A Genetic Progression Model of Braf(V600E)-Induced Intestinal Tumorigenesis Reveals Targets for Therapeutic Intervention

We show that BRAF(V600E) initiates an alternative pathway to colorectal cancer (CRC), which progresses through a hyperplasia/adenoma/carcinoma sequence. This pathway underlies significant subsets of CRCs with distinctive pathomorphologic/genetic/epidemiologic/clinical characteristics. Genetic and fu...

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Autores principales: Rad, Roland, Cadiñanos, Juan, Rad, Lena, Varela, Ignacio, Strong, Alexander, Kriegl, Lydia, Constantino-Casas, Fernando, Eser, Stefan, Hieber, Maren, Seidler, Barbara, Price, Stacey, Fraga, Mario F., Calvanese, Vincenzo, Hoffman, Gary, Ponstingl, Hannes, Schneider, Günter, Yusa, Kosuke, Grove, Carolyn, Schmid, Roland M., Wang, Wei, Vassiliou, George, Kirchner, Thomas, McDermott, Ultan, Liu, Pentao, Saur, Dieter, Bradley, Allan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cell Press 2013
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3706745/
https://www.ncbi.nlm.nih.gov/pubmed/23845441
http://dx.doi.org/10.1016/j.ccr.2013.05.014
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author Rad, Roland
Cadiñanos, Juan
Rad, Lena
Varela, Ignacio
Strong, Alexander
Kriegl, Lydia
Constantino-Casas, Fernando
Eser, Stefan
Hieber, Maren
Seidler, Barbara
Price, Stacey
Fraga, Mario F.
Calvanese, Vincenzo
Hoffman, Gary
Ponstingl, Hannes
Schneider, Günter
Yusa, Kosuke
Grove, Carolyn
Schmid, Roland M.
Wang, Wei
Vassiliou, George
Kirchner, Thomas
McDermott, Ultan
Liu, Pentao
Saur, Dieter
Bradley, Allan
author_facet Rad, Roland
Cadiñanos, Juan
Rad, Lena
Varela, Ignacio
Strong, Alexander
Kriegl, Lydia
Constantino-Casas, Fernando
Eser, Stefan
Hieber, Maren
Seidler, Barbara
Price, Stacey
Fraga, Mario F.
Calvanese, Vincenzo
Hoffman, Gary
Ponstingl, Hannes
Schneider, Günter
Yusa, Kosuke
Grove, Carolyn
Schmid, Roland M.
Wang, Wei
Vassiliou, George
Kirchner, Thomas
McDermott, Ultan
Liu, Pentao
Saur, Dieter
Bradley, Allan
author_sort Rad, Roland
collection PubMed
description We show that BRAF(V600E) initiates an alternative pathway to colorectal cancer (CRC), which progresses through a hyperplasia/adenoma/carcinoma sequence. This pathway underlies significant subsets of CRCs with distinctive pathomorphologic/genetic/epidemiologic/clinical characteristics. Genetic and functional analyses in mice revealed a series of stage-specific molecular alterations driving different phases of tumor evolution and uncovered mechanisms underlying this stage specificity. We further demonstrate dose-dependent effects of oncogenic signaling, with physiologic Braf(V600E) expression being sufficient for hyperplasia induction, but later stage intensified Mapk-signaling driving both tumor progression and activation of intrinsic tumor suppression. Such phenomena explain, for example, the inability of p53 to restrain tumor initiation as well as its importance in invasiveness control, and the late stage specificity of its somatic mutation. Finally, systematic drug screening revealed sensitivity of this CRC subtype to targeted therapeutics, including Mek or combinatorial PI3K/Braf inhibition.
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spelling pubmed-37067452013-07-10 A Genetic Progression Model of Braf(V600E)-Induced Intestinal Tumorigenesis Reveals Targets for Therapeutic Intervention Rad, Roland Cadiñanos, Juan Rad, Lena Varela, Ignacio Strong, Alexander Kriegl, Lydia Constantino-Casas, Fernando Eser, Stefan Hieber, Maren Seidler, Barbara Price, Stacey Fraga, Mario F. Calvanese, Vincenzo Hoffman, Gary Ponstingl, Hannes Schneider, Günter Yusa, Kosuke Grove, Carolyn Schmid, Roland M. Wang, Wei Vassiliou, George Kirchner, Thomas McDermott, Ultan Liu, Pentao Saur, Dieter Bradley, Allan Cancer Cell Article We show that BRAF(V600E) initiates an alternative pathway to colorectal cancer (CRC), which progresses through a hyperplasia/adenoma/carcinoma sequence. This pathway underlies significant subsets of CRCs with distinctive pathomorphologic/genetic/epidemiologic/clinical characteristics. Genetic and functional analyses in mice revealed a series of stage-specific molecular alterations driving different phases of tumor evolution and uncovered mechanisms underlying this stage specificity. We further demonstrate dose-dependent effects of oncogenic signaling, with physiologic Braf(V600E) expression being sufficient for hyperplasia induction, but later stage intensified Mapk-signaling driving both tumor progression and activation of intrinsic tumor suppression. Such phenomena explain, for example, the inability of p53 to restrain tumor initiation as well as its importance in invasiveness control, and the late stage specificity of its somatic mutation. Finally, systematic drug screening revealed sensitivity of this CRC subtype to targeted therapeutics, including Mek or combinatorial PI3K/Braf inhibition. Cell Press 2013-07-08 /pmc/articles/PMC3706745/ /pubmed/23845441 http://dx.doi.org/10.1016/j.ccr.2013.05.014 Text en © 2013 ELL & Excerpta Medica. https://creativecommons.org/licenses/by/3.0/ Open Access under CC BY 3.0 (https://creativecommons.org/licenses/by/3.0/) license
spellingShingle Article
Rad, Roland
Cadiñanos, Juan
Rad, Lena
Varela, Ignacio
Strong, Alexander
Kriegl, Lydia
Constantino-Casas, Fernando
Eser, Stefan
Hieber, Maren
Seidler, Barbara
Price, Stacey
Fraga, Mario F.
Calvanese, Vincenzo
Hoffman, Gary
Ponstingl, Hannes
Schneider, Günter
Yusa, Kosuke
Grove, Carolyn
Schmid, Roland M.
Wang, Wei
Vassiliou, George
Kirchner, Thomas
McDermott, Ultan
Liu, Pentao
Saur, Dieter
Bradley, Allan
A Genetic Progression Model of Braf(V600E)-Induced Intestinal Tumorigenesis Reveals Targets for Therapeutic Intervention
title A Genetic Progression Model of Braf(V600E)-Induced Intestinal Tumorigenesis Reveals Targets for Therapeutic Intervention
title_full A Genetic Progression Model of Braf(V600E)-Induced Intestinal Tumorigenesis Reveals Targets for Therapeutic Intervention
title_fullStr A Genetic Progression Model of Braf(V600E)-Induced Intestinal Tumorigenesis Reveals Targets for Therapeutic Intervention
title_full_unstemmed A Genetic Progression Model of Braf(V600E)-Induced Intestinal Tumorigenesis Reveals Targets for Therapeutic Intervention
title_short A Genetic Progression Model of Braf(V600E)-Induced Intestinal Tumorigenesis Reveals Targets for Therapeutic Intervention
title_sort genetic progression model of braf(v600e)-induced intestinal tumorigenesis reveals targets for therapeutic intervention
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3706745/
https://www.ncbi.nlm.nih.gov/pubmed/23845441
http://dx.doi.org/10.1016/j.ccr.2013.05.014
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