Discovery and optimization of a novel series of N-arylamide oxadiazoles as potent, highly selective and orally bioavailable cannabinoid receptor 2 (CB2) agonists |
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| Authors: | Cheng Yuan Albrecht Brian K Brown James Buchanan John L Buckner William H DiMauro Erin F Emkey Renee Fremeau Robert T Harmange Jean-Christophe Hoffman Beth J Huang Liyue Huang Ming Lee Josie Han Lin Fen-Fen Martin Matthew W Nguyen Hung Q Patel Vinod F Tomlinson Susan A White Ryan D Xia Xiaoyang Hitchcock Stephen A |
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| Affiliation: | Chemistry Research and Discovery, Amgen Inc., One Amgen Center Drive, Thousand Oaks, California 91320, USA. yuanc@amgen.com |
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| Abstract: | The CB2 receptor is an attractive therapeutic target for analgesic and anti-inflammatory agents. Herein we describe the discovery of a novel class of oxadiazole derivatives from which potent and selective CB2 agonist leads were developed. Initial hit 7 was identified from a cannabinoid target-biased library generated by virtual screening of sample collections using a pharmacophore model in combination with a series of physicochemical filters. 7 was demonstrated to be a selective CB2 agonist (CB2 EC50 = 93 nM, Emax = 98%, CB1 EC50 > 10 microM). However, this compound exhibited poor solubility and relatively high clearance in rat, resulting in low oral bioavailability. In this paper, we report detailed SAR studies on 7 en route toward improving potency, physicochemical properties, and solubility. This effort resulted in identification of 63 that is a potent and selective agonist at CB2 (EC50 = 2 nM, Emax = 110%) with excellent pharmacokinetic properties. |
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