Molecular and clinical characterization of two unrelated families with factor V deficiency, including a novel nonsense variant (p.Gln1532*)

IF 2.1 4区 医学 Q3 HEMATOLOGY
Ke Zhang, Longying Ye, Yanhui Jin, Yuan Chen, Shuting Jiang, Haixiao Xie, Lihong Yang, Mingshan Wang
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Abstract

Background

Factor V (FV) is an essential cofactor in the coagulation cascade. The characterization of novel mutations is advantageous for the clinical management of FV-deficient patients.

Methods

Coagulation screening and thrombin generation assay were performed with the plate-poor plasma. All 25 exons of the F5 gene were amplified and sequenced. The ClustalX-2.1 software was applied to the multiple sequence alignment. The possible adverse effects of mutations were investigated with online bioinformatics software and protein modeling.

Results

Two unrelated families with FV deficiency were under investigation. Proband A was an 18-year-old youth with recurrent epistaxis. Proband B was a 29-year-old woman who did not present with any bleeding symptoms. Three heterozygous mutations (p.Gln1532*, p.Phe218Ser, and p.Asp2222Gly) were detected. Interestingly, they were compound heterozygotes and both contained the p.Asp2222Gly, a polymorphism. The thrombin generation assay showed that both patients had impaired ability of thrombin generation, and in particular, proband A was more severe. Conservation, pathogenicity and protein modeling studies all indicated that these three mutations could cause deleterious effects on the function and structure of FV.

Conclusion

These three mutations are responsible for the FV-deficient in two pedigrees. Moreover, the nonsense variant p.Gln1532* is first reported in the world.

两个不相关的因子V缺乏家族的分子和临床特征,包括一个新的无义变异(p.Gln1532*)
背景因子V (FV)是凝血级联中必不可少的辅助因子。新突变的特征对fv缺陷患者的临床管理是有利的。方法用贫板血浆进行凝血筛选和凝血酶生成试验。对F5基因的全部25个外显子进行扩增和测序。应用ClustalX-2.1软件进行多序列比对。利用在线生物信息学软件和蛋白质模型研究突变可能产生的不良影响。结果对2个无血缘关系的FV缺陷家庭进行了调查。先证者A是一位复发性鼻出血的18岁青年。先证者B是一名29岁女性,未出现任何出血症状。检测到3个杂合突变(p.Gln1532*、p.Phe218Ser和p.Asp2222Gly)。有趣的是,它们都是复合杂合子,都含有p.Asp2222Gly多态性。凝血酶生成实验显示两例患者凝血酶生成能力均受损,且先证A更严重。保守性、致病性和蛋白质模型研究都表明,这三种突变可能对FV的功能和结构产生有害影响。结论这三种突变是导致两个家系fv缺陷的主要原因。此外,无义变异p.Gln1532*为国际上首次报道。
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来源期刊
CiteScore
4.90
自引率
0.00%
发文量
42
审稿时长
14 days
期刊介绍: Blood Cells, Molecules & Diseases emphasizes not only blood cells, but also covers the molecular basis of hematologic disease and studies of the diseases themselves. This is an invaluable resource to all those interested in the study of hematology, cell biology, immunology, and human genetics.
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