Impact of excessive alcohol abuse on age prediction using the VISAGE enhanced tool for epigenetic age estimation in blood

AbstractDNA methylation-based clocks provide the most accurate age estimates with practical implications for clinical and forensic genetics. However, the effects of external factors that may influence the estimates are poorly studied. Here, we evaluated the effect of alcohol consumption on epigenetic age prediction in a cohort of extreme alcohol abusers. Blood samples from deceased alcohol abusers and age- and sex-matched controls were analyzed using the VISAGE enhanced tool for age prediction from somatic tissues that enables examination of 44 CpGs within eight age markers. Significantly altered DNA methylation was recorded for alcohol abusers in MIR29B2CHG. This resulted in a mean predicted age of 1.4 years higher compared to the controls and this trend increased in older individuals. The association of alcohol abuse with epigenetic age acceleration, as determined by the prediction analysis performed based on MIR29B2CHG, was small but significant (β = 0.190; P-value = 0.007). However, the observed alteration in DNA methylation of MIR29B2CHG had a non-significant effect on age estimation with the VISAGE age prediction model. The mean absolute error in the alcohol-abusing cohort was 3.1 years, compared to 3.3 years in the control group. At the same time, upregulation of MIR29B2CHG expression may have a biological function, which merits further studies.

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Age prediction in living: Forensic epigenetic age estimation based on blood samples

Legal Medicine ◽

10.1016/j.legalmed.2020.101763 ◽

2020 ◽

Vol 47 ◽

pp. 101763

Author(s):

Helena Correia Dias ◽

Eugénia Cunha ◽

Francisco Corte Real ◽

Licínio Manco

Keyword(s):

Age Estimation ◽

Blood Samples ◽

Epigenetic Age ◽

Age Prediction

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Evidence for differences in DNA methylation between Germans and Japanese

International Journal of Legal Medicine ◽

10.1007/s00414-021-02736-3 ◽

2021 ◽

Author(s):

J. Becker ◽

P. Böhme ◽

A. Reckert ◽

S. B. Eickhoff ◽

B. E. Koop ◽

...

Keyword(s):

Dna Methylation ◽

Age Estimation ◽

Prediction Models ◽

Total Sample ◽

Training Data ◽

Research Strategies ◽

Different Populations ◽

The Impact ◽

Age Prediction

AbstractAs a contribution to the discussion about the possible effects of ethnicity/ancestry on age estimation based on DNA methylation (DNAm) patterns, we directly compared age-associated DNAm in German and Japanese donors in one laboratory under identical conditions. DNAm was analyzed by pyrosequencing for 22 CpG sites (CpGs) in the genes PDE4C, RPA2, ELOVL2, DDO, and EDARADD in buccal mucosa samples from German and Japanese donors (N = 368 and N = 89, respectively).Twenty of these CpGs revealed a very high correlation with age and were subsequently tested for differences between German and Japanese donors aged between 10 and 65 years (N = 287 and N = 83, respectively). ANCOVA was performed by testing the Japanese samples against age- and sex-matched German subsamples (N = 83 each; extracted 500 times from the German total sample). The median p values suggest a strong evidence for significant differences (p < 0.05) at least for two CpGs (EDARADD, CpG 2, and PDE4C, CpG 2) and no differences for 11 CpGs (p > 0.3).Age prediction models based on DNAm data from all 20 CpGs from German training data did not reveal relevant differences between the Japanese test samples and German subsamples. Obviously, the high number of included “robust CpGs” prevented relevant effects of differences in DNAm at two CpGs.Nevertheless, the presented data demonstrates the need for further research regarding the impact of confounding factors on DNAm in the context of ethnicity/ancestry to ensure a high quality of age estimation. One approach may be the search for “robust” CpG markers—which requires the targeted investigation of different populations, at best by collaborative research with coordinated research strategies.

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The combined effect of obesity and aging on human sperm DNA methylation signatures: inclusion of BMI in the paternal germ line age prediction model

Scientific Reports ◽

10.1038/s41598-020-71979-8 ◽

2020 ◽

Vol 10 (1) ◽

Author(s):

Albert Salas-Huetos ◽

Emma R. James ◽

Dallin S. Broberg ◽

Kenneth I. Aston ◽

Douglas T. Carrell ◽

...

