Biocatalysis in Drug Design: Engineered Reductive Aminases (RedAms) Are Used to Access Chiral Building Blocks with Multiple Stereocenters

Arnau Rué Casamajo; Yuqi Yu; Christian Schnepel; Charlotte Morrill; Rhys Barker; Colin W Levy; James Finnigan; Victor Spelling; Kristina Westerlund; Mark Petchey; Robert J Sheppard; Richard J Lewis; Francesco Falcioni; Martin A Hayes; Nicholas J Turner

doi:10.1021/jacs.3c07010

Biocatalysis in Drug Design: Engineered Reductive Aminases (RedAms) Are Used to Access Chiral Building Blocks with Multiple Stereocenters

Arnau Rué Casamajo, Yuqi Yu, Christian Schnepel, Charlotte Morrill, Rhys Barker, Colin W Levy, James Finnigan, Victor Spelling, Kristina Westerlund, Mark Petchey, Robert J Sheppard, Richard J Lewis, Francesco Falcioni, Martin A Hayes, Nicholas J Turner

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

Abstract

Novel building blocks are in constant demand during the search for innovative bioactive small molecule therapeutics by enabling the construction of structure-activity-property-toxicology relationships. Complex chiral molecules containing multiple stereocenters are an important component in compound library expansion but can be difficult to access by traditional organic synthesis. Herein, we report a biocatalytic process to access a specific diastereomer of a chiral amine building block used in drug discovery. A reductive aminase (RedAm) was engineered following a structure-guided mutagenesis strategy to produce the desired isomer. The engineered RedAm (IR-09 W204R) was able to generate the (S,S,S)-isomer 3 in 45% conversion and 95% ee from the racemic ketone 2. Subsequent palladium-catalyzed deallylation of 3 yielded the target primary amine 4 in a 73% yield. This engineered biocatalyst was used at preparative scale and represents a potential starting point for further engineering and process development.

Original language	English
Pages (from-to)	22041-22046
Number of pages	6
Journal	Journal of the American Chemical Society
Volume	145
Issue number	40
Early online date	2 Oct 2023
DOIs	https://doi.org/10.1021/jacs.3c07010
Publication status	Published - 11 Oct 2023

Keywords

Biocatalysis
Amines
Stereoisomerism
Drug Design

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Casamajo, A. R., Yu, Y., Schnepel, C., Morrill, C., Barker, R., Levy, C. W., Finnigan, J., Spelling, V., Westerlund, K., Petchey, M., Sheppard, R. J., Lewis, R. J., Falcioni, F., Hayes, M. A., & Turner, N. J. (2023). Biocatalysis in Drug Design: Engineered Reductive Aminases (RedAms) Are Used to Access Chiral Building Blocks with Multiple Stereocenters. Journal of the American Chemical Society, 145(40), 22041-22046. https://doi.org/10.1021/jacs.3c07010

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abstract = "Novel building blocks are in constant demand during the search for innovative bioactive small molecule therapeutics by enabling the construction of structure-activity-property-toxicology relationships. Complex chiral molecules containing multiple stereocenters are an important component in compound library expansion but can be difficult to access by traditional organic synthesis. Herein, we report a biocatalytic process to access a specific diastereomer of a chiral amine building block used in drug discovery. A reductive aminase (RedAm) was engineered following a structure-guided mutagenesis strategy to produce the desired isomer. The engineered RedAm (IR-09 W204R) was able to generate the (S,S,S)-isomer 3 in 45% conversion and 95% ee from the racemic ketone 2. Subsequent palladium-catalyzed deallylation of 3 yielded the target primary amine 4 in a 73% yield. This engineered biocatalyst was used at preparative scale and represents a potential starting point for further engineering and process development.",

keywords = "Biocatalysis, Amines, Stereoisomerism, Drug Design",

author = "Casamajo, {Arnau Ru{\'e}} and Yuqi Yu and Christian Schnepel and Charlotte Morrill and Rhys Barker and Levy, {Colin W} and James Finnigan and Victor Spelling and Kristina Westerlund and Mark Petchey and Sheppard, {Robert J} and Lewis, {Richard J} and Francesco Falcioni and Hayes, {Martin A} and Turner, {Nicholas J}",

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Casamajo, AR, Yu, Y, Schnepel, C, Morrill, C, Barker, R, Levy, CW, Finnigan, J, Spelling, V, Westerlund, K, Petchey, M, Sheppard, RJ, Lewis, RJ, Falcioni, F, Hayes, MA & Turner, NJ 2023, 'Biocatalysis in Drug Design: Engineered Reductive Aminases (RedAms) Are Used to Access Chiral Building Blocks with Multiple Stereocenters', Journal of the American Chemical Society, vol. 145, no. 40, pp. 22041-22046. https://doi.org/10.1021/jacs.3c07010

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AU - Yu, Yuqi

AU - Schnepel, Christian

AU - Morrill, Charlotte

AU - Barker, Rhys

AU - Levy, Colin W

AU - Finnigan, James

AU - Spelling, Victor

AU - Westerlund, Kristina

AU - Petchey, Mark

AU - Sheppard, Robert J

AU - Lewis, Richard J

AU - Falcioni, Francesco

AU - Hayes, Martin A

AU - Turner, Nicholas J

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Biocatalysis in Drug Design: Engineered Reductive Aminases (RedAms) Are Used to Access Chiral Building Blocks with Multiple Stereocenters

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