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首页> 外文期刊>FEMS Microbiology Letters >Characterization of SgcE6, the flavin reductase component supporting FAD-dependent halogenation and hydroxylation in the biosynthesis of the enediyne antitumor antibiotic C-1027
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Characterization of SgcE6, the flavin reductase component supporting FAD-dependent halogenation and hydroxylation in the biosynthesis of the enediyne antitumor antibiotic C-1027

机译:SgcE6的特征,黄酮还原酶成分支持烯二炔抗肿瘤抗生素C-1027生物合成中FAD依赖的卤化和羟基化作用

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摘要

The C-1027 enediyne antitumor antibiotic from Streptomyces globisporus possesses an (S)-3-chloro-5-hydroxy-beta-tyrosine moiety, the chloro- and hydroxy-substituents of which are installed by a flavin-dependent halogenase SgcC3 and monooxygenase SgcC, respectively. Interestingly, a single flavin reductase, SgcE6, can provide reduced flavin to both enzymes. Bioinformatics analysis reveals that, similar to other flavin reductases involved in natural product biosynthesis, SgcE6 belongs to the HpaC-like subfamily of the Class I flavin reductases. The present study describes the steady-state kinetic characterization of SgcE6 as a strictly NADH- and FAD-specific enzyme.
机译:球形双链霉菌的C-1027烯二炔抗肿瘤抗生素具有(S)-3-氯-5-羟基-β-酪氨酸部分,其氯和羟基取代基由黄素依赖性卤化酶SgcC3和单加氧酶SgcC安装, 分别。有趣的是,单一的黄素还原酶SgcE6可以为这两种酶提供减少的黄素。生物信息学分析表明,与参与天然产物生物合成的其他黄素还原酶相似,SgcE6属于I类黄素还原酶的HpaC样亚家族。本研究描述了SgcE6作为严格的NADH和FAD特异性酶的稳态动力学特征。

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