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十三肽菌素:选择性靶向革兰氏阴性菌的非核糖体肽。

The tridecaptins: non-ribosomal peptides that selectively target Gram-negative bacteria.

作者信息

Bann Samantha J, Ballantine Ross D, Cochrane Stephen A

机构信息

School of Chemistry and Chemical Engineering, Queens University Belfast David Keir Building, Stranmillis Road Belfast BT9 5AG UK

出版信息

RSC Med Chem. 2021 Jan 22;12(4):538-551. doi: 10.1039/d0md00413h.

Abstract

Tridecaptins are a re-emerging class of non-ribosomal antibacterial peptides (NRAPs) with potent activity against highly problematic strains of Gram-negative bacteria. An intricate mode of action has been reported to explain the bactericidal activity of these NRAPs, wherein they bind selectivity to the Gram-negative version of the peptidoglycan precursor lipid II on the outer leaflet of the inner membrane and disrupt the proton-motive force. Tridecaptins are highly amenable to synthetic modification owing to their linear structure, therefore, various synthetic analogues have been reported, several of which have enhanced antimicrobial activity, reduced cost of synthesis and/or improved stability towards d-peptidase mediated hydrolysis. It has also been demonstrated that unacylated tridecaptins can act synergistically with clinically relevant antibiotics by sensitizing the outer membrane. This review will summarize past literature on the development/discovery of novel tridecaptin analogues (up until the end of 2020), some of which may be useful therapeutic agents to treat insidious Gram-negative bacterial infections.

摘要

十三肽菌素是一类重新出现的非核糖体抗菌肽(NRAPs),对革兰氏阴性菌的高致病性菌株具有强大活性。据报道,其作用方式复杂,可解释这些NRAPs的杀菌活性,即它们选择性地结合内膜外小叶上革兰氏阴性菌版本的肽聚糖前体脂质II,并破坏质子动力。由于其线性结构,十三肽菌素非常适合进行合成修饰,因此,已报道了多种合成类似物,其中一些具有增强的抗菌活性、降低的合成成本和/或提高了对d-肽酶介导水解的稳定性。还已证明,未酰化的十三肽菌素可通过使外膜敏感化而与临床相关抗生素协同作用。本综述将总结过去关于新型十三肽菌素类似物开发/发现的文献(截至2020年底),其中一些可能是治疗隐匿性革兰氏阴性菌感染的有用治疗剂。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7ff5/8127968/4fbd056e26bb/d0md00413h-f1.jpg

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