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后腹侧被盖区而非前腹侧被盖区的 GABAA 受体介导 Ro15-4513 减轻 C57BL/6J 雌性小鼠 binge 样乙醇消耗。

GABAA receptors in the posterior, but not anterior, ventral tegmental area mediate Ro15-4513-induced attenuation of binge-like ethanol consumption in C57BL/6J female mice.

机构信息

Psychobiology of Addictions, Department of Psychology, Indiana University/Purdue University-Indianapolis, Indianapolis, IN 46202, USA.

出版信息

Behav Brain Res. 2011 Jun 20;220(1):230-7. doi: 10.1016/j.bbr.2011.02.014. Epub 2011 Feb 12.

DOI:10.1016/j.bbr.2011.02.014
PMID:21320533
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3070426/
Abstract

GABA(A) receptors have been shown to modulate dopaminergic output from the ventral tegmental area (VTA) in studies of both natural and drug rewards, including alcohol. Ro15-4513, the imidazobenzodiazepine derivative and allosteric modulator at the GABA(A) receptor, reliably antagonizes the behavioral effects of alcohol. Various models of alcohol consumption show a decrease in consummatory behaviors, specific to ethanol, following acute administration of the drug. In the present study, Ro15-4513 was systemically administered, or microinjected into the anterior or posterior VTA, to explore the role of GABA(A) receptors at this region in modulating the high pattern of alcohol consumption by C57BL/6J inbred mice in the Drinking in the Dark (DID) model. Animals had 2h access to ethanol for 6 days prior to drug manipulations. Immediately before the seventh day of access, mice were systemically (I.P.) or site-specifically administered Ro15-4513. Systemic Ro15-4513 (at 10mg/kg) decreased binge-like ethanol intake in the DID paradigm. Additionally, there was a stepwise decrease in consumption following Ro15-4513 microinjection into the posterior VTA, with the highest dose significantly decreasing ethanol intake. There was no effect found following microinjection into the anterior VTA, nor was there an effect of systemic or intra-posterior VTA Ro15-4513 on consumption of a 5% sucrose solution or water. The present findings support a role for Ro15-4513 sensitive VTA-GABA(A) receptors in modulating binge-like ethanol consumption. Moreover, the work here adds to the growing body of literature suggesting regional heterogeneity in the VTA.

摘要

GABA(A) 受体已被证明在自然和药物奖赏(包括酒精)的研究中调节腹侧被盖区(VTA)的多巴胺能输出。Ro15-4513 是咪唑并苯并二氮杂䓬衍生物和 GABA(A) 受体的别构调节剂,可靠地拮抗酒精的行为效应。各种酒精消费模型显示,在药物急性给药后,对乙醇的消耗行为会减少。在本研究中,全身性给予 Ro15-4513,或在前或后 VTA 中微注射,以探讨 GABA(A) 受体在调节 C57BL/6J 近交系小鼠在暗饮(DID)模型中高酒精消费模式中的作用。动物在药物操作前有 6 天 2 小时接触乙醇。在第七天接触之前,立即对小鼠进行全身性(IP)或特异性给予 Ro15-4513。全身性 Ro15-4513(10mg/kg)降低了 DID 范式中的 binge-like 乙醇摄入。此外,在 Ro15-4513 微注射到后 VTA 后,消费呈逐步下降,最高剂量显著降低了乙醇摄入。在前 VTA 微注射后没有发现影响,也没有发现全身性或 VTA 后 Ro15-4513 对 5%蔗糖溶液或水的消费有影响。本研究结果支持 Ro15-4513 敏感的 VTA-GABA(A) 受体在调节 binge-like 乙醇消费中的作用。此外,这里的工作增加了越来越多的文献表明 VTA 存在区域异质性。

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本文引用的文献

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Extrasynaptic GABAA receptors: form, pharmacology, and function.突触外GABAA受体:形态、药理学及功能
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外侧隔社交经验和性别依赖性调节通过 extrasynaptic δGABA 受体的攻击性。
Psychopharmacology (Berl). 2020 Feb;237(2):329-344. doi: 10.1007/s00213-019-05368-z. Epub 2019 Nov 6.
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Sex and β-Endorphin Influence the Effects of Ethanol on Limbic Expression in a Mouse Binge Drinking Model.性别和β-内啡肽对小鼠暴饮模型中乙醇对边缘系统表达的影响
Front Genet. 2018 Nov 29;9:567. doi: 10.3389/fgene.2018.00567. eCollection 2018.
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