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Optimization of imidazole amide derivatives as cannabinoid-1 receptor antagonists for the treatment of obesity
Authors:Smith Roger A  Fathi Zahra  Achebe Furahi  Akuche Christiana  Brown Su-Ellen  Choi Soongyu  Fan Jianmei  Jenkins Susan  Kluender Harold C E  Konkar Anish  Lavoie Rico  Mays Ronald  Natoli Jennifer  O'Connor Stephen J  Ortiz Astrid A  Su Ning  Taing Christy  Tomlinson Susan  Tritto Theresa  Wang Gan  Wirtz Stephan-Nicholas  Wong Wai  Yang Xiao-Fan  Ying Shihong  Zhang Zhonghua
Affiliation:Department of Chemistry Research, Bayer HealthCare, Pharmaceuticals Division, West Haven, CT 06516, USA. rosmith@angio.com
Abstract:Several imidazole-based cyclohexyl amides were identified as potent CB-1 antagonists, but they exhibited poor oral exposure in rodents. Incorporation of a hydroxyl moiety on the cyclohexyl ring provided a dramatic improvement in oral exposure, together with a ca. 10-fold decrease in potency. Further optimization provided the imidazole 2-hydroxy-cyclohexyl amide 45, which exhibited hCB-1 K(i)=3.7nM, and caused significant appetite suppression and robust, dose-dependent reduction of body weight gain in industry-standard rat models.
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