Bioequivalence of Two Oral Dimethyl Fumarate Extended Release Capsules in Healthy Subjects: A Randomized, Open Label, Single-Dose, 2-Way Crossover Study

Journal of Bioequivalence & Bioavailability Pub Date : 2018-01-01 DOI:10.4172/0975-0851.1000380

Maligne Ge, Feleder Ec, Yerino Ga, Otero Am, Roldán Eja

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Abstract

The hypothesis for the design of this project was that the extended release formulation containing dimethyl fumarate 240 mg DIMEFUL®, developed by Gador will present similar bioavailability with respect to the reference formulation, TECFIDERA® by Biogen Idec, measured in terms of speed and absorption. A clinical study of single-dose bioequivalence (in 2 stages) was designed to be carried out in healthy subjects. This study was opened of two periods, two sequences, crossed, randomized under fasting conditions. Eight out of ten subjects involved in this pilot study (stage 1) were randomized and completed the 2 periods of administration of the treatments. Data of all the subjects who completed the 2 periods of treatment administration were used for pharmacokinetic purposes. The design of the study was adequate to determine the bioequivalence of the Test and Reference Products. The 7- day washout period was sufficient to allow the complete elimination of the formulations before the next dosing period. Conclusion: In relation to monomethyl fumarate; The extended release formulation containing dimethyl fumarate 240 mg, developed by Gador, DIMEFUL®, presents similar bioavailability, measured in terms of speed and extension of absorption in relation to the reference formulation, TECFIDERA® by Biogen Idec. Intrasubject CVs were on the order of 30% to 40% for the 3 pharmacokinetic parameters; indicating that the molecule and/or the formulation shows high variability in absorption and must be considered for the calculation of sample size of Stage 2. This improved process will serve for clinical assessment in patients. Individual plasma concentrations showed results lower than the lower limit of quantification of the validated analytical method. It is suggested to adjust the method by lowering said level for Stage 2. It is possible to consider extending the range of Bioequivalence for Cmax to 70-143% in Stage 2; since the intrasubject CV was >30% and the Reference geometric mean is between 0.80-1.25 in Stage 1.

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两种口服富马酸二甲酯缓释胶囊在健康受试者中的生物等效性:一项随机、开放标签、单剂量、双向交叉研究

本项目设计的假设是，Gador开发的含有富马酸二甲酯240 mg DIMEFUL®的缓释制剂在速度和吸收方面与Biogen Idec的参比制剂TECFIDERA®具有相似的生物利用度。设计了一项在健康受试者中进行的单剂量生物等效性临床研究(分两个阶段)。本研究在禁食条件下分为两个时间段，两个序列，交叉，随机。参与该初步研究(第一阶段)的10名受试者中有8名被随机分配并完成了2个疗程的治疗。完成2期治疗的所有受试者的数据用于药代动力学目的。该研究的设计足以确定试验产品和参比产品的生物等效性。7天的洗脱期足以使制剂在下一个给药期前完全排出。结论:与富马酸单甲基有关;Gador公司开发的含有富马酸二甲酯240 mg的缓释制剂DIMEFUL®与Biogen Idec公司的参比制剂TECFIDERA®具有相似的生物利用度，在吸收速度和扩展方面进行了测量。3个药代动力学参数的受试者内cv值为30% ~ 40%;表明分子和/或配方在吸收方面表现出很高的可变性，必须在计算第二阶段的样本量时加以考虑。这一改进的过程将用于患者的临床评估。个体血浆浓度显示的结果低于验证分析方法的定量下限。建议调整方法，在第二阶段降低该水平。在第二阶段可以考虑将Cmax的生物等效性范围扩大到70-143%;因为第一阶段受试者内CV >30%，参考几何平均值在0.80-1.25之间。

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Journal of Bioequivalence & Bioavailability

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