Loss of the Urothelial Differentiation Marker FOXA1 Is Associated with High Grade, Late Stage Bladder Cancer and Increased Tumor Proliferation

Approximately 50% of patients with muscle-invasive bladder cancer (MIBC) develop metastatic disease, which is almost invariably lethal. However, our understanding of pathways that drive aggressive behavior of MIBC is incomplete. Members of the FOXA subfamily of transcription factors are implicated i...

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Autores principales: DeGraff, David J., Clark, Peter E., Cates, Justin M., Yamashita, Hironobu, Robinson, Victoria L., Yu, Xiuping, Smolkin, Mark E., Chang, Sam S., Cookson, Michael S., Herrick, Mary K., Shariat, Shahrokh F., Steinberg, Gary D., Frierson, Henry F., Wu, Xue-Ru, Theodorescu, Dan, Matusik, Robert J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3349679/
https://www.ncbi.nlm.nih.gov/pubmed/22590586
http://dx.doi.org/10.1371/journal.pone.0036669
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author DeGraff, David J.
Clark, Peter E.
Cates, Justin M.
Yamashita, Hironobu
Robinson, Victoria L.
Yu, Xiuping
Smolkin, Mark E.
Chang, Sam S.
Cookson, Michael S.
Herrick, Mary K.
Shariat, Shahrokh F.
Steinberg, Gary D.
Frierson, Henry F.
Wu, Xue-Ru
Theodorescu, Dan
Matusik, Robert J.
author_facet DeGraff, David J.
Clark, Peter E.
Cates, Justin M.
Yamashita, Hironobu
Robinson, Victoria L.
Yu, Xiuping
Smolkin, Mark E.
Chang, Sam S.
Cookson, Michael S.
Herrick, Mary K.
Shariat, Shahrokh F.
Steinberg, Gary D.
Frierson, Henry F.
Wu, Xue-Ru
Theodorescu, Dan
Matusik, Robert J.
author_sort DeGraff, David J.
collection PubMed
description Approximately 50% of patients with muscle-invasive bladder cancer (MIBC) develop metastatic disease, which is almost invariably lethal. However, our understanding of pathways that drive aggressive behavior of MIBC is incomplete. Members of the FOXA subfamily of transcription factors are implicated in normal urogenital development and urologic malignancies. FOXA proteins are implicated in normal urothelial differentiation, but their role in bladder cancer is unknown. We examined FOXA expression in commonly used in vitro models of bladder cancer and in human bladder cancer specimens, and used a novel in vivo tissue recombination system to determine the functional significance of FOXA1 expression in bladder cancer. Logistic regression analysis showed decreased FOXA1 expression is associated with increasing tumor stage (p<0.001), and loss of FOXA1 is associated with high histologic grade (p<0.001). Also, we found that bladder urothelium that has undergone keratinizing squamous metaplasia, a precursor to the development of squamous cell carcinoma (SCC) exhibited loss of FOXA1 expression. Furthermore, 81% of cases of SCC of the bladder were negative for FOXA1 staining compared to only 40% of urothelial cell carcinomas. In addition, we showed that a subpopulation of FOXA1 negative urothelial tumor cells are highly proliferative. Knockdown of FOXA1 in RT4 bladder cancer cells resulted in increased expression of UPK1B, UPK2, UPK3A, and UPK3B, decreased E-cadherin expression and significantly increased cell proliferation, while overexpression of FOXA1 in T24 cells increased E-cadherin expression and significantly decreased cell growth and invasion. In vivo recombination of bladder cancer cells engineered to exhibit reduced FOXA1 expression with embryonic rat bladder mesenchyme and subsequent renal capsule engraftment resulted in enhanced tumor proliferation. These findings provide the first evidence linking loss of FOXA1 expression with histological subtypes of MIBC and urothelial cell proliferation, and suggest an important role for FOXA1 in the malignant phenotype of MIBC.
