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首页> 外文期刊>Stem cells and development >Increased levels of FoxA1 transcription factor in pluripotent P19 embryonal carcinoma cells stimulate neural differentiation.
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Increased levels of FoxA1 transcription factor in pluripotent P19 embryonal carcinoma cells stimulate neural differentiation.

机译:多能P19胚胎癌细胞中FoxA1转录因子水平的增加刺激神经分化。

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Transcription factor FoxA1 plays a critical role during embryonic development and is activated during retinoic acid (RA)-induced neural differentiation of pluripotent P19 embryonal carcinoma cells at the early stage, which is marked by decreased expression of Nanog and increased expression of neural stem cell marker Nestin. To further understand how FoxA1 mediates neural differentiation, we have overexpressed FoxA1 through an adenovirus vector in P19 cells and identified that early neurogenesis-related sonic hedgehog (Shh) gene is activated directly by FoxA1. Knockdown of FoxA1 expression during P19 cell neural differentiation results in prevention of Shh and Nestin induction. FoxA1 binds to Shh promoter at -486 to -462 bp region and activates the promoter in cotransfection assays. Furthermore, overexpression of FoxA1 alone in P19 cells stimulates expression of Nestin and results in decreased protein levels of Nanog. During RA-induced P19 cell differentiation, elevated levels of FoxA1 increase the population of neurons, evidenced by stimulated expression of neuron-specific Neurofilament-1 and Tubulin betaIII. Together, our results suggest a critical involvement of FoxA1 in stimulating neural differentiation of pluripotent stem cells at early stages.
机译:转录因子FoxA1在胚胎发育中起关键作用,并在视黄酸(RA)诱导的多能P19胚胎癌细胞早期神经分化过程中被激活,其特征在于Nanog的表达降低和神经干细胞标记物的表达增加巢蛋白为了进一步了解FoxA1如何介导神经分化,我们已经通过P19细胞中的腺病毒载体过表达FoxA1,并确定了早期的神经发生相关声波刺猬(Shh)基因被FoxA1直接激活。在P19细胞神经分化过程中抑制FoxA1表达可预防Shh和Nestin的诱导。 FoxA1在-486至-462 bp区域与Shh启动子结合,并在共转染试验中激活该启动子。此外,单独的FoxA1在P19细胞中的过表达刺激了Nestin的表达,并导致Nanog的蛋白质水平降低。在RA诱导的P19细胞分化过程中,FoxA1的水平升高会增加神经元的数量,这可通过神经元特异性Neurofilament-1和Tubulin betaIII的刺激表达来证明。在一起,我们的结果表明FoxA1在早期阶段多能干细胞的神经分化的关键参与。

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