Open Access
Open access
Pharmacology Research and Perspectives, volume 1, issue 1, publication number prp2.3

Evaluation of AMG 076, a potent and selective MCHR 1 antagonist, in rodent and primate obesity models

Alykhan S. Motani 1
Jian Luo 1
Lingming Liang 1
Jeffrey T Mihalic 1
Xiaoqi Chen 1
Liang Tang 1
Leping Li 1
Juan Jaen 1
Jin-Long Chen 1
Kang Dai 1
Show full list: 10 authors
Publication typeJournal Article
Publication date2013-09-17
scimago Q1
SJR0.790
CiteScore5.3
Impact factor2.9
ISSN20521707
PubMed ID:  25505557
General Pharmacology, Toxicology and Pharmaceutics
Neurology
Abstract
Melanin-concentrating hormone (MCH) regulates food intake through activation of the receptor, MCHR1. We have identified AMG 076 as an orally bioavailable potent and selective small molecule antagonist of MCHR1. In mouse models of obesity, AMG 076 caused a reduction in body weight gain in wild-type (MCHR1+/+) but not in knockout (MCHR1-/-) mice. The body weight reduction was associated with decreases in food intake and increases in energy expenditure. Importantly, we show that these MCHR1-dependent effects of AMG 076 were also reflected in improved metabolic phenotypes, increased glucose tolerance and insulin sensitivity. Preliminary data on effects of AMG 076 in obese cynomolgus monkeys are also presented.
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