Breast cancer proteomics reveals correlation between estrogen receptor status and differential phosphorylation of PGRMC1

INTRODUCTION: Breast tumors lacking the estrogen receptor-α (ER-α) have increased incidence of resistance to therapy and poorer clinical prognosis. METHODS: Whole tissue sections from 16 cryopreserved breast cancer tumors that were either positive or negative for the ER (eight ER positive and eight...

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Autores principales: Neubauer, Hans, Clare, Susan E, Wozny, Wojciech, Schwall, Gerhard P, Poznanović, Slobodan, Stegmann, Werner, Vogel, Ulrich, Sotlar, Karl, Wallwiener, Diethelm, Kurek, Raffael, Fehm, Tanja, Cahill, Michael A
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2008
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2614521/
https://www.ncbi.nlm.nih.gov/pubmed/18922159
http://dx.doi.org/10.1186/bcr2155
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author Neubauer, Hans
Clare, Susan E
Wozny, Wojciech
Schwall, Gerhard P
Poznanović, Slobodan
Stegmann, Werner
Vogel, Ulrich
Sotlar, Karl
Wallwiener, Diethelm
Kurek, Raffael
Fehm, Tanja
Cahill, Michael A
author_facet Neubauer, Hans
Clare, Susan E
Wozny, Wojciech
Schwall, Gerhard P
Poznanović, Slobodan
Stegmann, Werner
Vogel, Ulrich
Sotlar, Karl
Wallwiener, Diethelm
Kurek, Raffael
Fehm, Tanja
Cahill, Michael A
author_sort Neubauer, Hans
collection PubMed
description INTRODUCTION: Breast tumors lacking the estrogen receptor-α (ER-α) have increased incidence of resistance to therapy and poorer clinical prognosis. METHODS: Whole tissue sections from 16 cryopreserved breast cancer tumors that were either positive or negative for the ER (eight ER positive and eight ER negative) were differentially analyzed by multiplex imaging of two-dimensional PAGE gels using 54 cm isoelectric focusing. Differentially detected spots of Progesterone Receptor Membrane Component 1 (PGRMC1) were shown to differ in phosphorylation status by differential two dimensional polyacrylamide gel electrophoresis of phosphatase-treated tumor proteins. Site directed mutagenesis was used to create putative phosphorylation site point mutants in PGRMC1. Stable transfectants of these mutants in MCF7 cells were assayed for their survival after oxidative stress, and for AKT kinase phosphorylation. Immune fluorescence using anti-PGRMC1 monoclonal antibody 5G7 was performed on breast cancer tissue microarrays. RESULTS: Proteins significantly differentially abundant between estrogen receptor negative and estrogen receptor positive tumors at the 0.1% level were consistent with published profiles, suggesting an altered keratin pool, and increased inflammation and wound responses in estrogen receptor negative tumors. Two of three spots of PGRMC1 were more abundant in estrogen receptor negative tumors. Phosphatase treatment of breast tumor proteins indicated that the PGRMC1 isoforms differed in their phosphorylation status. Simultaneous mutation of PGRMC1 serine-56 and serine-181 fully abrogated the sensitivity of stably transfected MCF7 breast cancer cells to peroxide-induced cell death. Immune fluorescence revealed that PGRMC1 was primarily expressed in ER-negative basal epithelial cells of mammary ductules. Even in advanced tumors, high levels of ER or PGRMC1 were almost mutually exclusive in individual cells. In five out of five examined ductal in situ breast cancers of comedo type, PGRMC1 was expressed in glucose transporter 1 negative or positive poorly oxygenated cells surrounding the necrotic core, surrounded by a more distal halo of ER-positive cells. CONCLUSIONS: PGRMC1 phosphorylation may be involved in the clinical differences that underpin breast tumors of differing ER status.
