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Biochemical and transcription analysis of acetohydroxyacid synthase isoforms in Mycobacterium tuberculosis identifies these enzymes as potential targets for drug development

机译:结核分枝杆菌乙酰羟基酸合酶同种型的生化和转录分析将这些酶作为药物发育的潜在目标鉴定

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Acetohydroxyacid synthase (AHAS) is a biosynthetic enzyme essential for de novo synthesis of branched-chain amino acids. The genome sequence of Mycobacterium tuberculosis revealed genes encoding four catalytic subunits, ilvB1 (Rv3003c), ilvB2 (Rv3470c), ilvG (Rv1820) and ilvX (Rv3509c), and one regulatory subunit, ilvN (Rv3002c), of AHAS. All these genes were found to be expressed in M. tuberculosis growing in vitro. Each AHAS subunit gene was cloned and expressed in Escherichia coli. AHAS activity of IlvB1 and IlvG was found in cell-free lysates and with recombinant purified proteins. Kinetic studies with purified IlvG revealed positive cooperativity towards substrate and cofactors. To understand the role of the catalytic subunits in the biology of M. tuberculosis, expression of AHAS genes was analysed in different physiological conditions. ilvB1, ilvB2 and ilvG were differentially expressed. The role of ilvB1 in persistence is known, but the upregulation of ilvB2 and ilvG in extended stationary phase, ex vivo, and in acid stress and hypoxic environments, suggests the relevance of AHAS enzymes in the metabolism and survival of M. tuberculosis by functioning as catabolic AHAS. These enzymes are therefore potential targets for drug development.
机译:乙酰羟基酸合酶(AHAs)是一种生物合成酶,对于De Novo合成支链氨基酸必不可少。结核分枝杆菌的基因组序列揭示了编码四个催化亚基,ILVB1(RV3003C),ILVB2(RV3470C),ILVG(RV1820)和ILVX(RV3509C)的基因,以及AHA的一个调节亚基ILVN(RV3002C)。发现所有这些基因在体外生长的肺部结核病中表达。每个AHAS亚基基因被克隆并在大肠杆菌中表达。在无细胞裂解物和重组纯化的蛋白质中发现ILVB1和ILVG的AHAS活性。纯化ILVG的动力学研究显示朝向基底和辅因子的正合作。为了了解催化亚基在核心结核病生物学中的作用,在不同的生理条件下分析了AHAS基因的表达。 ILVB1,ILVB2和ILVG差异表达。 ILVB1在持续性中的作用是已知的,但在延长的固定相,离体和酸性胁迫和缺氧环境中对ILVB2和ILVG的上调表明AHAS酶在代谢中的相关性和通过发挥作用的结核病的相关性分解AHA。因此,这些酶是药物发育的潜在目标。

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