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首页> 外文期刊>BMC Molecular Biology >Liver-enriched transcription factors are critical for the expression of hepatocyte marker genes in mES-derived hepatocyte-lineage cells
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Liver-enriched transcription factors are critical for the expression of hepatocyte marker genes in mES-derived hepatocyte-lineage cells

机译:富含肝脏的转录因子对于mES来源的肝细胞系细胞中肝细胞标志物基因的表达至关重要

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摘要

Background Induction of stem cell differentiation toward functional hepatocytes is hampered by lack of knowledge of the hepatocyte differentiation processes. The overall objective of this project is to characterize key stages in the hepatocyte differentiation process.Results We established a mouse embryonic stem (mES) cell culture system which exhibited changes in gene expression profiles similar to those observed in the development of endodermal and hepatocyte-lineage cells previously described in the normal mouse embryo. Transgenic mES cells were established that permitted isolation of enriched hepatocyte-lineage populations. This approach has isolated mES-derived hepatocyte-lineage cells that express several markers of mature hepatocytes including albumin, glucose-6-phosphatase, tyrosine aminotransferase, cytochrome P450-3a, phosphoenolpyruvate carboxykinase and tryptophan 2,3-dioxygenase. In addition, our results show that the up-regulation of the expression levels of hepatocyte nuclear factor-3α, -4α, -6, and CCAAT-enhancer binding protein-β might be critical for passage into late-stage differentiation towards functional hepatocytes. These data present important steps for definition of regulatory phenomena that direct specific cell fate determination.Conclusion The mES cell culture system generated in this study provides a model for studying transition between stages of the hepatocyte development and has significant potential value for studying the molecular basis of hepatocyte differentiation in vitro.
机译:背景技术由于缺乏对肝细胞分化过程的了解,阻碍了干细胞向功能性肝细胞分化的诱导。该项目的总体目标是表征肝细胞分化过程中的关键阶段。结果我们建立了小鼠胚胎干(mES)细胞培养系统,该系统表现出与内胚层和肝细胞谱系发育相似的基因表达谱变化先前在正常小鼠胚胎中描述的细胞。建立了可分离富集肝细胞谱系种群的转基因mES细胞。该方法已分离出表达了成熟肝细胞的几种标志物的mES衍生的肝细胞谱系细胞,这些标志物包括白蛋白,葡萄糖6磷酸酶,酪氨酸转氨酶,细胞色素P450-3a,磷酸烯醇丙酮酸羧激酶和色氨酸2,3-双加氧酶。此外,我们的研究结果表明,肝细胞核因子-3α,-4α,-6和CCAAT增强子结合蛋白-β的表达水平上调对于晚期分化为功能性肝细胞可能至关重要。这些数据为定义指导特定细胞命运确定的调控现象提供了重要步骤。结论本研究产生的mES细胞培养系统为研究肝细胞发育各阶段之间的过渡提供了模型,并且对于研究肝细胞的分子基础具有重要的潜在价值。体外肝细胞分化。

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