达托霉素
抗生素
动作(物理)
医学
微生物学
金黄色葡萄球菌
生物
细菌
万古霉素
物理
遗传学
量子力学
作者
Jessica A. Buttress,A. L. Schaefer,Alan Koh,Jessica Wheatley,Katarzyna Mickiewicz,Michaela Wenzel,Henrik Strahl
出处
期刊:
[Cold Spring Harbor Laboratory]
日期:2024-12-21
被引量:4
标识
DOI:10.1101/2024.12.20.629673
摘要
ABSTRACT Daptomycin is a lipopeptide antibiotic, commonly used as last resort treatment against multidrug resistant Gram-positive pathogens. Despite its clinical success, the mechanism through which daptomycin exerts its antibacterial properties has remained controversial. Much of the debate is focused around daptomycin’s ability to depolarise the cytoplasmic membrane, potential formation of large membrane pores, and its more recently discovered capability to inhibit cell wall synthesis and disturb membrane lipid domain organisation through interactions with cell wall precursor lipids. Here we show that, rather than representing different facets of a single underlying activity, daptomycin exhibits two independent antibacterial mechanisms of action: (i) targeting of cell wall precursor lipids that leads to cell wall synthesis inhibition and (ii) membrane depolarisation that does not rely on interactions with cell wall precursor lipids. This dual mechanism of action provides an explanation for the frequently disagreeing findings obtained through in vivo and in vitro studies and explains why resistance development towards daptomycin is slow and multifactorial. In a broader context, this demonstrates that dual mechanism antibiotics can be clinically successful and exhibit favourable characteristics in terms of real-world, clinically relevant resistance development.
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