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A POMC variant implicates beta-melanocyte-stimulating hormone in the control of human energy balance
Authors:Lee Yung Seng  Challis Ben G  Thompson Darren A  Yeo Giles S H  Keogh Julia M  Madonna Michael E  Wraight Vicki  Sims Matthew  Vatin Vincent  Meyre David  Shield Julian  Burren Christine  Ibrahim Zala  Cheetham Tim  Swift Peter  Blackwood Anthea  Hung Chiao-Chien Connie  Wareham Nicholas J  Froguel Philippe  Millhauser Glenn L  O'Rahilly Stephen  Farooqi I Sadaf
Affiliation:University Department of Clinical Biochemistry, Cambridge Institute for Medical Research, Addenbrooke's Hospital, Cambridge, CB2 2XY, United Kingdom.
Abstract:The melanocortin-4 receptor (MC4R) plays a critical role in the control of energy balance. Of its two pro-opiomelanocortin (POMC)-derived ligands, alpha- and beta-MSH, the majority of attention has focused on alpha-MSH, partly reflecting the absence of beta-MSH in rodents. We screened the POMC gene in 538 patients with severe, early-onset obesity and identified five unrelated probands who were heterozygous for a rare missense variant in the region encoding beta-MSH, Tyr221Cys. This frequency was significantly increased (p < 0.001) compared to the general UK Caucasian population and the variant cosegregated with obesity/overweight in affected family members. Compared to wild-type beta-MSH, the variant peptide was impaired in its ability to bind to and activate signaling from the MC4R. Obese children carrying the Tyr221Cys variant were hyperphagic and showed increased linear growth, both of which are features of MC4R deficiency. These studies support a role for beta-MSH in the control of human energy homeostasis.
Keywords:MOLNEURO   HUMDISEASE
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