A Alvarez, A Barroso, M Robledo, E Arranz, J Outeiriño, J Benítez
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引用次数: 0
Abstract
Unlabelled: Factor V Leiden and G20210A mutation of the prothrombin gene have been described as risk factors in thrombophilic pathologies. Our objective has been to know the prevalence of these two mutations in a group of patients with thrombophilic pathology and to compare it with its prevalence in a control group of Spanish population.
Patients and methods: 64 patients were divided in two groups. First, 39 patients with deep venous thrombosis (DVT): 24 with an unique episode of DVT; 11 with more than one episode; 3 with DVT and pulmonary thromboembolism, and one with DVT and more than one episode of cerebral thrombosis. Second, 25 patients with other pathologies, such as pulmonary thromboembolism (9 patients), acute cerebrovascular accident (10 patients) and 6 who came to our Department because there were some carrier in their families. The 20210A allele was analyzed in 37 of the 64 patients. Some of the 64 patients had haematological determinations of the activated protein C resistance (APC resistance). As well, 103 unrelated subjects with unknown thrombotic pathologies were analyzed.
Results: We have found a prevalence of factor V Leiden in the group of patients of 14.1% (9 carriers in 64 patients, all of them in the first group of 39 patients with DVT) versus 1% in the control group (1 carrier in 103 controls). On the other hand, the difference between the prevalence of the 20210A allele was not statistically significant between the group of patients and the control group (2.7% vs 2.9%). In 75% of the patients no haematological results of APC resistance were obtained, generally because they were with anticoagulant treatment, and in 11.1% of the carriers the result of the determination was considered as ambiguous or false negative.
Conclusion: Factor V Leiden is well established as risk factor in the thrombophilic pathology, but more studies are needed to know the meaning of the G20210A mutation of the prothrombin gene.
未标记:因子V Leiden和凝血酶原基因的G20210A突变已被描述为血栓性疾病的危险因素。我们的目标是了解这两种突变在一组有血栓形成病理的患者中的患病率,并将其与西班牙人口对照组中的患病率进行比较。患者与方法:64例患者分为两组。首先,39例深静脉血栓(DVT)患者:24例有独特的DVT发作;11集以上;3例伴有深静脉血栓和肺血栓栓塞,1例伴有深静脉血栓和一次以上脑血栓发作。其次,其他病理患者25例,如肺血栓栓塞(9例),急性脑血管意外(10例),6例因家族有携带者而来我科就诊。64例患者中有37例分析了20210A等位基因。64例患者中部分患者有活动性蛋白C耐药(APC耐药)血液学检测。同时,对103例不相关的未知血栓病理进行了分析。结果:我们发现Leiden因子V在患者组中的患病率为14.1%(64例患者中有9例携带者,均为第1组(39例DVT患者)),而对照组为1%(103例对照中有1例携带者)。另一方面,20210A等位基因的患病率在患者组与对照组之间差异无统计学意义(2.7% vs 2.9%)。75%的患者未获得APC耐药血液学结果,通常是因为他们接受了抗凝治疗,11.1%的携带者的检测结果被认为是模糊或假阴性。结论:凝血酶原基因G20210A突变在血栓形成病理中的危险因素已被证实,但凝血酶原基因G20210A突变的意义尚需进一步研究。
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