通过供体筛选降低人免疫球蛋白产品中的异凝集素。

Biologics in therapy Pub Date : 2014-12-01 Epub Date: 2014-05-20 DOI:10.1007/s13554-014-0016-2

Brigitte Siani, Katharina Willimann, Sandra Wymann, Adriano A Marques, Eleonora Widmer

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引用次数: 35

摘要

简介:溶血被认为是一类效应，是静脉注射人正常免疫球蛋白(即静脉注射免疫球蛋白(IVIG))治疗后可能发生的罕见不良事件。来源于供体血浆的抗a /B异凝集素(也称为等血凝素)存在于多价免疫球蛋白G (IgG)产品中，被认为是溶血的可能危险因素。我们假设，通过排除高异凝集素滴度供者的血浆，最终IVIG产品将显著降低抗a /B异凝集素滴度。方法:建立了一种用自动间接凝集试验(IAT)筛选供体血浆抗A异凝集素的方法。定义了供体血浆排除的截止值。根据Privigen(®)(CSL Behring, Berne, Switzerland)的制造工艺制备工业规模的供体血浆池和最终IVIG产品;人体10%液体IVIG)。通过IAT、直接凝集试验和基于流式细胞术的测定[荧光活化细胞分选(FACS)抗a]来测定混合血浆和最终IVIG产品中的抗a /B异凝集素含量。结果:对705名献血者的血浆进行筛选，发现48名(6.8%)献血者血浆中抗a异凝集素滴度高(IAT凝集评分≥2+，1:20 00预稀释)。排除这些供者的血浆导致汇集血浆中抗a异凝集素浓度降低一滴级，通过FACS anti-A测量的抗a异凝集素浓度降低两倍(1,352 vs 2,467 μ g/g IgG)证实。当同样的筛选和排除应用于工业规模的血浆池时(导致5%的献血者的血浆被排除在外)，抗a异凝集素在最终IVIG产品中降低了一个滴度。抗- b异凝集素也降低了一个滴度，因为许多具有高抗- a异凝集素的献血者也具有高抗- b。结论:通过实施抗a供体筛选，降低IVIG产品中抗a /B异凝集素滴度在工业规模上是可行的，可降低IVIG治疗后溶血的风险。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

Isoagglutinin Reduction in Human Immunoglobulin Products by Donor Screening.

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Isoagglutinin Reduction in Human Immunoglobulin Products by Donor Screening.

Introduction: Hemolysis is considered a class effect and a rare adverse event that can occur following therapy with human normal immunoglobulin for intravenous administration [i.e., intravenous immunoglobulin (IVIG)]. Anti-A/B isoagglutinins (also referred to as isohemagglutinins) originating from donor plasma are present in polyvalent immunoglobulin G (IgG) products and are considered a probable risk factor for hemolysis. We hypothesized that, by excluding plasma from donors with high isoagglutinin titers, the final IVIG product would have a meaningful reduction in anti-A/B isoagglutinin titers.

Methods: A method for screening donor plasma for anti-A isoagglutinins using an automated indirect agglutination test (IAT) was developed. A cut-off for donor plasma exclusion was defined. Industry-scale donor plasma pools and final IVIG product were prepared according to the manufacturing process of Privigen(®) (CSL Behring, Berne, Switzerland; human 10% liquid IVIG). Anti-A/B isoagglutinin content in pooled plasma and final IVIG product was measured by IAT, direct agglutination test, and a flow cytometry-based assay [fluorescence-activated cell sorting (FACS) anti-A].

Results: Screening of plasma from 705 donors identified 48 (6.8%) donors with high anti-A isoagglutinin titers in plasma (IAT agglutination score ≥2+ in a 1:200 pre-dilution). Exclusion of plasma from these donors resulted in a one-titer-step reduction of anti-A isoagglutinin in pooled plasma, confirmed by a twofold anti-A isoagglutinin concentration reduction measured by FACS anti-A (1,352 vs. 2,467 µg/g IgG). When the same screening and exclusion were applied to industrial-scale plasma pools (resulting in the exclusion of plasma from 5% of donors), anti-A isoagglutinins were reduced by one titer step in the final IVIG product. Anti-B isoagglutinins were also reduced by one titer step, as many donors with high anti-A isoagglutinins also have high anti-B.

Conclusion: Reduction of anti-A/B isoagglutinin titers in IVIG products on an industrial scale is feasible through implementation of anti-A donor screening, which may reduce the risk of hemolysis following IVIG therapy.

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Biologics in therapy

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