首页> 外文期刊>Journal of the American Chemical Society >Oxidative Phenol Coupling Reactions Catalyzed by OxyB: A Cytochrome P450 from the Vancomycin Producing Organism. Implications for Vancomycin Biosynthesis
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Oxidative Phenol Coupling Reactions Catalyzed by OxyB: A Cytochrome P450 from the Vancomycin Producing Organism. Implications for Vancomycin Biosynthesis

机译:OxyB催化的氧化苯酚偶联反应:来自万古霉素生产生物的细胞色素P450。对万古霉素生物合成的意义

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OxyB is a cytochrome P450 enzyme that catalyzes the first phenol coupling reaction during the biosynthesis of vancomycin-like glycopeptide antibiotics. The phenol coupling reaction occurs on a linear peptide intermediate linked as a C-terminal thioester to a peptide carrier protein (PCP) domain within the multidomain glycopeptide nonribosomal peptide synthetase (NRPS). Using model peptides with the sequence (R)(NMe)Leu-(R)Tyr-(S)Asn-(R)Hpg-(R)Hpg-(S)Tyr-S-PCP and (R)(NMe)Leu-(R)Tyr-(S)Asn-(R)-Hpg-(R)Hpg-(S)Tyr-(S)Dpg-S-PCP (where Hpg = 4-hydroxyphenylglycine, and Dpg = 3,5-dihydroxyphenylglycine), or containing (R)Leu instead of (R)(NMe)Leu, attached to recombinant PCPs derived from modules-6 and -7 in the vancomycin NRPS, we show that cross-linking of Hpg4 and Tyr6 by OxyB can occur in both hexapeptide- and heptapeptide-PCP conjugates. Thus, whereas OxyB may act preferentially on a hexapeptide still linked to the PCP-6 in NRPS subunit-2, it is possible that a linear heptapeptide intermediate linked to PCP-7 in NRPS subunit-3 may also be transformed into monocyclic product. For turnover, OxyB requires electrons, which in vitro can be supplied by spinach ferredoxin and E. coli flavodoxin reductase. Turnover is also dependent upon the presence of molecular oxygen. The model substrate (R)-(NMe)Leu-(R)Tyr-(S)Asn-(R)Hpg-(R)Hpg-(S)Tyr-S-PCP is transformed into cross-linked product by OxyB with a k_(cat) of 0.1 s~(-1) and K_m in the range 4-13 μM. Equilibrium binding of this substrate to OxyB, monitored by UV-vis, is accompanied by a typical low-to-high spin state change in the heme, characterized with a K_d of 17± 5 μM.
机译:OxyB是一种细胞色素P450酶,可在万古霉素样糖肽抗生素的生物合成过程中催化第一个酚偶联反应。酚偶联反应发生在线性肽中间体上,该中间体作为C末端硫酯与多结构域糖肽非核糖体肽合成酶(NRPS)中的肽载体蛋白(PCP)域连接。使用具有(R)(NMe)Leu-(R)Tyr-(S)Asn-(R)Hpg-(R)Hpg-(S)Tyr-S-PCP和(R)(NMe)Leu序列的模型肽-(R)Tyr-(S)Asn-(R)-Hpg-(R)Hpg-(S)Tyr-(S)Dpg-S-PCP(其中Hpg = 4-羟基苯基甘氨酸,Dpg = 3,5-二羟基苯基甘氨酸),或含有(R)Leu而不是(R)(NMe)Leu,与万古霉素NRPS中衍生自模块6和-7的重组PCP相连,我们显示可以通过OxyB发生Hpg4和Tyr6的交联在六肽-和七肽-PCP缀合物中都存在。因此,尽管OxyB可以优先作用于仍与NRPS亚基2中的PCP-6连接的六肽,但也有可能将与NRPS亚基3中的PCP-7连接的线性七肽中间体转化为单环产物。对于营业额,OxyB需要电子,菠菜铁氧还蛋白和大肠杆菌黄酮毒素还原酶可以提供体外电子。周转率还取决于分子氧的存在。 (R)-(NMe)Leu-(R)Tyr-(S)Asn-(R)Hpg-(R)Hpg-(S)Tyr-S-PCP的模型底物通过OxyB转化为交联产物k_(cat)为0.1 s〜(-1),K_m在4-13μM的范围内。该底物与OxyB的平衡结合(通过UV-vis监测)伴随着血红素中典型的从低到高自旋状态变化,特征在于K_d为17±5μM。

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