Ventral tegmental self‐stimulation selectively induces opioid peptide release in rat CNS

Stein, Elliot A.

doi:10.1002/syn.890130109

Cited by 15 publications

(7 citation statements)

References 65 publications

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“…Fifth, saturating concentration of a MOR agonist occludes ethanol-induced excitation of VTA DA neurons (Xiao et al, 2007), probably resulted from a maximal inhibition of GABAergic synaptic transmission. These results are in line with previous observations that ethanol increases the release of β-endorphin in the brain, which activates MORs (Stein, 1993, Herz, 1997, Marinelli et al, 2004.…”

Section: The Role Of µ-Opioid Receptors In Ethanol Inhibition Of Gabasupporting

confidence: 83%

“…Acute ethanol increases the release of β-endorphin, an endogenous ligand for MORs in the rat brain (Stein, 1993, Herz, 1997, Marinelli et al, 2004. Our recent study supports the postulation that ethanol might inhibit the activity of VTA GABAergic neurons through the activation of postsynaptic MORs following its enhancement of β-endorphin release (Xiao et al, 2007).…”

Section: Ethanol Enhanced Evoked and Spontaneous Ipsc In The Presencesupporting

confidence: 66%

“…Activation of MORs hyperpolarizes and inhibits VTA GABAergic neurons (Di Chiara and North, 1992, Johnson and North, 1992a, Margolis et al, 2003. Several lines of evidence indicate that MORs are involved in ethanol-induced excitation of VTA DA neurons: (1) ethanol enhances the release of β-endorphin in several brain regions, which activates MORs (Stein, 1993, Herz, 1997, Marinelli et al, 2004; (2) Naloxone, an opioid receptor antagonist, greatly attenuates ethanolinduced inhibition of VTA GABAergic neurons (Xiao et al, 2007); (3) Both naloxone and MOR agonist attenuated the effect of ethanol on VTA DA neurons (Xiao et al, 2007).…”

Section: Introductionmentioning

confidence: 99%

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Ethanol dually modulates GABAergic synaptic transmission onto dopaminergic neurons in ventral tegmental area: Role of μ-opioid receptors

Xia

2008

Neuroscience

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The mesolimbic dopaminergic system, originating from the ventral tegmental area (VTA) is implicated in the rewarding properties of ethanol. VTA dopaminergic neurons are under the tonic control of GABAergic innervations. Application of GABAergic agents changes ethanol consumption. However, it is unclear how acute ethanol modulates GABAergic inputs to dopaminergic neurons in the VTA. This report describes ethanol at clinically relevant concentrations (10-40 mM) dually modulates inhibitory postsynaptic currents (IPSCs). IPSCs were mediated by GABA A receptors and were recorded from VTA dopaminergic neurons in acute midbrain slices of rats. Acute application of ethanol reduced the amplitude and increased the paired pulse ratio of evoked IPSCs. Ethanol lowered the frequency but not the amplitude of spontaneous IPSCs. Nevertheless, ethanol had no effect on miniature IPSCs recorded in the presence of tetrodotoxin. These data indicate that ethanol inhibits GABAergic synaptic transmission to dopaminergic neurons by presynaptic mechanisms, and that ethanol inhibition depends on the firing of GABAergic neurons. Application of CGP 52432, a GABA B receptor antagonist did not change ethanol inhibition of IPSCs. Tyr-DAla-Gly-N-Me-Phe-Gly-ol enkephalin (DAMGO), a µ-opioid receptor agonist, conversely, silenced VTA GABAergic neurons and inhibited IPSCs. Of note, in the presence of saturating concentration of DAMGO (3 µM), ethanol potentiated the remaining IPSCs. Thus, ethanol dually modulates GABAergic transmission to dopaminergic neurons in the VTA. Ethanol modulation depends on the activity of VTA GABAergic neurons, which were inhibited by the activation of µ-opioid receptors. This dual modulation of GABAergic transmission by ethanol may be an important mechanism underlying alcohol addiction.

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Section: The Role Of µ-Opioid Receptors In Ethanol Inhibition Of Gabasupporting

confidence: 83%

Section: Ethanol Enhanced Evoked and Spontaneous Ipsc In The Presencesupporting

confidence: 66%

Section: Introductionmentioning

confidence: 99%

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Ethanol dually modulates GABAergic synaptic transmission onto dopaminergic neurons in ventral tegmental area: Role of μ-opioid receptors

Xia

2008

Neuroscience

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“…As VTA GABA neurons are the primary source of inhibitory input to VTA DA neurons, ethanol inhibition of GABA IPSCs appears to dominate over the potentiating effect of ethanol on other GABAergic or opioidergic inputs to VTA neurons. Third, ethanol enhances the release of β‐endorphin (Herz, 1997; Marinelli et al., 2004; Stein, 1993), which might activate MORs on VTA GABA neurons. Thus, acupuncture effects on VTA GABA neurons might result from combined effects on opiodergic actions on VTA GABA neurons via MORs or on accumbal GABA input to VTA GABA neurons via DORs.…”

