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革兰氏阴性病原体的黏附器通过经典的伴侣蛋白/usher 机制组装:从临床角度看结构与功能。

Adhesive organelles of Gram-negative pathogens assembled with the classical chaperone/usher machinery: structure and function from a clinical standpoint.

机构信息

Joint Biotechnology Laboratory, University of Turku, Turku, Finland.

出版信息

FEMS Microbiol Rev. 2010 May;34(3):317-78. doi: 10.1111/j.1574-6976.2009.00201.x. Epub 2009 Dec 2.

Abstract

This review summarizes current knowledge on the structure, function, assembly and biomedical applications of the superfamily of adhesive fimbrial organelles exposed on the surface of Gram-negative pathogens with the classical chaperone/usher machinery. High-resolution three-dimensional (3D) structure studies of the minifibers assembling with the FGL (having a long F1-G1 loop) and FGS (having a short F1-G1 loop) chaperones show that they exploit the same principle of donor-strand complementation for polymerization of subunits. The 3D structure of adhesive subunits bound to host-cell receptors and the final architecture of adhesive fimbrial organelles reveal two functional families of the organelles, respectively, possessing polyadhesive and monoadhesive binding. The FGL and FGS chaperone-assembled polyadhesins are encoded exclusively by the gene clusters of the γ3- and κ-monophyletic groups, respectively, while gene clusters belonging to the γ1-, γ2-, γ4-, and π-fimbrial clades exclusively encode FGS chaperone-assembled monoadhesins. Novel approaches are suggested for a rational design of antimicrobials inhibiting the organelle assembly or inhibiting their binding to host-cell receptors. Vaccines are currently under development based on the recombinant subunits of adhesins.

摘要

这篇综述总结了目前关于经典伴侣/usher 机制暴露在革兰氏阴性病原体表面的粘附纤毛器官超家族的结构、功能、组装和生物医学应用的知识。具有长 F1-G1 环的 FGL 和具有短 F1-G1 环的 FGS 伴侣组装的微小纤维的高分辨率三维 (3D) 结构研究表明,它们利用供体链互补的相同原理进行亚基聚合。与宿主细胞受体结合的粘附亚基的 3D 结构和粘附纤毛器官的最终结构揭示了该器官的两个功能家族,分别具有多粘附和单粘附结合。FGL 和 FGS 伴侣组装的多粘附素仅由γ3 和κ单系群的基因簇编码,而属于γ1、γ2、γ4 和π菌毛枝系的基因簇仅编码 FGS 伴侣组装的单粘附素。提出了新的方法来合理设计抑制器官体组装或抑制其与宿主细胞受体结合的抗菌药物。目前正在基于粘附素的重组亚基开发疫苗。

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