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双组分信号转导应答调节因子CpxR的信号整合

Signal integration by the two-component signal transduction response regulator CpxR.

作者信息

Wolfe Alan J, Parikh Niyati, Lima Bruno P, Zemaitaitis Bozena

机构信息

Department of Microbiology and Immunology, Loyola University Medical School, 2160 S. First Ave., Bldg. 105, Maywood, IL 60153, USA.

出版信息

J Bacteriol. 2008 Apr;190(7):2314-22. doi: 10.1128/JB.01906-07. Epub 2008 Jan 25.

Abstract

The CpxAR two-component signal transduction system in Escherichia coli and other pathogens senses diverse envelope stresses and promotes the transcription of a variety of genes that remedy these stresses. An important member of the CpxAR regulon is cpxP. The CpxA-dependent transcription of cpxP has been linked to stresses such as misfolded proteins and alkaline pH. It also has been proposed that acetyl phosphate, the intermediate of the phosphotransacetylase (Pta)-acetate kinase (AckA) pathway, can activate the transcription of cpxP in a CpxA-independent manner by donating its phosphoryl group to CpxR. We tested this hypothesis by measuring the transcription of cpxP using mutants with mutations in the CpxAR pathway, mutants with mutations in the Pta-AckA pathway, and mutants with a combination of both types of mutations. From this epistasis analysis, we learned that CpxR integrates diverse stimuli. The stimuli that originate in the envelope depend on CpxA, while those associated with growth and central metabolism depend on the Pta-AckA pathway. While CpxR could receive a phosphoryl group from acetyl phosphate, this global signal was not the primary trigger for CpxR activation associated with the Pta-AckA pathway. On the strength of these results, we contend that the interactions between central metabolism and signal transduction can be quite complex and that successful investigations of such interactions must include a complete epistatic analysis.

摘要

大肠杆菌及其他病原体中的CpxAR双组分信号转导系统可感知多种包膜应激,并促进多种应对这些应激的基因的转录。CpxAR调控子的一个重要成员是cpxP。cpxP依赖CpxA的转录与诸如错误折叠蛋白和碱性pH等应激有关。也有人提出,磷酸转乙酰酶(Pta)-乙酸激酶(AckA)途径的中间产物乙酰磷酸可通过将其磷酰基捐赠给CpxR,以不依赖CpxA 的方式激活cpxP的转录。我们通过使用CpxAR途径发生突变的突变体、Pta-AckA途径发生突变的突变体以及两种类型突变组合的突变体来测量cpxP的转录,对这一假设进行了测试。通过这种上位性分析,我们了解到CpxR整合了多种刺激。源自包膜的刺激依赖于CpxA,而与生长和中心代谢相关的刺激则依赖于Pta-AckA途径。虽然CpxR可以从乙酰磷酸接收一个磷酰基,但这种全局信号并不是与Pta-AckA途径相关的CpxR激活的主要触发因素。基于这些结果,我们认为中心代谢与信号转导之间的相互作用可能相当复杂,并且对此类相互作用的成功研究必须包括完整的上位性分析。

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