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Human pluripotent stem cell derived HLC transcriptome data enables molecular dissection of hepatogenesis

机译:人类多能干细胞来源的HLC转录组数据可实现肝发生的分子解剖

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Induced pluripotent stem cells (iPSCs) and human embryonic stem cells (hESCs) differentiated into hepatocyte-like cells (HLCs) provide a defined and renewable source of cells for drug screening, toxicology and regenerative medicine. We previously reprogrammed human fetal foreskin fibroblast cells (HFF1) into iPSCs employing an episomal plasmid-based integration-free approach, this iPSC-line and the hESC lines H1 and H9 were used to model hepatogenesis in vitro. Biochemical characterisation confirmed glycogen storage, ICG uptake and release, urea and bile acid production, as well as CYP3A4 activity. Microarray-based transcriptome analyses was carried out using RNA isolated from the undifferentiated pluripotent stem cells and subsequent differentiation stages- definitive endoderm (DE) hepatic endoderm (HE) and HLCs. K-means identified 100 distinct clusters, for example, POU5F1/OCT4 marking the undifferentiated stage, SOX17 the DE stage, HNF4α the HE stage, and ALB specific to HLCs, fetal liver and primary human hepatocytes (PHH). This data descriptor describes these datasets which should be useful for gaining new insights into the molecular basis of hepatogenesis and associated gene regulatory networks.
机译:诱导多能干细胞(iPSC)和分化成肝细胞样细胞(HLC)的人类胚胎干细胞(hESC)为药物筛选,毒理学和再生医学提供了确定的可再生细胞来源。我们以前使用基于游离质粒的无整合方法将人胎儿包皮成纤维细胞(HFF1)重编程为iPSC,此iPSC系和hESC系H1和H9用于体外肝生成模型。生化特征证实了糖原的储存,ICG的吸收和释放,尿素和胆汁酸的产生以及CYP3A4的活性。基于芯片的转录组分析是使用从未分化的多能干细胞以及随后的分化阶段(定形内胚层(DE),肝内胚层(HE)和HLC)分离的RNA进行的。 K-均值确定了100个不同的簇,例如标记未分化阶段的POU5F1 / OCT4,DE阶段的SOX17,HE阶段的HNF4α和HLC,胎儿肝脏和原代人肝细胞(PHH)特异的ALB。该数据描述符描述了这些数据集,这些数据集可用于获得对肝发生和相关基因调控网络的分子基础的新见解。

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