Alcohol consumption does not impact delta and kappa opioid receptor-mediated synaptic depression in dorsolateral striatum of adult male mice

IF 2.5 4区医学 Q3 PHARMACOLOGY & PHARMACY

Alcohol Pub Date : 2024-06-08 DOI:10.1016/j.alcohol.2024.06.002

Braulio Muñoz , Brady K. Atwood

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引用次数: 0

Abstract

Many drugs of abuse, including alcohol, disrupt long-term synaptic depression (LTD) at dorsal striatal glutamate synapses. This disruption is common to many forms of LTD that are mediated by G protein coupled receptors (GPCRs) that signal through the inhibitory G_i/o class of G proteins. A loss of LTD is thought to mediate behavioral changes associated with the development of substance use disorders. We have previously shown in multiple studies that LTD mediated by the G_i/o-coupled mu opioid receptor is disrupted by in vivo opioid and alcohol exposure in adolescent and adult mice. One of our previous studies suggested that LTD mediated by delta and kappa opioid receptors was resistant to the LTD-disrupting properties of in vivo opioid exposure. We hypothesized that delta and kappa opioid receptor-mediated LTD would be exceptions to the generalizable observation that forms of dorsal striatal G_i/o-coupled receptor LTD are disrupted by drugs of abuse. Specifically, we predicted that these forms of LTD would be resistant to the deleterious effects of alcohol consumption, just as they were resistant to opioid exposure. Indeed, in adult male mice that drank alcohol for 3 weeks, delta and kappa opioid receptor-mediated LTD at glutamatergic inputs to direct pathway and indirect pathway medium spiny neurons in the dorsolateral striatum was unaffected by alcohol. These data demonstrate that alcohol effects on GPCR-mediated LTD are not generalizable across all types of G_i/o-coupled GPCRs.

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饮酒不会影响成年雄性小鼠背外侧纹状体中 delta 和 kappa 阿片受体介导的突触抑制。

包括酒精在内的许多滥用药物会破坏背侧纹状体谷氨酸突触的长期突触抑制（LTD）。这种破坏是由 G 蛋白偶联受体（GPCR）介导的多种形式的突触抑制所共有的，GPCR 通过抑制性的 Gi/o 类 G 蛋白发出信号。据认为，LTD 的缺失介导了与药物使用障碍发展相关的行为变化。我们之前的多项研究表明，青少年和成年小鼠体内阿片类药物和酒精暴露会破坏由Gi/o偶联μ阿片受体介导的LTD。我们之前的一项研究表明，由 delta 和 kappa 阿片受体介导的 LTD 不受体内阿片暴露的 LTD 破坏特性的影响。我们假设，δ和卡帕阿片受体介导的LTD将是可普遍观察到的背纹状体Gi/o偶联受体LTD形式被滥用药物破坏的例外情况。具体来说，我们预测这些形式的LTD会抵制饮酒的有害影响，就像它们抵制阿片类药物暴露一样。事实上，在连续饮酒 3 周的成年雄性小鼠中，背外侧纹状体中直接通路和间接通路中刺神经元的谷氨酸能输入的 delta 和 kappa 阿片受体介导的 LTD 不受酒精的影响。这些数据表明，酒精对 GPCR 介导的 LTD 的影响并不能普遍适用于所有类型的 Gi/o 偶联 GPCR。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Alcohol 医学-毒理学

CiteScore

4.60

自引率

4.30%

发文量

审稿时长

15.6 weeks

期刊介绍： Alcohol is an international, peer-reviewed journal that is devoted to publishing multi-disciplinary biomedical research on all aspects of the actions or effects of alcohol on the nervous system or on other organ systems. Emphasis is given to studies into the causes and consequences of alcohol abuse and alcoholism, and biomedical aspects of diagnosis, etiology, treatment or prevention of alcohol-related health effects. Intended for both research scientists and practicing clinicians, the journal publishes original research on the neurobiological, neurobehavioral, and pathophysiological processes associated with alcohol drinking, alcohol abuse, alcohol-seeking behavior, tolerance, dependence, withdrawal, protracted abstinence, and relapse. In addition, the journal reports studies on the effects alcohol on brain mechanisms of neuroplasticity over the life span, biological factors associated with adolescent alcohol abuse, pharmacotherapeutic strategies in the treatment of alcoholism, biological and biochemical markers of alcohol abuse and alcoholism, pathological effects of uncontrolled drinking, biomedical and molecular factors in the effects on liver, immune system, and other organ systems, and biomedical aspects of fetal alcohol spectrum disorder including mechanisms of damage, diagnosis and early detection, treatment, and prevention. Articles are published from all levels of biomedical inquiry, including the following: molecular and cellular studies of alcohol''s actions in vitro and in vivo; animal model studies of genetic, pharmacological, behavioral, developmental or pathophysiological aspects of alcohol; human studies of genetic, behavioral, cognitive, neuroimaging, or pathological aspects of alcohol drinking; clinical studies of diagnosis (including dual diagnosis), treatment, prevention, and epidemiology. The journal will publish 9 issues per year; the accepted abbreviation for Alcohol for bibliographic citation is Alcohol.