Your search keyword '"Jung, Chol-Hee"' showing total 5 results

1. Methylation marks of prenatal exposure to maternal smoking and risk of cancer in adulthood.

Author

Dugué, Pierre-Antoine, Hodge, Allison M, Wong, Ee Ming, Joo, JiHoon E, Jung, Chol-Hee, Hopper, John L, English, Dallas R, Giles, Graham G, Milne, Roger L, and Southey, Melissa C

Subjects

MATERNAL exposure, METHYLATION, SMOKING, DNA methylation, TRANSITIONAL cell carcinoma, UROTHELIUM, ADENOMATOUS polyps, P16 gene, PRENATAL exposure delayed effects, TUMORS, LONGITUDINAL method

Abstract

Background: Prenatal exposure to maternal smoking is detrimental to child health but its association with risk of cancer has seldom been investigated. Maternal smoking induces widespread and long-lasting DNA methylation changes, which we study here for association with risk of cancer in adulthood.Methods: Eight prospective case-control studies nested within the Melbourne Collaborative Cohort Study were used to assess associations between maternal-smoking-associated methylation marks in blood and risk of several cancers: breast (n = 406 cases), colorectal (n = 814), gastric (n = 166), kidney (n = 139), lung (n = 327), prostate (n = 847) and urothelial (n = 404) cancer and B-cell lymphoma (n = 426). We used conditional logistic regression models to estimate odds ratios (ORs) and 95% confidence intervals (CIs) for associations between cancer and five methylation scores calculated as weighted averages for 568, 19, 15, 28 and 17 CpG sites. Models were adjusted for confounders, including personal smoking history (smoking status, pack-years, age at starting and quitting) and methylation scores for personal smoking.Results: All methylation scores for maternal smoking were strongly positively associated with risk of urothelial cancer. Risk estimates were only slightly attenuated after adjustment for smoking history, other potential confounders and methylation scores for personal smoking. Potential negative associations were observed with risk of lung cancer and B-cell lymphoma. No associations were observed for other cancers.Conclusions: We found that methylation marks of prenatal exposure to maternal smoking are associated with increased risk of urothelial cancer. Our study demonstrates the potential for using DNA methylation to investigate the impact of early-life, unmeasured exposures on later-life cancer risk. [ABSTRACT FROM AUTHOR]

Published

2021

2. Alcohol consumption is associated with widespread changes in blood DNA methylation: Analysis of cross-sectional and longitudinal data.

Author

Dugué, Pierre‐Antoine, Wilson, Rory, Lehne, Benjamin, Jayasekara, Harindra, Wang, Xiaochuan, Jung, Chol‐Hee, Joo, JiHoon E., Makalic, Enes, Schmidt, Daniel F., Baglietto, Laura, Severi, Gianluca, Gieger, Christian, Ladwig, Karl‐Heinz, Peters, Annette, Kooner, Jaspal S., Southey, Melissa C., English, Dallas R., Waldenberger, Melanie, Chambers, John C., and Giles, Graham G.

Subjects

DNA methylation, ALCOHOL drinking, DNA analysis, CROSS-sectional method, BLOOD alcohol, EPIGENOMICS, RESEARCH, SEQUENCE analysis, DNA, RESEARCH methodology, MEDICAL cooperation, EVALUATION research, COMPARATIVE studies, GENES, LONGITUDINAL method

Abstract

DNA methylation may be one of the mechanisms by which alcohol consumption is associated with the risk of disease. We conducted a large-scale, cross-sectional, genome-wide DNA methylation association study of alcohol consumption and a longitudinal analysis of repeated measurements taken several years apart. Using the Illumina HumanMethylation450 BeadChip, DNA methylation was measured in blood samples from 5606 Melbourne Collaborative Cohort Study (MCCS) participants. For 1088 of them, these measures were repeated using blood samples collected a median of 11 years later. Associations between alcohol intake and blood DNA methylation were assessed using linear mixed-effects regression models. Independent data from the London Life Sciences Prospective Population (LOLIPOP) (N = 4042) and Cooperative Health Research in the Augsburg Region (KORA) (N = 1662) cohorts were used to replicate associations discovered in the MCCS. Cross-sectional analyses identified 1414 CpGs associated with alcohol intake at P < 10-7 , 1243 of which had not been reported previously. Of these novel associations, 1078 were replicated (P < .05) using LOLIPOP and KORA data. Using the MCCS data, we also replicated 403 of 518 previously reported associations. Interaction analyses suggested that associations were stronger for women, non-smokers, and participants genetically predisposed to consume less alcohol. Of the 1414 CpGs, 530 were differentially methylated (P < .05) in former compared with current drinkers. Longitudinal associations between the change in alcohol intake and the change in methylation were observed for 513 of the 1414 cross-sectional associations. Our study indicates that alcohol intake is associated with widespread changes in DNA methylation across the genome. Longitudinal analyses showed that the methylation status of alcohol-associated CpGs may change with alcohol consumption changes in adulthood. [ABSTRACT FROM AUTHOR]

