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眶额皮质亚区抑制 binge 样和抗厌恶酒精摄入。

Orbitofrontal cortex subregion inhibition during binge-like and aversion-resistant alcohol drinking.

机构信息

Department of Psychology and Center for Neuroscience and Behavior, Miami University, Oxford, OH, United States.

Department of Psychology and Center for Neuroscience and Behavior, Miami University, Oxford, OH, United States.

出版信息

Alcohol. 2022 Mar;99:1-8. doi: 10.1016/j.alcohol.2021.11.004. Epub 2021 Dec 1.

Abstract

Two important contributors to alcohol-related problems and alcohol use disorder (AUD) are binge- and compulsive-like drinking. The orbitofrontal cortex (OFC), a brain region implicated in outcome valuation and behavioral flexibility, is functionally altered by alcohol exposure. Data from animal models also suggest that both the medial (mOFC) and lateral (lOFC) subregions of the OFC regulate alcohol-related behaviors. The current study was designed to examine the contributions of mOFC and lOFC using a model of binge-like and aversion-resistant ethanol drinking in C57BL/6J male and female mice. The inhibitory Designer Receptor Exclusively Activated by Designer Drugs (DREADD) hM4Di were used to inhibit neurons in either the mOFC or the lOFC in mice drinking 15% ethanol in a two-bottle, limited-access, modified drinking in the dark paradigm. The effects of chemogenetic inhibition on consumption of quinine-adulterated ethanol, water, and water + quinine were also assessed. Inhibiting the mOFC did not alter consumption of ethanol or aversion-resistant drinking of ethanol + quinine. In contrast, inhibition of neurons in the lOFC increased consumption, but not preference, of ethanol alone. mOFC and lOFC inhibition did not alter water or quinine-adulterated water intake, indicating the effects shown here are specific to ethanol drinking. These data support the role of the lOFC in regulating alcohol consumption but fail to find a similar role for mOFC.

摘要

两种重要的导致酒精相关问题和酒精使用障碍(AUD)的因素是 binge 和强迫样饮酒。眶额叶皮层(OFC)是一个与结果评估和行为灵活性有关的大脑区域,其功能会因酒精暴露而改变。动物模型的数据还表明,OFC 的内侧(mOFC)和外侧(lOFC)亚区都调节与酒精相关的行为。本研究旨在使用 C57BL/6J 雄性和雌性小鼠 binge 样和回避抵抗性乙醇饮用量表,来研究 mOFC 和 lOFC 的作用。使用 Designer Receptor Exclusively Activated by Designer Drugs(DREADD)hM4Di 抑制 mOFC 或 lOFC 中的神经元,在双瓶、有限接入、改良的暗箱饮酒模型中,让小鼠饮用 15%乙醇。还评估了化学遗传抑制对含奎宁的乙醇、水和水+奎宁的影响。抑制 mOFC 不会改变乙醇的消耗或回避抵抗性的乙醇+奎宁的消耗。相比之下,抑制 lOFC 中的神经元会增加乙醇的消耗,但不会增加乙醇的偏好。mOFC 和 lOFC 的抑制都不会改变水或含奎宁的水的摄入,表明这里显示的影响是特异性针对乙醇摄入的。这些数据支持 lOFC 在调节酒精消耗中的作用,但没有发现 mOFC 有类似的作用。

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