多次静脉给药后HX575(重组人epoetin α)和比较物epoetin α的生物等效性:一项开放标签随机对照试验。

Fritz Sörgel, Ursula Thyroff-Friesinger, Andrea Vetter, Bernhard Vens-Cappell, Martina Kinzig
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引用次数: 8

摘要

背景:HX575是一种重组人促生成素,于2007年在欧洲药品管理局生物仿制药批准途径下被批准在欧洲使用。因此,为了证明HX575与现有的epoetin alfa的生物等效性,在多次静脉给药后,比较HX575和比较物epoetin alfa对稳态循环浓度的药代动力学和药效学反应。方法:对80名健康成年男性进行开放、随机、平行组研究。受试者随机接受多次静脉注射剂量为100 IU/kg体重的HX575或比较药物eppoetin,每周3次,持续4周。采用酶联免疫吸附法测定血清生成素浓度,并比较两种治疗方法的药代动力学参数。以血液学特征的作用曲线下面积比和时间过程作为疗效评价的替代参数。结果:两种治疗的血液学特征相似,从他们的人群平均曲线和AUECHb比率和90%置信区间(99.9%[98.5-101.2%])确定,这是本研究的主要药效学终点。单次给药后药代动力学参数差异不大,稳态给药后无差异。多次给药后,HX575在外源性生成素暴露率和暴露程度方面与对照物具有生物等效性(AUCtau比值和90%置信区间:89.2%[82.5-96.2%])。研究药物耐受性良好,两种治疗的安全性无临床相关差异。未检出抗生成素抗体。结论:在稳态循环药物浓度下,HX575与比较物epoetin具有生物等效的药代动力学特征和药效学作用。这支持了HX575和比较物epoetin α在静脉注射时同样有效,并且可以作为治疗替代的结论。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Bioequivalence of HX575 (recombinant human epoetin alfa) and a comparator epoetin alfa after multiple intravenous administrations: an open-label randomised controlled trial.

Background: HX575 is a human recombinant epoetin alfa that was approved for use in Europe in 2007 under the European Medicines Agency biosimilar approval pathway. Therefore, in order to demonstrate the bioequivalence of HX575 to an existing epoetin alfa, the pharmacokinetic and pharmacodynamic response to steady state circulating concentrations of HX575 and a comparator epoetin alfa were compared following multiple intravenous administrations.

Methods: An open, randomised, parallel group study was conducted in 80 healthy adult males. Subjects were randomised to multiple intravenous doses of 100 IU/kg body weight of HX575 or of the comparator epoetin alfa three-times-weekly for four weeks. Serum epoetin concentrations were measured using an enzyme-linked immunosorbent assay and pharmacokinetic parameters for the two treatments were compared. The time course and area under the effect curve ratio of haematological characteristics were used as surrogate parameters for efficacy evaluation.

Results: The haematological profiles of both treatments were similar, as determined from their population mean curves and the AUECHb ratio and 90% confidence interval (99.9% [98.5-101.2%]), the primary pharmacodynamic endpoint of this study. The pharmacokinetic parameters after the treatments showed minor differences after single dosing, but not at steady state doses. After multiple doses, HX575 was bioequivalent to the comparator with respect to the rate and extent of exposure of exogenous epoetin (AUCtau ratio and 90% confidence interval: 89.2% [82.5-96.2%]). Study medication was well tolerated with no clinically relevant differences between safety profiles of the treatments. Anti-epoetin antibodies were not detected.

Conclusion: HX575 and the comparator epoetin alfa were bioequivalent at steady state circulating drug concentrations with respect to their pharmacokinetic profile and pharmacodynamic action. This supports the conclusion that HX575 and the comparator epoetin alfa, when administered intraveneously, will be equally efficacious and may be interchangeable as therapy.

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