Genetic and environmental causes of variation in epigenetic aging across the lifespan

S. Li; T.L. Nguyen; E.M. Wong; P-A Dugué; G.S. Dite; N.J. Armstrong; J.M. Craig; K.A. Mather; P.S. Sachdev; R. Saffery; J. Sung; Q. Tan; A. Thalamuthu; R.L. Milne; G.G. Giles; M.C. Southey; J.L. Hopper

doi:10.1186/s13148-020-00950-1

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Genetic and environmental causes of variation in epigenetic aging across the lifespan

Journal article

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Genetic and environmental causes of variation in epigenetic aging across the lifespan

S. Li, T.L. Nguyen, E.M. Wong, P-A Dugué, G.S. Dite, N.J. Armstrong, J.M. Craig, K.A. Mather, P.S. Sachdev, R. Saffery, …

Clinical Epigenetics, Vol.12(1), Art. 158

2020

DOI: https://doi.org/10.1186/s13148-020-00950-1

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Abstract

Background DNA methylation-based biological age (DNAm age) is an important biomarker for adult health. Studies in specific age ranges have found widely varying results about its genetic and environmental causes of variation. However, these studies are not able to provide a comprehensive view of the causes of variation over the lifespan. Results In order to investigate the genetic and environmental causes of DNAm age variation across the lifespan, we pooled genome-wide DNA methylation data for 4217 people aged 0–92 years from 1871 families. DNAm age was calculated using the Horvath epigenetic clock. We estimated familial correlations in DNAm age for monozygotic (MZ) twin, dizygotic (DZ) twin, sibling, parent–offspring, and spouse pairs by cohabitation status. Genetic and environmental variance components models were fitted and compared. We found that twin pair correlations were − 0.12 to 0.18 around birth, not different from zero (all P > 0.29). For all pairs of relatives, their correlations increased with time spent living together (all P < 0.02) at different rates (MZ > DZ and siblings > parent–offspring; P < 0.001) and decreased with time spent living apart (P = 0.02) at similar rates. These correlation patterns were best explained by cohabitation-dependent shared environmental factors, the effects of which were 1.41 (95% confidence interval [CI] 1.16 to 1.66) times greater for MZ pairs than for DZ and sibling pairs, and the latter were 2.03 (95% CI 1.13 to 9.47) times greater than for parent–offspring pairs. Genetic factors explained 13% (95% CI − 10 to 35%) of variation (P = 0.27). Similar results were found for another two epigenetic clocks, suggesting that our observations are robust to how DNAm age is measured. In addition, results for the other clocks were consistent with there also being a role for prenatal environmental factors in determining their variation. Conclusions Variation in DNAm age is mostly caused by environmental factors, including those shared to different extents by relatives while living together and whose effects persist into old age. The equal environment assumption of the classic twin study might not hold for epigenetic aging.

Details

Title: Genetic and environmental causes of variation in epigenetic aging across the lifespan
Authors/Creators: S. Li (Author/Creator) - University of Cambridge
T.L. Nguyen (Author/Creator) - The University of Melbourne
E.M. Wong (Author/Creator) - The University of Melbourne
P-A Dugué (Author/Creator) - Cancer Council Victoria
G.S. Dite (Author/Creator) - The University of Melbourne
N.J. Armstrong (Author/Creator) - Murdoch University
J.M. Craig (Author/Creator) - Deakin University
K.A. Mather (Author/Creator) - UNSW Sydney
P.S. Sachdev (Author/Creator) - UNSW Sydney
R. Saffery (Author/Creator) - Murdoch Children's Research Institute
J. Sung (Author/Creator) - Seoul National University
Q. Tan (Author/Creator) - University of Southern Denmark
A. Thalamuthu (Author/Creator) - UNSW Sydney
R.L. Milne (Author/Creator) - Cancer Council Victoria
G.G. Giles (Author/Creator) - Cancer Council Victoria
M.C. Southey (Author/Creator) - Cancer Council Victoria
J.L. Hopper (Author/Creator) - The University of Melbourne
Publication Details: Clinical Epigenetics, Vol.12(1), Art. 158
Publisher: BioMed Central
Identifiers: 991005542931907891
Copyright: © 2020 The Author(s).
Murdoch Affiliation: Information Technology, Mathematics and Statistics
Language: English
Resource Type: Journal article

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Collaboration types: Domestic collaboration; International collaboration
Citation topics: 1 Clinical & Life Sciences; 1.54 Molecular & Cell Biology - Genetics; 1.54.100 Epigenetic Regulation
Web Of Science research areas: Genetics & Heredity; Oncology
ESI research areas: Clinical Medicine