1. Academic Validation
  2. TRPA1 Contributes to FGFR2c Signaling and to Its Oncogenic Outcomes in Pancreatic Ductal Adenocarcinoma-Derived Cell Lines

TRPA1 Contributes to FGFR2c Signaling and to Its Oncogenic Outcomes in Pancreatic Ductal Adenocarcinoma-Derived Cell Lines

  • Cancers (Basel). 2024 Jan 31;16(3):609. doi: 10.3390/cancers16030609.
Vanessa Mancini 1 Salvatore Raffa 1 Alessandra Fiorio Pla 2 Deborah French 1 Maria Rosaria Torrisi 1 Danilo Ranieri 1 3 Francesca Belleudi 1
Affiliations

Affiliations

  • 1 Department of Clinical and Molecular Medicine, Sapienza University of Rome, 00161 Rome, Italy.
  • 2 Turin Cell Physiology Laboratory, Department of Life Sciences and Systems Biology, University of Turin, 10125 Torino, Italy.
  • 3 Dipartimento di Scienze della Vita, della Salute e delle Professioni Sanitarie, Università degli Studi "Link Campus University", 00165 Rome, Italy.
Abstract

Fibroblast Growth Factor receptor (FGFR) signaling is a key modulator of cellular processes dysregulated in Cancer. We recently found that the high expression of the mesenchymal FGFR2c variant in human pancreatic ductal adenocarcinoma (PDAC)-derived cells triggers the PKCε-mediated improvement of EMT and of Mcl-1/SRC-dependent cell invasion. Since other membrane proteins can affect the receptor tyrosine kinase signaling, including transient receptor potential channels (TRPs), in this work, we investigated the role of TRPs in the FGFR2c/PKCε oncogenic axis. Our results highlighted that either the FGFR2c/PKCε axis shut-off obtained by shRNA or its sustained activation via ligand stimulation induces TRPA1 downregulation, suggesting a channel/receptor dependence. Indeed, biochemical molecular and immunofluorescence approaches demonstrated that the transient depletion of TRPA1 by siRNA was sufficient to attenuate FGFR2c downstream signaling pathways, as well as the consequent enhancement of EMT. Moreover, the biochemical check of MCL1/Src signaling and the in vitro assay of cellular motility suggested that TRPA1 also contributes to the FGFR2c-induced enhancement of PDAC cell invasiveness. Finally, the use of a selective channel antagonist indicated that the contribution of TRPA1 to the FGFR2c oncogenic potential is independent of its pore function. Thus, TRPA1 could represent a putative candidate for future target therapies in PDAC.

Keywords

EMT; FGFR2; PDAC; PKCε; TRPA1.

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