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首页> 外文期刊>Biochemical Society Transactions >Modulation of the Rcs-mediated signal transfer by conformational flexibility.
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Modulation of the Rcs-mediated signal transfer by conformational flexibility.

机译:通过构象柔韧性调节RCS介导的信号传输。

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The Rcs (regulator of capsule synthesis) signalling complex comprises the membrane-associated hybrid sensor kinases RcsC and RcsD, the transcriptional regulator RcsB and the two co-inducers RcsA and RcsF. Acting as a global regulatory network, the Rcs phosphorelay controls multiple cellular pathways including capsule synthesis, cell division, motility, biofilm formation and virulence mechanisms. Signal-dependent communication of the individual Rcs domains showing histidine kinase, phosphoreceiver, phosphoryl transfer and DNA-binding activities is characteristic and essential for the modulation of signal transfer. We have analysed the structures of core elements of the Rcs network including the RcsC-PR (phosphoreceiver domain of RcsC) and the RcsD-HPt (histidine phosphotransfer domain of RcsD), and we have started to characterize the dynamics and recognition mechanisms of the proteins. RcsC-PR represents a typical CheY-like alpha/beta/alpha sandwich fold and it shows a large conformational flexibility near the active-site residue Asp(875). NMR analysis revealed that RcsC-PR is able to adopt preferred conformations upon Mg(2+) co-ordination, BeF(3)(-) activation, phosphate binding and RcsD-HPt recognition. In contrast, the alpha-helical structure of RcsD-HPt is conformationally stable and contains a recognition area in close vicinity to the active-site His(842) residue. Our studies indicate the importance of protein dynamics and conformational exchange for the differential response to the variety of signals perceived by complex regulatory networks.
机译:RCS(胶囊合成的调节剂)信号传导复合物包括与膜相关的杂化传感器激酶RCSC和RCSD,转录调节器RCSB以及两个共同诱导剂RCSA和RCSF。 RCS Phosphoray充当全球调节网络,控制了包括胶囊合成,细胞分裂,运动,生物膜形成和毒力机制在内的多个细胞途径。单个RCS结构域的信号依赖性通信,显示了组氨酸激酶,磷酸盐,磷酸化转移和DNA结合活性对于信号转移的调节是必不可少的。我们已经分析了RCS网络的核心元素的结构,包括RCSC-PR(RCSC的磷酸酯结构域)和RCSD-HPT(RCSD的组氨酸磷酸转移域),我们已经开始表征蛋白质的动力学和识别机制。 RCSC-PR代表典型的chey状α/β/α夹层褶皱,它在活动位置残基ASP附近显示出较大的构象灵活性(875)。 NMR分析表明,RCSC-PR能够在Mg(2+)协调时采用首选构象,BEF(3)( - )激活,磷酸盐结合和RCSD-HPT识别。相比之下,RCSD-HPT的α螺旋结构在构象上是稳定的,并且包含一个识别区域,附近与主动位点他的(842)残基相邻。我们的研究表明,蛋白质动力学和构象交换对复杂调节网络感知的各种信号的差异响应的差异交换的重要性。

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