首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Repressor element 1 silencing transcription factor (REST) controls radial migration and temporal neuronal specification during neocortical development
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Repressor element 1 silencing transcription factor (REST) controls radial migration and temporal neuronal specification during neocortical development

机译:抑制因子1沉默转录因子(REST)控制新皮层发育期间的径向迁移和颞神经元规范

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摘要

Neurogenesis requires mechanisms that coordinate early cell-fate decisions, migration, and terminal differentiation. Here, we show that the transcriptional repressor, repressor element 1 silencing transcription factor (REST), regulates radial migration and the timing of neural progenitor differentiation during neocortical development, and that the regulation is contingent upon differential REST levels. Specifically, a sustained presence of REST blocks migration and greatly delays—but does not prevent—neuronal differentiation, resulting in a subcortical band heterotopia-like phenotype, reminiscent of loss of doublecortin. We further show that doublecortin is a direct gene target of REST, and that its overexpression rescues, at least in part, the aberrant phenotype caused by persistent presence of REST. Our studies support the view that the targeted down-regulation of REST to low levels in neural progenitors, and its subsequent disappearance during neurogenesis, is critical for timing the spatiotemporal transition of neural progenitor cells to neurons.
机译:神经发生需要协调早期细胞命运决定,迁移和终末分化的机制。在这里,我们表明,转录阻遏物,阻遏物元件1沉默转录因子(REST),调节了新皮层发育过程中的径向迁移和神经祖细胞分化的时机,并且该调节取决于不同的REST水平。特别是,持续存在的REST会阻止迁移,并极大地延迟(但不能阻止)神经元分化,从而导致皮层下带异位症样表型,使人联想到双皮质素的丢失。我们进一步表明,双皮质素是REST的直接基因靶标,并且它的过表达至少部分挽救了由REST的持续存在引起的异常表型。我们的研究支持这样的观点,即在神经祖细胞中将REST有针对性地下调至低水平,以及随后在神经发生过程中消失,对于定时神经祖细胞向神经元的时空过渡至关重要。

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