Genetic Analysis of Hereditary Coagulation Factor V Deficiency in Two Chinese Families Caused by Compound Heterozygous Mutations.

IF 2.7 4区 医学 Q2 HEMATOLOGY Hamostaseologie Pub Date : 2023-12-01 Epub Date: 2023-06-15 DOI:10.1055/a-2086-4328
Yuan Chen, Ke Zhang, Yanhui Jin, Manlin Zeng, Kaiqi Jia, Lihong Yang, Mingshan Wang
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Abstract

Objective:  This study aims to provide a preliminary discussion of the molecular basis of FV deficiency caused by compound heterozygous mutations in two Chinese families.

Methods:  Relative coagulation index was measured by the one-stage clotting method and the FV:Ag was measured by ELISA. All exons and flanking regions of the F5 gene were amplified by PCR and directly sequenced. ClustalX-2.1-win was used to analyze the conservation of mutations. The online software was used to predict the pathogenicity of mutations. PyMOL was used to analyze the variation in the spatial structure of the FV protein before and after mutations. Calibrated automated thrombogram was used to analyze the function of the mutant protein.

Results:  Phenotyping suggested that both probands had a simultaneous decrease in FV:C and FV:Ag. Their genetic tests showed that proband A had a missense mutation p.Ser111Ile in exon 3 and a polymorphism p.Arg2222Gly in exon 25. At the same time, the proband B had a missense mutation p.Asp96His in exon 3 and a frame-shift mutation p.Pro798Leufs*13 in exon 13. Meanwhile, the p.Ser111Ile is conserved among homologous species. The bioinformatics and protein model analysis revealed that p.Ser111Ile and p.Pro798Leufs*13 were pathogenic and could affect the structure of the FV protein. The thrombin generation test revealed that the clotting function of proband A and B had been affected.

Conclusion:  These four mutations may be responsible for the reduction of FV levels in two Chinese families. Moreover, the p.Ser111Ile mutation is a novel pathogenic variant that has not been reported.

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由复合杂合突变导致的两个中国家庭遗传性凝血因子 V 缺乏症的基因分析
研究目的本研究旨在初步探讨两个中国家庭中由复合杂合突变引起的 FV 缺乏症的分子基础:方法:用一级凝血法测定相对凝血指数,用酶联免疫吸附法测定 FV:Ag。用 PCR 扩增 F5 基因的所有外显子和侧翼区并直接测序。使用ClustalX-2.1-win分析突变的保守性。使用在线软件预测突变的致病性。使用 PyMOL 分析突变前后 FV 蛋白空间结构的变化。使用校准自动血栓图分析突变蛋白的功能:结果:表型分析表明,两个探针的 FV:C 和 FV:Ag 同时下降。他们的基因检测结果显示,探针 A 在第 3 号外显子中存在一个错义突变 p.Ser111Ile,在第 25 号外显子中存在一个多态突变 p.Arg2222Gly。同时,病例 B 的第 3 号外显子中有一个错义突变 p.Asp96His,第 13 号外显子中有一个移帧突变 p.Pro798Leufs*13。同时,p.Ser111Ile 在同源物种中是保守的。生物信息学和蛋白质模型分析表明,p.Ser111Ile 和 p.Pro798Leufs*13 是致病基因,会影响 FV 蛋白的结构。凝血酶生成试验显示,概率 A 和概率 B 的凝血功能受到了影响:结论:这四个突变可能是导致两个中国家庭中 FV 水平降低的原因。此外,p.Ser111Ile 突变是一种新的致病变异,尚未见报道。
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来源期刊
Hamostaseologie
Hamostaseologie HEMATOLOGY-
CiteScore
5.50
自引率
6.20%
发文量
62
审稿时长
6-12 weeks
期刊介绍: Hämostaseologie is an interdisciplinary specialist journal on the complex topics of haemorrhages and thromboembolism and is aimed not only at haematologists, but also at a wide range of specialists from clinic and practice. The readership consequently includes both specialists for internal medicine as well as for surgical diseases.
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