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以及对 α,β-香树脂醇外排泵抑制作用的评价。

and evaluation of efflux pumps inhibition of α,β-amyrin.

机构信息

Graduate Program in Biological Chemistry, Department of Biological Chemistry, Regional University of Cariri, Crato, CE, Brazil.

Science and Technology Centre, Course of Chemistry, State University Vale do Acaraú, Sobral, CE, Brazil.

出版信息

J Biomol Struct Dyn. 2022;40(23):12785-12799. doi: 10.1080/07391102.2021.1976277. Epub 2021 Sep 16.

DOI:10.1080/07391102.2021.1976277
PMID:34528866
Abstract

The use of the bacterial efflux pump mechanism to reduce the concentrations of antibiotics in the intracellular to the extracellular region is one of the main mechanisms by which bacteria acquire resistance to antibiotics. The present study aims to evaluate the antibacterial activity of the α,β-amyrin mixture isolated from against the multidrug-resistant strains of 06 and 10, and to verify the inhibition of the efflux resistance mechanisms against the strains of 1199B and K2068, carrying the NorA and MepA efflux pumps, respectively. The α,β-amyrin did not show clinically relevant direct bacterial activity. However, the α,β-amyrin when associated with the gentamicin antibiotic presented synergistic effect against the multidrug-resistant bacterial strain of 10. In strains with efflux pumps, α,β-amyrin was able to inhibit the action of the efflux protein NorA against Ethidium Bromide. However, this inhibitory effect was not observed in the MepA efflux pump. In addition, when evaluating the effect of standard efflux pump inhibitors, clorptomazine and CCCP, α,β-amyrin showed a decrease in MIC, demonstrating the presence of the efflux mechanism through synergism. Docking studies indicate that α, β-amyrin have a higher affinity energy to MepA, and NorA than ciprofloxacin and norfloxacin. Also, α, β-amyrin bind to the same region of the binding site as these antibiotics. It was concluded that the α, β-amyrin has the potential to increase antibacterial activity with the association of antibiotics, together with the ability to be a strong candidate for an efflux pump inhibitor.Communicated by Ramaswamy H. Sarma.

摘要

细菌外排泵机制将抗生素在细胞内的浓度降低到细胞外区域是细菌获得抗生素耐药性的主要机制之一。本研究旨在评估从 中分离出的α,β-齐墩果酸混合物对 06 和 10 株多药耐药株的抗菌活性,并验证其对分别携带 NorA 和 MepA 外排泵的 1199B 和 K2068 株抑制外排耐药机制的作用。α,β-齐墩果酸没有显示出临床相关的直接细菌活性。然而,当与庆大霉素抗生素联合使用时,α,β-齐墩果酸对 10 株多药耐药菌表现出协同作用。在外排泵菌株中,α,β-齐墩果酸能够抑制外排蛋白 NorA 对溴化乙锭的作用。然而,这种抑制作用在 MepA 外排泵中没有观察到。此外,当评估标准外排泵抑制剂氯丙嗪和 CCCP 的作用时,α,β-齐墩果酸显示 MIC 降低,表明存在通过协同作用的外排机制。对接研究表明,α,β-齐墩果酸与环丙沙星和诺氟沙星相比,对 MepA 和 NorA 具有更高的亲和能。此外,α,β-齐墩果酸与这些抗生素结合在相同的结合部位。研究结果表明,α,β-齐墩果酸具有与抗生素联合增加抗菌活性的潜力,同时也具有成为一种强大的外排泵抑制剂的潜力。通讯作者为 Ramaswamy H. Sarma。

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