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Identification of novel muscarinic M(3) selective antagonists with a conformationally restricted Hyp-Pro spacer
Authors:Sagara Yufu  Kimura Toshifumi  Fujikawa Toru  Noguchi Kazuhito  Ohtake Norikazu
Affiliation:Banyu Tsukuba Research Institute in collaboration with Merck Research Laboratories, Okubo-3, Ibaraki, Japan. oowadayf@banyu.co.jp
Abstract:The identification of potent and selective muscarinic M(3) antagonists that are based on the recently discovered triphenylpropioamide derivative, 1, and have a unique amino acid spacer group is described. The introduction of a hydroxyproline-proline group to the spacer site and the use of a propyl or cyclopropylmethyl group as the piperidine N-substituent led to the discovery of the novel M(3) selective antagonists [8c, 8g; K(i)<2 nM (M(3)), M(1)/M(3)>700-fold, M(2)/M(3)>180-fold], which have a more rigid structure than 1.
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