卡马西平与一些抗癫痫药物在儿童和青少年癫痫治疗中的药代动力学相互作用。

B Steinborn
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引用次数: 0

摘要

目的:本研究的目的是获得卡马西平(CBZ)及其不与蛋白质结合的组分在拉莫三嗪(LTG)、托吡酯(TPM)、维加巴林(VGB)或丙戊酸(VPA)联合治疗儿童和青少年癫痫中的药代动力学数据。材料和方法:本次研究的参与者为波兹纳夫医科大学发育神经内科控制的55名癫痫患者。所有患者均采用CBZ联合LTG、TPM、VGB或VPA治疗。在稳态条件下采集血液样本,在早晨给药前,随后每3或2次采集24小时。使用TDX分析仪(美国雅培诊断公司)测定血浆中CBZ水平。游离CBZ馏分采用超滤系统(Amicon, USA)分离。总CBZ和游离CBZ的药动学计算采用标准化程序的单室模型。结果:四组CBZ联合LTG、TPM、VGB、VPA双药组未结合CBZ的药动学参数均无显著差异。总CBZ的药代动力学变化与CBZ浓度、曲线下面积(AUC)、L/D/kg比值和清除率(Cl)/kg的差异有关。CBZ+VGB双治疗导致CBZ总浓度升高。在CBZ+VPA联合治疗组,未结合CBZ未见增加。结论:儿童CBZ与LTG、TPM、VGB或VPA的药动学相互作用仅与CBZ总参数的变化有关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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Pharmacokinetic interactions of carbamazepine with some antiepileptic drugs during epilepsy treatment in children and adolescents.

Purpose: The aim of the study was to obtain pharmacokinetic data for carbamazepine (CBZ) and its fractions not bound with proteins in bitherapy with lamotrigine (LTG), topiramate (TPM), vigabatrin (VGB) or valproic acid (VPA) in children and adolescents treated for epilepsy.

Material and methods: The participants of the presented investigations were fifty-five patients with epilepsy who were under control of The Department of Developmental Neurology, University of Medical Sciences in Poznaf. All of patients were treated with CBZ in bitherapy with LTG, TPM, VGB or VPA. The blood samples were taken under steady-state conditions, before the morning dose and subsequently every 3 or 2 for 24 h. The plasma levels of CBZ were determined using TDX analyzer (Abbott Diagnostic Division, USA). Free CBZ fraction was isolated with the use of ultrafiltration system (Amicon, USA). For pharmacokinetic calculations of total and free CBZ, one-compartment model was used according to standardized procedure.

Results: No significant differences in pharmacokinetic parameters of unbound CBZ in four groups of patients on bitherapy with CBZ and LTG, TPM, VGB or VPA were found. The changes in pharmacokinetics of total CBZ were related with difference in CBZ concentrations, area under curve (AUC), L/D/kg ratios and clearance (Cl)/kg. CBZ+VGB bitherapy led to higher total CBZ concentrations. In the group on bitherapy with CBZ+VPA, no increase in unbound CBZ was detected.

Conclusions: Pharmacokinetic interactions of CBZ with LTG, TPM, VGB or VPA in children are associated only with the changes in total CBZ parameters.

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The cortical evoked potentials in children with developmental coordination disorder (DCD). Neuroprotection possibilities in epileptic children. New antiepileptic drugs--an overview. Youth's knowledge and attitude to epilepsy. Community nursing care of the elderly during transformation of the primary health care system.
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