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  • Inactivation of the mouse melanocortin-3 receptor results in increased fat mass and reduced lean body mass.

Inactivation of the mouse melanocortin-3 receptor results in increased fat mass and reduced lean body mass.

Nature genetics (2000-09-06)
A S Chen, D J Marsh, M E Trumbauer, E G Frazier, X M Guan, H Yu, C I Rosenblum, A Vongs, Y Feng, L Cao, J M Metzger, A M Strack, R E Camacho, T N Mellin, C N Nunes, W Min, J Fisher, S Gopal-Truter, D E MacIntyre, H Y Chen, L H Van der Ploeg
RESUMO

Genetic and pharmacological studies have defined a role for the melanocortin-4 receptor (Mc4r) in the regulation of energy homeostasis. The physiological function of Mc3r, a melanocortin receptor expressed at high levels in the hypothalamus, has remained unknown. We evaluated the potential role of Mc3r in energy homeostasis by studying Mc3r-deficient (Mc3r(-/-)) mice and compared the functions of Mc3r and Mc4r in mice deficient for both genes. The 4-6-month Mc3r-/- mice have increased fat mass, reduced lean mass and higher feed efficiency than wild-type littermates, despite being hypophagic and maintaining normal metabolic rates. (Feed efficiency is the ratio of weight gain to food intake.) Consistent with increased fat mass, Mc3r(-/-) mice are hyperleptinaemic and male Mc3r(-/-) mice develop mild hyperinsulinaemia. Mc3r(-/-) mice did not have significantly altered corticosterone or total thyroxine (T4) levels. Mice lacking both Mc3r and Mc4r become significantly heavier than Mc4r(-/-) mice. We conclude that Mc3r and Mc4r serve non-redundant roles in the regulation of energy homeostasis.