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外膜 usher 通过选择性地催化成熟菌毛相邻亚基之间的供体链交换,保证功能性菌毛的形成。

The outer membrane usher guarantees the formation of functional pili by selectively catalyzing donor-strand exchange between subunits that are adjacent in the mature pilus.

机构信息

Institute of Molecular Biology and Biophysics, ETH Zurich, 8093 Zurich, Switzerland.

出版信息

J Mol Biol. 2010 Feb 12;396(1):1-8. doi: 10.1016/j.jmb.2009.12.005. Epub 2010 Jan 13.

DOI:10.1016/j.jmb.2009.12.005
PMID:20004668
Abstract

Type 1 pili from uropathogenic Escherichia coli are a prototype of adhesive surface organelles assembled and secreted by the conserved chaperone/usher pathway. They are composed of four different homologous protein subunits that need to be assembled in a defined order. In the periplasm, the pilus chaperone FimC donates a beta-strand segment to the subunits to complete their imperfect immunoglobulin-like fold. During subunit assembly, this segment of the chaperone is displaced by an amino-terminal extension of an incoming subunit in a reaction termed donor-strand exchange. To date, the molecular mechanisms underlying the coordinated subunit assembly, in particular the role of the outer membrane usher FimD, are still poorly understood. Here we show that the binding of complexes between FimC and the different pilus subunits to the amino-terminal substrate recognition domain of FimD is an extremely fast process, with association rate constants in the range of 10(7)-10(8) M(-)(1) s(-1) at 20 degrees C. Furthermore, we demonstrate that the ordered assembly of pilus subunits is a consequence of the usher's ability to selectively catalyze the assembly of defined subunit-subunit pairs that are adjacent in the mature pilus. The usher therefore coordinates the assembly of pilus subunits at the stage of donor-strand exchange between pairs of subunits and not at the level of the initial binding of chaperone-subunit complexes.

摘要

尿路致病性大肠杆菌的 1 型菌毛是由保守的伴侣蛋白/usher 途径组装和分泌的粘附表面器官的原型。它们由四个不同的同源蛋白亚基组成,这些亚基需要按照特定的顺序组装。在周质中,菌毛伴侣蛋白 FimC 将一个β-折叠片段捐赠给亚基,以完成它们不完整的免疫球蛋白样折叠。在亚基组装过程中,伴侣蛋白的这个片段被进入的亚基的氨基末端延伸置换,这一反应称为供体链交换。迄今为止,协调亚基组装的分子机制,特别是外膜 usher FimD 的作用,仍然知之甚少。在这里,我们表明 FimC 与不同菌毛亚基之间的复合物与 FimD 的氨基末端底物识别结构域的结合是一个非常快速的过程,在 20°C 时,结合速率常数在 10(7)-10(8) M(-)(1) s(-1)的范围内。此外,我们证明了菌毛亚基的有序组装是 usher 选择性催化成熟菌毛中相邻的特定亚基-亚基对组装的结果。因此,usher 在亚基对之间的供体链交换阶段协调菌毛亚基的组装,而不是在伴侣蛋白-亚基复合物的初始结合水平上。

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