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SAR studies of C2 ethers of 2H-pyrano[2,3-d]pyrimidine-2,4,7(1H,3H)-triones as nicotinic acid receptor (NAR) agonist
Authors:Huang Xianhai  Su Jing  Rao Ashwin U  Tang Haiqun  Zhou Wei  Zhu Xiaohong  Chen Xiao  Liu Zhidan  Huang Ying  Degrado Sylvia  Xiao Dong  Qin Jun  Aslanian Robert  McKittrick Brian A  Greenfeder Scott  Heek Margaret van  Chintala Madhu  Palani Anandan
Affiliation:Department of Chemical Research, Merck Research Laboratory, 2015 Galloping Hill Road, Kenilworth, NJ 07033, USA. xianhai.huang@merck.com
Abstract:Based on in house screening lead compound 1 for the NAR project, SAR studies have been focused on the modification of the C2 ethers of the pyrimidinedione core structure. In this effort, an unpredictable SAR trend was overcome in the alkyl ether and arylalkyl ether series to identify compound 24 with improved in vitro activity compared to nicotinic acid. More consistent and predictable SAR was achieved in the propargyl ether series. Lead compound 41 was identified with good in vitro and in vivo activity in rat, and much improved rat PK profile.
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