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Evaluation of Potential Drug–Drug Interaction Between Delayed‐Release Dimethyl Fumarate and a Commonly Used Oral Contraceptive (Norgestimate/Ethinyl Estradiol) in Healthy Women

机译:评估延迟释放二甲基富马酸酯之间的潜在药物 - 药物相互作用和健康女性中常用口服避孕药(NORESTIMATE /乙炔雌二醇)

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摘要

Abstract Delayed‐release dimethyl fumarate (DMF) is an oral therapy for relapsing multiple sclerosis with anti‐inflammatory and neuroprotective properties. This 2‐period crossover study was conducted to evaluate the potential for drug–drug interaction between DMF (240 mg twice daily) and a combined oral contraceptive (OC; norgestimate 250 μg, ethinyl estradiol 35 μg). Forty‐six healthy women were enrolled; 32 completed the study. After the lead‐in period (OC alone), 41 eligible participants were randomized 1:1 to sequence 1 (OC and DMF coadministration in period 1; OC alone in period 2) or sequence 2 (regimens reversed). Mean concentration profiles of plasma norelgestromin (primary metabolite of norgestimate) and ethinyl estradiol were superimposable following OC alone and OC coadministered with DMF, with 90% confidence intervals of geometric mean ratios for area under the plasma concentration–time curve over the dosing interval and peak plasma concentration contained within the 0.8–1.25 range. Low serum progesterone levels during combined treatment confirmed suppression of ovulation. The pharmacokinetics of DMF (measured via its primary active metabolite, monomethyl fumarate) were consistent with historical data when DMF was administered alone. No new safety concerns were identified. These results suggest that norgestimate/ethinyl estradiol–based OCs may be used with DMF without dose modification.
机译:摘要延迟释放二甲基富马酸盐(DMF)是一种口服治疗,用于复发多发性硬化,具有抗炎和神经保护性能。进行该2周期的交叉研究以评估DMF(每日两次240毫克)和组合口服避孕药物(OC; NORESTIMATE250μg,乙炔雌二醇35μg)的药物 - 药物相互作用的可能性。注册了四十六名健康妇女; 32完成了这项研究。在进入期(OC单独)之后,41个符合条件的参与者随机1:1至序列1(OC和DMF共同分析在1期间; OC单独在第2期)或序列2(逆转的方案)。血浆Norelgestromin(Norestmate的初级代谢素)和乙炔雌二醇的平均浓度谱在单独的OC和oc与DMF共同调节后,在剂量间隔和峰值下的等离子体浓度 - 时间曲线下具有90%的几何平均比的置信区间血浆浓度在0.8-1.25范围内。结合治疗期间低血清孕酮水平证实抑制排卵。当单独给药时,DMF的药代动力学(通过其初级活性代谢物,单甲基富马酸盐测量)与历史数据一致。没有确定新的安全问题。这些结果表明,非糖基因/乙炔雌二醇基OC也可以与DMF一起使用而没有剂量改性。

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