Catalysts on Demand: Selective Oxidations by Laboratory-Evolved Cytochrome P450 BM3

Authors

  • Jared C. Lewis
  • Frances H. Arnold

DOI:

https://doi.org/10.2533/chimia.2009.309

Keywords:

Biocatalysis, Evolution, Drug metabolite, Oxidation, P450

Abstract

Efficient catalysts for selective oxidation of C–H bonds using atmospheric oxygen are highly desirable to decrease the economic and environmental costs associated with conventional oxidation processes. We have used methods of directed evolution to generate variants of bacterial cytochrome P450 BM3 that catalyze hydroxylation and epoxidation of a wide range of nonnative substrates. This fatty acid hydroxylase was converted to a propane monooxygenase (PMO) capable of hydroxylating propane at rates comparable to that of BM3 on its natural substrates. Variants along the PMO evolutionary lineage showed broadened substrate scope; these became the starting points for evolution of a wide array of enzymes that can hydroxylate and derivatize organic scaffolds. This work demonstrates how a single member of enzyme family is readily converted by evolution into a whole family of catalysts for organic synthesis.

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Published

2009-06-24

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Scientific Articles