The melanocortin-4 receptor (MC4R), a centrally expressed G protein-coupled receptor (GPCR), is essential for the maintenance of long-term energy balance in humans. Mutations in MC4R are the most common genetic cause of obesity. Since activation of this receptor leads to a decrease in food intake, MC4R is also a major therapeutic target for the treatment of obesity. Control of MC4R activity in vivo is modulated by the opposing effects of the anorexigenic agonist alpha-melanocyte-stimulating hormone (alpha-MSH) and the orexigenic antagonist agouti-related protein (AGRP). In addition, experiments in vitro have demonstrated that the human MC4R has an intrinsic constitutive activity on which AGRP also acts as an inverse agonist. The physiological role of this constitutive activity in the control of energy balance as well as the domain of the protein implicated in its maintenance are unknown. By systematically studying functional defects in naturally occurring MC4R mutations from obese patients, we defined a cluster of N-terminal mutations that selectively impair the constitutive activity of the receptor. Further characterization of this domain demonstrated that it functions as a tethered intramolecular ligand that maintains the constitutive activity of MC4R and may provide novel avenues for the design of drugs targeting this receptor. Our results also suggest that the tonic satiety signal provided by the constitutive activity of MC4R may be required for maintaining long-term energy homeostasis in humans.
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机译:黑皮质素-4 受体 (MC4R) 是一种中枢表达的 G 蛋白偶联受体 (GPCR),对于维持人类的长期能量平衡至关重要。MC4R突变是肥胖最常见的遗传原因。由于该受体的激活导致食物摄入量减少,MC4R也是治疗肥胖症的主要治疗靶点。体内MC4R活性的控制受厌食激动剂α-黑素细胞刺激素(α-MSH)和促食欲拮抗剂刺鼠相关蛋白(AGRP)的相反作用的调节。此外,体外实验表明,人MC4R具有内在的组成型活性,AGRP也作为反向激动剂。这种组成活性在控制能量平衡中的生理作用以及与其维持有关的蛋白质结构域尚不清楚。通过系统地研究肥胖患者自然发生的 MC4R 突变的功能缺陷,我们定义了一组选择性损害受体组成型活性的 N 端突变。该结构域的进一步表征表明,它作为一种拴系的分子内配体发挥作用,可维持MC4R的组成型活性,并可能为靶向该受体的药物设计提供新的途径。我们的研究结果还表明,MC4R的组成活性提供的强直饱腹感信号可能是维持人类长期能量稳态所必需的。
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