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Ⅰ类羊毛硫抗生素枯草菌素识别靶标的分子机制

Molecular mechanism of target recognition by subtilin, a class I lanthionine antibiotic.

作者信息

Parisot Judicaël, Carey Sarah, Breukink Eefjan, Chan Weng C, Narbad Arjan, Bonev Boyan

机构信息

School of Biomedical Sciences, University of Nottingham, Nottingham NG7 2UH, United Kingdom.

出版信息

Antimicrob Agents Chemother. 2008 Feb;52(2):612-8. doi: 10.1128/AAC.00836-07. Epub 2007 Nov 12.

DOI:10.1128/AAC.00836-07
PMID:17999970
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2224776/
Abstract

The increasing resistance of human pathogens to conventional antibiotics presents a growing threat to the chemotherapeutic management of infectious diseases. The lanthionine antibiotics, still unused as therapeutic agents, have recently attracted significant scientific interest as models for targeting and management of bacterial infections. We investigated the action of one member of this class, subtilin, which permeabilizes lipid membranes in a lipid II-dependent manner and binds bactoprenyl pyrophosphate, akin to nisin. The role the C and N termini play in target recognition was investigated in vivo and in vitro by using the natural N-terminally succinylated subtilin as well as enzymatically truncated subtilin variants. Fluorescence dequenching experiments show that subtilin induces leakage in membranes in a lipid II-dependent manner and that N-succinylated subtilin is roughly 75-fold less active. Solid-state nuclear magnetic resonance was used to show that subtilin forms complexes with membrane isoprenyl pyrophosphates. Activity assays in vivo show that the N terminus of subtilin plays a critical role in its activity. Succinylation of the N terminus resulted in a 20-fold decrease in its activity, whereas deletion of N-terminal Trp abolished activity altogether.

摘要

人类病原体对传统抗生素的耐药性不断增强,这对传染病的化疗管理构成了日益严重的威胁。羊毛硫抗生素作为治疗药物仍未得到应用,但最近作为针对和管理细菌感染的模型引起了科学界的极大兴趣。我们研究了这类抗生素中的一种——枯草菌素的作用,它以脂质II依赖性方式使脂质膜通透,并与细菌萜醇焦磷酸结合,类似于乳链菌肽。通过使用天然N端琥珀酰化的枯草菌素以及酶切截短的枯草菌素变体,在体内和体外研究了C端和N端在靶标识别中的作用。荧光猝灭实验表明,枯草菌素以脂质II依赖性方式诱导膜渗漏,且N-琥珀酰化枯草菌素的活性大约低75倍。固态核磁共振用于表明枯草菌素与膜异戊二烯焦磷酸形成复合物。体内活性测定表明,枯草菌素的N端在其活性中起关键作用。N端琥珀酰化导致其活性降低20倍,而删除N端色氨酸则完全消除了活性。

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