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人钙敏感受体中配体激活的结构机制

Structural mechanism of ligand activation in human calcium-sensing receptor.

作者信息

Geng Yong, Mosyak Lidia, Kurinov Igor, Zuo Hao, Sturchler Emmanuel, Cheng Tat Cheung, Subramanyam Prakash, Brown Alice P, Brennan Sarah C, Mun Hee-Chang, Bush Martin, Chen Yan, Nguyen Trang X, Cao Baohua, Chang Donald D, Quick Matthias, Conigrave Arthur D, Colecraft Henry M, McDonald Patricia, Fan Qing R

机构信息

Department of Pharmacology, Columbia University, New York, United States.

Shanghai Institute of Materia Medica, Chinese Academy of Sciences, Shanghai, China.

出版信息

Elife. 2016 Jul 19;5:e13662. doi: 10.7554/eLife.13662.

Abstract

Human calcium-sensing receptor (CaSR) is a G-protein-coupled receptor (GPCR) that maintains extracellular Ca(2+) homeostasis through the regulation of parathyroid hormone secretion. It functions as a disulfide-tethered homodimer composed of three main domains, the Venus Flytrap module, cysteine-rich domain, and seven-helix transmembrane region. Here, we present the crystal structures of the entire extracellular domain of CaSR in the resting and active conformations. We provide direct evidence that L-amino acids are agonists of the receptor. In the active structure, L-Trp occupies the orthosteric agonist-binding site at the interdomain cleft and is primarily responsible for inducing extracellular domain closure to initiate receptor activation. Our structures reveal multiple binding sites for Ca(2+) and PO4(3-) ions. Both ions are crucial for structural integrity of the receptor. While Ca(2+) ions stabilize the active state, PO4(3-) ions reinforce the inactive conformation. The activation mechanism of CaSR involves the formation of a novel dimer interface between subunits.

摘要

人类钙敏感受体(CaSR)是一种G蛋白偶联受体(GPCR),通过调节甲状旁腺激素分泌来维持细胞外Ca(2+) 稳态。它作为一个由三个主要结构域组成的二硫键连接的同型二聚体发挥作用,这三个结构域分别是捕蝇草模块、富含半胱氨酸结构域和七螺旋跨膜区域。在此,我们展示了处于静息和活性构象的CaSR整个细胞外结构域的晶体结构。我们提供了直接证据表明L-氨基酸是该受体的激动剂。在活性结构中,L-色氨酸占据结构域间裂隙处的正构激动剂结合位点,并主要负责诱导细胞外结构域闭合以启动受体激活。我们的结构揭示了Ca(2+) 和PO4(3-) 离子的多个结合位点。这两种离子对于受体的结构完整性都至关重要。虽然Ca(2+) 离子稳定活性状态,但PO4(3-) 离子加强非活性构象。CaSR的激活机制涉及亚基之间形成一个新的二聚体界面。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6a49/4977154/cdcf76b47cd0/elife-13662-fig1.jpg

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