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结核分枝杆菌 VKOR 的膜拓扑结构和突变分析,VKOR 是一种参与二硫键形成的蛋白质,与人类维生素 K 环氧化物还原酶同源。

Membrane topology and mutational analysis of Mycobacterium tuberculosis VKOR, a protein involved in disulfide bond formation and a homologue of human vitamin K epoxide reductase.

机构信息

College of Life Science, State Key Laboratory of Crop Biology, Shandong Agricultural University, Tai'an, P.R. China.

出版信息

Antioxid Redox Signal. 2011 Apr 15;14(8):1413-20. doi: 10.1089/ars.2010.3558. Epub 2011 Feb 18.

Abstract

We have presented evidence that a homologue of vertebrate membrane protein vitamin K epoxide reductase (VKOR) is an important component of the protein disulfide bond-forming pathway in many bacteria. Bacterial VKOR appears to take the place of the nonhomologous DsbB found in Escherichia coli. We also determined the structure of a VKOR from a Cyanobacterium and showed that two or four conserved cysteines are required, according to different reductants for activity in an in vitro assay. Here we present evidence for the topologic arrangement in the cytoplasmic membrane of the VKOR from Mycobacterium tuberculosis (Mtb). The results show that Mtb VKOR is a membrane protein that spans the membrane 5 times with its N-terminus in the cytoplasm, C-terminus in the periplasm, and all four cysteines facing the periplasm. The essentiality of the four conserved cysteine residues has also been demonstrated in promoting disulfide bond formation in vivo and a mixed disulfide between a cysteine of DsbA of E. coli, and one of the cysteines (Cys(57)) of the VKOR homologue has been identified to be a likely intermediate in the disulfide bond-forming pathway. These studies may inform future resolution of issues surrounding the functioning of human VKOR.

摘要

我们已经提供了证据表明脊椎动物膜蛋白维生素 K 环氧化物还原酶(VKOR)的同源物是许多细菌中蛋白质二硫键形成途径的重要组成部分。细菌 VKOR 似乎取代了大肠杆菌中非同源的 DsbB。我们还测定了一种蓝细菌的 VKOR 结构,并在体外试验中根据不同的还原剂显示出两个或四个保守半胱氨酸对于活性是必需的。在这里,我们提出了结核分枝杆菌(Mtb)VKOR 在内质网膜中的拓扑排列的证据。结果表明,Mtb VKOR 是一种跨膜 5 次的膜蛋白,其 N 端在细胞质中,C 端在周质中,所有四个半胱氨酸都面向周质。在体内促进二硫键形成和大肠杆菌 DsbA 中的一个半胱氨酸(Cys(57))与 VKOR 同源物的一个半胱氨酸之间形成混合二硫键也证明了四个保守半胱氨酸残基的必要性,这可能是二硫键形成途径中的一个中间产物。这些研究可能为解决围绕人类 VKOR 功能的问题提供信息。

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