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IgG 型自身反应性 B 细胞缺失和 Fas(lpr)狼疮小鼠缺陷。

Deletion of IgG-switched autoreactive B cells and defects in Fas(lpr) lupus mice.

机构信息

Department of Immunology and Microbial Science, The Scripps Research Institute, La Jolla, CA 92037, USA.

出版信息

J Immunol. 2010 Jul 15;185(2):1015-27. doi: 10.4049/jimmunol.1000698. Epub 2010 Jun 16.

Abstract

During a T cell-dependent Ab response, B cells undergo Ab class switching and V region hypermutation, with the latter process potentially rendering previously innocuous B cells autoreactive. Class switching and hypermutation are temporally and anatomically linked with both processes dependent on the enzyme, activation-induced deaminase, and occurring principally, but not exclusively, in germinal centers. To understand tolerance regulation at this stage, we generated a new transgenic mouse model expressing a membrane-tethered gamma2a-reactive superantigen (gamma2a-macroself Ag) and assessed the fate of emerging IgG2a-expressing B cells that have, following class switch, acquired self-reactivity of the Ag receptor to the macroself-Ag. In normal mice, self-reactive IgG2a-switched B cells were deleted, leading to the selective absence of IgG2a memory responses. These findings identify a novel negative selection mechanism for deleting mature B cells that acquire reactivity to self-Ag. This process was only partly dependent on the Bcl-2 pathway, but markedly inefficient in MRL-Fas(lpr) lupus mice, suggesting that defective apoptosis of isotype-switched autoreactive B cells is central to Fas mutation-associated systemic autoimmunity.

摘要

在 T 细胞依赖性 Ab 反应期间,B 细胞经历 Ab 类别转换和 V 区超突变,后一过程可能使先前无害的 B 细胞自身反应性。类别转换和超突变在时间和解剖上与两者过程相关,这两个过程都依赖于酶激活诱导脱氨酶,主要但不是排他性地发生在生发中心。为了在这个阶段理解耐受调节,我们生成了一种新的转基因小鼠模型,表达膜结合的 γ2a 反应性超抗原(γ2a-macroself Ag),并评估了具有 Ag 受体自身反应性的新出现的 IgG2a 表达 B 细胞的命运,该受体在类别转换后获得了自身反应性。在正常小鼠中,自身反应性 IgG2a 转换的 B 细胞被删除,导致 IgG2a 记忆应答的选择性缺失。这些发现确定了一种新的成熟 B 细胞负选择机制,该机制可针对自身 Ag 产生反应性。该过程仅部分依赖于 Bcl-2 途径,但在 MRL-Fas(lpr)狼疮小鼠中效率明显降低,这表明同种型转换的自身反应性 B 细胞凋亡缺陷是 Fas 突变相关系统性自身免疫的核心。

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