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B 细胞受体微簇形成和信号转导的构象诱导寡聚化模型。

A conformation-induced oligomerization model for B cell receptor microclustering and signaling.

机构信息

Laboratory of Immunogenetics, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Rockville, MD 20852, USA.

出版信息

Curr Top Microbiol Immunol. 2010;340:155-69. doi: 10.1007/978-3-642-03858-7_8.

Abstract

The B cell receptor (BCR) generates both antigen-independent and dependent intracellular signals that are essential for B cell development and antibody responses against pathogens. However, the molecular mechanisms underlying the initiation of BCR signaling are not understood completely yet. The advent of new imaging technologies is allowing the earliest events in B cell signaling to be viewed both in vivo in lymphoid tissues and in vitro in living cells, in real-time, down to the single molecule level. Here we review recent progress in the use of these technologies to decipher the earliest events that follow B cell antigen recognition. Based on recent data using these techniques, we propose a model for the initiation of BCR signaling in which the binding of antigen induces a conformational change in the BCR's extracellular domains leading to BCR oligomerization and signaling. We conclude that testing this model will require an in-depth understanding of the unique structural and organizational features of the BCR in the plasma membrane of living B cells in the presence and absence of antigen.

摘要

B 细胞受体 (BCR) 产生抗原非依赖性和依赖性的细胞内信号,这些信号对于 B 细胞的发育和针对病原体的抗体反应至关重要。然而,BCR 信号转导起始的分子机制尚未完全了解。新的成像技术的出现使得我们能够实时地在体内的淋巴组织和体外的活细胞中,在单细胞水平上观察到 B 细胞信号转导的最早事件。在这里,我们综述了这些技术在解析 B 细胞抗原识别后最早事件中的应用的最新进展。基于最近使用这些技术获得的数据,我们提出了一个 BCR 信号转导起始的模型,该模型认为抗原结合诱导 BCR 胞外结构域的构象变化,导致 BCR 寡聚化和信号转导。我们得出结论,要验证该模型,需要深入了解在存在和不存在抗原的情况下,活 B 细胞的质膜中 BCR 的独特结构和组织特征。

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