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播散淋病奈瑟菌 PorB 孔蛋白的结构与功能。

Structure and function of the PorB porin from disseminating Neisseria gonorrhoeae.

机构信息

Max Planck Institute for Developmental Biology, Spemannstr. 35, 72076 Tübingen, Germany.

出版信息

Biochem J. 2013 Feb 1;449(3):631-42. doi: 10.1042/BJ20121025.

DOI:10.1042/BJ20121025
PMID:23095086
Abstract

The outer membrane of Gram-negative bacteria contains a large number of channel-forming proteins, porins, for the uptake of small nutrient molecules. Neisseria gonorrhoeae PorBIA (PorB of serotype A) are associated with disseminating diseases and mediate a rapid bacterial invasion into host cells in a phosphate-sensitive manner. To gain insights into this structure-function relationship we analysed PorBIA by X-ray crystallography in the presence of phosphate and ATP. The structure of PorBIA in the complex solved at a resolution of 3.3 Å (1 Å=0.1 nm) displays a surplus of positive charges inside the channel. ATP ligand-binding in the channel is co-ordinated by the positively charged residues of the channel interior. These residues ligate the aromatic, sugar and pyrophosphate moieties of the ligand. Two phosphate ions were observed in the structure, one of which clamped by two arginine residues (Arg92 and Arg124) localized at the extraplasmic channel exit. A short β-bulge in β2-strand together with the long L3 loop narrow the barrel diameter significantly and further support substrate specificity through hydrogen bond interactions. Interestingly the structure also comprised a small peptide as a remnant of a periplasmic protein which physically links porin molecules to the peptidoglycan network. To test the importance of Arg92 on bacterial invasion the residue was mutated. In vivo assays of bacteria carrying a R92S mutation confirmed the importance of this residue for host-cell invasion. Furthermore systematic sequence and structure comparisons of PorBIA from Neisseriaceae indicated Arg92 to be unique in disseminating N. gonorrhoeae thereby possibly distinguishing invasion-promoting porins from other neisserial porins.

摘要

革兰氏阴性菌的外膜含有大量的通道形成蛋白,孔蛋白,用于吸收小分子营养物质。淋病奈瑟菌 PorBIA(A 型 PorB)与传播疾病有关,并以磷酸盐敏感的方式介导细菌快速侵入宿主细胞。为了深入了解这种结构-功能关系,我们通过 X 射线晶体学在磷酸盐和 ATP 的存在下分析了 PorBIA。在磷酸盐和 ATP 存在下解决的复合物的 PorBIA 结构在 3.3 Å 的分辨率下显示通道内存在大量正电荷。通道内的正电荷残基协调 ATP 配体结合。这些残基连接配体的芳香族、糖和焦磷酸部分。在结构中观察到两个磷酸盐离子,其中一个被两个位于外质通道出口处的精氨酸残基(Arg92 和 Arg124)夹住。β2 链上的短β-凸起与长 L3 环一起显着缩小桶直径,并通过氢键相互作用进一步支持底物特异性。有趣的是,该结构还包含一小段肽作为周质蛋白的残留物,该残留物将孔蛋白分子物理连接到肽聚糖网络上。为了测试 Arg92 对细菌入侵的重要性,该残基发生了突变。携带 R92S 突变的细菌的体内测定证实了该残基对宿主细胞入侵的重要性。此外,淋病奈瑟菌属的 PorBIA 的系统序列和结构比较表明 Arg92 在传播淋病奈瑟菌中是独特的,从而可能将促进入侵的孔蛋白与其他奈瑟氏菌孔蛋白区分开来。

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