450K Epigenome-Wide Scan Identifies Differential DNA Methylation in Newborns Related to Maternal Smoking during Pregnancy

Joubert, Bonnie R.; Håberg, Siri E.; Nilsen, Roy Miodini; Wang, Xuting; Vollset, Stein Emil; Murphy, Susan K.; Huang, Zhiqing; Hoyo, Cathrine; Midttun, Øivind; Cupul-Uicab, Lea A.; Ueland, Per Magne; Wu, Michael C.; Nystad, Wenche; Bell, Douglas A.; Peddada, Shyamal D.; London, Stephanie J.

doi:10.1289/ehp.1205412

Cited by 650 publications

(715 citation statements)

References 38 publications

(49 reference statements)

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“…However, close inspection of the data in Joubert et al revealed that 1 of the 4 differentially methylated CpG sites was more highly methylated among infants whose mothers were smokers. 12 Additionally, the magnitude of AHRR DNA methylation difference between mothers with undetectable vs. high cotinine levels at each of their 4 significant sites was of similar magnitude (»4%) as associations with our categorical predictors (2-3%). We did not analyze the same CpG sites as the smoking-associated CpG sites reported in prior studies but instead chose to maximize the CpG sites in the AHRR promoter region that our pyrosequencing assay would capture.…”

Section: Discussionsupporting

confidence: 50%

“…13 Others have demonstrated that these same methylation sites differed in the offspring of women who smoked during pregnancy, compared to offspring of non-smokers. 12,28 Prior studies demonstrating associations between smoking and AHRR DNA methylation used epigenome-wide methylation assays designed to discover previously unknown associations. 12,13 Given the results of these prior studies demonstrating that AHRR DNA methylation is modifiable during pregnancy, 12 we chose AHRR as a candidate gene to conduct a hypothesis-driven study of perinatal predictors of AHRR DNA methylation in cord blood.…”

Section: Discussionmentioning

confidence: 99%

“…9 Prenatal smoke exposure may also be associated with a higher risk of later obesity and cardiometabolic disorders. 10 Recent studies demonstrate that smoke exposure in adults 11 and among fetuses exposed to maternal smoking 12 is associated with altered leukocyte DNA methylation of the aryl-hydrocarbon receptor repressor (AHRR) gene, located on chromosome 5. 12,13 AHRR methylation is particularly interesting to study during pregnancy because the aryl-hydrocarbon receptor (AHR) is involved in metabolizing xenobiotics 14 that might affect fetal development.…”

Section: Introductionmentioning

confidence: 99%

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Offspring DNA methylation of the aryl-hydrocarbon receptor repressor gene is associated with maternal BMI, gestational age, and birth weight

et al. 2015

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(2015) Offspring DNA methylation of the arylhydrocarbon receptor repressor gene is associated with maternal BMI, gestational age, and birth weight, Epigenetics, 10:10, 913-921, DOI: 10.1080/15592294.2015 Prenatal smoke exposure, maternal obesity, aberrant fetal growth, and preterm birth are all risk factors for offspring metabolic syndrome. Cord blood aryl-hydrocarbon receptor repressor (AHRR) DNA methylation is responsive to maternal smoking during pregnancy. AHRR serves not only to inhibit aryl-hydrocarbon receptor (AHR) transcription, which is involved in mediating xenobiotic metabolism, but it is also involved in cell growth and differentiation. Other than maternal smoking, other predictors of offspring AHRR DNA methylation status remain unknown; we sought to identify them among newborns. We enrolled pregnant women in the PROGRESS birth cohort in Mexico City. Using pyrosequencing, we analyzed DNA methylation of 3 CpG sites within the AHRR gene promoter from the umbilical cord blood of 531 infants. We used generalized estimating equations to account for the correlation of DNA methylation between CpG sites. Multivariable models were used to adjust for maternal age, BMI, education, parity, smoke-exposure, infant sex, gestational age, and birth weight-for-gestational age. AHRR DNA methylation was positively associated with maternal BMI (P D 0.0009) and negatively associated with the length of gestation (P < 0.0001) and birth weight-forgestational age (P < 0.0001). AHRR DNA methylation was 2.1% higher in offspring of obese vs. normal weight mothers and 3.1% higher in preterm vs. term infants, representing a third and a half standard deviation differences in methylation, respectively. In conclusion, offspring AHRR DNA methylation was associated with maternal obesity during pregnancy as well as infant gestational age and birth weight-for-gestational age. Further work to discover the health impacts of altered AHRR DNA methylation is warranted.

