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复杂的双组分信号传导调节α-变形菌纲细菌的一般应激反应。

Complex two-component signaling regulates the general stress response in Alphaproteobacteria.

作者信息

Kaczmarczyk Andreas, Hochstrasser Ramon, Vorholt Julia A, Francez-Charlot Anne

机构信息

Department of Biology, Institute of Microbiology, Eidgenössiche Technische Hochschule Zurich, 8093 Zurich, Switzerland.

Department of Biology, Institute of Microbiology, Eidgenössiche Technische Hochschule Zurich, 8093 Zurich, Switzerland

出版信息

Proc Natl Acad Sci U S A. 2014 Dec 2;111(48):E5196-204. doi: 10.1073/pnas.1410095111. Epub 2014 Nov 17.

Abstract

The general stress response (GSR) in Alphaproteobacteria was recently shown to be controlled by a partner-switching mechanism that is triggered by phosphorylation of the response regulator PhyR. Activation of PhyR ultimately results in release of the alternative extracytoplasmic function sigma factor σ(EcfG), which redirects transcription toward the GSR. Little is known about the signal transduction pathway(s) controlling PhyR phosphorylation. Here, we identified the single-domain response regulator (SDRR) SdrG and seven histidine kinases, PakA to PakG, belonging to the HWE/HisKA2 family as positive modulators of the GSR in Sphingomonas melonis Fr1. Phenotypic analyses, epistasis experiments, and in vitro phosphorylation assays indicate that Paks directly phosphorylate PhyR and SdrG, and that SdrG acts upstream of or in concert with PhyR, modulating its activity in a nonlinear pathway. Furthermore, we found that additional SDRRs negatively affect the GSR in a way that strictly requires PhyR and SdrG. Finally, analysis of GSR activation by thermal, osmotic, and oxidative stress indicates that Paks display different degrees of redundancy and that a specific kinase can sense multiple stresses, suggesting that the GSR senses a particular condition as a combination of, rather than individual, molecular cues. This study thus establishes the alphaproteobacterial GSR as a complex and interlinked network of two-component systems, in which multiple histidine kinases converge to PhyR, the phosphorylation of which is, in addition, subject to regulation by several SDRRs. Our finding that most HWE/HisKA2 kinases contribute to the GSR in S. melonis Fr1 opens the possibility that this notion might also be true for other Alphaproteobacteria.

摘要

最近研究表明,α-变形菌纲中的一般应激反应(GSR)受一种伴侣切换机制控制,该机制由反应调节因子PhyR的磷酸化触发。PhyR的激活最终导致替代胞外功能σ因子σ(EcfG)的释放,从而使转录重定向至GSR。关于控制PhyR磷酸化的信号转导途径知之甚少。在此,我们鉴定出单结构域反应调节因子(SDRR)SdrG以及属于HWE/HisKA2家族的七个组氨酸激酶(从PakA到PakG),它们是甜瓜鞘氨醇单胞菌Fr1中GSR的正向调节因子。表型分析、上位性实验和体外磷酸化分析表明,Paks直接磷酸化PhyR和SdrG,并且SdrG在PhyR的上游起作用或与其协同作用,以非线性途径调节其活性。此外,我们发现其他SDRR以严格依赖PhyR和SdrG的方式对GSR产生负面影响。最后,对热应激、渗透应激和氧化应激下GSR激活的分析表明,Paks表现出不同程度的冗余性,并且特定的激酶可以感知多种应激,这表明GSR将特定条件感知为分子线索的组合而非单个线索。因此,本研究将α-变形菌纲的GSR确立为一个由双组分系统组成的复杂且相互关联的网络,其中多个组氨酸激酶汇聚于PhyR,此外,PhyR的磷酸化还受到多个SDRR的调控。我们发现大多数HWE/HisKA2激酶对甜瓜鞘氨醇单胞菌Fr1中的GSR有贡献,这使得这一概念在其他α-变形菌纲中也可能成立。

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