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细菌趋化性的控制。

Control of bacterial chemotaxis.

作者信息

Eisenbach M

机构信息

Department of Membrane Research and Biophysics, Weizmann Institute of Science, Rehovot, Israel.

出版信息

Mol Microbiol. 1996 Jun;20(5):903-10. doi: 10.1111/j.1365-2958.1996.tb02531.x.

Abstract

Bacterial chemotaxis, which has been extensively studied for three decades, is the most prominent model system for signal transduction in bacteria. Chemotaxis is achieved by regulating the direction of flagellar rotation. The regulation is carried out by the chemotaxis protein, CheY. This protein is activated by a stimulus-dependent phosphorylation mediated by an autophosphorylatable kinase (CheA) whose activity is controlled by chemoreceptors. Upon phosphorylation, CheY dissociates from its kinase, binds to the switch at the base of the flagellar motor, and changes the motor rotation from the default direction (counter-clockwise) to clockwise. Phosphorylation may also be involved in terminating the response. Phosphorylated CheY binds to the phosphatase CheZ and modulates its oligomeric state and thereby its dephosphorylating activity. Thus CheY phosphorylation appears to be involved in controlling both the excitation and adaptation mechanisms of bacterial chemotaxis. Additional control sites might be involved in bacterial chemotaxis, e.g. lateral control at the receptor level, control at the motor level, or control by metabolites that link central metabolism with chemotaxis.

摘要

细菌趋化性已被广泛研究了三十年,是细菌信号转导中最突出的模型系统。趋化性是通过调节鞭毛旋转方向来实现的。这种调节由趋化蛋白CheY执行。该蛋白由一种自磷酸化激酶(CheA)介导的刺激依赖性磷酸化激活,CheA的活性受化学感受器控制。磷酸化后,CheY与其激酶解离,与鞭毛马达基部的开关结合,并将马达旋转从默认方向(逆时针)变为顺时针。磷酸化也可能参与终止反应。磷酸化的CheY与磷酸酶CheZ结合,调节其寡聚状态,从而调节其去磷酸化活性。因此,CheY磷酸化似乎参与控制细菌趋化性的兴奋和适应机制。细菌趋化性可能还涉及其他控制位点,例如受体水平的侧向控制、马达水平的控制或通过将中心代谢与趋化性联系起来的代谢物进行的控制。

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