Page 613 - Veterinary Immunology, 10th Edition
P. 613

FIG. 20.4  How the thymus induces central T cell tolerance by
  VetBooks.ir              yet can still respond to foreign antigenic peptides in association with
                           negative selection. Surviving T cells are unreactive to autoantigens

                                     MHC molecules as a result of positive selection.


                  The negative selection process is assisted by the presence of many
               different self-antigens in the thymus. Normally, each tissue
               possesses its own tissue-specific antigens. Thus “skin antigens” are

               usually restricted to the skin, whereas “liver antigens” are restricted
               to the liver, and so forth. However, the epithelial cells in the thymic
               medulla show uniquely “promiscuous” gene expression. Thymic

               epithelial cells use a transcription factor called the autoimmune
               regulator (AIRE) that promotes the expression of thousands of non-
               thymic protein antigens in the thymic medullary epithelium.
               Examples include insulin, thyroglobulin, and myelin basic protein.
               In this way, the thymic epithelial cells ensure that self-reactive T

               cells encounter most normal tissue antigens and are eliminated if
               they respond too strongly. In addition, some normal tissue antigens
               may be taken up by macrophages and carried to the thymus. Self-

               reactive T cells that respond to these antigens are also eliminated.
               However, this raises another question: What about self-antigens
               that are not expressed in, or do not enter, the thymus? Antigens
               from the eye, testis, or brain are not processed in this way, and as a
               result central tolerance to these antigens does not develop.

                  These selection processes together ensure that cells that can bind
               self-antigens are positively selected and those that bind these
               antigens with very low or very high affinity are subsequently

               deleted. As a result, the moderate-affinity clones survive and are
               available to recognize foreign antigens. An additional factor that
               probably determines thymocyte survival is the dose of antigen
               presented to the cells. If the amount of a specific antigen is high (as
               one might anticipate for a self-antigen), multiple TCRs will be

               occupied on each thymocyte and trigger apoptosis. In contrast, if
               the amount is low, this will occupy only a few TCRs, and the weak
               signal may result in positive selection and thymocyte proliferation.



               Receptor Editing

               When the antigen receptors of a developing T cell bind to self-
               antigens, another strategy that prevents autoimmunity is receptor





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