Tumor Evolution in Two Patients with Basal-like Breast Cancer: A Retrospective Genomics Study of Multiple Metastases

BACKGROUND: Metastasis is the main cause of cancer patient deaths and remains a poorly characterized process. It is still unclear when in tumor progression the ability to metastasize arises and whether this ability is inherent to the primary tumor or is acquired well after primary tumor formation. N...

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Autores principales: Hoadley, Katherine A., Siegel, Marni B., Kanchi, Krishna L., Miller, Christopher A., Ding, Li, Zhao, Wei, He, Xiaping, Parker, Joel S., Wendl, Michael C., Fulton, Robert S., Demeter, Ryan T., Wilson, Richard K., Carey, Lisa A., Perou, Charles M., Mardis, Elaine R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2016
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5140046/
https://www.ncbi.nlm.nih.gov/pubmed/27923045
http://dx.doi.org/10.1371/journal.pmed.1002174
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author Hoadley, Katherine A.
Siegel, Marni B.
Kanchi, Krishna L.
Miller, Christopher A.
Ding, Li
Zhao, Wei
He, Xiaping
Parker, Joel S.
Wendl, Michael C.
Fulton, Robert S.
Demeter, Ryan T.
Wilson, Richard K.
Carey, Lisa A.
Perou, Charles M.
Mardis, Elaine R.
author_facet Hoadley, Katherine A.
Siegel, Marni B.
Kanchi, Krishna L.
Miller, Christopher A.
Ding, Li
Zhao, Wei
He, Xiaping
Parker, Joel S.
Wendl, Michael C.
Fulton, Robert S.
Demeter, Ryan T.
Wilson, Richard K.
Carey, Lisa A.
Perou, Charles M.
Mardis, Elaine R.
author_sort Hoadley, Katherine A.
collection PubMed
description BACKGROUND: Metastasis is the main cause of cancer patient deaths and remains a poorly characterized process. It is still unclear when in tumor progression the ability to metastasize arises and whether this ability is inherent to the primary tumor or is acquired well after primary tumor formation. Next-generation sequencing and analytical methods to define clonal heterogeneity provide a means for identifying genetic events and the temporal relationships between these events in the primary and metastatic tumors within an individual. METHODS AND FINDINGS: We performed DNA whole genome and mRNA sequencing on two primary tumors, each with either four or five distinct tissue site-specific metastases, from two individuals with triple-negative/basal-like breast cancers. As evidenced by their case histories, each patient had an aggressive disease course with abbreviated survival. In each patient, the overall gene expression signatures, DNA copy number patterns, and somatic mutation patterns were highly similar across each primary tumor and its associated metastases. Almost every mutation found in the primary was found in a metastasis (for the two patients, 52/54 and 75/75). Many of these mutations were found in every tumor (11/54 and 65/75, respectively). In addition, each metastasis had fewer metastatic-specific events and shared at least 50% of its somatic mutation repertoire with the primary tumor, and all samples from each patient grouped together by gene expression clustering analysis. TP53 was the only mutated gene in common between both patients and was present in every tumor in this study. Strikingly, each metastasis resulted from multiclonal seeding instead of from a single cell of origin, and few of the new mutations, present only in the metastases, were expressed in mRNAs. Because of the clinical differences between these two patients and the small sample size of our study, the generalizability of these findings will need to be further examined in larger cohorts of patients. CONCLUSIONS: Our findings suggest that multiclonal seeding may be common amongst basal-like breast cancers. In these two patients, mutations and DNA copy number changes in the primary tumors appear to have had a biologic impact on metastatic potential, whereas mutations arising in the metastases were much more likely to be passengers.
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spelling pubmed-51400462016-12-21 Tumor Evolution in Two Patients with Basal-like Breast Cancer: A Retrospective Genomics Study of Multiple Metastases Hoadley, Katherine A. Siegel, Marni B. Kanchi, Krishna L. Miller, Christopher A. Ding, Li Zhao, Wei He, Xiaping Parker, Joel S. Wendl, Michael C. Fulton, Robert S. Demeter, Ryan T. Wilson, Richard K. Carey, Lisa A. Perou, Charles M. Mardis, Elaine R. PLoS Med Research Article BACKGROUND: Metastasis is the main cause of cancer patient deaths and remains a poorly characterized process. It is still unclear when in tumor progression the ability to metastasize arises and whether this ability is inherent to the primary tumor or is acquired well after primary tumor formation. Next-generation sequencing and analytical methods to define clonal heterogeneity provide a means for identifying genetic events and the temporal relationships between these events in the primary and metastatic tumors within an individual. METHODS AND FINDINGS: We performed DNA whole genome and mRNA sequencing on two primary tumors, each with either four or five distinct tissue site-specific metastases, from two individuals with triple-negative/basal-like breast cancers. As evidenced by their case histories, each patient had an aggressive disease course with abbreviated survival. In each patient, the overall gene expression signatures, DNA copy number patterns, and somatic mutation patterns were highly similar across each primary tumor and its associated metastases. Almost every mutation found in the primary was found in a metastasis (for the two patients, 52/54 and 75/75). Many of these mutations were found in every tumor (11/54 and 65/75, respectively). In addition, each metastasis had fewer metastatic-specific events and shared at least 50% of its somatic mutation repertoire with the primary tumor, and all samples from each patient grouped together by gene expression clustering analysis. TP53 was the only mutated gene in common between both patients and was present in every tumor in this study. Strikingly, each metastasis resulted from multiclonal seeding instead of from a single cell of origin, and few of the new mutations, present only in the metastases, were expressed in mRNAs. Because of the clinical differences between these two patients and the small sample size of our study, the generalizability of these findings will need to be further examined in larger cohorts of patients. CONCLUSIONS: Our findings suggest that multiclonal seeding may be common amongst basal-like breast cancers. In these two patients, mutations and DNA copy number changes in the primary tumors appear to have had a biologic impact on metastatic potential, whereas mutations arising in the metastases were much more likely to be passengers. Public Library of Science 2016-12-06 /pmc/articles/PMC5140046/ /pubmed/27923045 http://dx.doi.org/10.1371/journal.pmed.1002174 Text en © 2016 Hoadley 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
Hoadley, Katherine A.
Siegel, Marni B.
Kanchi, Krishna L.
Miller, Christopher A.
Ding, Li
Zhao, Wei
He, Xiaping
Parker, Joel S.
Wendl, Michael C.
Fulton, Robert S.
Demeter, Ryan T.
Wilson, Richard K.
Carey, Lisa A.
Perou, Charles M.
Mardis, Elaine R.
Tumor Evolution in Two Patients with Basal-like Breast Cancer: A Retrospective Genomics Study of Multiple Metastases
title Tumor Evolution in Two Patients with Basal-like Breast Cancer: A Retrospective Genomics Study of Multiple Metastases
title_full Tumor Evolution in Two Patients with Basal-like Breast Cancer: A Retrospective Genomics Study of Multiple Metastases
title_fullStr Tumor Evolution in Two Patients with Basal-like Breast Cancer: A Retrospective Genomics Study of Multiple Metastases
title_full_unstemmed Tumor Evolution in Two Patients with Basal-like Breast Cancer: A Retrospective Genomics Study of Multiple Metastases
title_short Tumor Evolution in Two Patients with Basal-like Breast Cancer: A Retrospective Genomics Study of Multiple Metastases
title_sort tumor evolution in two patients with basal-like breast cancer: a retrospective genomics study of multiple metastases
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5140046/
https://www.ncbi.nlm.nih.gov/pubmed/27923045
http://dx.doi.org/10.1371/journal.pmed.1002174
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