F8 variants and their genotype-phenotype correlations in Thai patients with haemophilia A: a nationwide multicentre study.

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS
Chayanit Trirut, Darintr Sosothikul, Rungnapa Ittiwut, Chupong Ittiwut, Sureeporn Pongsewalak, Natsaruth Songthawee, Rungrote Natesirinilkul, Pallapa Banjerdlak, Pokpong Na Songkhla, Patcharee Komvilaisak, Chatphatai Moonla, Kanya Suphapeetiporn
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引用次数: 0

Abstract

Aims: Analysis of the F8 gene helps predict the risk of developing factor VIII (FVIII) inhibitors and the depth of phenotype in haemophilia A (HA) patients. Since data in Southeast Asian countries remain scarce, we aim to study F8 variation correlated with HA phenotypes in Thailand.

Methods: Thai patients with HA were enrolled from seven haemophilia treatment centres during 2022-2023. Using peripheral blood DNA, inverse shifting-polymerase chain reaction (IS-PCR) for F8-intron 22 inversion (Inv22) and F8-intron 1 inversion (Inv1) was performed. Whole exome sequencing (WES) was explored in cases without Inv22/Inv1.

Results: Of 124 patients with HA, 91.9% were detected with a causative F8 variant, including Inv22 (30.6%), Inv1 (1.6%), missense (23.4%), nonsense (16.9%) and small insertion/deletion (16.1%) mutations. Inv22, small insertion/deletion and nonsense were associated with severe HA, compared with missense variants, by the ORs of 13.9 (95% CI, 4.2 to 56.7), 14.7 (95% CI, 3.4 to 104.7) and 15.6 (95% CI, 3.6 to 110.2), respectively. While nonsense variants affecting the light chain increased the risk of developing FVIII inhibitors (OR, 6.8; 95% CI, 1.5 to 32.6) compared with the low-risk (small insertion/deletion, missense and splice-site) variants. Twelve patients (9.7%) harboured novel F8 variants, comprising five missense (p.Pro540Leu, p.Ser564Pro, p.Leu668Pro, p.Ala1721Glu, p.His2024Pro), five small insertion/deletion (p.Val502SerfsTer13, p.Ile522PhefsTer13, p.Phe992LysfsTer11, p.Leu1223PhefsTer18, c.6427_6429+3delATGGTA) and one nonsense mutations (p.Glu1292Ter).

Conclusions: IS-PCR followed by WES successfully assesses F8 alterations in most HA cases. With several unique variants, severe HA in Thailand is considerably caused by Inv22, small insertion/deletion and nonsense, whereas missense variants are more responsible for nonsevere HA phenotypes.

泰国 A 型血友病患者的 F8 变异及其基因型与表型的相关性:一项全国性多中心研究。
目的:对 F8 基因的分析有助于预测 A 型血友病(HA)患者罹患第八因子(FVIII)抑制剂的风险和表型的深度。由于东南亚国家的数据仍然很少,我们旨在研究泰国 F8 变异与血友病表型的相关性:方法:2022-2023 年期间,我们从七个血友病治疗中心招募了泰国的 HA 患者。使用外周血 DNA 进行反变换聚合酶链反应(IS-PCR),检测 F8-intron 22 反转(Inv22)和 F8-intron 1 反转(Inv1)。对无Inv22/Inv1的病例进行了全外显子组测序(WES):结果:在124例HA患者中,91.9%的患者被检测出致病的F8变异,包括Inv22(30.6%)、Inv1(1.6%)、错义(23.4%)、无义(16.9%)和小插入/缺失(16.1%)突变。与错义变异相比,Inv22、小插入/缺失和无义变异与严重HA相关,OR值分别为13.9(95% CI,4.2至56.7)、14.7(95% CI,3.4至104.7)和15.6(95% CI,3.6至110.2)。与低风险(小插入/缺失、错义和剪接位点)变异相比,影响轻链的无义变异会增加患 FVIII 抑制剂的风险(OR,6.8;95% CI,1.5 至 32.6)。有 12 名患者(9.7%)携带新型 F8 变异,包括 5 个错义变异(p.Pro540Leu、p.Ser564Pro、p.Leu668Pro、p.Ala1721Glu、p.His2024Pro)、5 个小插入/缺失变异(p.Val502SerfsTer13、p.Ile522PhefsTer13、p.Phe992LysfsTer11、p.Leu1223PhefsTer18、c.6427_6429+3delATGGTA)和一个无义突变(p.Glu1292Ter):IS-PCR和WES成功地评估了大多数HA病例的F8变异。泰国的重度HA主要由Inv22、小插入/缺失和无义变异引起,而错义变异则更多地导致非重度HA表型。
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
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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