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

Research output: Contribution to journal › Article › peer-review

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.

Original language	English
Pages (from-to)	188-198
Number of pages	11
Journal	Organic and Biomolecular Chemistry
Volume	19
Issue number	1
DOIs	https://doi.org/10.1039/d0ob01848a
Publication status	Published - 7 Jan 2021

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10.1039/d0ob01848a

https://hdl.handle.net/10468/11423Licence: CC BY-NC-ND

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title = "Exploring the synthetic potential of a marine transaminase including discrimination at a remote stereocentre",

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.",

author = "Maria Schwarz and Murphy, \{Edel J.\} and Foley, \{Aoife M.\} and Woods, \{David F.\} and Castilla, \{Ignacio Abreu\} and Reen, \{F. Jerry\} and Collins, \{Stuart G.\} and Fergal O'gara and Maguire, \{Anita R.\}",

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doi = "10.1039/d0ob01848a",

language = "English",

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T1 - Exploring the synthetic potential of a marine transaminase including discrimination at a remote stereocentre

AU - Schwarz, Maria

AU - Murphy, Edel J.

AU - Foley, Aoife M.

AU - Woods, David F.

AU - Castilla, Ignacio Abreu

AU - Reen, F. Jerry

AU - Collins, Stuart G.

AU - O'gara, Fergal

AU - Maguire, Anita R.

PY - 2021/1/7

Y1 - 2021/1/7

N2 - 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.

AB - 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.

UR - https://www.scopus.com/pages/publications/85099241061

U2 - 10.1039/d0ob01848a

DO - 10.1039/d0ob01848a

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AN - SCOPUS:85099241061

SN - 1477-0520

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SP - 188

EP - 198

JO - Organic and Biomolecular Chemistry

JF - Organic and Biomolecular Chemistry

IS - 1

ER -

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

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