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冷冻电镜断层分析末端细胞器突变体提示支原体的运动机制。

Cryo-electron tomography analyses of terminal organelle mutants suggest the motility mechanism of Mycoplasma genitalium.

机构信息

Buchmann Institute for Molecular Life Sciences and Institute of Biophysics, Goethe University Frankfurt, Max-von-Laue Str. 15, Frankfurt 60438, Germany.

Departament de Bioquímica i Biologia Molecular and Institut de Biotecnologia i Biomedicina, Universitat Autònoma de Barcelona, Cerdanyola del Vallès 08193, Spain.

出版信息

Mol Microbiol. 2018 May;108(3):319-329. doi: 10.1111/mmi.13938. Epub 2018 Mar 24.

Abstract

The terminal organelle of Mycoplasma genitalium is responsible for bacterial adhesion, motility and pathogenicity. Localized at the cell tip, it comprises an electron-dense core that is anchored to the cell membrane at its distal end and to the cytoplasm at its proximal end. The surface of the terminal organelle is also covered with adhesion proteins. We performed cellular cryoelectron tomography on deletion mutants of eleven proteins that are implicated in building the terminal organelle, to systematically analyze the ultrastructural effects. These data were correlated with microcinematographies, from which the motility patterns can be quantitatively assessed. We visualized diverse phenotypes, ranging from mild to severe cell adhesion, motility and segregation defects. Based on our observations, we propose a double-spring ratchet model for the motility mechanism that explains our current and previous observations. Our model, which expands and integrates the previously suggested inchworm model, allocates specific functions to each of the essential components of this unique bacterial motility system.

摘要

生殖道支原体的末端细胞器负责细菌的黏附、运动和致病性。它定位于细胞顶端,由一个电子致密核心组成,其远端锚定在细胞膜上,近端锚定在细胞质上。末端细胞器的表面也覆盖有黏附蛋白。我们对参与构建末端细胞器的十一种蛋白质的缺失突变体进行了细胞冷冻电子断层扫描,以系统地分析超微结构的影响。这些数据与微电影相关联,可从中定量评估运动模式。我们观察到了不同的表型,从轻度到严重的细胞黏附、运动和分离缺陷都有。基于我们的观察结果,我们提出了一个用于运动机制的双弹簧棘轮模型,该模型解释了我们目前和以前的观察结果。我们的模型扩展并整合了以前提出的尺蠖模型,为这个独特的细菌运动系统的每个基本组成部分分配了特定的功能。

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