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Section: Discussionsupporting

confidence: 50%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Offspring DNA methylation of the aryl-hydrocarbon receptor repressor gene is associated with maternal BMI, gestational age, and birth weight

et al. 2015

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“…This balance of responsiveness to stimuli and heritability results in a unique mechanism for lasting signatures of prior exposures that accumulate over the lifetime (Cortessis et al ., 2012; Feil & Fraga, 2012). As an example of a specific exposure that has been shown to leave a lasting signature, cigarette smoke has been linked to changes in DNA methylation at the AHRR locus both in smokers and in children of smokers (Saxonov et al ., 2006; Monick et al ., 2012; Joubert et al ., 2012; Shenker et al ., 2013; Sun et al ., 2013 Elliott et al ., 2014; Lee et al ., 2015; Shah et al ., 2014). Smoking‐associated DNA methylation changes have also been found in genes involved in inflammatory networks, important candidates in the risk of age‐related diseases such as heart disease and stroke (Breitling et al ., 2012; Dogan et al ., 2014).…”

Section: Epigenetic Drift Vs the Epigenetic Clock: Two Phenomena Undmentioning

confidence: 99%

DNA methylation and healthy human aging

2015

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SummaryThe process of aging results in a host of changes at the cellular and molecular levels, which include senescence, telomere shortening, and changes in gene expression. Epigenetic patterns also change over the lifespan, suggesting that epigenetic changes may constitute an important component of the aging process. The epigenetic mark that has been most highly studied is DNA methylation, the presence of methyl groups at CpG dinucleotides. These dinucleotides are often located near gene promoters and associate with gene expression levels. Early studies indicated that global levels of DNA methylation increase over the first few years of life and then decrease beginning in late adulthood. Recently, with the advent of microarray and next‐generation sequencing technologies, increases in variability of DNA methylation with age have been observed, and a number of site‐specific patterns have been identified. It has also been shown that certain CpG sites are highly associated with age, to the extent that prediction models using a small number of these sites can accurately predict the chronological age of the donor. Together, these observations point to the existence of two phenomena that both contribute to age‐related DNA methylation changes: epigenetic drift and the epigenetic clock. In this review, we focus on healthy human aging throughout the lifetime and discuss the dynamics of DNA methylation as well as how interactions between the genome, environment, and the epigenome influence aging rates. We also discuss the impact of determining ‘epigenetic age’ for human health and outline some important caveats to existing and future studies.

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“…Several studies have investigated the epigenome-wide association between smoking, an important PM source, and DNA methylation. Using the 450K platform and Bonferroni correction, Joubert et al 17 identified 26 CpGs with methylation changes in newborns related to maternal smoking during pregnancy in a large Norwegian birth cohort. Specifically, the authors documented changes at CpGs in cytochrome p450 1A1 (CYP1A1) and aryl-hydrocarbon receptor repressor (AHRR), genes known to play a key role in the aryl hydrocarbon receptor (AhR) signaling pathway that mediates the detoxification of components of tobacco smoke.…”

Section: Introductionmentioning

confidence: 99%

Differential DNA methylation and PM_2.5 species in a 450K epigenome-wide association study

et al. 2017

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Although there is growing evidence that exposure to ambient particulate matter is associated with global DNA methylation and gene-specific methylation, little is known regarding epigenome-wide changes in DNA methylation in relation to particles and, especially, particle components. Using the Illumina Infinium HumanMethylation450 BeadChip, we examined the relationship between one-year moving averages of PM 2.5 species (Al, Ca, Cu, Fe, K, Na, Ni, S, Si, V, and Zn) and DNA methylation at 484,613 CpG probes in a longitudinal cohort that included 646 subjects. Bonferroni correction was applied to adjust for multiple comparisons. Bioinformatics analysis of the Kyoto Encyclopedia of Genes and Genomes (KEGG) pathway enrichment was also performed. We observed 20 Bonferroni significant (P-value < 9.4£ 10 ¡9 ) CpGs for Fe, 8 for Ni, and 1 for V. Particularly, methylation at Schlafen Family Member 11 (SLFN11) cg10911913 was positively associated with measured levels of all 3 species. The SLFN11 gene codes for an interferoninduced protein that inhibits retroviruses and sensitizes cancer cells to DNA-damaging agents. Bioinformatics analysis suggests that gene targets may be relevant to pathways including cancers, signal transduction, and cell growth and death. Ours is the first study to examine the epigenome-wide association between ambient particles species and DNA methylation. We found that long-term exposures to specific components of ambient particle pollution, especially particles emitted during oil combustion, were associated with methylation changes in genes relevant to immune responses. Our findings provide insight into potential biologic mechanisms on an epigenetic level.

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450K Epigenome-Wide Scan Identifies Differential DNA Methylation in Newborns Related to Maternal Smoking during Pregnancy

Cited by 650 publications

References 38 publications

Offspring DNA methylation of the aryl-hydrocarbon receptor repressor gene is associated with maternal BMI, gestational age, and birth weight

Offspring DNA methylation of the aryl-hydrocarbon receptor repressor gene is associated with maternal BMI, gestational age, and birth weight

DNA methylation and healthy human aging

Differential DNA methylation and PM_2.5 species in a 450K epigenome-wide association study

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450K Epigenome-Wide Scan Identifies Differential DNA Methylation in Newborns Related to Maternal Smoking during Pregnancy

Cited by 650 publications

References 38 publications

Offspring DNA methylation of the aryl-hydrocarbon receptor repressor gene is associated with maternal BMI, gestational age, and birth weight

Offspring DNA methylation of the aryl-hydrocarbon receptor repressor gene is associated with maternal BMI, gestational age, and birth weight

DNA methylation and healthy human aging

Differential DNA methylation and PM2.5 species in a 450K epigenome-wide association study

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Differential DNA methylation and PM_2.5 species in a 450K epigenome-wide association study