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DNA defects, epigenetics, and gene expression in cancer-adjacent breast: a study from The Cancer Genome Atlas

Recurrence rates after breast-conserving therapy may depend on genomic characteristics of cancer-adjacent, benign-appearing tissue. Studies have not evaluated recurrence in association with multiple genomic characteristics of cancer-adjacent breast tissue. To estimate the prevalence of DNA defects a...

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Autores principales: Troester, Melissa A, Hoadley, Katherine A, D’Arcy, Monica, Cherniack, Andrew D, Stewart, Chip, Koboldt, Daniel C, Robertson, A Gordon, Mahurkar, Swapna, Shen, Hui, Wilkerson, Matthew D, Sandhu, Rupninder, Johnson, Nicole B, Allison, Kimberly H, Beck, Andrew H, Yau, Christina, Bowen, Jay, Sheth, Margi, Hwang, E Shelley, Perou, Charles M, Laird, Peter W, Ding, Li, Benz, Christopher C
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5515343/
https://www.ncbi.nlm.nih.gov/pubmed/28721375
http://dx.doi.org/10.1038/npjbcancer.2016.7
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author Troester, Melissa A
Hoadley, Katherine A
D’Arcy, Monica
Cherniack, Andrew D
Stewart, Chip
Koboldt, Daniel C
Robertson, A Gordon
Mahurkar, Swapna
Shen, Hui
Wilkerson, Matthew D
Sandhu, Rupninder
Johnson, Nicole B
Allison, Kimberly H
Beck, Andrew H
Yau, Christina
Bowen, Jay
Sheth, Margi
Hwang, E Shelley
Perou, Charles M
Laird, Peter W
Ding, Li
Benz, Christopher C
author_facet Troester, Melissa A
Hoadley, Katherine A
D’Arcy, Monica
Cherniack, Andrew D
Stewart, Chip
Koboldt, Daniel C
Robertson, A Gordon
Mahurkar, Swapna
Shen, Hui
Wilkerson, Matthew D
Sandhu, Rupninder
Johnson, Nicole B
Allison, Kimberly H
Beck, Andrew H
Yau, Christina
Bowen, Jay
Sheth, Margi
Hwang, E Shelley
Perou, Charles M
Laird, Peter W
Ding, Li
Benz, Christopher C
author_sort Troester, Melissa A
collection PubMed
description Recurrence rates after breast-conserving therapy may depend on genomic characteristics of cancer-adjacent, benign-appearing tissue. Studies have not evaluated recurrence in association with multiple genomic characteristics of cancer-adjacent breast tissue. To estimate the prevalence of DNA defects and RNA expression subtypes in cancer-adjacent, benign-appearing breast tissue at least 2 cm from the tumor margin, cancer-adjacent, pathologically well-characterized, benign-appearing breast tissue specimens from The Cancer Genome Atlas project were analyzed for DNA sequence, copy-number variation, DNA methylation, messenger RNA (mRNA) sequence, and mRNA/microRNA expression. Additional samples were also analyzed by at least one of these genomic data types and associations between genomic characteristics of normal tissue and overall survival were assessed. Approximately 40% of cancer-adjacent, benign-appearing tissues harbored genomic defects in DNA copy number, sequence, methylation, or in RNA sequence, although these defects did not significantly predict 10-year overall survival. Two mRNA/microRNA expression phenotypes were observed, including an active mRNA subtype that was identified in 40% of samples. Controlling for tumor characteristics and the presence of genomic defects, this active subtype was associated with significantly worse 10-year survival among estrogen receptor (ER)-positive cases. This multi-platform analysis of breast cancer-adjacent samples produced genomic findings consistent with current surgical margin guidelines, and provides evidence that extratumoral RNA expression patterns in cancer-adjacent tissue predict overall survival among patients with ER-positive disease.
