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苯妥英钠与丙戊酸钠之间的药效学相互作用会改变癫痫阈值和发作模式。

Pharmacodynamic interaction between phenytoin and sodium valproate changes seizure thresholds and pattern.

作者信息

Della Paschoa O E, Kruk M R, Hamstra R, Voskuyl R A, Danhof M

机构信息

Division of Pharmacology, Leiden/Amsterdam Center for Drug Research, Leiden, The Netherlands.

出版信息

Br J Pharmacol. 1998 Nov;125(5):997-1004. doi: 10.1038/sj.bjp.0702155.

Abstract
  1. In this study we used cortical stimulation to assess the effects of phenytoin (PHT), sodium valproate (VPA), and their interaction on total motor seizure and on the constituent elements of the seizure. 2. PHT (40 mg kg(-1)) was administered as an intravenous bolus infusion to animals receiving either a continuous infusion of VPA or saline. VPA plasma concentration was maintained at levels that produced no detectable anticonvulsant effect. 3. Analysis of ictal components (eyes closure, jerk, gasp, forelimb, clonus, and hindlimb tonus) and their durations revealed both qualitative and quantitative differences in drug effects. 4. The anticonvulsant effect is represented by the increase in the duration of the stimulation required to reach a given seizure threshold. PHT significantly increased the duration of the stimulation and of the motor seizure. This increase was greatly enhanced by VPA. In addition, ictal component analysis revealed that the combination of PHT and VPA causes the reduction of a specific seizure component (JERK). 5. Neither the free fraction of PHT nor the biophase equilibration kinetics changes in the presence of VPA. It is concluded that the synergism may be due to a pharmacodynamic rather than a pharmacokinetic interaction.
摘要
  1. 在本研究中,我们使用皮质刺激来评估苯妥英(PHT)、丙戊酸钠(VPA)及其相互作用对全面性运动性癫痫发作以及癫痫发作构成要素的影响。2. 以静脉推注的方式给持续输注VPA或生理盐水的动物注射PHT(40mg/kg(-1))。将VPA血浆浓度维持在未产生可检测到的抗惊厥作用的水平。3. 对发作期成分(闭眼、抽搐、喘息、前肢、阵挛和后肢强直)及其持续时间的分析揭示了药物作用在定性和定量方面的差异。4. 抗惊厥作用表现为达到给定癫痫发作阈值所需刺激持续时间的增加。PHT显著增加了刺激持续时间和运动性癫痫发作的持续时间。VPA极大地增强了这种增加。此外,发作期成分分析表明,PHT和VPA的联合使用导致特定癫痫发作成分(抽搐)减少。5. 在VPA存在的情况下,PHT的游离分数和生物相平衡动力学均未改变。得出的结论是,这种协同作用可能是由于药效学相互作用而非药代动力学相互作用。

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