DNA Methylation Changes in the<i>IGF1R</i>Gene in Birth Weight Discordant Adult Monozygotic Twins

Tsai, Pei-Chien; Dongen, Jenny van; Tan, Qihua; Willemsen, Gonneke; Christiansen, Lene; Boomsma, Dorret I.; Spector, Tim D.; Valdes, Ana M.; Bell, Jordana T.

doi:10.1017/thg.2015.76

Cited by 24 publications

(18 citation statements)

References 95 publications

(140 reference statements)

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“…These epigenetic differences may account for phenotypic discordance in MZ twins. Multiple studies have explored the epigenetic changes in twins discordant for a range of congenital diseases, including autism spectrum disorder (Nguyen et al, 2010 ; Wong et al, 2014 ), birth weight (Souren et al, 2013 ; Tsai et al, 2015 ), congenital renal agenesis (Jin et al, 2014 ), and congenital cataracts (Wei et al, 2015 ). Recently, epigenetic aberrations have been sought in CHDs (Serra-Juhé et al, 2015 ; Vecoli et al, 2015 ) but not in CHD-discordant twins.…”

Section: Discussionmentioning

confidence: 99%

Copy Number Variants and Exome Sequencing Analysis in Six Pairs of Chinese Monozygotic Twins Discordant for Congenital Heart Disease

Tian

Cao

et al. 2017

Twin Res Hum Genet

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Congenital heart disease (CHD) is one of the most common birth defects. More than 200 susceptibility loci have been identified for CHDs, yet a large part of the genetic risk factors remain unexplained. Monozygotic (MZ) twins are thought to be completely genetically identical; however, discordant phenotypes have been found in MZ twins. Recent studies have demonstrated genetic differences between MZ twins. We aimed to test whether copy number variants (CNVs) and/or genetic mutation differences play a role in the etiology of CHDs by using single nucleotide polymorphism (SNP) genotyping arrays and whole exome sequencing of twin pairs discordant for CHDs. Our goal was to identify mutations present only in the affected twins, which could identify novel candidates for CHD susceptibility loci. We present a comprehensive analysis for the CNVs and genetic mutation results of the selected individuals but detected no consistent differences within the twin pairs. Our study confirms that chromosomal structure or genetic mutation differences do not seem to play a role in the MZ twins discordant for CHD.

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Section: Discussionmentioning

confidence: 99%

Copy Number Variants and Exome Sequencing Analysis in Six Pairs of Chinese Monozygotic Twins Discordant for Congenital Heart Disease

Tian

Cao

et al. 2017

Twin Res Hum Genet

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“…DNA was extracted from whole blood, bisulfite converted and subsequently analyzed using the Infinium 450K kit as previously described [ 50 ]. The beta mixture quantile dilation (BMIQ) method was performed to correct for technical variation [ 51 ].…”

Section: Methodsmentioning

confidence: 99%

Metabolomics profiling reveals novel markers for leukocyte telomere length

Zierer

Kastenmüller

Suhre

et al. 2016

Aging

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Leukocyte telomere length (LTL) is considered one of the most predictive markers of biological aging. The aim of this study was to identify novel pathways regulating LTL using a metabolomics approach. To this end, we tested associations between 280 blood metabolites and LTL in 3511 females from TwinsUK and replicated our results in the KORA cohort. We furthermore tested significant metabolites for associations with several aging-related phenotypes, gene expression markers and epigenetic markers to investigate potential underlying pathways. Five metabolites were associated with LTL: Two lysolipids, 1-stearoylglycerophosphoinositol (P=1.6×10−5) and 1-palmitoylglycerophosphoinositol (P=1.6×10−5), were found to be negatively associated with LTL and positively associated with phospholipase A2 expression levels suggesting an involvement of fatty acid metabolism and particularly membrane composition in biological aging. Moreover, two gamma-glutamyl amino acids, gamma-glutamyltyrosine (P=2.5×10−6) and gamma-glutamylphenylalanine (P=1.7×10−5), were negatively correlated with LTL. Both are products of the glutathione cycle and markers for increased oxidative stress. Metabolites were also correlated with functional measures of aging, i.e. higher blood pressure and HDL cholesterol levels and poorer lung, liver and kidney function. Our results suggest an involvement of altered fatty acid metabolism and increased oxidative stress in human biological aging, reflected by LTL and age-related phenotypes of vital organ systems.

