[PDF][PDF] Self-reactive B lymphocytes overexpressing Bcl-xL escape negative selection and are tolerized by clonal anergy and receptor editing

W Fang, BC Weintraub, B Dunlap, P Garside, KA Pape… - Immunity, 1998 - cell.com
W Fang, BC Weintraub, B Dunlap, P Garside, KA Pape, MK Jenkins, CC Goodnow
Immunity, 1998cell.com
Self-reactive B cells Tg for both a bcl-x L death inhibitory gene and an Ig receptor
recognizing hen egg lysozyme (HEL-Ig) efficiently escaped developmental arrest and
deletion in mice expressing membrane-bound self-antigen (mHEL). In response to the same
antigen, Tg HEL-Ig B cells not expressing bcl-x L were deleted, while cells expressing bcl-2
were arrested at the immature B stage. Bcl-x L Tg B cells escaping negative selection were
anergic in both in vitro and in vivo assays and showed some evidence for receptor editing …
Abstract
Self-reactive B cells Tg for both a bcl-xL death inhibitory gene and an Ig receptor recognizing hen egg lysozyme (HEL-Ig) efficiently escaped developmental arrest and deletion in mice expressing membrane-bound self-antigen (mHEL). In response to the same antigen, Tg HEL-Ig B cells not expressing bcl-xL were deleted, while cells expressing bcl-2 were arrested at the immature B stage. Bcl-xL Tg B cells escaping negative selection were anergic in both in vitro and in vivo assays and showed some evidence for receptor editing. These studies suggest that Bcl-x may have a distinct role in controlling survival at the immature stage of B cell development and demonstrate that tolerance is preserved when self-reactive B cells escape central deletion.
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