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针对单一生物体开发的抗菌药物:对新型抗艰难梭菌化合物非达霉素和LFF571敏感性降低的机制及频率

Antibacterials Developed to Target a Single Organism: Mechanisms and Frequencies of Reduced Susceptibility to the Novel Anti-Clostridium difficile Compounds Fidaxomicin and LFF571.

作者信息

Leeds Jennifer A

机构信息

Infectious Disease Area, Novartis Institutes for BioMedical Research, Emeryville, California 94608.

出版信息

Cold Spring Harb Perspect Med. 2016 Feb 1;6(2):a025445. doi: 10.1101/cshperspect.a025445.

Abstract

Clostridium difficile is the most common cause of antibacterial-associated diarrhea. Clear clinical presentation and rapid diagnostics enable targeted therapy for C. difficile infection (CDI) to start quickly. CDI treatment includes metronidazole and vancomycin (VAN). Despite decades of use for CDI, no clinically meaningful resistance to either agent has emerged. Fidaxomicin (FDX), an RNA polymerase inhibitor, is also approved to treat CDI. Mutants with reduced susceptibility to FDX have been selected in vitro by single and multistep methods. Strains with elevated FDX minimum inhibitory concentrations (MICs) were also identified from FDX-treated patients in clinical trials. LFF571 is an exploratory agent that inhibits EF-Tu. In a proof-of-concept study, LFF571 was safe and effective for treating CDI. Spontaneous mutants with reduced susceptibility to LFF571 were selected in vitro in a single step, but not via serial passage. Although there are several agents in development for treatment of CDI, this review summarizes the frequencies and mechanisms of C. difficile mutants displaying reduced susceptibility to FDX or LFF71.

摘要

艰难梭菌是抗菌药物相关性腹泻最常见的病因。清晰的临床表现和快速诊断使得艰难梭菌感染(CDI)的靶向治疗能够迅速启动。CDI的治疗包括甲硝唑和万古霉素(VAN)。尽管这两种药物用于CDI治疗已有数十年,但尚未出现临床上有意义的耐药情况。非达霉素(FDX),一种RNA聚合酶抑制剂,也被批准用于治疗CDI。通过单步和多步方法在体外筛选出了对FDX敏感性降低的突变体。在临床试验中,也从接受FDX治疗的患者中鉴定出了FDX最低抑菌浓度(MIC)升高的菌株。LFF571是一种抑制EF-Tu的探索性药物。在一项概念验证研究中,LFF571治疗CDI安全有效。在体外单步筛选出了对LFF571敏感性降低的自发突变体,但连续传代未筛选出。尽管有几种治疗CDI的药物正在研发中,但本综述总结了艰难梭菌对FDX或LFF71敏感性降低的突变体的频率和机制。

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