PLoS ONE (Jan 2014)

Alteration in Mir-21/PTEN expression modulates gefitinib resistance in non-small cell lung cancer.

  • Hua Shen,
  • Fang Zhu,
  • Jinyuan Liu,
  • Tongpeng Xu,
  • Dong Pei,
  • Rong Wang,
  • Yingying Qian,
  • Qi Li,
  • Lin Wang,
  • Zhumei Shi,
  • Jitai Zheng,
  • Qiudan Chen,
  • Binghua Jiang,
  • Yongqian Shu

DOI
https://doi.org/10.1371/journal.pone.0103305
Journal volume & issue
Vol. 9, no. 7
p. e103305

Abstract

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Resistance to TKI treatment is a major obstacle in effective treatment of NSCLC. Besides EGFR mutation status, the mechanisms involved are largely unknown. Some evidence supports a role for microRNA 21 in modulating drug sensitivity of chemotherapy but its role in NSCLC TKI resistance still remains unexplored. This study aimed to investigate whether NSCLC miR-21 mediated resistance to TKIs also results from Pten targeting. Here, we show miR-21 promotes cancer by negatively regulating Pten expression in human NSCLC tissues: high miR-21 expression levels were associated with shorter DFS in 47 NSCLC patients; high miR-21/low Pten expression levels indicated a poor TKI clinical response and shorter overall survival in another 46 NSCLC patients undergoing TKI treatment. In vitro assays showed that miR-21 was up-regulated concomitantly to down-regulation of Pten in pc-9/GR cells in comparison with pc-9 cells. Moreover, over-expression of miR-21 significantly decreased gefitinib sensitivity by down-regulating Pten expression and activating Akt and ERK pathways in pc-9 cells, while miR-21 knockdown dramatically restored gefitinib sensitivity of pc-9/GR cells by up-regulation of Pten expression and inactivation of AKT and ERK pathways, in vivo and in vitro. We propose alteration of miR-21/Pten expression as a novel mechanism for TKI resistance in NSCLC cancer. Our findings provide a new basis for using miR 21/Pten-based therapeutic strategies to reverse gefitinib resistance in NSCLC.