Litcius/Paper detail

Engineering Cytochrome P450s for Enantioselective Cyclopropenation of Internal Alkynes

Kai Chen, Frances H. Arnold

2020Journal of the American Chemical Society94 citationsDOI

Abstract

We report a biocatalytic platform of engineered cytochrome P450 enzymes to carry out efficient cyclopropene synthesis via carbene transfer to internal alkynes. Directed evolution of a serine-ligated P450 variant, P411-C10, yielded a lineage of engineered P411 enzymes that together accommodate a variety of internal aromatic alkynes as substrates for cyclopropenation with unprecedented efficiencies and stereoselectivities (up to 5760 TTN, and all with >99.9% ee). Using an internal aliphatic alkyne bearing a propargylic ether group, different P411 variants can selectively catalyze cyclopropene formation, carbene insertion into a propargylic C–H bond or [3 + 2]-cycloaddition. This tunable reaction selectivity further highlights the benefit of using genetically encoded catalysts to address chemoselectivity challenges.

Topics & Concepts

ChemistryCyclopropeneCarbeneAlkyneEnantioselective synthesisChemoselectivityCycloadditionEtherStereochemistryCatalysisCombinatorial chemistryOrganic chemistryCyclopropane Reaction MechanismsCatalytic C–H Functionalization MethodsSynthetic Organic Chemistry Methods