Pathobiology of dynorphins in trauma and disease

Kurt F. Hauser; Jane V. Aldrich; Kevin J. Anderson; Georgy Bakalkin; MacDonald J. Christie; Edward D. Hall; Pamela E. Knapp; Stephen W. Scheff; Indrapal N. Singh; Bryce Vissel; Amina S. Woods; Tatiana Yakovleva; Toni S. Shippenberg

Pathobiology of dynorphins in trauma and disease

Kurt F. Hauser, Jane V. Aldrich, Kevin J. Anderson, Georgy Bakalkin, MacDonald J. Christie, Edward D. Hall, Pamela E. Knapp, Stephen W. Scheff, Indrapal N. Singh, Bryce Vissel, Amina S. Woods, Tatiana Yakovleva, Toni S. Shippenberg

Research output: Contribution to journal › Article › peer-review

66 Scopus citations

Abstract

Dynorphins, endogenous opioid neuropeptides derived from the prodynorphin gene, are involved in a variety of normative physiologic functions including antinociception and neuroendocrine signaling, and may be protective to neurons and oligodendroglia via their opioid receptor-mediated effects. However, under experimental or pathophysiological conditions in which dynorphin levels are substantially elevated, these peptides are excitotoxic largely through actions at glutamate receptors. Because the excitotoxic actions of dynorphins require supraphysiological concentrations or prolonged tissue exposure, there has likely been little evolutionary pressure to ameliorate the maladaptive, non-opioid receptor mediated consequences of dynorphins. Thus, dynorphins can have protective and/or proapoptotic actions in neurons and glia, and the net effect may depend upon the distribution of receptors in a particular region and the amount of dynorphin released. Increased prodynorphin gene expression is observed in several disease states and disruptions in dynorphin processing can accompany pathophysiological situations. Aberrant processing may contribute to the net negative effects of dysregulated dynorphin production by tilting the balance towards dynorphin derivatives that are toxic to neurons and/or oligodendroglia. Evidence outlined in this review suggests that a variety of CNS pathologies alter dynorphin biogenesis. Such alterations are likely maladaptive and contribute to secondary injury and the pathogenesis of disease.

Original language	English (US)
Pages (from-to)	216-235
Number of pages	20
Journal	Frontiers in bioscience : a journal and virtual library
Volume	10
Issue number	1
State	Published - 2005
Externally published	Yes

Keywords

κ-opioid receptors
AMPA
Apoptosis
Drug abuse
Excitotoxicity
Glutamate
N-methyl-D-aspartate
Neuropeptides
Neuropeptides processing
Neurotoxicity
Neurotrauma
Opioids
Pain
Review
Spinal cord injury
Striatum

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology
Biochemistry
Cell Biology

Cite this

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title = "Pathobiology of dynorphins in trauma and disease",

abstract = "Dynorphins, endogenous opioid neuropeptides derived from the prodynorphin gene, are involved in a variety of normative physiologic functions including antinociception and neuroendocrine signaling, and may be protective to neurons and oligodendroglia via their opioid receptor-mediated effects. However, under experimental or pathophysiological conditions in which dynorphin levels are substantially elevated, these peptides are excitotoxic largely through actions at glutamate receptors. Because the excitotoxic actions of dynorphins require supraphysiological concentrations or prolonged tissue exposure, there has likely been little evolutionary pressure to ameliorate the maladaptive, non-opioid receptor mediated consequences of dynorphins. Thus, dynorphins can have protective and/or proapoptotic actions in neurons and glia, and the net effect may depend upon the distribution of receptors in a particular region and the amount of dynorphin released. Increased prodynorphin gene expression is observed in several disease states and disruptions in dynorphin processing can accompany pathophysiological situations. Aberrant processing may contribute to the net negative effects of dysregulated dynorphin production by tilting the balance towards dynorphin derivatives that are toxic to neurons and/or oligodendroglia. Evidence outlined in this review suggests that a variety of CNS pathologies alter dynorphin biogenesis. Such alterations are likely maladaptive and contribute to secondary injury and the pathogenesis of disease.",

keywords = "κ-opioid receptors, AMPA, Apoptosis, Drug abuse, Excitotoxicity, Glutamate, N-methyl-D-aspartate, Neuropeptides, Neuropeptides processing, Neurotoxicity, Neurotrauma, Opioids, Pain, Review, Spinal cord injury, Striatum",

author = "Hauser, {Kurt F.} and Aldrich, {Jane V.} and Anderson, {Kevin J.} and Georgy Bakalkin and Christie, {MacDonald J.} and Hall, {Edward D.} and Knapp, {Pamela E.} and Scheff, {Stephen W.} and Singh, {Indrapal N.} and Bryce Vissel and Woods, {Amina S.} and Tatiana Yakovleva and Shippenberg, {Toni S.}",

year = "2005",

language = "English (US)",

volume = "10",

pages = "216--235",

journal = "Frontiers in bioscience : a journal and virtual library",

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publisher = "Frontiers in Bioscience",

number = "1",

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TY - JOUR

T1 - Pathobiology of dynorphins in trauma and disease

AU - Hauser, Kurt F.

