Inhibition of endothelin A receptor by a novel, selective receptor antagonist enhances morphine-induced analgesia: Possible functional interaction of dimerized endothelin A and μ-opioid receptors

Yui Kuroda; Miki Nonaka; Yuji Kamikubo; Haruo Ogawa; Takashi Murayama; Nagomi Kurebayashi; Hakushun Sakairi; Kanako Miyano; Akane Komatsu; Tetsushi Dodo; Kyoko Nakano-Ito; Keisuke Yamaguchi; Takashi Sakurai; Masako Iseki; Masakazu Hayashida; Yasuhito Uezono

doi:10.1016/j.biopha.2021.111800

Inhibition of endothelin A receptor by a novel, selective receptor antagonist enhances morphine-induced analgesia: Possible functional interaction of dimerized endothelin A and μ-opioid receptors

Biomed Pharmacother. 2021 Sep:141:111800. doi: 10.1016/j.biopha.2021.111800. Epub 2021 Jun 24.

Authors

Yui Kuroda¹, Miki Nonaka², Yuji Kamikubo³, Haruo Ogawa⁴, Takashi Murayama³, Nagomi Kurebayashi³, Hakushun Sakairi³, Kanako Miyano⁵, Akane Komatsu¹, Tetsushi Dodo⁶, Kyoko Nakano-Ito⁷, Keisuke Yamaguchi⁸, Takashi Sakurai³, Masako Iseki⁹, Masakazu Hayashida⁹, Yasuhito Uezono¹⁰

Affiliations

¹ Department of Anesthesiology and Pain Medicine, Juntendo University Graduate School of Medicine, Tokyo, Japan; Department of Pain Control Research, The Jikei University School of Medicine, Tokyo, Japan.
² Department of Pain Control Research, The Jikei University School of Medicine, Tokyo, Japan.
³ Department of Cellular and Molecular Pharmacology, Juntendo University Graduate School of Medicine, Tokyo, Japan.
⁴ Institute of Molecular and Cellular Biosciences, The University of Tokyo, Tokyo, Japan.
⁵ Department of Pain Control Research, The Jikei University School of Medicine, Tokyo, Japan; Division of Cancer Pathophysiology, National Cancer Center Research Institute, Tokyo, Japan.
⁶ Strategy Planning & Operations, Medicine Development Center, Eisai Co., Ltd., Ibaraki, Japan.
⁷ Global Drug Safety, Medicine Development Center, Eisai Co., Ltd., Ibaraki, Japan.
⁸ Department of Pain Medicine, Juntendo University Graduate School of Medicine, Tokyo, Japan.
⁹ Department of Anesthesiology and Pain Medicine, Juntendo University Graduate School of Medicine, Tokyo, Japan; Department of Pain Medicine, Juntendo University Graduate School of Medicine, Tokyo, Japan.
¹⁰ Department of Pain Control Research, The Jikei University School of Medicine, Tokyo, Japan; Department of Pain Medicine, Juntendo University Graduate School of Medicine, Tokyo, Japan; Supportive and Palliative Care Research Support Office, National Center Hospital East, Chiba, Japan; Project for Supportive Care Research, Exploratory Oncology Research and Clinical Trial Center, National Cancer Center, Tokyo, Japan. Electronic address: yuezono@jikei.ac.jp.

PMID: 34175819
DOI: 10.1016/j.biopha.2021.111800

Abstract

Background: The misuse of opioids has led to an epidemic in recent times. The endothelin A receptor (ETAR) has recently attracted attention as a novel therapeutic target to enhance opioid analgesia. We hypothesized that endothelin A receptors may affect pain mechanisms by heterodimerization with μ opioid receptors. We examined the mechanisms of ETAR-mediated pain and the potential therapeutic effects of an ETAR antagonist, Compound-E, as an agent for analgesia.

Methods: Real-time in vitro effect of Compound-E on morphine response was assessed in HEK293 cells expressing both endothelin A and μ opioid receptors through CellKey™ and cADDis cAMP assays. Endothelin A/μ opioid receptor dimerization was assessed by immunoprecipitation and live cell imaging. The in vivo effect of Compound-E was evaluated using a morphine analgesia mouse model that observed escape response behavior, body temperature, and locomotor activity.

Results: In CellKey™ and cAMP assays, pretreatment of cells with endothelin-1 attenuated morphine-induced responses. These responses were improved by Compound-E, but not by BQ-123 nor by bosentan, an ETAR and endothelin B receptor antagonist. Dimerization of ETARs and μ opioid receptors was confirmed by Western blot and total internal reflection fluorescence microscopy in live cells. In vivo, Compound-E potentiated and prolonged the analgesic effects of morphine, enhanced hypothermia, and increased locomotor activity compared to morphine alone.

Conclusion: The results suggest that attenuation by endothelin-1 of morphine analgesia may be caused by dimerization of Endothelin A/μ opioid receptors. The novel ETAR antagonist Compound-E could be an effective adjunct to reduce opioid use.

Keywords: Analgesic; BQ-123 sodium salt (PubChem CID: 52943236); BQ-788 sodium salt (PubChem CID: 23693553); Endothelin A receptor antagonist; G protein-coupled receptor; Morphine; Pain; Receptor heterodimerization; and Bosentan Monohydrate (PubChem CID: 185462); included endothelin-1 (PubChem CID: 16212950); morphine hydrochloride (PubChem CID: 5464110).

MeSH terms

Analgesics, Opioid / administration & dosage*
Animals
Dose-Response Relationship, Drug
Endothelin A Receptor Antagonists / administration & dosage*
HEK293 Cells
Humans
Male
Mice
Mice, Inbred C57BL
Morphine / administration & dosage*
Pain Measurement / drug effects
Pain Measurement / methods
Peptides, Cyclic / administration & dosage
Protein Multimerization / drug effects
Protein Multimerization / physiology*
Receptor, Endothelin A / metabolism*
Receptors, Opioid, mu / metabolism*

Substances

Analgesics, Opioid
Endothelin A Receptor Antagonists
Peptides, Cyclic
Receptor, Endothelin A
Receptors, Opioid, mu
Morphine
cyclo(Trp-Asp-Pro-Val-Leu)