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Structural and dynamic insights into supra-physiological activation and allosteric modulation of a muscarinic acetylcholine receptor

Author

Listed:
  • Jun Xu

    (Stanford University School of Medicine
    Tsinghua University)

  • Qinggong Wang

    (Chinese University of Hong Kong
    University of Science and Technology of China)

  • Harald Hübner

    (Friedrich-Alexander University)

  • Yunfei Hu

    (Peking University
    Innovation Academy for Precision Measurement Science and Technology, CAS)

  • Xiaogang Niu

    (Peking University)

  • Haoqing Wang

    (Stanford University School of Medicine)

  • Shoji Maeda

    (Stanford University School of Medicine
    Medical School, University of Michigan 1150 Medical Center Dr., 1315 Medical Science Research Bldg III)

  • Asuka Inoue

    (Tohoku University)

  • Yuyong Tao

    (University of Science and Technology of China)

  • Peter Gmeiner

    (Friedrich-Alexander University)

  • Yang Du

    (Chinese University of Hong Kong)

  • Changwen Jin

    (Peking University)

  • Brian K. Kobilka

    (Stanford University School of Medicine)

Abstract

The M2 muscarinic receptor (M2R) is a prototypical G-protein-coupled receptor (GPCR) that serves as a model system for understanding GPCR regulation by both orthosteric and allosteric ligands. Here, we investigate the mechanisms governing M2R signaling versatility using cryo-electron microscopy (cryo-EM) and NMR spectroscopy, focusing on the physiological agonist acetylcholine and a supra-physiological agonist iperoxo, as well as a positive allosteric modulator LY2119620. These studies reveal that acetylcholine stabilizes a more heterogeneous M2R-G-protein complex than iperoxo, where two conformers with distinctive G-protein orientations were determined. We find that LY2119620 increases the affinity for both agonists, but differentially modulates agonists efficacy in G-protein and β-arrestin pathways. Structural and spectroscopic analysis suggest that LY211620 stabilizes distinct intracellular conformational ensembles from agonist-bound M2R, which may enhance β-arrestin recruitment while impairing G-protein activation. These results highlight the role of conformational dynamics in the complex signaling behavior of GPCRs, and could facilitate design of better drugs.

Suggested Citation

  • Jun Xu & Qinggong Wang & Harald Hübner & Yunfei Hu & Xiaogang Niu & Haoqing Wang & Shoji Maeda & Asuka Inoue & Yuyong Tao & Peter Gmeiner & Yang Du & Changwen Jin & Brian K. Kobilka, 2023. "Structural and dynamic insights into supra-physiological activation and allosteric modulation of a muscarinic acetylcholine receptor," Nature Communications, Nature, vol. 14(1), pages 1-16, December.
  • Handle: RePEc:nat:natcom:v:14:y:2023:i:1:d:10.1038_s41467-022-35726-z
    DOI: 10.1038/s41467-022-35726-z
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    2. Aslihan Shenol & Ricardo Tenente & Michael Lückmann & Thomas M. Frimurer & Thue W. Schwartz, 2024. "Multiple recent HCAR2 structures demonstrate a highly dynamic ligand binding and G protein activation mode," Nature Communications, Nature, vol. 15(1), pages 1-10, December.

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