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孕期早期接触砷会改变脐带血中全基因组的DNA甲基化,对男孩的影响尤为明显。

Arsenic exposure in early pregnancy alters genome-wide DNA methylation in cord blood, particularly in boys.

作者信息

Broberg K, Ahmed S, Engström K, Hossain M B, Jurkovic Mlakar S, Bottai M, Grandér M, Raqib R, Vahter M

机构信息

1Institute of Environmental Medicine,Unit of Metals and Health,Karolinska Institutet,Stockholm,Sweden.

2Department of Laboratory Medicine,Section of Occupational and Environmental Medicine,Lund University,Lund,Sweden.

出版信息

J Dev Orig Health Dis. 2014 Aug;5(4):288-98. doi: 10.1017/S2040174414000221.

Abstract

Early-life inorganic arsenic exposure influences not only child health and development but also health in later life. The adverse effects of arsenic may be mediated by epigenetic mechanisms, as there are indications that arsenic causes altered DNA methylation of cancer-related genes. The objective was to assess effects of arsenic on genome-wide DNA methylation in newborns. We studied 127 mothers and cord blood of their infants. Arsenic exposure in early and late pregnancy was assessed by concentrations of arsenic metabolites in maternal urine, measured by high performance liquid chromatography-inductively coupled plasma mass spectrometry. Genome-wide 5-methylcytosine methylation in mononuclear cells from cord blood was analyzed by Infinium HumanMethylation450K BeadChip. Urinary arsenic in early gestation was associated with cord blood DNA methylation (Kolmogorov-Smirnov test, P-value<10-15), with more pronounced effects in boys than in girls. In boys, 372 (74%) of the 500 top CpG sites showed lower methylation with increasing arsenic exposure (r S -values>-0.62), but in girls only 207 (41%) showed inverse correlation (r S -values>-0.54). Three CpG sites in boys (cg15255455, cg13659051 and cg17646418), but none in girls, were significantly correlated with arsenic after adjustment for multiple comparisons. The associations between arsenic and DNA methylation were robust in multivariable-adjusted linear regression models. Much weaker associations were observed with arsenic exposure in late compared with early gestation. Pathway analysis showed overrepresentation of affected cancer-related genes in boys, but not in girls. In conclusion, early prenatal arsenic exposure appears to decrease DNA methylation in boys. Associations between early exposure and DNA methylation might reflect interference with de novo DNA methylation.

摘要

生命早期无机砷暴露不仅会影响儿童健康和发育,还会影响成年后的健康。砷的不良影响可能由表观遗传机制介导,因为有迹象表明砷会导致癌症相关基因的DNA甲基化改变。目的是评估砷对新生儿全基因组DNA甲基化的影响。我们研究了127名母亲及其婴儿的脐带血。通过高效液相色谱 - 电感耦合等离子体质谱法测量母体尿液中砷代谢物的浓度,评估妊娠早期和晚期的砷暴露情况。采用Infinium HumanMethylation450K BeadChip分析脐带血单个核细胞中的全基因组5-甲基胞嘧啶甲基化。妊娠早期的尿砷与脐带血DNA甲基化相关(柯尔莫哥洛夫 - 斯米尔诺夫检验,P值<10-15),对男孩的影响比对女孩更明显。在男孩中,500个顶级CpG位点中的372个(74%)显示随着砷暴露增加甲基化降低(rS值>-0.62),但在女孩中只有207个(41%)显示负相关(rS值>-0.54)。在进行多重比较调整后,男孩中的三个CpG位点(cg15255455、cg13659051和cg17646418)与砷显著相关,而女孩中没有。在多变量调整线性回归模型中,砷与DNA甲基化之间的关联很强。与妊娠早期相比,妊娠晚期砷暴露的关联要弱得多。通路分析显示受影响的癌症相关基因在男孩中过度表达,而在女孩中没有。总之,产前早期砷暴露似乎会降低男孩的DNA甲基化。早期暴露与DNA甲基化之间的关联可能反映了对从头DNA甲基化的干扰。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d87d/4283288/9eb93459ad22/S2040174414000221_fig1.jpg

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