Enhancement of Farnesoid X Receptor Inhibits Migration, Adhesion and Angiogenesis through Proteasome Degradation and VEGF Reduction in Bladder Cancers

(1) Background: Bladder cancer is a malignant tumor mainly caused by exposure to environmental chemicals, with a high recurrence rate. NR1H4, also known as Farnesoid X Receptor (FXR), acts as a nuclear receptor that can be activated by binding with bile acids, and FXR is highly correlated with the p...

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Autores principales: Lai, Chien-Rui, Wang, Hisao-Hsien, Chang, Hsin-Han, Tsai, Yu-Ling, Tsai, Wen-Chiuan, Lee, Chen-Ray, Changchien, Chih-Ying, Cheng, Yu-Chen, Wu, Sheng-Tang, Chen, Ying
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9103877/
https://www.ncbi.nlm.nih.gov/pubmed/35563650
http://dx.doi.org/10.3390/ijms23095259
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author Lai, Chien-Rui
Wang, Hisao-Hsien
Chang, Hsin-Han
Tsai, Yu-Ling
Tsai, Wen-Chiuan
Lee, Chen-Ray
Changchien, Chih-Ying
Cheng, Yu-Chen
Wu, Sheng-Tang
Chen, Ying
author_facet Lai, Chien-Rui
Wang, Hisao-Hsien
Chang, Hsin-Han
Tsai, Yu-Ling
Tsai, Wen-Chiuan
Lee, Chen-Ray
Changchien, Chih-Ying
Cheng, Yu-Chen
Wu, Sheng-Tang
Chen, Ying
author_sort Lai, Chien-Rui
collection PubMed
description (1) Background: Bladder cancer is a malignant tumor mainly caused by exposure to environmental chemicals, with a high recurrence rate. NR1H4, also known as Farnesoid X Receptor (FXR), acts as a nuclear receptor that can be activated by binding with bile acids, and FXR is highly correlated with the progression of cancers. The aim of this study was to verify the role of FXR in bladder cancer cells. (2) Methods: A FXR overexpressed system was established to investigate the effect of cell viability, migration, adhesion, and angiogenesis in low-grade TSGH8301 and high-grade T24 cells. (3) Results: After FXR overexpression, the ability of migration, adhesion, invasion and angiogenesis of bladder cancer cells declined significantly. Focal adhesive complex, MMP2, MMP9, and angiogenic-related proteins were decreased, while FXR was overexpressed in bladder cancer cells. Moreover, FXR overexpression reduced vascular endothelial growth factor mRNA and protein expression and secretion in bladder cancer cells. After treatment with the proteosome inhibitor MG132, the migration, adhesion and angiogenesis caused by FXR overexpression were all reversed in bladder cancer cells. (4) Conclusions: These results may provide evidence on the role of FXR in bladder cancer, and thus may improve the therapeutic efficacy of urothelial carcinoma in the future.
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spelling pubmed-91038772022-05-14 Enhancement of Farnesoid X Receptor Inhibits Migration, Adhesion and Angiogenesis through Proteasome Degradation and VEGF Reduction in Bladder Cancers Lai, Chien-Rui Wang, Hisao-Hsien Chang, Hsin-Han Tsai, Yu-Ling Tsai, Wen-Chiuan Lee, Chen-Ray Changchien, Chih-Ying Cheng, Yu-Chen Wu, Sheng-Tang Chen, Ying Int J Mol Sci Article (1) Background: Bladder cancer is a malignant tumor mainly caused by exposure to environmental chemicals, with a high recurrence rate. NR1H4, also known as Farnesoid X Receptor (FXR), acts as a nuclear receptor that can be activated by binding with bile acids, and FXR is highly correlated with the progression of cancers. The aim of this study was to verify the role of FXR in bladder cancer cells. (2) Methods: A FXR overexpressed system was established to investigate the effect of cell viability, migration, adhesion, and angiogenesis in low-grade TSGH8301 and high-grade T24 cells. (3) Results: After FXR overexpression, the ability of migration, adhesion, invasion and angiogenesis of bladder cancer cells declined significantly. Focal adhesive complex, MMP2, MMP9, and angiogenic-related proteins were decreased, while FXR was overexpressed in bladder cancer cells. Moreover, FXR overexpression reduced vascular endothelial growth factor mRNA and protein expression and secretion in bladder cancer cells. After treatment with the proteosome inhibitor MG132, the migration, adhesion and angiogenesis caused by FXR overexpression were all reversed in bladder cancer cells. (4) Conclusions: These results may provide evidence on the role of FXR in bladder cancer, and thus may improve the therapeutic efficacy of urothelial carcinoma in the future. MDPI 2022-05-09 /pmc/articles/PMC9103877/ /pubmed/35563650 http://dx.doi.org/10.3390/ijms23095259 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Lai, Chien-Rui
Wang, Hisao-Hsien
Chang, Hsin-Han
Tsai, Yu-Ling
Tsai, Wen-Chiuan
Lee, Chen-Ray
Changchien, Chih-Ying
Cheng, Yu-Chen
Wu, Sheng-Tang
Chen, Ying
Enhancement of Farnesoid X Receptor Inhibits Migration, Adhesion and Angiogenesis through Proteasome Degradation and VEGF Reduction in Bladder Cancers
title Enhancement of Farnesoid X Receptor Inhibits Migration, Adhesion and Angiogenesis through Proteasome Degradation and VEGF Reduction in Bladder Cancers
title_full Enhancement of Farnesoid X Receptor Inhibits Migration, Adhesion and Angiogenesis through Proteasome Degradation and VEGF Reduction in Bladder Cancers
title_fullStr Enhancement of Farnesoid X Receptor Inhibits Migration, Adhesion and Angiogenesis through Proteasome Degradation and VEGF Reduction in Bladder Cancers
title_full_unstemmed Enhancement of Farnesoid X Receptor Inhibits Migration, Adhesion and Angiogenesis through Proteasome Degradation and VEGF Reduction in Bladder Cancers
title_short Enhancement of Farnesoid X Receptor Inhibits Migration, Adhesion and Angiogenesis through Proteasome Degradation and VEGF Reduction in Bladder Cancers
title_sort enhancement of farnesoid x receptor inhibits migration, adhesion and angiogenesis through proteasome degradation and vegf reduction in bladder cancers
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9103877/
https://www.ncbi.nlm.nih.gov/pubmed/35563650
http://dx.doi.org/10.3390/ijms23095259
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