Epigenetic influences on aging: a longitudinal genome-wide methylation study in old Swedish twins

Wang, Yunzhang; Karlsson, Robert; Lampa, Erik; Zhang, Qian; Hedman, Åsa K.; Almgren, Malin; Almqvist, Catarina; McRae, Allan F.; Marioni, Riccardo E.; Ingelsson, Erik; Visscher, Peter M.; Deary, Ian J.; Lind, Lars; Morris, Tiffany; Beck, Stephan; Pedersen, Nancy L.; Hägg, Sara

doi:10.1080/15592294.2018.1526028

Cited by 72 publications

(54 citation statements)

References 37 publications

(59 reference statements)

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“…Furthermore, EML was negatively correlated with CD4+ T cells (meta r = -0.121, meta P-value = 4.24E-22), plasmablasts (meta r = -0.085, meta P-value = 1.14E-11), and granulocytes (meta r = -0.064, meta P-value = 3.70E-07), but positively with exhausted CD8+ (defined as CD8+CD28-CD45RA-) T cells. These results are consistent with known age-related changes in blood cell composition [ 34 , 35 ].…”

Section: Resultssupporting

confidence: 92%

Epigenetic mutation load is weakly correlated with epigenetic age acceleration

Paul

et al. 2020

Aging

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DNA methylation (DNAm) age estimators are widely used to study aging-related conditions. It is not yet known whether DNAm age is associated with the accumulation of stochastic epigenetic mutations (SEMs), which reflect dysfunctions of the epigenetic maintenance system. Here, we defined epigenetic mutation load (EML) as the total number of SEMs per individual. We assessed associations between EML and DNAm age acceleration estimators using biweight midcorrelations in four population-based studies (total n = 6,388). EML was not only positively associated with chronological age (meta r = 0.171), but also with four measures of epigenetic age acceleration: the Horvath pan tissue clock, intrinsic epigenetic age acceleration, the Hannum clock, and the GrimAge clock (meta-analysis correlation ranging from r = 0.109 to 0.179). We further conducted pathway enrichment analyses for each participant’s SEMs. The enrichment result demonstrated the stochasticity of epigenetic mutations, meanwhile implicated several pathways: signaling, neurogenesis, neurotransmitter, glucocorticoid, and circadian rhythm pathways may contribute to faster DNAm age acceleration. Finally, investigating genomic-region specific EML, we found that EMLs located within regions of transcriptional repression (TSS1500, TSS200, and 1stExon) were associated with faster age acceleration. Overall, our findings suggest a role for the accumulation of epigenetic mutations in the aging process.

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Section: Resultssupporting

confidence: 92%

Epigenetic mutation load is weakly correlated with epigenetic age acceleration

Paul

et al. 2020

Aging

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“…Meanwhile, the same type of study design is now seen for projects in epigenetics, where population-based cohorts with similar genome-wide DNA methylation data join forces to identify methylation marks associated with a trait of interest. Aging studies on the epigenome have been far more successful; thousands of DNA methylation changes have been associated with the aging process in humans and validated across different cohorts [63][64][65]. Another type of study using recent GWAS findings within genetic and molecular epidemiology is the application of Mendelian randomizations to assess causal associations in aging.…”

Section: New Developments In Molecular Epidemiology Of Agingmentioning

confidence: 99%

Developments in molecular epidemiology of aging

Hägg

Belsky

Cohen

2019

Emerging Topics in Life Sciences

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The field of molecular epidemiology of aging involves the application of molecular methods to measure aging processes and their genetic determinants in human cohorts. Over the last decade, the field has undergone rapid progress with a dramatic increase in the number of papers published. The aim of this review is to give an overview of the research field, with a specific focus on new developments, opportunities, and challenges.Aging occurs at multiple hierarchical levels. There is increasing consensus that agingrelated changes at the molecular level cause declines in physiological integrity, functional capacity, and ultimately lifespan. Molecular epidemiology studies seek to quantify this process. Telomere length, composite scores integrating clinical biomarkers, and omics clocks are among the most well-studied metrics in molecular epidemiology studies.New developments in the field include bigger data and hypothesis-free analysis together with new modes of collaborations in interdisciplinary teams and open access norms around data sharing. Key challenges facing the field are the lack of a gold standard by which to evaluate molecular measures of aging, inconsistency in which metrics of aging are measured and analyzed across studies, and a need for more longitudinal data necessary to observe change over time.

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“…This notion proposes an increased rate of stochastic methylation errors across the entire genome during aging. Indeed, several reports provided compelling evidence that older monozygotic twins exhibit global differences in DNA methylation (DNAm) patterns when compared to their younger counterparts (Fraga et al, 2005;Lévesque et al, 2014;Tan et al, 2016;Wang et al, 2018). Similarly, a centenarian's methylome displays reduced DNA methylation levels as well as a decreased pair-wise correlation in the methylation status of neighboring CpG sites relative to the methylome of a newborn (Heyn et al, 2012).…”

Section: Introductionmentioning

confidence: 99%

DNA Methylation Biomarkers in Aging and Age-Related Diseases

2020

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Recent research efforts provided compelling evidence of genome-wide DNA methylation alterations in aging and age-related disease. It is currently well established that DNA methylation biomarkers can determine biological age of any tissue across the entire human lifespan, even during development. There is growing evidence suggesting epigenetic age acceleration to be strongly linked to common diseases or occurring in response to various environmental factors. DNA methylation based clocks are proposed as biomarkers of early disease risk as well as predictors of life expectancy and mortality. In this review, we will summarize key advances in epigenetic clocks and their potential application in precision health. We will also provide an overview of progresses in epigenetic biomarker discovery in Alzheimer's, type 2 diabetes, and cardiovascular disease. Furthermore, we will highlight the importance of prospective study designs to identify and confirm epigenetic biomarkers of disease.

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Epigenetic influences on aging: a longitudinal genome-wide methylation study in old Swedish twins

Cited by 72 publications

References 37 publications

Epigenetic mutation load is weakly correlated with epigenetic age acceleration

Epigenetic mutation load is weakly correlated with epigenetic age acceleration

Developments in molecular epidemiology of aging

DNA Methylation Biomarkers in Aging and Age-Related Diseases

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