AU - Aldrich, Jane V.

AU - Anderson, Kevin J.

AU - Bakalkin, Georgy

AU - Christie, MacDonald J.

AU - Hall, Edward D.

AU - Knapp, Pamela E.

AU - Scheff, Stephen W.

AU - Singh, Indrapal N.

AU - Vissel, Bryce

AU - Woods, Amina S.

AU - Yakovleva, Tatiana

AU - Shippenberg, Toni S.

PY - 2005

Y1 - 2005

N2 - Dynorphins, endogenous opioid neuropeptides derived from the prodynorphin gene, are involved in a variety of normative physiologic functions including antinociception and neuroendocrine signaling, and may be protective to neurons and oligodendroglia via their opioid receptor-mediated effects. However, under experimental or pathophysiological conditions in which dynorphin levels are substantially elevated, these peptides are excitotoxic largely through actions at glutamate receptors. Because the excitotoxic actions of dynorphins require supraphysiological concentrations or prolonged tissue exposure, there has likely been little evolutionary pressure to ameliorate the maladaptive, non-opioid receptor mediated consequences of dynorphins. Thus, dynorphins can have protective and/or proapoptotic actions in neurons and glia, and the net effect may depend upon the distribution of receptors in a particular region and the amount of dynorphin released. Increased prodynorphin gene expression is observed in several disease states and disruptions in dynorphin processing can accompany pathophysiological situations. Aberrant processing may contribute to the net negative effects of dysregulated dynorphin production by tilting the balance towards dynorphin derivatives that are toxic to neurons and/or oligodendroglia. Evidence outlined in this review suggests that a variety of CNS pathologies alter dynorphin biogenesis. Such alterations are likely maladaptive and contribute to secondary injury and the pathogenesis of disease.

AB - Dynorphins, endogenous opioid neuropeptides derived from the prodynorphin gene, are involved in a variety of normative physiologic functions including antinociception and neuroendocrine signaling, and may be protective to neurons and oligodendroglia via their opioid receptor-mediated effects. However, under experimental or pathophysiological conditions in which dynorphin levels are substantially elevated, these peptides are excitotoxic largely through actions at glutamate receptors. Because the excitotoxic actions of dynorphins require supraphysiological concentrations or prolonged tissue exposure, there has likely been little evolutionary pressure to ameliorate the maladaptive, non-opioid receptor mediated consequences of dynorphins. Thus, dynorphins can have protective and/or proapoptotic actions in neurons and glia, and the net effect may depend upon the distribution of receptors in a particular region and the amount of dynorphin released. Increased prodynorphin gene expression is observed in several disease states and disruptions in dynorphin processing can accompany pathophysiological situations. Aberrant processing may contribute to the net negative effects of dysregulated dynorphin production by tilting the balance towards dynorphin derivatives that are toxic to neurons and/or oligodendroglia. Evidence outlined in this review suggests that a variety of CNS pathologies alter dynorphin biogenesis. Such alterations are likely maladaptive and contribute to secondary injury and the pathogenesis of disease.

KW - κ-opioid receptors

KW - AMPA

KW - Apoptosis

KW - Drug abuse

KW - Excitotoxicity

KW - Glutamate

KW - N-methyl-D-aspartate

KW - Neuropeptides

KW - Neuropeptides processing

KW - Neurotoxicity

KW - Neurotrauma

KW - Opioids

KW - Pain

KW - Review

KW - Spinal cord injury

KW - Striatum

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M3 - Article

C2 - 15574363

AN - SCOPUS:20244386405

SN - 1093-9946

VL - 10

SP - 216

EP - 235

JO - Frontiers in bioscience : a journal and virtual library

JF - Frontiers in bioscience : a journal and virtual library

IS - 1

ER -

Pathobiology of dynorphins in trauma and disease

Abstract

Keywords

ASJC Scopus subject areas

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