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首页> 外文期刊>The Journal of Pharmacology and Experimental Therapeutics: Official Publication of the American Society for Pharmacology and Experimental Therapeutics >Antagonism of the discriminative stimulus effects of positive gamma-aminobutyric acid(A) modulators in rhesus monkeys discriminating midazolam.
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Antagonism of the discriminative stimulus effects of positive gamma-aminobutyric acid(A) modulators in rhesus monkeys discriminating midazolam.

机译:在鉴别咪达唑仑的恒河猴中,对正γ-氨基丁酸(A)调节剂的鉴别刺激作用的拮抗作用。

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The extent to which individual subtypes of benzodiazepine receptors are functionally independent has not been elucidated in vivo. This study used apparent pA(2) analysis to test the hypothesis that a single receptor subtype mediates the discriminative stimulus effects of midazolam, triazolam, and diazepam, three positive gamma-aminobutyric acid(A) (GABA(A)) modulators. Four rhesus monkeys discriminated 0.56 mg/kg midazolam from vehicle under a fixed-ratio 5 schedule of stimulus-shock termination. Midazolam, triazolam, and diazepam increased responding on the midazolam-appropriate lever. The neutral GABA(A) modulator flumazenil shifted dose-effect curves for triazolam and diazepam to the right, and the negative GABA(A) modulators Ro 15-4513 and ethyl beta-carboline-3-carboxylate (beta-CCE) shifted dose-effect curves for midazolam and triazolam to the right. Slopes of Schild plots for flumazenil and Ro 15-4513 conformed to unity. The apparent pA(2) values were 7.41 and 7.69 for flumazenil in combination with triazolam and diazepam, respectively, and 7.53 and 6.88 for Ro 15-4513 in combination with midazolam and triazolam, respectively. The slope of the Schild plot for beta-CCE in combination with midazolam deviated from unity. Slopes of Schild plots obtained with flumazenil and Ro 15-4513 support the notion that a single benzodiazepine receptor subtype mediates the effects of midazolam, triazolam, or diazepam. The similarity in apparent pA(2) values for flumazenil in combination with triazolam and diazepam or for Ro 15-4513 in combination with midazolam and triazolam suggests that the same subtype mediates the effects of these positive modulators. In contrast, beta-CCE and midazolam do not appear to interact in a simple, competitive manner.
机译:体内尚未阐明苯二氮卓类受体的各个亚型在功能上独立的程度。这项研究使用了明显的pA(2)分析来检验以下假设:单个受体亚型介导了咪达唑仑,三唑仑和地西epa,三种正γ-氨基丁酸(A)(GABA(A)调节剂)的歧视性刺激作用。四只恒河猴在固定比例5刺激休克时间表下从媒介物中鉴别出0.56 mg / kg咪达唑仑。咪达唑仑,三唑仑和地西epa在适当的咪达唑仑杠杆上的响应增加。中性GABA(A)调节剂氟马西尼将三唑仑和地西epa的剂量效应曲线移至右侧,而负GABA(A)调节剂Ro 15-4513和β-咔啉-3-羧酸乙酯(β-CCE)移出剂量-咪达唑仑和三唑仑的效果曲线在右侧。氟马西尼和Ro 15-4513的Schild样地的坡度一致。氟马西尼联合三唑仑和地西epa的表观pA(2)值分别为7.41和7.69,Ro 15-4513与咪达唑仑和三唑仑的表观pA(2)值分别为7.53和6.88。 β-CCE与咪达唑仑组合的Schild图的斜率偏离单位。用氟马西尼和Ro 15-4513获得的Schild样地的斜率支持以下观点,即单个苯二氮杂receptor受体亚型介导了咪达唑仑,三唑仑或地西epa的作用。氟马西尼与三唑仑和地西epa组合或Ro 15-4513与咪达唑仑和三唑仑的表观pA(2)值相似,表明相同的亚型介导了这些正调节剂的作用。相反,β-CCE和咪达唑仑似乎没有以简单的竞争方式相互作用。

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