抗磷脂抗体患者中的凝血因子V莱顿突变、凝血酶原基因突变与血栓形成风险

Factor V Leiden, prothrombin gene mutation, and thrombosis risk in patients with antiphospholipid antibodies.

作者信息

Chopra Nikhil, Koren Sharon, Greer Wenda L, Fortin Paul R, Rauch Joyce, Fortin Isabelle, Senécal Jean-Luc, Docherty Peter, Hanly John G

机构信息

Division of Rheumatology, Dalhousie University, Halifax, Nova Scotia, Canada.

出版信息

J Rheumatol. 2002 Aug;29(8):1683-8.

PMID:12180730

Abstract

OBJECTIVE

To determine if the prevalence of 2 prothrombotic genetic factors, factor V Leiden and prothrombin gene mutation, is increased in patients with antiphospholipid (aPL) antibodies with a history of venous/arterial thrombosis compared to patients with aPL antibodies with no history of thrombosis.

METHODS

One hundred fifty-seven patients with aPL antibodies were studied. The occurrence of venous and arterial thrombotic events since the time of antibody detection was determined retrospectively, using appropriate clinical and diagnostic criteria. Clinical risk factors for thrombosis were documented and included hypertension, hyperlipidemia, cigarette smoking, diabetes, positive family history, use of oral contraceptive, pregnancy, trauma, hospitalization, varicose veins, and malignancy. Genomic DNA was extracted from blood cells for determination of factor V Leiden mutation G1691 --> A and prothrombin mutation G20210 --> A by polymerase chain reaction and restriction fragment length polymorphism analysis.

RESULTS

Of 157 patients, 69 had a history of thrombosis (venous 37, arterial 32); 147 (94%) patients had anticardiolipin (aCL) antibodies; 69 (45%) had lupus anticoagulant (LAC). The prevalence of factor V Leiden in patients with thrombosis was 13% compared to 4.6% in patients without thrombosis (OR 3.11, CI 0.92-10.6). In patients with aCL antibodies, 15% of patients with arterial thrombosis had factor V mutation compared to 3.5% of patients without thrombosis (OR 4.9, CI 1.2-19.3). The prothrombin gene mutation was identified in 5 patients, none of whom had thrombosis. Stepwise logistic regression analysis indicated that LAC (p = 0.005), male sex (p = 0.04), and hypertension (p = 0.03) were the strongest risk factors for developing thrombosis and that no additional risk was conferred by factor V Leiden (p = 0.13) and prothrombin gene mutation.

CONCLUSION

Although the prevalence of factor V Leiden is modestly increased in patients with autoimmune aPL antibodies and thrombosis, these results suggest that its detection does not significantly increase the risk of a thrombotic event, once other clinical risk factors have been considered. Prothrombin gene mutation is not associated with thrombosis in patients with aPL antibodies.

摘要

目的

确定与无血栓形成病史的抗磷脂（aPL）抗体患者相比，有静脉/动脉血栓形成病史的aPL抗体患者中两种促血栓形成遗传因素，即凝血因子V莱顿突变和凝血酶原基因突变的患病率是否增加。

方法

对157例aPL抗体患者进行研究。自抗体检测以来的静脉和动脉血栓形成事件的发生情况通过回顾性研究确定，采用适当的临床和诊断标准。记录血栓形成的临床危险因素，包括高血压、高脂血症、吸烟、糖尿病、阳性家族史、口服避孕药的使用、妊娠、创伤、住院、静脉曲张和恶性肿瘤。从血细胞中提取基因组DNA，通过聚合酶链反应和限制性片段长度多态性分析来确定凝血因子V莱顿突变G1691→A和凝血酶原突变G20210→A。

结果

157例患者中，69例有血栓形成病史（静脉血栓37例，动脉血栓32例）；147例（94%）患者有抗心磷脂（aCL）抗体；69例（45%）有狼疮抗凝物（LAC）。有血栓形成的患者中凝血因子V莱顿突变的患病率为13%，无血栓形成的患者中为4.6%（比值比3.11，可信区间0.92 - 10.6）。在有aCL抗体的患者中，动脉血栓形成患者中有15%有凝血因子V突变，无血栓形成的患者中为3.5%（比值比4.9，可信区间1.2 - 19.3）。在5例患者中检测到凝血酶原基因突变，这些患者均无血栓形成。逐步逻辑回归分析表明，LAC（p = 0.005）、男性（p = 0.04）和高血压（p = 0.03）是发生血栓形成的最强危险因素，而凝血因子V莱顿突变（p = 0.13）和凝血酶原基因突变并未增加额外风险。