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首页> 外文期刊>Journal of microbiology and biotechnology >Development of a bioconversion system using saccharomyces cerevisiae reductase YOR120W and bacillus subtilis glucose dehydrogenase for chiral alcohol synthesis
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Development of a bioconversion system using saccharomyces cerevisiae reductase YOR120W and bacillus subtilis glucose dehydrogenase for chiral alcohol synthesis

机译:使用酿酒酵母还原酶YOR120W和枯草芽孢杆菌葡萄糖脱氢酶生物转化系统的开发,用于手性醇的合成

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摘要

Reductases convert some achiral ketone compounds into chiral alcohols, which are important materials for the synthesis of chiral drugs. The Saccharomyces cerevisiae reductase YOR120W converts ethyl-4-chloro-3-oxobutanoate (ECOB) enantioselectively into (R)-ethyl-4-chloro-3-hydroxybutanoate ((R)-ECHB), an intermediate of a pharmaceutical. As YOR120W requires NADPH as a cofactor for the reduction reaction, a cofactor recycling system using Bacillus subtilis glucose dehydrogenase was employed. Using this coupling reaction system, 100 mM ECOB was converted to (R)-ECHB. A homology modeling and site-directed mutagenesis experiment were performed to determine the NADPH-binding site of YOR120W. Four residues (Q29, K264, N267, and R270) were suggested by homology and docking modeling to interact directly with 2'-phosphate of NADPH. Among them, two positively charged residues (K264 and R270) were experimentally demonstrated to be necessary for NADPH 2'-phosphate binding. A mutant enzyme (Q29E) showed an enhanced enantiomeric excess value compared with that of the wild-type enzyme.
机译:还原酶将一些非手性酮化合物转化为手性醇,手性醇是合成手性药物的重要原料。酿酒酵母还原酶YOR120W将4-氯-3-氧代丁酸乙酯(ECOB)对映选择性地转化为(R)-4-氯-3-羟基丁酸乙酯((-)-ECHB),其为药物中间体。由于YOR120W需要NADPH作为还原反应的辅助因子,因此采用了使用枯草芽孢杆菌葡萄糖脱氢酶的辅助因子循环系统。使用该偶联反应系统,将100mM ECOB转化为(R)-ECHB。进行同源性建模和定点诱变实验以确定YOR120W的NADPH结合位点。通过同源性和对接模型建议了四个残基(Q29,K264,N267和R270)直接与NADPH的2'-磷酸相互作用。其中,实验证明两个带正电荷的残基(K264和R270)对于NADPH 2'-磷酸结合是必需的。与野生型酶相比,突变酶(Q29E)的对映体过量值有所提高。

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