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两种不同的可溶性苯二氮䓬受体:离子的差异调节作用。

Two distinct solubilized benzodiazepine receptors: differential modulation by ions.

作者信息

Lo M M, Snyder S H

出版信息

J Neurosci. 1983 Nov;3(11):2270-9. doi: 10.1523/JNEUROSCI.03-11-02270.1983.

Abstract

The modulation of solubilized type 1 and type 2 benzodiazepine receptors from cow brain by gamma-aminobutyric acid (GABA), divalent cations, and anions has been evaluated. GABA stimulates [3H] flunitrazepam binding of both receptor subtypes, whereas divalent cations and anions selectively stimulate solubilized type 2 receptors. Of numerous anions examined, only chloride, bromide, and iodide enhance [3H] flunitrazepam binding. Chloride and bromide increase mainly receptor affinity for [3H]flunitrazepam, whereas iodide largely influences Bmax values. Divalent cations also stimulate soluble type 2 receptors. Calcium, zinc, manganese, barium, and magnesium have similar potencies in enhancing [3H]flunitrazepam binding, whereas copper and nickel are about 4 to 5 times more potent. The 2- to 3-fold increase in type 2 receptor binding by divalent cations involves change in numbers of binding sites. Effects of combinations of GABA, calcium, and chloride suggest that they may exert their modulating effects on type 2 receptors through different mechanisms. GABA, calcium, and chloride also protect [3H]flunitrazepam binding from heat inactivation, indicating a close link in the native state between the GABA, ions, and the benzodiazepine recognition sites. Since physiologic concentrations of calcium and chloride influence type 2 receptors, these ions may be involved in those pharmacologic effects of benzodiazepines mediated by type 2 sites.

摘要

已评估了γ-氨基丁酸(GABA)、二价阳离子和阴离子对牛脑可溶性1型和2型苯二氮䓬受体的调节作用。GABA刺激两种受体亚型的[³H]氟硝西泮结合,而二价阳离子和阴离子则选择性地刺激可溶性2型受体。在众多检测的阴离子中,只有氯离子、溴离子和碘离子能增强[³H]氟硝西泮结合。氯离子和溴离子主要增加受体对[³H]氟硝西泮的亲和力,而碘离子则主要影响最大结合量(Bmax)值。二价阳离子也刺激可溶性2型受体。钙、锌、锰、钡和镁在增强[³H]氟硝西泮结合方面具有相似的效力,而铜和镍的效力约高4至5倍。二价阳离子使2型受体结合增加2至3倍涉及结合位点数量的变化。GABA、钙和氯组合的作用表明它们可能通过不同机制对2型受体发挥调节作用。GABA、钙和氯还能保护[³H]氟硝西泮结合免受热失活影响,表明在天然状态下GABA、离子与苯二氮䓬识别位点之间存在紧密联系。由于钙和氯的生理浓度会影响2型受体,这些离子可能参与由2型位点介导的苯二氮䓬的药理作用。

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