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Higher chromatin mobility supports totipotency and precedes pluripotency in vivo

机译:较高的染色质迁移率可支持全能并在体内先​​于多能性

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摘要

The fusion of the gametes upon fertilization results in the formation of a totipotent cell. Embryonic chromatin is expected to be able to support a large degree of plasticity. However, whether this plasticity relies on a particular conformation of the embryonic chromatin is unknown. Moreover, whether chromatin plasticity is functionally linked to cellular potency has not been addressed. Here, we adapted fluorescence recovery after photobleaching (FRAP) in the developing mouse embryo and show that mobility of the core histones H2A, H3.1, and H3.2 is unusually high in two-cell stage embryos and decreases as development proceeds. The transition toward pluripotency is accompanied by a decrease in histone mobility, and, upon lineage allocation, pluripotent cells retain higher mobility than the differentiated trophectoderm. Importantly, totipotent two-cell-like embryonic stem cells also display high core histone mobility, implying that reprogramming toward totipotency entails changes in chromatin mobility. Our data suggest that changes in chromatin dynamics underlie the transitions in cellular plasticity and that higher chromatin mobility is at the nuclear foundations of totipotency.
机译:受精后配子融合导致全能细胞的形成。期望胚胎染色质能够支持很大程度的可塑性。然而,这种可塑性是否依赖于胚胎染色质的特定构型尚不清楚。此外,尚未探讨染色质可塑性是否在功能上与细胞效能有关。在这里,我们适应了发展中的小鼠胚胎中光漂白(FRAP)后的荧光恢复,并表明核心组蛋白H2A,H3.1和H3.2的迁移率在两细胞阶段的胚胎中异常高,并且随着发育的进行而降低。向多能性的转变伴随着组蛋白迁移率的降低,并且在谱系分配中,多能细胞比分化的滋养外胚层保留更高的迁移率。重要的是,全能的两细胞样胚胎干细胞也显示出高的核心组蛋白迁移率,这意味着向全能性重新编程必然导致染色质迁移率发生变化。我们的数据表明,染色质动力学的变化是细胞可塑性转变的基础,而较高的染色质迁移率是全能性的核基础。

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