In vivo ablation of surface immunoglobulin on mature B cells by inducible gene targeting results in rapid cell death
- PMID: 9323135
- DOI: 10.1016/s0092-8674(00)80373-6
In vivo ablation of surface immunoglobulin on mature B cells by inducible gene targeting results in rapid cell death
Abstract
Gene targeting experiments have demonstrated that the expression of immunoglobulin heavy chain in the pre-B cell receptor (pBCR) and of heavy and light chains in the B cell antigen receptor (BCR) marks checkpoints in early B cell development that the cells have to pass to survive. To investigate whether the persistence of mature B cells in the peripheral immune system also depends on BCR expression, we have generated a transgenic mouse in which the BCR can be inducibly ablated through V region gene deletion. Ablation leads to rapid death of mature B lymphocytes, which is preceded by down-regulation of MHC antigens and up-regulation of CD95 (Fas) and can be delayed by constitutive bcl-2 expression.
Comment in
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Antigen receptor signaling gives lymphocytes a long life.Cell. 1997 Sep 19;90(6):971-3. doi: 10.1016/s0092-8674(00)80362-1. Cell. 1997. PMID: 9323124 Review. No abstract available.
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