预测部分发作性癫痫从辅助治疗转换为醋酸埃斯卡巴西平800毫克每日1次的单一治疗的疗效。

IF 3.1 Q2 PHARMACOLOGY & PHARMACY
Clinical Pharmacology : Advances and Applications Pub Date : 2017-06-27 eCollection Date: 2017-01-01 DOI:10.2147/CPAA.S133815
Soujanya Sunkaraneni, Julie A Passarell, Elizabeth A Ludwig, Jill Fiedler-Kelly, Janet K Pitner, Todd A Grinnell, David Blum
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引用次数: 1

摘要

目的:醋酸埃斯卡巴西平(ESL)是一种每日一次(QD)口服抗癫痫药物(AED),适用于部分发作性癫痫发作(POS)。临床研究逐渐转换为ESL 1200和1600 mg QD单药治疗,以前曾在1或2个aed控制不佳的POS患者中进行过。本报告描述了血浆eslicarbazepine (ESL的主要活性代谢物)浓度和单药治疗研究结束时间的建模和模拟,以预测转换为低剂量800 mg ESL单药治疗的疗效,作为需要或不耐受高剂量的患者的选择,因为该方案是poss的有效辅助治疗。先前开发的ESL单药治疗人群药代动力学模型用于预测1500名虚拟患者的最低血浆eslicarbazepine浓度(Cmin),这些患者在基线时服用1个(n= 1000)或2个(n=500) aed,以ESL 400 mg QD治疗1周,随后以800 mg QD治疗17周(类似于ESL单药治疗试验,在滴定到随机ESL剂量后的前6周内停用其他aed)。在500个模拟ESL单药治疗试验中,使用模型预测的Cmin作为时变协变量和基线aed数量来确定每个患者达到退出标准的每周概率(65.3%阈值),表明癫痫控制恶化。使用先前开发的扩展Cox比例危害暴露-反应模型将时变埃司卡巴西平暴露与研究退出时间联系起来。结果:对于接受ESL单药治疗(800mg QD)的虚拟患者,基线时服用1个AED的患者在112天退出率的95%预测上限(34.9%)远低于历史对照试验的65.3%阈值,而服用2个AED的患者的估计(70.6%)略高于历史对照阈值。结论:这一基于模型的评估支持转换为ESL 800mg QD单药治疗服用1 AED的成人POS。然而,对于同时服用2种AEDs的患者,如果考虑转换为ESL单药治疗,开处方者应考虑维持剂量1200或1600 mg ESL QD,以减少癫痫发作恶化的可能性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Prediction of efficacy for conversion from adjunctive therapy to monotherapy with eslicarbazepine acetate 800 mg once daily for partial-onset epilepsy.

Prediction of efficacy for conversion from adjunctive therapy to monotherapy with eslicarbazepine acetate 800 mg once daily for partial-onset epilepsy.

Prediction of efficacy for conversion from adjunctive therapy to monotherapy with eslicarbazepine acetate 800 mg once daily for partial-onset epilepsy.

Prediction of efficacy for conversion from adjunctive therapy to monotherapy with eslicarbazepine acetate 800 mg once daily for partial-onset epilepsy.

Purpose: Eslicarbazepine acetate (ESL) is a once-daily (QD) oral antiepileptic drug (AED) indicated for partial-onset seizures (POS). Clinical studies of gradual conversion to ESL 1,200 and 1,600 mg QD monotherapies were previously conducted in patients with POS who were not well-controlled by 1 or 2 AEDs. This report describes modeling and simulation of plasma eslicarbazepine (primary active metabolite of ESL) concentrations and time to monotherapy study exit to predict efficacy for conversion to ESL monotherapy at a lower dose of 800 mg, as an option for patients requiring or not tolerating higher doses since this regimen is effective in adjunctive therapy for POS.

Patients and methods: A previously developed population pharmacokinetic model for ESL monotherapy was used to predict minimum plasma eslicarbazepine concentration (Cmin) in 1,500 virtual patients taking 1 (n=1,000) or 2 (n=500) AEDs at baseline, treated with ESL 400 mg QD for 1 week, followed by 800 mg QD for 17 weeks (similar to ESL monotherapy trials where the other AEDs were withdrawn during the first 6 weeks following titration to the randomized ESL dose). Model-predicted Cmin as a time-varying covariate and number of baseline AEDs were used to determine the weekly probability of each patient meeting exit criteria (65.3% threshold) indicative of worsening seizure control in 500 simulated ESL monotherapy trials. A previously developed extended Cox proportional hazards exposure-response model was used to relate time-varying eslicarbazepine exposure to the time to study exit.

Results: For virtual patients receiving ESL monotherapy (800 mg QD), the 95% upper prediction limit for exit rate at 112 days of 34.9% in patients taking 1 AED at baseline was well below the 65.3% threshold from historical control trials, while the estimate for patients taking 2 AEDs (70.6%) was slightly above the historical control threshold.

Conclusion: This model-based assessment supports conversion to ESL 800 mg QD monotherapy for POS in adults taking 1 AED. For patients taking 2 concomitant AEDs, however, prescribers should consider maintenance doses of 1,200 or 1,600 mg ESL QD to reduce the likelihood of seizure worsening if conversion to ESL monotherapy is contemplated.

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来源期刊
CiteScore
4.60
自引率
0.00%
发文量
14
审稿时长
16 weeks
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