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多种高扭矩细菌鞭毛马达利用保守的蛋白质支架组装更宽的定子环。

Diverse high-torque bacterial flagellar motors assemble wider stator rings using a conserved protein scaffold.

作者信息

Beeby Morgan, Ribardo Deborah A, Brennan Caitlin A, Ruby Edward G, Jensen Grant J, Hendrixson David R

机构信息

Department of Life Sciences, Imperial College of London, London SW7 2AZ, United Kingdom;

Department of Microbiology, University of Texas Southwestern Medical Center, Dallas, TX 75390;

出版信息

Proc Natl Acad Sci U S A. 2016 Mar 29;113(13):E1917-26. doi: 10.1073/pnas.1518952113. Epub 2016 Mar 14.

Abstract

Although it is known that diverse bacterial flagellar motors produce different torques, the mechanism underlying torque variation is unknown. To understand this difference better, we combined genetic analyses with electron cryo-tomography subtomogram averaging to determine in situ structures of flagellar motors that produce different torques, from Campylobacter and Vibrio species. For the first time, to our knowledge, our results unambiguously locate the torque-generating stator complexes and show that diverse high-torque motors use variants of an ancestrally related family of structures to scaffold incorporation of additional stator complexes at wider radii from the axial driveshaft than in the model enteric motor. We identify the protein components of these additional scaffold structures and elucidate their sequential assembly, demonstrating that they are required for stator-complex incorporation. These proteins are widespread, suggesting that different bacteria have tailored torques to specific environments by scaffolding alternative stator placement and number. Our results quantitatively account for different motor torques, complete the assignment of the locations of the major flagellar components, and provide crucial constraints for understanding mechanisms of torque generation and the evolution of multiprotein complexes.

摘要

虽然已知不同的细菌鞭毛马达产生不同的扭矩,但其扭矩变化的潜在机制尚不清楚。为了更好地理解这种差异,我们将遗传分析与电子冷冻断层扫描亚断层图平均技术相结合,以确定弯曲杆菌属和弧菌属中产生不同扭矩的鞭毛马达的原位结构。据我们所知,我们的结果首次明确地定位了产生扭矩的定子复合体,并表明不同的高扭矩马达使用一个祖先相关结构家族的变体,在比模型肠道马达离轴向驱动轴更远的半径处,搭建额外定子复合体的整合支架。我们确定了这些额外支架结构的蛋白质成分,并阐明了它们的顺序组装,证明它们是定子复合体整合所必需的。这些蛋白质分布广泛,表明不同的细菌通过搭建替代定子的位置和数量,针对特定环境调整了扭矩。我们的结果定量地解释了不同的马达扭矩,完成了主要鞭毛成分位置的确定,并为理解扭矩产生机制和多蛋白复合体的进化提供了关键的限制条件。

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