Exploitation of a novel adjuvant for polymyxin B against multidrug-resistant Acinetobacter baumannii

被引:6
|
作者
Kim, Seon-Yeong [1 ,2 ]
Seo, Hwi Won [1 ]
Park, Min-Seon [1 ]
Park, Chul Min [3 ,4 ]
Seo, Jinho [5 ]
Rho, Jaerang [2 ]
Myung, Subeen [3 ,4 ]
Ko, Kwan Soo [6 ]
Kim, Jun-Seob [7 ]
Ryu, Choong-Min [1 ]
机构
[1] KRIBB, Infect Dis Res Ctr, Daejeon 34141, South Korea
[2] Chungnam Natl Univ, Dept Microbiol & Mol Biol, Daejeon 34134, South Korea
[3] Korea Res Inst Chem Technol, Dept Infect Dis Res, Daejeon 34114, South Korea
[4] Korea Univ Sci & Technol, Med Chem & Pharmacol, Daejeon 34114, South Korea
[5] KRIBB, Environental Dis Res Ctr, Daejeon 34141, South Korea
[6] Sungkyunkwan Univ, Dept Microbiol, Sch Med, Suwon 16419, South Korea
[7] Incheon Natl Univ, Dept Nanobioengineering, Incheon 22012, South Korea
基金
新加坡国家研究基金会;
关键词
D O I
10.1093/jac/dkac445
中图分类号
R51 [传染病];
学科分类号
100401 ;
摘要
Background Although polymyxin has been used as a last-resort antibiotic against resistant bacteria, its use is restricted due to nephrotoxicity and neurotoxicity. While the present antibiotic resistance issue compels clinicians to reconsider polymyxin use in severe illness cases, polymyxin-resistant microorganisms exert an effect. Objectives To address the issue of antibiotic resistance, the cycle of developing new antibiotics to counteract emerging resistance must be discontinued. Here we tried to develop novel therapies that do not rely on direct antimicrobial activity and thus do not promote antibiotic resistance. Methods By a high-throughout screening system based on bacterial respiration, chemical compounds accelerating the antimicrobial effects of polymyxin B were screened. In vitro and in vivo tests were performed to validate adjuvanticity. In addition, membrane depolarization and total transcriptome analysis were used to determine molecular mechanisms. Results PA108, a newly discovered chemical compound, was used to eradicate polymyxin-resistant A. baumannii and three other species in the presence of polymyxin B at concentrations less than the MIC. Since this molecule lacks self-bactericidal action, we hypothesized that PA108 acts as an antibiotic adjuvant, enhancing the antimicrobial activity of polymyxin B against resistant bacteria. At working concentrations, no toxicity was observed in cell lines or mice, although co-treatment with PA108 and polymyxin B increased survival of infected mouse and decreased bacterial loads in organs. Conclusions Boosting antibiotic efficiency through the use of antibiotic adjuvants holds significant promise for tackling the rise in bacterial antibiotic resistance.
引用
收藏
页码:923 / 932
页数:10
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