Epigenetic age acceleration is related to cognitive decline in the elderly: Results of the Austrian Stroke Prevention Study.

IF 5 3区 医学 Q1 CLINICAL NEUROLOGY
Psychiatry and Clinical Neurosciences Pub Date : 2025-05-01 Epub Date: 2025-02-08 DOI:10.1111/pcn.13793
Piyush Gampawar, Sai Pavan Kumar Veeranki, Katja-Elisabeth Petrovic, Reinhold Schmidt, Helena Schmidt
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Abstract

Aim: Epigenetic clocks, quantifying biological age through DNA methylation (DNAmAge), have emerged as potential indicators of brain aging. As the variety of DNAmAge algorithms grows, consensus on their efficacy in predicting age-related changes is lacking. This study aimed to explore the intricate relationship between diverse DNAmAge algorithms and structural and cognitive markers of brain aging.

Methods: Within a cohort of 796 elderly patients (mean age, 65.8 ± 7.9 years), we scrutinized 11 DNAmAge algorithms, including Horvath, Hannum, Zhang's clocks, PhenoAge, GrimAge, DunedinPACE, and principal component (PC)-based PCHorvath, PCHannum, PCPhenoAge, and PCGrimAge. We evaluated their association with baseline cognition and cognitive decline, assessed through follow-up evaluations at three (T1) and six (T2) years postbaseline. Additionally, we examined their relationship with structural magnetic resonance imaging markers of brain aging, including white matter.

Results: Zhang's clock was the best predictor of decline in memory (β = -0.04) and global cognition (β = -0.03), whereas PCGrimAge was the best predictor of speed decline (β = -0.17). The DNAmAge algorithms were the second-best predictors in explaining cognitive variability after education in memory and global cognition (R2 partial = 1.66% to 2.82%) and the best predictors for speed decline (R2 partial = 2.13%). PC-trained DNAmAge algorithms outperformed their respective original version.

Conclusion: DNAmAge algorithms are strong and independent predictors of cognitive decline in the normal elderly population and explain additional variability in cognitive decline beyond that accounted for by conventional risk factors.

表观遗传年龄加速与老年人认知能力下降有关:奥地利中风预防研究的结果。
目的:表观遗传时钟,通过DNA甲基化(DNAmAge)来量化生物年龄,已经成为大脑衰老的潜在指标。随着各种DNAmAge算法的增长,对它们在预测年龄相关变化方面的有效性缺乏共识。本研究旨在探索不同DNAmAge算法与大脑衰老的结构和认知标志物之间的复杂关系。方法:在796例老年患者(平均年龄65.8±7.9岁)的队列中,我们仔细检查了11种DNAmAge算法,包括Horvath、Hannum、Zhang的时钟、PhenoAge、GrimAge、DunedinPACE以及基于主成分(PC)的PCHorvath、PCHannum、PCPhenoAge和PCGrimAge。我们通过基线后3年(T1)和6年(T2)的随访评估,评估了它们与基线认知和认知衰退的关系。此外,我们还研究了它们与脑老化的结构磁共振成像标志物(包括白质)的关系。结果:张氏时钟是记忆衰退(β = -0.04)和整体认知衰退(β = -0.03)的最佳预测因子,而PCGrimAge是速度衰退的最佳预测因子(β = -0.17)。DNAmAge算法在解释记忆和整体认知教育之后的认知变异方面是第二好的预测因子(R2偏= 1.66%至2.82%),在解释速度下降方面是最好的预测因子(R2偏= 2.13%)。pc训练的DNAmAge算法比它们各自的原始版本表现得更好。结论:DNAmAge算法是正常老年人认知能力下降的强大而独立的预测因子,并解释了传统危险因素之外认知能力下降的额外变异性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
7.40
自引率
4.20%
发文量
181
审稿时长
6-12 weeks
期刊介绍: PCN (Psychiatry and Clinical Neurosciences) Publication Frequency: Published 12 online issues a year by JSPN Content Categories: Review Articles Regular Articles Letters to the Editor Peer Review Process: All manuscripts undergo peer review by anonymous reviewers, an Editorial Board Member, and the Editor Publication Criteria: Manuscripts are accepted based on quality, originality, and significance to the readership Authors must confirm that the manuscript has not been published or submitted elsewhere and has been approved by each author
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