Syndecan Binding Protein (SDCBP) Is Overexpressed in Estrogen Receptor Negative Breast Cancers, and Is a Potential Promoter for Tumor Proliferation

BACKGROUND: Syndecan binding protein (SDCBP), an adapter protein containing PDZ domains, contributes to the tumorigenicity and metastasis of many malignant tumors, such as malignant melanoma. Our study aimed in revealing the expression profile of SDCBP in breast cancer (BCa) and its role in tumor ce...

Descripción completa

Detalles Bibliográficos
Autores principales: Qian, Xiao-Long, Li, Ya-Qing, Yu, Bin, Gu, Feng, Liu, Fang-Fang, Li, Wei-Dong, Zhang, Xin-Min, Fu, Li
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3606191/
https://www.ncbi.nlm.nih.gov/pubmed/23533663
http://dx.doi.org/10.1371/journal.pone.0060046
_version_ 1782263963355971584
author Qian, Xiao-Long
Li, Ya-Qing
Yu, Bin
Gu, Feng
Liu, Fang-Fang
Li, Wei-Dong
Zhang, Xin-Min
Fu, Li
author_facet Qian, Xiao-Long
Li, Ya-Qing
Yu, Bin
Gu, Feng
Liu, Fang-Fang
Li, Wei-Dong
Zhang, Xin-Min
Fu, Li
author_sort Qian, Xiao-Long
collection PubMed
description BACKGROUND: Syndecan binding protein (SDCBP), an adapter protein containing PDZ domains, contributes to the tumorigenicity and metastasis of many malignant tumors, such as malignant melanoma. Our study aimed in revealing the expression profile of SDCBP in breast cancer (BCa) and its role in tumor cell proliferation, and then exploring its value in the targeted treatment of BCa. METHODOLOGY/PRINCIPAL FINDINGS: We first evaluated the SDCBP expression by immunohistochemistry in normal breast and BCa tissues. Then we explored the expression profile of SDCBP in different BCa cell lines. By constructing SDCBP-silenced BCa cell clones, we further assessed the effects of SDCBP suppression on tumor cells in vitro by cell culture and in vivo by tumorigenicity. SDCBP expression was detected in 80.6% (n = 160) of BCa tissues, in contrast to its expression in 13% (n = 23) of normal breast tissues (P<0.001). Among the tumors, the level of its expression was positively correlated with histological grade and tumor staging while negatively correlated with the estrogen receptor (ER) expression. Higher expression of SDCBP was also noted in ER-negative BCa cell lines. It was also identified that SDCBP expression was down-regulated in a dose-dependent mode by 17-β estradiol in estrogen-responsive MCF-7. Furthermore, SDCBP silence inhibited ER-negative tumor cell growth in vivo and in vitro. Cell cycle studies showed that SDCBP silence increased G1 cell population and resulted in related cell-cycle-regulator changes: up-regulation of p21 and p27 while down-regulation of cyclin E. CONCLUSION/SIGNIFICANCE: Our results suggested that SDCBP played an important role in tumor growth of ER-negative BCas. In these tumors where the estrogen signaling pathway is not available, SDCBP probably contribute to tumor growth through an alternative signaling pathway by promoting tumor cells passing the G1/S checkpoint into the cell cycle. Suppression of SDCBP expression may have its potential to become a targeted therapy for ER-negative BCas.
format Online
Article
Text
id pubmed-3606191
institution National Center for Biotechnology Information
language English
publishDate 2013
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-36061912013-03-26 Syndecan Binding Protein (SDCBP) Is Overexpressed in Estrogen Receptor Negative Breast Cancers, and Is a Potential Promoter for Tumor Proliferation Qian, Xiao-Long Li, Ya-Qing Yu, Bin Gu, Feng Liu, Fang-Fang Li, Wei-Dong Zhang, Xin-Min Fu, Li PLoS One Research Article BACKGROUND: Syndecan binding protein (SDCBP), an adapter protein containing PDZ domains, contributes to the tumorigenicity and metastasis of many malignant tumors, such as malignant melanoma. Our study aimed in revealing the expression profile of SDCBP in breast cancer (BCa) and its role in tumor cell proliferation, and then exploring its value in the targeted treatment of BCa. METHODOLOGY/PRINCIPAL FINDINGS: We first evaluated the SDCBP expression by immunohistochemistry in normal breast and BCa tissues. Then we explored the expression profile of SDCBP in different BCa