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Rv1218c, an ABC transporter of Mycobacterium tuberculosis with implications in drug discovery.

机译:Rv1218c,一种结核分枝杆菌的ABC转运蛋白,对药物发现有影响。

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Efflux systems are important in determining the efficacy of antibiotics used in the treatment of bacterial infections. In the last decade much attention has been paid to studying the efflux pumps of mycobacteria. New classes of compounds are under investigation for development into potential candidate drugs for the treatment of tuberculosis. Quite often, these have poor bactericidal activities but exhibit excellent target (biochemical) inhibition. Microarray studies conducted in our laboratories for deciphering the mode of action of experimental drugs revealed the presence of putative ABC transporters. Among these transporters, Rv1218c was chosen for studying its physiological relevance in mediating efflux in Mycobacterium tuberculosis. A DeltaRv1218c mutant of M. tuberculosis displayed a 4- to 8-fold increase in the inhibitory and bactericidal potency for different classes of compounds. The MICs and MBCs were reversed to wild-type values when the full-length Rv1218c gene was reintroduced into the DeltaRv1218c mutant on a multicopy plasmid. Most of the compound classes had significantly better bactericidal activity in the DeltaRv1218c mutant than in the wild-type H37Rv, suggesting the involvement of Rv1218c gene product in effluxing these compounds from M. tuberculosis. The implication of these findings on tuberculosis drug discovery is discussed.
机译:外排系统对于确定用于治疗细菌感染的抗生素的功效很重要。在过去的十年中,已经非常注意研究分枝杆菌的外排泵。目前正在研究新型化合物,以开发出可能用于治疗结核病的候选药物。通常,它们的杀菌活性较差,但具有出色的靶标(生化)抑制作用。在我们实验室中进行的用于破译实验药物作用方式的微阵列研究表明存在假定的ABC转运蛋白。在这些转运蛋白中,选择Rv1218c来研究其在介导结核分枝杆菌外排中的生理相关性。结核分枝杆菌的DeltaRv1218c突变体对不同种类的化合物显示出4至8倍的抑制力和杀菌力。当将全长Rv1218c基因重新引入多拷贝质粒上的DeltaRv1218c突变体中时,MIC和MBC反转为野生型值。大多数化合物类别在DeltaRv1218c突变体中具有比野生型H37Rv明显更好的杀菌活性,表明Rv1218c基因产物参与了从结核分枝杆菌中排出这些化合物。讨论了这些发现对结核病药物发现的意义。

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