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基于表观遗传学的美国老年人代表性样本的年龄加速:与与衰老相关的发病率和死亡率的关联。

Epigenetic-based age acceleration in a representative sample of older Americans: Associations with aging-related morbidity and mortality.

机构信息

Survey Research Center, Institute for Social Research, University of Michigan, Ann Arbor, MI 48104.

Davis School of Gerontology, University of Southern California, Los Angeles, CA 90089.

出版信息

Proc Natl Acad Sci U S A. 2023 Feb 28;120(9):e2215840120. doi: 10.1073/pnas.2215840120. Epub 2023 Feb 21.

Abstract

Biomarkers developed from DNA methylation (DNAm) data are of growing interest as predictors of health outcomes and mortality in older populations. However, it is unknown how epigenetic aging fits within the context of known socioeconomic and behavioral associations with aging-related health outcomes in a large, population-based, and diverse sample. This study uses data from a representative, panel study of US older adults to examine the relationship between DNAm-based age acceleration measures in the prediction of cross-sectional and longitudinal health outcomes and mortality. We examine whether recent improvements to these scores, using principal component (PC)-based measures designed to remove some of the technical noise and unreliability in measurement, improve the predictive capability of these measures. We also examine how well DNAm-based measures perform against well-known predictors of health outcomes such as demographics, SES, and health behaviors. In our sample, age acceleration calculated using "second and third generation clocks," PhenoAge, GrimAge, and DunedinPACE, is consistently a significant predictor of health outcomes including cross-sectional cognitive dysfunction, functional limitations and chronic conditions assessed 2 y after DNAm measurement, and 4-y mortality. PC-based epigenetic age acceleration measures do not significantly change the relationship of DNAm-based age acceleration measures to health outcomes or mortality compared to earlier versions of these measures. While the usefulness of DNAm-based age acceleration as a predictor of later life health outcomes is quite clear, other factors such as demographics, SES, mental health, and health behaviors remain equally, if not more robust, predictors of later life outcomes.

摘要

从 DNA 甲基化 (DNAm) 数据开发的生物标志物作为预测老年人健康结果和死亡率的指标越来越受到关注。然而,在一个大型、基于人群且多样化的样本中,尚不清楚表观遗传衰老与已知的社会经济和行为因素与衰老相关的健康结果之间的关系如何。本研究使用来自美国老年人代表性的面板研究的数据,检验了基于 DNAm 的年龄加速测量值在预测横断面和纵向健康结果和死亡率方面的关系。我们检验了这些评分的最近改进,使用基于主成分 (PC) 的测量方法来消除测量中的一些技术噪声和不可靠性,是否能提高这些测量的预测能力。我们还检验了基于 DNAm 的测量值与已知的健康结果预测因素(如人口统计学、SES 和健康行为)相比的表现如何。在我们的样本中,使用“第二代和第三代时钟”、PhenoAge、GrimAge 和 DunedinPACE 计算的年龄加速是健康结果的一个显著预测因素,包括横断面认知功能障碍、功能限制和慢性疾病,这些疾病在 DNAm 测量后 2 年和 4 年死亡进行评估。与这些措施的早期版本相比,基于 PC 的表观遗传年龄加速措施并不会显著改变 DNAm 年龄加速措施与健康结果或死亡率之间的关系。虽然基于 DNAm 的年龄加速作为预测晚年健康结果的指标非常有效,但其他因素,如人口统计学、SES、心理健康和健康行为,同样是(如果不是更强大)预测晚年结果的因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c0d8/9992763/169f87f9d8a3/pnas.2215840120fig01.jpg

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