The effects of chronic high-dose morphine on microgliosis and the microglial transcriptome in rat spinal cord

Background: Opioids are efficacious and safe analgesic drugs in short-term use for acute pain but chronic use can lead to tolerance and dependence. Opioid-induced microglial activation may contribute to the development of tolerance and this process may differ between males and females. A link is sug...

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Autores principales: Ahlström, Fredrik HG, Viisanen, Hanna, Karhinen, Leena, Mätlik, Kert, Blomqvist, Kim J, Lilius, Tuomas O, Sidorova, Yulia A, Palada, Vinko, Rauhala, Pekka V, Kalso, Eija A
Formato: Online Artículo Texto
Lenguaje:English
Publicado: SAGE Publications 2023
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10331785/
https://www.ncbi.nlm.nih.gov/pubmed/37285551
http://dx.doi.org/10.1177/17448069231183902
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author Ahlström, Fredrik HG
Viisanen, Hanna
Karhinen, Leena
Mätlik, Kert
Blomqvist, Kim J
Lilius, Tuomas O
Sidorova, Yulia A
Palada, Vinko
Rauhala, Pekka V
Kalso, Eija A
author_facet Ahlström, Fredrik HG
Viisanen, Hanna
Karhinen, Leena
Mätlik, Kert
Blomqvist, Kim J
Lilius, Tuomas O
Sidorova, Yulia A
Palada, Vinko
Rauhala, Pekka V
Kalso, Eija A
author_sort Ahlström, Fredrik HG
collection PubMed
description Background: Opioids are efficacious and safe analgesic drugs in short-term use for acute pain but chronic use can lead to tolerance and dependence. Opioid-induced microglial activation may contribute to the development of tolerance and this process may differ between males and females. A link is suggested between this microglial activation and inflammation, disturbances of circadian rhythms, and neurotoxic effects. We set out to further delineate the effects of chronic morphine on pain behaviour, microglial and neuronal staining, and the transcriptome of spinal microglia, to better understand the role of microglia in the consequences of long-term high-dose opioid administration. Experimental Approach: In two experiments, we administered increasing subcutaneous doses of morphine hydrochloride or saline to male and female rats. Thermal nociception was assessed with the tail flick and hot plate tests. In Experiment I, spinal cord (SC) samples were prepared for immunohistochemical staining for microglial and neuronal markers. In Experiment II, the transcriptome of microglia from the lumbar SC was analysed. Key Results: Female and male rats had similar antinociceptive responses to morphine and developed similar antinociceptive tolerance to thermal stimuli following chronic increasing high doses of s.c. morphine. The area of microglial IBA1-staining in SC decreased after 2 weeks of morphine administration in both sexes. Following morphine treatment, the differentially expressed genes identified in the microglial transcriptome included ones related to the circadian rhythm, apoptosis, and immune system processes. Conclusions: Female and male rats showed similar pain behaviour following chronic high doses of morphine. This was associated with decreased staining of spinal microglia, suggesting either decreased activation or apoptosis. High-dose morphine administration also associated with several changes in gene expression in SC microglia, e.g., those related to the circadian rhythm (Per2, Per3, Dbp). These changes should be considered in the clinical consequences of long-term high-dose administration of opioids.
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spelling pubmed-103317852023-07-11 The effects of chronic high-dose morphine on microgliosis and the microglial transcriptome in rat spinal cord Ahlström, Fredrik HG Viisanen, Hanna Karhinen, Leena Mätlik, Kert Blomqvist, Kim J Lilius, Tuomas O Sidorova, Yulia A Palada, Vinko Rauhala, Pekka V Kalso, Eija A Mol Pain Research Article Background: Opioids are efficacious and safe analgesic drugs in short-term use for acute pain but chronic use can lead to tolerance and dependence. Opioid-induced microglial activation may contribute to the development of tolerance and this process may differ between males and females. A link is suggested between this microglial activation and inflammation, disturbances of circadian rhythms, and neurotoxic effects. We set out to further delineate the effects of chronic morphine on pain behaviour, microglial and neuronal staining, and the transcriptome of spinal microglia, to better understand the role of microglia in the consequences of long-term high-dose opioid administration. Experimental Approach: In two experiments, we administered increasing subcutaneous doses of morphine hydrochloride or saline to male and female rats. Thermal nociception was assessed with the tail flick and hot plate tests. In Experiment I, spinal cord (SC) samples were prepared for immunohistochemical staining for microglial and neuronal markers. In Experiment II, the transcriptome of microglia from the lumbar SC was analysed. Key Results: Female and male rats had similar antinociceptive responses to morphine and developed similar antinociceptive tolerance to thermal stimuli following chronic increasing high doses of s.c. morphine. The area of microglial IBA1-staining in SC decreased after 2 weeks of morphine administration in both sexes. Following morphine treatment, the differentially expressed genes identified in the microglial transcriptome included ones related to the circadian rhythm, apoptosis, and immune system processes. Conclusions: Female and male rats showed similar pain behaviour following chronic high doses of morphine. This was associated with decreased staining of spinal microglia, suggesting either decreased activation or apoptosis. High-dose morphine administration also associated with several changes in gene expression in SC microglia, e.g., those related to the circadian rhythm (Per2, Per3, Dbp). These changes should be considered in the clinical consequences of long-term high-dose administration of opioids. SAGE Publications 2023-06-26 /pmc/articles/PMC10331785/ /pubmed/37285551 http://dx.doi.org/10.1177/17448069231183902 Text en © The Author(s) 2023 https://creativecommons.org/licenses/by/4.0/This article is distributed under the terms of the Creative Commons Attribution 4.0 License (https://creativecommons.org/licenses/by/4.0/) which permits any 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
Ahlström, Fredrik HG
Viisanen, Hanna
Karhinen, Leena
Mätlik, Kert
Blomqvist, Kim J
Lilius, Tuomas O
Sidorova, Yulia A
Palada, Vinko
Rauhala, Pekka V
Kalso, Eija A
The effects of chronic high-dose morphine on microgliosis and the microglial transcriptome in rat spinal cord
title The effects of chronic high-dose morphine on microgliosis and the microglial transcriptome in rat spinal cord
title_full The effects of chronic high-dose morphine on microgliosis and the microglial transcriptome in rat spinal cord
title_fullStr The effects of chronic high-dose morphine on microgliosis and the microglial transcriptome in rat spinal cord
title_full_unstemmed The effects of chronic high-dose morphine on microgliosis and the microglial transcriptome in rat spinal cord
title_short The effects of chronic high-dose morphine on microgliosis and the microglial transcriptome in rat spinal cord
title_sort effects of chronic high-dose morphine on microgliosis and the microglial transcriptome in rat spinal cord
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10331785/
https://www.ncbi.nlm.nih.gov/pubmed/37285551
http://dx.doi.org/10.1177/17448069231183902
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