Exploring the synthetic potential of a marine transaminase including discrimination at a remote stereocentre

Maria Schwarz; Edel J. Murphy; Aoife M. Foley; David F. Woods; Ignacio Abreu Castilla; F. Jerry Reen; Stuart G. Collins; Fergal O'Gara; Anita R. Maguire

doi:10.1039/D0OB01848A

Exploring the synthetic potential of a marine transaminase including discrimination at a remote stereocentre†

Maria Schwarz,‡^ab Edel J. Murphy,

‡^a Aoife M. Foley,

^ab David F. Woods,^c Ignacio Abreu Castilla,^c F. Jerry Reen,^bcd Stuart G. Collins,

^ab Fergal O'Gara*^bcef and Anita R. Maguire

*^abg

Author affiliations

* Corresponding authors

^a School of Chemistry, Analytical and Biological Chemistry Research Facility, University College Cork, Cork, Ireland
E-mail: a.maguire@ucc.ie

^b Synthesis and Solid-State Pharmaceutical Centre, University College Cork, Cork, Ireland

^c BIOMERIT Research Centre; School of Microbiology, University College Cork, T12 K8AF Cork, Ireland
E-mail: f.ogara@ucc.ie

^d School of Microbiology, University College Cork, Cork, Ireland

^e Human Microbiome Programme, School of Pharmacy and Biomedical Sciences, Curtin Health Innovation Research Institute, Curtin University, Perth, WA 6102, Australia

^f Telethon Kids Institute, Perth, WA 6008, Australia

^g School of Pharmacy, University College Cork, Cork, Ireland

Abstract

The marine transaminase, P-ω-TA, can be employed for the transamination from 1-aminotetralins and 1-aminoindanes with differentiation of stereochemistry at both the site of reaction and at a remote stereocentre resulting in formation of ketone products with up to 93% ee. While 4-substituents are tolerated on the tetralin core, the presence of 3- or 8-substituents is not tolerated by the transaminase. In general P-ω-TA shows capacity for remote diastereoselectivity, although both the stereoselectivity and efficiency are dependent on the specific substrate structure. Optimum efficiency and selectivity are seen with 4-haloaryl-1-aminotetralins and 3-haloaryl-1-aminoindanes, which may be associated with the marine origin of this enzyme.

This article is part of the themed collection: Catalysis & biocatalysis in OBC

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Article information

DOI: https://doi.org/10.1039/D0OB01848A
Article type: Paper
Submitted: 07 Sep 2020
Accepted: 23 Oct 2020
First published: 23 Oct 2020

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Org. Biomol. Chem., 2021,19, 188-198

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Exploring the synthetic potential of a marine transaminase including discrimination at a remote stereocentre

M. Schwarz, E. J. Murphy, A. M. Foley, D. F. Woods, I. A. Castilla, F. J. Reen, S. G. Collins, F. O'Gara and A. R. Maguire, Org. Biomol. Chem., 2021, 19, 188 DOI: 10.1039/D0OB01848A

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Organic & Biomolecular Chemistry

Exploring the synthetic potential of a marine transaminase including discrimination at a remote stereocentre†

Abstract

Supplementary files

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Exploring the synthetic potential of a marine transaminase including discrimination at a remote stereocentre

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