Brivaracetam exposure-response predictions in pediatric patients from age 1 month: Extrapolation of levetiracetam adult-pediatric scaling to brivaracetam

IF 2 4区 医学 Q3 CLINICAL NEUROLOGY
Rik Schoemaker , Walter Krauwinkel , Jan-Peer Elshoff , Armel Stockis
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引用次数: 0

Abstract

Background

An adult population pharmacokinetic/pharmacodynamic (PK/PD) model for the antiseizure medication (ASM) brivaracetam (BRV) was previously extended to children aged 4–16 years by using a pediatric BRV population PK model. Effects were scaled using information from a combined adult-pediatric PK/PD model of a related ASM, levetiracetam (LEV).

Objective

To scale an existing adult population PK/PD model for BRV to children aged 1 month to < 4 years using information from a combined adult-pediatric PK/PD model for LEV, and to predict the effective dose of BRV in children aged 1 month to < 4 years using the adult BRV PK/PD model modified for the basal seizure rate in children.

Material and methods

An existing adult population PK/PD model for BRV was scaled to children aged from 1 month to < 4 years using information from a combined adult-pediatric PK/PD model for LEV, an ASM binding to the same target protein as BRV. An existing adult-pediatric PK/PD model for LEV was extended using data from UCB study N01009 (NCT00175890) to include children as young as 1 month of age. The BRV population PK model was updated with data up to 180 days after first administration from BRV pediatric studies N01263 (NCT00422422) and N01266 (NCT01364597). PK and PD simulations for BRV were performed for a range of mg/kg doses to predict BRV effect in pediatric participants, and to provide dosing recommendations.

Results

The extended adult-pediatric LEV PK/PD model was able to describe the adult and pediatric data using the same PD model parameters in adults and children and supported the extension of the adult BRV PK/PD model to pediatric patients aged 1 month to < 4 years. Simulations predicted exposures similar to adults receiving BRV 100 mg twice daily (b.i.d.), when using 3 mg/kg b.i.d. for weight < 10 kg, 2.5 mg/kg b.i.d. for weight ≥ 10 kg and < 20 kg, and 2 mg/kg b.i.d. for weight ≥ 20 kg in children aged 1 month to < 4 years. PK/PD simulations show that maximum BRV response is expected to occur with 2–3 mg/kg b.i.d. dosing of BRV in children aged 1 month to < 4 years, with an effective dose of 1 mg/kg b.i.d. for some participants.

Conclusion

Development of an adult-pediatric BRV PK/PD model allowed characterization of the exposure-response relationship of BRV in children aged 1 to < 4 years, providing a maximal dose allowance based on weight.

对 1 个月以上儿童患者的 Brivaracetam 暴露-反应预测:将左乙拉西坦的成人-儿童比例外推至布利伐沙坦
以前曾利用一个小儿 BRV 群体 PK 模型,将抗癫痫药物 (ASM) brivaracetam (BRV) 的成人群体药代动力学/药效学 (PK/PD) 模型扩展到 4-16 岁的儿童。利用相关 ASM 左乙拉西坦(LEV)的成人-儿童暴露-反应(PK/PD)联合模型中的信息对其效应进行了缩放。利用来自左乙拉西坦成人-儿科暴露-反应(PK/PD)联合模型的信息,将现有的BRV成人人群PK/PD模型扩展到1个月至小于4岁的儿童,并利用根据儿童基础癫痫发作率修改的成人BRV PK/PD模型,预测1个月至小于4岁儿童服用BRV的有效剂量。利用与 BRV 相同的靶蛋白结合的 ASM--LEV 的成人-儿科 PK/PD 模型的信息,将 BRV 现有的成人 PK/PD 模型按比例扩展到 1 个月至小于 4 岁的儿童。利用 UCB N01009 (NCT00175890) 研究的数据,对现有的 LEV 成人-儿童 PK/PD 模型进行了扩展,以纳入 1 个月大的儿童。利用 BRV 儿科研究 N01263 (NCT00422422) 和 N01266 (NCT01364597) 中首次给药后 180 天内的数据更新了 BRV 群体 PK 模型。针对一系列 mg/kg 剂量进行了 BRV 的 PK 和 PD 模拟,以预测 BRV 对儿科参与者的影响,并提供剂量建议。扩展的成人-儿童LEV PK/PD模型能够使用成人和儿童相同的PD模型参数描述成人和儿童数据,并支持将成人BRV PK/PD模型扩展到1个月至小于4岁的儿童患者。当体重<10千克的儿童使用3毫克/千克体重剂量(b.i.d.)、体重≥10千克和<20千克的儿童使用2.5毫克/千克体重剂量(b.i.d.)以及体重≥20千克的儿童使用2毫克/千克体重剂量(b.i.d.)时,模拟预测的暴露量与成人每日两次服用BRV 100毫克(b.i.d.)的暴露量相似。PK/PD模拟显示,在1个月至小于4岁的儿童中,BRV剂量为2-3mg/kg b.i.d.时,预计会产生最大的BRV反应,部分参与者的有效剂量为1mg/kg b.i.d.。通过建立成人-儿童BRV PK/PD模型,可确定BRV在1至<4岁儿童中的暴露-反应关系,并根据体重提供最大剂量允许值。
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来源期刊
Epilepsy Research
Epilepsy Research 医学-临床神经学
CiteScore
0.10
自引率
4.50%
发文量
143
审稿时长
62 days
期刊介绍: Epilepsy Research provides for publication of high quality articles in both basic and clinical epilepsy research, with a special emphasis on translational research that ultimately relates to epilepsy as a human condition. The journal is intended to provide a forum for reporting the best and most rigorous epilepsy research from all disciplines ranging from biophysics and molecular biology to epidemiological and psychosocial research. As such the journal will publish original papers relevant to epilepsy from any scientific discipline and also studies of a multidisciplinary nature. Clinical and experimental research papers adopting fresh conceptual approaches to the study of epilepsy and its treatment are encouraged. The overriding criteria for publication are novelty, significant clinical or experimental relevance, and interest to a multidisciplinary audience in the broad arena of epilepsy. Review articles focused on any topic of epilepsy research will also be considered, but only if they present an exceptionally clear synthesis of current knowledge and future directions of a research area, based on a critical assessment of the available data or on hypotheses that are likely to stimulate more critical thinking and further advances in an area of epilepsy research.
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