Aging of blood can be tracked by DNA methylation changes at just three CpG sites

We combined 575 DNAm profiles derived from blood cells from four different studies spanning an age range of 0 to 78 years (Table S1 in Additional file 1) [15,16,22,23]. All of these DNAm profiles were generated with the HumanMethylation27 BeadChip platform, which covers 27,578 individual CpG sites [24]. AR-CpGs with linear DNAm changes during aging were selected by Pearson correlation (either r > 0.85 or r < −0.85): 102 CpG sites passed these stringent parameters, including 58 hypomethylated and 44 hypermethylated CpGs (Figure 1a; Additional file 2).

In particular, the hypomethylated AR-CpGs were associated with genes involved in 'hematopoietic regulation', indicating that these age-related DNAm (AR-DNAm) changes reveal some tissue specificity (Table S3 in Additional file 1). Hypermethylated AR-CpGs were enriched within GC-rich sequences (Figure S1a in Additional file 1) [13]. Predicted transcription factor binding sites within 1 kb up- and downstream of AR-CpG sites differed considerably for hypo- and hypermethylated loci (Figure S1b in Additional file 1). Furthermore, only hypermethylated CpGs were significantly enriched in regions with bivalent histone modifications in embryonic stem cells (ESCs) and the H3K27me3 (trimethylation of lysine 27 of histone 3) marker in monocytes and mononuclear cells (Figure S2 in Additional file 1) [25,26], which has also been described before [15]. Overall, age-associated hypermethylation occurred particularly in regions with low DNAm levels, whereas age-related hypomethylation occurred at highly methylated regions. This trend towards a moderate methylation level has recently been described by other authors and may support the notion that many AR-DNAm changes are due to epigenetic drift evoked by increasing entropy of CpG markers, which tends towards 50% (Figure S3 in Additional file 1) [19,27]. Either way, the underlying mechanism resulting in AR-DNAm changes at specific genomic regions seems to differ for hypo- and hyper-methylated CpGs.

We trained a multivariate linear model to predict donor age based on the 102 AR-CpG sites selected by Pearson correlation. The results correlated well with chronological age with a mean absolute deviation (MAD) from chronological age of only 3.34 years (root mean square error (RMSE) = 4.26 years; R² = 0.98; Figure 1b). These AR-CpG sites were further validated in three other publicly available datasets derived from blood samples [28-30] using the same multivariate linear model: the MAD from chronological age in these datasets was only slightly higher (GSE49904↗, 5.79 years; GSE41037↗, 5.52 years; GSE37008↗, 4.02 years; Figure S4a in Additional file 1). Furthermore, we considered the recently published dataset by Hannum and co-workers [19] of 656 DNAm profiles derived from blood samples (from donors aged 19 to 101 years). This dataset has been analyzed on the HumanMethylation450 BeadChip, which assays 485,577 CpG sites, including 99 of the 102 AR-CpG sites [31]. When we applied our multivariate linear model to this dataset, there was a clear correlation between age prediction and chronological age (R² = 0.71). However, the linear offset indicated a systematic bias that might be due to the three missing CpG sites or to the different assay design of the two microarray platforms [31]. Therefore, we adjusted the multivariate regression model to facilitate age predictions based on these 99 AR-CpG sites, similar to the above-mentioned model (MAD, 4.12 years; RMSE, 5.34 years; R² = 0.87; Figure S4b,c in Additional file 1).

We have recently demonstrated that senescence-associated DNAm changes - which accumulate during long-term culture of cells in vitro - can be reversed by reprogramming into induced pluripotent stem cells (iPSCs) [32,33]. Here, we analyzed if AR-DNAm changes are also reversed in this dataset upon reprogramming: although our aging model had been trained on freshly isolated blood samples, it enabled moderate estimations of age in culture-expanded mesenchymal stromal cells as well. Notably, AR-DNAm changes were hardly affected by replicative senescence during culture expansion in vitro, indicating that AR-DNAm changes are not identical to DNAm changes acquired during in vitro culture (Figure 1c). Interestingly, CpG sites that are hypermethylated during aging are hypomethylated in pluripotent cells and vice versa. Using our multivariate model, the ESCs and iPSCs were even predicted to be of negative age (Figure 1d), which may reflect the reversal beyond the new-born state to the embryonic cell state. However, when we applied our multivariate model to a dataset with 19 undifferentiated human ESC lines and 5 iPSC lines (GSE34869↗) [34], they were predicted to have a mean donor age of −0.06 and 5.20 years, respectively (Figure S5 in Additional file 1). Thus, the deviation of ESCs and especially of iPSCs from zero might also be due to culture conditions or the comparison between different datasets. Either way, the data clearly indicate that AR-DNAm changes are, overall, reversed upon reprogramming. These findings fit nicely with other recent observations that iPSCs generated from senescent cells or centenarian donors reset telomere length, gene expression profiles, and other physiological features to those of young cells [35,36]. In addition, our results indicate that iPSCs are rejuvenated also on the epigenetic level.

