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Oncogenic BRAF mutation induces DNA methylation changes in a murine model for human serrated colorectal neoplasia

Colorectal cancer is a major cause of cancer death and approximately 20% arises within serrated polyps, which are under-recognized and poorly understood. Human serrated colorectal polyps frequently exhibit both oncogenic BRAF mutation and widespread DNA methylation changes, which are important in si...

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Autores principales: Bond, Catherine E., Liu, Cheng, Kawamata, Futoshi, McKeone, Diane M., Fernando, Winnie, Jamieson, Saara, Pearson, Sally-Ann, Kane, Alexandra, Woods, Susan L., Lannagan, Tamsin R. M., Somashekar, Roshini, Lee, Young, Dumenil, Troy, Hartel, Gunter, Spring, Kevin J., Borowsky, Jennifer, Fennell, Lochlan, Bettington, Mark, Lee, Jason, Worthley, Daniel L., Leggett, Barbara A., Whitehall, Vicki L. J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Taylor & Francis 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5836984/
https://www.ncbi.nlm.nih.gov/pubmed/29235923
http://dx.doi.org/10.1080/15592294.2017.1411446
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author Bond, Catherine E.
Liu, Cheng
Kawamata, Futoshi
McKeone, Diane M.
Fernando, Winnie
Jamieson, Saara
Pearson, Sally-Ann
Kane, Alexandra
Woods, Susan L.
Lannagan, Tamsin R. M.
Somashekar, Roshini
Lee, Young
Dumenil, Troy
Hartel, Gunter
Spring, Kevin J.
Borowsky, Jennifer
Fennell, Lochlan
Bettington, Mark
Lee, Jason
Worthley, Daniel L.
Leggett, Barbara A.
Whitehall, Vicki L. J.
author_facet Bond, Catherine E.
Liu, Cheng
Kawamata, Futoshi
McKeone, Diane M.
Fernando, Winnie
Jamieson, Saara
Pearson, Sally-Ann
Kane, Alexandra
Woods, Susan L.
Lannagan, Tamsin R. M.
Somashekar, Roshini
Lee, Young
Dumenil, Troy
Hartel, Gunter
Spring, Kevin J.
Borowsky, Jennifer
Fennell, Lochlan
Bettington, Mark
Lee, Jason
Worthley, Daniel L.
Leggett, Barbara A.
Whitehall, Vicki L. J.
author_sort Bond, Catherine E.
collection PubMed
description Colorectal cancer is a major cause of cancer death and approximately 20% arises within serrated polyps, which are under-recognized and poorly understood. Human serrated colorectal polyps frequently exhibit both oncogenic BRAF mutation and widespread DNA methylation changes, which are important in silencing genes restraining neoplastic progression. Here, we investigated whether in vivo induction of mutant Braf is sufficient to result in coordinated promoter methylation changes for multiple cancer-related genes. The Braf(V637E) mutation was induced in murine intestine on an FVB;C57BL/6J background and assessed for morphological and DNA methylation changes at multiple time points from 10 days to 14 months. Extensive intestinal hyperplasia developed by 10 days post-induction of the mutation. By 8 months, most mice had murine serrated adenomas with dysplasia and invasive cancer developed in 40% of mice by 14 months. From 5 months onwards, Braf mutant mice showed extensive, gene-specific increases in DNA methylation even in hyperplastic mucosa without lesions. This demonstrates that persistent oncogenic Braf signaling is sufficient to induce widespread DNA methylation changes. This occurs over an extended period of time, mimicking the long latency followed by rapid progression of human serrated neoplasia. This study establishes for the first time that DNA methylation arises slowly in direct response to prolonged oncogenic Braf signaling in serrated polyps; this finding has implications both for chemoprevention and for understanding the origin of DNA hypermethylation in cancer generally.
