An epigenome-wide association study of sex-specific chronological ageing

McCartney, Daniel L.; Zhang, Futao; Hillary, Robert F.; Zhang, Qian; Stevenson, Anna J.; Walker, Rosie M.; Bermingham, Mairead Lesley; Boutin, Thibaud; Morris, Stewart W.; Campbell, Archie; Murray, Alison; Whalley, Heather C.; Porteous, David J.; Hayward, Caroline; Evans, Kathryn; Chandra, Tamir; Deary, Ian J.; McIntosh, Andrew M.; Yang, Jian; Visscher, Peter M.; McRae, Allan F.; Marioni, Riccardo E.

doi:10.1186/s13073-019-0693-z

Cited by 82 publications

(93 citation statements)

References 51 publications

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“…Finally, we searched for those probes displaying different DNA methylation trajectories in males and females during aging. We identified 8 probes having age-by-sex interaction, 2 of which were recently reported by McCartney et al in an independent dataset [32]. In particular we found that FIGN gene, which encodes for an ATP-dependent microtubule severing enzyme which catalyzes internal breaks in microtubules, included both probes from the saDMPs list and displaying age-by-sex interactions.…”

Section: I) Sadmps In Healthy Subjects Of Different Ages and Populatisupporting

confidence: 61%

“…Meta-analysis resulted in 8 CpG probes whose methylation showed different aging trajectories according to sex (Supplementary File 4). Two of these CpG sites were previously identified as having age-by-sex interaction in whole blood [32], and the most significant CpG site (cg18834375) mapped within FIGN gene, that was the top ranker also in the list of saDMPs and included multiple CpG sites showing sex-and age-dependent methylation (cg01620164, cg19156483, cg10864319, cg18834375, cg15259986 and cg03878133).…”

Section: Identification Of Sex-and Age-associated Differentially Methmentioning

confidence: 99%

“…Furthermore, although some ancestries are included, many are missing, and the study of additional populations will be necessary to distinguish the effects of sex and gender in shaping age-related methylation changes. Finally, similarly to [22], our study includes only autosomal probes (after the removal of crossreactive probes), while recently McCartney et al found that many of the probes with a sex by age interaction are on the X chromosome [32].…”

Section: Strengths and Limitationsmentioning

confidence: 99%

“…Our results are compared with the only study that, to the best of our knowledge, recently investigated normative age-by-sex DNA methylation differences in whole blood of a single population, i.e. a large Scottish cohort [32].…”

Section: Introductionmentioning

confidence: 99%

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Age-related DNA methylation changes are sex-specific: a comprehensive assessment

Yusipov

Bacalini

Kalyakulina

et al. 2020

Preprint

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Current epidemiological data indicate that, in humans, females live longer than males but experience a worse quality of life in advanced age. The reasons for this sex disparity are still unknown, but it is likely that it derives from a strict interplay between biological and cultural factors. Epigenetic modifications likely contribute to shape sex gap in aging and longevity, and genome-wide DNA methylation differences between males and females in autosomal chromosomes have been reported. Several studies showed that DNA methylation patterns are profoundly remodelled during aging, modulated in part by environmental exposures. However, few studies have specifically investigated if DNA methylation is differently affected by aging in males and females. Here we performed a meta-analysis of 4 large whole blood datasets including males and females of different ages and we compared 4 aspects of epigenetic age-dependent remodelling between males and females: normative changes, variability, epimutations, and entropy. While we did not find differences in the ageassociated increase in epimutations and in entropy, we reported a list of highly reproducible sex-specific age-associated differentially methylated positions (saDMPs) and sex-specific age-associated variably methylated positions (saVMPs). We investigated the enrichment in saDMPs and saVMPs in genomic regions, imprinted and sex hormone-related genes and Reactome pathways. Furthermore, we experimentally validated the most robust saDMPs, mapping in FIGN and PRR4 genes, and showed sex-specific deviations of their methylation patterns in models of successful (centenarians) and unsuccessful (Down syndrome) aging.In conclusion, we provided a comprehensive description of sex-differences in DNA methylation changes with aging in whole blood. Our results can pave the way to the identification of possible molecular triggers of the sex gap in aging and longevity. DNA methylation profiles tend to diverge among individuals during life course [4][5][6], shaped by an intricated combination of environmental exposures, random events and genetically-driven mechanisms. At the same time, several epigenome-wide association studies (EWAS) have shown that a subset of the about 28 million CpG sites of the genome undergoes age-associated normative changes, i.e. reproducible hypermethylation or hypomethylation events that characterize aging individuals [7,8]. Despite some controversial results [9,10], at least a fraction of normative changes is tissue specific, indicating that the cellular microenvironment affects the activity of the molecular writers of DNA methylation patterns during aging. The number of studies identifying age-associated DNA methylation changes at the level of single CpG sites has exponentially increased in the last 10 years, paving the way for the development of mathematical models, termed "epigenetic clocks", that predict the age of an individual on the basis of his/her epigenetic profile [11]. Epigenetic clocks are an appealing resource for chronological age estimation in ...

