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首页> 外文期刊>Epilepsia: Journal of the International League against Epilepsy >Characterization of the anticonvulsant, behavioral and pharmacokinetic interaction profiles of stiripentol in combination with clonazepam, ethosuximide, phenobarbital, and valproate using isobolographic analysis.
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Characterization of the anticonvulsant, behavioral and pharmacokinetic interaction profiles of stiripentol in combination with clonazepam, ethosuximide, phenobarbital, and valproate using isobolographic analysis.

机译:使用等效线描记法分析了替比妥特与氯硝西am,乙妥昔芬,苯巴比妥和丙戊酸酯联用的抗惊厥,行为和药代动力学相互作用的特征。

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摘要

PURPOSE: Isobolographic analysis was used to characterize the interactions between stiripentol (STP) and clonazepam (CZP), ethosuximide (ETS), phenobarbital (PB), and valproate (VPA) in suppressing pentylenetetrazole (PTZ)-induced clonic seizures in mice. METHODS: The anticonvulsant and acute adverse (neurotoxic) effects of STP in combination with the various conventional antiepileptic drugs (AEDs), at fixed ratios of 1:3, 1:1, and 3:1, were evaluated in the PTZ and chimney tests in mice using the isobolographic analysis. Additionally, protective indices (PI) and benefit indices (BI) were calculated to identify their pharmacological profiles so that a ranking in relation to advantageous combination could be established. Moreover, adverse-effect paradigms were determined by use of the step-through passive avoidance task (long-term memory), threshold for the first pain reaction, grip-strength test (neuromuscular tone), and the hot plate test (acute thermal pain). Brain AED concentrations were also measured so as to ascertain any pharmacokinetic contribution to the pharmacodynamic interactions. RESULTS: All AED combinations comprising of STP and CZP, ETS, PB, and VPA (at the fixed ratios of 1:3, 1:1 and 3:1) were additive in terms of clonic seizure suppression in the PTZ test. However, these interactions were complicated by changes in brain AED concentrations consequent to pharmacokinetic interactions. Thus STP significantly increased total brain ETS and PB concentrations, and decreased VPA concentrations, but was without effect on CZP concentrations. In contrast, PB significantly decreased and VPA increased total brain STP concentrations while CZP and ETS were without effect. Furthermore, while isobolographic analysis revealed that STP and CZP in combination, at the fixed ratios of 1:1 and 3:1, were supraadditive (synergistic; p < 0.05), the combinations of STP with CZP (1:3), ETS, PB, or VPA (at all fixed ratios of 1:3, 1:1, and 3:1) were barely additivity in terms of acute neurotoxic adverse effects in the chimney test. Additionally, none of the examined combinations of STP with conventional AEDs (CZP, ETS, PB, VPA--at their median effective doses from the PTZ-test) affected long-term memory, threshold for the first pain reaction, neuromuscular tone, and acute thermal pain. CONCLUSIONS: Based on BI values, the combination of STP with PB at the fixed ratio of 1:3 appears to be a particularly favourable combination. In contrast, STP and CZP or ETS (at the fixed ratios of 1:1 and 3:1) were unfavorable combinations. However, these conclusions are confounded by the fact that STP is associated with significant pharmacokinetic interactions. The remaining combinations of STP with PB (1:1 and 3:1), CZP (1:3), ETS (1:3), and VPA (at all fixed ratios of 1:3, 1:1, and 3:1) do not appear to be potential favorable AED combinations.
机译:用途:等效线描图分析用于表征替比妥尔(STP)与氯硝西am(CZP),乙巯乙酰亚胺(ETS),苯巴比妥(PB)和丙戊酸盐(VPA)之间的相互作用,以抑制戊四氮(PTZ)诱导的小鼠阵挛性癫痫发作。方法:在PTZ和烟囱测试中,以固定比例1:3、1:1和3:1的比例评估了STP与各种常规抗癫痫药(AED)联合使用对抗惊厥和急性不利(神经毒性)的作用。使用等效线描记法分析小鼠。另外,计算保护指数(PI)和有益指数(BI)以确定其药理特性,以便可以建立相对于有利组合的评级。此外,不良反应范式是通过逐步被动回避任务(长期记忆),初次疼痛反应的阈值,握力测试(神经肌肉张力)和热板测试(急性热痛)确定的。 )。还测量了脑AED浓度,以确定对药效相互作用的任何药代动力学贡献。结果:就PTZ测试中的阵挛性癫痫发作抑制而言,由STP和CZP,ETS,PB和VPA组成的所有AED组合(固定比例为1:3、1:1和3:1)是相加的。但是,这些相互作用由于药代动力学相互作用而导致大脑AED浓度变化而变得复杂。因此,STP显着增加了总脑ETS和PB浓度,并降低了VPA浓度,但对CZP浓度没有影响。相反,PB明显降低,VPA增加了总脑STP浓度,而CZP和ETS没有影响。此外,等效线描记法分析显示,STP和CZP的组合以固定比例1:1和3:1具有超加性(协同作用; p <0.05),而STP和CZP的组合(1:3),ETS,就烟囱试验中的急性神经毒性不良反应而言,PB或VPA(所有固定比率为1:3、1:1和3:1)几乎没有可加性。此外,STP与常规AED(CZP,ETS,PB,VPA-以PTZ测试得出的中位有效剂量)的任何检查组合均未影响长期记忆,首次疼痛反应阈值,神经肌肉紧张和急性热痛。结论:基于BI值,固定比例为1:3的STP与PB的组合似乎是一个特别有利的组合。相反,STP和CZP或ETS(固定比例为1:1和3:1)是不利的组合。但是,这些结论被STP与显着的药代动力学相互作用相关的事实所迷惑。 STP与PB(1:1和3:1),CZP(1:3),ETS(1:3)和VPA的其余组合(所有固定比例为1:3、1:1和3: 1)似乎不是潜在的有利AED组合。

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