PLoS ONE (Mar 2008)

p16(INK4a) translation suppressed by miR-24.

  • Ashish Lal,
  • Hyeon Ho Kim,
  • Kotb Abdelmohsen,
  • Yuki Kuwano,
  • Rudolf Pullmann,
  • Subramanya Srikantan,
  • Ramesh Subrahmanyam,
  • Jennifer L Martindale,
  • Xiaoling Yang,
  • Fariyal Ahmed,
  • Francisco Navarro,
  • Derek Dykxhoorn,
  • Judy Lieberman,
  • Myriam Gorospe

DOI
https://doi.org/10.1371/journal.pone.0001864
Journal volume & issue
Vol. 3, no. 3
p. e1864

Abstract

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Expression of the tumor suppressor p16(INK4a) increases during aging and replicative senescence.Here, we report that the microRNA miR-24 suppresses p16 expression in human diploid fibroblasts and cervical carcinoma cells. Increased p16 expression with replicative senescence was associated with decreased levels of miR-24, a microRNA that was predicted to associate with the p16 mRNA coding and 3'-untranslated regions. Ectopic miR-24 overexpression reduced p16 protein but not p16 mRNA levels. Conversely, introduction of antisense (AS)-miR-24 blocked miR-24 expression and markedly enhanced p16 protein levels, p16 translation, and the production of EGFP-p16 reporter bearing the miR-24 target recognition sites.Together, our results suggest that miR-24 represses the initiation and elongation phases of p16 translation.