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通过核比例调整甲基化水平突出了与子痫前期相关的差异甲基化胞嘧啶的功能意义。

Adjusting methylation levels with nucleus proportions highlights functional significance of differentially methylated cytosines associated with pre-eclampsia.

机构信息

International Peace Maternal and Child Health Hospital, School of Medicine, Shanghai Jiao Tong University, Shanghai, China.

Shanghai Key Laboratory of Embryo Original Diseases, Shanghai, China.

出版信息

Mol Hum Reprod. 2024 Oct 12;30(10). doi: 10.1093/molehr/gaae032.

Abstract

Studies on DNA methylation alterations associated with pre-eclampsia (PE) have improved our understanding of the mechanisms underlying this disorder. However, differentially methylated cytosines (DMCs) have not been adjusted for cell-type heterogeneity, hampering the identification of alterations that drive disease risk. Using a reference-based, cell-type deconvolution approach, we estimated the nuclear proportions of 335 placental samples based on DNA methylation data. We found that the nuclei of total trophoblast lineages accounted for more than 80% of the placental samples, with a significant increase in PE placentas. The nuclear proportions of stromal and Hofbauer cells decreased in PE placentas. Our nuclear proportion estimation reflected previous histological knowledge on the changes in cell type proportions in PE placentas. We corrected 2125 DMCs associated with early-onset PE for cell-type heterogeneity by adjusting for the nuclear proportions and observed a notable reduction in the association signals, with 145 probes not reaching epigenome-wide significance. After correction, the top 200 significant DMCs were strongly enriched in active enhancers in trophoblast lineages, whereas 145 non-significant probes were enriched in regions with a quiescent state of chromatin. Our results suggest that future epigenetic studies of PE should focus on functional regulatory sequences.

摘要

与子痫前期(PE)相关的 DNA 甲基化改变的研究提高了我们对这种疾病发病机制的理解。然而,差异甲基化胞嘧啶(DMC)尚未针对细胞类型异质性进行调整,这阻碍了对驱动疾病风险的改变的识别。我们使用基于参考的细胞类型去卷积方法,根据 DNA 甲基化数据估计了 335 个胎盘样本的核比例。我们发现,总滋养层谱系的核比例超过了 80%的胎盘样本,PE 胎盘中的核比例显著增加。PE 胎盘中的基质和成纤维细胞的核比例减少。我们的核比例估计反映了关于 PE 胎盘中细胞类型比例变化的先前组织学知识。我们通过调整核比例纠正了与早发型 PE 相关的 2125 个 DMC 与细胞类型异质性的关联,观察到关联信号明显减少,有 145 个探针未达到全基因组显著水平。校正后,前 200 个显著的 DMC 在滋养层谱系的活性增强子中强烈富集,而 145 个非显著探针在染色质静止状态的区域中富集。我们的研究结果表明,未来对 PE 的表观遗传学研究应集中在功能调节序列上。

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