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首页> 外文期刊>Scientific reports. >Deciphering transcriptional regulation in human embryonic stem cells specified towards a trophoblast fate
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Deciphering transcriptional regulation in human embryonic stem cells specified towards a trophoblast fate

机译:解入对滋养品命运的人胚胎干细胞中的转录调节

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Differentiated human embryonic stem cells (hESC) continue to provide a model for studying early trophoblast cells (TB), but many questions have been raised regarding their true identity. Therefore, we carried out a global and unbiased analysis on previously published transcriptomic profiles for hESC differentiated to TB by means of bone morphogenetic protein-4 and inhibitors of activin A and fibroblast growth factor-2 signaling (BAP treatment). Our results confirm that BAP treated hESC (ESCd) lack a mesoderm signature and are a subtype of placental cells unlike those present at term. ESCd display a high level of expression of genes implicated in migration and invasion compared to commonly used, immortalized TB cell lines and primary cells from term placenta. Co-expression network analysis also identified gene modules involved in cell migration and adhesion, processes that are likely critical during the beginning stages of placentation. Finally, protein-protein interaction analysis predicted several additional genes that may play important roles in early stages of placental development. Together, our analyses provide novel insights into the transcriptional programs that are active in ESCd.
机译:分化的人胚胎干细胞(HESC)继续提供用于研究早期滋养细胞(TB)的模型,但是已经提出了许多问题关于其真实身份。因此,我们对通过骨形态发生蛋白-4和活素A和成纤维细胞生长因子-2信号传导(BAP处理)的骨形态发生蛋白-4和抑制剂来对先前公布的HERC转录组分布的全局和无偏异分析。我们的结果证实,BAP处理的HESC(ESCD)缺乏中胚层特征,并且是胎盘细胞的亚型,与术语目前的那些。 ESCD显示与术语胎儿术语的常用,永生的TB细胞系和原代细胞相比,涉及迁移和侵袭的基因的高水平表达。共表达网络分析还鉴定了涉及细胞迁移和粘附的基因模块,在置入的开始阶段可能临时的过程。最后,蛋白质 - 蛋白质相互作用分析预测了几种可能在胎盘开发早期阶段起到重要作用的额外基因。我们的分析在一起,对ESCD中活跃的转录计划提供了新的见解。

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