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首页> 外文期刊>PLoS Biology >Two-Component Signal Transduction Pathways Regulating Growth and Cell Cycle Progression in a Bacterium: A System-Level Analysis
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Two-Component Signal Transduction Pathways Regulating Growth and Cell Cycle Progression in a Bacterium: A System-Level Analysis

机译:调节细菌中生长和细胞周期进展的双组分信号转导途径:系统级分析

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Two-component signal transduction systems, comprised of histidine kinases and their response regulator substrates, are the predominant means by which bacteria sense and respond to extracellular signals. These systems allow cells to adapt to prevailing conditions by modifying cellular physiology, including initiating programs of gene expression, catalyzing reactions, or modifying protein–protein interactions. These signaling pathways have also been demonstrated to play a role in coordinating bacterial cell cycle progression and development. Here we report a system-level investigation of two-component pathways in the model organism Caulobacter crescentus. First, by a comprehensive deletion analysis we show that at least 39 of the 106 two-component genes are required for cell cycle progression, growth, or morphogenesis. These include nine genes essential for growth or viability of the organism. We then use a systematic biochemical approach, called phosphotransfer profiling, to map the connectivity of histidine kinases and response regulators. Combining these genetic and biochemical approaches, we identify a new, highly conserved essential signaling pathway from the histidine kinase CenK to the response regulator CenR, which plays a critical role in controlling cell envelope biogenesis and structure. Depletion of either cenK or cenR leads to an unusual, severe blebbing of cell envelope material, whereas constitutive activation of the pathway compromises cell envelope integrity, resulting in cell lysis and death. We propose that the CenK–CenR pathway may be a suitable target for new antibiotic development, given previous successes in targeting the bacterial cell wall. Finally, the ability of our in vitro phosphotransfer profiling method to identify signaling pathways that operate in vivo takes advantage of an observation that histidine kinases are endowed with a global kinetic preference for their cognate response regulators. We propose that this system-wide selectivity insulates two-component pathways from one another, preventing unwanted cross-talk.
机译:由组分的信号转导系统组成,由组氨酸激酶及其反应调节剂衬底组成,是细菌感觉和对细胞外信号的主要方法。这些系统允许细胞通过改变细胞生理学来适应普遍的条件,包括启动基因表达,催化反应或改性蛋白质 - 蛋白质相互作用的程序。也已经证明了这些信号通路在协调细菌细胞周期进展和发育中起起作用。在这里,我们报告了模型生物裂缝杆菌中的双组分途径的系统级调查。首先,通过综合缺失分析,我们表明,细胞周期进展,生长或形态发生需要106个双组分基因中的至少39个。这些包括九个基因,对于生物体的生长或活力是必不可少的。然后,我们使用一种称为PhosPhospheransfer分析的系统生化方法,以映射组氨酸激酶和响应调节剂的连接性。结合这些遗传和生化方法,我们鉴定了从组氨酸激酶CENK到响应调节器CENR的新的高度保守的必需信号通路,这在控制细胞包络生物发生和结构中起着关键作用。 CENK或CENR的消耗导致细胞包络材料的不寻常严重的膨胀,而途径的组成型活化会损害细胞包膜完整性,导致细胞裂解和死亡。我们提出CENK-CENR途径可以是新的抗生素发育的合适靶标,鉴于靶向细菌细胞壁的先前成功。最后,我们的体外Phosphot ransfer分析方法识别在体内操作的信号通路的能力利用了组氨酸激酶赋予其同源反应调节剂的全球动力学偏好的观察结果。我们提出这种系统宽的选择性彼此的双组分路径,防止了不必要的串扰。

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