Preclinical safety and efficacy characterization of an LpxC inhibitor against Gram-negative pathogens

抗生素 体内 脂质A 药理学 脂多糖 微生物学 毒性 细菌外膜 体外 败血症 革兰氏阴性菌 生物 医学 免疫学 生物化学 大肠杆菌 内科学 基因 生物技术
作者
Jinshi Zhao,C. Skyler Cochrane,Javaria Najeeb,David M. Gooden,Carly A. Sciandra,Fan Ping,Nadine Lemaître,Kate Newns,Robert A. Nicholas,Ziqiang Guan,Joshua T. Thaden,Vance G. Fowler,Ivan Spasojević,Florent Sebbane,Eric J. Toone,Clayton Duncan,Richard E. Gammans,Pei Zhou
出处
期刊:Science Translational Medicine [American Association for the Advancement of Science]
卷期号:15 (708) 被引量:20
标识
DOI:10.1126/scitranslmed.adf5668
摘要

The UDP-3- O -( R -3-hydroxyacyl)- N -acetylglucosamine deacetylase LpxC is an essential enzyme in the biosynthesis of lipid A, the outer membrane anchor of lipopolysaccharide and lipooligosaccharide in Gram-negative bacteria. The development of LpxC-targeting antibiotics toward clinical therapeutics has been hindered by the limited antibiotic profile of reported non-hydroxamate inhibitors and unexpected cardiovascular toxicity observed in certain hydroxamate and non–hydroxamate-based inhibitors. Here, we report the preclinical characterization of a slow, tight-binding LpxC inhibitor, LPC-233, with low picomolar affinity. The compound is a rapid bactericidal antibiotic, unaffected by established resistance mechanisms to commercial antibiotics, and displays outstanding activity against a wide range of Gram-negative clinical isolates in vitro. It is orally bioavailable and efficiently eliminates infections caused by susceptible and multidrug-resistant Gram-negative bacterial pathogens in murine soft tissue, sepsis, and urinary tract infection models. It displays exceptional in vitro and in vivo safety profiles, with no detectable adverse cardiovascular toxicity in dogs at 100 milligrams per kilogram. These results establish the feasibility of developing oral LpxC-targeting antibiotics for clinical applications.
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