Analysis of DNAm in a small subset of AR-CpGs might be sufficient for robust age predictions. Restriction to the most relevant CpGs would facilitate site-specific analysis of DNAm instead of profiling approaches. Therefore, we searched for subsets of AR-CpGs that, when combined, yield the best age predictions. AR-CpGs with the highest variation in DNAm levels were used for recursive feature elimination to select subsets of five CpG sites for testing in multivariate linear regression models. Predictions for each of these subsets were made by iterative divisions of the dataset into training and test sets (split ratios; Figure 2a). For further analysis we considered only those subsets of five CpGs that performed better than the average of models based on all 51 AR-CpG sites (Figure S6 in Additional file 1). Five specific CpGs occurred in more than 50% of the remaining subsets, indicating that they complement each other for age prediction (Figure 2b). These CpG sites are associated with EDAR-associated death domain (EDARADD), which has been associated with AR-DNAm changes before [20]; integrin, alpha 2b (ITGA2B); RAB36, a member of the RAS oncogene family (RAB36); phosphodiesterase 4C, cAMP specific (PDE4C); and aspartoacylase (ASPA) (Figure S7 in Additional file 1). Nevertheless, gene expression profiles indicated that expression of the five corresponding genes is hardly affected by aging (Figure S8 in Additional file 1) [37].

DNAm at these CpG sites was subsequently analyzed by pyrosequencing after bisulfite conversion in an independent training set derived from 82 blood samples. The sequences in the vicinity of cg09809672 (EDARADD) and cg15379633 (RAB36) were not ideal for the primer design and therefore we focused on the remaining three AR-CpGs. As expected, we observed a clear age-associated correlation for each of the three CpGs. In fact, the upstream located CpG site cg17861230 (PDE4C), which was covered by the same pyrosequencing assay, revealed an even better age-association and was therefore considered instead (Figure 2c,d). A multivariate linear regression model based on these pyrosequencing results facilitated age predictions with a MAD from chronological age of 5.4 years (RMSE, 7.2 years; Figure 2e). The corresponding equation is provided in the Material and methods section. To further simplify application of the epigenetic aging signature, we have compiled an online calculator that implements this equation [38].

Subsequently, we used this method on an independent validation set derived from 69 blood samples; this validation set was analyzed two months after the training set. DNAm levels at the three relevant CpGs were integrated into the above mentioned linear regression model established with the training set. Notably, the predictions for the validation set correlated even better with chronological age (MAD, 4.5 years; RMSE, 5.6 years; Figure 2f), indicating that pyrosequencing of these three CpG sites enables reliable age prediction.

Our epigenetic age predictions might also be influenced by differences in the cellular composition in blood that result from aging [30]. Between the second and seventh decade a moderate decline in lymphocytes [39] and erythrocytes [40] has been described. When we analyzed DNAm of the three relevant CpG sites (cg02228185 in ASPA, cg25809905 in ITGA2B, and cg17861230 in PDE4C) in a publicly available dataset of cell type-specific DNAm profiles [41] the results indicated that the age predictions made using our epigenetic aging signature were not evoked by myeloid skewing (Figure S9a in Additional file 1). Furthermore, we made age predictions based on the three AR-CpGs using publicly available DNAm profiles of fractionated monocytes (CD14), T cells (CD4), granulocytes (CD16), and hematopoietic stem and progenitor cells (CD34) (GSE20242↗; E-MTAB-487) [15,42]. The results demonstrated that age predictions were feasible in purified cell populations, even though the MAD from chronological age was higher (Figure S9b in Additional file 1). Alternatively, we used another dataset to determine if the percentage of monocytes, lymphocytes, neutrophils, basophils, or eosinophils correlates with predicted age and there were no clear associations (GSE37008↗; Figure S10 in Additional file 1) [30]. These results indicate that AR-DNAm changes are due to intrinsic DNAm changes rather than to changes in cellular composition.