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spelling pubmed-26145212009-01-08 Breast cancer proteomics reveals correlation between estrogen receptor status and differential phosphorylation of PGRMC1 Neubauer, Hans Clare, Susan E Wozny, Wojciech Schwall, Gerhard P Poznanović, Slobodan Stegmann, Werner Vogel, Ulrich Sotlar, Karl Wallwiener, Diethelm Kurek, Raffael Fehm, Tanja Cahill, Michael A Breast Cancer Res Research Article INTRODUCTION: Breast tumors lacking the estrogen receptor-α (ER-α) have increased incidence of resistance to therapy and poorer clinical prognosis. METHODS: Whole tissue sections from 16 cryopreserved breast cancer tumors that were either positive or negative for the ER (eight ER positive and eight ER negative) were differentially analyzed by multiplex imaging of two-dimensional PAGE gels using 54 cm isoelectric focusing. Differentially detected spots of Progesterone Receptor Membrane Component 1 (PGRMC1) were shown to differ in phosphorylation status by differential two dimensional polyacrylamide gel electrophoresis of phosphatase-treated tumor proteins. Site directed mutagenesis was used to create putative phosphorylation site point mutants in PGRMC1. Stable transfectants of these mutants in MCF7 cells were assayed for their survival after oxidative stress, and for AKT kinase phosphorylation. Immune fluorescence using anti-PGRMC1 monoclonal antibody 5G7 was performed on breast cancer tissue microarrays. RESULTS: Proteins significantly differentially abundant between estrogen receptor negative and estrogen receptor positive tumors at the 0.1% level were consistent with published profiles, suggesting an altered keratin pool, and increased inflammation and wound responses in estrogen receptor negative tumors. Two of three spots of PGRMC1 were more abundant in estrogen receptor negative tumors. Phosphatase treatment of breast tumor proteins indicated that the PGRMC1 isoforms differed in their phosphorylation status. Simultaneous mutation of PGRMC1 serine-56 and serine-181 fully abrogated the sensitivity of stably transfected MCF7 breast cancer cells to peroxide-induced cell death. Immune fluorescence revealed that PGRMC1 was primarily expressed in ER-negative basal epithelial cells of mammary ductules. Even in advanced tumors, high levels of ER or PGRMC1 were almost mutually exclusive in individual cells. In five out of five examined ductal in situ breast cancers of comedo type, PGRMC1 was expressed in glucose transporter 1 negative or positive poorly oxygenated cells surrounding the necrotic core, surrounded by a more distal halo of ER-positive cells. CONCLUSIONS: PGRMC1 phosphorylation may be involved in the clinical differences that underpin breast tumors of differing ER status. BioMed Central 2008 2008-10-15 /pmc/articles/PMC2614521/ /pubmed/18922159 http://dx.doi.org/10.1186/bcr2155 Text en Copyright © 2008 Neubauer 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
Neubauer, Hans
Clare, Susan E
Wozny, Wojciech
Schwall, Gerhard P
Poznanović, Slobodan
Stegmann, Werner
Vogel, Ulrich
Sotlar, Karl
Wallwiener, Diethelm
Kurek, Raffael
Fehm, Tanja
Cahill, Michael A
Breast cancer proteomics reveals correlation between estrogen receptor status and differential phosphorylation of PGRMC1
title Breast cancer proteomics reveals correlation between estrogen receptor status and differential phosphorylation of PGRMC1
title_full Breast cancer proteomics reveals correlation between estrogen receptor status and differential phosphorylation of PGRMC1
title_fullStr Breast cancer proteomics reveals correlation between estrogen receptor status and differential phosphorylation of PGRMC1
title_full_unstemmed Breast cancer proteomics reveals correlation between estrogen receptor status and differential phosphorylation of PGRMC1
title_short Breast cancer proteomics reveals correlation between estrogen receptor status and differential phosphorylation of PGRMC1
title_sort breast cancer proteomics reveals correlation between estrogen receptor status and differential phosphorylation of pgrmc1
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2614521/
https://www.ncbi.nlm.nih.gov/pubmed/18922159
http://dx.doi.org/10.1186/bcr2155
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