Page 1192 - Veterinary Immunology, 10th Edition
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VetBooks.ir  Abnormal Immune Responses





               Failure of Regulatory Control


               Although autoimmunity may be triggered by hidden autoantigens,
               a sustained autoimmune response is necessary for disease to
               develop. This may result from a failure of the normal control

               mechanisms of the immune system and can be demonstrated
               simply by injecting mice with rat red blood cells. Following such an
               injection, mice not only make antibodies to the rat cells but also
               develop a self-limited and transient autoimmune response to their
               own red blood cells. This autoimmune response is rapidly

               controlled by regulatory cells and lasts for only a few days. If,
               however, regulatory cell activity in these mice is impaired, as
               occurs in New Zealand Black (NZB) mice, for example, these

               autoantibodies will persist to cause red blood cell destruction and
               anemia.
                  It is common to find autoimmune diseases associated with
               lymphoid tumors. For example, myasthenia gravis, an autoimmune
               disease involving the neuromuscular junction, is commonly

               associated with the presence of a thymic carcinoma. In humans,
               there is a four-fold increase in the incidence of rheumatoid arthritis
               in patients with malignant lymphoid tumors, and there is evidence

               for a similar association in other mammals. Since many lymphoid
               tumors result from a failure in immunological control mechanisms,
               a simultaneous failure in self-tolerance may also occur.
               Alternatively, some lymphoid tumors may consist of cells
               producing autoantibodies. It is also possible that some lymphoid

               tumors may develop as a result of prolonged stimulation of the
               immune system by autoantigens.
                  Potentially harmful, self-reactive lymphocytes are normally

               destroyed in the thymus by apoptosis triggered through CD95
               (Chapter 18). Defects in CD95 or its ligand CD95L (CD178) cause
               autoimmunity by permitting abnormal T cells to survive. This is
               well demonstrated in the lpr strain of mice. These animals have a
               mutation that alters the structure of the intracellular domain of

               CD95 and blocks its functions. A mutation (called gld) in CD95L has





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