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Bcl-2在记忆B细胞发育过程中阻碍自身反应性、高度突变的抗体V区的阴性选择。

Bcl-2 obstructs negative selection of autoreactive, hypermutated antibody V regions during memory B cell development.

作者信息

Hande S, Notidis E, Manser T

机构信息

Department of Microbiology and Immunology and The Kimmel Cancer Institute, Thomas Jefferson Medical College, Philadelphia, Pennsylvania 19107, USA.

出版信息

Immunity. 1998 Feb;8(2):189-98. doi: 10.1016/s1074-7613(00)80471-9.

Abstract

We analyzed the participation of a predominant B cell clonotype in the anti-arsonate immune response of mice in which Bcl-2 expression was enforced in B cells. Many of the antibodies expressed by the arsonate-induced memory compartment of these mice were "dual-reactive," displaying increased affinity acquired via V region somatic hypermutation for both arsonate and the autoantigen DNA. The hypermutated antibodies expressed by the anti-arsonate memory B cell compartment of normal mice have increased affinity for arsonate but lack measurable affinity for DNA. Thus, interference with apoptotic pathways allows developing memory B cells that have acquired autoreactivity to bypass a peripheral tolerance checkpoint. These data demonstrate that both positive and negative selection, working in concert with V gene somatic hypermutation, result in the "specificity maturation" of the antibody response.

摘要

我们分析了一种占主导地位的B细胞克隆型在Bcl-2在B细胞中过表达的小鼠抗砷酸盐免疫反应中的参与情况。这些小鼠的砷酸盐诱导记忆区表达的许多抗体是“双反应性”的,通过V区体细胞超突变对砷酸盐和自身抗原DNA都表现出亲和力增加。正常小鼠抗砷酸盐记忆B细胞区表达的超突变抗体对砷酸盐的亲和力增加,但对DNA缺乏可测量的亲和力。因此,对凋亡途径的干扰使得已获得自身反应性的记忆B细胞能够绕过外周耐受检查点。这些数据表明,正向和负向选择与V基因体细胞超突变协同作用,导致抗体反应的“特异性成熟”。

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