靶向新一代测序揭示沙特静脉血栓栓塞患者中血栓形成倾向相关基因的新变异和已知变异。
Targeted next-generation sequencing reveals novel and known variants of thrombophilia associated genes in Saudi patients with venous thromboembolism.
作者信息
Athar Mohammad, Ghita Ibrahim S, Albagenny Amani A, Abduljaleel Zainularifeen, Shadab Ghulam, Elsendiony Ahmed, Halawani Saeed H, Alkazmi Mohammad M, Alquthami Khalid, Alkhuzae Mohammad M, Althebyani Abdulaziz A, Bogari Neda M, Dannoun Anas, Al-Allaf Faisal A
机构信息
Department of Medical Genetics, Faculty of Medicine, Umm Al-Qura University, Makkah, Saudi Arabia; Science and Technology Unit, Umm Al-Qura University, Makkah, Saudi Arabia.
Hematology Department, Al-Noor Specialist Hospital, Makkah, Saudi Arabia.
出版信息
Clin Chim Acta. 2021 Aug;519:247-254. doi: 10.1016/j.cca.2021.05.012. Epub 2021 May 18.
BACKGROUND
Thrombophilia is a substantial source of indisposition and mortality in several countries, including Arab populations. Deep venous thrombosis (DVT) with or without pulmonary embolism (PE) is the prevalent clinical manifestation of thrombophilia. While many genetic risk factors for DVT are known, almost all associated with hemostasis, many genetic factors remain unexplained. Nowadays, Next Generation Sequencing (NGS) offers a potential solution that allows several candidate genes to be analyzed simultaneously at a reasonable expense.
METHODS
We performed variant screening in the thrombophilia associated genes in Factor V Leiden (FVL) mutation-negative patients using Ion Torrent Next-generation sequencing (NGS). Ion AmpliSeq panel for 18 genes was designed. Twenty-nine unrelated patients with idiopathic VTE were recruited for NGS.
RESULTS
We were able to identify 19 variants (1 novel and 18 previously reported) in 10 out of 18 targeted genes. Pathogenic variants were identified in 22 patients demonstrating mutation detection rates of 76%. Previously reported variants in the F5, MTHFR, PROS1, PROC, F8, F9, SERPINA10, SERPIND1, and HRG genes were recognized in 21 patients. More than one variant in the targeted genes was detected in some of the patients with VTE. We identified SERPINA10 recurrent variant p.(R88*) in seven patients representing 32% of VTE cases. Additionally, we report one novel variant c.356G > T, p.(G119V) in the F7 gene, considered to be pathogenic in this study.
CONCLUSIONS
Our studies finding illustrates the ability of targeted next-generation sequencing to uncover uncommon/unknown genetic variants that may predispose to thrombophilia. The finding of the novel variant in the F7 gene extends the spectrum of variants affecting thrombosis. While a comparatively small number of subjects have been included in our cohort, the findings summarize the possible genetic features of thrombophilia.
背景
在包括阿拉伯人群在内的多个国家,血栓形成倾向是疾病和死亡的一个重要原因。伴有或不伴有肺栓塞(PE)的深静脉血栓形成(DVT)是血栓形成倾向的常见临床表现。虽然已知许多DVT的遗传风险因素,且几乎所有这些因素都与止血相关,但仍有许多遗传因素无法解释。如今,新一代测序(NGS)提供了一种潜在的解决方案,能够以合理的费用同时分析多个候选基因。
方法
我们使用Ion Torrent新一代测序(NGS)技术,对凝血因子V莱顿(FVL)突变阴性的血栓形成倾向相关基因进行变异筛查。设计了一个针对18个基因的Ion AmpliSeq检测板。招募了29例特发性静脉血栓栓塞症(VTE)患者进行NGS检测。
结果
我们在18个目标基因中的10个基因中鉴定出19个变异(1个新变异和18个先前报道的变异)。在22例患者中鉴定出致病变异,突变检出率为76%。在21例患者中识别出F5、MTHFR、PROS1、PROC、F8、F9、SERPINA10、SERPIND1和HRG基因中先前报道的变异。在一些VTE患者中检测到目标基因中的多个变异。我们在7例患者中鉴定出SERPINA10重复变异p.(R88*),占VTE病例的32%。此外,我们在F7基因中报告了一个新变异c.356G>T,p.(G119V),本研究认为该变异具有致病性。
结论
我们的研究结果表明,靶向新一代测序能够发现可能导致血栓形成倾向的罕见/未知遗传变异。F7基因中新变异的发现扩展了影响血栓形成的变异谱。虽然我们队列中的受试者数量相对较少,但这些发现总结了血栓形成倾向可能的遗传特征。
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