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γ-氨基丁酸(GABA)增强[3H]唑吡坦与大鼠脑膜和脑切片中ω1位点结合的区域差异。

Regional differences in the enhancement by GABA of [3H]zolpidem binding to omega 1 sites in rat brain membranes and sections.

作者信息

Ruano D, Benavides J, Machado A, Vitorica J

机构信息

Departamento de Bioquímica, Bromatología y Toxicología, Facultad de Farmacia, Universidad de Sevilla, Spain.

出版信息

Brain Res. 1993 Jan 8;600(1):134-40. doi: 10.1016/0006-8993(93)90411-f.

Abstract

The potential heterogeneity in the allosteric coupling between GABA and omega 1 binding sites within the native GABAA receptor complex has been evaluated in the rat by measuring the enhancement by GABA of [3H]zolpidem binding to omega 1 site in membranes from three rat brain structures (neocortex, cerebellum and hippocampus) and brain sections. The maximal stimulatory effect of GABA was significantly higher (265 +/- 47%) in cortical membranes than in cerebellar (165 +/- 48%) or in hippocampal (118 +/- 17%) membranes. These differences are not due either to the presence of different amounts of residual GABA in the membrane preparations or to the labeling, in presence of GABA, of binding sites other than omega 1 since: (1) the pharmacological properties of the [3H]zolpidem binding sites were similar in the three regions; (2) the degree of allosteric enhancement was unrelated to the relative proportion of omega 1 sites in each structure; and (3) GABA did not increase the Bmax for [3H]zolpidem. Regional differences in the effect of 100 microM GABA on [3H]zolpidem binding were also observed by quantitative autoradiography. Regions where the strongest (3-4-fold) effects of GABA in [3H]zolpidem binding were observed included the substantia nigra, lateral geniculate body, olfactory tubercule and red nucleus. A large increase in [3H]zolpidem binding was also demonstrated in the cingulate and frontoparietal cortices with higher effects in deep (4.2-fold) rather than in superficial layers (3.3-fold). Heterogeneous subregional increases in [3H]zolpidem binding in the presence of GABA were quantified within the cerebellum, hippocampus and superior colliculus.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

通过测量γ-氨基丁酸(GABA)对[³H]唑吡坦与来自大鼠三个脑结构(新皮层、小脑和海马体)及脑切片膜中ω1位点结合的增强作用,评估了天然GABAA受体复合物中GABA与ω1结合位点之间变构偶联的潜在异质性。GABA的最大刺激作用在皮层膜中(265±47%)显著高于小脑膜(165±48%)或海马体膜(118±17%)。这些差异既不是由于膜制剂中存在不同量的残余GABA,也不是由于在GABA存在下对ω1以外的结合位点进行标记,原因如下:(1)[³H]唑吡坦结合位点在这三个区域的药理学特性相似;(2)变构增强程度与每个结构中ω1位点的相对比例无关;(3)GABA并未增加[³H]唑吡坦的Bmax。通过定量放射自显影也观察到100微摩尔GABA对[³H]唑吡坦结合作用的区域差异。观察到GABA对[³H]唑吡坦结合有最强(3至4倍)作用的区域包括黑质、外侧膝状体、嗅结节和红核。在扣带回和额顶叶皮层也证明了[³H]唑吡坦结合的大幅增加,深层(4.2倍)比浅层(3.3倍)的作用更大。在小脑、海马体和上丘内对GABA存在下[³H]唑吡坦结合的异质性亚区域增加进行了定量分析。(摘要截取自250字)

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