欧洲北部和南部血浆凝血酶活化纤维蛋白溶解抑制剂抗原浓度和基因型与心肌梗死的关系

I. Juhan-vague, P. Morange, Hélène Aubert, M. Henry, M. Aillaud, M. Alessi, A. Samnegård, E. Hawe, J. Yudkin, M. Margaglione, G. Minno, A. Hamsten, S. Humphries
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引用次数: 175

摘要

凝血酶活化纤维蛋白溶解抑制剂(TAFI)是最近发现的一种纤维蛋白溶解抑制剂,可减少纤溶酶原与纤维蛋白表面的结合。血浆TAFI浓度几乎完全由基因决定。我们研究了血浆TAFI水平和TAFI基因多态性是否可以构成心肌梗死(MI)的危险标志。ELISA检测血浆TAFI抗原(Ag)水平,并在一项大型欧洲病例对照研究中测定了2个TAFI基因多态性(3 '非翻译区Ala147Thr和C+1542G)。这项研究比较了598名在心肌梗死后3 - 6个月招募的男性和653名来自北欧(瑞典斯德哥尔摩和英国伦敦)和南欧(法国马赛和意大利圣乔凡尼罗通多)的年龄匹配的对照组。TAFI Ag值高于第90百分位与心肌梗死风险显著降低相关(比值比0.55,P <0.02),表明TAFI升高可能对心肌梗死有保护作用。如前所述,2个TAFI基因多态性处于强连锁不平衡状态,与TAFI Ag浓度相关,其中Thr147和1542C等位基因的携带者水平较高(P <0.0005)。这些影响在对照组和病例中以及在每个中心都是相似的。Ala147Thr多态性的等位基因频率与对照组存在差异,斯德哥尔摩(P =0.03)和San Giovanni Rotondo (P =0.03)两个中心的对照组携带Thr147等位基因的频率高于对照组(P =0.03);整个队列的优势比为0.78 (P <0.05)。总之,近期心肌梗死患者TAFI Ag值较低,“TAFI减少”等位基因频率较高。所观察到的地理差异并不能解释欧洲心肌梗死风险的南北梯度。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Plasma Thrombin-Activatable Fibrinolysis Inhibitor Antigen Concentration and Genotype in Relation to Myocardial Infarction in the North and South of Europe
The thrombin-activatable fibrinolysis inhibitor (TAFI) is a recently described inhibitor of fibrinolysis that decreases plasminogen binding to the fibrin surface. The plasma TAFI concentration is almost entirely genetically determined. We investigated whether plasma TAFI levels and polymorphisms located in the TAFI gene could constitute risk markers of myocardial infarction (MI). Plasma TAFI antigen (Ag) levels were assayed by ELISA and 2 TAFI gene polymorphisms (Ala147Thr and C+1542G in the 3′ untranslated region) were determined in a large European case-control study. This study compared 598 men recruited 3 to 6 months after MI with 653 age-matched controls from North Europe (Stockholm, Sweden, and London, England) and South Europe (Marseilles, France, and San Giovanni Rotondo, Italy). A TAFI Ag value above the 90th percentile was associated with a significantly lower risk of MI (odds ratio 0.55, P <0.02), indicating that elevated TAFI may be protective against MI. As previously shown, the 2 TAFI gene polymorphisms were in strong linkage disequilibrium and were associated with the TAFI Ag concentration, with carriers of the Thr147 and 1542C alleles having higher levels (P <0.0005). These effects were similar in controls and cases and in each center. There was a difference in allele frequency between cases and controls for the Ala147Thr polymorphism, with Thr147 allele carriers being more frequent in controls than in cases in 2 centers, Stockholm (P =0.03) and San Giovanni Rotondo (P =0.03); the odds ratio for the entire cohort was 0.78 (P <0.05). In conclusion, patients with a recent MI presented lower values of TAFI Ag and higher frequencies of the “TAFI-decreasing” alleles. The geographical differences observed do not contribute to explaining the North-South gradient in MI risk in Europe.
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