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酒精给药后自由活动小鼠海马 CA1 区微血管和神经元活动的双色微尺度成像。

Dual-color miniscope imaging of microvessels and neuronal activity in the hippocampus CA1 region of freely moving mice following alcohol administration.

机构信息

Department of Pharmacology, Addiction Science, and Toxicology, College of Medicine, The University of Tennessee Health Science Center, Memphis, Tennessee, United States.

出版信息

Am J Physiol Regul Integr Comp Physiol. 2023 Dec 1;325(6):R769-R781. doi: 10.1152/ajpregu.00044.2023. Epub 2023 Oct 23.

Abstract

Moderate-to-heavy episodic ("binge") drinking is the most common form of alcohol consumption in the United States. Alcohol at binge drinking concentrations reduces brain artery diameter in vivo and in vitro in many species including rats, mice, and humans. Despite the critical role played by brain vessels in maintaining neuronal function, there is a shortage of methodologies to simultaneously assess neuron and blood vessel function in deep brain regions. Here, we investigate cerebrovascular responses to ethanol by choosing a deep brain region that is implicated in alcohol disruption of brain function, the hippocampal CA1, and describe the process for obtaining simultaneous imaging of pyramidal neuron activity and diameter of nearby microvessels in freely moving mice via a dual-color miniscope. Recordings of neurovascular events were performed upon intraperitoneal injection of saline versus 3 g/kg ethanol in the same mouse. In male mice, ethanol mildly increased the amplitude of calcium signals while robustly decreasing their frequency. Simultaneously, ethanol decreased microvessel diameter. In females, ethanol did not change the amplitude or frequency of calcium signals from CA1 neurons but decreased microvessel diameter. A linear regression of ethanol-induced reduction in number of active neurons and microvessel constriction revealed a positive correlation ( = 0.981) in females. Together, these data demonstrate the feasibility of simultaneously evaluating neuronal and vascular components of alcohol actions in a deep brain area in freely moving mice, as well as the sexual dimorphism of hippocampal neurovascular responses to alcohol.

摘要

中度至重度阵发性(“ binge”)饮酒是美国最常见的饮酒形式。在包括大鼠、小鼠和人类在内的许多物种中, binge 饮酒浓度的酒精会在体内和体外降低脑动脉直径。尽管脑血管在维持神经元功能方面起着至关重要的作用,但缺乏同时评估深部脑区神经元和血管功能的方法。在这里,我们选择一个与酒精扰乱大脑功能有关的深部脑区——海马 CA1,研究脑血管对乙醇的反应,并描述了一种通过双通道微型显微镜在自由活动的小鼠中同时记录海马 CA1 锥体神经元活动和附近微血管直径的方法。在同一只小鼠中,通过腹腔注射生理盐水与 3 g/kg 乙醇来记录神经血管事件。在雄性小鼠中,乙醇轻度增加钙信号的幅度,而强烈降低其频率。同时,乙醇使微血管直径减小。在雌性小鼠中,乙醇不改变 CA1 神经元钙信号的幅度或频率,但使微血管直径减小。乙醇诱导的活跃神经元数量减少和微血管收缩之间的线性回归显示,在雌性小鼠中存在正相关( = 0.981)。这些数据共同证明了在自由活动的小鼠中,同时评估深部脑区中酒精作用的神经元和血管成分的可行性,以及海马神经血管对酒精的反应存在性别二态性。

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