PLoS ONE (Jan 2013)

MiR-424/503-mediated Rictor upregulation promotes tumor progression.

  • Chitose Oneyama,
  • Yoriko Kito,
  • Rei Asai,
  • Jun-ichiro Ikeda,
  • Takuya Yoshida,
  • Daisuke Okuzaki,
  • Rie Kokuda,
  • Kyoko Kakumoto,
  • Ken-ichi Takayama,
  • Satoshi Inoue,
  • Eiichi Morii,
  • Masato Okada

DOI
https://doi.org/10.1371/journal.pone.0080300
Journal volume & issue
Vol. 8, no. 11
p. e80300

Abstract

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mTOR complex 2 (mTORC2) signaling is upregulated in multiple types of human cancer, but the molecular mechanisms underlying its activation and regulation remain elusive. Here, we show that microRNA-mediated upregulation of Rictor, an mTORC2-specific component, contributes to tumor progression. Rictor is upregulated via the repression of the miR-424/503 cluster in human prostate and colon cancer cell lines that harbor c-Src upregulation and in Src-transformed cells. The tumorigenicity and invasive activity of these cells were suppressed by re-expression of miR-424/503. Rictor upregulation promotes formation of mTORC2 and induces activation of mTORC2, resulting in promotion of tumor growth and invasion. Furthermore, downregulation of miR-424/503 is associated with Rictor upregulation in colon cancer tissues. These findings suggest that the miR-424/503-Rictor pathway plays a crucial role in tumor progression.