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High-throughput identification of G protein-coupled receptor modulators through affinity mass spectrometry screening

  • Shanshan Qin
  • , Mengmeng Meng
  • , Dehua Yang
  • , Wenwen Bai
  • , Yan Lu
  • , Yao Peng
  • , Gaojie Song
  • , Yiran Wu
  • , Qingtong Zhou
  • , Suwen Zhao
  • , Xiping Huang
  • , John D. McCorvy
  • , Xiaoqing Cai
  • , Antao Dai
  • , Bryan L. Roth
  • , Michael A. Hanson
  • , Zhi Jie Liu
  • , Ming Wei Wang*
  • , Raymond C. Stevens
  • , Wenqing Shui
  • *此作品的通讯作者
  • ShanghaiTech University
  • Nankai University
  • CAS - Shanghai Institute of Materia Medica
  • University of North Carolina at Chapel Hill
  • GPCR Consortium
  • Fudan University

科研成果: 期刊稿件文章同行评审

摘要

G protein-coupled receptors (GPCRs) represent the largest class of cell surface proteins and thus constitute an important family of therapeutic targets. Therefore, significant effort has been put towards the identification of novel ligands that can modulate the activity of a GPCR target with high efficacy and selectivity. However, due to limitations inherent to the most common techniques for GPCR ligand discovery, there is a pressing need for more efficient and effective ligand screening methods especially for the identification of potential allosteric modulators. Here we present a high-throughput, label-free and unbiased screening approach for the identification of small molecule ligands towards GPCR targets based on affinity mass spectrometry. This new approach features the usage of target-expressing cell membranes rather than purified proteins for ligand screening and allows the detection of both orthosteric and allosteric ligands targeting specific GPCRs. Screening a small compound library with this approach led to the rapid discovery of an antagonist for the 5-HT receptor and four positive allosteric modulators for GLP-1 receptor that were not previously reported.

源语言英语
页(从-至)3192-3199
页数8
期刊Chemical Science
9
12
DOI
出版状态已出版 - 2018
已对外发布

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