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Site-specific methylation in Bacillus subtilis chemotaxis: effect of covalent modifications to the chemotaxis receptor McpB

机译:枯草芽孢杆菌的特异性甲基化:共价修饰对趋化性受体MCPB的影响

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The Bacillus subtilis chemotaxis pathway employs a receptor methylation system that functions differently from the one in the canonical Escherichia coli pathway. Previously, we hypothesized that B. subtilis employs a site-specific methylation system for adaptation where methyl groups are added and removed at different sites. This study investigated how covalent modifications to the adaptation region of the chemotaxis receptor McpB altered its apparent affinity for its cognate ligand, asparagine, and also its ability to activate the CheA kinase. This receptor has three closely spaced adaptation sites located at residues Gln371, Glu630 and Glu637. We found that amidation, a putative methylation mimic, of site 371 increased the receptor's apparent affinity for asparagine and its ability to activate the CheA kinase. Conversely, amidation of sites 630 and 637 reduced the receptor's ability to activate the kinase but did not affect the apparent affinity for asparagine, suggesting that activity and sensitivity are independently controlled in B. subtilis. We also examined how electrostatic interactions may underlie this behaviour, using homology models. These findings further our understanding of the site-specific methylation system in B. subtilis by demonstrating how the modification of specific sites can have varying effects on receptor function.
机译:枯草芽孢杆菌趋化性途径采用受体甲基化体系,其与规范大肠杆菌途径中的一种不同。以前,我们假设B.枯草芽孢杆菌采用位点特异性甲基化体系,以适应加入甲基并在不同位点除去。该研究研究了对趋化性的受体MCPB的适应区域的共价修饰如何改变了其对其同源配体,天冬酰胺的表观亲和力,以及其活化乳酸激酶的能力。该受体具有位于残留物GLN371,GLU630和GLU637的三个紧密间隔的适应部位。我们发现,酰胺化,推定的甲基化模拟物,位点371增加了受体对芦酰胺的表观亲和力及其激活Chea激酶的能力。相反,对位点630和637的酰胺化减少了受体激活激酶的能力,但不影响天冬酰胺的表观亲和力,表明活动和敏感性在B.枯草芽孢杆菌中独立地控制。我们还检查了静电交互如何使用同源模型来实现这种行为。这些发现进一步了解B.枯草芽孢杆菌在枯草芽孢杆菌中的理解,通过证明如何对受体功能具有不同的影响。

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