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bcl-x在B细胞发育和激活过程中呈现出受调控的表达,并在转基因小鼠中调节淋巴细胞存活。

bcl-x exhibits regulated expression during B cell development and activation and modulates lymphocyte survival in transgenic mice.

作者信息

Grillot D A, Merino R, Pena J C, Fanslow W C, Finkelman F D, Thompson C B, Nunez G

机构信息

Department of Pathology, University of Michigan Medical School, Ann Arbor 48109, USA.

出版信息

J Exp Med. 1996 Feb 1;183(2):381-91. doi: 10.1084/jem.183.2.381.

Abstract

We have assessed during B cell development, the regulation and function of bcl-x, a member of the bcl-2 family of apoptosis regulatory genes. Here we show that Bcl-xL, a product of bcl-x, is expressed in pre-B cells but downregulated at the immature and mature stages of B cell development. Bcl-xL but not Bcl-2 is rapidly induced in peripheral B cells upon surface immunoglobulin M (IgM) cross-linking, CD40 signaling, or LPS stimulation. Transgenic mice that overexpressed Bcl-xL within the B cell lineage exhibited marked accumulation of peripheral B cells in lymphoid organs and enhanced survival of developing and mature B cells. B cell survival was further increased by simultaneous expression of bcl-xL and bcl-2 transgenes. These studies demonstrate that Bcl-2 and Bcl-xL are regulated differentially during B cell development and activation of mature B cells. Induction of Bcl-xL after signaling through surface IgM and CD40 appears to provide mature B cells with an additional protective mechanism against apoptotic signals associated with antigen-induced activation and proliferation.

摘要

我们评估了在B细胞发育过程中,凋亡调节基因bcl-2家族成员bcl-x的调控及功能。在此我们表明,bcl-x的产物Bcl-xL在pre-B细胞中表达,但在B细胞发育的未成熟和成熟阶段表达下调。在表面免疫球蛋白M(IgM)交联、CD40信号传导或LPS刺激后,外周B细胞中可快速诱导出Bcl-xL而非Bcl-2。在B细胞谱系中过表达Bcl-xL的转基因小鼠在淋巴器官中表现出外周B细胞的显著积累,并且发育中和成熟B细胞的存活率提高。同时表达bcl-xL和bcl-2转基因可进一步提高B细胞存活率。这些研究表明,在B细胞发育和成熟B细胞激活过程中,Bcl-2和Bcl-xL受到不同的调控。通过表面IgM和CD40信号传导后诱导Bcl-xL,似乎为成熟B细胞提供了一种额外的保护机制,以抵御与抗原诱导的激活和增殖相关的凋亡信号。

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