A candidate molecular signature associated with tamoxifen failure in primary breast cancer

INTRODUCTION: Few markers are available that can predict response to tamoxifen treatment in estrogen receptor (ER)-positive breast cancers. Identification of such markers would be clinically useful. We attempted to identify molecular markers associated with tamoxifen failure in breast cancer. METHOD...

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Autores principales: Vendrell, Julie A, Robertson, Katherine E, Ravel, Patrice, Bray, Susan E, Bajard, Agathe, Purdie, Colin A, Nguyen, Catherine, Hadad, Sirwan M, Bieche, Ivan, Chabaud, Sylvie, Bachelot, Thomas, Thompson, Alastair M, Cohen, Pascale A
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2008
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2614524/
https://www.ncbi.nlm.nih.gov/pubmed/18928543
http://dx.doi.org/10.1186/bcr2158
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author Vendrell, Julie A
Robertson, Katherine E
Ravel, Patrice
Bray, Susan E
Bajard, Agathe
Purdie, Colin A
Nguyen, Catherine
Hadad, Sirwan M
Bieche, Ivan
Chabaud, Sylvie
Bachelot, Thomas
Thompson, Alastair M
Cohen, Pascale A
author_facet Vendrell, Julie A
Robertson, Katherine E
Ravel, Patrice
Bray, Susan E
Bajard, Agathe
Purdie, Colin A
Nguyen, Catherine
Hadad, Sirwan M
Bieche, Ivan
Chabaud, Sylvie
Bachelot, Thomas
Thompson, Alastair M
Cohen, Pascale A
author_sort Vendrell, Julie A
collection PubMed
description INTRODUCTION: Few markers are available that can predict response to tamoxifen treatment in estrogen receptor (ER)-positive breast cancers. Identification of such markers would be clinically useful. We attempted to identify molecular markers associated with tamoxifen failure in breast cancer. METHODS: Eighteen initially ER-positive patients treated with tamoxifen requiring salvage surgery (tamoxifen failure [TF] patients) were compared with 17 patients who were disease free 5 years after surgery plus tamoxifen adjuvant therapy (control patients). cDNA microarray, real-time quantitative PCR, and immunohistochemistry on tissue microarrays were used to generate and confirm a gene signature associated with tamoxifen failure. An independent series of 33 breast tumor samples from patients who relapsed (n = 14) or did not relapse (n = 19) under tamoxifen treatment from a different geographic location was subsequently used to explore the gene expression signature identified. RESULTS: Using a screening set of 18 tumor samples (from eight control patients and 10 TF patients), a 47-gene signature discriminating between TF and control samples was identified using cDNA arrays. In addition to ESR1/ERα, the top-ranked genes selected by statistical cross-analyses were MET, FOS, SNCG, IGFBP4, and BCL2, which were subsequently validated in a larger set of tumor samples (from 17 control patients and 18 TF patients). Confirmation at the protein level by tissue microarray immunohistochemistry was observed for ER-α, γ-synuclein, and insulin-like growth factor binding protein 4 proteins in the 35 original samples. In an independent series of breast tumor samples (19 nonrelapsing and 14 relapsing), reduced expression of ESR1/ERα, IGFBP4, SNCG, BCL2, and FOS was observed in the relapsing group and was associated with a shorter overall survival. Low mRNA expression levels of ESR1/ERα, BCL2, and FOS were also associated with a shorter relapse-free survival (RFS). Using a Cox multivariate regression analysis, we identified BCL2 and FOS as independent prognostic markers associated with RFS. Finally, the BCL2/FOS signature was demonstrated to have more accurate prognostic value for RFS than ESR1/ERα alone (likelihood ratio test). CONCLUSIONS: We identified molecular markers including a BCL2/FOS signature associated with tamoxifen failure; these markers may have clinical potential in the management of ER-positive breast cancer.
