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来自大肠杆菌的外膜蛋白酶OmpT的晶体结构揭示了一个新的催化位点。

Crystal structure of the outer membrane protease OmpT from Escherichia coli suggests a novel catalytic site.

作者信息

Vandeputte-Rutten L, Kramer R A, Kroon J, Dekker N, Egmond M R, Gros P

机构信息

Department of Crystal and Structural Chemistry, Bijvoet Center for Biomolecular Research, Utrecht University, Padualaan 8, 3584 CH Utrecht, The Netherlands.

出版信息

EMBO J. 2001 Sep 17;20(18):5033-9. doi: 10.1093/emboj/20.18.5033.

Abstract

OmpT from Escherichia coli belongs to a family of highly homologous outer membrane proteases, known as omptins, which are implicated in the virulence of several pathogenic Gram-negative bacteria. Here we present the crystal structure of OmpT, which shows a 10-stranded antiparallel beta-barrel that protrudes far from the lipid bilayer into the extracellular space. We identified a putative binding site for lipopolysaccharide, a molecule that is essential for OmpT activity. The proteolytic site is located in a groove at the extracellular top of the vase-shaped beta-barrel. Based on the constellation of active site residues, we propose a novel proteolytic mechanism, involving a His-Asp dyad and an Asp-Asp couple that activate a putative nucleophilic water molecule. The active site is fully conserved within the omptin family. Therefore, the structure described here provides a sound basis for the design of drugs against omptin-mediated bacterial pathogenesis. Coordinates are in the Protein Data Bank (accession No. 1I78)

摘要

来自大肠杆菌的OmpT属于一类高度同源的外膜蛋白酶家族,即omptin,它与几种致病性革兰氏阴性菌的毒力有关。在此,我们展示了OmpT的晶体结构,其呈现出一个由10条链组成的反平行β桶,该结构从脂质双层向外显著延伸至细胞外空间。我们确定了一个脂多糖的假定结合位点,脂多糖是OmpT活性所必需的分子。蛋白水解位点位于花瓶状β桶细胞外顶部的一条凹槽中。基于活性位点残基的组合,我们提出了一种新的蛋白水解机制,涉及一个组氨酸 - 天冬氨酸二元组和一个天冬氨酸 - 天冬氨酸对,它们激活一个假定的亲核水分子。活性位点在omptin家族中完全保守。因此,这里描述的结构为设计针对omptin介导的细菌致病机制的药物提供了坚实的基础。坐标存于蛋白质数据库(登录号1I78)

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