Heterozygous Prothrombin Mutation-Associated Thrombophilia.

IF 5 2区 医学 Q1 HEMATOLOGY Thrombosis and haemostasis Pub Date : 2024-07-02 DOI:10.1055/a-2350-8338
Xi Wu, Lei Li, Zhengjing Lu, Xiaobo Hu, Yeling Lu, Yu Liu, Guanqun Xu, Qiulan Ding, Xuefeng Wang, Wenman Wu, Peipei Jin, Jing Dai
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Abstract

Background:  Venous thromboembolism (VTE) is predisposed by thrombotic mutations in patients with hereditary thrombophilia. Although prothrombin deficiencies caused by homozygous or compound heterozygous mutations are associated with bleeding diathesis, rare cases have shown a correlation between heterozygous prothrombin mutations and thrombosis.

Materials and methods:  We surveyed genetic variants involved in thrombosis and hemostasis in 347 patients with unprovoked VTE or having a positive family history of thrombosis. For patients identified with heterozygous prothrombin mutations, we conducted family investigations and performed a thrombin generation test (TGT) to elucidate the thrombotic risk. Novel mutants were expressed and subjected to functional assays to clarify the underlying thrombotic mechanisms.

Results:  Heterozygous prothrombin mutations were identified in 3.5% of patients (12/347), including three novel mutations Phe382Ser, Phe382Leu, and Asp597Tyr found in one patient each, as well as previously reported Arg541Trp mutation in four patients and Arg596Gln mutation in five patients. A total of 42 mutation carriers were identified within the 12 pedigrees, among whom 64.3% (27/42) had experienced thrombotic events. TGT results demonstrated hypercoagulability for carriers of the five mutations, with Arg596Gln showing the highest thrombin generation potential followed by Arg541Trp. The Phe382-associated mutations severely impaired thrombomodulin-binding ability of thrombin, resulting in obviously reduced protein C (PC) activation. The Asp597Tyr mutation exhibited a mild reduction in both inactivation by antithrombin and PC activation reactions.

Conclusion: The presence of heterozygous prothrombin mutations represents a potential genetic predisposition for VTE. All thrombosis-associated mutations potentiate coagulation activity by either conferring antithrombin resistance and/or impairing PC pathway activity.

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与血栓性疾病相关的凝血酶原杂合子突变。
背景:静脉血栓栓塞症(VTE)易因遗传性血栓性疾病患者的血栓突变而发生。虽然由同型或复合杂合型突变导致的凝血酶原缺乏症与出血性疾病有关,但罕见病例显示杂合型凝血酶原突变与血栓形成之间存在相关性:我们调查了 347 名无诱因 VTE 患者或有阳性血栓形成家族史的患者中与血栓形成和止血有关的基因变异。对于发现有凝血酶原杂合突变的患者,我们进行了家族调查,并进行了凝血酶原生成试验(TGT),以阐明血栓风险。我们表达了新的突变体,并对其进行了功能测试,以阐明其潜在的血栓形成机制:结果:3.5%的患者(12/347)发现了凝血酶原杂合子突变,其中包括一名患者发现的 Phe382Ser、Phe382Leu 和 Asp597Tyr 三种新型突变,以及之前报道的四名患者的 Arg541Trp 突变和五名患者的 Arg596Gln 突变。12 个血统中总共发现了 42 个突变携带者,其中 64.3%(27/42)的人发生过血栓事件。TGT结果显示,五个突变的携带者都有高凝血功能,其中Arg596Gln的凝血酶生成潜能最高,其次是Arg541Trp。与 Phe382 相关的突变严重削弱了凝血酶与凝血调节蛋白的结合能力,导致蛋白 C(PC)活化能力明显降低。Asp597Tyr突变则轻度降低了抗凝血酶抑制和PC激活反应:结论:凝血酶原杂合突变的存在代表了 VTE 的潜在遗传易感性。所有与血栓形成相关的突变都会通过赋予抗凝血酶抗性和/或损害 PC 通路活性来增强凝血活性。
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来源期刊
Thrombosis and haemostasis
Thrombosis and haemostasis 医学-外周血管病
CiteScore
11.90
自引率
9.00%
发文量
140
审稿时长
1 months
期刊介绍: Thrombosis and Haemostasis publishes reports on basic, translational and clinical research dedicated to novel results and highest quality in any area of thrombosis and haemostasis, vascular biology and medicine, inflammation and infection, platelet and leukocyte biology, from genetic, molecular & cellular studies, diagnostic, therapeutic & preventative studies to high-level translational and clinical research. The journal provides position and guideline papers, state-of-the-art papers, expert analysis and commentaries, and dedicated theme issues covering recent developments and key topics in the field.
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