OncoImmunology (Apr 2019)

Immune evasion by TGFβ-induced miR-183 repression of MICA/B expression in human lung tumor cells

  • Thu Le Trinh,
  • Wendy M. Kandell,
  • Sarah S. Donatelli,
  • Nhan Tu,
  • Melba M. Tejera,
  • Danielle L. Gilvary,
  • Erika A. Eksioglu,
  • Alexis Burnette,
  • William A. Adams,
  • Jinhong Liu,
  • Jamie K. Teer,
  • Julie Y. Djeu,
  • Domenico Coppola,
  • Sheng Wei

DOI
https://doi.org/10.1080/2162402X.2018.1557372
Journal volume & issue
Vol. 8, no. 4

Abstract

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Immune escape is a hallmark of cancer. In human lung cancer, we have identified a unique microRNA (miR)-based pathway employed by tumor cells to repress detection by immune cells via the NKG2D-MICA/B receptor-ligand system. MICA/B is readily induced by cell transformation and serves as a danger signal and ligand to alert NK and activated CD8+ T cells. However, immunohistochemical analysis indicated that human lung adenocarcinoma and squamous cell carcinoma specimens express little MICA/B while high levels of miR-183 were detected in both tumor types in a TCGA database. Human lung tumor cell lines confirmed the reverse relationship in expression of MICA/B and miR-183. Importantly, a miR-183 binding site was identified on the 3ʹuntranslated region (UTR) of both MICA and MICB, suggesting its role in MICA/B regulation. Luciferase reporter constructs bearing the 3ʹUTR of MICA or MICB in 293 cells supported the function of miR-183 in repressing MICA/B expression. Additionally, anti-sense miR-183 transfection into H1355 or H1299 tumor cells caused the upregulation of MICA/B. Abundant miR-183 expression in tumor cells was traced to transforming growth factor-beta (TGFβ), as evidenced by antisense TGFβ transfection into H1355 or H1299 tumor cells which subsequently lost miR-183 expression accompanied by MICA/B upregulation. Most significantly, anti-sense miR-183 transfected tumor cells became more sensitive to lysis by activated CD8+ T cells that express high levels of NKG2D. Thus, high miR-183 triggered by TGFβ expressed in lung tumor cells can target MICA/B expression to circumvent detection by NKG2D on immune cells.

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