EMDB/PDB/SASBDBから引用されている文献のデータベース

キーワード
構造解析手法	All X線回折 NMR 電子顕微鏡小角散乱中性子線回折線維回折粉末回折赤外分光 EPR FRET 理論モデルハイブリッド
著者・登録者
ジャーナル
IF	>30 >20 >10 >5 all

タイトル	Tethered peptide activation mechanism of the adhesion GPCRs ADGRG2 and ADGRG4.
ジャーナル・号・ページ	Nature, Vol. 604, Issue 7907, Page 771-778, Year 2022
掲載日	2022年4月13日
著者	Peng Xiao / Shengchao Guo / Xin Wen / Qing-Tao He / Hui Lin / Shen-Ming Huang / Lu Gou / Chao Zhang / Zhao Yang / Ya-Ni Zhong / Chuan-Cheng Yang / Yu Li / Zheng Gong / Xiao-Na Tao / Zhi-Shuai Yang / Yan Lu / Shao-Long Li / Jun-Yan He / Chuanxin Wang / Lei Zhang / Liangliang Kong / Jin-Peng Sun / Xiao Yu /
PubMed 要旨	Adhesion G protein-coupled receptors (aGPCRs) constitute an evolutionarily ancient family of receptors that often undergo autoproteolysis to produce α and β subunits. A tethered agonism mediated by ...Adhesion G protein-coupled receptors (aGPCRs) constitute an evolutionarily ancient family of receptors that often undergo autoproteolysis to produce α and β subunits. A tethered agonism mediated by the 'Stachel sequence' of the β subunit has been proposed to have central roles in aGPCR activation. Here we present three cryo-electron microscopy structures of aGPCRs coupled to the G heterotrimer. Two of these aGPCRs are activated by tethered Stachel sequences-the ADGRG2-β-G complex and the ADGRG4-β-G complex (in which β indicates the β subunit of the aGPCR)-and the other is the full-length ADGRG2 in complex with the exogenous ADGRG2 Stachel-sequence-derived peptide agonist IP15 (ADGRG2(FL)-IP15-G). The Stachel sequences of both ADGRG2-β and ADGRG4-β assume a U shape and insert deeply into the seven-transmembrane bundles. Constituting the FXφφφXφ motif (in which φ represents a hydrophobic residue), five residues of ADGRG2-β or ADGRG4-β extend like fingers to mediate binding to the seven-transmembrane domain and activation of the receptor. The structure of the ADGRG2(FL)-IP15-G complex reveals the structural basis for the improved binding affinity of IP15 compared with VPM-p15 and indicates that rational design of peptidic agonists could be achieved by exploiting aGPCR-β structures. By converting the 'finger residues' to acidic residues, we develop a method to generate peptidic antagonists towards several aGPCRs. Collectively, our study provides structural and biochemical insights into the tethered activation mechanism of aGPCRs.
リンク	Nature / PubMed:35418677
手法	EM (単粒子)
解像度	2.9 - 3.3 Å
構造データ	32836 7wui EMDB-32836, PDB-7wui: Tethered peptide activation mechanism of adhesion GPCRs ADGRG2 and ADGRG4 手法: EM (単粒子) / 解像度: 3.1 Å 32837 7wuj EMDB-32837, PDB-7wuj: Tethered peptide activation mechanism of adhesion GPCRs ADGRG2 and ADGRG4 手法: EM (単粒子) / 解像度: 3.3 Å 32838 7wuq EMDB-32838, PDB-7wuq: Tethered peptide activation mechanism of adhesion GPCRs ADGRG2 and ADGRG4 手法: EM (単粒子) / 解像度: 2.9 Å
由来	homo sapiens (ヒト) lama glama (ラマ) mus musculus (ハツカネズミ) synthetic construct (人工物) psychromonas sp. b3m02 (バクテリア)
キーワード	MEMBRANE PROTEIN / GPCR / ADGRG2 / ADGRG4