Factor IX inhibitors in haemophilia B: A report of National Haemophilia Registry in China

医学 血友病 因子IX 血友病B 内科学 血友病A C1抑制剂 儿科 错义突变 肾病综合征 美罗华 突变 基因 化学 血管性水肿 淋巴瘤 生物化学
作者
Xueqing Dou,Wenhui Zhang,Man‐Chiu Poon,Xinsheng Zhang,Runhui Wu,Xiaoqin Feng,Linhua Yang,Cheng Peng,Shu Chen,Ying Wang,Hu Zhou,Meijuan Huang,Yanping Song,Cheng‐Hao Jin,Donglei Zhang,Ling‐Ling Chen,Wei Liu,Lei Zhang,Feng Xue,Renchi Yang
出处
期刊:Haemophilia [Wiley]
卷期号:29 (1): 123-134 被引量:9
标识
DOI:10.1111/hae.14665
摘要

The development of inhibitors against factor FIX (FIX) is the most serious complication of FIX replacement therapy in haemophilia B (HB) patients. Currently, only few cohorts of HB inhibitor patients have been reported worldwide.This Chinese nationwide study of HB inhibitor patients explored their risk factors for FIX inhibitor development and experience on their management.We retrospectively analysed patient characteristics, F9 genotypes, treatment strategies and outcomes of HB inhibitor patients registered to the Chinese National Registry and Patient Organization Registry.Forty-four unique HB inhibitor patients were identified in 4485 unique HB patients registered by year 2021 to the two Registries. Inhibitor diagnosis were usually delayed and the low prevalence (.98%) may suggest some inhibitor patients were not identified. Their median age at inhibitor diagnosis was 7.5 (IQR, 3.0-14.8) years. Most patients (95.5%) had high-titre inhibitors. Allergic/Anaphylactic reactions occurred in 59.1% patients. Large deletions and nonsense mutations were the most common F9 mutation types in our FIX inhibitor patients. Patients with large F9 gene deletions were more likely to develop inhibitors (p = .0002), while those with missense mutations had a low risk (p < .0001). Thirteen (29.5%) patients received immune tolerance induction (ITI) therapy using low-dose prothrombin complex concentrate regimens. Twelve completed ITI with three (25.0%) achieving success. Nephrotic syndrome developed in two (16.7%) patients during ITI.This study reports the largest Chinese cohort of HB inhibitor patients. Large deletions were most significantly associated with inhibitor development. Low-dose ITI might be feasible for FIX inhibitor eradication.
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