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Genetic ablation of Rest leads to in vitro-specific derepression of neuronal genes during neurogenesis

机译:休息的遗传消融导致神经发生过程中神经元基因的体外特异性抑制。

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Rest (RE1-silencing transcription factor, also called Nrsf) is involved in the maintenance of the undifferentiated state of neuronal stem/progenitor cells in vitro by preventing precocious expression of neuronal genes. However, the function of Rest during neurogenesis in vivo remains to be elucidated because of the early embryonic lethal phenotype of conventional Rest knockout mice. In the present study, we have generated Rest conditional knockout mice, which allow the effect of genetic ablation of Rest during embryonic neurogenesis to be examined in vivo. We show that Rest plays a role in suppressing the expression of neuronal genes in cultured neuronal cells in vitro, as well as in non-neuronal cells outside of the central nervous system, but that it is dispensable for embryonic neurogenesis in vivo. Our findings highlight the significance of extrinsic signals for the proper intrinsic regulation of neuronal gene expression levels in the specification of cell fate during embryonic neurogenesis in vivo.
机译:Rest(RE1沉默转录因子,也称为Nrsf)通过防止神经元基因过早表达,参与了体外神经元干/祖细胞未分化状态的维持。但是,由于传统的Rest基因敲除小鼠的早期胚胎致死表型,在体内神经发生过程中Rest的功能仍有待阐明。在本研究中,我们已经产生了Rest条件性基因敲除小鼠,可以在体内检查胚胎神经发生过程中Rest基因的遗传消融作用。我们显示Rest在抑制体外培养的神经元细胞以及中枢神经系统外的非神经元细胞中神经元基因的表达中发挥作用,但它对于体内胚胎神经发生是必不可少的。我们的发现突出了外在信号对体内胚胎神经发生过程中细胞命运的规范中神经元基因表达水平的适当内在调节的重要性。

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