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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 >Antiepileptogenic effects of the novel anticonvulsant levetiracetam (ucb L059) in the kindling model of temporal lobe epilepsy.
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Antiepileptogenic effects of the novel anticonvulsant levetiracetam (ucb L059) in the kindling model of temporal lobe epilepsy.

机译:新型抗惊厥药左乙拉西坦(ucb L059)在颞叶癫痫发作模型中的抗癫痫作用。

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We have previously shown that the novel anticonvulsant levetiracetam exerts potent anticonvulsant activity against both focal and secondarily generalized seizures in fully amygdala-kindled rats, i.e. , a model of temporal lobe epilepsy. We examined whether levetiracetam also exhibits antiepileptogenic activity, i.e., prevents or retards acquisition or development of amygdala-kindling in rats. Before the experiments with chronic administration of levetiracetam at different doses, we determined the pharmacokinetics of the drug after i.p. injection. Levetiracetam had a relatively short half-life (about 2-3 hr) in rats, so that any lasting effects of the drug after chronic administration were certainly not due to drug accumulation. When rats were treated with levetiracetam during kindling acquisition at daily i.p. doses of 13, 27 or 54 mg/kg, the drug dose-dependently suppressed the increase in seizure severity and duration induced by repeated amygdala stimulation. After termination of daily treatment with 54 mg/kg, duration of behavioral seizures and of afterdischarges recorded from the amygdala remained to be significantly shorter compared to vehicle controls, although amygdala stimulations were continued in the absence of drug. These data thus indicate that levetiracetam not simply masked the expression of kindled seizures through an anticonvulsant action, but exerted a true antiepileptogenic effect. Adverse effects were not observed at any dose of levetiracetam tested in kindled rats. The powerful antiepileptogenic activity of levetiracetam in the kindling model indicates that levetiracetam is not only an interesting novel drug for symptomatic treatment of epilepsy but might be suited for pharmacological prevention of this disease in patients with a high prospective risk of the development of epilepsy.
机译:先前我们已经表明,新型抗惊厥性左乙拉西坦在完全杏仁化的大鼠(即颞叶癫痫模型)中对局灶性和继发性全身性癫痫发作均具有有效的抗惊厥活性。我们检查了左乙拉西坦是否还表现出抗癫痫活性,即,预防或延迟了大鼠杏仁核的获取或发育。在以不同剂量长期服用左乙拉西坦的实验之前,我们确定了i.p.后的药物药代动力学。注射。左乙拉西坦在大鼠中的半衰期相对较短(约2-3小时),因此,长期给药后该药物的任何持久作用肯定不是由于药物蓄积引起的。在每天腹腔注射点燃期间用左乙拉西坦治疗大鼠时。当剂量为13、27或54 mg / kg时,该药物剂量依赖性地抑制了反复杏仁核刺激引起的癫痫发作严重程度和持续时间的增加。在以54 mg / kg的每日治疗终止后,杏仁核记录的行为性癫痫发作持续时间和出院后的持续时间与媒介物对照组相比明显缩短,尽管杏仁核刺激在没有药物的情况下仍继续进行。因此,这些数据表明左乙拉西坦不仅通过抗惊厥作用掩盖了点燃的癫痫发作的表达,而且发挥了真正的抗癫痫作用。在点燃的大鼠中测试的任何剂量的左乙拉西坦均未观察到不良反应。左乙拉西坦在点燃模型中具有强大的抗癫痫活性,这表明左乙拉西坦不仅是对症治疗癫痫的一种有趣的新药,而且可能适合在具有高前瞻性癫痫发展风险的患者中对该病进行药理预防。

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