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人类分泌型免疫球蛋白M核心的结构

Structure of the human secretory immunoglobulin M core.

作者信息

Kumar Nikit, Arthur Christopher P, Ciferri Claudio, Matsumoto Marissa L

机构信息

Department of Structural Biology, Genentech, 1 DNA Way, South San Francisco, CA 94080, USA.

Department of Structural Biology, Genentech, 1 DNA Way, South San Francisco, CA 94080, USA.

出版信息

Structure. 2021 Jun 3;29(6):564-571.e3. doi: 10.1016/j.str.2021.01.002. Epub 2021 Jan 28.

Abstract

Immunoglobulins (Ig) A and M are the only human antibodies that form oligomers and undergo transcytosis to mucosal secretions via the polymeric Ig receptor (pIgR). When complexed with the J-chain (JC) and the secretory component (SC) of pIgR, secretory IgA and IgM (sIgA and sIgM) play critical roles in host-pathogen defense. Recently, we determined the structure of sIgA-Fc which elucidated the mechanism of polymeric IgA assembly and revealed an extensive binding interface between IgA-Fc, JC, and SC. Despite low sequence identity shared with IgA-Fc, IgM-Fc also undergoes JC-mediated assembly and binds pIgR. Here, we report the structure of sIgM-Fc and carryout a systematic comparison to sIgA-Fc. Our structural analysis reveals a remarkably conserved mechanism of JC-templated oligomerization and SC recognition of both IgM and IgA through a highly conserved network of interactions. These studies reveal the structurally conserved features of sIgM and sIgA required for function in mucosal immunity.

摘要

免疫球蛋白(Ig)A和M是仅有的能形成寡聚体并通过聚合免疫球蛋白受体(pIgR)经转胞吞作用进入黏膜分泌物的人类抗体。当与pIgR的连接链(JC)和分泌成分(SC)结合时,分泌型IgA和IgM(sIgA和sIgM)在宿主抵御病原体过程中发挥关键作用。最近,我们确定了sIgA-Fc的结构,阐明了聚合IgA组装的机制,并揭示了IgA-Fc、JC和SC之间广泛的结合界面。尽管IgM-Fc与IgA-Fc的序列同一性较低,但它也会经历JC介导的组装并结合pIgR。在此,我们报告了sIgM-Fc的结构,并与sIgA-Fc进行了系统比较。我们的结构分析揭示了通过高度保守的相互作用网络,JC模板化的IgM和IgA寡聚化以及SC识别的显著保守机制。这些研究揭示了sIgM和sIgA在黏膜免疫中发挥功能所需的结构保守特征。

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