Structure-Selectivity Relationship of a Peptide Catalyst

C. E. Jakobsche; G. Peris; S. J. Miller

doi:10.1055/s-2008-1078153

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Synfacts 2008(10): 1100-1100
DOI: 10.1055/s-2008-1078153

Organo- and Biocatalysis

Structure-Selectivity Relationship of a Peptide Catalyst

Contributor(s): Benjamin List, Frank Lay
C. E. Jakobsche, G. Peris, S. J. Miller*
Yale University, New Haven, USA

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Publication History

Publication Date:
22 September 2008 (online)

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Significance

A detailed study on the mode of action of catalyst 1 employed in asymmetric epoxidations is presented. The observed, nearly retained enantiomeric excess achieved with analogue 2 suggests that the NHBoc group is not involved in a key H-bonding interaction with the substrate. On the other hand, replacement of the amide function with an alkene 4 or a fluoroalkene 3 group leads to a significant drop in enantiomeric excess. Mechanistic insights in their mode of action are provided by the structure-dependent catalytic behavior of these isosteric peptides.