Keyword(s):

Dna Methylation ◽

Germ Line ◽

Age Groups ◽

Human Sperm ◽

Absolute Error ◽

Epigenetic Aging ◽

Epigenetic Age ◽

Sperm Dna ◽

Epigenetic Age Acceleration ◽

The Impact

Abstract Male aging and obesity have both been shown to contribute to declines in fertility in men. Recent work in aging has shown consistent epigenetic changes to sperm as a man ages. In fact, our lab has built a tool that utilizes DNA methylation signatures from sperm to effectively predict an individual’s age. Herein, we performed this preliminary cohort study to determine if increased BMI accelerates the epigenetic aging in sperm. A total of 96 participants were divided into four age groups (22–24, 30, 40–41, and > 48 years of age) and additionally parsed into two BMI sub-categories (normal and high/obese). We found no statistically significant epigenetic age acceleration. However, it is important to note that within each age category, high BMI individuals were predicted to be older on average than their actual age (~ 1.4 years), which was not observed in the normal BMI group. To further investigate this, we re-trained a model using only the present data with and without BMI as a feature. We found a modest but non-significant improvement in prediction with BMI [r2 = 0.8814, mean absolute error (MAE) = 3.2913] compared to prediction without BMI (r2 = 0.8739, MAE = 3.3567). Future studies with higher numbers of age-matched individuals are needed to definitively understand the impact of BMI on epigenetic aging in sperm.

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Postmortem age estimation via DNA methylation analysis in buccal swabs from corpses in different stages of decomposition—a “proof of principle” study

International Journal of Legal Medicine ◽

10.1007/s00414-020-02360-7 ◽

2020 ◽

Vol 135 (1) ◽

pp. 167-173 ◽

Cited By ~ 1

Author(s):

Barbara Elisabeth Koop ◽

Felix Mayer ◽

Tanju Gündüz ◽

Jacqueline Blum ◽

Julia Becker ◽

...

Keyword(s):

Dna Methylation ◽

Age Estimation ◽

Buccal Swab ◽

Methylation Analysis ◽

Forensic Research ◽

Epigenetic Age ◽

Buccal Swabs ◽

Validation Set ◽

Methylation Patterns ◽

Dna Methylation Analysis

AbstractAge estimation based on the analysis of DNA methylation patterns has become a focus of forensic research within the past few years. However, there is little data available regarding postmortem DNA methylation analysis yet, and literature mainly encompasses analysis of blood from corpses without any signs of decomposition. It is not entirely clear yet which other types of specimen are suitable for postmortem epigenetic age estimation, and if advanced decomposition may affect methylation patterns of CpG sites. In living persons, buccal swabs are an easily accessible source of DNA for epigenetic age estimation. In this work, the applicability of this approach (buccal swabs as source of DNA) under different postmortem conditions was tested. Methylation levels of PDE4C were investigated in buccal swab samples collected from 73 corpses (0–90 years old; mean: 51.2) in different stages of decomposition. Moreover, buccal swab samples from 142 living individuals (0–89 years old; mean 41.2) were analysed. As expected, methylation levels exhibited a high correlation with age in living individuals (training set: r2 = 0.87, validation set: r2 = 0.85). This was also the case in postmortem samples (r2 = 0.90), independent of the state of decomposition. Only in advanced putrified cases with extremely low DNA amounts, epigenetic age estimation was not possible. In conclusion, buccal swabs are a suitable and easy to collect source for DNA methylation analysis as long as sufficient amounts of DNA are present.

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Novel epigenetic age estimation in wild-caught Gulf of Mexico reef fishes

Canadian Journal of Fisheries and Aquatic Sciences ◽

10.1139/cjfas-2021-0240 ◽

2021 ◽

Author(s):

D. Nick Weber ◽

Andrew T. Fields ◽

William F. Patterson ◽

Beverly K. Barnett ◽

Christopher M. Hollenbeck ◽

...

Keyword(s):

Dna Methylation ◽

Gulf Of Mexico ◽

Age Estimation ◽

Reef Fishes ◽

Lutjanus Campechanus ◽

Cpg Sites ◽

Epigenetic Aging ◽

Epigenetic Age ◽

Red Grouper ◽

Species Specific

Cutting-edge DNA methylation-based epigenetic aging techniques were applied to Gulf of Mexico northern red snapper (Lutjanus campechanus; n = 10; 1–26 years old) and red grouper (Epinephelus morio; n = 10; 2–14 years old). Bisulfite-converted restriction site-associated DNA sequencing was used to identify CpG sites (cytosines followed by guanines) that exhibit age-correlated DNA methylation, and species-specific epigenetic clocks developed from 100s of CpG sites in each species showed strong agreements between predicted and otolith-derived ages (r2 > 0.99 for both species). Results suggest epigenetic age estimation could provide an accurate and efficient approach to mass-aging fishes in a non-invasive manner.

