Chen Xu , Qipeng Cheng , Kaichao Chen , Pui kin So , Wenbin Jin , Yanjuan Gu , Iris Lai-king Wong , Edward Wai Chi Chan , Kwok-Yin Wong , Kin Fai Chan , Sheng Chen
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These compounds were found to insert their long carbon chain to a hydrophobic pocket of bacterial phosphoethanolamine transferases including MCR-1, competitively blocking the binding of lipid A tail for substrate recognition and modification, resulting in the increase of bacterial sensitivity to colistin. In addition, these compounds were also found to dissipate bacterial membrane potential leading to the increase of bacterial sensitivity to colistin. Importantly, combinational use of DOM with colistin exhibited remarkable protection of test animals against infections by colistin-resistant bacteria in both mouse thigh infection and sepsis models. For mice infected by colistin-susceptible bacteria, the combinational use of DOM and colistin enable us to use lower dose of colistin to for efficient treatment. These properties render DOM excellent adjuvant candidates that help transform colistin into a highly potent antimicrobial agent for treatment of colistin-resistant Gram-negative bacterial infections and allowed us to use of a much lower dosage of colistin to reduce its toxicity against colistin-susceptible bacterial infection such as carbapenem-resistant Enterobacterales.</p></div>","PeriodicalId":18564,"journal":{"name":"Microbiological research","volume":"288 ","pages":"Article 127879"},"PeriodicalIF":6.1000,"publicationDate":"2024-08-15","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Repurposing cetylpyridinium chloride and domiphen bromide as phosphoethanolamine transferase inhibitor to combat colistin-resistant Enterobacterales\",\"authors\":\"Chen Xu , Qipeng Cheng , Kaichao Chen , Pui kin So , Wenbin Jin , Yanjuan Gu , Iris Lai-king Wong , Edward Wai Chi Chan , Kwok-Yin Wong , Kin Fai Chan , Sheng Chen\",\"doi\":\"10.1016/j.micres.2024.127879\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<div><p>The emergence of plasmid-encoded colistin resistance mechanisms, MCR-1, a phosphoethanolamine transferase, rendered colistin ineffective as last resort antibiotic against severe infections caused by clinical Gram-negative bacterial pathogens. 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引用次数: 0
摘要
质粒编码的可乐定耐药机制(MCR-1,一种磷乙醇胺转移酶)的出现,使可乐定无法作为抗击临床革兰氏阴性细菌病原体引起的严重感染的最后手段。通过筛选美国食品和药物管理局(FDA)批准的药物库,我们发现了两种结构相似的化合物,即氯化十六烷基吡啶(CET)和溴化多米酚(DOM),这两种化合物在耐大肠杆菌素和易感肠杆菌属中都能增强大肠杆菌素的活性。研究发现,这些化合物能将其长碳链插入细菌磷乙醇胺转移酶(包括 MCR-1)的疏水口袋,竞争性地阻断脂质 A 尾的结合以识别和修饰底物,从而提高细菌对可乐定的敏感性。此外,研究还发现这些化合物还能消除细菌膜电位,从而提高细菌对可乐定的敏感性。重要的是,在小鼠大腿感染和败血症模型中,联合使用 DOM 和可乐定可显著保护试验动物免受耐可乐定细菌的感染。对于被可乐定敏感细菌感染的小鼠,DOM 和可乐定的联合使用使我们能够使用较低剂量的可乐定来进行有效治疗。DOM 的这些特性使其成为极佳的辅助候选药物,有助于将秋水仙素转化为治疗耐秋水仙素革兰氏阴性菌感染的高效抗菌剂,并使我们能够使用更低剂量的秋水仙素来降低其对耐碳青霉烯类肠杆菌等秋水仙素敏感细菌感染的毒性。
Repurposing cetylpyridinium chloride and domiphen bromide as phosphoethanolamine transferase inhibitor to combat colistin-resistant Enterobacterales
The emergence of plasmid-encoded colistin resistance mechanisms, MCR-1, a phosphoethanolamine transferase, rendered colistin ineffective as last resort antibiotic against severe infections caused by clinical Gram-negative bacterial pathogens. Through screening FDA-approved drug library, we identified two structurally similar compounds, namely cetylpyridinium chloride (CET) and domiphen bromide (DOM), which potentiated colistin activity in both colistin-resistant and susceptible Enterobacterales. These compounds were found to insert their long carbon chain to a hydrophobic pocket of bacterial phosphoethanolamine transferases including MCR-1, competitively blocking the binding of lipid A tail for substrate recognition and modification, resulting in the increase of bacterial sensitivity to colistin. In addition, these compounds were also found to dissipate bacterial membrane potential leading to the increase of bacterial sensitivity to colistin. Importantly, combinational use of DOM with colistin exhibited remarkable protection of test animals against infections by colistin-resistant bacteria in both mouse thigh infection and sepsis models. For mice infected by colistin-susceptible bacteria, the combinational use of DOM and colistin enable us to use lower dose of colistin to for efficient treatment. These properties render DOM excellent adjuvant candidates that help transform colistin into a highly potent antimicrobial agent for treatment of colistin-resistant Gram-negative bacterial infections and allowed us to use of a much lower dosage of colistin to reduce its toxicity against colistin-susceptible bacterial infection such as carbapenem-resistant Enterobacterales.
期刊介绍:
Microbiological Research is devoted to publishing reports on prokaryotic and eukaryotic microorganisms such as yeasts, fungi, bacteria, archaea, and protozoa. Research on interactions between pathogenic microorganisms and their environment or hosts are also covered.