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一个精制的原型沙门氏菌 SPI-1 T3SS 基础体模型揭示了其组装的分子基础。

A refined model of the prototypical Salmonella SPI-1 T3SS basal body reveals the molecular basis for its assembly.

机构信息

Department of Biochemistry and Molecular Biology, and Centre for Blood Research, University of British Columbia, Vancouver, British Columbia, Canada.

出版信息

PLoS Pathog. 2013;9(4):e1003307. doi: 10.1371/journal.ppat.1003307. Epub 2013 Apr 25.

Abstract

The T3SS injectisome is a syringe-shaped macromolecular assembly found in pathogenic Gram-negative bacteria that allows for the direct delivery of virulence effectors into host cells. It is composed of a "basal body", a lock-nut structure spanning both bacterial membranes, and a "needle" that protrudes away from the bacterial surface. A hollow channel spans throughout the apparatus, permitting the translocation of effector proteins from the bacterial cytosol to the host plasma membrane. The basal body is composed largely of three membrane-embedded proteins that form oligomerized concentric rings. Here, we report the crystal structures of three domains of the prototypical Salmonella SPI-1 basal body, and use a new approach incorporating symmetric flexible backbone docking and EM data to produce a model for their oligomeric assembly. The obtained models, validated by biochemical and in vivo assays, reveal the molecular details of the interactions driving basal body assembly, and notably demonstrate a conserved oligomerization mechanism.

摘要

T3SS 注射器是一种在致病性革兰氏阴性细菌中发现的注射器状大分子组装体,它允许将毒力效应物直接递送到宿主细胞中。它由一个“基础体”、一个跨越两个细菌膜的“螺母”结构和一个从细菌表面突出的“针”组成。一个中空的通道贯穿整个装置,允许效应蛋白从细菌细胞质向宿主质膜易位。基础体主要由三个形成寡聚同心环的膜嵌入蛋白组成。在这里,我们报告了典型沙门氏菌 SPI-1 基础体的三个结构域的晶体结构,并使用一种新方法,结合对称灵活的骨架对接和 EM 数据,生成了它们的寡聚组装模型。通过生化和体内测定验证的获得模型揭示了驱动基础体组装的相互作用的分子细节,并特别证明了一种保守的寡聚化机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6903/3635987/aa72706c19ef/ppat.1003307.g001.jpg

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