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A small noncoding RNA links ribosome recovery and translation control to dedifferentiation during salamander limb regeneration. | LitMetric

AI Article Synopsis

  • Salamander limb regeneration involves the formation of a blastema, where stump cells undergo dedifferentiation to contribute to regrowth.
  • A mechanism of protein synthesis inhibition during this process has been identified, and relieving this inhibition boosts cell cycling and speeds up regeneration.
  • The study highlights miR-10b-5p’s role in regulating ribosomal mRNA and protein synthesis, showing that its downregulation is essential for effective limb regeneration in newts.

Article Abstract

Building a blastema from the stump is a key step of salamander limb regeneration. Stump-derived cells temporarily suspend their identity as they contribute to the blastema by a process generally referred to as dedifferentiation. Here, we provide evidence for a mechanism that involves an active inhibition of protein synthesis during blastema formation and growth. Relieving this inhibition results in a higher number of cycling cells and enhances the pace of limb regeneration. By small RNA profiling and fate mapping of skeletal muscle progeny as a cellular model for dedifferentiation, we find that the downregulation of miR-10b-5p is critical for rebooting the translation machinery. miR-10b-5p targets ribosomal mRNAs, and its artificial upregulation causes decreased blastema cell proliferation, reduction in transcripts that encode ribosomal subunits, diminished nascent protein synthesis, and retardation of limb regeneration. Taken together, our data identify a link between miRNA regulation, ribosome biogenesis, and protein synthesis during newt limb regeneration.

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Source
http://dx.doi.org/10.1016/j.devcel.2023.02.007DOI Listing

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