黑素皮质素4受体
兴奋剂
受体
食欲
细胞生物学
机制(生物学)
敌手
黑素皮质素
信号转导
黑素皮质素3受体
化学
内分泌学
内科学
生物
生物化学
黑素皮质激素受体
医学
哲学
认识论
作者
Hadar Israeli,Oksana Degtjarik,Fabrizio Fierro,Vidicha Chunilal,Amandeep Kaur Gill,Nicolas J. Roth,Joaquín Botta,Vadivel Prabahar,Yoav Peleg,Li F. Chan,Danny Ben‐Zvi,Peter J. McCormick,Masha Y. Niv,Moran Shalev-Benami
出处
期刊:Science
[American Association for the Advancement of Science]
日期:2021-04-15
卷期号:372 (6544): 808-814
被引量:92
标识
DOI:10.1126/science.abf7958
摘要
Obesity is a global epidemic that causes morbidity and impaired quality of life. The melanocortin receptor 4 (MC4R) is at the crux of appetite, energy homeostasis, and body-weight control in the central nervous system and is a prime target for anti-obesity drugs. Here, we present the cryo-electron microscopy (cryo-EM) structure of the human MC4R-Gs signaling complex bound to the agonist setmelanotide, a cyclic peptide recently approved for the treatment of obesity. The work reveals the mechanism of MC4R activation, highlighting a molecular switch that initiates satiation signaling. In addition, our findings indicate that calcium (Ca2+) is required for agonist, but not antagonist, efficacy. These results fill a gap in the understanding of MC4R activation and could guide the design of future weight-management drugs.
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