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大肠杆菌中由含组氨酸磷酸转移结构域的ArcB杂合传感器激酶介导的双信号传导机制。

A dual-signaling mechanism mediated by the ArcB hybrid sensor kinase containing the histidine-containing phosphotransfer domain in Escherichia coli.

作者信息

Matsushika A, Mizuno T

机构信息

Laboratory of Molecular Microbiology, School of Agriculture, Nagoya University, Chikusa-ku, Nagoya 464-8601, Japan.

出版信息

J Bacteriol. 1998 Aug;180(15):3973-7. doi: 10.1128/JB.180.15.3973-3977.1998.

Abstract

The two components ArcB and ArcA play a crucial role in the signal transduction implicated in the complex transcriptional regulatory network that allows Escherichia coli to sense various respiratory growth conditions. ArcB is a hybrid sensor kinase having multiple phosphorylation sites in its primary amino acid sequence, including a transmitter, a receiver, and a histidine-containing phosphotransfer (HPt) domain. ArcA is a DNA-binding transcriptional regulator with a receiver domain. Results of recent in vitro studies revealed multistep His-to-Asp phosphotransfer circuitry in the ArcB-ArcA signaling system. For this report we conducted a series of in vivo experiments using a set of crucial ArcB mutants to evaluate the regulation of the sdh operon. The results suggested that the phosphorylated His-717 site in the HPt domain of ArcB is essential for anaerobic repression of sdh. Nonetheless, the ArcB mutant lacking this crucial His-717 site does not necessarily exhibit a null phenotype with respect to ArcB-ArcA signaling. The HPt mutant appears to maintain an ability to signal ArcA, particularly under aerobic conditions, which results in a significant repression of sdh. Based on these and other in vivo results, we propose a model in which ArcB functions in its own right as a dual-signaling sensor that is capable of propagating two types of stimuli through two distinct phosphotransfer pathways.

摘要

ArcB和ArcA这两个组分在复杂的转录调控网络所涉及的信号转导中起着关键作用,该网络使大肠杆菌能够感知各种呼吸生长条件。ArcB是一种杂合传感器激酶,在其一级氨基酸序列中有多个磷酸化位点,包括一个发射器、一个接收器和一个含组氨酸的磷酸转移(HPt)结构域。ArcA是一种具有接收器结构域的DNA结合转录调节因子。最近的体外研究结果揭示了ArcB-ArcA信号系统中的多步组氨酸到天冬氨酸的磷酸转移途径。在本报告中,我们使用一组关键的ArcB突变体进行了一系列体内实验,以评估sdh操纵子的调控。结果表明,ArcB的HPt结构域中磷酸化的His-717位点对于sdh的厌氧抑制至关重要。尽管如此,缺乏这个关键His-717位点的ArcB突变体在ArcB-ArcA信号传导方面不一定表现出无效表型。HPt突变体似乎保持了向ArcA发出信号的能力,特别是在有氧条件下,这导致了sdh的显著抑制。基于这些及其他体内实验结果,我们提出了一个模型,其中ArcB本身作为一种双信号传感器发挥作用,能够通过两条不同的磷酸转移途径传递两种类型的刺激。

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本文引用的文献

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