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The antimicrobial effect of colistin methanesulfonate on Mycobacterium tuberculosis in vitro

机译:粘菌素甲磺酸盐对结核分枝杆菌的体外抗菌作用

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摘要

Polymyxins have previously been described to have activity against Mycobacterium tuberculosis (MTB), but further research was abandoned due to systemic toxicity concerns to achieve the required MIC. Colistin methanesulfonate (CMS), a polymyxin, is well tolerated when inhaled directly into the lungs, resulting in high local concentrations. We report here for the first time, MIC and MBC data for CMS determined by the microtiter Alamar Blue assay (MABA). We also determined how the MIC would be affected by the presence of pulmonary surfactant (PS) and if any synergy with isoniazid (INH) and rifampicin (RIF) exists. The effect of CMS on the ultrastructure of MTB was also determined. The MIC for CMS was 16 mg/L, while the MBC was 256 mg/L. MIC for CMS in PS was antagonised by eight fold. For synergy, indifference was determined while time-kill assays revealed a greater killing effect when CMS was used together with INH. Ultrastructure analysis suggests that the disruption of the outer polysaccharide layer of MTB by CMS may lead to enhanced uptake of INH. Our findings may provide insight for further investigations of CMS against MTB. (C) 2015 Elsevier Ltd. All rights reserved.
机译:先前已经描述了多粘菌素具有抗结核分枝杆菌(MTB)的活性,但是由于对系统毒性的担忧而无法获得所需的MIC,因此放弃了进一步的研究。直接吸入到肺中时,多粘菌素甲磺酸共利斯汀(CMS)具有良好的耐受性,导致局部浓度很高。我们首次在此报告通过微量滴定仪Alamar Blue分析(MABA)测定的CMS的MIC和MBC数据。我们还确定了肺表面活性剂(PS)的存在将如何影响MIC,以及是否与异烟肼(INH)和利福平(RIF)协同作用。还确定了CMS对MTB超微结构的影响。 CMS的MIC为16 mg / L,而MBC为256 mg / L。 PS中CMS的MIC拮抗了八倍。对于协同作用,可以确定冷漠,而将CMS与INH一起使用时进行的时间杀灭测定则显示出更大的杀伤效果。超微结构分析表明,CMS对MTB外部多糖层的破坏可能导致INH吸收增加。我们的发现可能为进一步针对CMS针对MTB进行调查提供见识。 (C)2015 Elsevier Ltd.保留所有权利。

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