新型烯基噻吩作为强效和选择性CB1大麻素受体拮抗剂的设计、合成及生物学评价
Design, synthesis, and biological evaluation of novel alkenylthiophenes as potent and selective CB1 cannabinoid receptor antagonists.
作者信息
Tai Chia-Liang, Hung Ming-Shiu, Pawar Vijay D, Tseng Shi-Liang, Song Jen-Shin, Hsieh Wan-Ping, Chiu Hua-Hao, Wu Hui-Chuan, Hsieh Min-Tsang, Kuo Chun-Wei, Hsieh Chia-Chien, Tsao Jing-Po, Chao Yu-Sheng, Shia Kak-Shan
机构信息
Division of Biotechnology and Pharmaceutical Research, National Health Research Institutes, Miaoli County 350, Taiwan, Republic of China.
出版信息
Org Biomol Chem. 2008 Feb 7;6(3):447-50. doi: 10.1039/b716434c. Epub 2007 Dec 10.
A novel class of (5-(pent-1-enyl)thiophen-2-yl)pyrazole antagonists was discovered, many of which exhibited potent CB1 activity and good CB1/2 selectivity, suggesting that along with a 1,3-transposition of the carbonyl of the pyrazole 3-carboxamide, bioisosteric replacement of the conventional pyrazole 5-aryl group with a thienyl ring substituted with an appropriate alkenyl moiety is viable.
发现了一类新型的(5-(戊-1-烯基)噻吩-2-基)吡唑拮抗剂,其中许多表现出强效的CB1活性和良好的CB1/2选择性,这表明除了吡唑3-甲酰胺羰基的1,3-位转移外,用适当烯基部分取代的噻吩环对传统吡唑5-芳基进行生物电子等排体取代是可行的。
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