Biocatalytic, Decarboxylative Addition of Malonates to Imines,
a ”Rodionovase

R. B. Hamed; J. R. Gomez-Castellanos; A. Thalhammer; D. Harding; C. Ducho; T. D. W. Claridge; C. J. Schofield

doi:10.1055/s-0030-1260423

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Synfacts 2011(6): 0679-0679
DOI: 10.1055/s-0030-1260423

Organo- and Biocatalysis

Biocatalytic, Decarboxylative Addition of Malonates to Imines, a ”Rodionovase"

Contributor(s): Benjamin List, Ji-Woong Lee
R. B. Hamed, J. R. Gomez-Castellanos, A. Thalhammer, D. Harding, C. Ducho, T. D. W. Claridge, C. J. Schofield*
University of Oxford, UK and Assiut University, Egypt

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Publication History

Publication Date:
19 May 2011 (online)

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Significance

Enolate anions are common carbon nucleophiles in organic synthesis. Herein, the authors demonstrate a biocatalytic addition of enolates to imines to afford N-heterocycles with high diastereoselectivity by using carboxymethylproline synthases (CMPSs), which are known to use enolate intermediates. Proper substitution of residues in the reaction site, especially the oxy-anion hole, gave mutants of higher reactivity and stereoselectivity than the wild-type enzymes. Moreover, engineered CMPSs could generate both diastereomers with good stereoselectivity. Also, control experiments with enantioenriched 2 imply stereospecific enolate stabilization in the reaction site prior to the diastereoselective addition to imines.