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肺炎克雷伯菌 MrkD1P 受体结合域的晶体结构及人源Ⅴ型胶原结合界面的鉴定

Crystal structure of the MrkD1P receptor binding domain of Klebsiella pneumoniae and identification of the human collagen V binding interface.

机构信息

Institute of Structural and Molecular Biology, University College London and Birkbeck College, Malet Street, London, WC1E 7HX, UK.

出版信息

Mol Microbiol. 2012 Nov;86(4):882-93. doi: 10.1111/mmi.12023. Epub 2012 Sep 18.

DOI:10.1111/mmi.12023
PMID:22988966
Abstract

Klebsiella species are members of the family enterobacteriaceae, opportunistic pathogens that are among the eight most prevalent infectious agents in hospitals. Among other virulence factors in Klebsiella, type 3 pili exhibit a unique binding pattern in the human kidney via interaction of two MrkD adhesion variants 1C1 and 1P to type IV and/or V collagen. However, very little is known about the nature of this recognition. Here we present the crystal structure of the plasmid born MrkD1P receptor domain (MrkDrd). The structure reveals a jelly-roll β-barrel fold comprising 17 β-strands very similar to the receptor domain of GafD, the tip adhesin from the F17 pilus that recognizes n-acetyl-d-glucosamine (GlcNAc). Analysis of collagen V binding of different MrkD1P mutants revealed that two regions were responsible for its binding: a pocket, that aligns approximately with the GlcNAc binding pocket of GafD involving residues R105 and Y155, and a transversally oriented patch that spans strands β2a, β9b and β6 including residues V49, T52, V91, R102 and I136. Taken together, these data provide structural and functional insights on MrkD1P recognition of host cells, providing a tool for future development of rationally designed drugs with the prospect of blocking Klebsiella adhesion to collagen V.

摘要

肺炎克雷伯菌属是肠杆菌科的成员,是医院中最常见的 8 种感染病原体之一。在肺炎克雷伯菌的其他毒力因子中,III 型菌毛通过 MrkD 黏附变体 1C1 和 1P 与 IV 型和/或 V 型胶原的相互作用,在人肾脏中表现出独特的结合模式。然而,关于这种识别的性质,我们知之甚少。在这里,我们展示了质粒衍生的 MrkD1P 受体结构域(MrkDrd)的晶体结构。该结构揭示了一种果冻卷 β-桶折叠,由 17 个β-链组成,与 GafD 的受体结构域非常相似,GafD 是 F17 菌毛的尖端黏附素,可识别 N-乙酰-D-葡萄糖胺(GlcNAc)。对不同 MrkD1P 突变体的胶原 V 结合分析表明,有两个区域负责其结合:一个口袋,大约与 GafD 的 GlcNAc 结合口袋对齐,涉及残基 R105 和 Y155,以及一个横向取向的斑块,跨越β2a、β9b 和β6 链,包括残基 V49、T52、V91、R102 和 I136。总的来说,这些数据提供了 MrkD1P 识别宿主细胞的结构和功能见解,为未来开发具有阻断肺炎克雷伯菌与胶原 V 黏附的合理设计药物提供了工具。

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