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金黄色葡萄球菌NorA多药转运蛋白的多种新型抑制剂

Multiple novel inhibitors of the NorA multidrug transporter of Staphylococcus aureus.

作者信息

Markham P N, Westhaus E, Klyachko K, Johnson M E, Neyfakh A A

机构信息

Influx, Inc., Chicago, Illinois 60612, USA.

出版信息

Antimicrob Agents Chemother. 1999 Oct;43(10):2404-8. doi: 10.1128/AAC.43.10.2404.

Abstract

The multidrug transporter NorA contributes to the resistance of Staphylococcus aureus to fluoroquinolone antibiotics by promoting their active extrusion from the cell. Previous studies with the alkaloid reserpine, the first identified inhibitor of NorA, indicate that the combination of a chemical NorA inhibitor with a fluoroquinolone could improve the efficacy of this class of antibiotics. Since reserpine is toxic to humans at the concentrations required to inhibit NorA, we sought to identify new inhibitors of NorA that may be used in a clinical setting. Screening of a chemical library yielded a number of structurally diverse inhibitors of NorA that were more potent than reserpine. The new inhibitors act in a synergistic manner with the most widely used fluoroquinolone, ciprofloxacin, by substantially increasing its activity against both NorA-overexpressing and wild-type S. aureus isolates. Furthermore, the inhibitors dramatically suppress the emergence of ciprofloxacin-resistant S. aureus upon in vitro selection with this drug. Some of these new inhibitors, or their derivatives, may prove useful for augmentation of the antibacterial activities of fluoroquinolones in the clinical setting.

摘要

多药转运蛋白NorA通过促进氟喹诺酮类抗生素从细胞中主动排出,从而导致金黄色葡萄球菌对这类抗生素产生耐药性。先前对第一种被鉴定出的NorA抑制剂——生物碱利血平的研究表明,一种化学NorA抑制剂与氟喹诺酮类药物联合使用可以提高这类抗生素的疗效。由于利血平在抑制NorA所需的浓度下对人体有毒,我们试图寻找可用于临床的新型NorA抑制剂。对一个化学文库进行筛选后,得到了许多结构各异的NorA抑制剂,它们比利血平更有效。这些新型抑制剂与使用最广泛的氟喹诺酮类药物环丙沙星协同作用,通过大幅提高其对NorA过表达和野生型金黄色葡萄球菌分离株的活性来发挥作用。此外,这些抑制剂在用环丙沙星进行体外筛选时,能显著抑制耐环丙沙星金黄色葡萄球菌的出现。其中一些新型抑制剂或其衍生物可能在临床上被证明有助于增强氟喹诺酮类药物的抗菌活性。

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