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基于母体血浆游离DNA核小体足迹的基因表达谱表明,在孕期进展过程中胎儿发育及母体免疫发生了变化。

Gene expression profiles based on maternal plasma cfDNA nucleosome footprints indicate fetal development and maternal immunity changes during pregnancy progress.

作者信息

Zhang Min, Li Kun, Huang Xiang, Zhou Huiling, Tan Jiayu, Guo Zhiwei, Wei Xingyu, Liu Yuming, Weng Shi, Ouyang Guojun, Yang Xuexi, Hao Wenbo, Li Fenxia

机构信息

Institute of Antibody Engineering, School of Laboratory Medicine and Biotechnology, Southern Medical University, 1838 N. Guangzhou Ave, Guangzhou, 510515, PR China.

Laboratory of Molecular Diagnostics, Affiliated Foshan Maternity & Child Healthcare Hospital, Southern Medical University, PR China.

出版信息

Placenta. 2025 Jan;159:84-92. doi: 10.1016/j.placenta.2024.12.005. Epub 2024 Dec 10.

Abstract

BACKGROUND

Pregnancy significantly alters the maternal immune system, affecting fetal development. The collection of tissues from the human placenta and fetus is not ethically or practically feasible at various gestational stages, thus limiting the study of gene expression in the fetus and placenta. Recent studies have shown that plasma cell-free DNA (cfDNA) nucleosome patterns can predict gene expression in the source tissue, offering insights into an individual's health status. This study aimed to identify pregnancy-related gene expression changes across gestational periods using cfDNA nucleosome distribution to understand fetal development and maternal immune changes.

METHODS

Plasma samples were collected from 150 healthy pregnant women in different trimesters (early, mid, and late) and 32 healthy nonpregnant women. The correlation between gene expression and physiological changes during pregnancy was evaluated by inferring differential expression profiles around the transcription start site (TSS) using cfDNA nucleosome distribution patterns obtained through whole-genome sequencing. We utilized Gene Ontology (GO) and Kyoto Encyclopedia of Genes and Genomes (KEGG) enrichment analyses to annotate differentially expressed genes with the mother and fetus.

RESULTS

We identified gene expression changes that support the regulation of fetal development and immune system function during pregnancy. Differential coverage genes were mainly enriched in pathways related to transcription and translation, organic compound metabolism, and immune regulation. In addition, differentially expressed genes with significant temporal trends were identified. Among them, the upregulated differential genes were mainly related to development, whereas those with downregulated trends were mainly related to the immune system response. This indicates that differential changes of the placenta and maternal are significantly correlated with the pregnancy status.

DISCUSSION

This study demonstrated the differential gene expression represented by the characteristic distribution of cfDNA nucleosome in maternal peripheral blood can effectively capture significant changes in maternal immunity and fetal development throughout pregnancy stages. It may help identify abnormal gene expression patterns associated with complications in pregnancy and childbirth, enhancing the quality of life and safety for both mother and fetus.

摘要

背景

妊娠会显著改变母体免疫系统,影响胎儿发育。在不同妊娠阶段,从人胎盘和胎儿采集组织在伦理或实际操作上并不可行,因此限制了对胎儿和胎盘基因表达的研究。最近的研究表明,血浆游离DNA(cfDNA)核小体模式可以预测源组织中的基因表达,从而深入了解个体的健康状况。本研究旨在利用cfDNA核小体分布来识别整个妊娠期与妊娠相关的基因表达变化,以了解胎儿发育和母体免疫变化。

方法

收集了150名处于不同孕期(早期、中期和晚期)的健康孕妇以及32名健康非孕妇的血浆样本。通过全基因组测序获得cfDNA核小体分布模式,推断转录起始位点(TSS)周围的差异表达谱,评估妊娠期间基因表达与生理变化之间的相关性。我们利用基因本体论(GO)和京都基因与基因组百科全书(KEGG)富集分析对母体和胎儿的差异表达基因进行注释。

结果

我们识别出了支持妊娠期间胎儿发育和免疫系统功能调节的基因表达变化。差异覆盖基因主要富集在与转录和翻译、有机化合物代谢以及免疫调节相关的途径中。此外,还识别出了具有显著时间趋势的差异表达基因。其中,上调的差异基因主要与发育相关,而呈下调趋势的基因主要与免疫系统反应相关。这表明胎盘和母体的差异变化与妊娠状态显著相关。

讨论

本研究表明,母体外周血中cfDNA核小体特征分布所代表的差异基因表达能够有效捕捉整个妊娠阶段母体免疫和胎儿发育的显著变化。它可能有助于识别与妊娠和分娩并发症相关的异常基因表达模式,提高母亲和胎儿的生活质量和安全性。

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