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spelling pubmed-26145242009-01-08 A candidate molecular signature associated with tamoxifen failure in primary breast cancer Vendrell, Julie A Robertson, Katherine E Ravel, Patrice Bray, Susan E Bajard, Agathe Purdie, Colin A Nguyen, Catherine Hadad, Sirwan M Bieche, Ivan Chabaud, Sylvie Bachelot, Thomas Thompson, Alastair M Cohen, Pascale A Breast Cancer Res Research Article INTRODUCTION: Few markers are available that can predict response to tamoxifen treatment in estrogen receptor (ER)-positive breast cancers. Identification of such markers would be clinically useful. We attempted to identify molecular markers associated with tamoxifen failure in breast cancer. METHODS: Eighteen initially ER-positive patients treated with tamoxifen requiring salvage surgery (tamoxifen failure [TF] patients) were compared with 17 patients who were disease free 5 years after surgery plus tamoxifen adjuvant therapy (control patients). cDNA microarray, real-time quantitative PCR, and immunohistochemistry on tissue microarrays were used to generate and confirm a gene signature associated with tamoxifen failure. An independent series of 33 breast tumor samples from patients who relapsed (n = 14) or did not relapse (n = 19) under tamoxifen treatment from a different geographic location was subsequently used to explore the gene expression signature identified. RESULTS: Using a screening set of 18 tumor samples (from eight control patients and 10 TF patients), a 47-gene signature discriminating between TF and control samples was identified using cDNA arrays. In addition to ESR1/ERα, the top-ranked genes selected by statistical cross-analyses were MET, FOS, SNCG, IGFBP4, and BCL2, which were subsequently validated in a larger set of tumor samples (from 17 control patients and 18 TF patients). Confirmation at the protein level by tissue microarray immunohistochemistry was observed for ER-α, γ-synuclein, and insulin-like growth factor binding protein 4 proteins in the 35 original samples. In an independent series of breast tumor samples (19 nonrelapsing and 14 relapsing), reduced expression of ESR1/ERα, IGFBP4, SNCG, BCL2, and FOS was observed in the relapsing group and was associated with a shorter overall survival. Low mRNA expression levels of ESR1/ERα, BCL2, and FOS were also associated with a shorter relapse-free survival (RFS). Using a Cox multivariate regression analysis, we identified BCL2 and FOS as independent prognostic markers associated with RFS. Finally, the BCL2/FOS signature was demonstrated to have more accurate prognostic value for RFS than ESR1/ERα alone (likelihood ratio test). CONCLUSIONS: We identified molecular markers including a BCL2/FOS signature associated with tamoxifen failure; these markers may have clinical potential in the management of ER-positive breast cancer. BioMed Central 2008 2008-10-17 /pmc/articles/PMC2614524/ /pubmed/18928543 http://dx.doi.org/10.1186/bcr2158 Text en Copyright © 2008 Vendrell 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
Vendrell, Julie A
Robertson, Katherine E
Ravel, Patrice
Bray, Susan E
Bajard, Agathe
Purdie, Colin A
Nguyen, Catherine
Hadad, Sirwan M
Bieche, Ivan
Chabaud, Sylvie
Bachelot, Thomas
Thompson, Alastair M
Cohen, Pascale A
A candidate molecular signature associated with tamoxifen failure in primary breast cancer
title A candidate molecular signature associated with tamoxifen failure in primary breast cancer
title_full A candidate molecular signature associated with tamoxifen failure in primary breast cancer
title_fullStr A candidate molecular signature associated with tamoxifen failure in primary breast cancer
title_full_unstemmed A candidate molecular signature associated with tamoxifen failure in primary breast cancer
title_short A candidate molecular signature associated with tamoxifen failure in primary breast cancer
title_sort candidate molecular signature associated with tamoxifen failure in primary breast cancer
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2614524/
https://www.ncbi.nlm.nih.gov/pubmed/18928543
http://dx.doi.org/10.1186/bcr2158
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