Structure of the human glucagon class B G-protein-coupled receptor

被引:0
|
作者
Fai Yiu Siu
Min He
Chris de Graaf
Gye Won Han
Dehua Yang
Zhiyun Zhang
Caihong Zhou
Qingping Xu
Daniel Wacker
Jeremiah S. Joseph
Wei Liu
Jesper Lau
Vadim Cherezov
Vsevolod Katritch
Ming-Wei Wang
Raymond C. Stevens
机构
[1] The Scripps Research Institute,Department of Integrative Structural and Computational Biology
[2] 10550 North Torrey Pines Road,Division of Medicinal Chemistry
[3] La Jolla,undefined
[4] California 92037,undefined
[5] USA,undefined
[6] The National Center for Drug Screening and the CAS Key Laboratory of Receptor Research,undefined
[7] Shanghai Institute of Materia Medica,undefined
[8] Chinese Academy of Sciences (CAS),undefined
[9] 189 Guo Shou Jing Road,undefined
[10] Shanghai,undefined
[11] 201203,undefined
[12] China,undefined
[13] Faculty of Sciences,undefined
[14] Amsterdam Institute for Molecules,undefined
[15] Medicines and Systems (AIMMS),undefined
[16] VU University of Amsterdam,undefined
[17] De Boelelaan 1083,undefined
[18] 1081 HV Amsterdam,undefined
[19] The Netherlands,undefined
[20] The Joint Center for Structural Genomics,undefined
[21] Stanford Synchrotron Radiation Lightsource,undefined
[22] SLAC National Accelerator Laboratory,undefined
[23] Menlo Park,undefined
[24] California 94025,undefined
[25] USA,undefined
[26] Protein & Peptide Chemistry,undefined
[27] Novo Nordisk,undefined
[28] Novo Nordisk Park,undefined
[29] 2760 Malov,undefined
[30] Denmark,undefined
来源
Nature | 2013年 / 499卷
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摘要
Binding of the glucagon peptide to the glucagon receptor (GCGR) triggers the release of glucose from the liver during fasting; thus GCGR plays an important role in glucose homeostasis. Here we report the crystal structure of the seven transmembrane helical domain of human GCGR at 3.4 Å resolution, complemented by extensive site-specific mutagenesis, and a hybrid model of glucagon bound to GCGR to understand the molecular recognition of the receptor for its native ligand. Beyond the shared seven transmembrane fold, the GCGR transmembrane domain deviates from class A G-protein-coupled receptors with a large ligand-binding pocket and the first transmembrane helix having a ‘stalk’ region that extends three alpha-helical turns above the plane of the membrane. The stalk positions the extracellular domain (∼12 kilodaltons) relative to the membrane to form the glucagon-binding site that captures the peptide and facilitates the insertion of glucagon’s amino terminus into the seven transmembrane domain.
引用
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页码:444 / 449
页数:5
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