Negative regulation of TGFβ-induced apoptosis by RAC1B enhances intestinal tumourigenesis

Negative regulation of TGFβ-induced apoptosis by RAC1B enhances intestinal tumourigenesis

Abstract RAC1B is a tumour-related alternative splice isoform of the small GTPase RAC1, found overexpressed in a large number of tumour types. Building evidence suggests it promotes tumour progression but compelling in vivo evidence, demonstrating a role in driving tumour invasion, is currently lack...

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Main Authors: Victoria Gudiño, Patrizia Cammareri, Caroline V. Billard, Kevin B. Myant
Format: Article
Language:English
Published: Nature Publishing Group 2021-09-01
Series:Cell Death and Disease
Online Access:https://doi.org/10.1038/s41419-021-04177-7
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spelling doaj-381b458820c14084a39556c04ee2ac1d2021-09-26T11:05:21ZengNature Publishing GroupCell Death and Disease2041-48892021-09-01121011210.1038/s41419-021-04177-7Negative regulation of TGFβ-induced apoptosis by RAC1B enhances intestinal tumourigenesisVictoria Gudiño0Patrizia Cammareri1Caroline V. Billard2Kevin B. Myant3Cancer Research UK Edinburgh Centre, MRC Institute of Genetics & Molecular Medicine, The University of Edinburgh, Western General HospitalCancer Research UK Edinburgh Centre, MRC Institute of Genetics & Molecular Medicine, The University of Edinburgh, Western General HospitalCancer Research UK Edinburgh Centre, MRC Institute of Genetics & Molecular Medicine, The University of Edinburgh, Western General HospitalCancer Research UK Edinburgh Centre, MRC Institute of Genetics & Molecular Medicine, The University of Edinburgh, Western General HospitalAbstract RAC1B is a tumour-related alternative splice isoform of the small GTPase RAC1, found overexpressed in a large number of tumour types. Building evidence suggests it promotes tumour progression but compelling in vivo evidence, demonstrating a role in driving tumour invasion, is currently lacking. In the present study, we have overexpressed RAC1B in a colorectal cancer mouse model with potential invasive properties. Interestingly, RAC1B overexpression did not trigger tumour invasion, rather it led to an acceleration of tumour initiation and reduced mouse survival. By modelling early stages of adenoma initiation we observed a reduced apoptotic rate in RAC1B overexpressing tumours, suggesting protection from apoptosis as a mediator of this phenotype. RAC1B overexpressing tumours displayed attenuated TGFβ signalling and functional analysis in ex vivo organoid cultures demonstrated that RAC1B negatively modulates TGFβ signalling and confers resistance to TGFβ-driven cell death. This work defines a novel mechanism by which early adenoma cells can overcome the cytostatic and cytotoxic effects of TGFβ signalling and characterises a new oncogenic function of RAC1B in vivo.https://doi.org/10.1038/s41419-021-04177-7
collection DOAJ
language English
format Article
sources DOAJ
author Victoria Gudiño
Patrizia Cammareri
Caroline V. Billard
Kevin B. Myant
spellingShingle Victoria Gudiño
Patrizia Cammareri
Caroline V. Billard
Kevin B. Myant
Negative regulation of TGFβ-induced apoptosis by RAC1B enhances intestinal tumourigenesis
Cell Death and Disease
author_facet Victoria Gudiño
Patrizia Cammareri
Caroline V. Billard
Kevin B. Myant
author_sort Victoria Gudiño
title Negative regulation of TGFβ-induced apoptosis by RAC1B enhances intestinal tumourigenesis
title_short Negative regulation of TGFβ-induced apoptosis by RAC1B enhances intestinal tumourigenesis
title_full Negative regulation of TGFβ-induced apoptosis by RAC1B enhances intestinal tumourigenesis
title_fullStr Negative regulation of TGFβ-induced apoptosis by RAC1B enhances intestinal tumourigenesis
title_full_unstemmed Negative regulation of TGFβ-induced apoptosis by RAC1B enhances intestinal tumourigenesis
title_sort negative regulation of tgfβ-induced apoptosis by rac1b enhances intestinal tumourigenesis
publisher Nature Publishing Group
series Cell Death and Disease
issn 2041-4889
publishDate 2021-09-01
description Abstract RAC1B is a tumour-related alternative splice isoform of the small GTPase RAC1, found overexpressed in a large number of tumour types. Building evidence suggests it promotes tumour progression but compelling in vivo evidence, demonstrating a role in driving tumour invasion, is currently lacking. In the present study, we have overexpressed RAC1B in a colorectal cancer mouse model with potential invasive properties. Interestingly, RAC1B overexpression did not trigger tumour invasion, rather it led to an acceleration of tumour initiation and reduced mouse survival. By modelling early stages of adenoma initiation we observed a reduced apoptotic rate in RAC1B overexpressing tumours, suggesting protection from apoptosis as a mediator of this phenotype. RAC1B overexpressing tumours displayed attenuated TGFβ signalling and functional analysis in ex vivo organoid cultures demonstrated that RAC1B negatively modulates TGFβ signalling and confers resistance to TGFβ-driven cell death. This work defines a novel mechanism by which early adenoma cells can overcome the cytostatic and cytotoxic effects of TGFβ signalling and characterises a new oncogenic function of RAC1B in vivo.
url https://doi.org/10.1038/s41419-021-04177-7
work_keys_str_mv AT victoriagudino negativeregulationoftgfbinducedapoptosisbyrac1benhancesintestinaltumourigenesis
AT patriziacammareri negativeregulationoftgfbinducedapoptosisbyrac1benhancesintestinaltumourigenesis
AT carolinevbillard negativeregulationoftgfbinducedapoptosisbyrac1benhancesintestinaltumourigenesis
AT kevinbmyant negativeregulationoftgfbinducedapoptosisbyrac1benhancesintestinaltumourigenesis
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