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Role of C-fibers in pain and morphine induced analgesia/hyperalgesia in rats

BACKGROUND: Usual dosage of morphine (10 mg/kg) induces analgesia and ultra-low dose (ULD) of morphine (1 µg/kg); hyperalgesia, and C-fibers are also bearing µ-opioid receptors; here the importance of C-fibers on pain and morphine induced analgesia/hyperalgesia is questioned and investigated using p...

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Autores principales: Alizadeh, Zahra, Fereidoni, Masoud, Behnam-Rassouli, Morteza, Hosseini, Shirin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Tehran University of Medical Sciences 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3968353/
https://www.ncbi.nlm.nih.gov/pubmed/24800043
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author Alizadeh, Zahra
Fereidoni, Masoud
Behnam-Rassouli, Morteza
Hosseini, Shirin
author_facet Alizadeh, Zahra
Fereidoni, Masoud
Behnam-Rassouli, Morteza
Hosseini, Shirin
author_sort Alizadeh, Zahra
collection PubMed
description BACKGROUND: Usual dosage of morphine (10 mg/kg) induces analgesia and ultra-low dose (ULD) of morphine (1 µg/kg); hyperalgesia, and C-fibers are also bearing µ-opioid receptors; here the importance of C-fibers on pain and morphine induced analgesia/hyperalgesia is questioned and investigated using pain evaluation methods and infant capsaicin treating for C-fibers lesioning. METHODS: Wistar male rats (200-250 grams) were assigned to three categories i.e. control, sham (receiving neonatal capsaicin vehicle) and c-lesion (receiving neonatal capsaicin), each one with three groups (n=7). They were injected intraperitoneally with single dosage of saline, 10 mg/kg or 1 µg/kg morphine, respectively. Thermal pain threshold was evaluated using the tail flick test before and 30 minutes after the injections. Chemical pain was assessed using the formalin test (FT) 30 minutes after the administrations. RESULTS: Results indicated that thermal (P < 0.001) and chemical pains in both neurogenic and inflammatory phases of FT (P < 0.05) were reduced in C-lesion animals. In the C-normal and C-lesion animals, 10 mg/kg morphine exerted analgesia both in thermal (P < 0.001) and two phases of FT (P < 0.01), but it was more potent in C-lesion animals (P < 0.05). Although ULD of morphine in C-normal animals produced hyperalgesic effect in thermal and chemical pains (P < 0.001), in C-lesion animals, it produced analgesia (P < 0.05) at the neurogenic phase of FT. CONCLUSION: Results can raise the C-fibers involvement for a significant portion of nociceptive transmission, because C-lesioning potentiated morphine induced analgesia and eliminated ULD of morphine induced hyperalgesia. Therefore C and Aδ fibers can be involved in morphine analgesia; while, just C-fibers are possibly responsible for only presynaptically hyperalgesic/excitatory action of ULD in morphine.
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spelling pubmed-39683532014-05-05 Role of C-fibers in pain and morphine induced analgesia/hyperalgesia in rats Alizadeh, Zahra Fereidoni, Masoud Behnam-Rassouli, Morteza Hosseini, Shirin Iran J Neurol Original Paper BACKGROUND: Usual dosage of morphine (10 mg/kg) induces analgesia and ultra-low dose (ULD) of morphine (1 µg/kg); hyperalgesia, and C-fibers are also bearing µ-opioid receptors; here the importance of C-fibers on pain and morphine induced analgesia/hyperalgesia is questioned and investigated using pain evaluation methods and infant capsaicin treating for C-fibers lesioning. METHODS: Wistar male rats (200-250 grams) were assigned to three categories i.e. control, sham (receiving neonatal capsaicin vehicle) and c-lesion (receiving neonatal capsaicin), each one with three groups (n=7). They were injected intraperitoneally with single dosage of saline, 10 mg/kg or 1 µg/kg morphine, respectively. Thermal pain threshold was evaluated using the tail flick test before and 30 minutes after the injections. Chemical pain was assessed using the formalin test (FT) 30 minutes after the administrations. RESULTS: Results indicated that thermal (P < 0.001) and chemical pains in both neurogenic and inflammatory phases of FT (P < 0.05) were reduced in C-lesion animals. In the C-normal and C-lesion animals, 10 mg/kg morphine exerted analgesia both in thermal (P < 0.001) and two phases of FT (P < 0.01), but it was more potent in C-lesion animals (P < 0.05). Although ULD of morphine in C-normal animals produced hyperalgesic effect in thermal and chemical pains (P < 0.001), in C-lesion animals, it produced analgesia (P < 0.05) at the neurogenic phase of FT. CONCLUSION: Results can raise the C-fibers involvement for a significant portion of nociceptive transmission, because C-lesioning potentiated morphine induced analgesia and eliminated ULD of morphine induced hyperalgesia. Therefore C and Aδ fibers can be involved in morphine analgesia; while, just C-fibers are possibly responsible for only presynaptically hyperalgesic/excitatory action of ULD in morphine. Tehran University of Medical Sciences 2014 /pmc/articles/PMC3968353/ /pubmed/24800043 Text en Copyright © 2014 Iranian Neurological Association, and Tehran University of Medical Sciences http://creativecommons.org/licenses/by/2.0/ This work is licensed under a Creative Commons Attribution-NonCommercial 3.0 Unported License which allows users to read, copy, distribute and make derivative works for non-commercial purposes from the material, as long as the author of the original work is cited properly.
spellingShingle Original Paper
Alizadeh, Zahra
Fereidoni, Masoud
Behnam-Rassouli, Morteza
Hosseini, Shirin
Role of C-fibers in pain and morphine induced analgesia/hyperalgesia in rats
title Role of C-fibers in pain and morphine induced analgesia/hyperalgesia in rats
title_full Role of C-fibers in pain and morphine induced analgesia/hyperalgesia in rats
title_fullStr Role of C-fibers in pain and morphine induced analgesia/hyperalgesia in rats
title_full_unstemmed Role of C-fibers in pain and morphine induced analgesia/hyperalgesia in rats
title_short Role of C-fibers in pain and morphine induced analgesia/hyperalgesia in rats
title_sort role of c-fibers in pain and morphine induced analgesia/hyperalgesia in rats
topic Original Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3968353/
https://www.ncbi.nlm.nih.gov/pubmed/24800043
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