Identification of a Putative Protein Profile Associated with Tamoxifen Therapy Resistance in Breast Cancer

Tamoxifen resistance is a major cause of death in patients with recurrent breast cancer. Current clinical factors can correctly predict therapy response in only half of the treated patients. Identification of proteins that are associated with tamoxifen resistance is a first step toward better respon...

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Autores principales: Umar, Arzu, Kang, Hyuk, Timmermans, Annemieke M., Look, Maxime P., Meijer-van Gelder, Marion E., den Bakker, Michael A., Jaitly, Navdeep, Martens, John W. M., Luider, Theo M., Foekens, John A., Paša-Tolić, Ljiljana
Formato: Texto
Lenguaje:English
Publicado: American Society for Biochemistry and Molecular Biology 2009
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2690491/
https://www.ncbi.nlm.nih.gov/pubmed/19329653
http://dx.doi.org/10.1074/mcp.M800493-MCP200
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author Umar, Arzu
Kang, Hyuk
Timmermans, Annemieke M.
Look, Maxime P.
Meijer-van Gelder, Marion E.
den Bakker, Michael A.
Jaitly, Navdeep
Martens, John W. M.
Luider, Theo M.
Foekens, John A.
Paša-Tolić, Ljiljana
author_facet Umar, Arzu
Kang, Hyuk
Timmermans, Annemieke M.
Look, Maxime P.
Meijer-van Gelder, Marion E.
den Bakker, Michael A.
Jaitly, Navdeep
Martens, John W. M.
Luider, Theo M.
Foekens, John A.
Paša-Tolić, Ljiljana
author_sort Umar, Arzu
collection PubMed
description Tamoxifen resistance is a major cause of death in patients with recurrent breast cancer. Current clinical factors can correctly predict therapy response in only half of the treated patients. Identification of proteins that are associated with tamoxifen resistance is a first step toward better response prediction and tailored treatment of patients. In the present study we intended to identify putative protein biomarkers indicative of tamoxifen therapy resistance in breast cancer using nano-LC coupled with FTICR MS. Comparative proteome analysis was performed on ∼5,500 pooled tumor cells (corresponding to ∼550 ng of protein lysate/analysis) obtained through laser capture microdissection (LCM) from two independently processed data sets (n = 24 and n = 27) containing both tamoxifen therapy-sensitive and therapy-resistant tumors. Peptides and proteins were identified by matching mass and elution time of newly acquired LC-MS features to information in previously generated accurate mass and time tag reference databases. A total of 17,263 unique peptides were identified that corresponded to 2,556 non-redundant proteins identified with ≥2 peptides. 1,713 overlapping proteins between the two data sets were used for further analysis. Comparative proteome analysis revealed 100 putatively differentially abundant proteins between tamoxifen-sensitive and tamoxifen-resistant tumors. The presence and relative abundance for 47 differentially abundant proteins were verified by targeted nano-LC-MS/MS in a selection of unpooled, non-microdissected discovery set tumor tissue extracts. ENPP1, EIF3E, and GNB4 were significantly associated with progression-free survival upon tamoxifen treatment for recurrent disease. Differential abundance of our top discriminating protein, extracellular matrix metalloproteinase inducer, was validated by tissue microarray in an independent patient cohort (n = 156). Extracellular matrix metalloproteinase inducer levels were higher in therapy-resistant tumors and significantly associated with an earlier tumor progression following first line tamoxifen treatment (hazard ratio, 1.87; 95% confidence interval, 1.25–2.80; p = 0.002). In summary, comparative proteomics performed on laser capture microdissection-derived breast tumor cells using nano-LC-FTICR MS technology revealed a set of putative biomarkers associated with tamoxifen therapy resistance in recurrent breast cancer.