Published

2021

3. Dietary intake of one-carbon metabolism nutrients and DNA methylation in peripheral blood.

Author

Chamberlain, James A, Dugué, Pierre-Antoine, Bassett, Julie K, Hodge, Allison M, Brinkman, Maree T, Joo, JiHoon E, Jung, Chol-Hee, Makalic, Enes, Schmidt, Daniel F, Hopper, John L, Buchanan, Daniel D, English, Dallas R, Southey, Melissa C, Giles, Graham G, and Milne, Roger L

Subjects

CARBON metabolism, AGE distribution, BIRTHPLACES, CHOLINE, DIETARY supplements, ALCOHOL drinking, ENZYMES, FOLIC acid, INGESTION, LONGITUDINAL method, METHIONINE, NUTRITIONAL assessment, PURINES, QUESTIONNAIRES, REGRESSION analysis, SEX distribution, SMOKING, VITAMIN B12, VITAMIN B2, VITAMIN B6, GENOMICS, CROSS-sectional method, BETAINE, DNA methylation, MEDITERRANEAN diet

Abstract

Background: Folate and other one-carbon metabolism nutrients are essential to enable DNA methylation to occur, but the extent to which their dietary intake influences methylation in adulthood is unclear. Objective: We assessed associations between dietary intake of these nutrients and DNA methylation in peripheral blood, overall and at specific genomic locations. Design: We conducted a cross-sectional study using baseline data and samples from 5186 adult participants in the Melbourne Collaborative Cohort Study (MCCS). Nutrient intake was estimated from a food-frequency questionnaire. DNA methylation was measured by using the Illumina Infinium HumanMethylation450 BeadChip array (HM450K). We assessed associations of intakes of folate, riboflavin, vitamins B-6 and B-12, methionine, choline, and betaine with methylation at individual cytosine-guanine dinucleotides (CpGs), and with median (genome-wide) methylation across all CpGs, CpGs in gene bodies, and CpGs in gene promoters. We also assessed associations with methylation at long interspersed nuclear element 1 (LINE-1), satellite 2 (Sat2), and Arthrobacter luteus restriction endonuclease (Alu) repetitive elements for a subset of participants. We used linear mixed regression, adjusting for age, sex, country of birth, smoking, energy intake from food, alcohol intake, Mediterranean diet score, and batch effects to assess loglinear associations with dietary intake of each nutrient. In secondary analyses, we assessed associations with low or high intakes defined by extreme quintiles. Results: No evidence of log-linear association was observed at P < 10−7 between the intake of one-carbon metabolism nutrients and methylation at individual CpGs. Low intake of riboflavin was associated with higher methylation at CpG cg21230392 in the first exon of PROM1 (P = 5.0 × 10−8). No consistent evidence of association was observed with genome-wide or repetitive element measures of methylation. Conclusion: Our findings suggest that dietary intake of onecarbon metabolism nutrients in adulthood, as measured by a foodfrequency questionnaire, has little association with blood DNA methylation. An association with low intake of riboflavin requires replication in independent cohorts. [ABSTRACT FROM AUTHOR]

Published

2018

4. Genome-wide measures of DNA methylation in peripheral blood and the risk of urothelial cell carcinoma: a prospective nested case-control study.