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“…One of the most stable epigenetic processes is DNA methylation, or the addition of a CH 3 methyl group to cytosine, typically in the context of cytosine paired sequentially to a guanine nucleotide, separated by a phosphate group (CpG). DNA methylation is known to play a role in gene expression and cell differentiation, and differential DNA methylation has been linked to multiple human complex traits and disease phenotypes . Studies performed using bone samples have identified epigenetic alterations that influence bone cell function .…”

Section: Introductionmentioning

confidence: 99%

“…DNA methylation is known to play a role in gene expression and cell differentiation, (7,8) and differential DNA methylation has been linked to multiple human complex traits and disease phenotypes. (5,(9)(10)(11)(12) Studies performed using bone samples have identified epigenetic alterations that influence bone cell function. (13,14) We studied epigenetic variation in whole blood, as a proxy for difficult-to-acquire samples such as bone, in relation to BMD because epigenetic markers are often stable across multiple tissues, and immune cells within blood are known to influence bone homeostasis.…”

Section: Introductionmentioning

confidence: 99%

Epigenome-wide Association of DNA Methylation in Whole Blood With Bone Mineral Density

Morris

Tsai

Joehanes

et al. 2017

Journal of Bone and Mineral Research

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Genetic and environmental determinants of skeletal phenotypes such as bone mineral density (BMD) may converge through the epigenome, providing a tool to better understand osteoporosis pathophysiology. Because the epigenetics of BMD have been largely unexplored in humans, we performed an epigenome‐wide association study (EWAS) of BMD. We undertook a large‐scale BMD EWAS using the Infinium HumanMethylation450 array to measure site‐specific DNA methylation in up to 5515 European‐descent individuals (NDiscovery = 4614, NValidation = 901). We associated methylation at multiple cytosine‐phosphate‐guanine (CpG) sites with dual‐energy X‐ray absorptiometry (DXA)‐derived femoral neck and lumbar spine BMD. We performed sex‐combined and stratified analyses, controlling for age, weight, smoking status, estimated white blood cell proportions, and random effects for relatedness and batch effects. A 5% false‐discovery rate was used to identify CpGs associated with BMD. We identified one CpG site, cg23196985, significantly associated with femoral neck BMD in 3232 females (p = 7.9 × 10−11) and 4614 females and males (p = 3.0 × 10−8). cg23196985 was not associated with femoral neck BMD in an additional sample of 474 females (p = 0.64) and 901 males and females (p = 0.60). Lack of strong consistent association signal indicates that among the tested probes, no large‐effect epigenetic changes in whole blood associated with BMD, suggesting future epigenomic studies of musculoskeletal traits measure DNA methylation in a different tissue with extended genome coverage. © 2017 The Authors. Journal of Bone and Mineral Research Published by Wiley Periodicals Inc.

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DNA Methylation Changes in theIGF1RGene in Birth Weight Discordant Adult Monozygotic Twins

Cited by 24 publications

References 95 publications

Copy Number Variants and Exome Sequencing Analysis in Six Pairs of Chinese Monozygotic Twins Discordant for Congenital Heart Disease

Copy Number Variants and Exome Sequencing Analysis in Six Pairs of Chinese Monozygotic Twins Discordant for Congenital Heart Disease

Metabolomics profiling reveals novel markers for leukocyte telomere length

Epigenome-wide Association of DNA Methylation in Whole Blood With Bone Mineral Density

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