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Control over single-cell distribution of G1 lengths by WNT governs pluripotency

机译:通过WNT控制G1长度的单细胞分布可控制多能性

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摘要

The link between single-cell variation and population-level fate choices lacks a mechanistic explanation despite extensive observations of gene expression and epigenetic variation among individual cells. Here, we found that single human embryonic stem cells (hESCs) have different and biased differentiation potentials toward either neuroectoderm or mesendoderm depending on their G1 lengths before the onset of differentiation. Single-cell variation in G1 length operates in a dynamic equilibrium that establishes a G1 length probability distribution for a population of hESCs and predicts differentiation outcome toward neuroectoderm or mesendoderm lineages. Although sister stem cells generally share G1 lengths, a variable proportion of cells have asymmetric G1 lengths, which maintains the population dispersion. Environmental Wingless-INT (WNT) levels can control the G1 length distribution, apparently as a means of priming the fate of hESC populations once they undergo differentiation. As a downstream mechanism, global 5-hydroxymethylcytosine levels are regulated by G1 length and thereby link G1 length to differentiation outcomes of hESCs. Overall, our findings suggest that intrapopulation heterogeneity in G1 length underlies the pluripotent differentiation potential of stem cell populations.
机译:尽管广泛观察到单个细胞之间的基因表达和表观遗传变异,但单细胞变异与种群水平的命运选择之间的联系缺乏机械的解释。在这里,我们发现单个人胚胎干细胞(hESCs)取决于分化开始前的G1长度,朝着神经外胚层或中胚层的分化潜能不同。 G1长度的单细胞变化在动态平衡中起作用,该动态平衡为hESC群体建立了G1长度概率分布,并预测了向神经外胚层或中胚层谱系的分化结果。尽管姐妹干细胞通常共享G1长度,但可变比例的细胞具有不对称的G1长度,从而保持了种群分散。 Wingless-INT(WNT)的环境水平可以控制G1长度的分布,这显然是引发hESC种群分化后命运的一种手段。作为下游机制,总的5-羟甲基胞嘧啶水平受G1长度调节,从而将G1长度与hESC的分化结果联系起来。总体而言,我们的发现表明,G1长度的种群内异质性是干细胞群体多能分化潜能的基础。

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