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An epigenetic biomarker of aging for lifespan and healthspan

Authors :
Morgan E. Levine
Abraham Aviv
James D. Stewart
Yongmei Liu
Kurt Lohman
Andrea A. Baccarelli
Steve Horvath
Austin Quach
Alex P. Reiner
Lifang Hou
Themistocles L. Assimes
Stefania Bandinelli
Ake T. Lu
Yun Li
Brian H. Chen
James G. Wilson
Luigi Ferrucci
Eric A. Whitsel
Source :
Aging (Albany NY)
Publication Year :
2018
Publisher :
Impact Journals, LLC, 2018.

Abstract

Identifying reliable biomarkers of aging is a major goal in geroscience. While the first generation of epigenetic biomarkers of aging were developed using chronological age as a surrogate for biological age, we hypothesized that incorporation of composite clinical measures of phenotypic age that capture differences in lifespan and healthspan may identify novel CpGs and facilitate the development of a more powerful epigenetic biomarker of aging. Using a innovative two-step process, we develop a new epigenetic biomarker of aging, DNAm PhenoAge, that strongly outperforms previous measures in regards to predictions for a variety of aging outcomes, including all-cause mortality, cancers, healthspan, physical functioning, and Alzheimer’s disease. While this biomarker was developed using data from whole blood, it correlates strongly with age in every tissue and cell tested. Based on an in-depth transcriptional analysis in sorted cells, we find that increased epigenetic, relative to chronological age, is associated increased activation of pro-inflammatory and interferon pathways, and decreased activation of transcriptional/translational machinery, DNA damage response, and mitochondrial signatures. Overall, this single epigenetic biomarker of aging is able to capture risks for an array of diverse outcomes across multiple tissues and cells, and provide insight into important pathways in aging.

Details

ISSN :
19454589
Volume :
10
Database :
OpenAIRE
Journal :
Aging
Accession number :
edsair.doi.dedup.....dcd3927bd4361bc689a918c42efcce49
Full Text :
https://doi.org/10.18632/aging.101414