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spelling pubmed-58369842018-03-07 Oncogenic BRAF mutation induces DNA methylation changes in a murine model for human serrated colorectal neoplasia Bond, Catherine E. Liu, Cheng Kawamata, Futoshi McKeone, Diane M. Fernando, Winnie Jamieson, Saara Pearson, Sally-Ann Kane, Alexandra Woods, Susan L. Lannagan, Tamsin R. M. Somashekar, Roshini Lee, Young Dumenil, Troy Hartel, Gunter Spring, Kevin J. Borowsky, Jennifer Fennell, Lochlan Bettington, Mark Lee, Jason Worthley, Daniel L. Leggett, Barbara A. Whitehall, Vicki L. J. Epigenetics Research Papers Colorectal cancer is a major cause of cancer death and approximately 20% arises within serrated polyps, which are under-recognized and poorly understood. Human serrated colorectal polyps frequently exhibit both oncogenic BRAF mutation and widespread DNA methylation changes, which are important in silencing genes restraining neoplastic progression. Here, we investigated whether in vivo induction of mutant Braf is sufficient to result in coordinated promoter methylation changes for multiple cancer-related genes. The Braf(V637E) mutation was induced in murine intestine on an FVB;C57BL/6J background and assessed for morphological and DNA methylation changes at multiple time points from 10 days to 14 months. Extensive intestinal hyperplasia developed by 10 days post-induction of the mutation. By 8 months, most mice had murine serrated adenomas with dysplasia and invasive cancer developed in 40% of mice by 14 months. From 5 months onwards, Braf mutant mice showed extensive, gene-specific increases in DNA methylation even in hyperplastic mucosa without lesions. This demonstrates that persistent oncogenic Braf signaling is sufficient to induce widespread DNA methylation changes. This occurs over an extended period of time, mimicking the long latency followed by rapid progression of human serrated neoplasia. This study establishes for the first time that DNA methylation arises slowly in direct response to prolonged oncogenic Braf signaling in serrated polyps; this finding has implications both for chemoprevention and for understanding the origin of DNA hypermethylation in cancer generally. Taylor & Francis 2018-02-19 /pmc/articles/PMC5836984/ /pubmed/29235923 http://dx.doi.org/10.1080/15592294.2017.1411446 Text en © 2018 The Author(s). Published by Informa UK Limited, trading as Taylor & Francis Group http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial-NoDerivatives License (http://creativecommons.org/licenses/by-nc-nd/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited, and is not altered, transformed, or built upon in any way.
spellingShingle Research Papers
Bond, Catherine E.
Liu, Cheng
Kawamata, Futoshi
McKeone, Diane M.
Fernando, Winnie
Jamieson, Saara
Pearson, Sally-Ann
Kane, Alexandra
Woods, Susan L.
Lannagan, Tamsin R. M.
Somashekar, Roshini
Lee, Young
Dumenil, Troy
Hartel, Gunter
Spring, Kevin J.
Borowsky, Jennifer
Fennell, Lochlan
Bettington, Mark
Lee, Jason
Worthley, Daniel L.
Leggett, Barbara A.
Whitehall, Vicki L. J.
Oncogenic BRAF mutation induces DNA methylation changes in a murine model for human serrated colorectal neoplasia
title Oncogenic BRAF mutation induces DNA methylation changes in a murine model for human serrated colorectal neoplasia
title_full Oncogenic BRAF mutation induces DNA methylation changes in a murine model for human serrated colorectal neoplasia
title_fullStr Oncogenic BRAF mutation induces DNA methylation changes in a murine model for human serrated colorectal neoplasia
title_full_unstemmed Oncogenic BRAF mutation induces DNA methylation changes in a murine model for human serrated colorectal neoplasia
title_short Oncogenic BRAF mutation induces DNA methylation changes in a murine model for human serrated colorectal neoplasia
title_sort oncogenic braf mutation induces dna methylation changes in a murine model for human serrated colorectal neoplasia
topic Research Papers
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5836984/
https://www.ncbi.nlm.nih.gov/pubmed/29235923
http://dx.doi.org/10.1080/15592294.2017.1411446
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