慢性酗酒者大脑皮层受损区GABAA受体的研究。

P R Dodd
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引用次数: 0

摘要

与相同病例的中央前回和匹配对照的额上回相比,未并发疾病的慢性酗酒者在额上回GABAA受体上显示出更大密度的GABA激动剂位点(用选择性配体[3H]muscimol标记)。与对照组相比,伴有韦尼克脑病的患者也可能有更多额叶上[3H]肌醇结合位点,而伴有肝硬化的酗酒者则表现出更微弱的差异。由于GABAA受体是一种多聚体复合物,也具有“中心型”苯二氮卓类配体的结合位点,因此可以预期,用这些化合物获得的数据应该与用[3H]muscimol获得的数据相似。但事实并非如此。[3H]氟硝西泮结合位点在病例组间差异不大,但存在明显的区域差异。[3H]地西泮在无并发症酗酒者和肝硬化酗酒者中的位置与[3H]muscimol相同,但在Wernicke病例中额上回的密度较低。GABAA受体亚基异构体基因的差异表达可能导致这些差异。
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GABAA receptors in damaged cerebral cortex areas in human chronic alcoholics.

Chronic alcoholics without complicating disease showed greater densities of GABA agonist sites (labelled with the selective ligand [3H]muscimol) on the GABAA receptor in the superior frontal gyrus, in comparison with both precentral gyrus in the same cases, and with superior frontal gyrus in matched controls. Whereas cases with concomitant Wernicke encephalopathy may also have had greater numbers of superior frontal [3H]muscimol binding sites than controls, alcoholics with cirrhosis of the liver showed more muted differences. Since the GABAA receptor is a multimeric complex which also possesses binding sites for "central-type" benzodiazepine ligands, it would be expected that data obtained with these compounds should mimic that obtained with [3H]muscimol. This was not so. [3H]Flunitrazepam binding sites showed little variation between case groups, although they showed clear regional differences. [3H]Diazepam sites followed those for [3H]muscimol in uncomplicated alcoholics and alcoholics with cirrhosis of the liver, but were at lower density in superior frontal gyrus in Wernicke cases. Differential expression of GABAA receptor subunit isoform genes may give rise to these disparities.

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