Bifunctional Imine Reductase Cascades for the Synthesis of Saturated N-Heterocycles

Jeremy I Ramsden; Bruna Zucoloto da Costa; Rachel S Heath; James R Marshall; Sasha R Derrington; Juan Mangas-Sanchez; Sarah L Montgomery; Keith R Mulholland; Sebastian C Cosgrove; Nicholas J Turner

doi:10.1021/acscatal.4c03832

Bifunctional Imine Reductase Cascades for the Synthesis of Saturated N-Heterocycles

ACS Catal. 2024 Sep 19;14(19):14703-14710. doi: 10.1021/acscatal.4c03832. eCollection 2024 Oct 4.

Affiliations

¹ Manchester Institute of Biotechnology, Department of Chemistry, University of Manchester, 131 Princess Street, Manchester M1 7DN, U.K.
² Chemical Development, Pharmaceutical Technology and Development, Operations, AstraZeneca, Silk Road Business Park, Macclesfield SK10 2NA, U.K.
³ School of Chemical and Physical Sciences and Keele Centre for Glycoscience, Keele University, Keele ST5 5BG, U.K.

Abstract

Saturated N-heterocycles constitute a vital scaffold for pharmaceutical chemistry but are challenging to access synthetically, particularly asymmetrically. Here, we demonstrate how imine reductases can achieve annulation through tandem inter- and intramolecular reductive amination processes. Imine reductases were used in combination with further enzymes to access unsubstituted, α-substituted, and α,α'-disubstituted N-heterocycles from simple starting materials in one pot and under benign conditions. This work shows the remarkable flexibility of these enzymes to have broad activity against numerous substrates derived from singlular starting materials.