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首页> 外文期刊>Mechanisms of Ageing and Development >A genome-wide association study confirms APOE as the major gene influencing survival in long-lived individuals.
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A genome-wide association study confirms APOE as the major gene influencing survival in long-lived individuals.

机译:全基因组关联研究证实APOE是影响长寿个体生存的主要基因。

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We conducted a case-control genome-wide association study (GWAS) of human longevity, comparing 664,472 autosomal SNPs in 763 long-lived individuals (LLI; mean age: 99.7 years) and 1085 controls (mean age: 60.2 years) from Germany. Only one association, namely that of SNP rs4420638 near the APOC1 gene, achieved genome-wide significance (allele-based P=1.8x10(-10)). However, logistic regression analysis revealed that this association, which was replicated in an independent German sample, is fully explicable by linkage disequilibrium with the APOE allele varepsilon4, the only variant hitherto established as a major genetic determinant of survival into old age. Our GWAS failed to identify any additional autosomal susceptibility genes. One explanation for this lack of success in our study would be that GWAS provide only limited statistical power for a polygenic phenotype with loci of small effect such as human longevity. A recent GWAS in Dutch LLI independently confirmed the APOE-longevity association, thus strengthening the conclusion that this locus is a very, if not the most, important genetic factor influencing longevity.
机译:我们进行了一项人类寿命的病例对照全基因组关联研究(GWAS),比较了来自德国的763个长寿个体(LLI;平均年龄:99.7岁)和1085个对照(平均年龄:60.2岁)中的664,472个常染色体SNP。只有一个关联,即APOC1基因附近的SNP rs4420638关联,实现了全基因组意义(基于等位基因的P = 1.8x10(-10))。但是,逻辑回归分析表明,这种关联在一个独立的德国样本中重复存在,可以通过与APOE等位基因varepsilon4的连锁不平衡来充分阐明,APOE等位基因varepsilon4是迄今为止确定为存活至老年的主要遗传决定因素。我们的GWAS无法识别任何其他常染色体易感性基因。对于我们的研究缺乏成功的一个解释是,GWAS仅对具有诸如人类长寿之类的小影响基因座的多基因表型提供有限的统计能力。荷兰LLI中最近的GWAS独立地证实了APOE与长寿的关联,因此进一步证实了该基因座是一个影响长寿的非常(即使不是最重要)遗传因素的结论。

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