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多粘菌素治疗失败的原因及填补空白的新衍生物。

Causes of polymyxin treatment failure and new derivatives to fill the gap.

作者信息

Chiu Selena, Hancock Anna M, Schofner Bob W, Sniezek Katherine J, Soto-Echevarria Nashaly, Leon Gabrielle, Sivaloganathan Darshan M, Wan Xuanqing, Brynildsen Mark P

机构信息

Department of Chemical and Biological Engineering, Princeton University, Princeton, NJ, USA.

Department of Molecular Biology, Princeton University, Princeton, NJ, USA.

出版信息

J Antibiot (Tokyo). 2022 Nov;75(11):593-609. doi: 10.1038/s41429-022-00561-3. Epub 2022 Sep 20.

Abstract

Polymyxins are a class of antibiotics that were discovered in 1947 from programs searching for compounds effective in the treatment of Gram-negative infections. Produced by the Gram-positive bacterium Paenibacillus polymyxa and composed of a cyclic peptide chain with a peptide-fatty acyl tail, polymyxins exert bactericidal effects through membrane disruption. Currently, polymyxin B and colistin (polymyxin E) have been developed for clinical use, where they are reserved as "last-line" therapies for multidrug-resistant (MDR) infections. Unfortunately, the incidences of strains resistant to polymyxins have been increasing globally, and polymyxin heteroresistance has been gaining appreciation as an important clinical challenge. These phenomena, along with bacterial tolerance to this antibiotic class, constitute important contributors to polymyxin treatment failure. Here, we review polymyxins and their mechanism of action, summarize the current understanding of how polymyxin treatment fails, and discuss how the next generation of polymyxins holds promise to invigorate this antibiotic class.

摘要

多粘菌素是一类抗生素,于1947年从寻找有效治疗革兰氏阴性菌感染化合物的项目中被发现。多粘菌素由革兰氏阳性菌多粘芽孢杆菌产生,由带有肽-脂肪酰基尾的环状肽链组成,通过破坏细胞膜发挥杀菌作用。目前,多粘菌素B和黏菌素(多粘菌素E)已被开发用于临床,作为多药耐药(MDR)感染的“最后一线”治疗药物。不幸的是,全球范围内对多粘菌素耐药菌株的发生率一直在上升,多粘菌素异质性耐药作为一项重要的临床挑战已受到更多关注。这些现象,连同细菌对这类抗生素的耐受性,是导致多粘菌素治疗失败的重要因素。在此,我们综述多粘菌素及其作用机制,总结目前对多粘菌素治疗失败原因的认识,并讨论新一代多粘菌素如何有望重振这类抗生素。

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