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非中和性 FVIII 特异性抗体特征在甲型血友病患者和健康供者中。

Nonneutralizing FVIII-specific antibody signatures in patients with hemophilia A and in healthy donors.

机构信息

Institute Krems Bioanalytics, IMC University of Applied Sciences Krems, Krems, Austria.

Clinical Division of Haematology and Haemostaseology, Department of Internal Medicine I, Medical University of Vienna, Vienna, Austria.

出版信息

Blood Adv. 2022 Feb 8;6(3):946-958. doi: 10.1182/bloodadvances.2021005745.

Abstract

Previous studies identified nonneutralizing FVIII-specific antibodies in the circulation of severe and nonsevere hemophilia A (sHA and nsHA) patients without FVIII inhibitors and also in some healthy individuals. To gain a better understanding of the nature of these nonneutralizing antibody responses, we analyzed and compared anti-FVIII antibody signatures in 3 study cohorts: previously treated sHA as well as nsHA patients without FVIII inhibitors, and healthy donors. FVIII-binding IgM, IgG1-4, and IgA antibodies were differentiated, FVIII-specificity was assessed, and associated apparent affinity constants were determined. Our results indicate that the nonneutralizing FVIII-specific antibody response in all study cohorts is dominated by IgG1 and IgA. Prevalences, titers, and affinities of these nonneutralizing antibodies were higher in the hemophilia A cohorts than in healthy donors. Stratification for the anti-hepatitis C virus (HCV) antibody status demonstrated the presence of FVIII-specific IgA with elevated titers in sHA patients with an active or past HCV infection when compared with HCV antibody-positive nsHA patients or HCV antibody-negative patients and healthy donors. Increased titers and affinities of FVIII-specific IgG1 antibodies were observed in a considerable number of hemophilia A patients as opposed to healthy subjects independently of the patients' anti-HCV antibody status. Overall, our findings support the hypothesis that the generation of nonneutralizing anti-FVIII antibodies in healthy individuals and in noninhibitor hemophilia A patients might be based on similar immune mechanisms. However, differences in prevalences, titers, and affinities of these antibodies indicate distinct differences in the antibody evolution between healthy individuals and patients.

摘要

先前的研究在没有 FVIII 抑制剂的严重和非严重血友病 A(sHA 和 nsHA)患者以及一些健康个体的循环中发现了非中和性 FVIII 特异性抗体。为了更好地了解这些非中和性抗体反应的性质,我们分析并比较了三个研究队列中的抗 FVIII 抗体特征:先前接受治疗的 sHA 以及无 FVIII 抑制剂的 nsHA 患者和健康供体。区分了 FVIII 结合的 IgM、IgG1-4 和 IgA 抗体,评估了 FVIII 特异性,并确定了相关的表观亲和力常数。我们的研究结果表明,所有研究队列中的非中和性 FVIII 特异性抗体反应均由 IgG1 和 IgA 主导。与健康供体相比,血友病 A 队列中非中和性抗体的流行率、滴度和亲和力更高。针对丙型肝炎病毒(HCV)抗体状态的分层表明,与 HCV 抗体阳性的 nsHA 患者或 HCV 抗体阴性的患者和健康供体相比,具有高滴度的 FVIII 特异性 IgA 存在于 sHA 患者的 HCV 感染活动期或过去感染期。与健康受试者相比,相当数量的血友病 A 患者中观察到 FVIII 特异性 IgG1 抗体的滴度和亲和力增加,而与患者的抗 HCV 抗体状态无关。总的来说,我们的研究结果支持这样一种假设,即健康个体和非抑制剂性血友病 A 患者中非中和性抗 FVIII 抗体的产生可能基于类似的免疫机制。然而,这些抗体的流行率、滴度和亲和力的差异表明了健康个体和患者之间的抗体演变存在明显的差异。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4d31/8945293/456452bfe712/advancesADV2021005745absf1.jpg

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