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抗体与共生微生物中超抗原样蛋白结合的分子特征。

The molecular characterization of antibody binding to a superantigen-like protein from a commensal microbe.

机构信息

Department of Biochemistry and Molecular Biology, University of Chicago, Chicago, IL 60637.

Department of Pathology, University of Chicago, Chicago, IL 60637.

出版信息

Proc Natl Acad Sci U S A. 2021 Sep 28;118(39). doi: 10.1073/pnas.2023898118.

DOI:10.1073/pnas.2023898118
PMID:34548394
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8488583/
Abstract

Microorganisms have coevolved diverse mechanisms to impair host defenses. A major one, superantigens, can result in devastating effects on the immune system. While all known superantigens induce vast immune cell proliferation and come from opportunistic pathogens, recently, proteins with similar broad specificity to antibody variable (V) domain families were identified in a commensal microbiota. These proteins, identified in the human commensal , are called immunoglobulin-binding protein (Ibp) A and B and have been shown to activate B cells in vitro expressing either human VH3 or murine VH5/6/7. Here, we provide molecular and functional studies revealing the basis of this Ibp/immunoglobulin (Ig) interaction. The crystal structure and biochemical assays of a truncated IbpA construct in complex with mouse VH5 antigen-binding fragment (Fab) shows a binding of Ig heavy chain framework residues to the Ibp Domain D and the C-terminal heavy chain binding domain (HCBD). We used targeted mutagenesis of contact residues and affinity measurements and performed studies of the Fab-IbpA complex to determine the stoichiometry between Ibp and VH domains, suggesting Ibp may serve to cluster full-length IgA antibodies in vivo. Furthermore, in vitro stimulation experiments indicate that binding of the Ibp HCBD alone is sufficient to activate responsive murine B cell receptors. The presence of these proteins in a commensal microbe suggest that binding a broad repertoire of immunoglobulins, particularly in the gut/microbiome environment, may provide an important function in the maintenance of host/microbiome homeostasis contrasting with the pathogenic role of structurally homologous superantigens expressed by pathogens.

摘要

微生物进化出了多种机制来损害宿主防御。其中一种主要的机制是超抗原,它会对免疫系统造成毁灭性的影响。虽然所有已知的超抗原都会诱导大量免疫细胞的增殖,而且都来自机会性病原体,但最近在共生菌群中发现了具有类似广泛特异性的抗体可变 (V) 结构域家族的蛋白质。这些在人类共生菌中发现的蛋白质被称为免疫球蛋白结合蛋白 (Ibp) A 和 B,已被证明能够在体外激活表达人 VH3 或鼠 VH5/6/7 的 B 细胞。在这里,我们提供了分子和功能研究,揭示了这种 Ibp/免疫球蛋白 (Ig) 相互作用的基础。与鼠 VH5 抗原结合片段 (Fab) 复合物的截断 IbpA 结构的晶体结构和生化测定显示,Ig 重链框架残基与 Ibp 结构域 D 和 C 末端重链结合结构域 (HCBD) 结合。我们使用接触残基的靶向诱变和亲和力测量,并对 Fab-IbpA 复合物进行了研究,以确定 Ibp 和 VH 结构域之间的化学计量比,表明 Ibp 可能在体内起到聚集全长 IgA 抗体的作用。此外,体外刺激实验表明,单独结合 Ibp HCBD 就足以激活有反应性的鼠 B 细胞受体。这些蛋白质存在于共生微生物中,表明结合广泛的免疫球蛋白 repertoire,特别是在肠道/微生物环境中,可能在维持宿主/微生物组平衡方面发挥重要作用,与病原体表达的结构同源超抗原的致病作用形成对比。

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