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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Influence of single nucleotide polymorphisms in factor VIII and von Willebrand factor genes on plasma factor VIII activity: The ARIC Study
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Influence of single nucleotide polymorphisms in factor VIII and von Willebrand factor genes on plasma factor VIII activity: The ARIC Study

机译:VIII因子和von Willebrand因子基因中的单核苷酸多态性对血浆VIII因子活性的影响:ARIC研究

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Factor VIII (FVIII) functions as a cofactor for factor IXa in the contact coagulation pathway and circulates in a protective complex with von Willebrand factor (VWF). Plasma FVIII activity is strongly influenced by environmental and genetic factors through VWF-dependent and -independent mechanisms. Single nucleotide polymorphisms (SNPs) of the coding and promoter sequence in the FVIII gene have been extensively studied for effects on FVIII synthesis, secretion, and activity, but impacts of non- disease-causing intronic SNPs remain largely unknown. We analyzed FVIII SNPs and FVIII activity in 10 434 healthy Americans of European (EA) or African (AA) descent in theAtherosclerosis Risk inCommunities (ARIC) study. Among covariates, age, race, diabetes, and ABO contributed 2.2%, 3.5%, 4%, and 10.7% to FVIII intersubject variation, respectively. Four intronic FVIII SNPsassociated with FVIII activityand8 with FVIII-VWF ratio in a sex- and race-dependent manner. The FVIII haplotypes AT and GCTTTT also associated with FVIII activity. SevenVWFSNPs were associated with FVIII activity in EA subjects, but no FVIII SNPs were associated with VWF Ag. These data demonstrate that intronic SNPs could directly or indirectly influence intersubject variation of FVIII activity. Further investigation may reveal novel mechanisms of regulating FVIII expression and activity.
机译:因子VIII(FVIII)在接触凝血途径中充当因子IXa的辅助因子,并在与von Willebrand因子(VWF)的保护性复合物中循环。血浆FVIII活性通过VWF依赖性和非依赖性机制受到环境和遗传因素的强烈影响。已经对FVIII基因中编码和启动子序列的单核苷酸多态性(SNP)对FVIII合成,分泌和活性的影响进行了广泛研究,但非致病性内含子SNP的影响仍然未知。在动脉粥样硬化风险社区研究(ARIC)中,我们分析了欧洲人(EA)或非洲人(AA)血统的10 434名健康美国人的FVIII SNP和FVIII活性。在协变量中,年龄,种族,糖尿病和ABO分别占FVIII受试者间变异的2.2%,3.5%,4%和10.7%。四个内含子FVIII SNP以性别和种族依赖性方式与FVIII活性和8具有FVIII-VWF比率相关。 FVIII单倍型AT和GCTTTT也与FVIII活性相关。 SevenVWFSNP与EA受试者的FVIII活性相关,但FVIII SNP没有与VWF Ag相关。这些数据表明内含子SNPs可以直接或间接影响受试者之间FVIII活性的变化。进一步的研究可能揭示调节FVIII表达和活性的新机制。

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