Ion channel TRPV1-dependent activation of PTP1B suppresses EGFR-associated intestinal tumorigenesis
Petrus R. de Jong, … , Maripat Corr, Eyal Raz
Petrus R. de Jong, … , Maripat Corr, Eyal Raz
Published August 1, 2014
Citation Information: J Clin Invest. 2014;124(9):3793-3806. https://doi.org/10.1172/JCI72340.
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Research Article Oncology

Ion channel TRPV1-dependent activation of PTP1B suppresses EGFR-associated intestinal tumorigenesis

Abstract

The intestinal epithelium has a high rate of turnover, and dysregulation of pathways that regulate regeneration can lead to tumor development; however, the negative regulators of oncogenic events in the intestinal epithelium are not fully understood. Here we identified a feedback loop between the epidermal growth factor receptor (EGFR), a known mediator of proliferation, and the transient receptor potential cation channel, subfamily V, member 1 (TRPV1), in intestinal epithelial cells (IECs). We found that TRPV1 was expressed by IECs and was intrinsically activated upon EGFR stimulation. Subsequently, TRPV1 activation inhibited EGFR-induced epithelial cell proliferation via activation of Ca2+/calpain and resulting activation of protein tyrosine phosphatase 1B (PTP1B). In a murine model of multiple intestinal neoplasia (ApcMin/+ mice), TRPV1 deficiency increased adenoma formation, and treatment of these animals with an EGFR kinase inhibitor reversed protumorigenic phenotypes, supporting a functional association between TRPV1 and EGFR signaling in IECs. Administration of a TRPV1 agonist suppressed intestinal tumorigenesis in ApcMin/+ mice, similar to — as well as in conjunction with — a cyclooxygenase-2 (COX-2) inhibitor, which suggests that targeting both TRPV1 and COX-2 has potential as a therapeutic approach for tumor prevention. Our findings implicate TRPV1 as a regulator of growth factor signaling in the intestinal epithelium through activation of PTP1B and subsequent suppression of intestinal tumorigenesis.

Authors

Petrus R. de Jong, Naoki Takahashi, Alexandra R. Harris, Jihyung Lee, Samuel Bertin, James Jeffries, Michael Jung, Jen Duong, Amy I. Triano, Jongdae Lee, Yaron Niv, David S. Herdman, Koji Taniguchi, Chang-Whan Kim, Hui Dong, Lars Eckmann, Stephanie M. Stanford, Nunzio Bottini, Maripat Corr, Eyal Raz

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Figure 3

TRPV1 inhibits epithelial cell proliferation and EGFR signaling in vitro.

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TRPV1 inhibits epithelial cell proliferation and EGFR signaling in vitro...
(A) Overexpression of TRPV1 inhibited EGF-induced EGFR activity in the IEC line HCT116. Cells were transfected with control or TRPV1 plasmid and stimulated with 1 ng/ml EGF for the indicated times, followed by Western blot analysis of total cell lysates. (B) TRPV1 knockdown enhanced EGFR signaling in IECs in vitro. HCT116 cells were transfected with control or TRPV1 shRNA. After obtaining stable cell lines, control and knockdown cells were stimulated with low-dose EGF (1 ng/ml) for the indicated times, and cell lysates were analyzed by Western blotting. (C) HCT116 cells treated with control or TRPV1 shRNA were cultured for 3 days in the presence or absence of gefitinib (1 μM). Cells were then analyzed for cell proliferation with the MTT assay. Results are presented as a percentage of day 1 of cell culture. Mean ± SEM. *P < 0.05 vs. control, ANOVA.