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遗传选择对小鼠酒精偏好的影响改变了背侧纹状体的神经传递。

Genetic Selection for Alcohol Preference in Mice Alters Dorsal Striatum Neurotransmission.

机构信息

Department of Pharmacology & Toxicology, Indiana University School of Medicine, Indianapolis, Indiana.

Stark Neurosciences Research Institute, Indiana University School of Medicine, Indianapolis, Indiana.

出版信息

Alcohol Clin Exp Res. 2019 Nov;43(11):2312-2321. doi: 10.1111/acer.14187. Epub 2019 Sep 23.

Abstract

BACKGROUND

Although it is widely acknowledged that the risk of developing an alcohol use disorder (AUD) is strongly influenced by genetic factors, very little is known about how this genetic predisposition may alter neurotransmission in a way that promotes AUD susceptibility. The dorsal striatum has garnered increased attention as a brain region of interest in AUD development given its significant roles in goal-directed and habitual behavior.

METHODS

In the present work, dorsal striatal neurotransmission parameters were measured in preclinical mouse models of high and low AUD risk. We performed brain slice whole-cell patch clamp electrophysiological recordings from medium spiny neurons (MSNs) in the dorsomedial (DMS) and dorsolateral (DLS) striatum of naïve adult male and female selectively bred high- and low-alcohol-preferring lines of mice (HAP and LAP).

RESULTS

We found that MSNs of HAP mice were significantly more excitable than those of LAP mice, specifically in the DLS. Additionally, the frequencies of spontaneous glutamate- and GABA-mediated currents were both elevated in HAP mice relative to LAP mice in both dorsal striatal subregions, whereas amplitude differences were more variable between lines and subregions. AMPAR/NMDAR current ratios were significantly lower in HAP mice in both DLS and DMS.

CONCLUSIONS

Collectively, these results suggest that genetic predisposition for high or low alcohol consumption produces significantly different basal functional states within both DLS and DMS which may be important factors in the behavioral phenotypes of HAP and LAP mice.

摘要

背景

尽管人们普遍认为,酗酒障碍(AUD)的发病风险受遗传因素的强烈影响,但对于这种遗传倾向如何以促进 AUD 易感性的方式改变神经传递,人们知之甚少。鉴于背侧纹状体在目标导向和习惯性行为中具有重要作用,因此它作为 AUD 发展的一个感兴趣的脑区引起了越来越多的关注。

方法

在本工作中,我们测量了高风险和低风险 AUD 临床前小鼠模型中的背侧纹状体神经传递参数。我们对新生成年雄性和雌性选择性繁殖的高和低酒精偏好线(HAP 和 LAP)小鼠的背侧纹状体的背内侧(DMS)和背外侧(DLS)纹状体中的中间神经元(MSNs)进行了脑片全细胞贴附式膜片钳电生理记录。

结果

我们发现,与 LAP 小鼠相比,HAP 小鼠的 MSNs 兴奋性更高,特别是在 DLS 中。此外,与 LAP 小鼠相比,HAP 小鼠的谷氨酸和 GABA 介导的自发性电流频率均升高,而背侧纹状体亚区之间的幅度差异更为多变。在 DLS 和 DMS 中,HAP 小鼠的 AMPAR/NMDAR 电流比值均显著降低。

结论

综上所述,这些结果表明,高或低酒精摄入的遗传倾向在 DLS 和 DMS 中产生了明显不同的基础功能状态,这可能是 HAP 和 LAP 小鼠行为表型的重要因素。

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