Determination of procoagulant activity in human normal immunoglobulin preparations for therapeutic use by FXIa chromogenic assay: Evaluation of test kit sensitivity, reference standard performance and product formulation effects on the FXIa assay.

Q4 Medicine Pharmeuropa bio & scientific notes Pub Date : 2024-01-01
M-E Behr-Gross, D Le Tallec, N Sinitskaya, C Milne, M Etscheid
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Abstract

In 2010, the reporting of thrombotic adverse events for one subcutaneous and certain intravenous immunoglobulins (IGs) raised some concerns. In Europe, regulatory bodies rapidly revised compendial specifications for therapeutic IGs to ensure they do not exhibit thrombogenic (procoagulant) activity (PCA). At the global level, a working group (GWG) was launched with the aim of assessing PCA measurement methods and limits, considering results obtained by human IG manufacturers during in-process controls. The GWG created three dedicated subgroups to investigate the FXIa chromogenic assay, the non-activated partial thromboplastin time (NAPTT) test and the thrombin generation assay (TGA). The European Directorate for the Quality of Medicines & HealthCare (EDQM) was responsible for co-ordinating the subgroup in charge of evaluating the FXIa chromogenic assay in a study that assessed the sensitivity and robustness of two commercial chromogenic FXIa test kits. The impact of IG product formulation on FXIa recovery and the suitability of PCA-containing IG products as potential reference standards/controls were also assessed. IG materials representative of marketed products were provided to four laboratories for a study that was carried out in two steps: 1) two chromogenic FXIa test kit manufacturers assessed the performance and determined optimal test conditions by their respective methods, 2) two OMCLs studied both kits using an optimised study design. Regarding sensitivity, the study results identified suitable dose-response intervals and limits with both chromogenic FXIa test kits. This allowed the establishment of dilution ranges for optimal detection of FXIa/PCA in 5 % and 10 % IG products in the range of 1-6 mIU/mL. However, careful optimisation of the sample dilutions was required (notably to avoid potential matrix effects) and the choice of the mode of data acquisition (kinetic or end-point method) contributed to sensitivity in routine use. Importantly, the composition of IG products was of minor concern for FXIa determination with both test kits. Potential reference materials evaluated in the study behaved as expected and could be useful should a separate reference standard to the FXIa WHO IS be deemed necessary in future.

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用 FXIa 色原测定法测定治疗用人用正常免疫球蛋白制剂中的促凝血活性:评估检测试剂盒的灵敏度、参照标准的性能和产品配方对 FXIa 检测法的影响。
2010 年,有关一种皮下注射免疫球蛋白和某些静脉注射免疫球蛋白血栓不良事件的报告引起了一些关注。在欧洲,监管机构迅速修订了治疗用免疫球蛋白的药典规范,以确保其不表现出血栓形成(促凝)活性(PCA)。在全球层面,成立了一个工作组(GWG),目的是评估 PCA 测量方法和限值,同时考虑人体 IG 制造商在过程控制中获得的结果。GWG 设立了三个专门分组,分别负责研究 FXIa 色原测定法、非活化部分凝血活酶时间(NAPTT)检测法和凝血酶生成测定法(TGA)。欧洲药品和保健质量管理局(EDQM)负责协调负责评估 FXIa 色原检测法的分组,该研究评估了两种商用色原 FXIa 检测试剂盒的灵敏度和稳健性。此外,还评估了 IG 产品配方对 FXIa 回收率的影响,以及含 PCA 的 IG 产品作为潜在参考标准/对照的适用性。我们向四家实验室提供了市售产品中具有代表性的 IG 材料,并分两步进行了研究:1) 两家色原 FXIa 检测试剂盒制造商通过各自的方法评估了性能并确定了最佳检测条件;2) 两家 OMCL 使用优化的研究设计对两种试剂盒进行了研究。在灵敏度方面,研究结果确定了两种色原 FXIa 检测试剂盒的合适剂量反应区间和限度。这就为 5 % 和 10 % IG 产品中 FXIa/PCA 的最佳检测确定了稀释范围,即 1-6 mIU/mL。不过,还需要对样品稀释液进行仔细优化(主要是为了避免潜在的基质效应),数据采集模式(动力学法或终点法)的选择也会影响常规使用中的灵敏度。重要的是,在使用这两种检测试剂盒测定 FXIa 时,IG 产品的成分并不重要。研究中评估的潜在参考材料的表现符合预期,如果将来认为有必要为 FXIa WHO IS 另设参考标准,这些材料可能会很有用。
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来源期刊
Pharmeuropa bio & scientific notes
Pharmeuropa bio & scientific notes Medicine-Medicine (all)
CiteScore
0.70
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期刊最新文献
Collaborative study for the establishment of Ph. Eur. Biological Reference Preparation for Human tetanus immunoglobulin batch 2. Collaborative study for the establishment of Ph. Eur. Biological Reference Preparation for Human tetanus immunoglobulin batch 2. Determination of procoagulant activity in human normal immunoglobulin preparations for therapeutic use by FXIa chromogenic assay: Evaluation of test kit sensitivity, reference standard performance and product formulation effects on the FXIa assay. Ph. Eur. testing for histamine and depressor substances using guinea-pigs and cats: the end of an era. Strategy for removal of animal tests for histamine and depressor substances and their vestiges from the Ph. Eur. International collaborative study to assess new stocks of candidate reference preparations to control the level of anti-D in IVIG
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