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      Anti-DNA antibodies from autoimmune mice arise by clonal expansion and somatic mutation

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      The Journal of Experimental Medicine
      The Rockefeller University Press

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          Abstract

          The proximate cause of autoantibodies characteristic of systemic autoimmune diseases has been controversial. One hypothesis is that autoantibodies are the result of polyclonal nonspecific B cell activation. Alternatively, autoantibodies could be the result of antigen-driven B cell activation, as observed in secondary immune responses. We have approached this question by studying monoclonal anti- DNA autoantibodies derived from unmanipulated spleen cells of the autoimmune MRL/lpr mouse strain. This analysis shows that anti-DNAs, like rheumatoid factors (19), are the result of specific antigen-driven stimulation. In addition, correlation of sequences with fine specificity shows that: (a) somatic mutations can cause specificity for dsDNA and that such mutations are selected for; (b) arginine residues play an important role in determining specificity; and (c) anti- idiotypes that recognize the majority of anti-DNA are probably not specific for any one family of V regions.

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          Author and article information

          Journal
          J Exp Med
          The Journal of Experimental Medicine
          The Rockefeller University Press
          0022-1007
          1540-9538
          1 January 1990
          : 171
          : 1
          : 265-292
          Article
          90111618
          10.1084/jem.171.1.265
          2187662
          2104919
          fd408fd5-1f4e-4fa8-a82c-7f248fb108ad
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          Medicine
          Medicine

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