Genetic variability in MCF-7 sublines: evidence of rapid genomic and RNA expression profile modifications

BACKGROUND: Both phenotypic and cytogenetic variability have been reported for clones of breast carcinoma cell lines but have not been comprehensively studied. Despite this, cell lines such as MCF-7 cells are extensively used as model systems. METHODS: In this work we documented, using CGH and RNA e...

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Autores principales: Nugoli, Mélanie, Chuchana, Paul, Vendrell, Julie, Orsetti, Béatrice, Ursule, Lisa, Nguyen, Catherine, Birnbaum, Daniel, Douzery, Emmanuel JP, Cohen, Pascale, Theillet, Charles
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2003
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC156633/
https://www.ncbi.nlm.nih.gov/pubmed/12713671
http://dx.doi.org/10.1186/1471-2407-3-13
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author Nugoli, Mélanie
Chuchana, Paul
Vendrell, Julie
Orsetti, Béatrice
Ursule, Lisa
Nguyen, Catherine
Birnbaum, Daniel
Douzery, Emmanuel JP
Cohen, Pascale
Theillet, Charles
author_facet Nugoli, Mélanie
Chuchana, Paul
Vendrell, Julie
Orsetti, Béatrice
Ursule, Lisa
Nguyen, Catherine
Birnbaum, Daniel
Douzery, Emmanuel JP
Cohen, Pascale
Theillet, Charles
author_sort Nugoli, Mélanie
collection PubMed
description BACKGROUND: Both phenotypic and cytogenetic variability have been reported for clones of breast carcinoma cell lines but have not been comprehensively studied. Despite this, cell lines such as MCF-7 cells are extensively used as model systems. METHODS: In this work we documented, using CGH and RNA expression profiles, the genetic variability at the genomic and RNA expression levels of MCF-7 cells of different origins. Eight MCF-7 sublines collected from different sources were studied as well as 3 subclones isolated from one of the sublines by limit dilution. RESULTS: MCF-7 sublines showed important differences in copy number alteration (CNA) profiles. Overall numbers of events ranged from 28 to 41. Involved chromosomal regions varied greatly from a subline to another. A total of 62 chromosomal regions were affected by either gains or losses in the 11 sublines studied. We performed a phylogenetic analysis of CGH profiles using maximum parsimony in order to reconstruct the putative filiation of the 11 MCF-7 sublines. The phylogenetic tree obtained showed that the MCF-7 clade was characterized by a restricted set of 8 CNAs and that the most divergent subline occupied the position closest to the common ancestor. Expression profiles of 8 MCF-7 sublines were analyzed along with those of 19 unrelated breast cancer cell lines using home made cDNA arrays comprising 720 genes. Hierarchical clustering analysis of the expression data showed that 7/8 MCF-7 sublines were grouped forming a cluster while the remaining subline clustered with unrelated breast cancer cell lines. These data thus showed that MCF-7 sublines differed at both the genomic and phenotypic levels. CONCLUSIONS: The analysis of CGH profiles of the parent subline and its three subclones supported the heteroclonal nature of MCF-7 cells. This strongly suggested that the genetic plasticity of MCF-7 cells was related to their intrinsic capacity to generate clonal heterogeneity. We propose that MCF-7, and possibly the breast tumor it was derived from, evolved in a node like pattern, rather than according to a linear progression model. Due to their capacity to undergo rapid genetic changes MCF-7 cells could represent an interesting model for genetic evolution of breast tumors.
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spelling pubmed-1566332003-06-05 Genetic variability in MCF-7 sublines: evidence of rapid genomic and RNA expression profile modifications Nugoli, Mélanie Chuchana, Paul Vendrell, Julie Orsetti, Béatrice Ursule, Lisa Nguyen, Catherine Birnbaum, Daniel Douzery, Emmanuel JP Cohen, Pascale Theillet, Charles BMC Cancer Research Article BACKGROUND: Both phenotypic and cytogenetic variability have been reported for clones of breast carcinoma cell lines but have not been comprehensively studied. Despite this, cell lines such as MCF-7 cells are extensively used as model systems. METHODS: In this work we documented, using CGH and RNA expression profiles, the genetic variability at the genomic and RNA expression levels of MCF-7 cells of different origins. Eight MCF-7 sublines collected from different sources were studied as well as 3 subclones isolated from one of the sublines by limit dilution. RESULTS: MCF-7 sublines showed important differences in copy number alteration (CNA) profiles. Overall numbers of events ranged from 28 to 41. Involved chromosomal regions varied greatly from a subline to another. A total of 62 chromosomal regions were affected by either gains or losses in the 11 sublines studied. We performed a phylogenetic analysis of CGH profiles using maximum parsimony in order to reconstruct the putative filiation of the 11 MCF-7 sublines. The phylogenetic tree obtained showed that the MCF-7 clade was characterized by a restricted set of 8 CNAs and that the most divergent subline occupied the position closest to the common ancestor. Expression profiles of 8 MCF-7 sublines were analyzed along with those of 19 unrelated breast cancer cell lines using home made cDNA arrays comprising 720 genes. Hierarchical clustering analysis of the expression data showed that 7/8 MCF-7 sublines were grouped forming a cluster while the remaining subline clustered with unrelated breast cancer cell lines. These data thus showed that MCF-7 sublines differed at both the genomic and phenotypic levels. CONCLUSIONS: The analysis of CGH profiles of the parent subline and its three subclones supported the heteroclonal nature of MCF-7 cells. This strongly suggested that the genetic plasticity of MCF-7 cells was related to their intrinsic capacity to generate clonal heterogeneity. We propose that MCF-7, and possibly the breast tumor it was derived from, evolved in a node like pattern, rather than according to a linear progression model. Due to their capacity to undergo rapid genetic changes MCF-7 cells could represent an interesting model for genetic evolution of breast tumors. BioMed Central 2003-04-24 /pmc/articles/PMC156633/ /pubmed/12713671 http://dx.doi.org/10.1186/1471-2407-3-13 Text en Copyright © 2003 Nugoli et al; licensee BioMed Central Ltd. This is an Open Access article: verbatim copying and redistribution of this article are permitted in all media for any purpose, provided this notice is preserved along with the article's original URL.
spellingShingle Research Article
Nugoli, Mélanie
Chuchana, Paul
Vendrell, Julie
Orsetti, Béatrice
Ursule, Lisa
Nguyen, Catherine
Birnbaum, Daniel
Douzery, Emmanuel JP
Cohen, Pascale
Theillet, Charles
Genetic variability in MCF-7 sublines: evidence of rapid genomic and RNA expression profile modifications
title Genetic variability in MCF-7 sublines: evidence of rapid genomic and RNA expression profile modifications
title_full Genetic variability in MCF-7 sublines: evidence of rapid genomic and RNA expression profile modifications
title_fullStr Genetic variability in MCF-7 sublines: evidence of rapid genomic and RNA expression profile modifications
title_full_unstemmed Genetic variability in MCF-7 sublines: evidence of rapid genomic and RNA expression profile modifications
title_short Genetic variability in MCF-7 sublines: evidence of rapid genomic and RNA expression profile modifications
title_sort genetic variability in mcf-7 sublines: evidence of rapid genomic and rna expression profile modifications
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC156633/
https://www.ncbi.nlm.nih.gov/pubmed/12713671
http://dx.doi.org/10.1186/1471-2407-3-13
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