Autoimmune hemolytic anemia is caused by autoantibodies that react with RBCs at temperatures ≥37° C (warm antibody hemolytic anemia) or < 37° C (cold agglutinin disease). Hemolysis is usually extravascular. The direct antiglobulin (Coombs') test establishes the diagnosis and may suggest the cause. Treatment depends on the cause and may include corticosteroids, splenectomy, IV immune globulin, immunosuppressants, avoidance of blood transfusions, and withdrawal of drugs.
Warm antibody hemolytic
anemia is the most common form of autoimmune hemolytic anemia (AIHA); it is
more common among women. Autoantibodies in warm antibody hemolytic anemia
generally react at temperatures ≥ 37° C. They may occur
spontaneously or in association with certain disorders (SLE, lymphoma, chronic
lymphocytic leukemia). Some drugs (eg, α-methyldopa, levodopa—see Table 3: Anemias Caused by Hemolysis: Drugs That
Cause Warm Antibody Hemolytic Anemia
)
stimulate production of autoantibodies against Rh antigens (α-methyldopa-type
of AIHA). Other drugs stimulate production of autoantibodies against the
antibiotic–RBC-membrane complex as part of a transient hapten mechanism; the
hapten may be stable (eg, high-dose penicillin, cephalosporins) or unstable
(eg, quinidine, sulfonamides).
)
stimulate production of autoantibodies against Rh antigens (α-methyldopa-type
of AIHA). Other drugs stimulate production of autoantibodies against the
antibiotic–RBC-membrane complex as part of a transient hapten mechanism; the
hapten may be stable (eg, high-dose penicillin, cephalosporins) or unstable
(eg, quinidine, sulfonamides).
In warm antibody hemolytic anemia, hemolysis occurs primarily in the
spleen. It is often severe and can be fatal. Most of the autoantibodies in warm
antibody hemolytic anemia are IgG. Most are panagglutinins and have limited
specificity.
Symptoms and Signs
Symptoms of warm antibody hemolytic anemia tend to be due to
the anemia. If the disorder is severe, fever, chest pain, syncope, or heart
failure may occur. Mild splenomegaly is typical.
Diagnosis
·
Assays for hemolytic anemia (eg, peripheral smear, reticulocyte count;
sometimes urinary hemosiderin, serum haptoglobin)
·
Direct antiglobulin test
AIHA is suspected in patients with hemolytic anemia, particularly if
symptoms are severe or other suggestive symptoms are present. Routine
laboratory tests generally suggest extravascular hemolysis (eg, hemosiderinuria
is absent; haptoglobin levels are near normal) unless anemia is sudden and
severe or PCH is the cause. Spherocytosis and a high MCHC are typical.
AIHA is diagnosed by detection of autoantibodies with the direct
antiglobulin (direct Coombs') test. Antiglobulin serum is added to washed RBCs
from the patient; agglutination indicates the presence of immunoglobulin or
complement (C) bound to the RBCs. Generally IgG is present in warm antibody
hemolytic anemia, and C3 (C3b and C3d) in cold antibody disease. The test is ≤ 98%
sensitive for AIHA; false-negative results can occur if antibody density is
very low or if the autoantibodies are IgA or IgM. In general, the intensity of
the direct antiglobulin test correlates with the number of molecules of IgG or
C3 bound to the RBC and, roughly, with the rate of hemolysis. A complementary
test consists of mixing the patient's plasma with normal RBCs to determine whether
such antibodies are free in the plasma (the indirect antiglobulin [indirect
Coombs'] test). A positive indirect antiglobulin test and a negative direct
test generally indicate an alloantibody caused by pregnancy, prior
transfusions, or lectin cross-reactivity rather than immune hemolysis. Even
identification of a warm antibody does not define hemolysis, because 1/10,000
healthy blood donors has a positive test result.
Once AIHA has been identified by the Coombs' test, testing should
differentiate between warm antibody hemolytic anemia and cold agglutinin
disease as well as the mechanism responsible for warm antibody hemolytic
anemia. This determination can often be made by observing the pattern of the
direct antiglobulin reaction. Three patterns are possible:
·
The reaction is positive with anti-IgG and negative with anti-C3. This
pattern is common in idiopathic AIHA and in the drug-associated or α-methyldopa-type
of AIHA, usually warm antibody hemolytic anemia.
·
The reaction is positive with anti-IgG and anti-C3. This pattern is common
in patients with SLE and idiopathic AIHA, usually warm antibody hemolytic
anemia, and is rare in drug-associated cases.
·
The reaction is positive with anti-C3 but negative with anti-IgG. This
pattern occurs in cold agglutinin disease. It is uncommon in idiopathic AIHA,
warm antibody hemolytic anemia, when the IgG antibody is of low affinity, in
some drug-associated cases, and in PCH.
Treatment
·
For drug-induced warm antibody hemolytic anemia, drug withdrawal, sometimes
IV immune globulin
·
For idiopathic warm antibody hemolytic anemia, corticosteroids
·
For cold agglutinin disease, avoidance of cold
In drug-induced warm antibody hemolytic anemias, drug withdrawal decreases
the rate of hemolysis. With α-methyldopa-type AIHA, hemolysis usually
ceases within 3 wk; however, a positive Coombs' test may persist for > 1
yr. With hapten-mediated AIHA, hemolysis ceases when the drug is cleared from
the plasma. Corticosteroids have only little effect in drug-induced hemolysis;
infusions of immune globulin may be more effective.Corticosteroids
(eg, prednisone1 mg/kg po once/day or higher doses) are the treatment of
choice in idiopathic warm antibody AIHA. In very severe hemolysis, an initial
loading dose of 100 to 200 mg is recommended. Most patients have an excellent
response, which in about 1/3 is sustained after
12 to 20 wk of therapy. When stable RBC values are achieved, corticosteroids
are tapered slowly. In patients who relapse after corticosteroid cessation or
who are not helped by corticosteroids, splenectomy is done. About 1/3 to 1/2 of
patients have a sustained response after splenectomy. In cases of fulminant
hemolysis, plasma exchange has been used. For less severe but uncontrolled
hemolysis, immune globulin infusions have provided temporary control. Long-term
management with immunosuppressants (including cyclosporine) has been
effective in patients in whom corticosteroids and splenectomy have been
ineffective.
The presence of panagglutinating antibodies in warm antibody hemolytic
anemia makes cross-matching of donor blood difficult. In addition, transfusions
often superimpose an alloantibody on the autoantibody, accelerating hemolysis.
Thus, transfusions should be avoided whenever possible. When necessary, they
should be given only in small aliquots (100 to 200 mL over 1 to 2 h, with
monitoring for hemolysis).
http://www.merckmanuals.com/professional/hematology_and_oncology/anemias_caused_by_hemolysis/autoimmune_hemolytic_anemia.html#v969941
Great and easy-to-understand tutorial, thnx!
SvaraEyðaToshiba PVT-375BT