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首页> 外文期刊>Epigenetics: official journal of the DNA Methylation Society >Identification of sex-specific DNA methylation changes driven by specific chemicals in cord blood in a Faroese birth cohort
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Identification of sex-specific DNA methylation changes driven by specific chemicals in cord blood in a Faroese birth cohort

机译:鉴定异教血液中的特定化学品在FaroeseTa生队队列中的特定化学物质鉴定性别的DNA甲基化变化

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摘要

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.
机译:Faroe islanders消耗与甲基汞(Mehg),多氯联苯(PCB)和与慢性疾病风险相关的其他毒物污染的海洋食品。脐带血中特定CPG位点的差异DNA甲基化可作为来自化学曝光的替代生物标志物。我们旨在识别与DNA甲基化的脐带血中的关键环境化学品,其群体升高到化学混合物的群体。我们研究了1986年至1987年间的Faroese Thillate Cohort的72名参与者,并在成年期之前追随。使用infinium人甲基化450珠芯片来分析脐带血DNA甲膜。我们确定了CpG部位随浓度的MeHG,主要PCB,其他有机氯化合物[六氯苯(HCB),P,P'-二氯二氯二氯二氯乙烯(P,P'-DDE)和P,P'-二氯二苯基三氯乙烷]和全氟烷基]物质。在综合性分析中,在研究的16种化学品中,PCB同志105(CB-105)暴露与大多数差异甲基化CpG位点有关(总共214个)。在仅女性分析中,检测到73个CB-105相关的CPG位点,其中44位被映射到ELAV1相关癌症网络中的基因。仅在雄性的亚辛烷磺酸盐,HCB和P,P'-DDE分别观察到甲基化变化,分别为10,598,1,238和1,473个CPG位点,其中15%在与神经系统相关的X-染色体的细胞虫中富集障碍。在这种多污染物和基因组的研究中,我们确定了关键的表观遗传毒性。特定X-染色体位点的重大富集在男性中暗示了潜在的性别特异性表述对产前化学曝光的反应。

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