Frontiers in Oncology (Nov 2019)

A High-Content Screening Approach to Identify MicroRNAs Against Head and Neck Cancer Cell Survival and EMT in an Inflammatory Microenvironment

  • Bruno Sangiorgi,
  • Bruno Sangiorgi,
  • Felipe Canto de Souza,
  • Felipe Canto de Souza,
  • Ildercílio Mota de Souza Lima,
  • Ildercílio Mota de Souza Lima,
  • Josiane Lilian dos Santos Schiavinato,
  • Josiane Lilian dos Santos Schiavinato,
  • Amanda Cristina Corveloni,
  • Amanda Cristina Corveloni,
  • Carolina Hassibe Thomé,
  • Carolina Hassibe Thomé,
  • Wilson Araújo Silva,
  • Wilson Araújo Silva,
  • Vitor Marcel Faça,
  • Vitor Marcel Faça,
  • Dimas Tadeu Covas,
  • Marco Antônio Zago,
  • Rodrigo Alexandre Panepucci,
  • Rodrigo Alexandre Panepucci

DOI
https://doi.org/10.3389/fonc.2019.01100
Journal volume & issue
Vol. 9

Abstract

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Head and neck squamous cell carcinoma (HNSCC) is among the most common cancer types. Metastasis, the main cause of death by cancer, can be promoted by an inflammatory microenvironment, which induces epithelial-mesenchymal transition (EMT) through a NF-κB-mediated stabilization of Snail. Here, we aimed to explore how microRNAs (miRs) can affect cell survival and EMT in HNSCC cells under an inflammatory microenvironment. By using a high-content screening (HCS) approach, we evaluated alterations in morphometric parameters, as well as expression/localization of Snail/Slug, in HNSCC cells primed with TNF-α. Based on those quantitation, we established the optimal experimental conditions of EMT induction driven by TNF-α. Those conditions were applied to cells transfected with distinct miRs (N = 31), followed by clusterization of miRs based on alterations related to cell survival and EMT. The signaling pathways enriched with molecular targets from each group of miRs were identified by in silico analyses. Finally, cells were transfected with siRNAs against signaling pathways targeted by miRs with anti-survival/EMT effect and evaluated for alterations in cell survival and EMT. Overall, we observed that TNF-α, at 20 ng/ml, induced EMT-related changes in cell morphology, Snail/Slug expression, and cell migration. Predicted targets of miRs with anti-survival/EMT effect were enriched with targets of NF-κB, PI3K/ATK, and Wnt/beta catenin pathways. Strikingly, individual gene silencing of elements from those pathways, namely RELA (NF-kB), AKT1 (PI3K/AKT), and CTNNB1 (Wnt/beta catenin) reduced cell survival and/or expression of Snail/Slug in cells stimulated with TNF-α. As a whole, our HCS approach allowed for the identification of miRs capable of inhibiting cell survival and EMT considering the presence of an inflammatory microenvironment, also indicating the common signaling pathways and molecular targets most likely to underlie those alterations. These findings may contribute to the development of targeted therapies against HNSCC.

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