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Two distinct mechanisms silence chinmo in Drosophila neuroblasts and neuroepithelial cells to limit their self-renewal

机译:两种不同的机制沉默中间在果蝇神经细胞和神经头脑细胞中的自我更新限制

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Whether common principles regulate the self-renewing potential of neural stem cells (NSCs) throughout the developing central nervous system is still unclear. In the Drosophila ventral nerve cord and central brain, asymmetrically dividing NSCs, called neuroblasts (NBs), progress through a series of sequentially expressed transcription factors that limits self-renewal by silencing a genetic module involving the transcription factor Chinmo. Here, we find that Chinmo also promotes neuroepithelium growth in the optic lobe during early larval stages by boosting symmetric self-renewing divisions while preventing differentiation. Neuroepithelium differentiation in late larvae requires the transcriptional silencing of chinmo by ecdysone, the main steroid hormone, therefore allowing coordination of neural stem cell self-renewal with organismal growth. In contrast, chinmo silencing in NBs is post-transcriptional and does not require ecdysone. Thus, during Drosophila development, humoral cues or tissue-intrinsic temporal specification programs respectively limit self-renewal in different types of neural progenitors through the transcriptional and post-transcriptional regulation of the same transcription factor.
机译:常见原理是否调节神经干细胞(NSCs)的自我更新潜力在整个显影中枢神经系统中尚不清楚。在果蝇腹侧神经帘线和中央大脑中,不对称地分开NSCs,称为神经细胞(NBS),通过一系列顺序表达的转录因子进行,这些转录因子通过沉默涉及转录因子Chinmo的遗传模块来限制自我更新。在这里,我们发现Chinmo在预防分化的同时通过提高对称的自我更新分区,在早期幼虫阶段也促进了视神经头脑中的神经脑卒中。晚期幼虫的神经沉皮细胞分化需要通过蜕皮酮,主要类固醇激素进行ChinMo的转录沉默,因此允许与有机体生长协调神经干细胞自我更新。相比之下,中间在NBS中的Chinmo沉默是转录后的,不需要蜕皮酮。因此,在果蝇发育期间,体液提示或组织内在时间规范程序通过对不同转录因子的转录和转录后调节来分别限制不同类型的神经祖细胞的自我更新。

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