Regio- and enantioselective alkane hydroxylation with modified cytochrome P450

Assignee

• CALIFORNIA INSTITUTE OF TECHNOLOGY · US

Inventors

• Frances H. Arnold · Pasadena, US
• Matthew W. Peters · Pasadena, US
• Peter Meinhold · Santa Monica, US

Key dates

Classification

• Technology area (CPC C)Chemistry; Metallurgy
• CPC primaryC12Y114/14001
• WIPO fieldBiotechnology
• WIPO sectorChemistry

Abstract

Cytochrome P450 BM-3 from Bacillus megaterium was engineered using a combination of directed evolution and site-directed mutagenesis to hydroxylate linear alkanes regio- and enantioselectively using atmospheric dioxygen as an oxidant. Mutant 9-10A-A328V hydroxylates octane primarily at the 2-positio to form S-2-octanol (40% ee). Another mutant, 1-12G, hydroxylates alkanes larger than hexane primarily at the 2-position, but forms R-2-alcohols (40-55% ee). These biocatalysts are highly active for alkane substrates and support thousands of product turnovers. These regio- and enantio-selectivities are retained in whole-cell biotransformations with E. coli, where the engineered P450s can be expressed at high levels and the expensive cofactor is supplied endogenously.