Ethanol Potentiation of GABAergic Synaptic Transmission May Be Self-Limiting: Role of Presynaptic GABAB Receptors
TLDR
It is demonstrated that, at perisomatic synapses in the rat hippocampus, ethanol enhances presynaptic GABAB autoreceptor function and that this interaction reduces the overall potentiating effect of ethanol at these synapses, suggesting that an interaction between ethanol and presynptic GABABAutoreceptor activity regulates the ethanol sensitivity of GABAergic synapses.Abstract:
Ethanol enhances GABAergic synaptic inhibition, and this interaction contributes to many of the behavioral and cognitive effects of this drug. Most studies suggest that ethanol enhances GABAergic neurotransmission via an allosteric potentiation of the postsynaptic GABA(A) receptors that mediate fast synaptic inhibition in the mammalian CNS. Despite widespread acceptance of this hypothesis, direct support for such a mechanism has been difficult to obtain. Ethanol does not enhance GABA(A) receptor function in all brain regions or under all experimental conditions, and factors responsible for this variability remain mostly unknown. Notably, blockade of GABA(B) receptors dramatically enhances ethanol potentiation of hippocampal GABA(A) IPSPs and IPSCs, suggesting that some unknown GABA(B) receptor mechanism limits the overall potentiating effect of ethanol on GABAergic synapses. In this study, we demonstrate that, at perisomatic synapses in the rat hippocampus, ethanol enhances presynaptic GABA(B) autoreceptor function and that this interaction reduces the overall potentiating effect of ethanol at these synapses. We further show that ethanol significantly elevates basal presynaptic GABA(B) receptor tone, possibly via an increase in spontaneous GABA release, and that pretreatment with a subthreshold concentration of the GABA(B) receptor agonist baclofen blocks ethanol but not flunitrazepam or pentobarbital potentiation of GABA(A) IPSCs. These data suggest that an interaction between ethanol and presynaptic GABA(B) autoreceptor activity regulates the ethanol sensitivity of GABAergic synapses. Given that the in vitro ethanol sensitivity of these synapses correlates with in vivo ethanol responsiveness in a number of rodent lines, our data further suggest that presynaptic GABA(B) receptor activity may play a role in regulating behavioral sensitivity to ethanol.read more
Citations
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The role of GABA(A) receptors in the acute and chronic effects of ethanol: a decade of progress.
Sandeep Kumar,Patrizia Porcu,David F. Werner,Douglas B. Matthews,Jaime L. Diaz-Granados,Rebecca S. Helfand,A. Leslie Morrow +6 more
TL;DR: The elucidation of the mechanisms that underlie adaptations to ethanol exposure are leading to a better understanding of the regulation of inhibitory transmission and new targets for therapies to support recovery from ethanol withdrawal and alcoholism.
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Withdrawal from chronic intermittent ethanol treatment changes subunit composition, reduces synaptic function, and decreases behavioral responses to positive allosteric modulators of GABAA receptors.
TL;DR: Data suggest that specific alterations in GABAR occur after CIE and may underlie the development of hyperexcitability and ethanol dependence.
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Alcohol and the Brain: Neuronal Molecular Targets, Synapses, and Circuits
TL;DR: This review highlights current progress in the field of ethanol use and abuse, focusing on recent and emerging molecular, cellular, and circuit effects of the drug that impact ethanol-related behaviors.
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Ethanol modulation of GABAergic transmission: The view from the slice
Jeff L. Weiner,C. F. Valenzuela +1 more
TL;DR: A focused review of recent evidence from in vitro brain slice electrophysiological studies offers new insight into the mechanisms through which acute and chronic ethanol exposures modulate the activity of GABAergic synapses.
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The γ-Aminobutyric Acid-B Receptor Agonist Baclofen Attenuates Responding for Ethanol in Ethanol-Dependent Rats
Brendan M. Walker,George F. Koob +1 more
TL;DR: The present experiment suggests that the GABA(B) receptor could be a potential pharmacotherapeutic target for the treatment of chronic alcoholism by producing increased self-administration of ethanol as reflected in increased ethanol intake and increased responding on a PR schedule of reinforcement.
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