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A Comprehensive Characterization of Genome-Wide Copy Number Aberrations in Colorectal Cancer Reveals Novel Oncogenes and Patterns of Alterations

To develop a comprehensive overview of copy number aberrations (CNAs) in stage-II/III colorectal cancer (CRC), we characterized 302 tumors from the PETACC-3 clinical trial. Microsatellite-stable (MSS) samples (n = 269) had 66 minimal common CNA regions, with frequent gains on 20 q (72.5%), 7 (41.8%)...

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Autores principales: Xie, Tao, d’ Ario, Giovanni, Lamb, John R., Martin, Eric, Wang, Kai, Tejpar, Sabine, Delorenzi, Mauro, Bosman, Fred T., Roth, Arnaud D., Yan, Pu, Bougel, Stephanie, Di Narzo, Antonio Fabio, Popovici, Vlad, Budinská, Eva, Mao, Mao, Weinrich, Scott L., Rejto, Paul A., Hodgson, J. Graeme
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3409212/
https://www.ncbi.nlm.nih.gov/pubmed/22860045
http://dx.doi.org/10.1371/journal.pone.0042001
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author Xie, Tao
d’ Ario, Giovanni
Lamb, John R.
Martin, Eric
Wang, Kai
Tejpar, Sabine
Delorenzi, Mauro
Bosman, Fred T.
Roth, Arnaud D.
Yan, Pu
Bougel, Stephanie
Di Narzo, Antonio Fabio
Popovici, Vlad
Budinská, Eva
Mao, Mao
Weinrich, Scott L.
Rejto, Paul A.
Hodgson, J. Graeme
author_facet Xie, Tao
d’ Ario, Giovanni
Lamb, John R.
Martin, Eric
Wang, Kai
Tejpar, Sabine
Delorenzi, Mauro
Bosman, Fred T.
Roth, Arnaud D.
Yan, Pu
Bougel, Stephanie
Di Narzo, Antonio Fabio
Popovici, Vlad
Budinská, Eva
Mao, Mao
Weinrich, Scott L.
Rejto, Paul A.
Hodgson, J. Graeme
author_sort Xie, Tao
collection PubMed
description To develop a comprehensive overview of copy number aberrations (CNAs) in stage-II/III colorectal cancer (CRC), we characterized 302 tumors from the PETACC-3 clinical trial. Microsatellite-stable (MSS) samples (n = 269) had 66 minimal common CNA regions, with frequent gains on 20 q (72.5%), 7 (41.8%), 8 q (33.1%) and 13 q (51.0%) and losses on 18 (58.6%), 4 q (26%) and 21 q (21.6%). MSS tumors have significantly more CNAs than microsatellite-instable (MSI) tumors: within the MSI tumors a novel deletion of the tumor suppressor WWOX at 16 q23.1 was identified (p<0.01). Focal aberrations identified by the GISTIC method confirmed amplifications of oncogenes including EGFR, ERBB2, CCND1, MET, and MYC, and deletions of tumor suppressors including TP53, APC, and SMAD4, and gene expression was highly concordant with copy number aberration for these genes. Novel amplicons included putative oncogenes such as WNK1 and HNF4A, which also showed high concordance between copy number and expression. Survival analysis associated a specific patient segment featured by chromosome 20 q gains to an improved overall survival, which might be due to higher expression of genes such as EEF1B2 and PTK6. The CNA clustering also grouped tumors characterized by a poor prognosis BRAF-mutant-like signature derived from mRNA data from this cohort. We further revealed non-random correlation between CNAs among unlinked loci, including positive correlation between 20 q gain and 8 q gain, and 20 q gain and chromosome 18 loss, consistent with co-selection of these CNAs. These results reinforce the non-random nature of somatic CNAs in stage-II/III CRC and highlight loci and genes that may play an important role in driving the development and outcome of this disease.
