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跨内膜Tol-Pal系统产生的力

Force-Generation by the Trans-Envelope Tol-Pal System.

作者信息

Webby Melissa N, Williams-Jones Daniel P, Press Cara, Kleanthous Colin

机构信息

Department of Biochemistry, University of Oxford, Oxford, United Kingdom.

出版信息

Front Microbiol. 2022 Mar 3;13:852176. doi: 10.3389/fmicb.2022.852176. eCollection 2022.

Abstract

The Tol-Pal system spans the cell envelope of Gram-negative bacteria, transducing the potential energy of the proton motive force (PMF) into dissociation of the TolB-Pal complex at the outer membrane (OM), freeing the lipoprotein Pal to bind the cell wall. The primary physiological role of Tol-Pal is to maintain OM integrity during cell division through accumulation of Pal molecules at division septa. How the protein complex couples the PMF at the inner membrane into work at the OM is unknown. The effectiveness of this trans-envelope energy transduction system is underscored by the fact that bacteriocins and bacteriophages co-opt Tol-Pal as part of their import/infection mechanisms. Mechanistic understanding of this process has been hindered by a lack of structural data for the inner membrane TolQ-TolR stator, of its complexes with peptidoglycan (PG) and TolA, and of how these elements combined power events at the OM. Recent studies on the homologous stators of Ton and Mot provide a starting point for understanding how Tol-Pal works. Here, we combine protein modeling with previous structural data on sub-complexes of Tol-Pal as well as mutagenesis, crosslinking, co-conservation analysis and functional data. Through this composite pooling of , , and data, we propose a mechanism for force generation in which PMF-driven rotary motion within the stator drives conformational transitions within a long TolA helical hairpin domain, enabling it to reach the TolB-Pal complex at the OM.

摘要

Tol-Pal系统跨越革兰氏阴性菌的细胞包膜,将质子动力势(PMF)的势能转化为外膜(OM)处TolB-Pal复合物的解离,使脂蛋白Pal游离出来以结合细胞壁。Tol-Pal的主要生理作用是通过在分裂隔膜处积累Pal分子,在细胞分裂过程中维持外膜的完整性。蛋白质复合物如何将内膜处的PMF与外膜处的作用相耦合尚不清楚。细菌素和噬菌体将Tol-Pal作为其导入/感染机制的一部分,这一事实凸显了这种跨包膜能量转导系统的有效性。由于缺乏内膜TolQ-TolR定子及其与肽聚糖(PG)和TolA的复合物的结构数据,以及这些元件如何共同驱动外膜处的能量事件,对这一过程的机制理解受到了阻碍。最近对Ton和Mot同源定子的研究为理解Tol-Pal的工作方式提供了一个起点。在这里,我们将蛋白质建模与Tol-Pal亚复合物的先前结构数据以及诱变、交联、共保守分析和功能数据相结合。通过这种对 、 和 数据的综合汇总,我们提出了一种力产生机制,即定子内PMF驱动的旋转运动驱动长TolA螺旋发夹结构域内的构象转变,使其能够在外膜处与TolB-Pal复合物结合。

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