Author/Authors :
Fabio C. Tucci، نويسنده , , Nicole S. White، نويسنده , , Stacy Markison، نويسنده , , Margaret Joppa، نويسنده , , Joe A. Tran، نويسنده , , Beth A. Fleck، نويسنده , , Ajay Madan، نويسنده , , Brian P. Dyck، نويسنده , , Jessica Parker، نويسنده , , Joseph Pontillo، نويسنده , , L. Melissa Arellano، نويسنده , , Dragan Marinkovic، نويسنده , , Wanlong Jiang، نويسنده , , Caroline W. Chen، نويسنده , , Kathleen R. Gogas، نويسنده , , Val S. Goodfellow، نويسنده , , John Saunders، نويسنده , , Alan C. Foster، نويسنده , , Chen Chen، نويسنده ,
Abstract :
The melanocortin-4 receptor (MC4R) plays an important role in the regulation of energy homeostasis. Recent studies have shown that blockade of the MC4R reverses tumor-induced weight loss in mice. Herein, we describe the synthesis and identification of potent and selective non-peptide antagonists of the human MC4R from a series of 2-ethoxycarbonylcyclohexyl-piperazines. Compound 12i was found to possess low nanomolar affinity for the MC4R, and exhibit oral bioavailability in rats. More importantly, when administered orally to mice (10 mg/kg), it led to statistically significant increases in food intake over a 24-h period.
Keywords :
GPCR , Antagonists , food intake , Melanocortin-4 receptor , SAR
