1. Academic Validation
  2. Stereoselective hydroxylation of isophorone by variants of the cytochromes P450 CYP102A1 and CYP101A1

Stereoselective hydroxylation of isophorone by variants of the cytochromes P450 CYP102A1 and CYP101A1

  • Enzyme Microb Technol. 2018 Apr;111:29-37. doi: 10.1016/j.enzmictec.2018.01.002.
Shaghayegh Dezvarei 1 Joel H Z Lee 1 Stephen G Bell 2
Affiliations

Affiliations

  • 1 Department of Chemistry, School of Physical Sciences, University of Adelaide, Adelaide, 5005, Australia.
  • 2 Department of Chemistry, School of Physical Sciences, University of Adelaide, Adelaide, 5005, Australia. Electronic address: stephen.bell@adelaide.edu.au.
Abstract

The stereoselective oxidation of hydrocarbons is an area of research where Enzyme biocatalysis can make a substantial impact. The cyclic ketone isophorone was stereoselectively hydroxylated (≥95%) by wild-type CYP102A1 to form (R)-4-hydroxyisophorone, an important chiral synthon and flavour and fragrance compound. CYP102A1 variants were also selective for 4-hydroxyisophorone formation and the product formation rate increased over the wild-type Enzyme by up to 285-fold, with the best mutants being R47L/Y51F/I401P and A74G/F87V/L188Q. The latter variant, which contained mutations in the distal substrate binding pocket, was marginally less selective. Combining perfluorodecanoic acid decoy molecules with the rate accelerating variant R47L/Y51F/I401P engendered further improvement with the purified Enzymes. However when the decoy molecules were used with A74G/F87V/L188Q the amount of product generated by the Enzyme was reduced. Addition of decoy molecules to whole-cell turnovers did not improve the productivity of these CYP102A1 systems. WT CYP101A1 formed significant levels of 7-hydroxyisophorone as a minor product alongside 4-hydroxyisophorone. However the F87W/Y96F/L244A/V247L CYP101A1 mutant was ≥98% selective for (R)-4-hydroxyisophorone. A comparison of the two Enzyme systems using whole-cell oxidation reactions showed that the best CYP101A1 variant was able to generate more product. We also characterised that the further oxidation metabolite 4-ketoisophorone was produced and then subsequently reduced to levodione by an endogenous Escherichia coli ene reductase.

Keywords

Cytochrome P450; Hydroxylation; Isophorone; Regioselective; Stereoselective.

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