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Transcription factor heterogeneity and epiblast pluripotency

机译:转录因子异质性和上皮多能性

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摘要

Stem cells are defined by the simultaneous possession of the seemingly incongruent properties of selfrenewal and multi-lineage differentiation potential. To maintain a stem cell population, these opposing forces must be balanced. Transcription factors that function to direct pluripotent cell identity are not all equally distributed throughout the pluripotent cell population. While Oct4 levels are relatively homogeneous, other transcription factors, such as Nanog, are more heterogeneously expressed. Moreover, Oct4 positive cells fluctuate between states of high Nanog expression associated with a high probability of self-renewal and low Nanog expression associated with an increased propensity to differentiate. As embryonic stem (ES) cells transit to the more developmentally advanced epiblast stem cell (EpiSC) state, the levels of pluripotency transcription factors are modulated. Such modulations are blunted in cells that overexpress Nanog and this may underlie the resistance of Nanog-overexpressing cells to transit to an EpiSC state. Interestingly, increasing the levels of Nanog in EpiSC can facilitate reversion to the ES cell state. Together these observations suggest that Nanog lies close to the top of the hierarchy of pluripotent transcription factor regulation.
机译:通过同时拥有自我更新和多谱系分化潜能的看似不一致的特性来定义干细胞。为了维持干细胞种群,必须平衡这些对立的力量。用于指导多能细胞特性的转录因子并非在整个多能细胞群体中均等分布。虽然Oct4的水平相对均一,但其他转录因子(例如Nanog)的异质表达却更多。此外,Oct4阳性细胞在高Nanog表达状态(与自我更新的可能性高相关)和低Nanog表达状态(与增加的分化倾向相关)之间波动。随着胚胎干(ES)细胞过渡到发育更先进的表皮干细胞(EpiSC)状态,多能性转录因子的水平得到调节。在过度表达Nanog的细胞中,这种调节变得迟钝,这可能是过度表达Nanog的细胞向EpiSC状态转变的抵抗力的基础。有趣的是,增加EpiSC中Nanog的水平可以促进回复ES细胞状态。这些观察结果共同表明,Nanog靠近多能转录因子调控体系的顶层。

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