Author

Dugué, Pierre-Antoine, Brinkman, Maree T, Milne, Roger L, Wong, Ee Ming, FitzGerald, Liesel M, Bassett, Julie K, Joo, Jihoon E, Jung, Chol-Hee, Makalic, Enes, Schmidt, Daniel F, Park, Daniel J, Chung, Jessica, Ta, Anthony D, Bolton, Damien M, Lonie, Andrew, Longano, Anthony, Hopper, John L, Severi, Gianluca, Saffery, Richard, and English, Dallas R

Subjects

BLOOD collection, CANCER invasiveness, DIET, DNA, LONGITUDINAL method, SMOKING, TIME, URINARY organs, RELATIVE medical risk, DISEASE incidence, CASE-control method, TRANSITIONAL cell carcinoma, DNA methylation, SEQUENCE analysis, TUMORS

Abstract

Background: Global DNA methylation has been reported to be associated with urothelial cell carcinoma (UCC) by studies using blood samples collected at diagnosis. Using the Illumina HumanMethylation450 assay, we derived genome-wide measures of blood DNA methylation and assessed them for their prospective association with UCC risk.Methods: We used 439 case-control pairs from the Melbourne Collaborative Cohort Study matched on age, sex, country of birth, DNA sample type, and collection period. Conditional logistic regression was used to compute odds ratios (OR) of UCC risk per s.d. of each genome-wide measure of DNA methylation and 95% confidence intervals (CIs), adjusted for potential confounders. We also investigated associations by disease subtype, sex, smoking, and time since blood collection.Results: The risk of superficial UCC was decreased for individuals with higher levels of our genome-wide DNA methylation measure (OR=0.71, 95% CI: 0.54-0.94; P=0.02). This association was particularly strong for current smokers at sample collection (OR=0.47, 95% CI: 0.27-0.83). Intermediate levels of our genome-wide measure were associated with decreased risk of invasive UCC. Some variation was observed between UCC subtypes and the location and regulatory function of the CpGs included in the genome-wide measures of methylation.Conclusions: Higher levels of our genome-wide DNA methylation measure were associated with decreased risk of superficial UCC and intermediate levels were associated with reduced risk of invasive disease. These findings require replication by other prospective studies. [ABSTRACT FROM AUTHOR]

Published

2016

5. Physical Activity, Television Viewing Time, and DNA Methylation in Peripheral Blood.

Author

VAN ROEKEL, ELINE H., DUGUÉ, PIERRE-ANTOINE, ENGLISH, DALLAS R., GILES, GRAHAM G., MILNE, ROGER L., LYNCH, BRIGID M., MAKALIC, ENES, JUNG, CHOL-HEE, JOO, JIHOON E., WONG, EE MING, and SOUTHEY, MELISSA C.

Subjects

*BIOLOGICAL assay, *BLOOD circulation, *CHRONIC diseases, *COMPARATIVE studies, *GENOMES, *INTERPROFESSIONAL relations, *LEISURE, *LONGITUDINAL method, *QUESTIONNAIRES, *REGRESSION analysis, *SELF-evaluation, *TELEVISION, *CROSS-sectional method, *PHYSICAL activity, *DNA methylation, *SCREEN time, *EVALUATION

Abstract

Supplemental digital content is available in the text. Introduction: Physical activity may affect health via DNA methylation. The epigenetic influences of sedentary behaviors such as television viewing are unknown. We performed a genomewide study of DNA methylation in peripheral blood in relation to physical activity and television viewing time. Methods: DNA methylation was measured using the Illumina Infinium HumanMethylation450K BeadChip array in blood samples collected at baseline (N = 5513) and follow-up (N = 1249) from participants in the Melbourne Collaborative Cohort Study. At baseline, times per week of leisure-time physical activity were self-reported. At follow-up, the International Physical Activity Questionnaire was used to assess MET-hours per week of total and leisure-time physical activity and hours per day of television viewing time. Linear mixed models were used to assess associations between physical activity and television viewing measures and DNA methylation at individual CpG sites, adjusted for potential confounders and batch effects. Results: At follow-up, total physical activity was associated with DNA methylation at cg10266336 (P = 6.0 × 10−9), annotated to the SAA2 gene. Weaker evidence of associations (P < 1.0 × 10−5) were observed for an additional 14 CpG sites with total physical activity, for 7 CpG sites with leisure-time physical activity, and for 9 CpG sites with television viewing time. Changes in leisure-time physical activity between baseline and follow-up were associated with methylation changes (P < 0.05) at four of the seven CpG sites with weaker evidence of cross-sectional associations with leisure-time physical activity. Conclusion: Physical activity and television viewing may be associated with blood DNA methylation, a potential pathway to chronic disease development. Further research using accelerometer data and larger sample sizes is warranted. [ABSTRACT FROM AUTHOR]

Published

2019