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Bacterial ATP-driven transporters of transition metals: physiological roles, mechanisms of action, and roles in bacterial virulence

机译:细菌ATP驱动的过渡金属转运蛋白:生理作用,作用机理和细菌毒力作用

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摘要

Maintaining adequate intracellular levels of transition metals is fundamental to the survival of all organisms. While all transition metals are toxic at elevated intracellular concentrations, metals such as iron, zinc, copper, and manganese are essential to many cellular functions. In prokaryotes, the concerted action of a battery of membrane-embedded transport proteins controls a delicate balance between sufficient acquisition and overload. Representatives from all major families of transporters participate in this task, including ion-gradient driven systems and ATP-utilizing pumps. P-type ATPases and ABC transporters both utilize the free energy of ATP hydrolysis to drive transport. Each of these very different families of transport proteins has a distinct role in maintaining transition metal homeostasis: P-type ATPases prevent intracellular overloading of both essential and toxic metals through efflux while ABC transporters import solely the essential ones. In the present review we discuss how each system is adapted to perform its specific task from mechanistic and structural perspectives. Despite the mechanistic and structural differences between P-type ATPases and ABC transporters, there is one important commonality: in many clinically relevant bacterial pathogens, transporters of transition metals are essential for virulence. Here we present several such examples and discuss how these may be exploited for future antibacterial drug development.
机译:维持足够的细胞内过渡金属含量对所有生物的生存至关重要。尽管所有过渡金属在升高的细胞内浓度下均具有毒性,但诸如铁,锌,铜和锰等金属对于许多细胞功能至关重要。在原核生物中,一系列膜嵌入的转运蛋白的协同作用控制了足够的摄取和超负荷之间的微妙平衡。来自所有主要运输商家族的代表都参加了这项任务,包括离子梯度驱动系统和利用ATP的泵。 P型ATP酶和ABC转运蛋白均利用ATP水解的自由能来驱动转运。这些非常不同的转运蛋白家族中的每一个在维持过渡金属稳态中均具有独特的作用:P型ATPase通过外排阻止必需和有毒金属的细胞内超载,而ABC转运蛋白仅进口必需的。在当前的审查中,我们从机械和结构的角度讨论了如何使每个系统执行其特定任务。尽管P型ATP酶和ABC转运蛋白在机制和结构上存在差异,但仍有一个重要的共性:在许多临床相关的细菌病原体中,过渡金属的转运蛋白对于毒力至关重要。在这里,我们介绍几个这样的例子,并讨论如何将它们用于未来的抗菌药物开发。

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  • 来源
    《Metallomics》 |2011年第11期|p.1098-1108|共11页
  • 作者

    Joshua S. Klein; Oded Lewinson;

  • 作者单位

    1. Department of Microbiology,The Ruth and Bruce Rappaport Faculty of Medicine,The Technion-Israel Institute of Technology, Haifa, Israel;

    1. Department of Microbiology,The Ruth and Bruce Rappaport Faculty of Medicine,The Technion-Israel Institute of Technology, Haifa, Israel;

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