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Crystallographic trapping in the rebeccamycin biosynthetic enzyme RebC

机译:瑞贝卡霉素生物合成酶RebC中的晶体学陷阱

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The biosynthesis of rebeccamycin, an antitumor compound, involves the remarkable eight-electron oxidation of chlorinated chromopyrrolic acid. Although one rebeccamycin biosynthetic enzyme is capable of generating low levels of the eight-electron oxidation product on its own, a second protein, RebC, is required to accelerate product formation and eliminate side reactions. However, the mode of action of RebC was largely unknown. Using crystallography, we have determined a likely function for RebC as a flavin hydroxylase, captured two snapshots of its dynamic catalytic cycle, and trapped a reactive molecule, a putative substrate, in its binding pocket. These studies strongly suggest that the role of RebC is to sequester a reactive intermediate produced by its partner protein and to react with it enzymatically, preventing its conversion to a suite of degradation products that includes, at low levels, the desired product.
机译:抗肿瘤化合物瑞贝卡霉素的生物合成涉及氯化铬吡咯酸的显着八电子氧化。尽管一种雷贝卡霉素生物合成酶能够自行产生低水平的八电子氧化产物,但仍需要第二种蛋白质RebC来加速产物形成并消除副反应。但是,RebC的作用方式在很大程度上是未知的。使用晶体学,我们确定了RebC作为黄素羟化酶的可能功能,捕获了其动态催化循环的两个快照,并在其结合袋中捕获了一种反应性分子(一种假定的底物)。这些研究强烈表明,RebC的作用是隔离由其伴侣蛋白产生的反应性中间体,并与之进行酶促反应,从而防止其转化为一系列降解产物,包括低水平的所需产物。

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