cryoglobulinemia has been estimated at
    approximately 1100,000
  • Detectable levels of circulating CGs have been
    seen in a significant proportion of patients with
    chronic infections and/or inflammation
  • HIV-15-20
  • Connective Tissue Dz-15-25
  • HEP C-40-50

6
Brouet Classification
  • Uses the immunological analysis of the CG to
    delineate the clonality of the responsible CG
  • Type I Criterion is presence of isolated
    monoclonal Ig 5-25 of cases most commonly
    ass. w/ LPD
  • Type II A mixture of polyclonal Ig in
    association with a monoclonal Ig 40-60 of
    cases most commly ass. w/ chronic viral inf
  • Type III Mixed cryoglobulins consisting of
    polyclonal Ig 40-50 of cases most commonly
    ass. w/ CTD

7
Etiology and Pathogenesis
  • CGs are often detectable in the serum of healthy
    pts, thus speculated that CGs reflect the ongoing
    physiological clearance of endogenous immune
    complexes by Igs with RF activity
  • Pathogenic CG responses may result from several
    factors next slide

8
Etiology and Pathogenesis
  • Chronic immune stimulation and/or
    lymphoproliferation, resulting in the production
    of higher concentrations of mono-, oligo-, or
    polyclonal CG.
  • Immune complex formation among CG and/or their
    target antigens
  • Defective and/or insufficient clearance of the
    resulting immune complexes, which accumulate and
    mediate disease

9
Clinical Manifestations
Signs Sx Type I Type II Type III
Purpura
Gangrene/Acrocyano / /-
ArthralgiasgtArthritis
Renal
Neurologic
Liver /-
10
Clinical Manifestations
  • Cutaneous Nearly all pts with CG syndromes
    develop erythematous macules to purpuric papules
    of the lower extremities (90-95).
  • More commonly in Type I CG are infarction,
    hemorrhagic crusts and ulcers (10-25) raynaud
    phenomenon, livedo reticularis, acrocyanosis and
    post-inflammatory hyperpigmentation (30-50).

11
Palpable Purpura
12
Clinical Manifestations
  • Musculoskeletal Arthralgias and myalgias are
    common in type Type II and III CGs (gt70). Most
    commonly affect metacarpophalangeals, proximal
    phalangeals, knees, and ankles
  • Neuropathy Affects 70-80 of pts with mixed CG
    (Type II III). Thought to be 2/2 vasculitis
  • Pulmonary Generally affects Types II III
    (40-50). PFTs often reveal evidence of small
    airways disease and impairment of gas exchange
    sx generally range from dyspnea to cough and
    pleurisy

13
Clinical Manifestations
  • Renal Renal disease in mixed CG often results
    from immune complex disease less frequently 2/2
    thrombotic dz (more common in Type I)
  • Membranoproliferative glomerulonephritis seems to
    be more common in mixed CG
  • Isolated proteinuria or hematuria occur much more
    frequently than nephrotic or nephritic syndromes
    or acute renal failure.

14
Clinical Manifestations
  • Other Sjogrens syndrome (4-20) Raynaud
    phenomenon (50) hepatomegaly, abnormal liver
    function tests or abnormal liver biopsy (90)
    lymphadenopathy (20) splenomegaly (30)
    abdominal pain (20). All of the above are more
    common in Types II III
  • CNS, heart, and retinal vessels are rarely
    affected unless in association with
    hyperviscosity due to type I CG

15
Cutaneous Pathological Findings
  • Mixed CG most often reveal leukocytoclastic
    vasculitis (50), less commonly inflammatory or
    noninflammatory purpura (10-20), noninflammatory
    hyaline thrombosis (10), or post-inflammatory
    sequelae (10)
  • Type I CGs more often induce noninflammatory
    thrombotic lesions, sometimes with evidence of
    cutaneous infarction or hemorrhage

16
Skin lesion in mixed cryoglobulinemia (PAS Stain)
17
Renal Pathological Findings
  • Light and immunofluorescence microscopy In Mixed
    CG, most common is membranoproliferative
    glomerulonephritis (60-80), with endocapillary
    proliferation and subendothelial and/or
    intraluminal deposits of CGs, immunoglobulin,
    and/or complement proteins
  • Type I CG generally produce noninflammatory
    glomerulopathies, including thrombotic and
    hypocellular lesions, without evidence of
    vasculitis.

18
Renal involvement in type II cryoglobulinemia
19
Laboratory Findings
  • Measureable Cryoglobulins Types II III (1 to 5
    mg/dL) Type I (5 to 10 mg/dl)
  • Complement Normal in Type I Decreased CH50,
    C1q, C2 and C4 and normal C3 in Types II III
  • Elevated ESR and CRP
  • Autoantibodies Types II III often have
    elevated RF, ANA (many others as well)
  • Evidence of Viral Inf HCV, HBV, HIV, EBV

20
Treatment
  • Mild Dz Mild symptoms, such as fatigue,
    arthralgias and myalgias, in the absence of clear
    evidence for end-organ damage. Initial trx is
    cold avoidance and nsaids. Low dose prednisone
    for inflam sx not responsive to nsaids
  • Mod-Severe Dz pathologically-proven, CG-related,
    end-organ-threatening vasculitis or thrombosis
  • -Type I (malignancy related) chemo and/or
    radiation for bone lesions

21
Treatment
  • Type I (non-malignancy)-Prednisone and
    Cycylophosphamide
  • Types II III-generally involves
    immunosuppression and may also require
    plasmapheresis May be combined with antiviral
    therapy when indicated
  • Severe Dz hyperviscosity syndrome or vasculitis
    in Type I CG, or life or organ threatening
    vasculitis in mixed CG (Types II or III) warrants
    the addition of plasmapheresis to quickly reduce
    the CG burden

22
Prognosis
  • The presence of CG does not seem to confer a
    significant morbidity or mortality risk over and
    above the underlying conditions
  • Survival Mean survival is approximately 70 at
    10 years after the onset of symptoms, 50 at 10
    years after diagnosis, with death typically
    resulting from infection and cardiovascular
    disease
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