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Engineering the Amine Transaminase from Vibrio fluvialis towards Branched-Chain Substrates

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논문

Engineering the Amine Transaminase from Vibrio fluvialis towards Branched-Chain Substrates

학술지

ChemCatChem

저자명

Genz, Maika; Melse, Okke; Schmidt, Sandy; Vickers, Clare; Dö rr, Mark; van den Bergh, Tom; Joosten, Henk‐ Jan; Bornscheuer, Uwe T.

초록

<P><B>Abstract</B></P><P>Chiral amines are important building blocks, especially for the pharmaceutical industry. Although amine transaminases (ATAs) are versatile enzymes to synthesize chiral amines, the wildtype enzymes do not accept ketones with two large substituents next to the carbonyl functionality. Using bioinformatic tools to design a seven&#8208;site mutant library followed by high&#8208;throughput screening, we were able to identify variants of the enzyme from <I>Vibrio fluvialis</I> (VF&#8208;ATA) with a widened binding pocket, as exemplified for a range of ketones. Three variants allowed the asymmetric synthesis of 2,2&#8208;dimethyl&#8208;1&#8208;phenylpropan&#8208;1&#8208;amine&mdash;not accessible by any wildtype ATA described so far. The best variant containing four mutations (L56V, W57C, F85V, V153A) gave 100 % conversion of the ketone to yield the amine with an enantiomeric excess value >99 %, notably with preference for the (<I>R</I>)&#8208;enantiomer. In silico modeling enabled the reconstruction of the substrate binding mode to the newly evolved pocket and, hence, allowed explanation of the experimental results.</P>

발행연도

2016

ISSN

1867-3880

ISSN

1867-3899

8

20

페이지

pp.3199-3202

주제어

amines; bioinformatics; enzyme catalysis; protein engineering; transaminases

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논문; 2016-12-31

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