首页> 美国卫生研究院文献>Haematologica >Platelet adhesion to decorin but not collagen I correlates with the integrin α2 dimorphism E534K the basis of the human platelet alloantigen (HPA)-5 system
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Platelet adhesion to decorin but not collagen I correlates with the integrin α2 dimorphism E534K the basis of the human platelet alloantigen (HPA)-5 system

机译:血小板对除蛋白的粘附而不是胶原蛋白I与整联蛋白α2二态性E534K相关后者是人血小板同种抗原(HPA)-5系统的基础

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摘要

A single nucleotide polymorphism in the integrin α2 gene ITGA2 (rs1801106; G1600A) creates the non-conservative amino acid substitution E534K, the basis of the human platelet alloantigen system HPA-5. Yet HPA-5 alleles do not influence binding of α2β1 to its primary ligand collagen I, and the effect of HPA-5 on platelet function has not been determined. We used a direct platelet adhesion assay to evaluate whether differential inheritance of HPA-5 alleles influences platelet adhesion to collagen I or an alternative ligand, decorin. Platelets from donors bearing one or more minor allele HPA-5b showed attenuated adhesion to purified decorin but not collagen I. Adhesion to decorin was significantly inhibited by human alloantibodies specific for HPA-5a but not by the collagen I sequence GFOGER or α2-specific inhibitory monoclonal antibodies. The minor allele 534K attenuates platelet adhesion to decorin but not collagen I, providing the first evidence of a functional effect of HPA-5 alleles.
机译:整联蛋白α2基因ITGA2(rs1801106; G1600A)中的单核苷酸多态性产生了非保守氨基酸取代E534K,这是人血小板同种抗原系统HPA-5的基础。然而,HPA-5等位基因并不影响α2β1与其主要配体胶原蛋白I的结合,并且尚未确定HPA-5对血小板功能的影响。我们使用直接血小板粘附测定法评估HPA-5等位基因的差异遗传是否影响血小板与胶原蛋白I或替代配体decorin的粘附。来自带有一个或多个次要等位基因HPA-5b的供体的血小板显示与纯化的除蛋白而不是胶原I的粘附力减弱。对除蛋白的粘附被HPA-5a特异的人同种抗体显着抑制,但不受胶原蛋白I序列GFOGER或α2特异性抑制单克隆抗体。次要等位基因534K减弱了血小板对除蛋白的粘附力,但不减弱胶原蛋白I,这是HPA-5等位基因发挥功能作用的第一个证据。

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