Debra D Pittman, Charles Carrieri, Holly Soares, John McKay, Charles Y Tan, John Z Liang, Swapnil Rakhe, Jean-Claude Marshall, John E Murphy, Puneet Gaitonde, Jeremy Rupon
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Data from ongoing trials suggest FIX activity varies between different OS and CS assays.</p><p><strong>Material and methods: </strong> To better understand FIX-R338L activity in clinical samples, an international multisite field study was conducted across a central laboratory and 18 local laboratories, using standard protocols, reagents, and instrumentation, with individual participant samples from a phase 1/2a study of fidanacogene elaparvovec.</p><p><strong>Results: </strong> Unlike the wild-type FIX control, FIX-R338L activity was higher with the OS silica-based assay versus OS ellagic acid-based and CS assays. Variation in FIX activity was greater at the lowest activity levels. Activated FIX (FIXa) in plasma could result in higher OS assay activity or increased thrombin generation, which could overestimate FIX activity. However, FIXa was not detected in the participant samples, indicating that it was not contributing to the OS assay differences. 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引用次数: 0
摘要
背景:Fidanacogene elaparvovec是一种表达高活性因子IX(FIX)变体FIX-R338L的基于腺相关病毒的基因治疗载体,目前正在开发用于治疗B型血友病。正在进行的试验数据表明,FIX活性在不同的OS和CS测定法中存在差异:为了更好地了解临床样本中FIX-R338L的活性,我们在一个中心实验室和18个地方实验室开展了一项国际多点实地研究,使用标准协议、试剂和仪器,对来自fidanacogene elaparvovec的1/2a期研究的个体参与者样本进行了检测:结果:与野生型 FIX 对照组不同,基于 OS 硅的检测方法与基于 OS 鞣酸的检测方法和 CS 检测方法相比,FIX-R338L 的活性更高。最低活性水平的 FIX 活性差异更大。血浆中的活化 FIX(FIXa)可能导致 OS 检测活性升高或凝血酶生成增加,从而高估 FIX 活性。不过,参与者样本中未检测到 FIXa,这表明它不会导致 OS 检测结果的差异。由于接受基因治疗的患者可能会接受外源性替代 FIX 产品,因此在患者血浆样本中添加了替代产品,以达到治疗浓度。外源性 FIX 与内源性 FIX-R338L 具有相加性,FIX-R338L 没有干扰:这些结果表明,在临床实验室中可以用 OS 和 CS 检测法测量 FIX-R338L 活性,并能深入了解用内源性 FIX-R338L 测量 FIX 时的检测变异性。这些发现可能有助于建立测量 FIX-R338L 活性的最佳实践(Clinicaltrials.gov 识别码:NCT02484092)。
Field Study and Correlative Studies of Factor IX Variant FIX-R338L in Participants Treated with Fidanacogene Elaparvovec.
Background: Fidanacogene elaparvovec, an adeno-associated virus-based gene therapy vector expressing the high-activity factor IX (FIX) variant FIX-R338L, is in development for hemophilia B. One-stage clotting (OS) assays and chromogenic substrate (CS) assays are commonly used to measure FIX-R338L variant activity. Data from ongoing trials suggest FIX activity varies between different OS and CS assays.
Material and methods: To better understand FIX-R338L activity in clinical samples, an international multisite field study was conducted across a central laboratory and 18 local laboratories, using standard protocols, reagents, and instrumentation, with individual participant samples from a phase 1/2a study of fidanacogene elaparvovec.
Results: Unlike the wild-type FIX control, FIX-R338L activity was higher with the OS silica-based assay versus OS ellagic acid-based and CS assays. Variation in FIX activity was greater at the lowest activity levels. Activated FIX (FIXa) in plasma could result in higher OS assay activity or increased thrombin generation, which could overestimate FIX activity. However, FIXa was not detected in the participant samples, indicating that it was not contributing to the OS assay differences. Since individuals on gene therapy may receive exogenous replacement FIX products, replacement products were spiked into patient plasma samples to target a therapeutic concentration. Exogenous FIX was additive to endogenous FIX-R338L, with no interference from FIX-R338L.
Conclusion: These results demonstrate FIX-R338L activity can be measured with OS and CS assays in clinical laboratories and provide insight into assay variability when measuring FIX with endogenously produced FIX-R338L. The findings may help establish best practices for measuring FIX-R338L activity (Clinicaltrials.gov identifier: NCT02484092).
期刊介绍:
Thrombosis and Haemostasis publishes reports on basic, translational and clinical research dedicated to novel results and highest quality in any area of thrombosis and haemostasis, vascular biology and medicine, inflammation and infection, platelet and leukocyte biology, from genetic, molecular & cellular studies, diagnostic, therapeutic & preventative studies to high-level translational and clinical research. The journal provides position and guideline papers, state-of-the-art papers, expert analysis and commentaries, and dedicated theme issues covering recent developments and key topics in the field.