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霍乱弧菌II型分泌系统蛋白EpsM周质结构域的晶体结构:铁氧化还原蛋白折叠的最简单形式。

The crystal structure of the periplasmic domain of the type II secretion system protein EpsM from Vibrio cholerae: the simplest version of the ferredoxin fold.

作者信息

Abendroth Jan, Rice Adrian E, McLuskey Karen, Bagdasarian Michael, Hol Wim G J

机构信息

Department of Biochemistry, Biomolecular Structure Center, School of Medicine, University of Washington, Box 357742, Seattle, WA 98195-7242, USA.

出版信息

J Mol Biol. 2004 Apr 30;338(3):585-96. doi: 10.1016/j.jmb.2004.01.064.

DOI:10.1016/j.jmb.2004.01.064
PMID:15081815
Abstract

The terminal branch of the general secretion pathway (Gsp or type II secretion system) is used by several pathogenic bacteria for the secretion of their virulence factors across the outer membrane. In these secretion systems, a complex of 12-15 Gsp proteins spans from the pore in the outer membrane via several associated signal or energy-transducing proteins in the inner membrane to a regulating ATPase in the cytosol. The human pathogen Vibrio cholerae uses such a system, called the Eps system, for the export of the cholera toxin and other virulence factors from its periplasm into the lumen of the gastrointestinal tract of the host. Here, we report the atomic structure of the periplasmic domain of the EpsM protein from V.cholerae, which is a part of the interface between the regulating part and the rest of the Eps system. The crystal structure was determined by Se-Met MAD phasing and the model was refined to 1.7A resolution. The monomer consists of two alphabetabeta-subdomains forming a sandwich of two alpha-helices and a four-stranded antiparallel beta-sheet. In the dimer, a deep cleft with a polar rim and a hydrophobic bottom made by conserved residues is located between the monomers. This cleft contains an extra electron density suggesting that this region might serve as a binding site of an unknown ligand or part of a protein partner. Unexpectedly, the fold of the periplasmic domain of EpsM is an undescribed circular permutation of the ferredoxin fold.

摘要

一般分泌途径(Gsp或II型分泌系统)的末端分支被几种致病细菌用于将其毒力因子分泌穿过外膜。在这些分泌系统中,由12 - 15种Gsp蛋白组成的复合物从外膜中的孔道开始,通过内膜中几种相关的信号或能量转导蛋白,延伸至胞质溶胶中的调节性ATP酶。人类病原体霍乱弧菌利用这样一种称为Eps系统的体系,将霍乱毒素和其他毒力因子从其周质转运到宿主胃肠道腔中。在此,我们报道了霍乱弧菌EpsM蛋白周质结构域的原子结构,它是Eps系统调节部分与其余部分之间界面的一部分。晶体结构通过硒代甲硫氨酸多波长反常散射(Se - Met MAD)相位法确定,模型精修至1.7埃分辨率。单体由两个αβ亚结构域组成,形成一个由两个α螺旋和一个四链反平行β折叠构成的三明治结构。在二聚体中,由保守残基形成的一个带有极性边缘和疏水底部的深裂缝位于单体之间。这个裂缝包含额外的电子密度,表明该区域可能作为未知配体的结合位点或蛋白质伴侣的一部分。出乎意料的是,EpsM周质结构域的折叠方式是铁氧化还原蛋白折叠的一种未描述的环形排列。

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