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首页> 外文期刊>Pharmacology, Biochemistry and Behavior >The novel anxiolytic U-101017: in vitro and ex vivo binding profile and effect on cerebellar cGMP.
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The novel anxiolytic U-101017: in vitro and ex vivo binding profile and effect on cerebellar cGMP.

机译:新型抗焦虑药物U-101017:体外和离体结合特征以及对小脑cGMP的作用。

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摘要

The binding affinities (Ki) of U-101017 and diazepam for the GABA(A) receptor in rat cortical membranes were determined using [3H]flunitrazepam ([3H]FNZ) as the ligand. The inhibition constants of U-101017 and diazepam were 3.78 nM and 6.36 nM, respectively. Brain uptake of U-101017 was studied by the ex vivo [3H]FNZ binding assay. A significant ex vivo inhibition of [3H]FNZ binding was observed 10 min after oral administration of U-101017, and the effect lasted for at least 240 min (the last time point of investigation). The potential anxiolytic activity of U-101017 and diazepam was investigated in nonstressed and stressed (electric foot shock) mice by quantitative estimation of cerebellar cyclic 3',5'-guanosine monophosphate (cGMP). Both U-101017 and diazepam dose-dependently decreased cGMP and attenuated stress-induced elevations in cGMP. These effects were antagonized by the GABA(A) receptor antagonist flumazenil. U-101017 was about two orders of magnitude more potent in stressed animals than in controls. The results of our investigation indicate that the anxiolytic-like activity of U-101017 is mediated via GABA(A) receptors.
机译:使用[3H]氟硝西m([3H] FNZ)作为配体,确定U-101017和地西epa对大鼠皮质膜中GABA(A)受体的结合亲和力(Ki)。 U-101017和地西epa的抑制常数分别为3.78 nM和6.36 nM。通过离体[3H] FNZ结合试验研究了U-101017的脑摄取。口服U-101017后10分钟观察到[3H] FNZ结合的显着体外抑制作用,该作用持续至少240分钟(研究的最后一个时间点)。通过定量估计小脑环状3',5'-单磷酸鸟苷(cGMP),研究了U-101017和地西epa在非应激和应激(电足电击)小鼠中的潜在抗焦虑活性。 U-101017和地西epa均剂量依赖性地降低cGMP并减弱应力诱导的cGMP升高。这些作用被GABA(A)受体拮抗剂氟马西尼拮抗。在受压动物中,U-101017的效力比对照组高约两个数量级。我们的研究结果表明,U-101017的抗焦虑活性是通过GABA(A)受体介导的。

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