Structural Mass Spectrometry Captures Residue-Resolved Comprehensive Conformational Rearrangements of a G Protein-Coupled Receptor
2024-07-24
发表期刊JOURNAL OF THE AMERICAN CHEMICAL SOCIETY (IF:14.4[JCR-2023],14.8[5-Year])
ISSN0002-7863
EISSN1520-5126
卷号146期号:29页码:20045-20058
发表状态已发表
DOI10.1021/jacs.4c03922
摘要

G protein-coupled receptor (GPCR) structural studies with in-solution spectroscopic approaches have offered distinctive insights into GPCR activation and signaling that highly complement those yielded from structural snapshots by crystallography or cryo-EM. While most current spectroscopic approaches allow for probing structural changes at selected residues or loop regions, they are not suitable for capturing a holistic view of GPCR conformational rearrangements across multiple domains. Herein, we develop an approach based on limited proteolysis mass spectrometry (LiP-MS) to simultaneously monitor conformational alterations of a large number of residues spanning both flexible loops and structured transmembrane domains for a given GPCR. To benchmark LiP-MS for GPCR conformational profiling, we studied the adenosine 2A receptor (A2AR) in response to different ligand binding (agonist/antagonist/allosteric modulators) and G protein coupling. Systematic and residue-resolved profiling of A2AR conformational rearrangements by LiP-MS precisely captures structural mechanisms in multiple domains underlying ligand engagement, receptor activation, and allostery, and may also reflect local conformational flexibility. Furthermore, these residue-resolution structural fingerprints of the A2AR protein allow us to readily classify ligands of different pharmacology and distinguish the G protein-coupled state. Thus, our study provides a new structural MS approach that would be generalizable to characterizing conformational transition and plasticity for challenging integral membrane proteins. © 2024 American Chemical Society.

关键词Activation analysis Chemical activation Ligands Proteins 'current G protein G protein coupled receptors Limited proteolysis Multiple domains Receptor activation Receptor signaling Structural mass Structural snapshots Structural studies
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收录类别SCI ; EI
语种英语
资助项目National Key R&D Program of China[2022YFA1302902] ; National Key R&D Program of China[
WOS研究方向Chemistry
WOS类目Chemistry, Multidisciplinary
WOS记录号WOS:001276278800001
出版者American Chemical Society
EI入藏号20243016766641
EI主题词Mass spectrometry
EI分类号801 Chemistry ; 801.4 Physical Chemistry ; 802.2 Chemical Reactions ; 804 Chemical Products Generally ; 804.1 Organic Compounds
原始文献类型Journal article (JA)
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文献类型期刊论文
条目标识符https://kms.shanghaitech.edu.cn/handle/2MSLDSTB/407224
专题iHuman研究所
生命科学与技术学院
iHuman研究所_PI研究组_徐菲组
iHuman研究所_PI研究组_水雯箐组
生命科学与技术学院_硕士生
生命科学与技术学院_博士生
共同第一作者Yan, Pengfei
通讯作者Xu, Fei; Shui, Wenqing
作者单位
1.iHuman Institute, ShanghaiTech University, Shanghai; 201210, China;
2.School of Life Science and Technology, ShanghaiTech University, Shanghai; 201210, China;
3.University of Chinese Academy of Sciences, Beijing; 100049, China;
4.Shanghai Institute of Materia Medica, Chinese Academy of Sciences, Shanghai; 201203, China;
5.Department of Pharmacology, School of Basic Medical Sciences, Fudan University, Shanghai; 200032, China;
6.Medicinal Chemistry and Bioinformatics Center, Shanghai Jiao Tong University School of Medicine, Shanghai; 200025, China
第一作者单位iHuman研究所;  生命科学与技术学院
通讯作者单位iHuman研究所;  生命科学与技术学院
第一作者的第一单位iHuman研究所
推荐引用方式
GB/T 7714
Liu, Hongyue,Yan, Pengfei,Zhang, Zhaoyu,et al. Structural Mass Spectrometry Captures Residue-Resolved Comprehensive Conformational Rearrangements of a G Protein-Coupled Receptor[J]. JOURNAL OF THE AMERICAN CHEMICAL SOCIETY,2024,146(29):20045-20058.
APA Liu, Hongyue.,Yan, Pengfei.,Zhang, Zhaoyu.,Han, Hongbo.,Zhou, Qingtong.,...&Shui, Wenqing.(2024).Structural Mass Spectrometry Captures Residue-Resolved Comprehensive Conformational Rearrangements of a G Protein-Coupled Receptor.JOURNAL OF THE AMERICAN CHEMICAL SOCIETY,146(29),20045-20058.
MLA Liu, Hongyue,et al."Structural Mass Spectrometry Captures Residue-Resolved Comprehensive Conformational Rearrangements of a G Protein-Coupled Receptor".JOURNAL OF THE AMERICAN CHEMICAL SOCIETY 146.29(2024):20045-20058.
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