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CD40与抗原受体的同时激活可保护幼稚和记忆性人类B细胞免受APO-1/Fas介导的凋亡。

Concurrent engagement of CD40 and the antigen receptor protects naive and memory human B cells from APO-1/Fas-mediated apoptosis.

作者信息

Lagresle C, Mondière P, Bella C, Krammer P H, Defrance T

机构信息

Institut National de la Santé et de la Recherche Médicale (INSERM) Unit 404, "Immunité et Vaccination," Institut Pasteur de Lyon, France.

出版信息

J Exp Med. 1996 Apr 1;183(4):1377-88. doi: 10.1084/jem.183.4.1377.

DOI:10.1084/jem.183.4.1377
PMID:8666896
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2192491/
Abstract

Naive and memory B cells were isolated from human tonsils and examined for expression of APO-1/Fas and for their sensitivity to the APO-1-dependent apoptosis. APO-1 was found to be constitutively expressed on memory but not on naive B cells. The susceptibility of both cell types to the APO-1 apoptotic pathway was acquired upon CD40 triggering and was correlated with increased expression of the APO-1 receptor. Both naive and memory B cells were protected from the APO-1-mediated death signal after dual ligation of the Ag receptor adn CD40. Our findings suggest that the APO-1 pathway controls the specificity of B cell responses to T-dependent Ags and that occupancy of the Ag receptor dictates the outcome of APO-1-ligation on B cell survival.

摘要

从人扁桃体中分离出初始B细胞和记忆B细胞,检测其APO-1/Fas的表达情况以及对APO-1依赖性凋亡的敏感性。发现APO-1在记忆B细胞上组成性表达,而在初始B细胞上不表达。两种细胞类型对APO-1凋亡途径的易感性在CD40触发后获得,且与APO-1受体表达增加相关。在抗原受体和CD40双重连接后,初始B细胞和记忆B细胞均受到保护,免受APO-1介导的死亡信号影响。我们的研究结果表明,APO-1途径控制B细胞对T依赖性抗原反应的特异性,并且抗原受体的占据决定了APO-1连接对B细胞存活的影响。

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