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抗菌药物组合的种属特异性活性。

Species-specific activity of antibacterial drug combinations.

机构信息

European Molecular Biology Laboratory, Genome Biology Unit, Heidelberg, Germany.

Institute of Microbiology & Infection, School of Biosciences, University of Birmingham, Birmingham, UK.

出版信息

Nature. 2018 Jul;559(7713):259-263. doi: 10.1038/s41586-018-0278-9. Epub 2018 Jul 4.

Abstract

The spread of antimicrobial resistance has become a serious public health concern, making once-treatable diseases deadly again and undermining the achievements of modern medicine. Drug combinations can help to fight multi-drug-resistant bacterial infections, yet they are largely unexplored and rarely used in clinics. Here we profile almost 3,000 dose-resolved combinations of antibiotics, human-targeted drugs and food additives in six strains from three Gram-negative pathogens-Escherichia coli, Salmonella enterica serovar Typhimurium and Pseudomonas aeruginosa-to identify general principles for antibacterial drug combinations and understand their potential. Despite the phylogenetic relatedness of the three species, more than 70% of the drug-drug interactions that we detected are species-specific and 20% display strain specificity, revealing a large potential for narrow-spectrum therapies. Overall, antagonisms are more common than synergies and occur almost exclusively between drugs that target different cellular processes, whereas synergies are more conserved and are enriched in drugs that target the same process. We provide mechanistic insights into this dichotomy and further dissect the interactions of the food additive vanillin. Finally, we demonstrate that several synergies are effective against multi-drug-resistant clinical isolates in vitro and during infections of the larvae of the greater wax moth Galleria mellonella, with one reverting resistance to the last-resort antibiotic colistin.

摘要

抗微生物药物耐药性的传播已成为一个严重的公共卫生关注点,使曾经可治愈的疾病再次致命,并破坏了现代医学的成就。药物联合使用可以帮助对抗多种耐药细菌感染,但它们在很大程度上尚未得到探索,并且很少在临床上使用。在这里,我们分析了来自三种革兰氏阴性病原体(大肠杆菌、肠炎沙门氏菌血清型 Typhimurium 和铜绿假单胞菌)的六个菌株中近 3000 种抗生素、人体靶向药物和食品添加剂的剂量解析组合,以确定抗菌药物联合使用的一般原则,并了解它们的潜力。尽管这三个物种具有系统发育相关性,但我们检测到的超过 70%的药物相互作用是物种特异性的,20%显示出菌株特异性,这表明窄谱疗法具有很大的潜力。总的来说,拮抗作用比协同作用更为常见,而且几乎只发生在针对不同细胞过程的药物之间,而协同作用则更为保守,并且在针对同一过程的药物中更为丰富。我们提供了对此二分法的机制见解,并进一步剖析了食品添加剂香草醛的相互作用。最后,我们证明了几种协同作用在体外和大蜡螟幼虫感染中对多药耐药临床分离株有效,其中一种协同作用使对最后一线抗生素粘菌素的耐药性恢复。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/47bc/6219701/62020b9a64d4/emss-78998-f005.jpg

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