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Homers at the Interface between Reward and Pain

Pain alters opioid reinforcement, presumably via neuroadaptations within ascending pain pathways interacting with the limbic system. Nerve injury increases expression of glutamate receptors and their associated Homer scaffolding proteins throughout the pain processing pathway. Homer proteins, and th...

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Autores principales: Obara, Ilona, Goulding, Scott P., Gould, Adam T., Lominac, Kevin D., Hu, Jia-Hua, Zhang, Ping Wu, von Jonquieres, Georg, Dehoff, Marlin, Xiao, Bo, Seeburg, Peter H., Worley, Paul F., Klugmann, Matthias, Szumlinski, Karen K.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3675508/
https://www.ncbi.nlm.nih.gov/pubmed/23761764
http://dx.doi.org/10.3389/fpsyt.2013.00039
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author Obara, Ilona
Goulding, Scott P.
Gould, Adam T.
Lominac, Kevin D.
Hu, Jia-Hua
Zhang, Ping Wu
von Jonquieres, Georg
Dehoff, Marlin
Xiao, Bo
Seeburg, Peter H.
Worley, Paul F.
Klugmann, Matthias
Szumlinski, Karen K.
author_facet Obara, Ilona
Goulding, Scott P.
Gould, Adam T.
Lominac, Kevin D.
Hu, Jia-Hua
Zhang, Ping Wu
von Jonquieres, Georg
Dehoff, Marlin
Xiao, Bo
Seeburg, Peter H.
Worley, Paul F.
Klugmann, Matthias
Szumlinski, Karen K.
author_sort Obara, Ilona
collection PubMed
description Pain alters opioid reinforcement, presumably via neuroadaptations within ascending pain pathways interacting with the limbic system. Nerve injury increases expression of glutamate receptors and their associated Homer scaffolding proteins throughout the pain processing pathway. Homer proteins, and their associated glutamate receptors, regulate behavioral sensitivity to various addictive drugs. Thus, we investigated a potential role for Homers in the interactions between pain and drug reward in mice. Chronic constriction injury (CCI) of the sciatic nerve elevated Homer1b/c and/or Homer2a/b expression within all mesolimbic structures examined and for the most part, the Homer increases coincided with elevated mGluR5, GluN2A/B, and the activational state of various down-stream kinases. Behaviorally, CCI mice showed pain hypersensitivity and a conditioned place-aversion (CPA) at a low heroin dose that supported conditioned place-preference (CPP) in naïve controls. Null mutations of Homer1a, Homer1, and Homer2, as well as transgenic disruption of mGluR5-Homer interactions, either attenuated or completely blocked low-dose heroin CPP, and none of the CCI mutant strains exhibited heroin-induced CPA. However, heroin CPP did not depend upon full Homer1c expression within the nucleus accumbens (NAC), as CPP occurred in controls infused locally with small hairpin RNA-Homer1c, although intra-NAC and/or intrathecal cDNA-Homer1c, -Homer1a, and -Homer2b infusions (to best mimic CCI’s effects) were sufficient to blunt heroin CPP in uninjured mice. However, arguing against a simple role for CCI-induced increases in either spinal or NAC Homer expression for heroin CPA, cDNA infusion of our various cDNA constructs either did not affect (intrathecal) or attenuated (NAC) heroin CPA. Together, these data implicate increases in glutamate receptor/Homer/kinase activity within limbic structures, perhaps outside the NAC, as possibly critical for switching the incentive motivational properties of heroin following nerve injury, which has relevance for opioid psychopharmacology in individuals suffering from neuropathic pain.
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spelling pubmed-36755082013-06-11 Homers at the Interface between Reward and Pain Obara, Ilona Goulding, Scott P. Gould, Adam T. Lominac, Kevin D. Hu, Jia-Hua Zhang, Ping Wu von Jonquieres, Georg Dehoff, Marlin Xiao, Bo Seeburg, Peter H. Worley, Paul F. Klugmann, Matthias Szumlinski, Karen K. Front Psychiatry Psychiatry Pain alters opioid reinforcement, presumably via neuroadaptations within ascending pain pathways interacting with the limbic system. Nerve injury increases expression of glutamate receptors and their associated Homer scaffolding proteins throughout the pain processing pathway. Homer proteins, and their associated glutamate receptors, regulate behavioral sensitivity to various addictive drugs. Thus, we investigated a potential role for Homers in the interactions between pain and drug reward in mice. Chronic constriction injury (CCI) of the sciatic nerve elevated Homer1b/c and/or Homer2a/b expression within all mesolimbic structures examined and for the most part, the Homer increases coincided with elevated mGluR5, GluN2A/B, and the activational state of various down-stream kinases. Behaviorally, CCI mice showed pain hypersensitivity and a conditioned place-aversion (CPA) at a low heroin dose that supported conditioned place-preference (CPP) in naïve controls. Null mutations of Homer1a, Homer1, and Homer2, as well as transgenic disruption of mGluR5-Homer interactions, either attenuated or completely blocked low-dose heroin CPP, and none of the CCI mutant strains exhibited heroin-induced CPA. However, heroin CPP did not depend upon full Homer1c expression within the nucleus accumbens (NAC), as CPP occurred in controls infused locally with small hairpin RNA-Homer1c, although intra-NAC and/or intrathecal cDNA-Homer1c, -Homer1a, and -Homer2b infusions (to best mimic CCI’s effects) were sufficient to blunt heroin CPP in uninjured mice. However, arguing against a simple role for CCI-induced increases in either spinal or NAC Homer expression for heroin CPA, cDNA infusion of our various cDNA constructs either did not affect (intrathecal) or attenuated (NAC) heroin CPA. Together, these data implicate increases in glutamate receptor/Homer/kinase activity within limbic structures, perhaps outside the NAC, as possibly critical for switching the incentive motivational properties of heroin following nerve injury, which has relevance for opioid psychopharmacology in individuals suffering from neuropathic pain. Frontiers Media S.A. 2013-06-07 /pmc/articles/PMC3675508/ /pubmed/23761764 http://dx.doi.org/10.3389/fpsyt.2013.00039 Text en Copyright © 2013 Obara, Goulding, Gould, Lominac, Hu, Zhang, von Jonquieres, Dehoff, Xiao, Seeburg, Worley, Klugmann and Szumlinski. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits use, distribution and reproduction in other forums, provided the original authors and source are credited and subject to any copyright notices concerning any third-party graphics etc.
spellingShingle Psychiatry
Obara, Ilona
Goulding, Scott P.
Gould, Adam T.
Lominac, Kevin D.
Hu, Jia-Hua
Zhang, Ping Wu
von Jonquieres, Georg
Dehoff, Marlin
Xiao, Bo
Seeburg, Peter H.
Worley, Paul F.
Klugmann, Matthias
Szumlinski, Karen K.
Homers at the Interface between Reward and Pain
title Homers at the Interface between Reward and Pain
title_full Homers at the Interface between Reward and Pain
title_fullStr Homers at the Interface between Reward and Pain
title_full_unstemmed Homers at the Interface between Reward and Pain
title_short Homers at the Interface between Reward and Pain
title_sort homers at the interface between reward and pain
topic Psychiatry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3675508/
https://www.ncbi.nlm.nih.gov/pubmed/23761764
http://dx.doi.org/10.3389/fpsyt.2013.00039
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