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Comparison of the Axis %CDT TIA and the CDTect method as laboratory tests of alcohol abuse

Clinical Chemistry ◽

10.1093/clinchem/44.6.1209 ◽

1998 ◽

Vol 44 (6) ◽

pp. 1209-1215 ◽

Cited By ~ 31

Author(s):

Katja Viitala ◽

Kaija Lähdesmäki ◽

Onni Niemelä

Keyword(s):

Alcohol Abuse ◽

Problem Drinking ◽

Inverse Correlation ◽

High Serum ◽

Control Group ◽

Specific Marker ◽

Serum Transferrin ◽

Alcohol Abusers ◽

Significant Difference ◽

Carbohydrate Deficient Transferrin

Abstract Carbohydrate-deficient transferrin (CDT) has been suggested as a specific marker of alcohol abuse. We designed this study to compare the conventional CDTect method (Pharmacia & Upjohn) and the new semiautomated Axis %CDT turbidimetric immunoassay (%CDT TIA) for their diagnostic performance to identify problem drinking. The sensitivities of the %CDT TIA and CDTect for correctly classifying heavy drinkers (n = 90) were 29% and 59% with the thresholds currently recommended by the manufacturers, respectively. In the control group (n = 114), which included hospitalized patients with abnormal serum transferrin concentrations, the CDTect assay gave 21 false-positive values (18%), whereas the %CDT TIA showed 100% specificity. With the cutoff limits based on the present healthy control group (mean + 2 SD), the sensitivities of the %CDT TIA and CDTect were 61% and 86%, respectively. For men, the ROC plot area of the CDTect results in comparisons of alcohol abusers and healthy controls was significantly (P <0.05) higher than that of the %CDT TIA results, whereas for women, there was no significant difference in this respect. The slope and intercept (with 95% confidence intervals) for linear regression between CDTect and %CDT TIA were 0.13 (0.12–0.15) and 1.16 (0.73–1.59), respectively (Sy‖x = 1.51, r = 0.744). CDTect results correlated positively with serum transferrin (r = 0.224, P <0.001), whereas the %CDT TIA results showed a slight inverse correlation with serum transferrin (r = −0.132, P = 0.07). The data suggest that CDTect is more sensitive than %CDT TIA in detecting drinking problems. However, the %CDT TIA method yields more specificity when analyzing samples from patients with high serum transferrin concentrations.

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P4134Impaired left ventricular systolic function in alcohol abusers expressed by both 3D calculated ejection fraction and longitudinal strain by AFI

European Heart Journal ◽

10.1093/eurheartj/ehz745.0706 ◽

2019 ◽

Vol 40 (Supplement_1) ◽

Author(s):

P Hamala ◽

J D Kasprzak ◽

P Lipiec ◽

K Wierzbowska-Drabik

Keyword(s):

