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法莫替丁通过影响 OmpA 增强利福平对鲍曼不动杆菌的活性。

Famotidine Enhances Rifampicin Activity against Acinetobacter baumannii by Affecting OmpA.

机构信息

College of Animal Science and Technology, Jilin Agricultural University, Changchun, China.

Branch of Animal Husbandry, Jilin Academy of Agricultural Science, Changchun, China.

出版信息

J Bacteriol. 2023 Aug 24;205(8):e0018723. doi: 10.1128/jb.00187-23. Epub 2023 Jul 13.

Abstract

The development of novel antibiotic adjuvants is imminent because of the frequent emergence of resistance in Gram-negative bacteria, which severely restricts the efficiency and longevity of commonly used clinical antibiotics. It is reported that famotidine, a clinical inhibitor of gastric acid secretion, enhances the antibacterial activity of rifamycin antibiotics, especially rifampicin, against Gram-negative bacteria and reverses drug resistance. Studies have shown that famotidine disrupts the cell membrane of Acinetobacter baumannii and inhibits the expression of the outer membrane protein gene, while causing a dissipation of the plasma membrane potential, compensatively upregulating the pH gradient and ultimately increasing the accumulation of reactive oxygen species by leading to increased bacterial mortality. In addition, famotidine also inhibited the efflux pump activity and the biofilm formation of A. baumannii. In the Galleria mellonella and mouse infection models, the combination of famotidine and rifampicin increased the survival rate of infected animals and decreased the bacterial load in mouse organs. In conclusion, famotidine has the potential to be a novel rifampicin adjuvant, providing a new option for the treatment of clinical Gram-negative bacterial infections. In this study, famotidine was discovered for the first time to have potential as an antibiotic adjuvant, enhancing the antibacterial activity of rifamycin antibiotics against A. baumannii and overcoming the limitations of drug therapy. With the discovery of novel applications for the guanidine-containing medication famotidine, the viability of screening prospective antibiotic adjuvants from guanidine-based molecules was further explored. In addition, famotidine exerts activity by affecting the OmpA protein of the cell membrane, indicating that this protein might be used as a therapeutic drug target to treat A. baumannii infections.

摘要

新型抗生素佐剂的开发迫在眉睫,因为革兰氏阴性菌的耐药性频繁出现,这严重限制了常用临床抗生素的效率和持久性。有报道称,法莫替丁是一种临床胃酸分泌抑制剂,可增强利福霉素类抗生素(尤其是利福平)对革兰氏阴性菌的抗菌活性,并逆转耐药性。研究表明,法莫替丁破坏鲍曼不动杆菌的细胞膜,抑制外膜蛋白基因的表达,同时导致质膜电位耗散,通过补偿性地上调 pH 梯度,最终增加活性氧的积累,从而导致细菌死亡率增加。此外,法莫替丁还抑制鲍曼不动杆菌的外排泵活性和生物膜形成。在金龟子幼虫和小鼠感染模型中,法莫替丁和利福平的联合使用提高了感染动物的存活率,并降低了小鼠器官中的细菌负荷。总之,法莫替丁有可能成为一种新型利福平佐剂,为治疗临床革兰氏阴性菌感染提供了新的选择。在这项研究中,法莫替丁首次被发现具有作为抗生素佐剂的潜力,增强了利福霉素类抗生素对鲍曼不动杆菌的抗菌活性,并克服了药物治疗的局限性。随着胍基药物法莫替丁新应用的发现,进一步探索了从胍基分子中筛选潜在抗生素佐剂的可行性。此外,法莫替丁通过影响细胞膜上的 OmpA 蛋白发挥作用,表明该蛋白可能被用作治疗鲍曼不动杆菌感染的治疗药物靶点。

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