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Snail Coordinately Regulates Downstream Pathways to Control Multiple Aspects of Mammalian Neural Precursor Development

机译:蜗牛协调调节下游途径以控制哺乳动物神经前体发育的多个方面。

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摘要

The Snail transcription factor plays a key role in regulating diverse developmental processes but is not thought to play a role in mammalian neural precursors. Here, we have examined radial glial precursor cells of the embryonic murine cortex and demonstrate that Snail regulates their survival, self-renewal, and differentiation into intermediate progenitors and neurons via two distinct and separable target pathways. First, Snail promotes cell survival by antagonizing a p53-dependent death pathway because coincident p53 knockdown rescues survival deficits caused by Snail knockdown. Second, we show that the cell cycle phosphatase Cdc25b is regulated by Snail in radial precursors and that Cdc25b coexpression is sufficient to rescue the decreased radial precursor proliferation and differentiation observed upon Snail knockdown. Thus, Snail acts via p53 and Cdc25b to coordinately regulate multiple aspects of mammalian embryonic neural precursor biology.
机译:Snail转录因子在调节各种发育过程中起关键作用,但认为在哺乳动物神经前体中不起作用。在这里,我们检查了胚胎鼠皮层的放射状胶质前体细胞,并证明Snail通过两个不同且可分离的靶途径调节其存活,自我更新和分化为中间祖细胞和神经元。首先,Snail通过拮抗p53依赖的死亡途径来促进细胞存活,因为同时发生的p53击倒可挽救Snail击倒导致的生存缺陷。其次,我们表明细胞周期磷酸酶Cdc25b在径向前体中受Snail调控,并且Cdc25b共表达足以挽救在Snail敲除后观察到的径向前体增殖和分化的降低。因此,Snail通过p53和Cdc25b发挥作用来协调调节哺乳动物胚胎神经前体生物学的多个方面。

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