去甲肾上腺素、γ -氨基丁酸和胆碱再摄取动力学及乙醇对长睡眠和短睡眠小鼠的影响。

Substance and alcohol actions/misuse Pub Date : 1982-01-01
T C Howerton, M J Marks, A C Collins
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引用次数: 0

摘要

研究了长睡眠(LS)和短睡眠(SS)小鼠对去甲肾上腺素、γ -氨基丁酸(GABA)和胆碱的再摄取特性。动力学分析显示,在皮质和小脑中测量的去甲肾上腺素和GABA的亲和力(Km)或最大速度(Vmax)以及纹状体和皮质中测量的胆碱在不同系之间没有显著差异。体外乙醇剂量-反应曲线(0-1.7 M)显示,除胆碱再摄取外,这些神经递质对皮质的再摄取有高度显著的抑制作用。两系小鼠对乙醇的所有反应都是相同的。GABA再摄取抑制在皮层的程度大于小脑。另一方面,胆碱再摄取在纹状体中对乙醇非常敏感,而在皮层中不受影响。这些数据表明乙醇的溶解度有一定的区域特异性。浓度大于0.86 M的乙醇对再摄取的抑制是不可逆的,不是由于高渗溶解。我们的数据与先前发表的研究完全一致,表明乙醇抑制神经递质再摄取。然而,由于LS和SS小鼠对乙醇的敏感性不同,并且由于我们发现两种小鼠在动力学参数或体外乙醇的急性反应方面没有差异,因此似乎抑制神经递质再摄取与乙醇的抑制作用无关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Norepinephrine, gamma-aminobutyric acid, and choline reuptake kinetics and the effects of ethanol in long-sleep and short-sleep mice.

The reuptake characteristics of norepinephrine, gamma-aminobutyric acid (GABA), and choline were investigated in the long-sleep (LS) and short-sleep (SS) mouse lines. Kinetic analysis revealed no significant differences between lines in affinity (Km) or maximal velocity (Vmax) for norepinephrine and GABA measured in cortex and cerebellum or for choline measured in striatum and cortex. In vitro ethanol dose-response curves (0-1.7 M) for these neurotransmitters showed highly significant inhibition of reuptake except for reuptake of choline in cortex. All responses to ethanol were identical in both lines of mice. The magnitude of GABA reuptake inhibition was greater in cortex than in cerebellum. On the other hand, choline reuptake was very sensitive to ethanol in striatum, but was unaffected in cortex. These data suggest some regional specificity in ethanol's solubility. Inhibition of reuptake by ethanol concentrations greater than 0.86 M was determined to be irreversible and not due to hypertonic lysis. Our data are in complete agreement with previously published studies which suggest that ethanol inhibits neurotransmitter reuptake. However, since the LS and SS mice were selected for differential sensitivity to ethanol, and since we found no differences between lines in kinetic parameters or acute responses to in vitro ethanol, it appears that inhibition of neurotransmitter reuptake is not involved in the depressant effects of ethanol.

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