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5HT3 受体的表观遗传和药理学调控控制小鼠强迫性乙醇觅药行为。

Epigenetic and pharmacological regulation of 5HT3 receptors controls compulsive ethanol seeking in mice.

机构信息

Department of Psychiatry, Yale University School of Medicine, 34 Park Street, Ribicoff Labs, New Haven, CT, 06519, USA.

Interdepartmental Neuroscience Program, Yale University School of Medicine, New Haven, CT, USA.

出版信息

Eur J Neurosci. 2014 Mar;39(6):999-1008. doi: 10.1111/ejn.12477. Epub 2014 Jan 21.

DOI:10.1111/ejn.12477
PMID:24772465
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4004969/
Abstract

Factors underlying individual vulnerability to develop alcoholism are largely unknown. In humans, the risk for alcoholism is associated with elevated cue reactivity. Recent evidence suggests that in animal models, reactivity to reward-paired cues is predictive of addictive behaviors. To model cue reactivity in mice, we used a Pavlovian approach (PA) paradigm in which mice were trained to associate a cue with delivery of a food reinforcer. We then investigated the relationship between PA status with habitual and compulsive-like ethanol seeking. After training mice to respond for 10% ethanol, habitual behavior was investigated using both an outcome devaluation paradigm, in which ethanol was devalued via association with lithium chloride-induced malaise, and a contingency degradation paradigm in which the relationship between action and outcome was disrupted. Compulsive-like behavior was investigated in a modified conditioned place preference paradigm in which footshock was paired with the reward-paired chamber. PA was found to be predictive of habitual and compulsive-like ethanol seeking. Additionally, innate risk status was related to epigenetic changes in the gene encoding the requisite subunit of the 5HT3 receptor, Htr3a, as well as 5HT3A protein expression in the amygdala. We then used pharmacological tools to demonstrate that risk status determines the ability of a 5HT3 antagonist to reduce compulsive ethanol seeking. These data indicate that risk status can be identified prior to any alcohol exposure by assessment of cue reactivity, and further that this endophenotype may be predictive of response to pharmacological treatment for components of alcoholism.

摘要

个体易患酒精中毒的因素在很大程度上尚不清楚。在人类中,酗酒的风险与线索反应性升高有关。最近的证据表明,在动物模型中,对与奖励相关的线索的反应性可预测成瘾行为。为了在小鼠中模拟线索反应性,我们使用了一种条件反射方法(PA)范式,其中训练小鼠将线索与食物强化物的传递相关联。然后,我们研究了 PA 状态与习惯性和强迫性样乙醇寻求之间的关系。在训练小鼠对 10%乙醇产生反应后,使用两种方法来研究习惯性行为:一种是结果贬值范式,其中通过与锂氯化物引起的不适相关联来使乙醇贬值;另一种是行为与结果之间的关系被破坏的连续降级范式。在修改后的条件性位置偏好范式中,通过将电击与奖励相关的腔室配对来研究强迫性样行为。发现 PA 可预测习惯性和强迫性样乙醇寻求。此外,内在风险状况与编码必需的 5-HT3 受体亚基 Htr3a 的基因的表观遗传变化以及杏仁核中 5-HT3A 蛋白表达有关。然后,我们使用药理学工具来证明风险状况决定了 5-HT3 拮抗剂减少强迫性乙醇寻求的能力。这些数据表明,可以通过评估线索反应性在任何酒精暴露之前识别出风险状况,并且进一步表明这种表型可能可以预测对治疗酒精中毒成分的药物治疗的反应。

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