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spelling pubmed-55153432017-07-18 DNA defects, epigenetics, and gene expression in cancer-adjacent breast: a study from The Cancer Genome Atlas Troester, Melissa A Hoadley, Katherine A D’Arcy, Monica Cherniack, Andrew D Stewart, Chip Koboldt, Daniel C Robertson, A Gordon Mahurkar, Swapna Shen, Hui Wilkerson, Matthew D Sandhu, Rupninder Johnson, Nicole B Allison, Kimberly H Beck, Andrew H Yau, Christina Bowen, Jay Sheth, Margi Hwang, E Shelley Perou, Charles M Laird, Peter W Ding, Li Benz, Christopher C NPJ Breast Cancer Article Recurrence rates after breast-conserving therapy may depend on genomic characteristics of cancer-adjacent, benign-appearing tissue. Studies have not evaluated recurrence in association with multiple genomic characteristics of cancer-adjacent breast tissue. To estimate the prevalence of DNA defects and RNA expression subtypes in cancer-adjacent, benign-appearing breast tissue at least 2 cm from the tumor margin, cancer-adjacent, pathologically well-characterized, benign-appearing breast tissue specimens from The Cancer Genome Atlas project were analyzed for DNA sequence, copy-number variation, DNA methylation, messenger RNA (mRNA) sequence, and mRNA/microRNA expression. Additional samples were also analyzed by at least one of these genomic data types and associations between genomic characteristics of normal tissue and overall survival were assessed. Approximately 40% of cancer-adjacent, benign-appearing tissues harbored genomic defects in DNA copy number, sequence, methylation, or in RNA sequence, although these defects did not significantly predict 10-year overall survival. Two mRNA/microRNA expression phenotypes were observed, including an active mRNA subtype that was identified in 40% of samples. Controlling for tumor characteristics and the presence of genomic defects, this active subtype was associated with significantly worse 10-year survival among estrogen receptor (ER)-positive cases. This multi-platform analysis of breast cancer-adjacent samples produced genomic findings consistent with current surgical margin guidelines, and provides evidence that extratumoral RNA expression patterns in cancer-adjacent tissue predict overall survival among patients with ER-positive disease. Nature Publishing Group 2016-05-04 /pmc/articles/PMC5515343/ /pubmed/28721375 http://dx.doi.org/10.1038/npjbcancer.2016.7 Text en Copyright © 2016 Breast Cancer Research Foundation/Macmillan Publishers Limited http://creativecommons.org/licenses/by/4.0/ This work is licensed under a Creative Commons Attribution 4.0 International License. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in the credit line; if the material is not included under the Creative Commons license, users will need to obtain permission from the license holder to reproduce the material. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/
spellingShingle Article
Troester, Melissa A
Hoadley, Katherine A
D’Arcy, Monica
Cherniack, Andrew D
Stewart, Chip
Koboldt, Daniel C
Robertson, A Gordon
Mahurkar, Swapna
Shen, Hui
Wilkerson, Matthew D
Sandhu, Rupninder
Johnson, Nicole B
Allison, Kimberly H
Beck, Andrew H
Yau, Christina
Bowen, Jay
Sheth, Margi
Hwang, E Shelley
Perou, Charles M
Laird, Peter W
Ding, Li
Benz, Christopher C
DNA defects, epigenetics, and gene expression in cancer-adjacent breast: a study from The Cancer Genome Atlas
title DNA defects, epigenetics, and gene expression in cancer-adjacent breast: a study from The Cancer Genome Atlas
title_full DNA defects, epigenetics, and gene expression in cancer-adjacent breast: a study from The Cancer Genome Atlas
title_fullStr DNA defects, epigenetics, and gene expression in cancer-adjacent breast: a study from The Cancer Genome Atlas
title_full_unstemmed DNA defects, epigenetics, and gene expression in cancer-adjacent breast: a study from The Cancer Genome Atlas
title_short DNA defects, epigenetics, and gene expression in cancer-adjacent breast: a study from The Cancer Genome Atlas
title_sort dna defects, epigenetics, and gene expression in cancer-adjacent breast: a study from the cancer genome atlas
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5515343/
https://www.ncbi.nlm.nih.gov/pubmed/28721375
http://dx.doi.org/10.1038/npjbcancer.2016.7
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