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Phospho-selective mechanisms of arrestin conformations and functions revealed by unnatural amino acid incorporation and 19F-NMR

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  • Fan Yang

    (Laboratory of Quantum Biophysics and Laboratory of RNA Biology, Institute of Biophysics, Chinese Academy of Sciences
    Shandong University School of Medicine
    Shandong University School of Medicine)

  • Xiao Yu

    (Shandong University School of Medicine
    Shandong University School of Medicine)

  • Chuan Liu

    (Shandong University School of Medicine)

  • Chang-Xiu Qu

    (Shandong University School of Medicine)

  • Zheng Gong

    (Shandong University School of Medicine)

  • Hong-Da Liu

    (Shandong University School of Medicine)

  • Fa-Hui Li

    (Laboratory of Quantum Biophysics and Laboratory of RNA Biology, Institute of Biophysics, Chinese Academy of Sciences)

  • Hong-Mei Wang

    (Shandong University School of Medicine)

  • Dong-Fang He

    (Shandong University School of Medicine
    Shandong University School of Medicine)

  • Fan Yi

    (Shandong University School of Medicine)

  • Chen Song

    (University of Oxford)

  • Chang-Lin Tian

    (Hefei National Laboratory for Physical Science at Microscale and School of Life Science, University of Science and Technology of China)

  • Kun-Hong Xiao

    (School of Medicine, University of Pittsburgh
    School of Medicine, Duke University)

  • Jiang-Yun Wang

    (Laboratory of Quantum Biophysics and Laboratory of RNA Biology, Institute of Biophysics, Chinese Academy of Sciences)

  • Jin-Peng Sun

    (Shandong University School of Medicine
    Shandong University School of Medicine)

Abstract

Specific arrestin conformations are coupled to distinct downstream effectors, which underlie the functions of many G-protein-coupled receptors (GPCRs). Here, using unnatural amino acid incorporation and fluorine-19 nuclear magnetic resonance (19F-NMR) spectroscopy, we demonstrate that distinct receptor phospho-barcodes are translated to specific β-arrestin-1 conformations and direct selective signalling. With its phosphate-binding concave surface, β-arrestin-1 ‘reads’ the message in the receptor phospho-C-tails and distinct phospho-interaction patterns are revealed by 19F-NMR. Whereas all functional phosphopeptides interact with a common phosphate binding site and induce the movements of finger and middle loops, different phospho-interaction patterns induce distinct structural states of β-arrestin-1 that are coupled to distinct arrestin functions. Only clathrin recognizes and stabilizes GRK2-specific β-arrestin-1 conformations. The identified receptor-phospho-selective mechanism for arrestin conformation and the spacing of the multiple phosphate-binding sites in the arrestin enable arrestin to recognize plethora phosphorylation states of numerous GPCRs, contributing to the functional diversity of receptors.

Suggested Citation

  • Fan Yang & Xiao Yu & Chuan Liu & Chang-Xiu Qu & Zheng Gong & Hong-Da Liu & Fa-Hui Li & Hong-Mei Wang & Dong-Fang He & Fan Yi & Chen Song & Chang-Lin Tian & Kun-Hong Xiao & Jiang-Yun Wang & Jin-Peng Su, 2015. "Phospho-selective mechanisms of arrestin conformations and functions revealed by unnatural amino acid incorporation and 19F-NMR," Nature Communications, Nature, vol. 6(1), pages 1-15, November.
  • Handle: RePEc:nat:natcom:v:6:y:2015:i:1:d:10.1038_ncomms9202
    DOI: 10.1038/ncomms9202
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    Cited by:

    1. Yutaro Shiraishi & Yutaka Kofuku & Takumi Ueda & Shubhi Pandey & Hemlata Dwivedi-Agnihotri & Arun K. Shukla & Ichio Shimada, 2021. "Biphasic activation of β-arrestin 1 upon interaction with a GPCR revealed by methyl-TROSY NMR," Nature Communications, Nature, vol. 12(1), pages 1-11, December.
    2. Ruibo Zhai & Zhuoqi Wang & Zhaofei Chai & Xiaogang Niu & Conggang Li & Changwen Jin & Yunfei Hu, 2023. "Distinct activation mechanisms of β-arrestin-1 revealed by 19F NMR spectroscopy," Nature Communications, Nature, vol. 14(1), pages 1-15, December.

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