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大鼠大脑皮层内源性γ-氨基丁酸和谷氨酸的释放。

The release of endogenous GABA and glutamate from the cerebral cortex in the rat.

作者信息

Moroni F, Corradetti R, Casamenti F, Moneti G, Pepeu G

出版信息

Naunyn Schmiedebergs Arch Pharmacol. 1981 Jun;316(3):235-9. doi: 10.1007/BF00505655.

Abstract
  1. The release of endogenous GABA and glutamate from the cerebral cortex was measured using a cortical cup technique in unanaesthetized freely moving rats and anaesthetized rats by means of a sensitive and specific mass-spectrometric procedure. 2. GABA release was not affected by the presence of the dura mater or by anaesthesia. Glutamate output was reduced by urethane but not by pentobarbital anaesthesia and by the presence of the dura. 3. An isotonic solution containing 50 mM KCl placed epidurally within the cup elicited a significant short-lasting increase in glutamate output, a decrease in GABA output and a short-lasting electrocorticogram (ECoG) activation. 4. When the dura was removed, a high K+ solution placed on the exposed cerebral cortex elicited a 7--8 fold increase in GABA output accompanied by a marked decrease in glutamate output and by ECoG synchronization. The changes in GABA and glutamate output had parallel time-course and were prevented by the application within the cup of tetrodotoxin (3 X 10(-5) M). 5. Amphetamine at the doses of 3.7 and 7.4 mumol . kg-1 i.v. increased glutamate output and at the dose of 37 mumol . kg-1 i.v. increased GABA output. Both effects were prevented or reduced by haloperidol pretreatment (0.65 mumol . kg-1 i.v.). 6. It is concluded that GABA and glutamate released from the cerebral cortex and diffused into an epidural or cortical cup originate at least in part from the brain. The rate of their release is influenced by changes in neuronal activity. The measurement of their rate of release offers a useful tool for the study of the functional role of cortical GABA and glutamate-releasing neurons.
摘要
  1. 采用皮质杯技术,借助灵敏且特异的质谱分析法,在未麻醉的自由活动大鼠和麻醉大鼠中测量大脑皮质内源性γ-氨基丁酸(GABA)和谷氨酸的释放。2. GABA的释放不受硬脑膜的存在或麻醉的影响。谷氨酸的输出量在氨基甲酸乙酯麻醉时减少,但在戊巴比妥麻醉和有硬脑膜存在时未减少。3. 置于杯内硬膜外的含50 mM氯化钾的等渗溶液可引起谷氨酸输出量显著短暂增加、GABA输出量减少以及短暂的皮质电图(ECoG)激活。4. 去除硬脑膜后,置于暴露大脑皮质上的高钾溶液可使GABA输出量增加7 - 8倍,同时谷氨酸输出量显著减少并伴有ECoG同步化。GABA和谷氨酸输出量的变化具有平行的时间进程,且在杯内应用河豚毒素(3×10⁻⁵ M)可阻止这种变化。5. 静脉注射剂量为3.7和7.4 μmol·kg⁻¹的苯丙胺可增加谷氨酸输出量,静脉注射剂量为37 μmol·kg⁻¹的苯丙胺可增加GABA输出量。这两种效应均可被氟哌啶醇预处理(静脉注射0.65 μmol·kg⁻¹)阻止或减弱。6. 得出结论:从大脑皮质释放并扩散到硬膜外或皮质杯内的GABA和谷氨酸至少部分源自大脑。它们的释放速率受神经元活动变化的影响。测量它们的释放速率为研究皮质释放GABA和谷氨酸的神经元的功能作用提供了一个有用的工具。

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