Fibroblast Growth Factor-14 Acts as Tumor Suppressor in Lung Adenocarcinomas

Investigation of the molecular dynamics in lung cancer is crucial for the development of new treatment strategies. Fibroblast growth factor (FGF) 14 belongs to the FGF family, which might play a crucial role in cancer progression. We analyzed lung adenocarcinoma (LUAC) patients samples and found that FGF14 was downregulated, correlating with reduced survival and oncogenic mutation status. FGF14 overexpression in lung cancer cell lines resulted in decreased proliferation, colony formation, and migration, as well as increased expression of epithelial markers and a decreased expression of mesenchymal markers, indicating a mesenchymal to epithelial transition in vitro. We verified these findings using small interfering RNA against FGF14 and further confirmed the suppressive effect of FGF14 in a NOD.Cg-Prkdc(scid) Il2rg(tm1Wjl)/SzJ immunodeficient xenograft tumor model. Moreover, FGF14 overexpressing tumor cell RNA sequencing data suggests that genes affected by FGF14 were related to the extracellular matrix, playing a role in proliferation and migration. Notably, newly identified FGF14 target genes, adenosine deaminase RNA specific B1 (ADARB1), collagen and calcium-binding epidermal growth factor domain-containing protein 1 (CCBE1), alpha1 chain of collagen XI (COL11A1), and mucin 16 (MUC16) expression was negatively correlated with overall survival when FGF14 was downregulated in LUAC. These findings led us to suggest that FGF14 regulates proliferation and migration in LUAC.

  • Turkowski, K.
  • Herzberg, F.
  • Gunther, S.
  • Brunn, D.
  • Weigert, A.
  • Meister, M.
  • Muley, T.
  • Kriegsmann, M.
  • Schneider, M. A.
  • Winter, H.
  • Thomas, M.
  • Grimminger, F.
  • Seeger, W.
  • Savai Pullamsetti, S.
  • Savai, R.

Keywords

  • fibroblast growth factor 14
  • lung adenocarcinoma
  • lung cancer mesenchymal epithelial transition
  • xenograft model
Publication details
DOI: 10.3390/cells9081755
Journal: Cells
Number: 8
Work Type: Original
Access number: 32707902
See publication on PubMed
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