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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >The Bacterial Enzyme IdeS Cleaves the IgG-Type of B Cell Receptor (BCR), Abolishes BCR-Mediated Cell Signaling, and Inhibits Memory B Cell Activation
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The Bacterial Enzyme IdeS Cleaves the IgG-Type of B Cell Receptor (BCR), Abolishes BCR-Mediated Cell Signaling, and Inhibits Memory B Cell Activation

机译:细菌酶IdeS消除IgG类型的B细胞受体(BCR),废除BCR介导的细胞信号传导,并抑制记忆B细胞活化

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摘要

Ag binding to the BCR is a critical step in B cell development and activation, initiating a cascade of signaling events ultimately leading to proliferation, differentiation, or cell death. A bacterial enzyme, IgG-degrading enzyme of Streptococcus pyogenes (IdeS), was shown to specifically cleave IgG molecules below the hinge region of soluble IgG and when IgG is bound to Ag, resulting in one F(ab')2 molecule and one homodimeric Fc fragment. Whether IdeS could also cleave the IgG molecule when it is present in the BCR attached to the B cell membrane in a complex with CD79a and CD79b is unknown. In this article, we present human in vitro and ex vivo data showing that IdeS cleaves the IgG present in the BCR complex and very efficiently blocks Ag binding to the BCR. As a consequence of IdeS cleaving the BCR, signaling cascades downstream of the BCR are blocked, and memory B cells are temporarily silenced, preventing them from responding to antigenic stimulation and their transition into Ab-producing cells.
机译:Ag与BCR的结合是B细胞发育和激活中的关键步骤,它启动了一系列信号传导事件,最终导致增殖,分化或细胞死亡。已显示一种细菌酶,即化脓性链球菌的IgG降解酶,可特异性裂解可溶性IgG铰链区下方的IgG分子,并且当IgG与Ag结合时,会产生一个F(ab')2分子和一个同型二聚体Fc片段。当IdeS存在于与CD79a和CD79b形成复合体的BCR附着在B细胞膜上的BCR中时,它是否还能裂解IgG分子尚不清楚。在本文中,我们提供了人类体外和离体数据,这些数据表明IdeS可以裂解BCR复合物中存在的IgG,并且非常有效地阻断Ag与BCR的结合。 IdeS裂解BCR的结果是,BCR下游的信号级联被阻断,记忆B细胞被暂时沉默,阻止它们对抗原刺激作出反应并转变为产生Ab的细胞。

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