PLoS Genetics (Sep 2011)

Conserved regulation of p53 network dosage by microRNA-125b occurs through evolving miRNA-target gene pairs.

  • Minh T N Le,
  • Ng Shyh-Chang,
  • Swea Ling Khaw,
  • Lingzi Chin,
  • Cathleen Teh,
  • Junliang Tay,
  • Elizabeth O'Day,
  • Vladimir Korzh,
  • Henry Yang,
  • Ashish Lal,
  • Judy Lieberman,
  • Harvey F Lodish,
  • Bing Lim

DOI
https://doi.org/10.1371/journal.pgen.1002242
Journal volume & issue
Vol. 7, no. 9
p. e1002242

Abstract

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MicroRNAs regulate networks of genes to orchestrate cellular functions. MiR-125b, the vertebrate homologue of the Caenorhabditis elegans microRNA lin-4, has been implicated in the regulation of neural and hematopoietic stem cell homeostasis, analogous to how lin-4 regulates stem cells in C. elegans. Depending on the cell context, miR-125b has been proposed to regulate both apoptosis and proliferation. Because the p53 network is a central regulator of both apoptosis and proliferation, the dual roles of miR-125b raise the question of what genes in the p53 network might be regulated by miR-125b. By using a gain- and loss-of-function screen for miR-125b targets in humans, mice, and zebrafish and by validating these targets with the luciferase assay and a novel miRNA pull-down assay, we demonstrate that miR-125b directly represses 20 novel targets in the p53 network. These targets include both apoptosis regulators like Bak1, Igfbp3, Itch, Puma, Prkra, Tp53inp1, Tp53, Zac1, and also cell-cycle regulators like cyclin C, Cdc25c, Cdkn2c, Edn1, Ppp1ca, Sel1l, in the p53 network. We found that, although each miRNA-target pair was seldom conserved, miR-125b regulation of the p53 pathway is conserved at the network level. Our results lead us to propose that miR-125b buffers and fine-tunes p53 network activity by regulating the dose of both proliferative and apoptotic regulators, with implications for tissue stem cell homeostasis and oncogenesis.