Development and Validation of an UHPLC-MS/MS Assay for the Therapeutic Monitoring of Brivaracetam Plasma Concentrations in Patients with Epilepsy

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Development and Validation of an UHPLC-MS/MS Assay for the Therapeutic Monitoring of Brivaracetam Plasma Concentrations in Patients with Epilepsy

机译：UHPLC-MS / MS测定的开发和验证癫痫患者血糖素血浆浓度的治疗监测

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Background: Brivaracetam is an antiepileptic drug used as an add-on therapy for partial-onset seizures in subjects aged 4 years and older. Owing to potential drug interactions and intersubject variability in plasma concentrations, therapeutic monitoring for brivaracetam may be useful. The aim of this study was to develop a simplified method for measuring brivaracetam plasma concentrations applicable to therapeutic drug monitoring in epilepsy. Methods: An ultra high-pressure liquid chromatography-tandem mass spectrometry method was developed and validated according to current guidelines for bioanalytical methods. Sample preparation (100 mu L) involved only a simple precipitation step by acetonitrile. Brivaracetam-d7 was used as internal standard. The chromatographic analysis was performed by a Synergi Fusion column using 0.1% formic acid in water/acetonitrile as a binary gradient mobile phase, at a flow rate of 0.3 mL/min. Both brivaracetam and the internal standard eluted at 1.01 minutes. This method was applied to measure trough and 1-hour postmorning dose brivaracetam plasma concentrations of 11 patients with epilepsy. Results: The method was validated over a concentration range of 0.10-10 mcg/mL. The mean recovery was 95%. Both intra- and inter-assay imprecision and inaccuracy were <15% for all quality control samples. The lower limit of quantitation and detection was 0.10 and 0.05 mcg/mL, respectively. No interferences or carry-over was observed. Median (25%-75% quartiles) trough and 1-hour postdosing brivaracetam plasma concentrations were 0.61 mcg/mL (0.47-0.83 mcg/mL) and 1.55 mcg/mL (1.24-2.12 mcg/mL), respectively, at a median dose of 80 mg/d (50-150 mg/d). Large, up to 8-fold, intrasubject fluctuations of brivaracetam concentrations between trough and 1-hour postdosing were observed. Conclusions: The present assay is faster and simpler than previously published analytical reports for brivaracetam in human plasma and is suitable for therapeutic drug monitoring.

机译：背景：Brivaracetam是一种抗癫痫药物，用作4岁及以上的受试者的部分发病癫痫发作的抗癫痫药物。由于血浆浓度的潜在药物相互作用和三立管可变性，Brivaracetam的治疗监测可能是有用的。本研究的目的是开发一种简化的方法，用于测量适用于癫痫中治疗药物监测的Brivaracetam血浆浓度。方法：根据生物分析方法的当前指南，开发和验证了超高压液相色谱 - 串联质谱法。样品制备（100μl）仅涉及乙腈的简单沉淀。 Brivaracetam-D7用作内标。通过0.1％甲酸在水/乙腈中的Synergi融合柱作为二元梯度流动相，通过0.3ml / min的流速进行色谱分析。 Brivaracetam和内标在1.01分钟后洗脱。该方法应用于测量槽和1小时后的癫痫患者的1小时后剂量Bivaracetam等离子体浓度。结果：该方法在0.10-10mcg / ml的浓度范围内验证。平均回收率为95％。对于所有质量控制样品，分析和测定间的不精确和不准确性的不准确性<15％。定量和检测的下限分别为0.10和0.05mcg / ml。没有观察到干扰或随身携带。中位数分别在中位数为0.61mcg / ml（0.47-0.83mcg / ml）和1.55mcg / ml（1.24-2.12mcg / ml）的0.61mcg / ml（1.24-2.12mcg / ml）和1小时的中位数（25％-75％）槽和1小时80 mg / d的剂量（50-150 mg / d）。较大，高达8倍，谷类酸蛋白浓度的肠道喷射波动浓度在槽中和1小时后的后末代末端。结论：目前的测定比以前公布的人血浆中的Brivaracetam发表的分析报告更快，更简单，适用于治疗药物监测。

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《Therapeutic Drug Monitoring》 |2020年第3期|共7页
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中图分类生药学（天然药物学）;
关键词
brivaracetam; antiepileptic drugs; LC-MS; MS; therapeutic drug monitoring;

机译：Brivaracetam;抗癫痫药物;LC-MS;MS;治疗药物监测;

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1. Development and Validation of an UHPLC-MS/MS Assay for the Therapeutic Monitoring of Brivaracetam Plasma Concentrations in Patients with Epilepsy [J] . Therapeutic Drug Monitoring . 2020,第3期

机译：UHPLC-MS / MS测定的开发和验证癫痫患者血糖素血浆浓度的治疗监测
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Development and Validation of an UHPLC-MS/MS Assay for the Therapeutic Monitoring of Brivaracetam Plasma Concentrations in Patients with Epilepsy

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