Title of article
Class switch recombination in B lymphopoiesis: a potential pathway for B cell autoimmunity
Author/Authors
Eran Diamant، نويسنده , , Doron Melamed، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2004
Pages
6
From page
464
To page
469
Abstract
Pathogenic autoantibodies detected in autoimmune diseases are predominantly IgG isotypes, reflecting the generation and activation of an autoimmune memory B cell repertoire. It is not completely understood how such autoreactive cells are generated and escape central and/or peripheral tolerance mechanisms, and several models to explain this have been proposed. It is generally thought that B lymphocytes utilize IgM receptors for development and tolerance establishment, whereas IgG receptors are primarily used to promote memory formation and signal for memory-type responses. In here we review recent findings suggesting that spontaneously occurring class switch recombination in B lymphopoiesis confer B lymphocytes with a novel developmental pathway that is driven by non-IgM receptors. The physiological relevance of this developmental pathway in generating an autoimmune memory repertoire, as well as a Fas-dependent mechanism regulating it, is discussed.
Keywords
memory , autoantibodies , Peripheral tolerance , Class switch recombination , B cell development
Journal title
Autoimmunity Reviews
Serial Year
2004
Journal title
Autoimmunity Reviews
Record number
474480
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