hoxc12/c13 as key regulators for rebooting the developmental program in Xenopus limb regeneration
During organ regeneration, after the initial responses to injury, gene expression patterns similar to those in normal development are reestablished during subsequent morphogenesis phases. This supports the idea that regeneration recapitulates development and predicts the existence of genes that rebo...
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Veröffentlicht in: | Nature communications 2024-04, Vol.15 (1), p.3340-3340, Article 3340 |
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Sprache: | eng |
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Zusammenfassung: | During organ regeneration, after the initial responses to injury, gene expression patterns similar to those in normal development are reestablished during subsequent morphogenesis phases. This supports the idea that regeneration recapitulates development and predicts the existence of genes that reboot the developmental program after the initial responses. However, such rebooting mechanisms are largely unknown. Here, we explore core rebooting factors that operate during
Xenopus
limb regeneration. Transcriptomic analysis of larval limb blastema reveals that
hoxc12/c13
show the highest regeneration specificity in expression. Knocking out each of them through genome editing inhibits cell proliferation and expression of a group of genes that are essential for development, resulting in autopod regeneration failure, while limb development and initial blastema formation are not affected. Furthermore, the induction of
hoxc12/c13
expression partially restores froglet regenerative capacity which is normally very limited compared to larval regeneration. Thus, we demonstrate the existence of genes that have a profound impact alone on rebooting of the developmental program in a regeneration-specific manner.
During organ regeneration, gene expression patterns similar to those in normal development are reestablished. Here, Kawasumi-Kita et al. explore core rebooting factors that operate during
Xenopus
limb regeneration. Their results indicate that
hoxc12
and
hoxc13
are critical for reactivating tissue growth. |
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ISSN: | 2041-1723 2041-1723 |
DOI: | 10.1038/s41467-024-47093-y |