首页> 外文期刊>Naunyn-Schmiedeberg's Archives of Pharmacology >Isobolographic characterization of interactions of retigabine with carbamazepine, lamotrigine, and valproate in the mouse maximal electroshock-induced seizure model.
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Isobolographic characterization of interactions of retigabine with carbamazepine, lamotrigine, and valproate in the mouse maximal electroshock-induced seizure model.

机译:在小鼠最大电击诱发的癫痫发作模型中,瑞替加滨与卡马西平,拉莫三嗪和丙戊酸盐的相互作用的等效线描写特征。

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The aim of this study was to characterize the pharmacodynamic, pharmacokinetic, and adverse-effect profiles of retigabine (RTG) in combination with carbamazepine (CBZ), lamotrigine (LTG), and valproate (VPA). The isobolographic analysis for parallel and nonparallel dose-response effects was used in the mouse maximal electroshock seizure (MES) model for evaluation of pharmacodynamic interaction. Potential adverse-effect profiles of interactions of RTG with CBZ, LTG, and VPA at the fixed ratio of 1:1 in the MES test were evaluated in the chimney (motor performance), passive avoidance (long-term memory), and grip strength (muscular strength) tests. Free plasma and total brain concentrations of CBZ, LTG, and VPA were determined by immunofluorescence and chromatography to assess pharmacokinetic interaction. In the MES model, RTG administered singly had its dose-response relationship curve (DRRC) parallel to that for VPA and nonparallel to that for CBZ and LTG. With isobolography for parallel DRRCs, the combination of RTG with VPA at fixed ratios of 1:3, 1:1, and 3:1 exerted supraadditive (synergistic) interaction. Isobolography for nonparallel DRRCs revealed that the combinations of RTG with CBZ and LTG at the fixed ratio of 1:1 produced additive interaction. In all combinations, neither motor coordination, long-term memory, nor muscular strength were affected. Only the combination of RTG with VPA at the fixed ratio of 3:1 was complicated by a pharmacokinetic increase in both free plasma and total brain VPA concentrations. All remaining combinations of RTG with VPA, CBZ, and LTG were pharmacodynamic in nature. RTG synergistically interacted with VPA and exerted additive interaction with CBZ and LTG in the mouse MES model.
机译:这项研究的目的是表征瑞替加滨(RTG)与卡马西平(CBZ),拉莫三嗪(LTG)和丙戊酸盐(VPA)结合的药效学,药代动力学和不良反应。在小鼠最大电休克发作(MES)模型中使用平行和非平行剂量反应效应的等效线分析法评估药效学相互作用。在MES测试中,以固定比例1:1的比例对RTG与CBZ,LTG和VPA相互作用的潜在不利影响分布进行了烟囱(运动性能),被动回避(长期记忆)和抓地力的评估(肌肉力量)测试。通过免疫荧光和色谱法测定游离血浆和脑中CBZ,LTG和VPA的总浓度,以评估药代动力学相互作用。在MES模型中,单独施用的RTG的剂量反应关系曲线(DRRC)与VPA平行,而与CBZ和LTG不平行。对于平行DRRC的等效线描记法,RTG与VPA的固定比例为1:3、1:1和3:1的组合发挥了超加性(协同)相互作用。对于非平行DRRC的等效线描记法显示,RTG与CBZ和LTG的固定比例为1:1的组合产生了加性相互作用。在所有组合中,运动协调,长期记忆和肌肉力量均未受影响。只有RTG与VPA的固定比例为3:1的组合,才能使游离血浆和总脑VPA浓度的药代动力学增加。 RTG与VPA,CBZ和LTG的所有其余组合本质上都是药效学的。 RTG与VPA协同相互作用,并在小鼠MES模型中与CBZ和LTG发挥加性相互作用。

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