首页> 外文期刊>Human Molecular Genetics >Heritable rather than age-related environmental and stochastic factors dominate variation in DNA methylation of the human IGF2/H19 locus.
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Heritable rather than age-related environmental and stochastic factors dominate variation in DNA methylation of the human IGF2/H19 locus.

机译:可遗传的而不是与年龄有关的环境和随机因素主导着人IGF2 / H19基因座DNA甲基化的变化。

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Epigenetic variation may significantly contribute to the risk of common disease. Currently, little is known about the extent and causes of epigenetic variation. Here, we investigated the contribution of heritable influences and the combined effect of environmental and stochastic factors to variation in DNA methylation of the IGF2/H19 locus. Moreover, we tested whether this locus was subject to age-related degeneration of epigenetic patterns as was previously suggested for global methylation. We measured methylation of the H19 and IGF2 differentially methylated regions (DMRs) in 196 adolescent and 176 middle-aged twins using a recently developed mass spectrometry-based method. We observed substantial variation in DNA methylation across individuals, underscoring that DNA methylation is a quantitative trait. Analysis of data in monozygotic and dizygotic twins revealed that a significant part of this variation could be attributed to heritable factors. The heritability of methylation of individual CpG sitesvaried between 20 and 74% for the H19 DMR and was even higher, between 57 and 97%, for the IGF2 DMR. Remarkably, the combined influence of environmental and stochastic factors on DNA methylation was not greater in middle-age than in adolescence, suggesting a limited role for age-related degeneration of methylation patterns at this locus. Single nucleotide polymorphisms in the IGF2/H19 locus were significantly associated with DNA methylation of the IGF2 DMR (P = 0.004). A preliminary analysis suggested an association between H19 DMR methylation and body size (P < 0.05). Our study shows that variation in DNA methylation of the IGF2/H19 locus is mainly determined by heritable factors and single nucleotide polymorphisms (SNPs) in cis, rather than the cumulative effect of environmental and stochastic factors occurring with age.
机译:表观遗传变异可能会大大增加患上普通疾病的风险。目前,关于表观遗传变异的程度和原因知之甚少。在这里,我们调查了遗传因素的影响以及环境因素和随机因素对IGF2 / H19基因座DNA甲基化变异的影响。此外,我们测试了该基因座是否遭受了与年龄有关的表观遗传模式的退化,如先前对全球甲基化所建议的那样。我们使用最近开发的基于质谱的方法测量了196名青少年和176名中年双胞胎中H19和IGF2差异甲基化区域(DMR)的甲基化。我们观察到个体间DNA甲基化的显着差异,强调了DNA甲基化是一个定量特征。单卵双卵和双卵双卵的数据分析表明,这种变异的很大一部分可能归因于遗传因素。对于H19 DMR,单个CpG位点甲基化的遗传力在20%到74%之间,对于IGF2 DMR更高,在57%到97%之间。值得注意的是,环境因素和随机因素对DNA甲基化的综合影响在中年并不比青春期大,这表明该基因座在与年龄相关的甲基化模式退化中作用有限。 IGF2 / H19基因座中的单核苷酸多态性与IGF2 DMR的DNA甲基化显着相关(P = 0.004)。初步分析表明,H19 DMR甲基化与体重之间存在关联(P <0.05)。我们的研究表明,IGF2 / H19基因座的DNA甲基化变异主要由遗传因素和顺式单核苷酸多态性(SNPs)决定,而不是环境和随机因素随年龄的累积影响而确定。

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