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Neurotrophin-3 influences the number and the laminar fate of cortical progenitors in the developing cerebral cortex of mice through the MEK/ERK1/2 signaling pathway

机译:Neurotrophin-3通过MEK / ERK1 / 2信号通路影响小鼠大脑皮质发育中皮质祖细胞的数量和层状命运

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The laminar formation in the developing cerebral cortex requires precisely regulated generation of phenotype-specific neurons. To determine whether neurotrophin-3 (NT3) is involved in this formation, we investigated the effects of NT3 administration in the telencephalic ventricular space on 13.5-day-old mouse embryos. NT3 increased the number of newly generated neurons and altered the neuronal phenotypes in the position and the transcription factors-expression profiles; the neuronal phenotypes originally committed for layer IV neurons were altered toward for layers II/III neurons. The former effects were observed when the parent progenitor cells were exposed to NT3 in the G1- to S-phase, whereas the latter effects were observed with exposure in the G1-phase. In addition, in vitro experiments revealed that the laminar fate alteration by NT3 was observed in the dissociated primary culture of cortical progenitors and the NT3 actions were suppressed by cotreatment with the MEK/ERK inhibitor. These observations suggest that NT3 is involved in the laminar formation of the developing cerebral cortex through the intercellular MEK/ERK pathway.
机译:在发育中的大脑皮层中的层流形成需要精确调节表型特异性神经元的生成。若要确定是否neurotrophin-3(NT3)参与这种形成,我们调查了NT3在端脑室空间中对13.5天大的小鼠胚胎的影响。 NT3增加了新产生的神经元的数量,并改变了位置和转录因子表达谱中的神经元表型。最初提交给第IV层神经元的神经元表型被改变为第II / III层神经元。当亲代祖细胞在G1到S期暴露于NT3时,观察到前者的效果,而在G1期暴露于NT3,则观察到后者的效果。此外,体外实验表明,在分离的皮质祖细胞原代培养物中观察到了NT3的层状命运改变,并且通过与MEK / ERK抑制剂共同处理抑制了NT3的作用。这些观察结果表明NT3通过细胞间MEK / ERK途径参与了发育中的大脑皮层的层状形成。

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