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Gene set analysis of GWAS data for human longevity highlights the relevance of the insulin/IGF-1 signaling and telomere maintenance pathways

机译:GWAS数据对人类寿命的基因集分析凸显了胰岛素/ IGF-1信号传导和端粒维持途径的相关性

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In genome-wide association studies (GWAS) of complex traits, single SNP analysis is still the most applied approach. However, the identified SNPs have small effects and provide limited biological insight. A more appropriate approach to interpret GWAS data of complex traits is to analyze the combined effect of a SNP set grouped per pathway or gene region. We used this approach to study the joint effect on human longevity of genetic variation in two candidate pathways, the insulin/insulin-like growth factor (IGF-1) signaling (IIS) pathway and the telomere maintenance (TM) pathway. For the analyses, we used genotyped GWAS data of 403 unrelated nonagenarians from long-lived sibships collected in the Leiden Longevity Study and 1,670 younger population controls. We analyzed 1,021 SNPs in 68 IIS pathway genes and 88 SNPs in 13 TM pathway genes using four self-contained pathway tests (PLINK set-based test, Global test, GRASS and SNP ratio test). Although we observed small differences between the results of the different pathway tests, they showed consistent significant association of the IIS and TM pathway SNP sets with longevity. Analysis of gene SNP sets from these pathways indicates that the association of the IIS pathway is scattered over several genes (AKT1, AKT3, FOXO4, IGF2, INS, PIK3CA, SGK, SGK2, and YWHAG), while the association of the TM pathway seems to be mainly determined by one gene (POT1). In conclusion, this study shows that genetic variation in genes involved in the IIS and TM pathways is associated with human longevity.
机译:在复杂性状的全基因组关联研究(GWAS)中,单SNP分析仍是最常用的方法。但是,已鉴定的SNP影响很小,并且生物学见识有限。解释复杂性状的GWAS数据的一种更合适的方法是分析按路径或基因区域分组的SNP集的组合效果。我们使用这种方法来研究两种候选途径(胰岛素/胰岛素样生长因子(IGF-1)信号传导(IIS)途径和端粒维持(TM)途径)对基因变异对人类寿命的共同影响。为了进行分析,我们使用了来自莱顿长寿研究中收集的403位无亲属长寿同胞和1670名年轻人口对照的基因分型GWAS数据。我们使用四个独立的途径测试(基于PLINK集的测试,全局测试,GRASS和SNP比率测试)分析了68个IIS途径基因中的1,021个SNP和13个TM途径基因中的88个SNP。尽管我们观察到了不同途径测试结果之间的细微差异,但它们显示了IIS和TM途径SNP集与寿命的持续显着关联。从这些途径分析基因SNP集表明,IIS途径的关联分散在多个基因(AKT1,AKT3,FOXO4,IGF2,INS,PIK3CA,SGK,SGK2和YWHAG)上,而TM途径的关联似乎主要由一个基因(POT1)决定。总之,这项研究表明,与IIS和TM途径有关的基因的遗传变异与人类寿命有关。

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