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Aging of blood can be tracked by DNA methylation changes at just three CpG sites
Carola I. Weidner, Qiong Lin, Carmen Koch, Lewin Eisele, Fabian Beier, Patrick Ziegler, Dirk Bauerschlag, Karl‐Heinz Jöckel, Raimund Erbel, Thomas W. Mühleisen, Martin Zenke, Tim H. Brümmendorf, Wolfgang Wagner
Genome biology · 2014 · ▲ 950 citations
Abstract
BACKGROUND: Human aging is associated with DNA methylation changes at specific sites in the genome. These epigenetic modifications may be used to track donor age for forensic analysis or to estimate biological age. RESULTS: We perform a comprehensive analysis of methylation profiles to narrow down 102 age-related CpG sites in blood. We demonstrate that most of these age-associated methylation changes are reversed in induced pluripotent stem cells (iPSCs). Methylation levels at three age-related CpGs--located in the genes ITGA2B, ASPA and PDE4C--were subsequently analyzed by bisulfite pyrosequencing of 151 blood samples. This epigenetic aging signature facilitates age predictions with a mean absolute deviation from chronological age of less than 5 years. This precision is higher than age predictions based on telomere(definition) length. Variation of age predictions correlates moderately with clinical and lifestyle parameters supporting the notion that age-associated methylation changes are associated more with biological age than with chronological age. Furthermore, patients with acquired aplastic anemia or dyskeratosis congenita--two diseases associated with progressive bone marrow failure and severe telomere attrition--are predicted to be prematurely aged. CONCLUSIONS: Our epigenetic aging signature provides a simple biomarker to estimate the state of aging in blood. Age-associated DNA methylation changes are counteracted in iPSCs. On the other hand, over-estimation of chronological age in bone marrow failure syndromes is indicative for exhaustion of the hematopoietic cell pool. Thus, epigenetic changes upon aging seem to reflect biological aging of blood.
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- 10.1186/gb-2014-15-2-r24
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- 2026-06-02 MST
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APA
Weidner, C.I., Lin, Q., Koch, C., Eisele, L., Beier, F., Ziegler, P., Bauerschlag, D., Jöckel, K., Erbel, R., Mühleisen, T.W., Zenke, M., Brümmendorf, T.H., & Wagner, W. (2014). Aging of blood can be tracked by DNA methylation changes at just three CpG sites. <em>Genome biology</em>. https://doi.org/10.1186/gb-2014-15-2-r24
Vancouver
Weidner CI, Lin Q, Koch C, Eisele L, Beier F, Ziegler P, et al. Aging of blood can be tracked by DNA methylation changes at just three CpG sites. Genome biology. 2014. doi:10.1186/gb-2014-15-2-r24.
BibTeX
@article{carola2014Agingo,
title = {Aging of blood can be tracked by DNA methylation changes at just three CpG sites},
author = {Carola I. Weidner and Qiong Lin and Carmen Koch and Lewin Eisele and Fabian Beier and Patrick Ziegler and Dirk Bauerschlag and Karl‐Heinz Jöckel and Raimund Erbel and Thomas W. Mühleisen and Martin Zenke and Tim H. Brümmendorf and Wolfgang Wagner},
journal = {Genome biology},
year = {2014},
doi = {10.1186/gb-2014-15-2-r24},
}
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