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金黄色葡萄球菌中纤连蛋白结合蛋白A和B(FnBPA和FnBPB)在宿主感染中的多价作用

The Multivalent Role of Fibronectin-Binding Proteins A and B (FnBPA and FnBPB) of in Host Infections.

作者信息

Speziale Pietro, Pietrocola Giampiero

机构信息

Department of Molecular Medicine, Unit of Biochemistry, University of Pavia, Pavia, Italy.

出版信息

Front Microbiol. 2020 Aug 26;11:2054. doi: 10.3389/fmicb.2020.02054. eCollection 2020.

Abstract

, one of the most important human pathogens, is the causative agent of several infectious diseases including sepsis, pneumonia, osteomyelitis, endocarditis and soft tissue infections. This pathogenicity is due to a multitude of virulence factors including several cell wall-anchored proteins (CWA). CWA proteins have modular structures with distinct domains binding different ligands. The majority of strains express two CWA fibronectin (Fn)-binding adhesins FnBPA and FnBPB (Fn-binding proteins A and B), which are encoded by closely related genes. The N-terminus of FnBPA and FnBPB comprises an A domain which binds ligands such as fibrinogen, elastin and plasminogen. The A domain of FnBPB also interacts with histones and this binding results in the neutralization of the antimicrobial activity of these molecules. The C-terminal moiety of these adhesins comprises a long, intrinsically disordered domain composed of 11/10 fibronectin-binding repeats. These repetitive motifs of FnBPs promote invasion of cells that are not usually phagocytic a mechanism by which they interact with integrin αβ through a Fn mediated-bridge. The FnBPA and FnBPB A domains engage in homophilic cell-cell interactions and promote biofilm formation and enhance platelet aggregation. In this review we update the current understanding of the structure and functional properties of FnBPs and emphasize the role they may have in the staphylococcal infections.

摘要

作为最重要的人类病原体之一,是包括败血症、肺炎、骨髓炎、心内膜炎和软组织感染在内的多种传染病的病原体。这种致病性归因于多种毒力因子,包括几种细胞壁锚定蛋白(CWA)。CWA蛋白具有模块化结构,其不同结构域结合不同配体。大多数菌株表达两种CWA纤连蛋白(Fn)结合黏附素FnBPA和FnBPB(Fn结合蛋白A和B),它们由密切相关的基因编码。FnBPA和FnBPB的N末端包含一个A结构域,该结构域结合纤维蛋白原、弹性蛋白和纤溶酶原等配体。FnBPB的A结构域还与组蛋白相互作用,这种结合导致这些分子的抗菌活性被中和。这些黏附素的C末端部分包含一个由11/10个纤连蛋白结合重复序列组成的长的、内在无序的结构域。FnBPs的这些重复基序促进通常不具有吞噬作用的细胞的侵袭,这是它们通过Fn介导的桥与整合素αβ相互作用的一种机制。FnBPA和FnBPB的A结构域参与同种型细胞间相互作用,促进生物膜形成并增强血小板聚集。在这篇综述中,我们更新了对FnBPs结构和功能特性的当前认识,并强调了它们在葡萄球菌感染中可能发挥的作用。

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