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The transcription factor Slug represses p16Ink4a and regulates murine muscle stem cell aging
Pei Zhu, Chunping Zhang, Yongxing Gao, Furen Wu, Yalu Zhou, Wenshu Wu
Nature Communications · 2019 · ▲ 63 citations
Abstract
Abstract Activation of the p16 Ink4a -associated senescence(definition) pathway during aging breaks muscle homeostasis and causes degenerative muscle disease by irreversibly dampening satellite cell (SC) self-renewal capacity. Here, we report that the zinc-finger transcription factor Slug is highly expressed in quiescent SCs of mice and functions as a direct transcriptional repressor of p16 Ink4a . Loss of Slug promotes derepression of p16 Ink4a in SCs and accelerates the entry of SCs into a fully senescent state upon damage-induced stress. p16 Ink4a depletion partially rescues defects in Slug -deficient SCs. Furthermore, reduced Slug expression is accompanied by p16 Ink4a accumulation in aged SCs. Slug overexpression ameliorates aged muscle regeneration by enhancing SC self-renewal through active repression of p16 Ink4a transcription. Our results identify a cell-autonomous mechanism underlying functional defects of SCs at advanced age. As p16 Ink4a dysregulation is the chief cause for regenerative defects of human geriatric SCs, these findings highlight Slug as a potential therapeutic target for aging-associated degenerative muscle disease.
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- 10.1038/s41467-019-10479-4
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- 2026-06-11 MST
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APA
Zhu, P., Zhang, C., Gao, Y., Wu, F., Zhou, Y., & Wu, W. (2019). The transcription factor Slug represses p16Ink4a and regulates murine muscle stem cell aging. <em>Nature Communications</em>. https://doi.org/10.1038/s41467-019-10479-4
Vancouver
Zhu P, Zhang C, Gao Y, Wu F, Zhou Y, Wu W. The transcription factor Slug represses p16Ink4a and regulates murine muscle stem cell aging. Nature Communications. 2019. doi:10.1038/s41467-019-10479-4.
BibTeX
@article{pei2019Thetra,
title = {The transcription factor Slug represses p16Ink4a and regulates murine muscle stem cell aging},
author = {Pei Zhu and Chunping Zhang and Yongxing Gao and Furen Wu and Yalu Zhou and Wenshu Wu},
journal = {Nature Communications},
year = {2019},
doi = {10.1038/s41467-019-10479-4},
}
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