[Correlation Analysis of FⅧGene Mutation and the Production of FⅧ Inhibitor with Severe Hemophilia A Patients in a Single Medical Center]

Lyu-Kai Zhu; Xia-Lin Zhang; Xiu-E Liu; Xiu-Yu Qin; Gang Wang; Lin-Hua Yang

doi:10.19746/j.cnki.issn.1009-2137.2022.05.036

[Correlation Analysis of FⅧGene Mutation and the Production of FⅧ Inhibitor with Severe Hemophilia A Patients in a Single Medical Center]

Zhongguo Shi Yan Xue Ye Xue Za Zhi. 2022 Oct;30(5):1536-1540. doi: 10.19746/j.cnki.issn.1009-2137.2022.05.036.

[Article in Chinese]

Authors

Lyu-Kai Zhu¹, Xia-Lin Zhang¹, Xiu-E Liu¹, Xiu-Yu Qin¹, Gang Wang², Lin-Hua Yang³

Affiliations

¹ Institute of Hematology, Department of Hematology, The Second Hospital of Shanxi Medical University(The Second Clinical Medical College), Taiyuan 030001, Shanxi Province, China.
² Institute of Hematology, Department of Hematology, The Second Hospital of Shanxi Medical University(The Second Clinical Medical College), Taiyuan 030001, Shanxi Province, China,E-mail：g.wang@sxmu.edu.cn.
³ Institute of Hematology, Department of Hematology, The Second Hospital of Shanxi Medical University(The Second Clinical Medical College), Taiyuan 030001, Shanxi Province, China,E-mail：yanglh5282@163.com.

PMID: 36208262
DOI: 10.19746/j.cnki.issn.1009-2137.2022.05.036

Abstract
in English, Chinese

Objective: To investigate the relationship between the type of FⅧgene mutation and the development of FⅧ inhibitors in patients with severe haemophilia A (HA).

Methods: The medical records of 172 patients with severe hemophilia A from January 2009 to September 2020 were reviewed. The types of FⅧgene mutations and the production of factor Ⅷ inhibitors were collected and divided into high-risk mutation group ( intron 1 inversions, large deletions, nonsense mutations), low-risk mutation group (missense mutations, small deletions and insertions, splice site mutations) and intron 22 inversions group. The correlation of FⅧgenotype and the production of FⅧ inhibitors in patients with HA were analyzed.

Results: Among 172 patients with severe HA, 21 cases(12.21%) developed FⅧ inhibitors. The cumulative incidence of FⅧ inhibitor development was 32%(10/31) in high risk group (75% patients with large deletions, 43% patients with intron 1 inversions, 20% patients with nonsense mutations) and 5%(2/43) in low risk group(6% patients with missense mutations, 5% patients with small deletions or insertions and 0% patient with a splice site mutation) and 9%(9/98) in intron 22 inversions group. Compared with the risk of FⅧ inhibitor development in intron 22 inversions group, the risk of FⅧ inhibitor development in high risk group was higher (OR＝4.7, 95% CI： 1.7-13.0), the risk of FⅧ inhibitor development in low risk group was equal (OR＝0.5, 95% CI： 0.1-2.3). Compared with the risk of inhibitor development in low risk group, the risk of FⅧ inhibitor development in high risk group was higher (OR＝9.8, 95% CI： 2.0-48.7).

Conclusion: Gene mutations of patients with severe HA in high-risk group which include intron 1 inversions, large deletions, nonsense mutations are a risk factor for FⅧ inhibitor production.

题目: 单中心重型血友病A患者FⅧ基因突变类型与FⅧ抑制物产生的相关性分析.

目的: 探讨重型血友病A（Hemophilia A，HA）患者的凝血因子Ⅷ（Factor Ⅷ，FⅧ）抑制物的产生与FⅧ基因突变之间的关系.

方法: 回顾2009年1月至2020年9月172例重型HA患者的病历资料，收集FⅧ基因突变类型与FⅧ抑制物产生情况，分为高风险突变组（包括1倒位、大片段缺失、无义突变）、低风险突变组（包括错义突变、小缺失/插入、剪接位点突变）和22倒位组。分析重型HA患者FⅧ基因型与FⅧ抑制物产生的关联性.

结果: 172例重型HA患者中，21例患者产生了FⅧ抑制物，高风险组FⅧ抑制物10例，发生率为32%（大片段缺失75%，1倒位43%，无义突变20%），低风险组FⅧ抑制物2例，发生率为5%（错义突变6%，小缺失/插入5%，剪接位点突变0%），22倒位组FⅧ抑制物9例，发生率为9%。与22倒位组相比，高风险组具有更高的FⅧ抑制物发生风险（OR＝4.7，95% CI： 1.7-13.0），低风险组与22倒位FⅧ抑制物发生风险无明显差异（OR＝0.5，95% CI： 0.1-2.3）。与低风险组相比，高风险组具有更高的FⅧ抑制物发生风险（OR＝9.8，95% CI： 2.0-48.7）.

结论: FⅧ基因发生1倒位、大片段缺失、无义突变是重型HA患者FⅧ抑制物产生的危险因素.

Keywords: FⅧ gene mutation; FⅧ inhibitor; factor Ⅷ; hemophilia A.

MeSH terms

Codon, Nonsense
DNA Mutational Analysis
Factor VIII / genetics*
Hemophilia A* / genetics
Humans
Introns
Mutation

Substances

Codon, Nonsense
F8 protein, human
Factor VIII

Abstract in English, Chinese

MeSH terms

Substances

Abstract
in English, Chinese