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抗菌肽预先处理的细菌会产生耐药性并持续存在。

Bacteria primed by antimicrobial peptides develop tolerance and persist.

机构信息

Freie Universität Berlin, Institut für Biologie, Evolutionary Biology, Berlin, Germany.

Institute of Integrative Biology, Zürich, Switzerland.

出版信息

PLoS Pathog. 2021 Mar 31;17(3):e1009443. doi: 10.1371/journal.ppat.1009443. eCollection 2021 Mar.

Abstract

Antimicrobial peptides (AMPs) are key components of innate immune defenses. Because of the antibiotic crisis, AMPs have also come into focus as new drugs. Here, we explore whether prior exposure to sub-lethal doses of AMPs increases bacterial survival and abets the evolution of resistance. We show that Escherichia coli primed by sub-lethal doses of AMPs develop tolerance and increase persistence by producing curli or colanic acid, responses linked to biofilm formation. We develop a population dynamic model that predicts that priming delays the clearance of infections and fuels the evolution of resistance. The effects we describe should apply to many AMPs and other drugs that target the cell surface. The optimal strategy to tackle tolerant or persistent cells requires high concentrations of AMPs and fast and long-lasting expression. Our findings also offer a new understanding of non-inherited drug resistance as an adaptive response and could lead to measures that slow the evolution of resistance.

摘要

抗菌肽 (AMPs) 是先天免疫防御的关键组成部分。由于抗生素危机,抗菌肽也成为了新药的焦点。在这里,我们探讨了先前接触亚致死剂量的抗菌肽是否会增加细菌的生存能力并助长耐药性的进化。我们发现,经亚致死剂量的抗菌肽预处理的大肠杆菌通过产生卷曲或菌毛酸来产生耐受性并增加持久性,这与生物膜形成有关。我们开发了一个群体动态模型,该模型预测预处理会延迟感染的清除并促进耐药性的进化。我们描述的这些影响应该适用于许多针对细胞表面的抗菌肽和其他药物。解决耐受或持久细胞的最佳策略需要高浓度的抗菌肽以及快速和持久的表达。我们的研究结果还为非遗传性耐药性作为一种适应性反应提供了新的认识,并可能导致减缓耐药性进化的措施。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/90fd/8041211/6c67091b9ea7/ppat.1009443.g001.jpg

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