Neuronal nicotinic acetylcholine receptor of the central amygdala modulates the ethanol-induced tolerance to anxiolysis and withdrawal-induced anxiety in male rats.

IF 1.6 4区 心理学 Q3 BEHAVIORAL SCIENCES
Behavioural Pharmacology Pub Date : 2024-04-01 Epub Date: 2024-02-22 DOI:10.1097/FBP.0000000000000770
Antariksha Duratkar, Richa Patel, Nishant Sudhir Jain
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引用次数: 0

Abstract

The nicotine acetylcholinergic receptor (nAchR) in the central nucleus of the amygdala (CeA) is known to modulate anxiety traits as well as ethanol-induced behavioral effects. Therefore, the present study investigated the role of CeA nAChR in the tolerance to ethanol anxiolysis and withdrawal-induced anxiety-related effects in rats on elevated plus maze (EPM). To develop ethanol dependence, rats were given free access to an ethanol-containing liquid diet for 10 days. To assess the development of tolerance, separate groups of rats were challenged with ethanol (2 g/kg, i.p.) on days 1, 3, 5, 7 and 10 during the period of ethanol exposure, followed by an EPM assessment. Moreover, expression of ethanol withdrawal was induced after switching ethanol-dependent rats to a liquid diet on day 11, and withdrawal-induced anxiety-like behavior was noted at different post-withdrawal time points using the EPM test. The ethanol-dependent rats were pretreated with intra-CeA (i.CeA) (bilateral) injections of nicotine (0.25 µg/rat) or mecamylamine (MEC) (5 ng/rat) before the challenge dose of ethanol on subthreshold tolerance on the 5th day or on peak tolerance day, that is, 7th or 10th, and before assessment of postwithdrawal anxiety on the 11th day on EPM. Bilateral i.CeA preadministration of nicotine before the challenge dose of ethanol on days 5, 7 and 10 exhibited enhanced tolerance, while injection of MEC, completely mitigated the tolerance to the ethanol-induced antianxiety effect. On the other hand, ethanol-withdrawn rats pretreated i.CeA with nicotine exacerbated while pretreatment with MEC, alleviated the ethanol withdrawal-induced anxiety on all time points. Thus, the present investigation indicates that stimulation of nAChR in CeA negatively modulates the ethanol-induced chronic behavioral effects on anxiety in rats. It is proposed that nAChR antagonists might be useful in the treatment of alcohol use disorder and ethanol withdrawal-related anxiety-like behavior.

杏仁核中枢的神经元烟碱乙酰胆碱受体调节乙醇诱导的雄性大鼠抗焦虑耐受性和戒断诱导的焦虑。
众所周知,杏仁核中央核(CeA)中的尼古丁乙酰胆碱能受体(nAchR)可调节焦虑特征以及乙醇诱导的行为效应。因此,本研究探讨了 CeA nAChR 在高架加迷宫(EPM)大鼠对乙醇抗焦虑耐受性和戒断诱导的焦虑相关效应中的作用。为了培养大鼠对乙醇的依赖性,研究人员让大鼠自由摄入含乙醇的液态食物 10 天。为了评估耐受性的发展情况,在乙醇暴露期间的第 1、3、5、7 和 10 天,分别给不同组的大鼠注射乙醇(2 克/千克,静脉注射),然后进行 EPM 评估。此外,在第 11 天将乙醇依赖大鼠换成流质饮食后,诱导其表现出乙醇戒断,并在戒断后的不同时间点使用 EPM 测试来观察戒断诱导的焦虑样行为。在第5天的阈下耐受日或第7天或第10天的峰值耐受日以及第11天的EPM戒断后焦虑评估前,对乙醇依赖大鼠进行阈内(i.CeA)(双侧)尼古丁(0.25 µg/鼠)或麦角胺(MEC)(5 ng/鼠)注射预处理。在第 5、7 和 10 天的乙醇挑战剂量之前,双侧 i.CeA 预先注射尼古丁会增强耐受性,而注射 MEC 则会完全减轻对乙醇诱导的抗焦虑效应的耐受性。另一方面,在所有时间点上,乙醇戒断大鼠用尼古丁预处理 i.CeA 会加剧乙醇戒断引起的焦虑,而用 MEC 预处理则会减轻乙醇戒断引起的焦虑。因此,本研究表明,刺激 CeA 中的 nAChR 可负向调节乙醇诱导的大鼠焦虑慢性行为效应。研究认为,nAChR 拮抗剂可能有助于治疗酒精使用障碍和乙醇戒断相关的焦虑样行为。
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来源期刊
Behavioural Pharmacology
Behavioural Pharmacology 医学-行为科学
CiteScore
3.40
自引率
0.00%
发文量
84
审稿时长
6-12 weeks
期刊介绍: Behavioural Pharmacology accepts original full and short research reports in diverse areas ranging from ethopharmacology to the pharmacology of schedule-controlled operant behaviour, provided that their primary focus is behavioural. Suitable topics include drug, chemical and hormonal effects on behaviour, the neurochemical mechanisms under-lying behaviour, and behavioural methods for the study of drug action. Both animal and human studies are welcome; however, studies reporting neurochemical data should have a predominantly behavioural focus, and human studies should not consist exclusively of clinical trials or case reports. Preference is given to studies that demonstrate and develop the potential of behavioural methods, and to papers reporting findings of direct relevance to clinical problems. Papers making a significant theoretical contribution are particularly welcome and, where possible and merited, space is made available for authors to explore fully the theoretical implications of their findings. Reviews of an area of the literature or at an appropriate stage in the development of an author’s own work are welcome. Commentaries in areas of current interest are also considered for publication, as are Reviews and Commentaries in areas outside behavioural pharmacology, but of importance and interest to behavioural pharmacologists. Behavioural Pharmacology publishes frequent Special Issues on current hot topics. The editors welcome correspondence about whether a paper in preparation might be suitable for inclusion in a Special Issue.
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