Diagnosis and management of factor XI alloinhibitors in patients with congenital factor XI deficiency—A large single-centre experience

IF 3 2区医学 Q2 HEMATOLOGY

Haemophilia Pub Date : 2024-07-22 DOI:10.1111/hae.15081

Kirollos Salah Kamel, Anne Riddell, Bilal Jradeh, Ewa Jaslowska, Keith Gomez

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引用次数: 0

Abstract

Introduction

Factor (F) XI deficiency is an inherited bleeding disorder with increased prevalence in Ashkenazi Jews where it is mainly caused by two variants, p.Glu135* (type II, leading to a null allele) and p.Phe301Leu (type III, missense variant). Inhibitor development is rare, and only seen in severe FXI deficiency (<20 IU/dL) upon exposure to plasma-based products. We report our experience of a large cohort of patients with severe FXI deficiency, including seven patients who developed FXI alloinhibitors, their presentation, natural history and subsequent perioperative management.

Methods

A single-centre retrospective database review of patients with FXI deficiency, including those who have subsequently developed inhibitors, and extraction of clinical, laboratory and genotype data, including operative management records.

Results

A total of 682 patients were identified with FXI deficiency, of whom 113 had FXI < 20 IU/dL and 42 had FXI ≤ 1 IU/dL. Factor XI inhibitors were seen in seven patients, six of whom were homozygous for the type II variant (prevalence of inhibitor with this genotype of 30%, risk of inhibitor upon plasma exposure 50%). FXI inhibitors were not seen, despite similar exposures, in patients with other genotypes. No alteration in bleeding phenotype occurred after inhibitor development and subsequent surgery was managed on 13 occasions with recombinant factor VIIa (rFVIIa), including low doses (15–30 µg/kg), with good haemostasis. The inhibitor spontaneously disappeared in four of seven patients over 1–22 years.

Conclusion

FXI inhibitors were only observed in severe FXI deficient patients homozygous for p.Glu135* (null allele) upon plasma or FXI concentrate exposure, with a 30% prevalence. The bleeding phenotype was not altered and inhibitors may disappear with time. Adequate haemostasis in the perioperative setting is achievable with low doses of rFVIIa.

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先天性 XI 因子缺乏症患者中 XI 因子异体抑制剂的诊断和管理--大型单中心经验。

导言：因子（F）XI 缺乏症是一种遗传性出血性疾病，在 Ashkenazi 犹太人中发病率较高，主要由两个变异体引起，即 p.Glu135*（II 型，导致无效等位基因）和 p.Phe301Leu（III 型，错义变异体）。抑制剂的产生非常罕见，只有在严重的 FXI 缺乏症中才会出现（方法：对 FXI 缺乏症患者（包括随后出现抑制剂的患者）进行单中心回顾性数据库审查，并提取临床、实验室和基因型数据，包括手术管理记录：结果：共发现 682 例 FXI 缺乏症患者，其中 113 例有 FXI 结论：只有在血浆或 FXI 浓缩物暴露时出现 p.Glu135*（空等位基因）的严重 FXI 缺乏患者中才能观察到 FXI 抑制剂，发生率为 30%。出血表型没有改变，随着时间的推移，抑制剂可能会消失。小剂量的 rFVIIa 可在围手术期实现充分止血。

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.