Section: Discussionmentioning

confidence: 99%

Acupuncture Inhibits GABA Neuron Activity in the Ventral Tegmental Area and Reduces Ethanol Self‐Administration

Yang

Yoon

Hansen

et al. 2010

Alcoholism Clin & Exp Res

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Background Withdrawal from chronic ethanol enhances ventral tegmental area (VTA) GABA neuron excitability and reduces mesolimbic dopamine (DA) neurotransmission, which is suppressed by acupuncture at Shenmen (HT7) points (Zhao et al., 2006). The aim of this study was to evaluate the effects of HT7 acupuncture on VTA GABA neuron excitability, ethanol inhibition of VTA GABA neuron firing rate, and ethanol self-administration. A role for opioid receptors (ORs) in ethanol and acupuncture effects is also explored. Methods Using electrophysiological methods in mature rats, we evaluated the effects of HT7 stimulation and opioid antagonists on VTA GABA neuron firing rate. Using behavioral paradigms in rats, we evaluated the effects of HT7 stimulation and opioid antagonists on ethanol self-administration using a modification of the sucrose fading procedure. Results HT7 stimulation produced a biphasic modulation of VTA GABA neuron firing rate characterized by transient enhancement followed by inhibition and subsequent recovery in 5 min. HT7 inhibition of VTA GABA neuron firing rate was blocked by systemic administration of the non-selective μ-opioid receptor (MOR) antagonist naloxone. HT7 stimulation significantly reduced ethanol suppression of VTA GABA neuron firing rate, which was also blocked by naloxone. HT7 acupuncture reduced ethanol self-administration without affecting sucrose consumption. Systemic administration of the δ-opioid receptor (DOR) antagonist naltrindole blocked ethanol suppression of VTA GABA neuron firing rate and significantly reduced ethanol self-administration without affecting sucrose consumption. Conclusions These findings suggest that DOR-mediated opioid modulation of VTA GABA neurons may mediate acupuncture’s role in modulating mesolimbic DA release and suppressing the reinforcing effects of ethanol.

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“…Several lines of evidence indicate that ethanol's action on neurons in the VTA involves MORs. Ethanol enhances the release of β-endorphin, which activates MORs in the VTA and several other brain regions (Stein, 1993; Herz, 1997; Mendez et al, 2003; Marinelli et al, 2004; Lam et al, 2008; Jarjour et al, 2009). Selective MOR antagonists reduce ethanol consumption (Krishnan-Sarin et al, 1998; Kim et al, 2000; Hyytia and Kiianmaa, 2001; Margolis et al, 2008).…”

Section: Introductionmentioning

confidence: 99%

Ethanol Blocks Long-Term Potentiation of GABAergic Synapses in the Ventral Tegmental Area Involving μ-Opioid Receptors

Guan¹,

Ye²

2010

Neuropsychopharmacol

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It is well documented that ethanol exposure alters GABA (γ-aminobutyric acid)-releasing synapses, and ethanol addiction is associated with endogenous opioid system. Emerging evidence indicates that opioids block long-term potentiation in the fast inhibitory GABAA receptor synapses (LTPGABA) onto dopamine-containing neurons in the ventral tegmental area (VTA), a brain region essential for reward-seeking behavior. However, how ethanol affects LTPGABA is not known. We report here that in acute midbrain slices from rats, clinically relevant concentrations of ethanol applied both in vitro and in vivo prevents LTPGABA, which is reversed respectively by in vitro and in vivo administration of naloxone, a μ opioid receptor (MOR) antagonist. Furthermore, the blockade of LTPGABA induced by a brief in vitro ethanol treatment is mimicked by DAMGO ([D-Ala2, N-MePhe4, Gly-ol]-enkephalin), a MOR agonist. Pared-pulse ratios are similar in slices 24 hours after in vivo injection with either saline or ethanol. Sp-cAMPS, a stable cAMP analog, and pCPT-cGMP, a cGMP analogue potentiates GABAA-mediated IPSCs in slices from ethanol treated rats, indicating that a single in vivo ethanol exposure does not maximally increase GABA release; instead, ethanol produces a long-lasting inability to generate LTPGABA. These neuroadaptations to ethanol might contribute to early stage of addiction.

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Ventral tegmental self‐stimulation selectively induces opioid peptide release in rat CNS

Cited by 15 publications

References 65 publications

Ethanol dually modulates GABAergic synaptic transmission onto dopaminergic neurons in ventral tegmental area: Role of μ-opioid receptors

Ethanol dually modulates GABAergic synaptic transmission onto dopaminergic neurons in ventral tegmental area: Role of μ-opioid receptors

Acupuncture Inhibits GABA Neuron Activity in the Ventral Tegmental Area and Reduces Ethanol Self‐Administration

Ethanol Blocks Long-Term Potentiation of GABAergic Synapses in the Ventral Tegmental Area Involving μ-Opioid Receptors

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