| Literature DB >> 17125262 |
Francis X Tavares1, Kamal A Al-Barazanji, Eric C Bigham, Michael J Bishop, Christy S Britt, David L Carlton, Paul L Feldman, Aaron S Goetz, Mary K Grizzle, Yu C Guo, Anthony L Handlon, Donald L Hertzog, Diane M Ignar, Daniel G Lang, Ronda J Ott, Andrew J Peat, Hui-Qiang Zhou.
Abstract
The high expression of MCH in the hypothalamus with the lean hypophagic phenotype coupled with increased resting metabolic rate and resistance to high fat diet-induced obesity of MCH KO mice has spurred considerable efforts to develop small molecule MCHR1 antagonists. Starting from a lead thienopyrimidinone series, structure-activity studies at the 3- and 6-positions of the thienopyrimidinone core afforded potent and selective MCHR1 antagonists with representative examples having suitable pharmacokinetic properties. Based on structure-activity relationships, a structural model for MCHR1 was constructed to explain the binding mode of these antagonists. In general, a good correlation was observed between pKas and activity in the right-hand side of the template, with Asp123 playing an important role in the enhancement of binding affinity. A representative example when evaluated chronically in diet-induced obese mice resulted in good weight loss effects. These antagonists provide a viable lead series in the discovery of new therapies for the treatment of obesity.Entities:
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Year: 2006 PMID: 17125262 DOI: 10.1021/jm060572f
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446