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Evolutionary Genomics Suggests That CheV Is an Additional Adaptor for Accommodating Specific Chemoreceptors within the Chemotaxis Signaling Complex

机译:进化基因组学表明,CheV是适应趋化性信号转导复合体内特定化学受体的额外适配器。

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摘要

Escherichia coli and Salmonella enterica are models for many experiments in molecular biology including chemotaxis, and most of the results obtained with one organism have been generalized to another. While most components of the chemotaxis pathway are strongly conserved between the two species, Salmonella genomes contain some chemoreceptors and an additional protein, CheV, that are not found in E. coli. The role of CheV was examined in distantly related species Bacillus subtilis and Helicobacter pylori, but its role in bacterial chemotaxis is still not well understood. We tested a hypothesis that in enterobacteria CheV functions as an additional adaptor linking the CheA kinase to certain types of chemoreceptors that cannot be effectively accommodated by the universal adaptor CheW. Phylogenetic profiling, genomic context and comparative protein sequence analyses suggested that CheV interacts with specific domains of CheA and chemoreceptors from an orthologous group exemplified by the Salmonella McpC protein. Structural consideration of the conservation patterns suggests that CheV and CheW share the same binding spot on the chemoreceptor structure, but have some affinity bias towards chemoreceptors from different orthologous groups. Finally, published experimental results and data newly obtained via comparative genomics support the idea that CheV functions as a “phosphate sink” possibly to off-set the over-stimulation of the kinase by certain types of chemoreceptors. Overall, our results strongly suggest that CheV is an additional adaptor for accommodating specific chemoreceptors within the chemotaxis signaling complex.
机译:大肠杆菌和肠沙门氏菌是许多分子生物学实验(包括趋化性)的模型,用一种生物获得的大多数结果已推广到另一种生物。虽然趋化途径的大多数组成部分在这两个物种之间是高度保守的,但沙门氏菌基因组包含一些化学感受器和一种在大肠杆菌中未发现的蛋白质CheV。在远缘物种枯草芽孢杆菌和幽门螺杆菌中检查了CheV的作用,但其在细菌趋化性中的作用仍未得到很好的了解。我们测试了一个假说,即肠道细菌中CheV充当将CheA激酶连接到某些类型的化学感受器的附加衔接子,而通用适配器CheW无法有效地容纳这些化学感受器。系统发育谱,基因组背景和比较蛋白质序列分析表明,CheV与CheA的特定结构域和来自直系同源组的化学感受器相互作用,例如以沙门氏菌McpC蛋白为例。保守模式的结构考虑表明,CheV和CheW在化学感受器结构上共享相同的结合点,但对来自不同直系同源组的化学感受器具有一定的亲和力偏向。最后,已发表的实验结果和通过比较基因组学新获得的数据支持了这样的观点,即CheV充当“磷酸盐沉陷”,可能抵消某些类型的化学感受器对激酶的过度刺激。总体而言,我们的结果强烈表明,CheV是在趋化性信号复合物中容纳特定化学感受器的额外衔接子。

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