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化学感受器在信号复合物中的作用:构象改变和不对称偶联。

Chemoreceptors in signalling complexes: shifted conformation and asymmetric coupling.

机构信息

Department of Biochemistry, 117 Schweitzer Hall, University of Missouri-Columbia, Columbia, MO 65211, USA.

出版信息

Mol Microbiol. 2010 Dec;78(5):1313-23. doi: 10.1111/j.1365-2958.2010.07408.x. Epub 2010 Oct 12.

Abstract

Bacterial chemotaxis is mediated by signalling complexes of chemoreceptors, histidine kinase CheA and coupling protein CheW. Interactions in complexes profoundly affect the kinase. We investigated effects of these interactions on chemoreceptors by comparing receptors alone and in complexes. Assays of initial rates of methylation indicated that signalling complexes shifted receptor conformation towards the methylation-on, higher-ligand-affinity, kinase-off state, tuning receptors for greater sensitivity. In contrast, transmembrane and conformational signalling within chemoreceptors was essentially unaltered, consistent with other evidence identifying receptor dimers as the fundamental units of such signalling. In signalling complexes, coupling of ligand binding to kinase activity is cooperative and the dynamic range of kinase control expanded > 100-fold by receptor adaptational modification. We observed no cooperativity in influence of ligand on receptor conformation, only on kinase activity. However, receptor modification generated increased dynamic range in a stepwise fashion, partly in coupling ligand to receptor conformation and partly in coupling receptor conformation to kinase activity. Thus, receptors and kinase were not equivalently affected by interactions in signalling complexes or by ligand binding and adaptational modification, indicating asymmetrical coupling between them. This has implications for mechanisms of precise adaptation. Coupling might vary, providing a previously unappreciated locus for sensory control.

摘要

细菌的化学趋性是由化学感受器、组氨酸激酶 CheA 和偶联蛋白 CheW 的信号复合物介导的。复合物中的相互作用对激酶有深远的影响。我们通过比较单独的受体和复合物来研究这些相互作用对受体的影响。初始甲基化速率测定表明,信号复合物将受体构象向甲基化、高配体亲和力、激酶关闭状态转变,使受体对配体的敏感性更高。相比之下,跨膜和化学感受器内的构象信号基本不变,这与其他将受体二聚体鉴定为这种信号的基本单位的证据一致。在信号复合物中,配体结合与激酶活性的偶联是协同的,通过受体适应性修饰,激酶控制的动态范围扩展了>100 倍。我们观察到配体对受体构象的影响没有协同性,而只有对激酶活性的影响。然而,受体修饰以逐步的方式产生了更大的动态范围,部分是通过将配体与受体构象偶联,部分是通过将受体构象与激酶活性偶联。因此,受体和激酶在信号复合物中的相互作用或配体结合和适应性修饰的影响下,没有被同等地影响,表明它们之间存在不对称的偶联。这对精确适应的机制有影响。耦合可能会有所不同,为感官控制提供了一个以前未被重视的位置。

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