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Identification of novel diphenyl urea inhibitors of Mt-GuaB2 active against Mycobacterium tuberculosis

机译:鉴定抗结核分枝杆菌的MT-GUAB2的新型二苯基尿素抑制剂

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In contrast with most bacteria, which harbour a single inosine monophosphate dehydrogenase (IMPDH) gene, the genomic sequence of Mycobacterium tuberculosis H37Rv predicts three genes encoding IMPDH: guaB1, guaB2 and guaB3. These three genes were cloned and expressed in Escherichia coli to evaluate functional IMPDH activity. Purified recombinant Mt-GuaB2, which uses inosine monophosphate as a substrate, was identified as the only active GuaB orthologue in M. tuberculosis and showed optimal activity at pH?8.5 and 37?°C. Mt-GuaB2 was inhibited significantly in vitro by a panel of diphenyl urea-based derivatives, which were also potent anti-mycobacterial agents against M. tuberculosis and Mycobacterium smegmatis, with MICs in the range of 0.2–0.5?μg ml?1. When Mt-GuaB2 was overexpressed on a plasmid in trans in M. smegmatis, a diphenyl urea analogue showed a 16-fold increase in MIC. Interestingly, when Mt-GuaB orthologues (Mt-GuaB1 and 3) were also overexpressed on a plasmid in trans in M. smegmatis, they also conferred resistance, suggesting that although these Mt-GuaB orthologues were inactive in vitro, they presumably titrate the effect of the inhibitory properties of the active compounds in vivo.
机译:与大多数细菌相比,涉及涉及单一的肌炎单磷酸脱氢酶(IMPh)基因的细菌,结核分枝杆菌的基因组序列H37RV预测了编码IMPDH的三种基因:GUAB1,GUAB2和GUAB3。将这三种基因克隆并在大肠杆菌中表达,以评估功能性IMPh活性。纯化的重组MT-GUAB2,其使用单磷酸钠作为底物,被鉴定为Cuberculosis中唯一的活性Guab直酯,并且在pHα.8.5和37℃下显示出最佳活性。通过基于二苯基尿素的衍生物的面板在体外显着抑制MT-Guab2,其也是针对M.结核病和分枝杆菌的抗分子药物的有效的抗分枝杆菌剂,其范围为0.2-0.5Ω××1。当MT-Guab2在M. Smogmatis的反式中的质粒上过表达时,二苯基脲类似物显示出MIC增加16倍。有趣的是,当MT-Guab orthologues(MT-Guab1和3)在M. Smogmatis中的反式中的质粒上过表达时,它们也赋予抗性,表明虽然这些MT-GUAA出生物在体外无活性,但是它们可能是滴定效果体内活性化合物的抑制性质。

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