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DNA methylation GrimAge strongly predicts lifespan and healthspan

机译:DNA甲基化GrimAge强烈预测寿命和健康寿命

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摘要

It was unknown whether plasma protein levels can be estimated based on DNA methylation (DNAm) levels, and if so, how the resulting surrogates can be consolidated into a powerful predictor of lifespan. We present here, seven DNAm-based estimators of plasma proteins including those of plasminogen activator inhibitor 1 (PAI-1) and growth differentiation factor 15. The resulting predictor of lifespan, DNAm GrimAge (in units of years), is a composite biomarker based on the seven DNAm surrogates and a DNAm-based estimator of smoking pack-years. Adjusting DNAm GrimAge for chronological age generated novel measure of epigenetic age acceleration, AgeAccelGrim.Using large scale validation data from thousands of individuals, we demonstrate that DNAm GrimAge stands out among existing epigenetic clocks in terms of its predictive ability for time-to-death (Cox regression P=2.0E-75), time-to-coronary heart disease (Cox P=6.2E-24), time-to-cancer (P= 1.3E-12), its strong relationship with computed tomography data for fatty liver/excess visceral fat, and age-at-menopause (P=1.6E-12). AgeAccelGrim is strongly associated with a host of age-related conditions including comorbidity count (P=3.45E-17). Similarly, age-adjusted DNAm PAI-1 levels are associated with lifespan (P=5.4E-28), comorbidity count (P= 7.3E-56) and type 2 diabetes (P=2.0E-26). These DNAm-based biomarkers show the expected relationship with lifestyle factors including healthy diet and educational attainment.Overall, these epigenetic biomarkers are expected to find many applications including human anti-aging studies.
机译:尚不清楚是否可以根据DNA甲基化(DNAm)水平估算血浆蛋白水平,如果可以,则如何将所得替代物整合为有效的寿命预测指标。我们在这里介绍了七个血浆蛋白的基于DNAm的估计,包括纤溶酶原激活物抑制剂1(PAI-1)和生长分化因子15的估计。DNAmGrimAge(以年为单位)的寿命预测结果是基于复合生物标记的七个DNAm替代物和一个基于DNAm的吸烟年数估计量。调整DNAm GrimAge的年龄​​可以产生表观遗传加速的新方法AgeAccelGrim。使用来自成千上万个体的大规模验证数据,我们证明了DNAm GrimAge就其对死亡时间的预测能力而言在现有的表观时钟中脱颖而出( Cox回归P = 2.0E-75),冠状动脉心脏病(Cox P = 6.2E-24),癌变时间(P = 1.3E-12),其与脂肪X线计算机断层扫描数据的强相关性肝脏/内脏脂肪过多和绝经年龄(P = 1.6E-12)。 AgeAccelGrim与许多与年龄相关的疾病(包括合并症计数)紧密相关(P = 3.45E-17)。同样,年龄调整后的DNAm PAI-1水平与寿命(P = 5.4E-28),合并症计数(P = 7.3E-56)和2型糖尿病(P = 2.0E-26)相关。这些基于DNAm的生物标志物显示出与生活方式因素(包括健康饮食和受教育程度)的预期关系。总体而言,这些表观遗传生物标志物有望在人类抗衰老研究中找到许多应用。

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