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中杏仁核盐皮质激素受体调节酒精自我给药。

Central amygdala mineralocorticoid receptors modulate alcohol self-administration.

机构信息

Bowles Center for Alcohol Studies, USA; Neuroscience Curriculum, USA.

Bowles Center for Alcohol Studies, USA.

出版信息

Neuropharmacology. 2020 Dec 15;181:108337. doi: 10.1016/j.neuropharm.2020.108337. Epub 2020 Sep 29.

Abstract

The mineralocorticoid receptor (MR) is an emerging target in the field of alcohol research. The MR is a steroid receptor in the same family as the glucocorticoid receptor, with which it shares the ligand corticosterone in addition to the MR selective ligand aldosterone. Recent studies have shown correlations between central amygdala (CeA) MR expression and alcohol drinking in rats and macaques, as well as correlations between aldosterone and alcohol craving in individuals with alcohol use disorder (AUD). Additionally, our previous work demonstrated that systemic treatment with the MR antagonist spironolactone reduced alcohol self-administration and response persistence in both male and female rats. This study examined if reductions in self-administration following MR antagonist treatment were related to dysregulation of MR-mediated corticosterone negative feedback. Female rats treated with spironolactone (50 mg/kg; IP) showed increased plasma corticosterone following self-administration, which correlated with reduced alcohol self-administration. Next, local microinjection of the MR-selective antagonist eplerenone was used to identify the brain-regional locus of MR action on alcohol self-administration. Eplerenone infusion produced dose-dependent reductions in alcohol self-administration in the CeA, but had no effect in the dorsal hippocampus. Finally, to assay the functional role of CeA MR expression in alcohol self-administration, CeA MR was knocked down by antisense oligonucleotide (ASO) infusion prior to alcohol self-administration. Rats showed a transient reduction in alcohol self-administration 1 day after ASO infusion. Together these studies demonstrate a functional role of CeA MR in modulating alcohol self-administration and make a case for studying MR antagonists as a novel treatment for AUD.

摘要

盐皮质激素受体 (MR) 是酒精研究领域的一个新兴靶点。MR 是糖皮质激素受体家族中的一种甾体受体,除了 MR 选择性配体醛固酮外,它还与糖皮质激素受体共享配体皮质酮。最近的研究表明,大鼠和猕猴的中央杏仁核 (CeA) MR 表达与饮酒之间存在相关性,以及个体的醛固酮与酒精渴求之间存在相关性酗酒障碍 (AUD)。此外,我们之前的工作表明,全身给予 MR 拮抗剂螺内酯可减少雄性和雌性大鼠的酒精自我给药和反应持续时间。这项研究检查了 MR 拮抗剂治疗后自我给药减少是否与 MR 介导的皮质酮负反馈失调有关。接受螺内酯(50mg/kg;IP)治疗的雌性大鼠在自我给药后表现出血浆皮质酮升高,这与酒精自我给药减少有关。接下来,使用 MR 选择性拮抗剂依普利酮进行局部微注射,以确定 MR 对酒精自我给药作用的脑区域定位。依普利酮输注可剂量依赖性地减少 CeA 中的酒精自我给药,但对背侧海马无影响。最后,为了检测 CeA MR 在酒精自我给药中的功能作用,在酒精自我给药之前通过抗 sense 寡核苷酸 (ASO) 输注敲低 CeA MR。大鼠在 ASO 输注后 1 天表现出酒精自我给药的短暂减少。这些研究共同证明了 CeA MR 在调节酒精自我给药中的功能作用,并为研究 MR 拮抗剂作为 AUD 的一种新治疗方法提供了依据。

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Central amygdala mineralocorticoid receptors modulate alcohol self-administration.中杏仁核盐皮质激素受体调节酒精自我给药。
Neuropharmacology. 2020 Dec 15;181:108337. doi: 10.1016/j.neuropharm.2020.108337. Epub 2020 Sep 29.

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