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检测 rifamycin SV 对旅行者腹泻和艰难梭菌相关病原体的体外活性和单步突变分析。

In vitro activity and single-step mutational analysis of rifamycin SV tested against enteropathogens associated with traveler's diarrhea and Clostridium difficile.

机构信息

JMI Laboratories, 345 Beaver Kreek Centre, Suite A, North Liberty, IA 52317, USA.

出版信息

Antimicrob Agents Chemother. 2011 Mar;55(3):992-6. doi: 10.1128/AAC.00688-10. Epub 2010 Dec 13.

Abstract

Rifamycin SV is a broad-spectrum, poorly absorbed antimicrobial agent that, when coupled with MMX technology, is being targeted for the oral treatment of traveler's diarrhea (TD) and Clostridium difficile-associated disease (CDAD). Rifamycin SV was tested for activity against 911 TD-associated enteropathogens and 30 C. difficile isolates collected from several global surveillance studies. Rifamycin SV demonstrated similar antimicrobial activity levels against the Enterobacteriaceae, with MIC₅₀ values ranging from 32 to 128 μg/ml for all but one strain (an enterotoxigenic Escherichia coli at >512 μg/ml). For non-Enterobacteriaceae strains, MIC₅₀ values ranged from 2 to 8 μg/ml, with the exception of Campylobacter spp., for which all strains had MIC values of >512 μg/ml. Rifamycin SV also demonstrated excellent activity (MIC₅₀ of ≤ 0.03 μg/ml) against most C. difficile strains (including one hypervirulent NAP1 strain), and this activity was even superior to the potency observed for vancomycin, metronidazole, and rifaximin. In mutational passaging studies, rifamycin SV induced stable resistance and showed a mutation frequency in E. coli similar to that of rifampin. This study presents the potency of rifamycin SV for enteropathogens commonly recovered from patients with TD and CDAD. Additional in vitro and in vivo studies appear necessary to determine the utility of rifamycin SV as an oral agent for the prevention and treatment of TD and CDAD.

摘要

利福霉素 SV 是一种广谱、吸收不良的抗菌药物,与 MMX 技术结合后,被用于治疗旅行者腹泻(TD)和艰难梭菌相关性疾病(CDAD)的口服治疗。研究人员测试了利福霉素 SV 对 911 株 TD 相关病原体和 30 株艰难梭菌分离株的活性,这些分离株来自几项全球监测研究。利福霉素 SV 对肠杆菌科的抗菌活性水平相似,除一株(产肠毒素大肠埃希菌,MIC₅₀值 >512 μg/ml)外,所有菌株的 MIC₅₀值均为 32 至 128 μg/ml。对于非肠杆菌科菌株,MIC₅₀值为 2 至 8 μg/ml,除弯曲杆菌属外,所有菌株的 MIC 值均 >512 μg/ml。利福霉素 SV 对大多数艰难梭菌菌株(包括一株高毒力 NAP1 菌株)也表现出优异的活性(MIC₅₀值≤0.03 μg/ml),其活性甚至优于万古霉素、甲硝唑和利福昔明。在突变传递研究中,利福霉素 SV 诱导了稳定的耐药性,并且在大肠杆菌中的突变频率与利福平相似。这项研究表明了利福霉素 SV 对 TD 和 CDAD 患者中常见病原体的效力。似乎需要进一步的体外和体内研究来确定利福霉素 SV 作为预防和治疗 TD 和 CDAD 的口服药物的实用性。

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