Breast tumor copy number aberration phenotypes and genomic instability

BACKGROUND: Genomic DNA copy number aberrations are frequent in solid tumors, although the underlying causes of chromosomal instability in tumors remain obscure. Genes likely to have genomic instability phenotypes when mutated (e.g. those involved in mitosis, replication, repair, and telomeres) are...

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Autores principales: Fridlyand, Jane, Snijders, Antoine M, Ylstra, Bauke, Li, Hua, Olshen, Adam, Segraves, Richard, Dairkee, Shanaz, Tokuyasu, Taku, Ljung, Britt Marie, Jain, Ajay N, McLennan, Jane, Ziegler, John, Chin, Koei, Devries, Sandy, Feiler, Heidi, Gray, Joe W, Waldman, Frederic, Pinkel, Daniel, Albertson, Donna G
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2006
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1459181/
https://www.ncbi.nlm.nih.gov/pubmed/16620391
http://dx.doi.org/10.1186/1471-2407-6-96
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author Fridlyand, Jane
Snijders, Antoine M
Ylstra, Bauke
Li, Hua
Olshen, Adam
Segraves, Richard
Dairkee, Shanaz
Tokuyasu, Taku
Ljung, Britt Marie
Jain, Ajay N
McLennan, Jane
Ziegler, John
Chin, Koei
Devries, Sandy
Feiler, Heidi
Gray, Joe W
Waldman, Frederic
Pinkel, Daniel
Albertson, Donna G
author_facet Fridlyand, Jane
Snijders, Antoine M
Ylstra, Bauke
Li, Hua
Olshen, Adam
Segraves, Richard
Dairkee, Shanaz
Tokuyasu, Taku
Ljung, Britt Marie
Jain, Ajay N
McLennan, Jane
Ziegler, John
Chin, Koei
Devries, Sandy
Feiler, Heidi
Gray, Joe W
Waldman, Frederic
Pinkel, Daniel
Albertson, Donna G
author_sort Fridlyand, Jane
collection PubMed
description BACKGROUND: Genomic DNA copy number aberrations are frequent in solid tumors, although the underlying causes of chromosomal instability in tumors remain obscure. Genes likely to have genomic instability phenotypes when mutated (e.g. those involved in mitosis, replication, repair, and telomeres) are rarely mutated in chromosomally unstable sporadic tumors, even though such mutations are associated with some heritable cancer prone syndromes. METHODS: We applied array comparative genomic hybridization (CGH) to the analysis of breast tumors. The variation in the levels of genomic instability amongst tumors prompted us to investigate whether alterations in processes/genes involved in maintenance and/or manipulation of the genome were associated with particular types of genomic instability. RESULTS: We discriminated three breast tumor subtypes based on genomic DNA copy number alterations. The subtypes varied with respect to level of genomic instability. We find that shorter telomeres and altered telomere related gene expression are associated with amplification, implicating telomere attrition as a promoter of this type of aberration in breast cancer. On the other hand, the numbers of chromosomal alterations, particularly low level changes, are associated with altered expression of genes in other functional classes (mitosis, cell cycle, DNA replication and repair). Further, although loss of function instability phenotypes have been demonstrated for many of the genes in model systems, we observed enhanced expression of most genes in tumors, indicating that over expression, rather than deficiency underlies instability. CONCLUSION: Many of the genes associated with higher frequency of copy number aberrations are direct targets of E2F, supporting the hypothesis that deregulation of the Rb pathway is a major contributor to chromosomal instability in breast tumors. These observations are consistent with failure to find mutations in sporadic tumors in genes that have roles in maintenance or manipulation of the genome.
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spelling pubmed-14591812006-05-11 Breast tumor copy number aberration phenotypes and genomic instability Fridlyand, Jane Snijders, Antoine M Ylstra, Bauke Li, Hua Olshen, Adam Segraves, Richard Dairkee, Shanaz Tokuyasu, Taku Ljung, Britt Marie Jain, Ajay N McLennan, Jane Ziegler, John Chin, Koei Devries, Sandy Feiler, Heidi Gray, Joe W Waldman, Frederic Pinkel, Daniel Albertson, Donna G BMC Cancer Research Article BACKGROUND: Genomic DNA copy number aberrations are frequent in solid tumors, although the underlying causes of chromosomal instability in tumors remain obscure. Genes likely to have genomic instability phenotypes when mutated (e.g. those involved in mitosis, replication, repair, and telomeres) are rarely mutated in chromosomally unstable sporadic tumors, even though such mutations are associated with some heritable cancer prone syndromes. METHODS: We applied array comparative genomic hybridization (CGH) to the analysis of breast tumors. The variation in the levels of genomic instability amongst tumors prompted us to investigate whether alterations in processes/genes involved in maintenance and/or manipulation of the genome were associated with particular types of genomic instability. RESULTS: We discriminated three breast tumor subtypes based on genomic DNA copy number alterations. The subtypes varied with respect to level of genomic instability. We find that shorter telomeres and altered telomere related gene expression are associated with amplification, implicating telomere attrition as a promoter of this type of aberration in breast cancer. On the other hand, the numbers of chromosomal alterations, particularly low level changes, are associated with altered expression of genes in other functional classes (mitosis, cell cycle, DNA replication and repair). Further, although loss of function instability phenotypes have been demonstrated for many of the genes in model systems, we observed enhanced expression of most genes in tumors, indicating that over expression, rather than deficiency underlies instability. CONCLUSION: Many of the genes associated with higher frequency of copy number aberrations are direct targets of E2F, supporting the hypothesis that deregulation of the Rb pathway is a major contributor to chromosomal instability in breast tumors. These observations are consistent with failure to find mutations in sporadic tumors in genes that have roles in maintenance or manipulation of the genome. BioMed Central 2006-04-18 /pmc/articles/PMC1459181/ /pubmed/16620391 http://dx.doi.org/10.1186/1471-2407-6-96 Text en Copyright © 2006 Fridlyand et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( (http://creativecommons.org/licenses/by/2.0) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Fridlyand, Jane
Snijders, Antoine M
Ylstra, Bauke
Li, Hua
Olshen, Adam
Segraves, Richard
Dairkee, Shanaz
Tokuyasu, Taku
Ljung, Britt Marie
Jain, Ajay N
McLennan, Jane
Ziegler, John
Chin, Koei
Devries, Sandy
Feiler, Heidi
Gray, Joe W
Waldman, Frederic
Pinkel, Daniel
Albertson, Donna G
Breast tumor copy number aberration phenotypes and genomic instability
title Breast tumor copy number aberration phenotypes and genomic instability
title_full Breast tumor copy number aberration phenotypes and genomic instability
title_fullStr Breast tumor copy number aberration phenotypes and genomic instability
title_full_unstemmed Breast tumor copy number aberration phenotypes and genomic instability
title_short Breast tumor copy number aberration phenotypes and genomic instability
title_sort breast tumor copy number aberration phenotypes and genomic instability
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1459181/
https://www.ncbi.nlm.nih.gov/pubmed/16620391
http://dx.doi.org/10.1186/1471-2407-6-96
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