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首页> 外文期刊>British Journal of Haematology >Genotype-phenotype relationship for six common polymorphisms in genes affecting platelet function from 286 healthy subjects and 160 patients with mucocutaneous bleeding of unknown cause.
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Genotype-phenotype relationship for six common polymorphisms in genes affecting platelet function from 286 healthy subjects and 160 patients with mucocutaneous bleeding of unknown cause.

机译:286位健康受试者和160位原因不明的粘膜皮肤出血患者的影响血小板功能的基因中的六个常见多态性的基因型与表型关系。

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摘要

Polymorphisms affecting platelet receptors and intracellular proteins have been extensively studied in relation to their potential influence in thrombosis and haemorrhages. However, few reports have addressed their impact on platelet function, with contradictory results. Limitations of these studies include, among others, small number of patients, the platelet functional parameters analyzed and their known variability in the healthy population. We studied the effect of six polymorphisms [ITGB3 1565T > C (HPA-1), GPIBA variable number tandem repeat and 524C > T (HPA-2), ITGA2 807C > T, ADRA2A 1780A > G, and TUBB1 Q43P] on platelet function in 286 healthy subjects and their potential pathogenetic role in 160 patients with hereditary mucocutaneous bleeding of unknown cause. We found no effect of any of these polymorphisms on platelet aggregation, secretion, PFA-100, and thrombin generation in platelet rich plasma. Furthermore, patients and controls showed no significant differences in the frequency of any of these polymorphisms. Thus, our study demonstrated that polymorphisms in genes affecting platelet function do not influence significantly major platelet functions and appear irrelevant in the pathogenesis of bleeding disorders.
机译:影响血小板受体和细胞内蛋白的多态性已被广泛研究,涉及其对血栓形成和出血的潜在影响。但是,很少有报道谈到其对血小板功能的影响,但结果却相矛盾。这些研究的局限性包括:少数患者,分析的血小板功能参数及其在健康人群中的已知变异性。我们研究了六种多态性[ITGB3 1565T> C(HPA-1),GPIBA可变数串联重复序列和524C> T(HPA-2),ITGA2 807C> T,ADRA2A 1780A> G和TUBB1 Q43P]在286名健康受试者中的研究及其在160例原因不明的遗传性皮肤黏膜出血患者中的潜在致病作用。我们发现这些多态性对富含血小板的血浆中的血小板聚集,分泌,PFA-100和凝血酶生成均无影响。此外,患者和对照组在这些多态性的频率上均无显着差异。因此,我们的研究表明,影响血小板功能的基因中的多态性不会显着影响主要的血小板功能,并且与出血性疾病的发病机制无关。

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