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Generation of Human Embryonic Stem Cell Reporter Lines Expressing GFP Specifically in Neural Progenitors

机译:专门在神经祖细胞中表达GFP的人类胚胎干细胞报告基因系的生成

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Generation of lineage-specific human embryonic stem cell (hESC) reporter lines will facilitate the real time monitoring of differentiation in live cells and the identification of factors governing these processes. It will also enable researchers to purify specific cell populations from heterogeneous differentiated hESC progeny. Here we report the generation of clonally derived nestin-EGFP reporter hESC lines that express GFP under the control of the neuroepithelial specific nestin 2nd intron enhancer. We show that the nestin-EGFP hESC reporter lines retain the features of undifferentiated hESCs, are able to self-renew in hESC culture conditions and to differentiate into cells of all three germ layers. The nestin-EGFP reporter exhibited high expression in neural progenitor cells upon differentiation, although it is detectable at a low level in the undifferentiated state. Furthermore, the expression of the transgene is exclusively confined to the neural progenitors after differentiation. The specific expression of the transgene is determined by collaborative binding motifs of POU and SOX transcription factors in the nestin enhancer. Deletion of either of the binding elements resulted in a significant reduction of enhancer/promoter activity. Taken together, the nestin-EGFP reporter hESC lines are invaluable not only for the study of the neural differentiation process from hESCs but also for the enrichment of neural progenitor cells from other cell lineages.
机译:谱系特异性的人类胚胎干细胞(hESC)报告基因系的产生将促进实时监测活细胞的分化并确定控制这些过程的因素。它还将使研究人员能够从异质分化的hESC后代中纯化特定的细胞群。在这里,我们报道了在神经上皮特异性巢蛋白第二内含子增强子的控制下表达GFP的克隆衍生巢蛋白-EGFP报告基因hESC系的生成。我们表明,巢蛋白EGFP hESC报告人行保留未分化的hESCs的功能,能够在hESC培养条件下自我更新,并分化成所有三个胚层的细胞。虽然在未分化状态下可以低水平检测到巢蛋白-EGFP报告基因,但在分化后在神经祖细胞中显示出高表达。此外,转基因的表达在分化后仅限于神经祖细胞。转基因的特异性表达取决于巢蛋白增强子中POU和SOX转录因子的协同结合基序。任一结合元件的缺失导致增强子/启动子活性的显着降低。综上所述,巢蛋白-EGFP报告基因hESC系不仅对于研究hESC的神经分化过程,而且对于丰富其他细胞系的神经祖细胞具有重要的价值。

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