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首页> 外文期刊>Nature Communications >Lin28a regulates neuronal differentiation and controls miR-9 production
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Lin28a regulates neuronal differentiation and controls miR-9 production

机译:Lin28a调节神经元分化并控制miR-9的产生

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摘要

microRNAs shape the identity and function of cells by regulating gene expression. It is known that brain-specific miR-9 is controlled transcriptionally; however, it is unknown whether posttranscriptional processes contribute to establishing its levels. Here we show that miR-9 is regulated transcriptionally and post-transcriptionally during neuronal differentiation of the embryonic carcinoma cell line P19. We demonstrate that miR-9 is more efficiently processed in differentiated than in undifferentiated cells. We reveal that Lin28a affects miR-9 by inducing the degradation of its precursor through a uridylation-independent mechanism. Furthermore, we show that constitutively expressed untagged but not GFP-tagged Lin28a decreases differentiation capacity of P19 cells, which coincides with reduced miR-9 levels. Finally, using an inducible system we demonstrate that Lin28a can also reduce miR-9 levels in differentiated P19 cells. Together, our results shed light on the role of Lin28a in neuronal differentiation and increase our understanding of the mechanisms regulating the level of brain-specific microRNAs.
机译:microRNA通过调节基因表达来塑造细胞的身份和功能。已知大脑特异性的miR-9受转录控制。但是,转录后过程是否有助于建立其水平尚不清楚。在这里,我们显示miR-9在胚胎癌细胞系P19的神经元分化过程中受到转录和转录后调控。我们证明,在未分化细胞中,miR-9在分化细胞中的处理效率更高。我们揭示了Lin28a通过与尿嘧啶无关的机制诱导其前体降解,从而影响miR-9。此外,我们显示组成性表达的未标记但未标记GFP的Lin28a降低了P19细胞的分化能力,这与降低的miR-9水平相吻合。最后,使用诱导型系统,我们证明Lin28a还可以降低分化的P19细胞中的miR-9水平。在一起,我们的结果揭示了Lin28a在神经元分化中的作用,并加深了我们对调节大脑特异性microRNA水平的机制的了解。

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