首页> 美国卫生研究院文献>Frontiers in Neurology >The Silencing Effect of microRNA miR-17 on p21 Maintains the Neural Progenitor Pool in the Developing Cerebral Cortex
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The Silencing Effect of microRNA miR-17 on p21 Maintains the Neural Progenitor Pool in the Developing Cerebral Cortex

机译:microRNA miR-17对p21的沉默作用在发育中的大脑皮层中维持神经祖细胞池

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摘要

Expansion of the neural progenitor pool in the developing cerebral cortex is crucial for controlling brain size, since proliferation defects have been associated with the pathogenesis of microcephaly in humans. Cell cycle regulators play important roles in proliferation of neural progenitors. Here, we show that the cyclin-dependent kinase inhibitor p21 (also called Cdkn1a and Cip1) negatively regulates proliferation of radial glial cells (RGCs) and intermediate progenitors (IPs) in the embryonic mouse cortex. MicroRNA-17 (miR-17) displays reciprocal expressions with p21 in the developing cortex. Opposite to p21, miR-17 promotes expansion of RGCs and IPs, as demonstrated by overexpressing miR-17 precursors and miR-17 sponges that can knock down the endogenous miR-17. Moreover, p21 is a putative target normally silenced by miR-17. Co-expression of miR-17 with p21 is sufficient to rescue the negative regulation of p21 on progenitor proliferation. Our results indicate a mechanism of controlling the neural progenitor pool, which is to suppress p21 by miR-17 in the developing cortex.
机译:神经祖细胞在发育中的大脑皮层中的扩张对于控制大脑的大小至关重要,因为增殖缺陷已与人类小头畸形的发病机理相关。细胞周期调节剂在神经祖细胞的增殖中起重要作用。在这里,我们显示出细胞周期蛋白依赖性激酶抑制剂p21(也称为Cdkn1a和Cip1)对胚胎小鼠皮层中的放射状胶质细胞(RGCs)和中间祖细胞(IPs)的增殖负调控。 MicroRNA-17(miR-17)在发育中的皮层中与p21相互表达。与p21相反,miR-17促进了RGC和IP的扩增,这可以通过过表达miR-17前体和可以敲除内源性miR-17的miR-17海绵来证明。而且,p21是通常被miR-17沉默的推定靶标。 miR-17与p21的共表达足以挽救p21对祖细胞增殖的负调控。我们的结果表明了一种控制神经祖细胞的机制,该机制是通过发育中的皮层中的miR-17抑制p21。

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