High resolution CryoEM structure of the ring-shaped virulence factor EspB from Mycobacterium tuberculosis

IF 3.5 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY
Jérémie Piton , Florence Pojer , Soichi Wakatsuki , Cornelius Gati , Stewart T. Cole
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引用次数: 17

Abstract

The EspB protein of Mycobacterium tuberculosis is a 60 kDa virulence factor, implicated in conjugation and exported by the ESX-1 system of which it may also be a component. Previous attempts to obtain high-resolution maps of EspB by cryo-electron microscopic examination of single particles have been thwarted by severe orientation bias of the particles. This was overcome by using detergent as a surfactant thereby allowing reconstruction of the EspB structure at 3.37 Å resolution. The final structure revealed the N-terminal domain of EspB to be organized as a cylindrical heptamer with dimensions of 90 Å x 90 Å and a central channel of 45 Å diameter whereas the C-terminal domain was unstructured. New atomic insight was obtained into the helical packing required for protomer interactions and the overall electrostatic potential. The external surface is electronegatively charged while the channel is lined with electropositive patches. EspB thus has many features of a pore-like transport protein that might allow the passage of an ESX-1 substrate such as the 35 Å diameter EsxA-EsxB heterodimer or B-form DNA consistent with its proposed role in DNA uptake.

Abstract Image

结核分枝杆菌环状毒力因子EspB的高分辨率CryoEM结构
结核分枝杆菌的EspB蛋白是一种60kDa的毒力因子,与结合有关,并由ESX-1系统输出,它也可能是ESX-1系统的一个组成部分。先前试图通过对单个粒子进行冷冻电子显微镜检查来获得EspB的高分辨率图谱,但由于粒子的严重取向偏差而受阻。这是通过使用洗涤剂作为表面活性剂来克服的,从而允许以3.37Å的分辨率重建EspB结构。最终结构显示,EspB的N端结构域被组织为尺寸为90Åx 90Å的圆柱形七聚体,中心通道直径为45Å,而C端结构域是非结构化的。对原聚体相互作用所需的螺旋堆积和整体静电势获得了新的原子见解。外表面带负电,而通道衬有正电片。因此,EspB具有孔样转运蛋白的许多特征,其可能允许ESX-1底物通过,例如直径为35Å的EsxA-EsxB异二聚体或与其在DNA摄取中的拟议作用一致的B型DNA。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Journal of Structural Biology: X
Journal of Structural Biology: X Biochemistry, Genetics and Molecular Biology-Structural Biology
CiteScore
6.50
自引率
0.00%
发文量
20
审稿时长
62 days
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