Factor VIII Antibodies Demonstrate Type I or Type II Kinetics in Acquired Haemophilia A.

IF 3 2区医学 Q2 HEMATOLOGY

Haemophilia Pub Date : 2025-01-15 DOI:10.1111/hae.15144

Kirollos Kamel, Sofia Sardo Infirri, Anne Riddell, Pratima Chowdary, Paul Batty

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引用次数: 0

Abstract

Background: Acquired haemophilia A (AHA) is an acquired bleeding disorder resulting from autoantibodies against Factor VIII (FVIII). Previous studies have reported differences in FVIII inhibitor kinetics (type I or type II) in AHA compared to severe haemophilia A.

Aim: To characterise inhibitor kinetics in AHA and evaluate the proportions displaying type I, II or indeterminate kinetics.

Methods: Single-centre retrospective study of inhibitor kinetics in adults with AHA. Type I kinetics were defined as linear FVIII inhibition with ≥ 97% FVIII inactivation. Type II kinetics were defined as non-linear kinetics and inability to completely neutralise FVIII. Inhibitor titres were calculated using two methods outlined by the International Council for Standardisation in Haematology.

Results: Baseline samples from 34 patients were included. Fifteen samples (44.1%) exhibited type I kinetics, 16 samples (47.1%) exhibited type II kinetics and 3 (8.8%) were indeterminate. Plateau mean residual FVIII:C was higher for inhibitors displaying type II compared to type I kinetics (18.6 vs. 2.9 IU/dL, p < 0.0001). Non-linear regression using a dose-response curve without categorisation for kinetics type yielded a poor fit (R² = 38%), which improved with refitting using categories of type I or II kinetics that explained 87% and 85% of the variability. The median difference in inhibitor titre between the two reporting methods was 5% and 15% in the type I and II kinetics groups, respectively.

Conclusion: FVIII autoantibodies demonstrate either type I or type II kinetics. Greater discrepancy in reported inhibitor titres depending on the method used is seen for inhibitors with type II kinetics.

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因子VIII抗体在获得性血友病A中表现出I型或II型动力学。

背景：获得性血友病A （AHA）是一种由抗因子VIII （FVIII）自身抗体引起的获得性出血性疾病。先前的研究报道了与严重血友病a相比，AHA中FVIII抑制剂动力学（I型或II型）的差异。目的：表征AHA中抑制剂动力学并评估显示I型，II型或不确定动力学的比例。方法：单中心回顾性研究成人AHA患者抑制剂动力学。I型动力学定义为线性FVIII抑制，FVIII失活≥97%。II型动力学被定义为非线性动力学和无法完全中和FVIII。使用国际血液学标准化理事会概述的两种方法计算抑制剂滴度。结果：纳入了34例患者的基线样本。15个样品（44.1%）表现为I型动力学，16个样品（47.1%）表现为II型动力学，3个样品（8.8%）不确定。II型抑制剂的平台平均残余FVIII:C比I型抑制剂高（18.6 vs 2.9 IU/dL, p < 0.0001）。使用没有对动力学类型进行分类的剂量-反应曲线的非线性回归产生了较差的拟合（R2 = 38%），使用I型或II型动力学类别进行改装，可以解释87%和85%的变异性，从而改善了拟合效果。在I型和II型动力学组中，两种报告方法之间抑制剂滴度的中位数差异分别为5%和15%。结论：FVIII自身抗体表现为I型或II型动力学。对于II型动力学抑制剂，根据所使用的方法，报告的抑制剂滴度差异更大。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Haemophilia 医学-血液学

CiteScore

6.50

自引率

28.20%

发文量

226

审稿时长

3-6 weeks

期刊介绍： Haemophilia is an international journal dedicated to the exchange of information regarding the comprehensive care of haemophilia. The Journal contains review articles, original scientific papers and case reports related to haemophilia care, with frequent supplements. Subjects covered include: clotting factor deficiencies, both inherited and acquired: haemophilia A, B, von Willebrand''s disease, deficiencies of factor V, VII, X and XI replacement therapy for clotting factor deficiencies component therapy in the developing world transfusion transmitted disease haemophilia care and paediatrics, orthopaedics, gynaecology and obstetrics nursing laboratory diagnosis carrier detection psycho-social concerns economic issues audit inherited platelet disorders.