Usefulness for the combination of G protein- and β-arrestin-biased ligands of μ-opioid receptors: Prevention of antinociceptive tolerance

BACKGROUND: µ-Opioid receptor internalization is considered to be critically linked to antinociceptive tolerance. Although µ-opioid receptor agonists have been administered simultaneously with other drugs to control pain, little information is available regarding opioid–opioid interactions. Therefor...

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Autores principales: Mori, Tomohisa, Kuzumaki, Naoko, Arima, Takamichi, Narita, Michiko, Tateishi, Ryunosuke, Kondo, Takashige, Hamada, Yusuke, Kuwata, Hirotsugu, Kawata, Miho, Yamazaki, Mitsuaki, Sugita, Kazuyuki, Matsuzawa, Akinobu, Baba, Kanae, Yamauchi, Takayasu, Higashiyama, Kimio, Nonaka, Miki, Miyano, Kanako, Uezono, Yasuhito, Narita, Minoru
Formato: Online Artículo Texto
Lenguaje:English
Publicado: SAGE Publications 2017
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5676499/
https://www.ncbi.nlm.nih.gov/pubmed/29056067
http://dx.doi.org/10.1177/1744806917740030
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author Mori, Tomohisa
Kuzumaki, Naoko
Arima, Takamichi
Narita, Michiko
Tateishi, Ryunosuke
Kondo, Takashige
Hamada, Yusuke
Kuwata, Hirotsugu
Kawata, Miho
Yamazaki, Mitsuaki
Sugita, Kazuyuki
Matsuzawa, Akinobu
Baba, Kanae
Yamauchi, Takayasu
Higashiyama, Kimio
Nonaka, Miki
Miyano, Kanako
Uezono, Yasuhito
Narita, Minoru
author_facet Mori, Tomohisa
Kuzumaki, Naoko
Arima, Takamichi
Narita, Michiko
Tateishi, Ryunosuke
Kondo, Takashige
Hamada, Yusuke
Kuwata, Hirotsugu
Kawata, Miho
Yamazaki, Mitsuaki
Sugita, Kazuyuki
Matsuzawa, Akinobu
Baba, Kanae
Yamauchi, Takayasu
Higashiyama, Kimio
Nonaka, Miki
Miyano, Kanako
Uezono, Yasuhito
Narita, Minoru
author_sort Mori, Tomohisa
collection PubMed
description BACKGROUND: µ-Opioid receptor internalization is considered to be critically linked to antinociceptive tolerance. Although µ-opioid receptor agonists have been administered simultaneously with other drugs to control pain, little information is available regarding opioid–opioid interactions. Therefore, the present study was designed to further investigate the utility of a new G protein-biased ligand for µ-opioid receptors, TRV130, which has an antinociceptive effect without β-arrestin-dependent µ-opioid receptor internalization, and its combination with fentanyl using µ-opioid receptor-expressing cells and mice. RESULTS: In the present study, we confirmed that fentanyl produced a profound increase in β-arrestin-2 recruitment accompanied by µ-opioid receptor internalization, whereas TRV130 did not induce either the recruitment of β-arrestin-2 or µ-opioid receptor internalization in µ-opioid receptor-expressing cells. Under these conditions, β-arrestin-2 recruitment accompanied by µ-opioid receptor internalization induced by fentanyl was abolished by TRV130, whereas TRV130 did not alter the reduction of cyclic adenosine monophosphate formation by fentanyl in µ-opioid receptor-expressing cells. In a behavioral assay, TRV130 exerted an antinociceptive effect in a hot-plate test in mice. In a combination test, the antinociceptive effect of TRV130 was synergistically increased by fentanyl. Fentanyl induced antihyperalgesia and development of its tolerance under a neuropathic pain-like state following sciatic nerve ligation. However, treatment of mice with an antinociceptive dose of TRV130 did not induce the rapid development of tolerance to its antihyperalgesic effect under a neuropathic pain-like state. Furthermore, the rapid development of tolerance to the antihyperalgesic effect induced by fentanyl plus TRV130 in mice with sciatic nerve ligation was not observed, unlike in the case of fentanyl alone. CONCLUSIONS: These findings provide evidence that activation of the G protein-biased pathway through µ-opioid receptors can alter signaling in the β-arrestin-2 pathway linked to the stimulation of µ-opioid receptors. Furthermore, the combination of G protein-biased and β-arrestin-biased ligands of µ-opioid receptors exerts an ideal antinociceptive effect without the rapid development of antinociceptive tolerance.
