Galanin Protects Against Behavioral and Neurochemical Correlates of Opiate Reward

Hawes, Jessica J.; Brunzell, Darlene H.; Narasimhaiah, Roopashree; Langel, Ülo; Wynick, David; Picciotto, Marina R.

doi:10.1038/sj.npp.1301579

Cited by 51 publications

(69 citation statements)

References 59 publications

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“…Similarly, leptin (15, 16, 34 -36, 41), galanin (21,52), neurotensin (6,17,23,30), and CART (29,31,51) have all been associated with the control of reward as well as arousal behavior. Indeed, neurotensin-LepRb neurons modulate the reward system via orexin neurons, although it is still unknown by which mechanisms leptin inhibits orexin neurons (40).…”

Section: Discussionmentioning

confidence: 99%

Leptin receptor neurons in the mouse hypothalamus are colocalized with the neuropeptide galanin and mediate anorexigenic leptin action

Laque

Zhang²,

Gettys³

et al. 2013

American Journal of Physiology-Endocrinology and Metabolism

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Section: Discussionmentioning

confidence: 99%

Leptin receptor neurons in the mouse hypothalamus are colocalized with the neuropeptide galanin and mediate anorexigenic leptin action

Laque

Zhang²,

Gettys³

et al. 2013

American Journal of Physiology-Endocrinology and Metabolism

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“…Local administration of galanin into the cerebral ventricle attenuates the rewarding effect of morphine in the mouse as measured by the place preference paradigm by shifting the dose response curve such that threshold doses are no longer rewarding in animals receiving galanin [1]. Consistent with the possibility that galanin signaling opposes opiate reward, galanin knockout mice showed increased sensitivity to a low dose of morphine in the place preference paradigm compared to their wild-type controls [11]. The effect of galanin on morphine-induced locomotion and morphine place preference occurred at very different doses, since at the threshold dose for morphine place preference (0.25 mg/kg), no locomotor activation was seen.…”

Section: Introductionmentioning

confidence: 86%

“…Indeed, inhibition of ERK phosphorylation in the VTA blocks the rewarding effects of morphine [58]. Morphine induces a significant increase in the activity of ERK in the VTA, NAc and amygdala of both galanin wild-type and knockout animals, but the increase is significantly greater in knockout mice lacking the galanin peptide [11]. In the VTA, galnon administration decreased morphine-induced ERK phosphorylation in both wild-type and galanin knockout mice, suggesting that activation of galanin receptors in the VTA can attenuate activity of DA neurons and decrease signaling related to opiate reward; however, the decrease in P-ERK by galnon was not complete, suggesting that morphine also regulates ERK activity independent of the galanin system.…”

Section: Regulation Of the Dopaminergic And Cholinergic Systems By Gamentioning

confidence: 98%

“…This compound has been useful for determining whether behavioral changes in galanin knockout mice are due to adaptation to the loss of the peptide during development or acute effects of galanin in the adult behaving animal. Galnon administration was able to reverse the morphine-induced increase in locomotor activation seen in galanin knockout mice, suggesting that even in the absence of galanin signaling throughout development, replacement of galanin action in adulthood could normalize morphine-induced locomotor activation [11]. Conditioned place preference is a contextual task that is thought to measure drug reward and drug seeking [14].…”

Section: Introductionmentioning

confidence: 99%

“…Thus, locomotor activation can provide a behavioral measure of sensitivity to drugs of abuse. Interestingly, knockout mice lacking the galanin peptide show increased locomotor responses to morphine across a number of doses compared to their wild-type controls [11]. Galnon is a non-peptide galanin receptor agonist that can cross the blood-brain barrier [12,13].…”

Section: Introductionmentioning

confidence: 99%

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Galanin – 25 years with a multitalented neuropeptide

Picciotto

2008

Cell. Mol. Life Sci.

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There has been increasing interest in the ability of neuropeptides involved in feeding to modulate circuits important for responses to drugs of abuse. A number of peptides with effects on hypothalamic function also modulate the mesolimbic dopamine system (ventral tegmental area and nucleus accumbens). Similarly, common stress-related pathways can modulate food intake, drug reward and symptoms of drug withdrawal. Galanin promotes food intake and the analgesic properties of opiates; thus it initially seemed possible that galanin might potentiate opiate reinforcement. Instead, galanin agonists decrease opiate reward, measured by conditioned place preference, and opiate withdrawal signs, whereas opiate reward and withdrawal are increased in knock-out mice lacking galanin. This is consistent with studies showing that galanin decreases activity-evoked dopamine release in striatal slices and decreases the firing rate of noradrenergic neurons in locus coeruleus, areas involved in drug reward and withdrawal, respectively. These data suggest that polymorphisms in genes encoding galanin or galanin receptors might be associated with susceptibility to opiate abuse. Further, galanin receptors might be potential targets for development of novel treatments for addiction.

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Galanin and Addiction

Picciotto

2010

Experientia Supplementum

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Galanin Protects Against Behavioral and Neurochemical Correlates of Opiate Reward

Cited by 51 publications

References 59 publications

Leptin receptor neurons in the mouse hypothalamus are colocalized with the neuropeptide galanin and mediate anorexigenic leptin action

Leptin receptor neurons in the mouse hypothalamus are colocalized with the neuropeptide galanin and mediate anorexigenic leptin action

Galanin – 25 years with a multitalented neuropeptide

Galanin and Addiction

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