谷氨酸能调节大鼠纹状体肽基因表达。

J Jolkkonen, P Jenner, C D Marsden
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引用次数: 15

摘要

在皮质消融、阻断n -甲基- d -天冬氨酸(NMDA)受体或拉莫三嗪抑制谷氨酸释放后,测定大鼠纹状体中编码脑啡肽和P物质的mRNA水平。大脑皮质单侧消融导致P物质mRNA水平下降,特别是在与病变同侧的吻侧背外侧纹状体和背内侧纹状体。脑啡肽mRNA水平的降低也有类似的趋势。连续在纹状体内灌注竞争性NMDA受体拮抗剂3-((+/-)-2- carboxypperazin -4-yl)-丙基-1-膦酸(CPP, 0.12和1.2微克/天),以剂量依赖的方式均匀地降低了邻近输注部位纹状体的脑啡肽mRNA和P物质mRNA。在亚慢性给药假定的谷氨酸释放抑制剂拉莫三嗪(5和20mg/kg IP)后,纹状体中脑啡肽mRNA或P物质mRNA水平均无显著变化。大鼠纹状体中脑啡肽mRNA和P物质mRNA的表达均通过突触后NMDA受体介导的机制被强直刺激。这与纹状体输出神经元中多肽的差异多巴胺能调节形成对比。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Glutamatergic regulation of striatal peptide gene expression in rats.

The mRNA levels encoding enkephalin and substance P were measured in the rat striatum following cortical ablation, blockade of N-methyl-D-aspartate (NMDA) receptors or inhibition of glutamate release by lamotrigine. Unilateral ablation of the cerebral cortex resulted in a decrease of substance P mRNA levels particularly in the rostral dorsolateral and dorsomedial striatum ipsilateral to the lesion. There was a similar trend for a reduction in levels of enkephalin mRNA. Continuous, intrastriatal infusion of the competitive NMDA receptor antagonist, 3-((+/-)-2-carboxypiperazin-4-yl)-propyl-1-phosphonic acid, (CPP, 0.12 and 1.2microg/day) decreased both enkephalin mRNA and substance P mRNA in dose-dependent manner evenly throughout the striatum adjacent to the infusion site. Following subchronic administration of the presumed glutamate release inhibitor, lamotrigine (5 and 20mg/kg IP) there was no significant alterations in either enkephalin mRNA or substance P mRNA levels in the striatum. Both enkephalin mRNA and substance P mRNA expression in the rat striatum appear tonically stimulated through postsynaptic NMDA receptor mediated mechanisms. This contrasts with differential dopaminergic modulation of peptides in striatal output neurons.

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