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spelling pubmed-34092122012-08-02 A Comprehensive Characterization of Genome-Wide Copy Number Aberrations in Colorectal Cancer Reveals Novel Oncogenes and Patterns of Alterations Xie, Tao d’ Ario, Giovanni Lamb, John R. Martin, Eric Wang, Kai Tejpar, Sabine Delorenzi, Mauro Bosman, Fred T. Roth, Arnaud D. Yan, Pu Bougel, Stephanie Di Narzo, Antonio Fabio Popovici, Vlad Budinská, Eva Mao, Mao Weinrich, Scott L. Rejto, Paul A. Hodgson, J. Graeme PLoS One Research Article To develop a comprehensive overview of copy number aberrations (CNAs) in stage-II/III colorectal cancer (CRC), we characterized 302 tumors from the PETACC-3 clinical trial. Microsatellite-stable (MSS) samples (n = 269) had 66 minimal common CNA regions, with frequent gains on 20 q (72.5%), 7 (41.8%), 8 q (33.1%) and 13 q (51.0%) and losses on 18 (58.6%), 4 q (26%) and 21 q (21.6%). MSS tumors have significantly more CNAs than microsatellite-instable (MSI) tumors: within the MSI tumors a novel deletion of the tumor suppressor WWOX at 16 q23.1 was identified (p<0.01). Focal aberrations identified by the GISTIC method confirmed amplifications of oncogenes including EGFR, ERBB2, CCND1, MET, and MYC, and deletions of tumor suppressors including TP53, APC, and SMAD4, and gene expression was highly concordant with copy number aberration for these genes. Novel amplicons included putative oncogenes such as WNK1 and HNF4A, which also showed high concordance between copy number and expression. Survival analysis associated a specific patient segment featured by chromosome 20 q gains to an improved overall survival, which might be due to higher expression of genes such as EEF1B2 and PTK6. The CNA clustering also grouped tumors characterized by a poor prognosis BRAF-mutant-like signature derived from mRNA data from this cohort. We further revealed non-random correlation between CNAs among unlinked loci, including positive correlation between 20 q gain and 8 q gain, and 20 q gain and chromosome 18 loss, consistent with co-selection of these CNAs. These results reinforce the non-random nature of somatic CNAs in stage-II/III CRC and highlight loci and genes that may play an important role in driving the development and outcome of this disease. Public Library of Science 2012-07-31 /pmc/articles/PMC3409212/ /pubmed/22860045 http://dx.doi.org/10.1371/journal.pone.0042001 Text en © 2012 Xie et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Xie, Tao
d’ Ario, Giovanni
Lamb, John R.
Martin, Eric
Wang, Kai
Tejpar, Sabine
Delorenzi, Mauro
Bosman, Fred T.
Roth, Arnaud D.
Yan, Pu
Bougel, Stephanie
Di Narzo, Antonio Fabio
Popovici, Vlad
Budinská, Eva
Mao, Mao
Weinrich, Scott L.
Rejto, Paul A.
Hodgson, J. Graeme
A Comprehensive Characterization of Genome-Wide Copy Number Aberrations in Colorectal Cancer Reveals Novel Oncogenes and Patterns of Alterations
title A Comprehensive Characterization of Genome-Wide Copy Number Aberrations in Colorectal Cancer Reveals Novel Oncogenes and Patterns of Alterations
title_full A Comprehensive Characterization of Genome-Wide Copy Number Aberrations in Colorectal Cancer Reveals Novel Oncogenes and Patterns of Alterations
title_fullStr A Comprehensive Characterization of Genome-Wide Copy Number Aberrations in Colorectal Cancer Reveals Novel Oncogenes and Patterns of Alterations
title_full_unstemmed A Comprehensive Characterization of Genome-Wide Copy Number Aberrations in Colorectal Cancer Reveals Novel Oncogenes and Patterns of Alterations
title_short A Comprehensive Characterization of Genome-Wide Copy Number Aberrations in Colorectal Cancer Reveals Novel Oncogenes and Patterns of Alterations
title_sort comprehensive characterization of genome-wide copy number aberrations in colorectal cancer reveals novel oncogenes and patterns of alterations
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3409212/
https://www.ncbi.nlm.nih.gov/pubmed/22860045
http://dx.doi.org/10.1371/journal.pone.0042001
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