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spelling pubmed-56764992017-11-21 Usefulness for the combination of G protein- and β-arrestin-biased ligands of μ-opioid receptors: Prevention of antinociceptive tolerance Mori, Tomohisa Kuzumaki, Naoko Arima, Takamichi Narita, Michiko Tateishi, Ryunosuke Kondo, Takashige Hamada, Yusuke Kuwata, Hirotsugu Kawata, Miho Yamazaki, Mitsuaki Sugita, Kazuyuki Matsuzawa, Akinobu Baba, Kanae Yamauchi, Takayasu Higashiyama, Kimio Nonaka, Miki Miyano, Kanako Uezono, Yasuhito Narita, Minoru Mol Pain Research Article BACKGROUND: µ-Opioid receptor internalization is considered to be critically linked to antinociceptive tolerance. Although µ-opioid receptor agonists have been administered simultaneously with other drugs to control pain, little information is available regarding opioid–opioid interactions. Therefore, the present study was designed to further investigate the utility of a new G protein-biased ligand for µ-opioid receptors, TRV130, which has an antinociceptive effect without β-arrestin-dependent µ-opioid receptor internalization, and its combination with fentanyl using µ-opioid receptor-expressing cells and mice. RESULTS: In the present study, we confirmed that fentanyl produced a profound increase in β-arrestin-2 recruitment accompanied by µ-opioid receptor internalization, whereas TRV130 did not induce either the recruitment of β-arrestin-2 or µ-opioid receptor internalization in µ-opioid receptor-expressing cells. Under these conditions, β-arrestin-2 recruitment accompanied by µ-opioid receptor internalization induced by fentanyl was abolished by TRV130, whereas TRV130 did not alter the reduction of cyclic adenosine monophosphate formation by fentanyl in µ-opioid receptor-expressing cells. In a behavioral assay, TRV130 exerted an antinociceptive effect in a hot-plate test in mice. In a combination test, the antinociceptive effect of TRV130 was synergistically increased by fentanyl. Fentanyl induced antihyperalgesia and development of its tolerance under a neuropathic pain-like state following sciatic nerve ligation. However, treatment of mice with an antinociceptive dose of TRV130 did not induce the rapid development of tolerance to its antihyperalgesic effect under a neuropathic pain-like state. Furthermore, the rapid development of tolerance to the antihyperalgesic effect induced by fentanyl plus TRV130 in mice with sciatic nerve ligation was not observed, unlike in the case of fentanyl alone. CONCLUSIONS: These findings provide evidence that activation of the G protein-biased pathway through µ-opioid receptors can alter signaling in the β-arrestin-2 pathway linked to the stimulation of µ-opioid receptors. Furthermore, the combination of G protein-biased and β-arrestin-biased ligands of µ-opioid receptors exerts an ideal antinociceptive effect without the rapid development of antinociceptive tolerance. SAGE Publications 2017-11-06 /pmc/articles/PMC5676499/ /pubmed/29056067 http://dx.doi.org/10.1177/1744806917740030 Text en © The Author(s) 2017 http://creativecommons.org/licenses/by-nc/4.0/ This article is distributed under the terms of the Creative Commons Attribution-NonCommercial 4.0 License (http://www.creativecommons.org/licenses/by-nc/4.0/) which permits non-commercial use, reproduction and distribution of the work without further permission provided the original work is attributed as specified on the SAGE and Open Access pages (https://us.sagepub.com/en-us/nam/open-access-at-sage).
spellingShingle Research Article
Mori, Tomohisa
Kuzumaki, Naoko
Arima, Takamichi
Narita, Michiko
Tateishi, Ryunosuke
Kondo, Takashige
Hamada, Yusuke
Kuwata, Hirotsugu
Kawata, Miho
Yamazaki, Mitsuaki
Sugita, Kazuyuki
Matsuzawa, Akinobu
Baba, Kanae
Yamauchi, Takayasu
Higashiyama, Kimio
Nonaka, Miki
Miyano, Kanako
Uezono, Yasuhito
Narita, Minoru
Usefulness for the combination of G protein- and β-arrestin-biased ligands of μ-opioid receptors: Prevention of antinociceptive tolerance
title Usefulness for the combination of G protein- and β-arrestin-biased ligands of μ-opioid receptors: Prevention of antinociceptive tolerance
title_full Usefulness for the combination of G protein- and β-arrestin-biased ligands of μ-opioid receptors: Prevention of antinociceptive tolerance
title_fullStr Usefulness for the combination of G protein- and β-arrestin-biased ligands of μ-opioid receptors: Prevention of antinociceptive tolerance
title_full_unstemmed Usefulness for the combination of G protein- and β-arrestin-biased ligands of μ-opioid receptors: Prevention of antinociceptive tolerance
title_short Usefulness for the combination of G protein- and β-arrestin-biased ligands of μ-opioid receptors: Prevention of antinociceptive tolerance
title_sort usefulness for the combination of g protein- and β-arrestin-biased ligands of μ-opioid receptors: prevention of antinociceptive tolerance
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5676499/
https://www.ncbi.nlm.nih.gov/pubmed/29056067
http://dx.doi.org/10.1177/1744806917740030
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