α 1 -抗胰蛋白酶缺乏症中Prolastin®-C与Prolastin®的药代动力学比较:一项随机研究。

James M Stocks, Mark L Brantly, Laurene Wang-Smith, Michael A Campos, Kenneth R Chapman, Friedrich Kueppers, Robert A Sandhaus, Charlie Strange, Gerard Turino
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引用次数: 35

摘要

背景:α 1抗胰蛋白酶(AAT)缺乏的特点是血液中α 1蛋白酶抑制剂(α 1 -PI)水平低,可能导致肺气肿。α 1 -PI保护肺组织免受蛋白水解酶作用造成的损害。用Prolastin®(α₁-蛋白酶抑制剂[人])增加α₁-PI水平的增强疗法治疗AAT缺乏症已有20多年的历史。对Prolastin生产工艺的修改,包括额外的纯化和病原体还原步骤,导致了α₁-PI产品的开发,命名为Prolastin®-C (α₁-蛋白酶抑制剂[人])。在AAT缺乏的受试者中,评估了促生素c与促生素的药动学可比性。方法:共有24名受试者随机接受60 mg/kg功能活性催活素c或催活素每周静脉输注,持续8周,然后切换到替代治疗再持续8周。第一次给药后7天抽取药代动力学血浆样本,第二次给药后10天抽取药代动力学血浆样本。药代动力学可比性的主要终点是通过效价(功能活性)测定α₁-PI给药后7天(AUC₀₇(天))血浆浓度与时间曲线下的面积。交叉期之后是8周的开放标签治疗期,仅使用促生素c。结果:Prolastin- c和Prolastin的平均AUC₀₇(天)分别为155.9和152.4 mg*h/mL。Prolastin- c与Prolastin的AUC 0₀₇(days)的几何最小二乘平均比值点估计为1.03,90%置信区间为0.97-1.09,表明两种产品的药代动力学等效。两种治疗的不良事件相似,Prolastin- c(仅双盲治疗阶段)和Prolastin每次输注的发生率分别为0.117和0.078 (p = 0.744)。在研究过程中,没有任何受试者出现人类免疫缺陷病毒、乙型或丙型肝炎或细小病毒B19的治疗突发病毒感染。结论:促生素c与促生素具有药代动力学等效性和相当的安全性。试验注册:ClinicalTrials.gov标识符:NCT00295061。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Pharmacokinetic comparability of Prolastin®-C to Prolastin® in alpha₁-antitrypsin deficiency: a randomized study.

Pharmacokinetic comparability of Prolastin®-C to Prolastin® in alpha₁-antitrypsin deficiency: a randomized study.

Pharmacokinetic comparability of Prolastin®-C to Prolastin® in alpha₁-antitrypsin deficiency: a randomized study.

Pharmacokinetic comparability of Prolastin®-C to Prolastin® in alpha₁-antitrypsin deficiency: a randomized study.

Background: Alpha1-antitrypsin (AAT) deficiency is characterized by low blood levels of alpha1-proteinase inhibitor (alpha₁-PI) and may lead to emphysema. Alpha₁-PI protects pulmonary tissue from damage caused by the action of proteolytic enzymes. Augmentation therapy with Prolastin® (Alpha₁-Proteinase Inhibitor [Human]) to increase the levels of alpha₁-PI has been used to treat individuals with AAT deficiency for over 20 years. Modifications to the Prolastin manufacturing process, incorporating additional purification and pathogen-reduction steps, have led to the development of an alpha₁-PI product, designated Prolastin®-C (Alpha₁-Proteinase inhibitor [Human]). The pharmacokinetic comparability of Prolastin-C to Prolastin was assessed in subjects with AAT deficiency.

Methods: In total, 24 subjects were randomized to receive 60 mg/kg of functionally active Prolastin-C or Prolastin by weekly intravenous infusion for 8 weeks before crossover to the alternate treatment for another 8 weeks. Pharmacokinetic plasma samples were drawn over 7 days following last dose in the first treatment period and over 10 days following the last dose in the second period. The primary end point for pharmacokinetic comparability was area under the plasma concentration versus time curve over 7 days post dose (AUC₀₋₇ (days)) of alpha₁-PI determined by potency (functional activity) assay. The crossover phase was followed by an 8-week open-label treatment phase with Prolastin-C only.

Results: Mean AUC₀₋₇ (days) was 155.9 versus 152.4 mg*h/mL for Prolastin-C and Prolastin, respectively. The geometric least squares mean ratio of AUC₀₋₇ (days) for Prolastin-C versus Prolastin had a point estimate of 1.03 and a 90% confidence interval of 0.97-1.09, demonstrating pharmacokinetic equivalence between the 2 products. Adverse events were similar for both treatments and occurred at a rate of 0.117 and 0.078 per infusion for Prolastin-C (double-blind treatment phase only) and Prolastin, respectively (p = 0.744). There were no treatment-emergent viral infections in any subject for human immunodeficiency virus, hepatitis B or C, or parvovirus B19 during the course of the study.

Conclusion: Prolastin-C demonstrated pharmacokinetic equivalence and a comparable safety profile to Prolastin.

Trial registration: ClinicalTrials.gov Identifier: NCT00295061.

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