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Genetic associations for two biological age measures point to distinct aging phenotypes

机译:两个生物学阶段措施的遗传关联指向明显的老化表型

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摘要

Biological age measures outperform chronological age in predicting various aging outcomes, yet little is known regarding genetic predisposition. We performed genome‐wide association scans of two age‐adjusted biological age measures (PhenoAgeAcceleration and BioAgeAcceleration), estimated from clinical biochemistry markers (Levine et al., 2018; Levine, 2013) in European‐descent participants from UK Biobank. The strongest signals were found in the APOE gene, tagged by the two major protein‐coding SNPs, PhenoAgeAccel—rs429358 (APOE e4 determinant) (p = 1.50 × 10−72); BioAgeAccel—rs7412 (APOE e2 determinant) (p = 3.16 × 10−60). Interestingly, we observed inverse APOE e2 and e4 associations and unique pathway enrichments when comparing the two biological age measures. Genes associated with BioAgeAccel were enriched in lipid related pathways, while genes associated with PhenoAgeAccel showed enrichment for immune system, cell function, and carbohydrate homeostasis pathways, suggesting the two measures capture different aging domains. Our study reaffirms that aging patterns are heterogeneous across individuals, and the manner in which a person ages may be partly attributed to genetic predisposition.
机译:生物学阶段测量比较时间的表现年龄在预测各种老化结果时,然而对于遗传易感性而言很少。我们进行了两年调整后的生物学措施(PhenoAcceoCeleration和生物胶质蛋白)的基因组 - 范围协会扫描,从临床生物化学标记估计(Levine等,2018; Levine,2013),来自英国Biobank的欧洲血统参与者。在ApoE基因中发现最强的信号,由两种主要蛋白质编码SNP标记,苯基乙酰脲-RS429358(APOE E4确定剂)(P = 1.50×10-72); BioAgeAccel-RS7412(Apoe E2决定簇)(P = 3.16×10-60)。有趣的是,在比较两个生物学措施时,我们观察到逆偶联E2和E4联想和独特的途径浓缩。与生物蛋白CCCEL相关的基因富集在脂质相关途径中,而与苯甲基CCH相关的基因显示出免疫系统,细胞功能和碳水化合物稳态途径的富集,这表明两种措施捕获不同的老化结构域。我们的研究重申,衰老模式在个体上是异质的,以及人们年龄可能部分归因于遗传易感性的方式。

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