The most common
antibody isotype involved in warm antibody AIHA is
IgG, though sometimes
IgA is found. The IgG antibodies attach to a red blood cell, leaving their FC portion exposed with maximal reactivity at 37 °C (versus cold antibody induced hemolytic anemia whose antibodies only bind red blood cells at low body temperatures, typically 28–31 °C). The FC region is recognized and grabbed onto by FC receptors found on monocytes and macrophages in the
spleen. These cells will pick off portions of the red cell membrane, almost as if they are taking a bite. The loss of membrane causes the red blood cells to become
spherocytes. Spherocytes are not as flexible as normal RBCs and will be singled-out for destruction in the
red pulp of the spleen as well as other portions of the reticuloendothelial system. The red blood cells trapped in the spleen cause the spleen to enlarge, leading to the
splenomegaly often seen in these patients. There are two models for this: the
hapten model and the autoantibody model. The hapten model proposes that certain drugs, especially
penicillin and
cephalosporins, will bind to certain proteins on the red cell membrane and act as haptens (small molecules that can elicit an immune response only when attached to a large carrier such as a protein; the carrier may be one that also does not elicit an immune response by itself). Antibodies are created against the protein-drug complex, leading to the destructive sequence described above. The autoantibody model proposes that, through a mechanism not yet understood, certain drugs will cause antibodies to be made against red blood cells which again leads to the same destructive sequence. It is possible for it to occur in an immunocompromised patient. ==Diagnosis==