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Impaired β-arrestin recruitment and reduced desensitization by non-catechol agonists of the D1 dopamine receptor

Author

Listed:
  • David L. Gray

    (Pfizer Worldwide Research & Development
    Pfizer Worldwide Research & Development)

  • John A. Allen

    (Pfizer Worldwide Research & Development
    University of Texas Medical Branch)

  • Scot Mente

    (Pfizer Worldwide Research & Development)

  • Rebecca E. O’Connor

    (Pfizer Worldwide Research & Development)

  • George J. DeMarco

    (Pfizer Worldwide Research & Development)

  • Ivan Efremov

    (Pfizer Worldwide Research & Development)

  • Patrick Tierney

    (Pfizer Worldwide Research & Development)

  • Dmitri Volfson

    (Pfizer Worldwide Research & Development)

  • Jennifer Davoren

    (Pfizer Worldwide Research & Development)

  • Edward Guilmette

    (Pfizer Worldwide Research & Development)

  • Michelle Salafia

    (Pfizer Worldwide Research & Development)

  • Rouba Kozak

    (Pfizer Worldwide Research & Development)

  • Michael D. Ehlers

    (Pfizer Worldwide Research & Development
    Biogen, Inc.)

Abstract

Selective activation of dopamine D1 receptors (D1Rs) has been pursued for 40 years as a therapeutic strategy for neurologic and psychiatric diseases due to the fundamental role of D1Rs in motor function, reward processing, and cognition. All known D1R-selective agonists are catechols, which are rapidly metabolized and desensitize the D1R after prolonged exposure, reducing agonist response. As such, drug-like selective D1R agonists have remained elusive. Here we report a novel series of selective, potent non-catechol D1R agonists with promising in vivo pharmacokinetic properties. These ligands stimulate adenylyl cyclase signaling and are efficacious in a rodent model of Parkinson's disease after oral administration. They exhibit distinct binding to the D1R orthosteric site and a novel functional profile including minimal receptor desensitization, reduced recruitment of β-arrestin, and sustained in vivo efficacy. These results reveal a novel class of D1 agonists with favorable drug-like properties, and define the molecular basis for catechol-specific recruitment of β-arrestin to D1Rs.

Suggested Citation

  • David L. Gray & John A. Allen & Scot Mente & Rebecca E. O’Connor & George J. DeMarco & Ivan Efremov & Patrick Tierney & Dmitri Volfson & Jennifer Davoren & Edward Guilmette & Michelle Salafia & Rouba , 2018. "Impaired β-arrestin recruitment and reduced desensitization by non-catechol agonists of the D1 dopamine receptor," Nature Communications, Nature, vol. 9(1), pages 1-17, December.
  • Handle: RePEc:nat:natcom:v:9:y:2018:i:1:d:10.1038_s41467-017-02776-7
    DOI: 10.1038/s41467-017-02776-7
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    Cited by:

    1. Xiao Teng & Sijia Chen & Yingying Nie & Peng Xiao & Xiao Yu & Zhenhua Shao & Sanduo Zheng, 2022. "Ligand recognition and biased agonism of the D1 dopamine receptor," Nature Communications, Nature, vol. 13(1), pages 1-11, December.

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