Botto Nicoletta, Spadoni Isabella, Giusti Sandra, Ait-Ali Lamia, Sicari Rosa, Andreassi Maria Grazia
CNR Institute of Clinical Physiology, G. Pasquinucci Hospital, Massa, Italy.
Stroke. 2007 Jul;38(7):2070-3. doi: 10.1161/STROKEAHA.106.480863. Epub 2007 May 24.
Patent foramen ovale (PFO) has been identified as a potential risk factor for cerebrovascular ischemia. Procoagulant mutations may increase the risk and impact the choice of appropriate therapy for secondary prevention. We evaluated the prevalence of the 2 most common genetic risk factors for thromboembolism, factor V Leiden (G1691A) and prothrombin G20210A, in young PFO patients who were referred for percutaneous transcatheter closure of their PFO.
Ninety-seven patients (50 men; mean+/-SD age, 40.9+/-10.0 years) with first-ever cerebrovascular events before the age of 55 years and 160 age-matched control subjects (69 men; mean+/-SD age, 40.4+/-10.5 years) were recruited into the study. Factor V Leiden and prothrombin G20210A mutations were detected by using a multiplex allele-specific polymerase chain reaction assay.
The prevalence of subjects carrying at least 1 prothrombotic genotype was significantly higher in the group of PFO patients than in the group of controls (10.3% vs 2.5%; chi(2)=7.2, P=0.008). Two patients (2.1%) versus 1 control subject (0.6%) and 8 cases (8.2%) versus 3 controls (1.9%) were carriers for factor V Leiden and prothrombin G20210A mutations, respectively. After adjustment for other vascular risk factors, the combination of either factor V Leiden or prothrombin G20210A and PFO was associated with a 4.7-fold (95% CI=1.4 to 16.1; P=0.008) increased risk of cerebral ischemia in young patients.
Our results indicate that prothrombotic mutations are important risk factors for cerebral ischemia in young patients with PFO. Screening for thrombotic mutations should be considered in young patients with PFO-related ischemic events.
卵圆孔未闭(PFO)已被确定为脑血管缺血的一个潜在危险因素。促凝血基因突变可能会增加风险,并影响二级预防中适当治疗方法的选择。我们评估了在因PFO而接受经皮导管封堵术的年轻患者中,两种最常见的血栓栓塞遗传危险因素——凝血因子V莱顿突变(G1691A)和凝血酶原G20210A的患病率。
招募了97例首次发生脑血管事件且年龄在55岁以下的患者(50例男性;平均±标准差年龄为40.9±10.0岁)以及160例年龄匹配的对照者(69例男性;平均±标准差年龄为40.4±10.5岁)纳入研究。采用多重等位基因特异性聚合酶链反应检测凝血因子V莱顿突变和凝血酶原G20210A突变。
携带至少一种促血栓形成基因型的受试者在PFO患者组中的患病率显著高于对照组(10.3%对2.5%;χ²=7.2,P=0.008)。分别有2例患者(2.1%)和1例对照者(0.6%)以及8例患者(8.2%)和3例对照者(1.9%)是凝血因子V莱顿突变和凝血酶原G20210A突变的携带者。在对其他血管危险因素进行校正后,凝血因子V莱顿突变或凝血酶原G20210A突变与PFO的组合使年轻患者发生脑缺血的风险增加了4.7倍(95%CI=1.4至16.1;P=0.008)。
我们的结果表明,促血栓形成突变是年轻PFO患者发生脑缺血的重要危险因素。对于有PFO相关缺血事件的年轻患者,应考虑进行血栓形成突变的筛查。
