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染料木黄酮(一种酪氨酸激酶抑制剂)对电压敏感性钠通道的直接阻断作用。

Direct block of voltage-sensitive sodium channels by genistein, a tyrosine kinase inhibitor.

作者信息

Paillart C, Carlier E, Guedin D, Dargent B, Couraud F

机构信息

Institut National de la Santé et de la Recherche Médicale U374, Institut Jean Roche, Faculté de Médecine, Marseille, France.

出版信息

J Pharmacol Exp Ther. 1997 Feb;280(2):521-6.

PMID:9023259
Abstract

Genistein, an isoflavone inhibitor of tyrosine-specific protein kinases, was shown to specifically block the 22Na+ influx through voltage-sensitive Na+ channels in cultured rat brain neurons, whereas other tyrosine kinase antagonists such as lavendustin A, compound 5, tyrphostin A47 and an erbstatin analog were inactive at concentrations known to block kinase activity in other neuronal systems. Dose-response curves for genistein indicated a half-maximum effect at 60 microM. Daidzein, an inactive analog of genistein, had a similar inhibitory effect on the 22Na+ influx with a half-maximum effect at 195 microM. The time course of genistein action was rapid, because maximum effect on 22Na+ influx was obtained in less than 20 s at 100 microM. Analysis of Na+ currents by the whole-cell recording technique showed that 20 microM genistein reduced the sodium current and shifted the voltage dependence of both activation and inactivation curves. No competition with [3H]saxitoxin binding was observed, whereas the binding of [3H]batrachotoxinin A 20-alpha-benzoate to rat brain synaptosomal membranes was partially inhibited, which suggested a direct or allosteric interaction with neurotoxin binding site 2. These data taken together clearly indicate that the inhibition of voltage-sensitive sodium channels by genistein is not mediated by tyrosine kinase inhibition.

摘要

染料木黄酮是一种酪氨酸特异性蛋白激酶的异黄酮抑制剂,已证明它能特异性地阻断培养的大鼠脑神经元中通过电压敏感性钠通道的22Na+内流,而其他酪氨酸激酶拮抗剂,如拉文达ustin A、化合物5、 tyrphostin A47和一种埃布他汀类似物,在已知能阻断其他神经元系统中激酶活性的浓度下没有活性。染料木黄酮的剂量反应曲线表明,在60 microM时达到最大效应的一半。大豆苷元是染料木黄酮的一种无活性类似物,对22Na+内流有类似的抑制作用,在195 microM时达到最大效应的一半。染料木黄酮作用的时间进程很快,因为在100 microM时,不到20秒就能对22Na+内流产生最大效应。通过全细胞记录技术对钠电流的分析表明,20 microM染料木黄酮可降低钠电流,并使激活曲线和失活曲线的电压依赖性发生偏移。未观察到与[3H]石房蛤毒素结合的竞争,而[3H]蛙毒素A 20-α-苯甲酸酯与大鼠脑突触体膜的结合受到部分抑制,这表明与神经毒素结合位点2存在直接或变构相互作用。这些数据综合起来清楚地表明,染料木黄酮对电压敏感性钠通道的抑制作用不是由酪氨酸激酶抑制介导的。

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