ATAC-clock: An aging clock based on chromatin accessibility

被引:0
|
作者
Francesco Morandini
Cheyenne Rechsteiner
Kevin Perez
Viviane Praz
Guillermo Lopez Garcia
Laura C. Hinte
Ferdinand von Meyenn
Alejandro Ocampo
机构
[1] University of Lausanne,Department of Biomedical Sciences
[2] EPITERNA SA,Departamento de Lenguajes y Ciencias de la Computación
[3] Universidad de Málaga,Department of Health Sciences and Technology
[4] ETH Zurich,undefined
来源
GeroScience | 2024年 / 46卷
关键词
Aging; Epigenetic clock; Chromatin accessibility; ATAC sequencing; Biomarker;
D O I
暂无
中图分类号
学科分类号
摘要
The establishment of aging clocks highlighted the strong link between changes in DNA methylation and aging. Yet, it is not known if other epigenetic features could be used to predict age accurately. Furthermore, previous studies have observed a lack of effect of age-related changes in DNA methylation on gene expression, putting the interpretability of DNA methylation-based aging clocks into question. In this study, we explore the use of chromatin accessibility to construct aging clocks. We collected blood from 159 human donors and generated chromatin accessibility, transcriptomic, and cell composition data. We investigated how chromatin accessibility changes during aging and constructed a novel aging clock with a median absolute error of 5.27 years. The changes in chromatin accessibility used by the clock were strongly related to transcriptomic alterations, aiding clock interpretation. We additionally show that our chromatin accessibility clock performs significantly better than a transcriptomic clock trained on matched samples. In conclusion, we demonstrate that the clock relies on cell-intrinsic chromatin accessibility alterations rather than changes in cell composition. Further, we present a new approach to construct epigenetic aging clocks based on chromatin accessibility, which bear a direct link to age-related transcriptional alterations, but which allow for more accurate age predictions than transcriptomic clocks.
引用
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页码:1789 / 1806
页数:17
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