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miR-124 function during Ciona intestinalis neuronal development includes extensive interaction with the Notch signaling pathway.

机译:Ciona肠神经元发育过程中的miR-124功能包括与Notch信号通路的广泛相互作用。

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摘要

The nervous system-enriched microRNA miR-124 is necessary for proper nervous system development, although the mechanism remains poorly understood. Here, through a comprehensive analysis of miR-124 and its gene targets, we demonstrate that, in the chordate ascidian Ciona intestinalis, miR-124 plays an extensive role in promoting nervous system development. We discovered that feedback interaction between miR-124 and Notch signaling regulates the epidermal-peripheral nervous system (PNS) fate choice in tail midline cells. Notch signaling silences miR-124 in epidermal midline cells, whereas in PNS midline cells miR-124 silences Notch, Neuralized and all three Ciona Hairy/Enhancer-of-Split genes. Furthermore, ectopic expression of miR-124 is sufficient to convert epidermal midline cells into PNS neurons, consistent with a role in modulating Notch signaling. More broadly, genome-wide target extraction with validation using an in vivo tissue-specific sensor assay indicates that miR-124 shapes neuronal progenitor fields by downregulating non-neural genes, notably the muscle specifier Macho-1 and 50 Brachyury-regulated notochord genes, as well as several anti-neural factors including SCP1 and PTBP1. 3'UTR conservation analysis reveals that miR-124 targeting of SCP1 is likely to have arisen as a shared, derived trait in the vertebrate/tunicate ancestor and targeting of PTBP1 is conserved among bilaterians except for ecdysozoans, while extensive Notch pathway targeting appears to be Ciona specific. Altogether, our results provide a comprehensive insight into the specific mechanisms by which miR-124 promotes neuronal development.
机译:尽管尚不清楚该机制,但富含神经系统的microRNA miR-124对于正常的神经系统发育是必需的。在这里,通过对miR-124及其基因靶点的全面分析,我们证明了在绒毛状海藻Ciona intestinalis中,miR-124在促进神经系统发育中起着广泛的作用。我们发现,miR-124和Notch信号之间的反馈相互作用调节了尾中线细胞中表皮-周围神经系统(PNS)的命运选择。 Notch信号使表皮中线细胞中的miR-124沉默,而在PNS中线细胞中,miR-124使Notch,Neuralized和所有三个Ciona Hairy / Enhancer-of-Split基因沉默。此外,miR-124的异位表达足以将表皮中线细胞转化为PNS神经元,这与调节Notch信号的作用一致。更广泛地讲,使用体内组织特异性传感器测定法进行验证的全基因组靶标提取表明,miR-124通过下调非神经基因(特别是肌肉指定者Macho-1和50个胸肌科调节的脊索基因)来塑造神经元祖细胞场,以及一些抗神经因素,包括SCP1和PTBP1。 3'UTR保守性分析显示,对SCP1的miR-124靶向可能是在脊椎动物/被膜祖先中共享的,衍生的性状产生的,并且对PTBP1的靶向在蜕皮动物中被保守,除了蜕皮动物,而广泛的Notch途径靶向似乎Ciona特定。总而言之,我们的结果为miR-124促进神经元发育的具体机制提供了全面的见解。

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