Opioid-Induced central immune signaling: Implications for opioid analgesia

Peter M. Grace; Steven F. Maier; Linda R. Watkins

doi:10.1111/head.12552

Opioid-Induced central immune signaling: Implications for opioid analgesia

Peter M. Grace, Steven F. Maier, Linda R. Watkins

Research output: Contribution to journal › Review article › peer-review

73 Scopus citations

Abstract

Despite being the mainstay of pain management, opioids are limited in their clinical utility by adverse effects, such as tolerance and paradoxical hyperalgesia. Research of the past 15 years has extended beyond neurons, to implicate central nervous system immune signaling in these adverse effects. This article will provide an overview of these central immune mechanisms in opioid tolerance and paradoxical hyperalgesia, including those mediated by Toll-like receptor 4, purinergic, ceramide, and chemokine signaling. Challenges for the future, as well as new lines of investigation will be highlighted.

Original language	English (US)
Pages (from-to)	475-489
Number of pages	15
Journal	Headache
Volume	55
Issue number	4
DOIs	https://doi.org/10.1111/head.12552
State	Published - Apr 1 2015
Externally published	Yes

Keywords

P2X4 receptor
P2X7 receptor
TLR4
allodynia
hyperalgesia
opioid receptor

ASJC Scopus subject areas

Neurology
Clinical Neurology

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10.1111/head.12552

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title = "Opioid-Induced central immune signaling: Implications for opioid analgesia",

abstract = "Despite being the mainstay of pain management, opioids are limited in their clinical utility by adverse effects, such as tolerance and paradoxical hyperalgesia. Research of the past 15 years has extended beyond neurons, to implicate central nervous system immune signaling in these adverse effects. This article will provide an overview of these central immune mechanisms in opioid tolerance and paradoxical hyperalgesia, including those mediated by Toll-like receptor 4, purinergic, ceramide, and chemokine signaling. Challenges for the future, as well as new lines of investigation will be highlighted.",

keywords = "P2X4 receptor, P2X7 receptor, TLR4, allodynia, hyperalgesia, opioid receptor",

author = "Grace, {Peter M.} and Maier, {Steven F.} and Watkins, {Linda R.}",

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T2 - Implications for opioid analgesia

AU - Grace, Peter M.

AU - Maier, Steven F.

AU - Watkins, Linda R.

PY - 2015/4/1

Y1 - 2015/4/1

N2 - Despite being the mainstay of pain management, opioids are limited in their clinical utility by adverse effects, such as tolerance and paradoxical hyperalgesia. Research of the past 15 years has extended beyond neurons, to implicate central nervous system immune signaling in these adverse effects. This article will provide an overview of these central immune mechanisms in opioid tolerance and paradoxical hyperalgesia, including those mediated by Toll-like receptor 4, purinergic, ceramide, and chemokine signaling. Challenges for the future, as well as new lines of investigation will be highlighted.

AB - Despite being the mainstay of pain management, opioids are limited in their clinical utility by adverse effects, such as tolerance and paradoxical hyperalgesia. Research of the past 15 years has extended beyond neurons, to implicate central nervous system immune signaling in these adverse effects. This article will provide an overview of these central immune mechanisms in opioid tolerance and paradoxical hyperalgesia, including those mediated by Toll-like receptor 4, purinergic, ceramide, and chemokine signaling. Challenges for the future, as well as new lines of investigation will be highlighted.

KW - P2X4 receptor

KW - P2X7 receptor

KW - TLR4

KW - allodynia

KW - hyperalgesia

KW - opioid receptor

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EP - 489

JO - Headache

JF - Headache

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ER -

Opioid-Induced central immune signaling: Implications for opioid analgesia

Abstract

Keywords

ASJC Scopus subject areas

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