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Ancestry-specific polygenic scores and SNP heritability of 25(OH)D in African- and European-ancestry populations

机译:在非洲和欧洲祖先人群中,祖先特异性的多基因分数和25(OH)D的SNP遗传性

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摘要

Vitamin D inadequacy, assessed by 25-hydroxyvitamin D [25(OH)D], affects around 50% of adults in the United States and is associated with numerous adverse health outcomes. Blood 25(OH)D concentrations are influenced by genetic factors that may determine how much vitamin D intake is required to reach optimal 25(OH)D. Despite large genome-wide association studies (GWASs), only a small portion of the genetic factors contributing to differences in 25(OH)D has been discovered. Therefore, knowledge of a fuller set of genetic factors could be useful for risk prediction of 25(OH)D inadequacy, personalized vitamin D supplementation, and prevention of downstream morbidity and mortality. Using PRSice and weights from published African- and European-ancestry GWAS summary statistics, ancestry-specific polygenic scores (PGSs) were created to capture a more complete set of genetic factors in those of European (n = 9569) or African ancestry (n = 2761) from three cohort studies. The PGS for African ancestry was derived using all input SNPs (a p value cutoff of 1.0) and had an R-2 of 0.3%; for European ancestry, the optimal PGS used a p value cutoff of 3.5 x 10(-4) in the target/tuning dataset and had an R-2 of 1.0% in the validation cohort. Those with highest genetic risk had 25(OH)D that was 2.8-3.0 ng/mL lower than those with lowest genetic risk (p = 0.0463-3.2 x 10(-13)), requiring an additional 467-500 IU of vitamin D intake to maintain equivalent 25(OH)D. PGSs are a powerful predictive tool that could be leveraged for personalized vitamin D supplementation to prevent the negative downstream effects of 25(OH)D inadequacy.
机译:维生素d不足,25羟d [25(OH)d]评估,影响大约50%的美国成年人中,并与众多不良健康结果相关联。血液25(OH)d浓度是由可确定如何的维生素d摄入需要达到最佳25(OH)d遗传因素的影响。尽管大的全基因组关联研究(GWASs),仅在25(OH)d有助于差的遗传因素的一小部分已发现。因此,更全面的集合的遗传因素的知识可能是25(OH)d不足的风险预测,个性化的维生素补充d,和预防下游发病率和死亡率是有用的。使用PRSice和权重,从公布的非裔和欧洲血统GWAS汇总统计,具体的血统,多基因的分数(PGSS)的建立是为了获取一套较为完整的遗传因素在那些欧洲的(N = 9569)或非洲血统(N = 2761)从三个队列研究。对非洲血统的PGS使用所有输入的SNP(一个1.0的p值截止值)导出并有一个R-2 0.3%;对于欧洲血统,最佳PGS在目标/调谐数据集使用的3.5×10(-4)的p值截止和有一个R-2 1.0%,在验证队列。那些具有最高遗传风险有这样的25(OH)d 2.8-3.0纳克/毫升比那些具有最低遗传风险降低(p = 0.0463-3.2×10(-13)),其要求维生素d额外467-500 IU进保持当量25(OH)d。 PGSS是一个强大的预测工具,可利用个性化的维生素补充d,以防止25(OH)d不足的负下游效应。

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  • 来源
    《Human Genetics》 |2019年第10期|共15页
  • 作者单位

    Univ Wisconsin Sch Med &

    Publ Hlth Dept Populat Hlth Sci Madison WI 53706 USA;

    Univ Wisconsin Sch Med &

    Publ Hlth Dept Biostat &

    Med Informat Madison WI 53706 USA;

    Marshfield Clin Res Inst Ctr Human Genet Marshfield WI 54449 USA;

    Johns Hopkins Univ Sch Med Ciccarone Ctr Prevent Cardiovasc Dis Baltimore MD 21287 USA;

    USDA ARS Childrens Nutr Res Ctr Baylor Coll Med Houston TX 77030 USA;

    Univ Wisconsin Sch Med &

    Publ Hlth Dept Populat Hlth Sci Madison WI 53706 USA;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 医学遗传学;
  • 关键词

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