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spelling pubmed-26904912009-07-24 Identification of a Putative Protein Profile Associated with Tamoxifen Therapy Resistance in Breast Cancer Umar, Arzu Kang, Hyuk Timmermans, Annemieke M. Look, Maxime P. Meijer-van Gelder, Marion E. den Bakker, Michael A. Jaitly, Navdeep Martens, John W. M. Luider, Theo M. Foekens, John A. Paša-Tolić, Ljiljana Mol Cell Proteomics Research Tamoxifen resistance is a major cause of death in patients with recurrent breast cancer. Current clinical factors can correctly predict therapy response in only half of the treated patients. Identification of proteins that are associated with tamoxifen resistance is a first step toward better response prediction and tailored treatment of patients. In the present study we intended to identify putative protein biomarkers indicative of tamoxifen therapy resistance in breast cancer using nano-LC coupled with FTICR MS. Comparative proteome analysis was performed on ∼5,500 pooled tumor cells (corresponding to ∼550 ng of protein lysate/analysis) obtained through laser capture microdissection (LCM) from two independently processed data sets (n = 24 and n = 27) containing both tamoxifen therapy-sensitive and therapy-resistant tumors. Peptides and proteins were identified by matching mass and elution time of newly acquired LC-MS features to information in previously generated accurate mass and time tag reference databases. A total of 17,263 unique peptides were identified that corresponded to 2,556 non-redundant proteins identified with ≥2 peptides. 1,713 overlapping proteins between the two data sets were used for further analysis. Comparative proteome analysis revealed 100 putatively differentially abundant proteins between tamoxifen-sensitive and tamoxifen-resistant tumors. The presence and relative abundance for 47 differentially abundant proteins were verified by targeted nano-LC-MS/MS in a selection of unpooled, non-microdissected discovery set tumor tissue extracts. ENPP1, EIF3E, and GNB4 were significantly associated with progression-free survival upon tamoxifen treatment for recurrent disease. Differential abundance of our top discriminating protein, extracellular matrix metalloproteinase inducer, was validated by tissue microarray in an independent patient cohort (n = 156). Extracellular matrix metalloproteinase inducer levels were higher in therapy-resistant tumors and significantly associated with an earlier tumor progression following first line tamoxifen treatment (hazard ratio, 1.87; 95% confidence interval, 1.25–2.80; p = 0.002). In summary, comparative proteomics performed on laser capture microdissection-derived breast tumor cells using nano-LC-FTICR MS technology revealed a set of putative biomarkers associated with tamoxifen therapy resistance in recurrent breast cancer. American Society for Biochemistry and Molecular Biology 2009-06 /pmc/articles/PMC2690491/ /pubmed/19329653 http://dx.doi.org/10.1074/mcp.M800493-MCP200 Text en Copyright © 2009, The American Society for Biochemistry and Molecular Biology Author's Choice - Final Version Full Access NIH Funded Research - Final Version Full Access Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/3.0/) applies to Author Choice Articles
spellingShingle Research
Umar, Arzu
Kang, Hyuk
Timmermans, Annemieke M.
Look, Maxime P.
Meijer-van Gelder, Marion E.
den Bakker, Michael A.
Jaitly, Navdeep
Martens, John W. M.
Luider, Theo M.
Foekens, John A.
Paša-Tolić, Ljiljana
Identification of a Putative Protein Profile Associated with Tamoxifen Therapy Resistance in Breast Cancer
title Identification of a Putative Protein Profile Associated with Tamoxifen Therapy Resistance in Breast Cancer
title_full Identification of a Putative Protein Profile Associated with Tamoxifen Therapy Resistance in Breast Cancer
title_fullStr Identification of a Putative Protein Profile Associated with Tamoxifen Therapy Resistance in Breast Cancer
title_full_unstemmed Identification of a Putative Protein Profile Associated with Tamoxifen Therapy Resistance in Breast Cancer
title_short Identification of a Putative Protein Profile Associated with Tamoxifen Therapy Resistance in Breast Cancer
title_sort identification of a putative protein profile associated with tamoxifen therapy resistance in breast cancer
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2690491/
https://www.ncbi.nlm.nih.gov/pubmed/19329653
http://dx.doi.org/10.1074/mcp.M800493-MCP200
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