Alcohol Abuse ◽

Ejection Fraction ◽

Longitudinal Strain ◽

Systolic Function ◽

Global Longitudinal Strain ◽

Harmful Effect ◽

Left Ventricular ◽

Control Group ◽

Lv Function ◽

Alcohol Abusers

Abstract Aim Despite knowledge regarding the existence of alcohol cardiomyopathy the exact impact of alcohol abuse in consecutive subject is poorly examined. We aimed to evaluate the left ventricle (LV) function in chronic abusers group and compared classical and novel echocardiography parameters in alcohol abusers (ALC) and control group (C). Methods We compared 75 adults (mean age 48±12, 60 male) without other overt heart disease, coronary artery disease excluded, but with alcohol abuse history: average alcohol intake 32 alcohol unit per week (AUW) with control group consisted of 40 subjects without history of excessive drinking, abstinents or drinking ≤8 AUW (mean age 50±4, 16 men). One unit was defined as 10 grams of pure etanol. All patients underwent TTE examination including ejection fraction (EF) calculation with 3D and longitudinal strain assessment by AFI method. Results ALC group showed LV systolic dysfunction expressed as EF 48±14 vs 60±9%, global longitudinal strain (AFI GLS) −15.6±6.6 vs −18.7±3.4; p<0.0001 and p 0.0064, respectively. On the other hand the LV and left atrial diameters as well as diastolic function were similar in both groups, indicating on relatively low advancement of heart remodeling. ALC vs Control group comparison ALC N75 C N40 p value Age 48±12 50±4 ns BMI 24±6 28±6 0.0009 LVd 48±13 47±4 ns LVs 34±15 32±4 ns LA 38±9 38±3 ns EF 48±14 60±9 <0.0001 E/A 1.1±0.6 1.1±0.3 ns E' lateral 10.6±3.9 10.6±2.9 ns AFI 2ch −15.9±6.9 −18.8±4.8 0.0143 AFI 3ch −15.9±6.9 −18.9±3.6 0.0116 AFI 4ch −15.2±7.1 −18.6±3.5 0.0053 AFI GLS −15.6±6.6 −18.7±3.4 0.0064 Conclusions Chronic alcohol abuse revealed harmful effect on LV systolic function which can be assessed quantitatively by both decreased EF and absolute values of myocardial longitudinal strain. This systolic function impairment seems to anticipate the overt remodelling of the heart.

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Validating dental age estimation in Kenyan black children and adolescents using the Willems method

Medicine Science and the Law ◽

10.1177/0025802420977379 ◽

2020 ◽

pp. 002580242097737

Author(s):

Maria Cadenas de Llano-Pérula ◽

Eunice Kihara ◽

Patrick Thevissen ◽

Donna Nyamunga ◽

Steffen Fieuws ◽

...

Keyword(s):

Age Estimation ◽

Tooth Development ◽

Absolute Error ◽

Black Children ◽

Specific Model ◽

Permanent Teeth ◽

Estimation Model ◽

One Year ◽

Willems Method ◽

Age Prediction

Purpose This study aimed to validate the Willems Belgian Caucasian (Willems BC) age estimation model in a Kenyan sample, to develop and validate a Kenyan-specific (Willems KB) age estimation model and to compare the age prediction performances of both models. Methods Panoramic radiographs of 1038 (523 female, 515 male) Kenyan children without missing permanent teeth and without all permanent teeth fully developed (except third molars) were retrospectively selected. Tooth development of the seven lower-left permanent teeth was staged according to Demirjian et al. The Willems BC model, performed on a Belgian Caucasian sample and a constructed Kenyan-specific model (Willems KB) were validated on the Kenyan sample. Their age prediction performances were quantified and compared using the mean error (ME), mean absolute error (MAE) and root-mean-square error (RMSE). Results The ME with Willems BC method equalled zero. Hence, there was no systematic under- or overestimation of the age. For males and females separately, the ME with Willems BC was significantly different from zero, but negligible in magnitude (–0.04 and 0.04, respectively). Willems KB was found not to outperform Willems BC, since the MAE and RMSE were comparable (0.98 vs 0.97 and 1.31 vs 1.29, respectively). Although Willems BC resulted in a higher percentage of subjects with predicted age within a one-year difference of the true age (63.3% vs 60.4%, p=0.018), this cannot be considered as clinically relevant. Conclusion There is no reason to use a country-specific (Willems KB) model in children from Kenya instead of the original Willems (BC) model.

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Problem drinking in the Naval Service: A study of personnel identified as alcohol abusers

Journal of The Royal Naval Medical Service ◽

10.1136/jrnms-82-34 ◽

1996 ◽

Vol 82 (1) ◽

pp. 34-39

Author(s):

S Micklewright

Keyword(s):

Family History ◽

Alcohol Abuse ◽

Problem Drinking ◽

Alcohol Problems ◽

Disciplinary Action ◽

Control Group ◽

Age Group ◽

Length Of Service ◽

Alcohol Abusers ◽

History Of

AbstractA group of naval personnel referred for alcohol problems was studied for a number of characteristics including sex, service status, age group, Branch, presenting factors, where serving, referral source, marital status, length of service and family history of alcohol abuse. They were compared with a control group of othernaval personnel.The alcohol referral group displayed a number of statistically significant differences from the control group. Junior rates, those aged below 20, communications branch personnel and those serving at sea were over represented. The alcohol referrals group were also more likely to be unmarried or divorced, and have a family history of alcohol abuse. Officers, Senior Rates and engineering branch personnel were under represented. With regard to male:female ratio, age group distribution over age 20 and length of service, there were no significant differences between the alcohol referral and control groups. The majority of alcohol referrals were made by Medical and Divisional Officers, the overwhelming reason being disciplinary action related to alcohol abuse.

