Division of Infectious Diseases, Department of Medicine II, University Hospital and Medical Center, Freiburg, Germany.
Faculty of Medicine, Albert-Ludwigs University, Freiburg, Germany.
Microbiol Spectr. 2024 Feb 6;12(2):e0304523. doi: 10.1128/spectrum.03045-23. Epub 2024 Jan 3.
Multidrug resistance poses global challenges, particularly with regard to Gram-negative bacterial infections. In view of the lack of new antibiotics, drug enhancers, such as efflux pump inhibitors (EPIs), have increasingly come into focus. A number of chemically diverse agents have been reported to inhibit AcrB, the main multidrug transporter in , and homologs in other Gram-negative bacteria. However, due to the often varying methodologies used for their characterization, results remain difficult to compare. In this study, using a defined selection of antibiotics known to be efflux substrates, we reevaluated 38 published compounds for their EPI activity. When examined in an strain with stable wild-type AcrB overexpression, we found 17 compounds showing at least fourfold enhancing potency with more than 2 out of 10 test drugs (belonging to eight antibiotic classes). Pyranopyridines (MBX series) were confirmed as the most potent inhibitors among agents reported so far. A new and surprising finding was that their activity, unlike that of the pyridylpiperazine EPI BDM88855, was highly susceptible to the AcrB double-mutation G141D_N282Y, which had previously been shown to diminish drug enhancing of 1-(1-naphthylmethyl)piperazine in a predominantly substrate-specific manner. Conversely, transmembrane region mutation V411A, while eliminating the drug potentiating of the BDM compound, did not decrease the activity of the MBX EPIs. Besides comparative reassessment of the potency of reported EPIs, the study demonstrated the usefulness of mutagenesis approaches providing tools for an initial discrimination of EPIs regarding their mode of function.IMPORTANCEInfections with difficult-to-treat multidrug-resistant bacteria pose an urgent global threat in view of the stagnating development of new antimicrobial substances. Efflux pumps in Gram-negative pathogens are known to substantially contribute to multidrug resistance making them promising targets for chemotherapeutic interventions to restore the efficacy of conventional antibiotics. In the present study, the activity of previously reported efflux pump inhibitors was reassessed using standardized conditions. Relevant drug sensitizing activity could be proven for almost half of the tested compounds. Further characterization of potent inhibitors was achieved by investigating the impact of specific efflux pump mutations. A double-mutation previously known to decrease the activity of the arylpiperazine 1-(1-naphthylmethyl)piperazine also impaired that of the highly efficient pyranopyridine efflux pump inhibitors. Our findings provide direct comparability of reported efflux pump inhibitors and contribute to the elucidation of their mode of action.
多药耐药性带来了全球性的挑战,尤其是在革兰氏阴性菌感染方面。鉴于新抗生素的缺乏,药物增强剂(如外排泵抑制剂[EPIs])越来越受到关注。已经有许多化学结构不同的试剂被报道可以抑制 中的主要多药转运蛋白 AcrB 和其他革兰氏阴性菌中的同源物。然而,由于用于其特征描述的方法往往不同,结果仍然难以比较。在这项研究中,我们使用了一组已知的作为外排底物的抗生素,重新评估了 38 种已发表的化合物的 EPI 活性。当在稳定过表达野生型 AcrB 的 菌株中进行测试时,我们发现有 17 种化合物对 2 种以上的 10 种测试药物(属于 8 种抗生素类别)具有至少 4 倍的增强效力。吡喃吡啶(MBX 系列)被确认为迄今为止报道的最有效的抑制剂。一个新的、令人惊讶的发现是,与吡啶哌嗪 EPI BDM88855 不同,它们的活性非常容易受到 AcrB 双突变 G141D_N282Y 的影响,以前的研究表明,这种突变以主要底物特异性的方式降低了 1-(1-萘基甲基)哌嗪的药物增强作用。相反,跨膜区突变 V411A 虽然消除了 BDM 化合物的药物增效作用,但并没有降低 MBX EPIs 的活性。除了对报道的 EPIs 进行比较性再评估外,该研究还证明了突变方法的有用性,为 EPIs 的功能模式提供了初始区分工具。
重要性
由于新型抗菌物质的发展停滞不前,难以治疗的多药耐药菌感染构成了紧迫的全球威胁。革兰氏阴性病原体中的外排泵被认为对多药耐药性有很大贡献,使它们成为化学治疗干预的有希望的靶点,以恢复传统抗生素的疗效。在本研究中,使用标准化条件重新评估了以前报道的外排泵抑制剂的 活性。几乎一半的测试化合物都能证明具有相关的药物敏化活性。通过研究特定外排泵突变的影响,进一步对有效抑制剂进行了表征。以前已知会降低芳基哌嗪 1-(1-萘基甲基)哌嗪活性的双突变也会降低高效吡喃吡啶外排泵抑制剂的活性。我们的发现提供了报道的外排泵抑制剂的直接可比性,并有助于阐明它们的作用模式。
