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Transcriptomic analysis reveals differential gene expression, alternative splicing, and novel exons during mouse trophoblast stem cell differentiation

机译:转录组分析显示小鼠滋养层干细胞分化期间的差异基因表达,替代剪接和新的外显子

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Differentiation of mouse trophoblast stem cells (TSCs) to trophoblast giant cells (TGCs) has been widely used as a model system to study placental development and function. While several differentially expressed genes, including regulators of TSC differentiation, have been identified, a comprehensive analysis of the global expression of genes and splice variants in the two cell types has not been reported. Here, we report ~?7800 differentially expressed genes in TGCs compared to TSCs which include regulators of the cell cycle, apoptosis, cytoskeleton, cell mobility, embryo implantation, metabolism, and various signaling pathways. We show that several mitotic proteins, including Aurora A kinase, were downregulated in TGCs and that the activity of Aurora A kinase is required for the maintenance of TSCs. We also identify hitherto undiscovered, cell-type specific alternative splicing events in 31 genes in the two cell types. Finally, we also report 19 novel exons in 12 genes which are expressed in both TSCs and TGCs. Overall, our results uncover several potential regulators of TSC differentiation and TGC function, thereby providing a valuable resource for developmental and molecular biologists interested in the study of stem cell differentiation and embryonic development.
机译:小鼠滋养细胞干细胞(TSC)对滋养细胞巨细胞(TCC)的分化已被广泛用作研究胎盘开发和功能的模型系统。虽然已经鉴定了几种差异表达的基因,包括TSC分化的调节剂,但尚未报告对两种细胞类型中的全局基因表达和剪接变体的全面分析。在这里,与TSCs相比,我们在TGC中报告〜?7800差异表达基因,包括细胞周期,细胞凋亡,细胞骨架,细胞迁移率,胚胎植入,代谢和各种信号通路的调节剂。我们表明,几种有丝分裂蛋白,包括极光激酶,在TGC中下调,并且需要维持TSC的Aurora激酶的活性。我们还在两种细胞类型中识别迄今为止未被发现的细胞型特异性替代剪接事件。最后,我们还在12个基因中报告了19个新的外显子,其在TSC和TGCS中表达。总体而言,我们的结果揭示了TSC分化和TGC功能的几个潜在调节因子,从而为对干细胞分化和胚胎发育的研究感兴趣的发育和分子生物学家提供有价值的资源。

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