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Deciphering the Molecular Recognition Mechanism of Multidrug Resistance Staphylococcus aureus NorA Efflux Pump Using a Supervised Molecular Dynamics Approach

机译:使用监督分子动力学方法破译金黄色葡萄球菌NorA外排泵的分子识别机制

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摘要

The use and misuse of antibiotics has resulted in critical conditions for drug-resistant bacteria emergency, accelerating the development of antimicrobial resistance (AMR). In this context, the co-administration of an antibiotic with a compound able to restore sufficient antibacterial activity may be a successful strategy. In particular, the identification of efflux pump inhibitors (EPIs) holds promise for new antibiotic resistance breakers (ARBs). Indeed, bacterial efflux pumps have a key role in AMR development; for instance, NorA efflux pump contributes to Staphylococcus aureus (S. aureus) resistance against fluoroquinolone antibiotics (e.g., ciprofloxacin) by promoting their active extrusion from the cells. Even though NorA efflux pump is known to be a potential target for EPIs development, the absence of structural information about this protein and the little knowledge available on its mechanism of action have strongly hampered rational drug discovery efforts in this area. In the present work, we investigated at the molecular level the substrate recognition pathway of NorA through a Supervised Molecular Dynamics (SuMD) approach, using a NorA homology model. Specific amino acids were identified as playing a key role in the efflux pump-mediated extrusion of its substrate, paving the way for a deeper understanding of both the mechanisms of action and the inhibition of such efflux pumps.
机译:抗生素的使用和滥用已导致紧急情况下耐药细菌的紧急状况,加速了抗菌素耐药性(AMR)的发展。在这种情况下,抗生素与能够恢复足够抗菌活性的化合物共同给药可能是成功的策略。特别是,外排泵抑制剂(EPI)的鉴定为新型抗生素耐药性阻断剂(ARB)带来了希望。实际上,细菌外排泵在AMR的发展中起着关键作用。例如,NorA外排泵通过促进金黄色葡萄球菌(S. aureus)对细胞中氟喹诺酮类抗生素(例如环丙沙星)的耐药性而起作用。尽管已知NorA外排泵是EPIs开发的潜在目标,但由于缺乏有关该蛋白质的结构信息以及对其作用机理的了解很少,因此严重阻碍了该领域的合理药物研发工作。在当前的工作中,我们使用NorA同源性模型,通过有监督的分子动力学(SuMD)方法在分子水平上研究了NorA的底物识别途径。特定氨基酸被鉴定为在外排泵介导的底物挤出中起关键作用,为更深入地了解这种外排泵的作用机理和抑制作用铺平了道路。

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