cell lines. By constructing SDCBP-silenced BCa cell clones, we further assessed the effects of SDCBP suppression on tumor cells in vitro by cell culture and in vivo by tumorigenicity. SDCBP expression was detected in 80.6% (n = 160) of BCa tissues, in contrast to its expression in 13% (n = 23) of normal breast tissues (P<0.001). Among the tumors, the level of its expression was positively correlated with histological grade and tumor staging while negatively correlated with the estrogen receptor (ER) expression. Higher expression of SDCBP was also noted in ER-negative BCa cell lines. It was also identified that SDCBP expression was down-regulated in a dose-dependent mode by 17-β estradiol in estrogen-responsive MCF-7. Furthermore, SDCBP silence inhibited ER-negative tumor cell growth in vivo and in vitro. Cell cycle studies showed that SDCBP silence increased G1 cell population and resulted in related cell-cycle-regulator changes: up-regulation of p21 and p27 while down-regulation of cyclin E. CONCLUSION/SIGNIFICANCE: Our results suggested that SDCBP played an important role in tumor growth of ER-negative BCas. In these tumors where the estrogen signaling pathway is not available, SDCBP probably contribute to tumor growth through an alternative signaling pathway by promoting tumor cells passing the G1/S checkpoint into the cell cycle. Suppression of SDCBP expression may have its potential to become a targeted therapy for ER-negative BCas. Public Library of Science 2013-03-22 /pmc/articles/PMC3606191/ /pubmed/23533663 http://dx.doi.org/10.1371/journal.pone.0060046 Text en © 2013 Qian et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Qian, Xiao-Long
Li, Ya-Qing
Yu, Bin
Gu, Feng
Liu, Fang-Fang
Li, Wei-Dong
Zhang, Xin-Min
Fu, Li
Syndecan Binding Protein (SDCBP) Is Overexpressed in Estrogen Receptor Negative Breast Cancers, and Is a Potential Promoter for Tumor Proliferation
title Syndecan Binding Protein (SDCBP) Is Overexpressed in Estrogen Receptor Negative Breast Cancers, and Is a Potential Promoter for Tumor Proliferation
title_full Syndecan Binding Protein (SDCBP) Is Overexpressed in Estrogen Receptor Negative Breast Cancers, and Is a Potential Promoter for Tumor Proliferation
title_fullStr Syndecan Binding Protein (SDCBP) Is Overexpressed in Estrogen Receptor Negative Breast Cancers, and Is a Potential Promoter for Tumor Proliferation
title_full_unstemmed Syndecan Binding Protein (SDCBP) Is Overexpressed in Estrogen Receptor Negative Breast Cancers, and Is a Potential Promoter for Tumor Proliferation
title_short Syndecan Binding Protein (SDCBP) Is Overexpressed in Estrogen Receptor Negative Breast Cancers, and Is a Potential Promoter for Tumor Proliferation
title_sort syndecan binding protein (sdcbp) is overexpressed in estrogen receptor negative breast cancers, and is a potential promoter for tumor proliferation
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3606191/
https://www.ncbi.nlm.nih.gov/pubmed/23533663
http://dx.doi.org/10.1371/journal.pone.0060046
work_keys_str_mv AT qianxiaolong syndecanbindingproteinsdcbpisoverexpressedinestrogenreceptornegativebreastcancersandisapotentialpromoterfortumorproliferation
AT liyaqing syndecanbindingproteinsdcbpisoverexpressedinestrogenreceptornegativebreastcancersandisapotentialpromoterfortumorproliferation
AT yubin syndecanbindingproteinsdcbpisoverexpressedinestrogenreceptornegativebreastcancersandisapotentialpromoterfortumorproliferation
AT gufeng syndecanbindingproteinsdcbpisoverexpressedinestrogenreceptornegativebreastcancersandisapotentialpromoterfortumorproliferation
AT liufangfang syndecanbindingproteinsdcbpisoverexpressedinestrogenreceptornegativebreastcancersandisapotentialpromoterfortumorproliferation
AT liweidong syndecanbindingproteinsdcbpisoverexpressedinestrogenreceptornegativebreastcancersandisapotentialpromoterfortumorproliferation
AT zhangxinmin syndecanbindingproteinsdcbpisoverexpressedinestrogenreceptornegativebreastcancersandisapotentialpromoterfortumorproliferation
AT fuli syndecanbindingproteinsdcbpisoverexpressedinestrogenreceptornegativebreastcancersandisapotentialpromoterfortumorproliferation

Ejemplares similares