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Young women with poor ovarian response exhibit epigenetic age acceleration based on evaluation of white blood cells using a DNA methylation-derived age prediction model

Human Reproduction ◽

10.1093/humrep/deaa206 ◽

2020 ◽

Vol 35 (11) ◽

pp. 2579-2588 ◽

Cited By ~ 1

Author(s):

Brent M Hanson ◽

Xin Tao ◽

Yiping Zhan ◽

Timothy G Jenkins ◽

Scott J Morin ◽

...

Keyword(s):

Dna Methylation ◽

Prediction Model ◽

Ovarian Stimulation ◽

White Blood Cells ◽

Ovarian Response ◽

Poor Ovarian Response ◽

Epigenetic Age ◽

Epigenetic Age Acceleration ◽

Methylation Patterns ◽

Age Prediction

Abstract STUDY QUESTION Is poor ovarian response associated with a change in predicted age based on a DNA methylation-derived age prediction model (the Horvath algorithm) in white blood cells (WBCs) or cumulus cells (CCs)? SUMMARY ANSWER In young women, poor ovarian response is associated with epigenetic age acceleration within WBC samples but is not associated with age-related changes in CC. WHAT IS KNOWN ALREADY The majority of human tissues follow predictable patterns of methylation which can be assessed throughout a person’s lifetime. DNA methylation patterns may serve as informative biomarkers of aging within various tissues. Horvath’s ‘epigenetic clock’, which is a DNA methylation-derived age prediction model, accurately predicts a subject’s true chronologic age when applied to WBC but not to CC. STUDY DESIGN, SIZE, DURATION A prospective cohort study was carried out involving 175 women undergoing ovarian stimulation between February 2017 and December 2018. Women were grouped according to a poor (≤5 oocytes retrieved) or good (>5 oocytes) response to ovarian stimulation. Those with polycystic ovary syndrome (PCOS) (n = 35) were placed in the good responder group. PARTICIPANTS/MATERIALS, SETTING, METHODS DNA methylation patterns from WBC and CC were assessed for infertile patients undergoing ovarian stimulation at a university-affiliated private practice. DNA was isolated from peripheral blood samples and CC. Bisulfite conversion was then performed and a DNA methylation array was utilized to measure DNA methylation levels throughout the genome. Likelihood ratio tests were utilized to assess the relationship between predicted age, chronologic age and ovarian response. MAIN RESULTS AND THE ROLE OF CHANCE The Horvath-predicted age for WBC samples was consistent with patients’ chronologic age. However, predicted age from analysis of CC was younger than chronologic age. In subgroup analysis of women less than 38 years of age, poor ovarian response was associated with an accelerated predicted age in WBC (P = 0.017). Poor ovarian response did not affect the Horvath-predicted age based on CC samples (P = 0.502). No alternative methylation-based calculation was identified to be predictive of age for CC. LIMITATIONS, REASONS FOR CAUTION To date, analyses of CC have failed to identify epigenetic changes that are predictive of the aging process within the ovary. Despite the poor predictive nature of both the Horvath model and the novel methylation-based age prediction model described here, it is possible that our efforts failed to identify appropriate sites which would result in a successful age-prediction model derived from the CC epigenome. Additionally, lower DNA input for CC samples compared to WBC samples was a methodological limitation. We acknowledge that a universally accepted definition of poor ovarian response is lacking. Furthermore, women with PCOS were included and therefore the group of good responders in the current study may not represent a population with entirely normal methylation profiles. WIDER IMPLICATIONS OF THE FINDINGS The process of ovarian and CC aging continues to be poorly understood. Women who demonstrate poor ovarian response to stimulation represent a common clinical challenge, so clarifying the exact biological changes that occur within the ovary over time is a worthwhile endeavor. The data from CC support a view that hormonally responsive tissues may possess distinct epigenetic aging patterns when compared with other tissue types. Future studies may be able to determine whether alternative DNA methylation sites can accurately predict chronologic age or ovarian response to stimulation from CC samples. Going forward, associations between epigenetic age acceleration and reproductive and general health consequences must also be clearly defined. STUDY FUNDING/COMPETING INTEREST(S) No external funding was obtained for the study and there are no conflicts of interest. TRIAL REGISTRATION NUMBER N/A.

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