Tpl2 regulates intestinal myofibroblast HGF release to suppress colitis-associated tumorigenesis
Vasiliki Koliaraki, … , Manolis Roulis, George Kollias
Vasiliki Koliaraki, … , Manolis Roulis, George Kollias
Published October 15, 2012
Citation Information: J Clin Invest. 2012;122(11):4231-4242. https://doi.org/10.1172/JCI63917.
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Research Article Oncology

Tpl2 regulates intestinal myofibroblast HGF release to suppress colitis-associated tumorigenesis

Abstract

The tumor microenvironment plays a significant role in colitis-associated cancer (CAC). Intestinal myofibroblasts (IMFs) are cells in the intestinal lamina propria secreting factors that are known to modulate carcinogenesis; however, the physiological role of IMFs and signaling pathways influencing CAC have remained unknown. Tumor progression locus 2 (Tpl2) is a MAPK that regulates inflammatory and oncogenic pathways. In this study we addressed the role of Tpl2 in CAC using complete and tissue-specific ablation of Tpl2 in mutant mice. Tpl2-deficient mice did not exhibit significant differences in inflammatory burdens following azoxymethane (AOM)/dextran sodium sulfate (DSS) administration compared with wild-type mice; however, the mutant mice developed significantly increased numbers and sizes of tumors, associated with enhanced epithelial proliferation and decreased apoptosis. Cell-specific ablation of Tpl2 in IMFs, but not in intestinal epithelial or myeloid cells, conferred a similar susceptibility to adenocarcinoma formation. Tpl2-deficient IMFs upregulated HGF production and became less sensitive to the negative regulation of HGF by TGF-β3. In vivo inhibition of HGF-mediated c-Met activation blocked early, enhanced colon dysplasia in Tpl2-deficient mice, indicating that Tpl2 normally suppresses the HGF/c-Met pathway. These findings establish a mesenchyme-specific role for Tpl2 in the regulation of HGF production and suppression of epithelial tumorigenesis.

Authors

Vasiliki Koliaraki, Manolis Roulis, George Kollias

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Figure 4

Tpl2IMFko mice display a pro-tumorigenic phenotype similar to Tpl2D/D mice.

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Tpl2IMFko mice display a pro-tumorigenic phenotype similar to Tpl2D/D m...
(A) Representative images from H&E, BrdU and TUNEL staining of colon tissue slides from Tpl2IMFko and Tpl2fl/fl mice on day 15 after AOM injection. Scale bars: 50 μm. (B) Dysplasia incidence was measured 15 days after the end of the AOM injection. The data correspond to the average of 4 experiments (n = 5). Data represent mean ± SEM. *P < 0.05. (C and D) Proliferation and apoptosis as determined by measuring BrdU-positive cells per crypt (C) and TUNEL-positive cells per field (D) in colon tissue from Tpl2IMFko and Tpl2fl/fl mice on day 15 after AOM injection. At least 20 random crypts and 10 random fields were used, respectively. Data represent mean ± SEM. n = 6; *P < 0.05. (E) qRT-PCR of colon tissue on day 15 of the experimental procedure relative to samples from untreated controls. Gene expression was normalized to B2m levels. Data represent mean ± SEM of 6 mice per genotype (2 mice from each of 3 individual experiments). *P < 0.05, **P < 0.01, ***P < 0.001.