Prostanoid receptor EP1 and Cox-2 in injured human nerves and a rat model of nerve injury: a time-course study

BACKGROUND: Recent studies show that inflammatory processes may contribute to neuropathic pain. Cyclooxygenase-2 (Cox-2) is an inducible enzyme responsible for production of prostanoids, which may sensitise sensory neurones via the EP1 receptor. We have recently reported that while macrophages infil...

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Autores principales: Durrenberger, Pascal F, Facer, Paul, Casula, Maria A, Yiangou, Yiangos, Gray, Roy A, Chessell, Iain P, Day, Nicola C, Collins, Sue D, Bingham, Sharon, Wilson, Alex W, Elliot, David, Birch, Rolfe, Anand, Praveen
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2006
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1361784/
https://www.ncbi.nlm.nih.gov/pubmed/16393343
http://dx.doi.org/10.1186/1471-2377-6-1
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author Durrenberger, Pascal F
Facer, Paul
Casula, Maria A
Yiangou, Yiangos
Gray, Roy A
Chessell, Iain P
Day, Nicola C
Collins, Sue D
Bingham, Sharon
Wilson, Alex W
Elliot, David
Birch, Rolfe
Anand, Praveen
author_facet Durrenberger, Pascal F
Facer, Paul
Casula, Maria A
Yiangou, Yiangos
Gray, Roy A
Chessell, Iain P
Day, Nicola C
Collins, Sue D
Bingham, Sharon
Wilson, Alex W
Elliot, David
Birch, Rolfe
Anand, Praveen
author_sort Durrenberger, Pascal F
collection PubMed
description BACKGROUND: Recent studies show that inflammatory processes may contribute to neuropathic pain. Cyclooxygenase-2 (Cox-2) is an inducible enzyme responsible for production of prostanoids, which may sensitise sensory neurones via the EP1 receptor. We have recently reported that while macrophages infiltrate injured nerves within days of injury, they express increased Cox-2-immunoreactivity (Cox-2-IR) from 2 to 3 weeks after injury. We have now investigated the time course of EP1 and Cox-2 changes in injured human nerves and dorsal root ganglia (DRG), and the chronic constriction nerve injury (CCI) model in the rat. METHODS: Tissue sections were immunostained with specific antibodies to EP1, Cox-2, CD68 (human macrophage marker) or OX42 (rat microglial marker), and neurofilaments (NF), prior to image analysis, from the following: human brachial plexus nerves (21 to 196 days post-injury), painful neuromas (9 days to 12 years post-injury), avulsion injured DRG, control nerves and DRG, and rat CCI model tissues. EP1 and NF-immunoreactive nerve fibres were quantified by image analysis. RESULTS: EP1:NF ratio was significantly increased in human brachial plexus nerve fibres, both proximal and distal to injury, in comparison with uninjured nerves. Sensory neurones in injured human DRG showed a significant acute increase of EP1-IR intensity. While there was a rapid increase in EP1-fibres and CD-68 positive macrophages, Cox-2 increase was apparent later, but was persistent in human painful neuromas for years. A similar time-course of changes was found in the rat CCI model with the above markers, both in the injured nerves and ipsilateral dorsal spinal cord. CONCLUSION: Different stages of infiltration and activation of macrophages may be observed in the peripheral and central nervous system following peripheral nerve injury. EP1 receptor level increase in sensory neurones, and macrophage infiltration, appears to precede increased Cox-2 expression by macrophages. However, other methods for detecting Cox-2 levels and activity are required. EP1 antagonists may show therapeutic effects in acute and chronic neuropathic pain, in addition to inflammatory pain.
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spelling pubmed-13617842006-02-09 Prostanoid receptor EP1 and Cox-2 in injured human nerves and a rat model of nerve injury: a time-course study Durrenberger, Pascal F Facer, Paul Casula, Maria A Yiangou, Yiangos Gray, Roy A Chessell, Iain P Day, Nicola C Collins, Sue D Bingham, Sharon Wilson, Alex W Elliot, David Birch, Rolfe Anand, Praveen BMC Neurol Research Article BACKGROUND: Recent studies show that inflammatory processes may contribute to neuropathic pain. Cyclooxygenase-2 (Cox-2) is an inducible enzyme responsible for production of prostanoids, which may sensitise sensory neurones via the EP1 receptor. We have recently reported that while macrophages infiltrate injured nerves within days of injury, they express increased Cox-2-immunoreactivity (Cox-2-IR) from 2 to 3 weeks after injury. We have now investigated the time course of EP1 and Cox-2 changes in injured human nerves and dorsal root ganglia (DRG), and the chronic constriction nerve injury (CCI) model in the rat. METHODS: Tissue sections were immunostained with specific antibodies to EP1, Cox-2, CD68 (human macrophage marker) or OX42 (rat microglial marker), and neurofilaments (NF), prior to image analysis, from the following: human brachial plexus nerves (21 to 196 days post-injury), painful neuromas (9 days to 12 years post-injury), avulsion injured DRG, control nerves and DRG, and rat CCI model tissues. EP1 and NF-immunoreactive nerve fibres were quantified by image analysis. RESULTS: EP1:NF ratio was significantly increased in human brachial plexus nerve fibres, both proximal and distal to injury, in comparison with uninjured nerves. Sensory neurones in injured human DRG showed a significant acute increase of EP1-IR intensity. While there was a rapid increase in EP1-fibres and CD-68 positive macrophages, Cox-2 increase was apparent later, but was persistent in human painful neuromas for years. A similar time-course of changes was found in the rat CCI model with the above markers, both in the injured nerves and ipsilateral dorsal spinal cord. CONCLUSION: Different stages of infiltration and activation of macrophages may be observed in the peripheral and central nervous system following peripheral nerve injury. EP1 receptor level increase in sensory neurones, and macrophage infiltration, appears to precede increased Cox-2 expression by macrophages. However, other methods for detecting Cox-2 levels and activity are required. EP1 antagonists may show therapeutic effects in acute and chronic neuropathic pain, in addition to inflammatory pain. BioMed Central 2006-01-04 /pmc/articles/PMC1361784/ /pubmed/16393343 http://dx.doi.org/10.1186/1471-2377-6-1 Text en Copyright © 2006 Durrenberger et al; licensee BioMed Central Ltd.
spellingShingle Research Article
Durrenberger, Pascal F
Facer, Paul
Casula, Maria A
Yiangou, Yiangos
Gray, Roy A
Chessell, Iain P
Day, Nicola C
Collins, Sue D
Bingham, Sharon
Wilson, Alex W
Elliot, David
Birch, Rolfe
Anand, Praveen
Prostanoid receptor EP1 and Cox-2 in injured human nerves and a rat model of nerve injury: a time-course study
title Prostanoid receptor EP1 and Cox-2 in injured human nerves and a rat model of nerve injury: a time-course study
title_full Prostanoid receptor EP1 and Cox-2 in injured human nerves and a rat model of nerve injury: a time-course study
title_fullStr Prostanoid receptor EP1 and Cox-2 in injured human nerves and a rat model of nerve injury: a time-course study
title_full_unstemmed Prostanoid receptor EP1 and Cox-2 in injured human nerves and a rat model of nerve injury: a time-course study
title_short Prostanoid receptor EP1 and Cox-2 in injured human nerves and a rat model of nerve injury: a time-course study
title_sort prostanoid receptor ep1 and cox-2 in injured human nerves and a rat model of nerve injury: a time-course study
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1361784/
https://www.ncbi.nlm.nih.gov/pubmed/16393343
http://dx.doi.org/10.1186/1471-2377-6-1
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