In an exploratory analysis to determine whether deviation of predicted age and chronological age correlated with other co-variables - such as clinical or lifestyle parameters - we focused on the 105 samples from the population-based prospective Heinz Nixdorf Recall (HNR) study [43]. Generally, age was estimated to be higher in men and in obese people (body mass index >30). These trends are in line with previous studies demonstrating an association with telomere length [44-46], but our results were not significant, which may be explained by the relatively small sample size (Figure S11 in Additional file 1). High alcohol consumption was also associated with overestimation of age (0.091 ± 0.045 years deviation per gram alcohol consumed per day; P = 0.049). Notably, age was increasingly underestimated according to increasing number of children in women (categories, 0, 1, 2, ≥3 children; -2.52 ± 0.84 years deviation per category; P = 0.0043), which has been associated with a longer lifespan before (Figure 3) [47].

Telomere length is well known to decline during aging - an average of 39 bp per year in granulocytes [48] - and this approach can also be used to estimate donor age. We analyzed telomere length in 104 blood samples (from donors aged 18 to 84 years) by flow-FISH. Despite a clear inverse correlation between telomere length and chronological age, the precision of age predictions based on telomere length was relatively low (MAD, 18.2 years; RMSE, 23.1 years; Figure 4a; Figure S12a in Additional file 1). Extremely shortened telomeres have been reported in severe acquired aplastic anemia (AA) and patients with dyskeratosis congenita (DKC), both of which are associated with progressive bone marrow failure syndromes. Telomere attrition in these patients might result either from increased hematopoietic cell turnover due to autoimmune-mediated depletion of the hematopoietic stem cell pool, or, particularly in DKC, due to direct functional impairment of the telomerase complex by inactivating mutations [49,50]. We analyzed blood from 15 AA and 5 DKC patients, which revealed significantly shorter telomeres than healthy controls (Figure S12b in Additional file 1). Notably, these samples were predicted to be significantly older than their chronological age using our epigenetic aging signature, which may reflect replicative exhaustion of the hematopoietic stem cell pool (Figure 4b,c) [18,49].

We used blood samples from the HNR study, which is a prospective population-based cohort study (105 samples) [43,56] from the Department of Obstetrics and Gynecology of the University Hospital Aachen (GYN; 27 samples), and from the Department of Oncology, Hematology and Stem Cell Transplantation of the University Hospital Aachen (HEM; 104 samples from healthy donors, 15 AA, 5 DKC). All samples were taken after written consent and according to the guidelines of the local ethics committees.

We considered all DNAm profiles derived from blood samples that were generated with the HumanMethylation27 BeadChip platform and available at the time (Table S1 in Additional file 1). Beta values were combined and 102 AR-CpG sites were selected by Pearson correlation (r > 0.85 or r < −0.85). We trained a multivariate linear model for these AR-CpGs and applied leave-one-out cross-validation to estimate the model's performance. Age association of these CpGs was then tested using datasets GSE49904↗ [28], GSE41037↗ [29], GSE37008↗ [30], GSE34869↗ [34], and GSE20242↗ [15], and E-MTAB-487 [42]. We also used dataset GSE40279↗ [19], although this was generated with the HumanMethylation450 BeadChip (different assay design with type II bead type and only 99 of 102 AR-CpGs) [31] and we therefore trained an alternative model for use with this platform.

Nucleotide sequences around each AR-CpG were retrieved from the human NCBI36/hg18 assembly. The frequency of nucleotides in the flanking regions was determined for 10 up- and downstream positions. FIMO (Find Individual Motif Occurrences) from the MEME Suite was utilized to scan for known transcription factor binding motifs within 1 kb flanking each CpG sites. The five most significantly enriched motifs in relation to all CpG sites on the array were depicted (P-values were estimated by Fisher’s exact test). The sequence logo plots were generated by the R seqLogo packages. Histone modifications at AR-CpG loci were analyzed using chromatin immunoprecipitation data for ESCs [25] (GSE8463↗ [26]; GSE29611↗, ENCODE project), CD14⁺ monocytes (GSE29611↗, ENCODE project), and MNCs (GSE31755↗, ENCODE project). Enrichment of H3K4me3, H3K27me3, the bivalent state or neither was estimated in relation to all CpG sites (Fisher’s exact test). Gene Ontology classification of genes associated with AR-CpGs was performed with GoMiner software [57] in relation to all CpGs on the BeadChip (Fisher’s exact test). For the five most important AR-CpGs, we analyzed gene expression data from the Leiden Longevity Study (150 samples; GSE16717↗) [37], which were generated with the 54 k CodeLink Human Whole Genome Bioarray. Methylation profiles of our top three AR-CpGs in subsets of different blood cells were analyzed using another dataset (GSE35069↗) [41].

