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An Inexpensive, Efficient Alternative to NADPH to Support Catalysis by Thermostable Cytochrome P450 Enzymes

机译:NADPH廉价,有效的替代方案,以通过热稳定的细胞色素P450酶支持催化

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摘要

Cytochrome P450 enzymes (P450s) are highly desirable catalysts for the regio- and stereo-selective, late-stage functionalization of pharmaceuticals and other fine chemicals. Recently, the resurrected ancestors of drug-metabolizing P450s were shown to be highly thermostable and expressed in high yield, while retaining similar substrate specificity to the extant forms. However, they still rely on NADPH and cytochrome P450 reductase (CPR) to enable catalysis of oxidative transformations. To identify an alternative support system, we screened 10 oxygen surrogates (OSs) for the ability to support P450 ancestors from three different families. Of the 23 ancestors examined, 17 were supported by at least one OS as well as, or better than, by CPR. Using two candidate P450s we showed that OS-dependent P450 catalysis can be optimized in a few steps, boosting product yield from similar to 2.2 % with CPR to 88-100 % with an OS. The principles applied here will facilitate faster evaluation and optimization of OS-supported P450 catalysis versus redox partner-dependent P450 catalysis.
机译:细胞色素P450酶(P450s)是高度理想的催化剂,用于药物和其他精细化学物质的重组和立体选择性,后期官能化。最近,将复合的药物代谢P450s祖先被证明是高稳定的并且以高产率表达,同时将类似的底物特异性保持在远端形式。然而,它们仍然依赖于NADPH和细胞色素P450还原酶(CPR)以使抗氧化转化的催化。为了确定替代支持系统,我们筛选了10个氧代理(OSS),以便能够支持来自三个不同家庭的P450祖先。在检查的23个祖先中,通过CPR至少一个操作系统,至少支持17个,或者比CPR支持。使用两种候选P450S,我们显示OS依赖性P450催化可以在几个步骤中进行优化,将产品产量从CPR与OS的CPR增加到88-100%的2.2%。此处应用的原则将促进OS支持的P450催化的速度评估和优化与氧化还原伙伴依赖的P450催化。

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