Directed evolution of P450 peroxide-mediated activity
Silberg, Jonathan Joseph   
California Institute of Technology, Pasadena, CA, United States

The major goal of this proposal is to use evolutionary protein design to explore the molecular mechanism(s) supporting H2O2-mediated oxygenation in heme-enzymes. Cytochrome P450 and chioroperoxidase (CPO) are both heme containing oxidoreductases that stereospecifically catalyze the H2O2-mediated oxygenation of organic substrates. These proteins, however, differ significantly in their catalytic efficiencies. It is not known why CPO catalyzes this reaction more efficiently than P450s and unclear whether a P450 scaffold is compatible with CPO-like activity. To better understand the molecular determinants that allow heme-enzymes to function efficiently, I plan to: 1) engineer P450 variants with CPO-like catalytic efficiency through directed evolution; 2) analyze the mechanism(s) by which P450 variants catalyze oxygenation; and 3) determine the structure of interesting mutants. Through comparison of the activities and structures of wild type and evolved P450 enzymes, I will determine whether P450s adapt a catalytic cycle and active site structure similar to CPO, or if they adapt properties distinct from known heme-enzymes. In addition to providing insight into heme-enzyme activity adaptation, these studies could also aid in the development of single-enzyme monooxygenases with sufficient activity to make them practical biocatalysts for medical and pharmaceutical applications.