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Section: I) Sadmps In Healthy Subjects Of Different Ages and Populatisupporting

confidence: 61%

Section: Identification Of Sex-and Age-associated Differentially Methmentioning

confidence: 99%

Section: Strengths and Limitationsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Age-related DNA methylation changes are sex-specific: a comprehensive assessment

Yusipov

Bacalini

Kalyakulina

et al. 2020

Preprint

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“…The IEAA-associated locus on chromosome 3 (lead SNP rs1047210) colocalized with an eQTL for TRIM59. DNA methylation levels at TRIM59 have been robustly associated with chronological age and its expression has been noted in multiple cancers [53,54,55,56,57].…”

Section: Mendelian Randomisation Between Age Acceleration Phenotypes mentioning

confidence: 99%

Genome-wide association studies identify 137 loci for DNA methylation biomarkers of ageing

McCartney¹,

Min²,

Richmond³

et al. 2020

Preprint

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AbstractBiological ageing estimators derived from DNA methylation (DNAm) data are heritable and correlate with morbidity and mortality. Leveraging DNAm and SNP data from >41,000 individuals, we identify 137 genome-wide significant loci (113 novel) from meta-analyses of four epigenetic clocks and epigenetic surrogate markers for granulocyte proportions and plasminogen activator inhibitor 1 levels, respectively. We report strong genetic correlations with longevity and lifestyle factors such as smoking, education, and obesity. Significant associations are observed in polygenic risk score analysis and to a lesser extent in Mendelian randomization analyses. This study illuminates the genetic architecture underlying epigenetic ageing and its shared genetic contributions with lifestyle factors and longevity.

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Genome‐wide identification of age‐related CpG sites for age estimation from blood DNA of Han Chinese individuals

Xiao

Huang

2021

Electrophoresis

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Age‐related CpG (AR‐CpG) sites are currently the most promising molecular markers for forensic age estimation. However, the AR‐CpG sites of Han Chinese population remains to be systematically characterized. In this study, we performed genome‐wide methylation analyses on 42 whole blood DNA from healthy Han Chinese volunteers (aged from 18 to 62 years) using the Illumina MethylationEPIC BeadChip microarray. As expected, both known and novel AR‐CpG sites were identified. Considering the sex difference in aging rate, we then separately selected AR‐CpG candidates and built pyrosequencing‐based multiple linear regression models for age estimation of males and females. The model constructed from the male sample group (n = 167, aged from 1.50 to 85.71 years) explained 95.22% of variation in age using five AR‐CpG sites (chr6:11044864 ELOVL2, chr1:207997068 C1orf132, cg19283806 CCDC102B, cg17740900, and chr10:73740306 CHST3) and yielded a mean absolute error (MAE) of 2.79 years. The model constructed from the female sample group (n = 141, aged from 3.33 to 80.38 years) explained 94.90% of variation in age with six AR‐CpG sites (chr6:11044867 ELOVL2, chr1:207997060 C1orf132, chr2:106015757 FHL2, cg26947034, chr16: 67184108 B3GNT9, and chr20:44658203 SLC12A5) and yielded an MAE of 2.53 years. Besides, the estimated age was highly correlated with the actual age (R > 0.97). The robustness of these AR‐CpG markers was demonstrated by 10‐fold cross‐validations. In conclusion, we updated the AR‐CpG sites of Han Chinese population and provided two sets of AR‐CpG sites for accurate age estimation.

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An epigenome-wide association study of sex-specific chronological ageing

Cited by 82 publications

References 51 publications

Age-related DNA methylation changes are sex-specific: a comprehensive assessment

Age-related DNA methylation changes are sex-specific: a comprehensive assessment

Genome-wide association studies identify 137 loci for DNA methylation biomarkers of ageing

Genome‐wide identification of age‐related CpG sites for age estimation from blood DNA of Han Chinese individuals

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