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MiR-302 Is Required for Timing of Neural Differentiation, Neural Tube Closure, and Embryonic Viability.


ABSTRACT: The evolutionarily conserved miR-302 family of microRNAs is expressed during early mammalian embryonic development. Here, we report that deletion of miR-302a-d in mice results in a fully penetrant late embryonic lethal phenotype. Knockout embryos have an anterior neural tube closure defect associated with a thickened neuroepithelium. The neuroepithelium shows increased progenitor proliferation, decreased cell death, and precocious neuronal differentiation. mRNA profiling at multiple time points during neurulation uncovers a complex pattern of changing targets over time. Overexpression of one of these targets, Fgf15, in the neuroepithelium of the chick embryo induces precocious neuronal differentiation. Compound mutants between mir-302 and the related mir-290 locus have a synthetic lethal phenotype prior to neurulation. Our results show that mir-302 helps regulate neurulation by suppressing neural progenitor expansion and precocious differentiation. Furthermore, these results uncover redundant roles for mir-290 and mir-302 early in development.

SUBMITTER: Parchem RJ 

PROVIDER: S-EPMC4741278 | biostudies-literature | 2015 Aug

REPOSITORIES: biostudies-literature

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miR-302 Is Required for Timing of Neural Differentiation, Neural Tube Closure, and Embryonic Viability.

Parchem Ronald J RJ   Moore Nicole N   Fish Jennifer L JL   Parchem Jacqueline G JG   Braga Tarcio T TT   Shenoy Archana A   Oldham Michael C MC   Rubenstein John L R JL   Schneider Richard A RA   Blelloch Robert R  

Cell reports 20150723 5


The evolutionarily conserved miR-302 family of microRNAs is expressed during early mammalian embryonic development. Here, we report that deletion of miR-302a-d in mice results in a fully penetrant late embryonic lethal phenotype. Knockout embryos have an anterior neural tube closure defect associated with a thickened neuroepithelium. The neuroepithelium shows increased progenitor proliferation, decreased cell death, and precocious neuronal differentiation. mRNA profiling at multiple time points  ...[more]

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