: The pro-tumourigenic role of epithelial TGFβ signalling in colorectal cancer (CRC) is controversial. Here, we identify a cohort of born to be bad early-stage (T1) colorectal tumours, with aggressive features and a propensity to disseminate early, that are characterised by high epithelial cell-intrinsic TGFβ signalling. In the presence of concurrent Apc and Kras mutations, activation of epithelial TGFβ signalling rampantly accelerates tumourigenesis and share transcriptional signatures with those of the born to be bad T1 human tumours and predicts recurrence in stage II CRC. Mechanistically, epithelial TGFβ signalling induces a growth-promoting EGFR-signalling module that synergises with mutant APC and KRAS to drive MAPK signalling that re-sensitise tumour cells to MEK and/or EGFR inhibitors. Together, we identify epithelial TGFβ signalling both as a determinant of early dissemination and a potential therapeutic vulnerability of CRC's with born to be bad traits.

Epithelial TGFβ engages growth-factor signalling to circumvent apoptosis and drive intestinal tumourigenesis with aggressive features

Mariella, Elisa;Bardelli, Alberto;
2022-01-01

Abstract

: The pro-tumourigenic role of epithelial TGFβ signalling in colorectal cancer (CRC) is controversial. Here, we identify a cohort of born to be bad early-stage (T1) colorectal tumours, with aggressive features and a propensity to disseminate early, that are characterised by high epithelial cell-intrinsic TGFβ signalling. In the presence of concurrent Apc and Kras mutations, activation of epithelial TGFβ signalling rampantly accelerates tumourigenesis and share transcriptional signatures with those of the born to be bad T1 human tumours and predicts recurrence in stage II CRC. Mechanistically, epithelial TGFβ signalling induces a growth-promoting EGFR-signalling module that synergises with mutant APC and KRAS to drive MAPK signalling that re-sensitise tumour cells to MEK and/or EGFR inhibitors. Together, we identify epithelial TGFβ signalling both as a determinant of early dissemination and a potential therapeutic vulnerability of CRC's with born to be bad traits.
2022
13
1
7551
-
https://www.nature.com/articles/s41467-022-35134-3
Flanagan, Dustin J; Amirkhah, Raheleh; Vincent, David F; Gundaz, Nuray; Gentaz, Pauline; Cammareri, Patrizia; McCooey, Aoife J; McCorry, Amy M B; Fisher, Natalie C; Davis, Hayley L; Ridgway, Rachel A; Lohuis, Jeroen; Leach, Joshua D G; Jackstadt, Rene; Gilroy, Kathryn; Mariella, Elisa; Nixon, Colin; Clark, William; Hedley, Ann; Markert, Elke K; Strathdee, Douglas; Bartholin, Laurent; Redmond, Keara L; Kerr, Emma M; Longley, Daniel B; Ginty, Fiona; Cho, Sanghee; Coleman, Helen G; Loughrey, Maurice B; Bardelli, Alberto; Maughan, Timothy S; Campbell, Andrew D; Lawler, Mark; Leedham, Simon J; Barry, Simon T; Inman, Gareth J; van Rheenen, Jacco; Dunne, Philip D; Sansom, Owen J
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2318/1888614
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