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spelling pubmed-33496792012-05-15 Loss of the Urothelial Differentiation Marker FOXA1 Is Associated with High Grade, Late Stage Bladder Cancer and Increased Tumor Proliferation DeGraff, David J. Clark, Peter E. Cates, Justin M. Yamashita, Hironobu Robinson, Victoria L. Yu, Xiuping Smolkin, Mark E. Chang, Sam S. Cookson, Michael S. Herrick, Mary K. Shariat, Shahrokh F. Steinberg, Gary D. Frierson, Henry F. Wu, Xue-Ru Theodorescu, Dan Matusik, Robert J. PLoS One Research Article Approximately 50% of patients with muscle-invasive bladder cancer (MIBC) develop metastatic disease, which is almost invariably lethal. However, our understanding of pathways that drive aggressive behavior of MIBC is incomplete. Members of the FOXA subfamily of transcription factors are implicated in normal urogenital development and urologic malignancies. FOXA proteins are implicated in normal urothelial differentiation, but their role in bladder cancer is unknown. We examined FOXA expression in commonly used in vitro models of bladder cancer and in human bladder cancer specimens, and used a novel in vivo tissue recombination system to determine the functional significance of FOXA1 expression in bladder cancer. Logistic regression analysis showed decreased FOXA1 expression is associated with increasing tumor stage (p<0.001), and loss of FOXA1 is associated with high histologic grade (p<0.001). Also, we found that bladder urothelium that has undergone keratinizing squamous metaplasia, a precursor to the development of squamous cell carcinoma (SCC) exhibited loss of FOXA1 expression. Furthermore, 81% of cases of SCC of the bladder were negative for FOXA1 staining compared to only 40% of urothelial cell carcinomas. In addition, we showed that a subpopulation of FOXA1 negative urothelial tumor cells are highly proliferative. Knockdown of FOXA1 in RT4 bladder cancer cells resulted in increased expression of UPK1B, UPK2, UPK3A, and UPK3B, decreased E-cadherin expression and significantly increased cell proliferation, while overexpression of FOXA1 in T24 cells increased E-cadherin expression and significantly decreased cell growth and invasion. In vivo recombination of bladder cancer cells engineered to exhibit reduced FOXA1 expression with embryonic rat bladder mesenchyme and subsequent renal capsule engraftment resulted in enhanced tumor proliferation. These findings provide the first evidence linking loss of FOXA1 expression with histological subtypes of MIBC and urothelial cell proliferation, and suggest an important role for FOXA1 in the malignant phenotype of MIBC. Public Library of Science 2012-05-10 /pmc/articles/PMC3349679/ /pubmed/22590586 http://dx.doi.org/10.1371/journal.pone.0036669 Text en DeGraff 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
DeGraff, David J.
Clark, Peter E.
Cates, Justin M.
Yamashita, Hironobu
Robinson, Victoria L.
Yu, Xiuping
Smolkin, Mark E.
Chang, Sam S.
Cookson, Michael S.
Herrick, Mary K.
Shariat, Shahrokh F.
Steinberg, Gary D.
Frierson, Henry F.
Wu, Xue-Ru
Theodorescu, Dan
Matusik, Robert J.
Loss of the Urothelial Differentiation Marker FOXA1 Is Associated with High Grade, Late Stage Bladder Cancer and Increased Tumor Proliferation
title Loss of the Urothelial Differentiation Marker FOXA1 Is Associated with High Grade, Late Stage Bladder Cancer and Increased Tumor Proliferation
title_full Loss of the Urothelial Differentiation Marker FOXA1 Is Associated with High Grade, Late Stage Bladder Cancer and Increased Tumor Proliferation
title_fullStr Loss of the Urothelial Differentiation Marker FOXA1 Is Associated with High Grade, Late Stage Bladder Cancer and Increased Tumor Proliferation
title_full_unstemmed Loss of the Urothelial Differentiation Marker FOXA1 Is Associated with High Grade, Late Stage Bladder Cancer and Increased Tumor Proliferation
title_short Loss of the Urothelial Differentiation Marker FOXA1 Is Associated with High Grade, Late Stage Bladder Cancer and Increased Tumor Proliferation
title_sort loss of the urothelial differentiation marker foxa1 is associated with high grade, late stage bladder cancer and increased tumor proliferation
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3349679/
https://www.ncbi.nlm.nih.gov/pubmed/22590586
http://dx.doi.org/10.1371/journal.pone.0036669
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