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首页> 外文期刊>Nature immunology >Recruitment of the cytoplasmic adaptor Grb2 to surface IgG and IgE provides antigen receptor-intrinsic costimulation to class-switched B cells.
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Recruitment of the cytoplasmic adaptor Grb2 to surface IgG and IgE provides antigen receptor-intrinsic costimulation to class-switched B cells.

机译:将细胞质衔接子Grb2募集至表面IgG和IgE,可为类转换B细胞提供抗原受体内在共刺激。

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摘要

The improved antibody responses of class-switched memory B cells depend on enhanced signaling from their B cell antigen receptors (BCRs). However, BCRs on both naive and antigen-experienced B cells use the canonical immunoglobulin-associated alpha and beta-protein signaling subunits. Here we identified a BCR isotype-specific signal-amplification mechanism. Whereas immunoglobulin M (IgM)-containing BCRs initiated intracellular signals exclusively through immunoglobulin-associated alpha- and beta-proteins, IgG- and IgE-containing BCRs also used a conserved tyrosine residue in the cytoplasmic segments of immunoglobulin heavy chains. When phosphorylated, this tyrosine recruited the adaptor Grb2, resulting in sustained protein kinase activation and prolonged generation of second messengers, which together culminated in enhanced B cell proliferation. Hence, membrane-bound IgG and IgE exert antigen recognition as well as costimulatory functions, thereby rendering memory B cells less dependent on T cell help.
机译:类切换记忆B细胞的改善的抗体应答依赖于来自其B细胞抗原受体(BCR)的增强的信号传导。然而,幼稚和抗原经历过的B细胞上的BCR都使用规范的免疫球蛋白相关的α和β蛋白信号亚基。在这里,我们确定了BCR同种型特异性信号放大机制。含免疫球蛋白M(IgM)的BCR仅通过免疫球蛋白相关的α和β蛋白引发细胞内信号,而含IgG和IgE的BCR在免疫球蛋白重链的细胞质区段中也使用了保守的酪氨酸残基。当被磷酸化时,该酪氨酸募集衔接子Grb2,导致持续的蛋白激酶活化和第二信使的延长生成,这最终导致增强的B细胞增殖。因此,膜结合的IgG和IgE发挥抗原识别以及共刺激功能,从而使记忆B细胞较少依赖T细胞帮助。

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