Extrasynaptic Glycine Receptors of Rodent Dorsal Raphe Serotonergic Neurons: A Sensitive Target for Ethanol

被引:0
|
作者
Edward P Maguire
Elizabeth A Mitchell
Scott J Greig
Nicole Corteen
David J K Balfour
Jerome D Swinny
Jeremy J Lambert
Delia Belelli
机构
[1] Medical Research Institute,Division of Neuroscience
[2] Ninewells Hospital and Medical School,undefined
[3] Dundee University,undefined
[4] Institute for Biomedical and Biomolecular Sciences,undefined
[5] School of Pharmacy and Biomedical Sciences,undefined
[6] University of Portsmouth,undefined
[7] 3Current address: Oxford PharmaGenesis Ltd,undefined
[8] Tubney Warren Barn,undefined
[9] Tubney,undefined
[10] Oxford OX13 5QJ,undefined
[11] UK.,undefined
来源
Neuropsychopharmacology | 2014年 / 39卷
关键词
glycine; tonic inhibition; alcohol; serotonin dorsal raphe;
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中图分类号
学科分类号
摘要
Alcohol abuse is a significant medical and social problem. Several neurotransmitter systems are implicated in ethanol’s actions, with certain receptors and ion channels emerging as putative targets. The dorsal raphe (DR) nucleus is associated with the behavioral actions of alcohol, but ethanol actions on these neurons are not well understood. Here, using immunohistochemistry and electrophysiology we characterize DR inhibitory transmission and its sensitivity to ethanol. DR neurons exhibit inhibitory ‘phasic’ post-synaptic currents mediated primarily by synaptic GABAA receptors (GABAAR) and, to a lesser extent, by synaptic glycine receptors (GlyR). In addition to such phasic transmission mediated by the vesicular release of neurotransmitter, the activity of certain neurons may be governed by a ‘tonic’ conductance resulting from ambient GABA activating extrasynaptic GABAARs. However, for DR neurons extrasynaptic GABAARs exert only a limited influence. By contrast, we report that unusually the GlyR antagonist strychnine reveals a large tonic conductance mediated by extrasynaptic GlyRs, which dominates DR inhibition. In agreement, for DR neurons strychnine increases their input resistance, induces membrane depolarization, and consequently augments their excitability. Importantly, this glycinergic conductance is greatly enhanced in a strychnine-sensitive fashion, by behaviorally relevant ethanol concentrations, by drugs used for the treatment of alcohol withdrawal, and by taurine, an ingredient of certain ‘energy drinks’ often imbibed with ethanol. These findings identify extrasynaptic GlyRs as critical regulators of DR excitability and a novel molecular target for ethanol.
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页码:1232 / 1244
页数:12
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