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首页> 外文期刊>Antimicrobial agents and chemotherapy. >Mycobacterium tuberculosis embB codon 306 mutations confer moderately increased resistance to ethambutol in vitro and in vivo.
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Mycobacterium tuberculosis embB codon 306 mutations confer moderately increased resistance to ethambutol in vitro and in vivo.

机译:结核分枝杆菌embB密码子306突变在体外和体内均赋予对乙胺丁醇的抗性适度增加。

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Ethambutol (EMB) is a major component of the first-line therapy of tuberculosis. Mutations in codon 306 of embB (embB306) were suggested as a major resistance mechanism in clinical isolates. To directly analyze the impact of individual embB306 mutations on EMB resistance, we used allelic exchange experiments to generate embB306 mutants of M. tuberculosis H37Rv. The level of EMB resistance conferred by particular mutations was measured in vitro and in vivo after EMB therapy by daily gavage in a mouse model of aerogenic tuberculosis. The wild-type embB306 ATG codon was replaced by embB306 ATC, ATA, or GTG, respectively. All of the obtained embB306 mutants exhibited a 2- to 4-fold increase in EMB MIC compared to the wild-type H37Rv. In vivo, the one selected embB306 GTG mutant required a higher dose of ethambutol to restrict its growth in the lung compared to wild-type H37Rv. These experiments demonstrate that embB306 point mutations enhance the EMB MIC in vitro to a moderate, but significant extent, and reduce the efficacy of EMB treatment in the animal model. We propose that conventional EMB susceptibility testing, in combination with embB306 genotyping, may guide dose adjustment to avoid clinical treatment failure in these low-level resistant strains.
机译:乙胺丁醇(EMB)是结核病一线治疗的主要组成部分。 embB(embB306)密码子306的突变被认为是临床分离株的主要耐药机制。为了直接分析单个embB306突变对EMB抗性的影响,我们使用了等位基因交换实验来生成结核分枝杆菌H37Rv的embB306突变体。由EMB治疗后在体外和体内通过日常管饲法在有氧结核的小鼠模型中测量由特定突变赋予的EMB抗性水平。野生型embB306 ATG密码子分别替换为embB306 ATC,ATA或GTG。与野生型H37Rv相比,所有获得的embB306突变体的EMB MIC均提高了2到4倍。在体内,与野生型H37Rv相比,一个选定的embB306 GTG突变体需要较高剂量的乙胺丁醇来限制其在肺中的生长。这些实验证明embB306点突变可在体外将EMB MIC增强至中等水平,但程度显着,并降低EMB治疗在动物模型中的功效。我们建议,常规的EMB敏感性测试与embB306基因分型相结合,可以指导剂量调整,以避免这些低水平耐药菌株的临床治疗失败。

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