Enantioselective, biocatalytic reduction of 3-substituted cyclopentenones: application to the asymmetric synthesis of an hNK-1 receptor antagonist.

Kevin R Campos Artis Klapars Yoshinori Kohmura David Pollard Hideaki Ishibashi Shinji Kato Akihiro Takezawa Jacob H Waldman Debra J Wallace Cheng-yi Chen Nobuyoshi Yasuda

Org Lett

Department of Process Chemistry, Merck Research Laboratories, Rahway, New Jersey 07065, USA.

Published: March 2011

A convergent and enantioselective route to the hNK-1 receptor antagonist (1) is described, which sets all six stereogenic centers with high diastereoselectivity and delivers 1 in only 11 steps and 23% overall yield. The process was enabled by the development of the enantioselective enzymatic reduction of 3-functionalized cyclopentenones and stereospecific Pd-catalyzed etherification coupling of fragments 6 and 7.

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http://dx.doi.org/10.1021/ol1030348	DOI Listing

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