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

被引:38
作者
Chen, Jerry S. [1 ,2 ]
Pedro, Matthew San [1 ,2 ]
Zeller, Robert W. [1 ,2 ,3 ]
机构
[1] San Diego State Univ, Computat Sci Res Ctr, San Diego, CA 92182 USA
[2] San Diego State Univ, Dept Biol, San Diego, CA 92182 USA
[3] San Diego State Univ, Ctr Appl & Expt Genom, San Diego, CA 92182 USA
来源
DEVELOPMENT | 2011年 / 138卷 / 22期
基金
美国国家科学基金会;
关键词
miR-124; microRNA targets; Notch signaling; Macho-1; SCP1; Notochord; Ciona intestinalis; PTBP1; PERIPHERAL NERVOUS-SYSTEM; ASCIDIAN EMBRYOS; GENE-EXPRESSION; CAENORHABDITIS-ELEGANS; TRANSGENE EXPRESSION; NEURAL DEVELOPMENT; CNS DEVELOPMENT; MESSENGER-RNA; MICRORNAS; CHORDATE;
D O I
10.1242/dev.068049
中图分类号
Q [生物科学];
学科分类号
07 ; 0710 ; 09 ;
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.
引用
收藏
页码:4943 / 4953
页数:11
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