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首页> 外文期刊>Developmental biology >A transition from SoxB1 to SoxE transcription factors is essential for progression from pluripotent blastula cells to neural crest cells
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A transition from SoxB1 to SoxE transcription factors is essential for progression from pluripotent blastula cells to neural crest cells

机译:从SOXB1转移到SOXE转录因子的转变对于从多能爆破细胞到神经顶部细胞的进展至关重要

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摘要

The neural crest is a stem cell population unique to vertebrate embryos that gives rise to derivatives from multiple embryonic germ layers. The molecular underpinnings of potency that govern neural crest potential are highly conserved with that of pluripotent blastula stem cells, suggesting that neural crest cells may have evolved through retention of aspects of the pluripotency gene regulatory network (GRN). A striking difference in the regulatory factors utilized in pluripotent blastula cells and neural crest cells is the deployment of different subfamilies of Sox transcription factors; SoxB1 factors play central roles in the pluripotency of naive blastula and ES cells, whereas neural crest cells require SoxE function. Here we explore the shared and distinct activities of these factors to shed light on the role that this molecular hand-off of Sox factor activity plays in the genesis of neural crest and the lineages derived from it. Our findings provide evidence that SoxB1 and SoxE factors have both overlapping and distinct activities in regulating pluripotency and lineage restriction in the embryo. We hypothesize that SoxE factors may transiently replace SoxB1 factors to control pluripotency in neural crest cells, and then poise these cells to contribute to glial, chondrogenic and melanocyte lineages at stages when SoxB1 factors promote neuronal progenitor formation.
机译:神经嵴是脊椎动物胚胎独有的干细胞群,其产生来自多个胚胎胚层的衍生物。神经波峰潜力的效力的分子支撑性具有高度保守的,具有多能突发干细胞的高度保守,这表明神经嵴细胞可以通过保留多能基因调节网络(GRN)的方面来演变。在多能Bustrula细胞和神经嵴细胞中使用的调节因素的显着差异是部署SOX转录因子的不同亚壳; SOXB1因素在幼稚Blastula和ES细胞的多能性中起中央角色,而神经嵴细胞需要SOXE功能。在这里,我们探讨了这些因素的共享和不同活动,以阐明这种分子交给SOx因子活动在神经嵴的成因中发挥的作用以及源自血管的作用。我们的调查结果提供了证据表明SOXB1和SOXE因子在调节胚胎中的多能性和谱系限制方面具有重叠和不同的活动。我们假设SOXE因子可能瞬间替代神经顶部细胞中的索X1因素来控制多能性,然后在SOxB1因素促进神经元祖细胞形成时,将这些细胞促进胶质,软骨菌和黑素细胞谱系。

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