血小板糖蛋白基因多态性与血栓形成的风险:事实和幻想。

A. Reiner, D. Siscovick, F. Rosendaal
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引用次数: 37

摘要

在过去的几年中,血小板糖蛋白基因多态性作为血栓形成倾向的可能遗传决定因素受到越来越多的关注。然而,它们在血栓性疾病遗传易感性中的作用仍然存在争议。糖蛋白IIIa Leu33Pro氨基酸替代似乎与体外血小板血栓形成性的微妙影响有关,但不是普通人群动脉血栓性疾病的主要危险因素。有证据表明,糖蛋白IIIa Pro33等位基因可能与冠状动脉再血管重建后血栓形成事件的风险增加有关,并且可能与年轻的动脉粥样硬化患者有关。糖蛋白Ia的核苷酸807T变异与血小板糖蛋白Ia/IIa受体密度增加、胶原诱导的血小板粘附以及早发性心肌梗死和卒中风险增加有关。由于糖蛋白Ibalpha Thr145Met和可变数量的串联重复多态性对血小板粘附功能缺乏明确的影响,以及两个位点之间强烈的连锁不平衡,对其作用的评估变得复杂。未来血小板糖蛋白基因多态性的流行病学研究将需要更大的样本量和基于家族的方法来进一步阐明与血栓性疾病的临床重要关联,包括基因-环境和基因-基因相互作用。在编码血小板膜蛋白的基因中,其他具有潜在功能意义的多态性无疑将被发现。挑战将是整合血小板生物学与分子和遗传流行病学的进展,以加强我们对常见但病因复杂的血栓性疾病的遗传决定因素的理解。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Platelet glycoprotein gene polymorphisms and risk of thrombosis: facts and fancies.
Over the past several years, platelet glycoprotein gene polymorphisms have received increasing attention as possible inherited determinants of prothrombotic tendency. However, their role in genetic susceptibility to thrombotic disease remains controversial. The glycoprotein IIIa Leu33Pro amino acid substitution appears to be associated with a subtle effect on platelet thrombogenicity in vitro, but is not a major risk factor for arterial thrombotic disease among the general population. Evidence suggests that the glycoprotein IIIa Pro33 allele may be associated with increased risk of thrombotic events following coronary re-vascularization and possibly among younger subjects with atherosclerosis. The nucleotide 807T variant of glycoprotein Ia is associated with increased platelet glycoprotein Ia/IIa receptor density, collagen-induced platelet adhesion and an increased risk of early onset myocardial infarction and stroke. Evaluation of the roles of the glycoprotein Ibalpha Thr145Met and variable number of tandem repeat polymorphisms has been complicated by their lack of well-defined effects on platelet adhesive function and the strong linkage disequilibrium between the two sites. Future epidemiologic studies of platelet glycoprotein gene polymorphisms will require larger sample sizes and family based approaches to further elucidate clinically important associations with thrombotic disease, including gene-environment and gene-gene interactions. Other polymorphisms of potential functional significance within genes encoding platelet membrane proteins will undoubtedly be discovered. The challenge will be to integrate advances in platelet biology with molecular and genetic epidemiology to enhance our understanding of the genetic determinants of common, but etiologically complex thrombotic diseases.
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