A non-canonical role for a small nucleolar RNA in ribosome biogenesis and senescence

Yujing Cheng, Siwen Wang, He Zhang, Jong Sun Lee, Chunyang Ni, Jason Guo, Eric Chen, Shenming Wang, Asha Acharya, Tsung Cheng Chang, Michael Buszczak, Hao Zhu, Joshua T. Mendell

Research output: Contribution to journalArticlepeer-review

1 Scopus citations

Abstract

Cellular senescence is an irreversible state of cell-cycle arrest induced by various stresses, including aberrant oncogene activation, telomere shortening, and DNA damage. Through a genome-wide screen, we discovered a conserved small nucleolar RNA (snoRNA), SNORA13, that is required for multiple forms of senescence in human cells and mice. Although SNORA13 guides the pseudouridylation of a conserved nucleotide in the ribosomal decoding center, loss of this snoRNA minimally impacts translation. Instead, we found that SNORA13 negatively regulates ribosome biogenesis. Senescence-inducing stress perturbs ribosome biogenesis, resulting in the accumulation of free ribosomal proteins (RPs) that trigger p53 activation. SNORA13 interacts directly with RPL23, decreasing its incorporation into maturing 60S subunits and, consequently, increasing the pool of free RPs, thereby promoting p53-mediated senescence. Thus, SNORA13 regulates ribosome biogenesis and the p53 pathway through a non-canonical mechanism distinct from its role in guiding RNA modification. These findings expand our understanding of snoRNA functions and their roles in cellular signaling.

Original languageEnglish (US)
JournalCell
DOIs
StateAccepted/In press - 2024

Keywords

  • RPL23
  • SNORA13
  • nucleolar stress
  • p53
  • ribosome biogenesis
  • senescence
  • snoRNA

ASJC Scopus subject areas

  • General Biochemistry, Genetics and Molecular Biology

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