4.8 Article

RNA-binding proteins direct myogenic cell fate decisions

Journal

ELIFE
Volume 11, Issue -, Pages -

Publisher

eLIFE SCIENCES PUBL LTD
DOI: 10.7554/eLife.75844

Keywords

RNA-binding protein; skeletal muscle; regeneration; RNA splicing; splicing network; post-transcriptional regulation; Mouse

Categories

Funding

  1. National Institutes of Health [T32GM008497, NIH-F30NS093682, NIH-F30AR068881, NIH-GM045443, NIH-R35GM119575, NIH-AR049446, NIH-AR070360, NIH-RM1-HG007735, NSF IGERT 1144807]
  2. American Cancer Society
  3. National Science Foundation [NSF IGERT 1144807]
  4. Glenn Foundation for Medical Research
  5. University of Colorado Boulder Biological Sciences Initiative
  6. University of Colorado Boulder University of Colorado Undergraduate Research Program
  7. Howard Hughes Medical Institute

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This research reveals that the timing of RNA-binding protein (RBPs) expression can specify the fate transitions of muscle stem cells, playing a crucial role in skeletal muscle regeneration.
RNA-binding proteins (RBPs), essential for skeletal muscle regeneration, cause muscle degeneration and neuromuscular disease when mutated. Why mutations in these ubiquitously expressed RBPs orchestrate complex tissue regeneration and direct cell fate decisions in skeletal muscle remains poorly understood. Single-cell RNA-sequencing of regenerating Mus musculus skeletal muscle reveals that RBP expression, including the expression of many neuromuscular disease-associated RBPs, is temporally regulated in skeletal muscle stem cells and correlates with specific stages of myogenic differentiation. By combining machine learning with RBP engagement scoring, we discovered that the neuromuscular disease-associated RBP Hnrnpa2b1 is a differentiation-specifying regulator of myogenesis that controls myogenic cell fate transitions during terminal differentiation in mice. The timing of RBP expression specifies cell fate transitions by providing post-transcriptional regulation of messenger RNAs that coordinate stem cell fate decisions during tissue regeneration.

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