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首页> 外文期刊>Environmental Health: A Global Access Science Source >Genome-wide DNA methylation at birth in relation to in utero arsenic exposure and the associated health in later life
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Genome-wide DNA methylation at birth in relation to in utero arsenic exposure and the associated health in later life

机译:出生时全基因组全基因组DNA甲基化与子宫内砷暴露及以后生命相关健康的关系

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BackgroundIn utero arsenic exposure may alter fetal developmental programming by altering DNA methylation, which may result in a higher risk of disease in later life. We evaluated the association between in utero arsenic exposure and DNA methylation (DNAm) in cord blood and its influence in later life. MethodsGenome-wide DNA methylation in cord blood from 64 subjects in the Taiwanese maternal infant and birth cohort was analyzed. Robust regressions were applied to assess the association of DNA methylation with in utero arsenic exposure. Multiple testing was adjusted by controlling false discovery rate (FDR) of 0.05. The DAVID bioinformatics tool was implemented for functional annotation analyses on the detected CpGs. The identified CpGs were further tested in an independent cohort. For the CpGs replicated in the independent cohort, linear mixed models were applied to assess the association of DNA methylation with low-density lipoprotein (LDL) at different ages (2, 5, 8, 11 and 14?years). ResultsIn total, 579 out of 385,183 CpGs were identified after adjusting for multiple testing (FDR?=?0.05), of which ~60% were positively associated with arsenic exposure. Functional annotation analysis on these CpGs detected 17 KEGG pathways (FDR?=?0.05) including pathways for cardiovascular diseases (CVD) and diabetes mellitus. In the independent cohort, about 46% (252 out of 553 CpGs) of the identified CpGs showed associations consistent with those in the study cohort. In total, 11 CpGs replicated in the independent cohort were in the pathways related to CVD and diabetes mellitus. Via longitudinal analyses, we found at 5 out of the 11 CpGs methylation was associated with LDL over time and interactions between DNA methylation and time were observed at 4 of the 5 CpGs, cg25189764 (coeff?=?0.157, p -value?=?0.047), cg04986899 (coeff. For interaction [coeff.int]?=?0.030, p -value?=?0.024), cg04903360 (coeff.int?=?0.026, p -value?=?0.032), cg08198265 (coeff.int?=??0.063, p -value?=?0.0021), cg10473311 (coeff.int?=??0.021, p -value?=?0.027). ConclusionIn utero arsenic exposure was associated with cord blood DNA methylation at various CpGs. The identified CpGs may help determine pathological epigenetic mechanisms linked to in utero arsenic exposure. Five CpGs (cg25189764, cg04986899, cg04903360, cg08198265 and cg10473311) may serve as epigenetic markers for changes in LDL later in life.
机译:背景子宫内砷暴露可能会通过改变DNA甲基化而改变胎儿的发育程序,这可能导致以后生活中疾病的风险更高。我们评估了子宫内砷暴露与脐带血中的DNA甲基化(DNAm)之间的关联及其对以后生活的影响。方法分析了台湾产妇和出生队列的64名受试者的脐血全基因组DNA甲基化。应用稳健的回归来评估DNA甲基化与子宫内砷暴露的关联。通过将错误发现率(FDR)控制为0.05,可以调整多项测试。使用DAVID生物信息学工具对检测到的CpG进行功能注释分析。所鉴定的CpG在独立队列中进一步测试。对于在独立队列中复制的CpG,应用线性混合模型评估不同年龄(2、5、8、11和14岁)的DNA甲基化与低密度脂蛋白(LDL)的关联。结果经过多次测试校正后,在385,183个CpG中总共发现579个(FDR?=?0.05),其中约60%与砷暴露呈正相关。对这些CpG的功能注释分析检测到了17种KEGG通路(FDRα=?0.05),包括心血管疾病(CVD)和糖尿病的通路。在独立队列中,约46%(553个CpG中的252个)显示出与研究队列中的相关性一致的关联。总体上,在独立队列中复制的11 CpG位于与CVD和糖尿病相关的途径中。通过纵向分析,我们发现在11个CpGs中有5个甲基化与LDL随时间变化相关联,并且在5个CpG中有4个cg25189764观察到了DNA甲基化和时间之间的相互作用(coeff?=?0.157,p-value?=?)。 0.047),cg04986899(coeff。对于交互作用[coeff.int]?=?0.030,p -value?=?0.024),cg04903360(coeff.int?=?0.026,p -value?=?0.032),cg08198265(coeff .int≥0.063,p值= 0.0021,cg10473311(coeff.int≥0.021,p值= 0.027)。结论子宫内砷暴露与脐带血DNA在各种CpGs甲基化有关。鉴定出的CpGs可能有助于确定与子宫内砷暴露相关的病理表观遗传机制。五个CpG(cg25189764,cg04986899,cg04903360,cg08198265和cg10473311)可以作为生命后期LDL变化的表观遗传标记。

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