Efficient preparation of an N-aryl β-amino acid via asymmetric hydrogenation and direct asymmetric reductive amination en route to Ezetimibe

Busscher, Guuske F.,; Cremers, Jozef G.O.,; Lange, Ben de,; Lefort, Laurent,; Matsumura, Kazuhiko,; Mottinelli, Marco,; Okamura, Yutaka,; Shimizu, Hideo,; Vries, André H.M. de,; Vries, Johannes G. de,; Wiertz, Roel W.,; Yusa, Yukinori,

Efficient preparation of an N-aryl β-amino acid via asymmetric hydrogenation and direct asymmetric reductive amination en route to Ezetimibe

Authors: Guuske F., Busscher
Jozef G.O., Cremers
Ben de, Lange
Laurent, Lefort
Kazuhiko, Matsumura
Marco, Mottinelli
Yutaka, Okamura
Hideo, Shimizu
André H.M. de, Vries
Johannes G. de, Vries
Roel W., Wiertz
Yukinori, Yusa
Publication date: 1 January 2010
Publisher
Doi

Abstract

Two routes for the preparation of an N-aryl β-amino acid, an important precursor for the cholesterol-lowering drug Ezetimibe, were investigated. The first pathway proceeds via an Rh- or Ir-catalyzed asymmetric hydrogenation of N-aryl enamine giving the desired product with up to 82% ee. The other pathway involves a direct asymmetric reductive amination (DARA) of the β-keto ester which yielded the β-amino ester in high yield and 97% ee. Subsequent copper-catalyzed N-arylation gave the target compound.