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Powering the ABC multidrug exporter LmrA: How nucleotides embrace the ion-motive force

机译:为ABC多药出口商LmrA提供动力:核苷酸如何拥抱离子动力

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LmrA is a bacterial ATP-binding cassette (ABC) multidrug exporter that uses metabolic energy to transport ions, cytotoxic drugs, and lipids. Voltage clamping in a Port-a-Patch was used to monitor electrical currents associated with the transport of monovalent cationic HEPES+ by single-LmrA transporters and ensembles of transporters. In these experiments, one proton and one chloride ion are effluxed together with each HEPES+ ion out of the inner compartment, whereas two sodium ions are transported into this compartment. Consequently, the sodium-motive force (interior negative and low) can drive this electrogenic ion exchange mechanism in cells under physiological conditions. The same mechanism is also relevant for the efflux of monovalent cationic ethidium, a typical multidrug transporter substrate. Studies in the presence of Mg-ATP (adenosine 5′-triphosphate) show that ion-coupled HEPES+ transport is associated with ATP-bound LmrA, whereas ion-coupled ethidium transport requires ATP binding and hydrolysis. HEPES+ is highly soluble in a water-based environment, whereas ethidium has a strong preference for residence in the water-repelling plasma membrane. We conclude that the mechanism of the ABC transporter LmrA is fundamentally related to that of an ion antiporter that uses extra steps (ATP binding and hydrolysis) to retrieve and transport membrane-soluble substrates from the phospholipid bilayer.
机译:LmrA是一种细菌ATP结合盒(ABC)多药出口商,利用代谢能来运输离子,细胞毒性药物和脂质。 Port-a-Patch中的电压钳位用于监视与单LmrA转运蛋白和转运蛋白集合体对单价阳离子HEPES +的转运相关的电流。在这些实验中,一个质子和一个氯离子与每个HEPES +离子一起流出内部隔室,而两个钠离子被输送到该隔室中。因此,在生理条件下,钠动力(内部负和低)可以驱动细胞中的这种电离子交换机制。相同的机理也与单价阳离子乙锭(一种典型的多药转运蛋白底物)的流出有关。在Mg-ATP(腺苷5'-三磷酸)存在下的研究表明,离子偶联的HEPES +转运与ATP结合的LmrA相关,而离子偶联的乙转运需要ATP结合和水解。 HEPES +在水基环境中高度可溶,而乙锭则强烈希望保留在疏水质膜中。我们得出的结论是,ABC转运蛋白LmrA的机理与使用额外步骤(ATP结合和水解)从磷脂双层中回收和转运膜可溶性底物的离子反转运蛋白的机理基本相关。

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