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探讨脐带血、脐带组织和胎盘内产前双酚暴露与组织特异性 DNA 甲基化反应。

Probing prenatal bisphenol exposures and tissue-specific DNA methylation responses in cord blood, cord tissue, and placenta.

机构信息

Department of Nutritional Sciences, University of Michigan School of Public Health, Ann Arbor, MI, USA.

Department of Environmental Health Sciences, University of Michigan School of Public Health, Ann Arbor, MI, USA.

出版信息

Reprod Toxicol. 2023 Jan;115:74-84. doi: 10.1016/j.reprotox.2022.11.005. Epub 2022 Dec 5.

Abstract

The early-gestational fetal epigenome establishes the landscape for fetal development and is susceptible to disruption via environmental stressors including chemical exposures. Research has explored how cell- and tissue-type-specific epigenomic signatures contribute to human disease, but how the epigenome in each tissue comparatively responds to environmental exposures is largely unknown. This pilot study compared DNA methylation in four previously identified genes across matched cord blood (CB), cord tissue (CT), and placental (PL) samples from 28 mother-infant pairs in tthe Michigan Mother Infant Pairs study; evaluated association between prenatal exposure to bisphenols (BPA, BPF, and BPS) and DNA methylation (DNAm) by tissue type; compared epigenome-wide DNAm of CB and PL; and explored associations between prenatal bisphenol exposures and epigenome-wide DNAm in PL. Bisphenol concentrations were quantified in first-trimester maternal urine. DNAm was assessed at four genes via pyrosequencing in three tissues; epigenome-wide DNAm analysis via Infinium MethylationEPIC array was completed on CB and PL. Candidate gene analysis revealed tissue-specific differences across all genes. In adjusted linear regression, BPA and BPF were associated with DNAm across candidate genes in PL but not CB and CT. Epigenome-wide comparison of matched CB and PL DNAm revealed tissue-specific differences at most CpG sites and modest associations between maternal first-trimester bisphenol exposures and PL but not CB DNAm. These data endorse inclusion of a variety of tissues in prenatal exposure studies. Overlapping and divergent responses in CB, CT, and PL demonstrate their utility in combination to capture a fuller picture of the epigenetic effect of developmental exposures.

摘要

胚胎早期的表观基因组为胎儿发育奠定了基础,并容易受到环境应激源的破坏,包括化学暴露。研究已经探讨了细胞和组织特异性表观基因组特征如何导致人类疾病,但每个组织的表观基因组如何相对应地对环境暴露做出反应在很大程度上是未知的。这项初步研究比较了 28 对密歇根母婴对研究中配对的脐带血(CB)、脐带组织(CT)和胎盘(PL)样本中四个先前确定的基因的 DNA 甲基化;评估了产前暴露于双酚(BPA、BPF 和 BPS)与组织类型的 DNA 甲基化(DNAm)之间的关联;比较了 CB 和 PL 的全基因组 DNAm;并探索了 PL 中产前双酚暴露与全基因组 DNAm 之间的关联。在孕早期测量了母亲尿液中的双酚浓度。通过焦磷酸测序在三个组织中评估了四个基因的 DNAm;通过 Infinium MethylationEPIC 阵列在 CB 和 PL 上完成了全基因组 DNAm 分析。候选基因分析显示,所有基因在所有组织中均存在组织特异性差异。在调整后的线性回归中,BPA 和 BPF 与 PL 中候选基因的 DNAm 相关,但与 CB 和 CT 无关。配对的 CB 和 PL DNAm 的全基因组比较显示,大多数 CpG 位点存在组织特异性差异,以及母体孕早期双酚暴露与 PL 但与 CB DNAm 之间存在适度关联。这些数据支持在产前暴露研究中纳入各种组织。CB、CT 和 PL 中的重叠和发散反应表明,它们联合使用可以更全面地捕捉发育暴露对表观遗传的影响。

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