To obtain a small set of AR-CpGs for age predictions based on locus-specific DNAm levels, we narrowed 102 AR-CpGs down to those with above median variations in beta values (above median level of interquartile ranges). The dataset was then randomly divided into training and validation sets by defined split ratios. Next we applied recursive feature elimination implemented in the R caret package [58] for a limited feature size of five CpGs using a linear model on the training set. Relevant CpG sites were then selected by their frequency in the best performing models (Figure S6 in Additional file 1). The five most relevant AR-CpGs were subsequently considered for locus-specific DNAm analysis by pyrosequencing. The sequences surrounding cg02228185 (ASPA), cg25809905 (ITGA2B), and cg17861230 (PDE4C) were best suited for this approach.

Genomic DNA was isolated from GYN samples with the QIAamp DNA Blood Midi Kit (QIAGEN, Hilden, Germany; GYN), from HEM samples with the DNeasy Mini Kit (QIAGEN), and from the HNR study samples using the Chemagic Magnetic Separation Module I (Chemagen, Baesweiler, Germany). Subsequently, 500 ng DNA were bisulfite-converted using the EpiTect Bisulfite Kit (QIAGEN). Converted DNA was amplified and 12 μl (ASPA, ITGA2B) or 20 to 25 μl (PDE4C) of PCR product was immobilized to 2 μl Streptavidin Sepharose™ HP beads (GE Healthcare, Piscataway, NJ, USA) followed by annealing to 1.0 μl sequencing primer (5 μM) for 2 minutes at 80°C. Primers for pyrosequencing analysis are listed in Table S4 in Additional file 1. Analysis was performed with PyroMark Q24 software. Initially, pyrosequencing was performed for 82 blood samples (27 GYN and 55 HNR) at Varionostic GmbH (Ulm, Germany); these samples were entirely independent from the DNAm profiles that were used to identify the three genomic locations. Based on the pyrosequencing results of the initial 82 blood samples, we generated the multivariate model. Beta values at the following three CpGs were used for age-prediction: (α) = cg02228185; (β) = cg25809905, and (γ) = a CpG site upstream of cg17861230 that revealed better correlation with age (Figure 2c).

This equation resembles also the underlying source code for the freely available online calculator [38]. This simple model was subsequently validated with an independent set of 69 samples (19 HEM and 50 HNR).

To estimate the impact of co-variables (for example, lifestyle or clinical parameters), we calculated univariate linear regression models using the deviation of predicted age and chronological age as dependent variable and the respective co-variable as independent variable (SAS, version 9.2, Cary, New Jersey, USA). Similar models were computed separately for males and females to assess gender differences. Some 52 male and 53 female donors from different age categories (intervals of 6 years per age category) were selected randomly from the HNR study (4,814 participants) [56]. Box-and-whisker plots (10 to 90 percentiles) were plotted with GraphPad Prism 5 (GraphPad Software, La Jolla, CA, USA). Statistical significance was assessed from statistical significance of parameter estimates of the linear regression model depicting the change in deviation per one unit increase in the corresponding co-variable.

Telomere length of granulocytes and lymphocytes was analyzed in 104 samples from healthy donors aged 18 to 84 years, 15 patients with AA, and 5 with DKC (all HEM) by flow-FISH as described before [59,60]. In brief, samples were analyzed in triplicates with and without FITC-(C3TA2)₃ PNA or Alexa488-(C3TA2) PNA (for healthy controls or AA and DKC, respectively; Panagene, Daejeon, South Korea). Cow thymocytes with known telomere length were used as an internal control to calculate telomere length in kilobases. The cow thymocytes as well as granulocytes and lymphocytes from human samples were identified based on forward scatter and LDS 751 binding to double-stranded DNA. For flow-FISH, telomere length was determined in absolute values. Age-related telomere length was estimated by linear regression on the 104 blood samples from healthy donors.