Active site model of (R)-selective ω-transaminase and its application to the production of d-amino acids

Park, Eul-Soo; Dong, Joo-Young; Shin, Jong-Shik

doi:10.1007/s00253-013-4846-5

Biotechnologically relevant enzymes and proteins
Published: 11 April 2013

Active site model of (R)-selective ω-transaminase and its application to the production of d-amino acids

Eul-Soo Park¹,
Joo-Young Dong¹ &
Jong-Shik Shin^1,2

Applied Microbiology and Biotechnology volume 98, pages 651–660 (2014)Cite this article

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28 Citations
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Abstract

ω-Transaminase (ω-TA) is one of the important biocatalytic toolkits owing to its unique enzyme property which enables the transfer of an amino group between primary amines and carbonyl compounds. In addition to preparation of chiral amines, ω-TA reactions have been exploited for the asymmetric synthesis of l-amino acids using (S)-selective ω-TAs. However, despite the availability of (R)-selective ω-TAs, catalytic utility of the ω-TAs has not been explored for the production of d-amino acids. Here, we investigated the substrate specificity of (R)-selective ω-TAs from Aspergillus terreus and Aspergillus fumigatus and demonstrated the asymmetric synthesis of d-amino acids from α-keto acids. Substrate specificity toward d-amino acids and α-keto acids revealed that the two (R)-selective ω-TAs possess strict steric constraints in the small binding pocket that precludes the entry of a substituent larger than an ethyl group, which is reminiscent of (S)-selective ω-TAs. Molecular models of the active site bound to an external aldimine were constructed and used to explain the observed substrate specificity and stereoselectivity. α-Methylbenzylamine (α-MBA) showed the highest amino donor reactivity among five primary amines (benzylamine, α-MBA, α-ethylbenzylamine, 1-aminoindan, and isopropylamine), leading us to employ α-MBA as an amino donor for the amination of 5 reactive α-keto acids (pyruvate, 2-oxobutyrate, fluoropyruvate, hydroxypyruvate, and 2-oxopentanoate) among 17 ones tested. Unlike the previously characterized (S)-selective ω-TAs, the enzyme activity of the (R)-selective ω-TAs was not inhibited by acetophenone (i.e., a deamination product of α-MBA). Using racemic α-MBA as an amino donor, five d-amino acids (d-alanine, d-homoalanine, d-fluoroalanine, d-serine, and d-norvaline) were synthesized with excellent product enantiopurity (enantiomeric excess >99.7 %).

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Acknowledgments

This work was supported by the Advanced Biomass R&D Center (ABC-2010-0029737) and the Basic Science Research Program (2010–0024448) through the National Research Foundation of Korea funded by the Ministry of Education, Science and Technology.

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Department of Biotechnology, Yonsei University, 262 Seongsanno, Seodaemun-gu, Seoul, 120-749, South Korea
Eul-Soo Park, Joo-Young Dong & Jong-Shik Shin
Yonsei University, Engineering Building 2 (Rm 507), 262 Seongsanno, Seodaemun-gu, Seoul, 120-749, South Korea
Jong-Shik Shin

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Eul-Soo Park
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Joo-Young Dong
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Jong-Shik Shin
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Correspondence to Jong-Shik Shin.

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Park, ES., Dong, JY. & Shin, JS. Active site model of (R)-selective ω-transaminase and its application to the production of d-amino acids. Appl Microbiol Biotechnol 98, 651–660 (2014). https://doi.org/10.1007/s00253-013-4846-5

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Received: 03 December 2012
Revised: 05 March 2013
Accepted: 08 March 2013
Published: 11 April 2013
Issue Date: January 2014
DOI: https://doi.org/10.1007/s00253-013-4846-5

Keywords

ω-Transaminase
d-Amino acid
Substrate specificity
Asymmetric synthesis
Active site model