Pentamidine sensitizes Gram-negative pathogens to antibiotics and overcomes acquired colistin resistance

粘菌素 微生物学 生物 抗生素 革兰氏阴性菌 细菌 抗生素耐药性 戊脒 革兰氏阴性细菌感染 病毒学 医学 大肠杆菌 肺炎 内科学 基因 遗传学
作者
Jonathan Stokes,Craig R. MacNair,Bushra Ilyas,Shawn French,Jean‐Philippe Côté,Catrien Bouwman,Maya A. Farha,Arthur O. Sieron,Chris Whitfield,Brian K. Coombes,Eric D. Brown
出处
期刊:Nature microbiology 卷期号:2 (5) 被引量:299
标识
DOI:10.1038/nmicrobiol.2017.28
摘要

The increasing use of polymyxins1 in addition to the dissemination of plasmid-borne colistin resistance threatens to cause a serious breach in our last line of defence against multidrug-resistant Gram-negative pathogens, and heralds the emergence of truly pan-resistant infections. Colistin resistance often arises through covalent modification of lipid A with cationic residues such as phosphoethanolamine-as is mediated by Mcr-1 (ref. 2)-which reduce the affinity of polymyxins for lipopolysaccharide3. Thus, new strategies are needed to address the rapidly diminishing number of treatment options for Gram-negative infections4. The difficulty in eradicating Gram-negative bacteria is largely due to their highly impermeable outer membrane, which serves as a barrier to many otherwise effective antibiotics5. Here, we describe an unconventional screening platform designed to enrich for non-lethal, outer-membrane-active compounds with potential as adjuvants for conventional antibiotics. This approach identified the antiprotozoal drug pentamidine6 as an effective perturbant of the Gram-negative outer membrane through its interaction with lipopolysaccharide. Pentamidine displayed synergy with antibiotics typically restricted to Gram-positive bacteria, yielding effective drug combinations with activity against a wide range of Gram-negative pathogens in vitro, and against systemic Acinetobacter baumannii infections in mice. Notably, the adjuvant activity of pentamidine persisted in polymyxin-resistant bacteria in vitro and in vivo. Overall, pentamidine and its structural analogues represent unexploited molecules for the treatment of Gram-negative infections, particularly those having acquired polymyxin resistance determinants.
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