Opioid receptors in GtoPdb v.2025.1

Authors

  • Anna Borsodi Hungarian Academy Of Sciences
  • Lee-Yuan Liu-Chen Temple University
  • Davide Malfacini University of Padova
  • Dominique Massot Université de Strasbourg
  • Jean-Claude Meunier Institute of Pharmacology and Structural Biology
  • Philip S. Portoghese University of Minnesota
  • Stefan Schulz Friedrich Schiller University
  • Toni S. Shippenberg National Institutes of Health
  • Eric J. Simon New York University
  • Lawrence Toll Florida Atlantic University
  • John R. Traynor University of Michigan
  • Hiroshi Ueda Nagasaki Univ Grad Biomed Sci
  • Yung H. Wong Hong Kong University of Science and Technology
  • Nurulain Zaveri Astraea Therapeutics, LLC
  • Mary-Jeanne Kreek Rockefeller University
  • Ian Kitchen University of Surrey
  • Brigitte Kieffer Université de Strasbourg
  • Michael Bruchas Washington University
  • Girolamo Caló University of Padova
  • Charles Chavkin University of Washington Sch Med
  • MacDonald J. Christie University of Sydney
  • Olivier Civelli University of California, Irvine
  • Mark Connor Macquarie University https://orcid.org/0000-0003-2538-2001
  • Brian M. Cox Uniformed Services University
  • Lakshmi A. Devi Mount Sinai School of Medicine
  • Christopher Evans University of California Los Angeles
  • Volker Höllt Otto-von-Guericke University
  • Graeme Henderson University of Bristol
  • Stephen Husbands University of Bath
  • Eamonn Kelly University of Bristol
  • Andreas Zimmer University of Bonn

DOI:

https://doi.org/10.2218/gtopdb/F50/2025.1

Abstract

Opioid and opioid-like receptors are activated by a variety of endogenous peptides including [Met]enkephalin (met), [Leu]enkephalin (leu), β-endorphin (β-end), α-neodynorphin, dynorphin A (dynA), dynorphin B (dynB), big dynorphin (Big dyn), nociceptin/orphanin FQ (N/OFQ); endomorphin-1 and endomorphin-2 are also potential endogenous peptides. The Greek letter nomenclature for the opioid receptors, μ, δ and κ, is well established, and NC-IUPHAR considers this nomenclature appropriate, along with the symbols spelled out (mu, delta, and kappa), and the acronyms, MOP, DOP, and KOP [126, 103, 94]. However the acronyms MOR, DOR and KOR are still widely used in the literature. The human N/OFQ receptor, NOP, is considered 'opioid-related' rather than opioid because, while it exhibits a high degree of structural homology with the conventional opioid receptors [310], it displays a distinct pharmacology. Currently there are numerous clinically used drugs, such as morphine and many other opioid analgesics, as well as antagonists such as naloxone. The majority of clinically used opiates are relatively selective μ agonists or partial agonists, though there are some μ/κ compounds, such as butorphanol, in clinical use. κ opioid agonists, such as the alkaloid nalfurafine and the peripherally acting peptide difelikefalin, are in clinical use for itch.

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Published

01-Apr-2025

Issue

Vol. 2025 No. 1 (2025)

Section

Articles

License

Copyright (c) 2025 The authors

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This work is licensed under a Creative Commons Attribution-ShareAlike 4.0 International License.

How to Cite

“Opioid receptors in GtoPdb v.2025.1” (2025) IUPHAR/BPS Guide to Pharmacology CITE, 2025(1). doi:10.2218/gtopdb/F50/2025.1.