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鉴定法罗群岛出生队列脐带血中特定化学物质驱动的性别特异性 DNA 甲基化变化。

Identification of sex-specific DNA methylation changes driven by specific chemicals in cord blood in a Faroese birth cohort.

机构信息

a Division of Environmental Genetics and Molecular Toxicology.

e Center of Environmental Genetics.

出版信息

Epigenetics. 2018;13(3):290-300. doi: 10.1080/15592294.2018.1445901. Epub 2018 May 16.

Abstract

Faroe islanders consume marine foods contaminated with methylmercury (MeHg), polychlorinated biphenyls (PCBs), and other toxicants associated with chronic disease risks. Differential DNA methylation at specific CpG sites in cord blood may serve as a surrogate biomarker of health impacts from chemical exposures. We aimed to identify key environmental chemicals in cord blood associated with DNA methylation changes in a population with elevated exposure to chemical mixtures. We studied 72 participants of a Faroese birth cohort recruited between 1986 and 1987 and followed until adulthood. The cord blood DNA methylome was profiled using Infinium HumanMethylation450 BeadChips. We determined the associations of CpG site changes with concentrations of MeHg, major PCBs, other organochlorine compounds [hexachlorobenzene (HCB), p,p'-dichlorodiphenyldichloroethylene (p,p'-DDE) and p,p'-dichlorodiphenyltrichloroethane], and perfluoroalkyl substances. In a combined sex analysis, among the 16 chemicals studied, PCB congener 105 (CB-105) exposure was associated with the majority of differentially methylated CpG sites (214 out of a total of 250). In female-only analysis, only 73 CB-105 associated CpG sites were detected, 44 of which were mapped to genes in the ELAV1-associated cancer network. In males-only, methylation changes were seen for perfluorooctane sulfonate, HCB, and p,p'-DDE in 10,598, 1,238, and 1,473 CpG sites, respectively, 15% of which were enriched in cytobands of the X-chromosome associated with neurological disorders. In this multiple-pollutant and genome-wide study, we identified key epigenetic toxicants. The significant enrichment of specific X-chromosome sites in males implies potential sex-specific epigenome responses to prenatal chemical exposures.

摘要

法罗群岛居民食用的海洋食品受到甲基汞(MeHg)、多氯联苯(PCBs)和其他与慢性病风险相关的有毒物质的污染。脐带血中特定 CpG 位点的差异 DNA 甲基化可能成为化学暴露对健康影响的替代生物标志物。我们旨在确定脐带血中与该人群化学混合物暴露升高相关的关键环境化学物质,这些化学物质与 DNA 甲基化变化有关。我们研究了 1986 年至 1987 年间招募并一直随访至成年的法罗群岛出生队列的 72 名参与者。使用 Infinium HumanMethylation450 BeadChips 对脐带血 DNA 甲基组进行了分析。我们确定了 CpG 位点变化与 MeHg、主要 PCBs、其他有机氯化合物[六氯苯(HCB)、p,p'-二氯二苯二氯乙烯(p,p'-DDE)和 p,p'-二氯二苯三氯乙烷]和全氟烷基物质浓度之间的关联。在一项综合性别分析中,在所研究的 16 种化学物质中,多氯联苯同系物 105(CB-105)暴露与大多数差异甲基化 CpG 位点(总共 250 个中的 214 个)有关。在仅女性分析中,仅检测到 73 个 CB-105 相关 CpG 位点,其中 44 个映射到 ELAV1 相关癌症网络中的基因。在男性中,仅在全氟辛烷磺酸、HCB 和 p,p'-DDE 中分别观察到 10,598、1,238 和 1,473 个 CpG 位点的甲基化变化,其中 15%在与神经紊乱相关的 X 染色体的细胞带中富集。在这项多污染物和全基因组研究中,我们确定了关键的表观遗传毒物。男性中特定 X 染色体位点的显著富集表明,男性对产前化学暴露的潜在性别特异性表观基因组反应。

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