首页> 外文期刊>Epilepsy research >Ivabradine attenuates the anticonvulsant potency of lamotrigine, but not that of lacosamide, pregabalin and topiramate in the tonic-clonic seizure model in mice
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Ivabradine attenuates the anticonvulsant potency of lamotrigine, but not that of lacosamide, pregabalin and topiramate in the tonic-clonic seizure model in mice

机译:ivabradine衰减甲噻吩的抗惊厥效力,但不是小鼠滋补克隆癫痫发作模型中的漆酰胺,普罗巴胺和托吡酯的抗惊厥性效力

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摘要

Hyperpolarization-activated cyclic nucleotide-gated (HCN) channels are involved not only in synaptic transmission and neuronal excitability under physiological conditions, but also in seizure activity. To determine the influence of ivabradine (an HCN channel inhibitor) on the anticonvulsant potency of four novel antiepileptic drugs (AEDs: lacosamide, lamotrigine, pregabalin and topiramate) in the mouse maximal electroshock-induced seizure (MES) model. Adult male albino Swiss mice were challenged with maximal electroconvulsions (electric current of 25 mA delivered via auricular electrodes). Total brain concentrations of AEDs were measured with high-pressure liquid chromatography. Ivabradine (10 mg/kg, i.p.) significantly reduced the anticonvulsant potency of lamotrigine by elevating the ED50 value of the AED from 7.48 (6.15-9.11) to 10.07 (8.85-11.45) mg/ kg (P < 0.05) in the mouse MES model. In contrast, ivabradine (10 mg/kg, i.p.) did not significantly affect the anticonvulsant potency of lacosamide, pregabalin or topiramate in the mouse MES model. Additionally, ivabradine had no impact on total brain concentrations of all the studied AEDs in mice. A special caution is advised when combining ivabradine with lamotrigine in epilepsy patients due to the possible pharmacodynamic reduction of the anticonvulsant action of the later drug. The combinations of ivabradine with lacosamide, pregabalin and topiramate seem to be pharmacodynamic and neutral from a preclinical viewpoint.
机译:超极化激活的循环核苷酸门控(HCN)通道不仅涉及生理条件下的突触透射和神经元兴奋性,而且涉及癫痫发作活性。在小鼠最大电泵诱导的癫痫发作(MES)模型中,确定IVABRADINE(AEDS:AEDS:LACOSAME,甲磺酰胺,吡甲酰胺,PREGABALIN和TOPABALIN,PREGABALIN和TOPABALIN和TOPALAMATE的影响。成年雄性白化瑞士小鼠面临着最大电压(电流为25 mA通过耳廓电极的电流)。用高压液相色谱法测量AED的总脑浓度。 ivabradine(10mg / kg,IP)通过将7.48(6.15-9.11)升高至10.07(8.85-11.45)Mg / kg(P <0.05)在小鼠MES中,显着降低了乳芳酮的抗惊厥效力模型。相反,Ivabradine(10mg / kg,i.p.)没有显着影响小鼠MES模型中漆萨米酰胺,普瑞巴林或托吡酯的抗惊厥效力。此外,Ivabradine对小鼠中所有研究AED的全脑浓度没有影响。在将Ivabradine与癫痫患者中与癫痫患者中的乳藻相结合时,建议特别谨慎,这是由于可能的后期药物的抗惊厥作用的药物动力学降低。 Ivabradine与漆糖苷,普瑞巴林和托吡酯的组合似乎是来自临床前观点的药物动力学和中性。

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