Crystal structures of the human adiponectin receptors

被引:0
|
作者
Hiroaki Tanabe
Yoshifumi Fujii
Miki Okada-Iwabu
Masato Iwabu
Yoshihiro Nakamura
Toshiaki Hosaka
Kanna Motoyama
Mariko Ikeda
Motoaki Wakiyama
Takaho Terada
Noboru Ohsawa
Masakatsu Hato
Satoshi Ogasawara
Tomoya Hino
Takeshi Murata
So Iwata
Kunio Hirata
Yoshiaki Kawano
Masaki Yamamoto
Tomomi Kimura-Someya
Mikako Shirouzu
Toshimasa Yamauchi
Takashi Kadowaki
Shigeyuki Yokoyama
机构
[1] RIKEN Systems and Structural Biology Center,Department of Biophysics and Biochemistry and Laboratory of Structural Biology
[2] Graduate School of Science,Division of Structural and Synthetic Biology
[3] The University of Tokyo,Department of Diabetes and Metabolic Diseases
[4] RIKEN Center for Life Science Technologies,Department of Integrated Molecular Science on Metabolic Diseases
[5] RIKEN Structural Biology Laboratory,Department of Cell Biology
[6] Graduate School of Medicine,Department of Chemistry
[7] The University of Tokyo,Division of Molecular Biosciences
[8] 22nd Century Medical and Research Center,undefined
[9] The University of Tokyo,undefined
[10] PRESTO,undefined
[11] Japan Science and Technology Agency,undefined
[12] Graduate School of Medicine,undefined
[13] Kyoto University,undefined
[14] JST,undefined
[15] Research Acceleration Program,undefined
[16] Membrane Protein Crystallography Project,undefined
[17] Graduate School of Science,undefined
[18] Chiba University,undefined
[19] Membrane Protein Crystallography Group,undefined
[20] Imperial College,undefined
[21] Diamond Light Source,undefined
[22] Harwell Science and Innovation Campus,undefined
[23] RIKEN SPring-8 Center,undefined
[24] Harima Institute,undefined
[25] CREST,undefined
[26] Japan Science and Technology Agency,undefined
来源
Nature | 2015年 / 520卷
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摘要
Adiponectin stimulation of its receptors, AdipoR1 and AdipoR2, increases the activities of 5′ AMP-activated protein kinase (AMPK) and peroxisome proliferator-activated receptor (PPAR), respectively, thereby contributing to healthy longevity as key anti-diabetic molecules. AdipoR1 and AdipoR2 were predicted to contain seven transmembrane helices with the opposite topology to G-protein-coupled receptors. Here we report the crystal structures of human AdipoR1 and AdipoR2 at 2.9 and 2.4 Å resolution, respectively, which represent a novel class of receptor structure. The seven-transmembrane helices, conformationally distinct from those of G-protein-coupled receptors, enclose a large cavity where three conserved histidine residues coordinate a zinc ion. The zinc-binding structure may have a role in the adiponectin-stimulated AMPK phosphorylation and UCP2 upregulation. Adiponectin may broadly interact with the extracellular face, rather than the carboxy-terminal tail, of the receptors. The present information will facilitate the understanding of novel structure–function relationships and the development and optimization of AdipoR agonists for the treatment of obesity-related diseases, such as type 2 diabetes.
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页码:312 / 316
页数:4
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