Rational protein design of ThDP-dependent enzymes-engineering stereoselectivity |
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Authors: | Gocke Dörte Walter Lydia Gauchenova Ekaterina Kolter Geraldine Knoll Michael Berthold Catrine L Schneider Gunter Pleiss Jürgen Müller Michael Pohl Martina |
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Affiliation: | Institute of Molecular Enzyme Technology, Heinrich-Heine University Düsseldorf, 52426 Jülich, Germany. |
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Abstract: | Benzoylformate decarboxylase (BFD) from Pseudomonas putida is an exceptional thiamin diphosphate-dependent enzyme, as it catalyzes the formation of (S)-2-hydroxy-1-phenylpropan-1-one from benzaldehyde and acetaldehyde. This is the only currently known S-selective reaction (92 % ee) catalyzed by this otherwise R-selective class of enzymes. Here we describe the molecular basis of the introduction of S selectivity into ThDP-dependent decarboxylases. By shaping the active site of BFD through the use of rational protein design, structural analysis, and molecular modeling, optimal steric stabilization of the acceptor aldehyde in a structural element called the S pocket was identified as the predominant interaction for adjusting stereoselectivity. Our studies revealed Leu461 as a hot spot for stereoselectivity in BFD. Exchange to alanine and glycine resulted in variants that catalyze the S-stereoselective addition of larger acceptor aldehydes, such as propanal with benzaldehyde and its derivatives-a reaction not catalyzed by the wild-type enzyme. Crystal structure analysis of the variant BFDL461A supports the modeling studies. |
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Keywords: | asymmetric synthesis biotransformations carboligation hydroxyketones site‐directed mutagenesis |
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