MicroRNA‐200a suppresses prostate cancer progression through BRD4/AR signaling pathway
Abstract Prostate cancer is still considered a significant health care challenge worldwide due in part to the distinct transformation of androgen‐dependent prostate cancer (ADPC) into treatment‐refractory castration‐resistant prostate cancer (CRPC). Consequently, there is an urgent need to explore n...
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doaj-b128256efce743b0b5361f8b4eaa7fe62020-11-25T01:33:18ZengWileyCancer Medicine2045-76342019-04-01841474148510.1002/cam4.2029MicroRNA‐200a suppresses prostate cancer progression through BRD4/AR signaling pathwayHan Guan0Zonghao You1Can Wang2Fang Fang3Rui Peng4Likai Mao5Bin Xu6Ming Chen7Department of Urology The First Affiliated Hospital of Bengbu Medical College Bengbu ChinaDepartment of Urology Affliated Zhongda Hospital of Southeast University Nanjing ChinaDepartment of Urology Affliated Zhongda Hospital of Southeast University Nanjing ChinaDepartment of Immunology Bengbu Medical College Bengbu ChinaDepartment of Graduate School Bengbu Medical College Bengbu ChinaDepartment of Urology The Second Affiliated Hospital of Bengbu Medical College Bengbu ChinaDepartment of Urology Affliated Zhongda Hospital of Southeast University Nanjing ChinaDepartment of Urology Affliated Zhongda Hospital of Southeast University Nanjing ChinaAbstract Prostate cancer is still considered a significant health care challenge worldwide due in part to the distinct transformation of androgen‐dependent prostate cancer (ADPC) into treatment‐refractory castration‐resistant prostate cancer (CRPC). Consequently, there is an urgent need to explore novel molecular mechanisms underlying treatment resistance in ADPC. Although numerous studies have alluded to the role of miR‐200a in several cancers, the biological significance of miR‐200a in prostate cancer remains unknown. After performing microarray analysis and reanalysis of the publicly available Memorial Sloan Kettering Cancer Center dataset, miR‐200a expression was found higher in ADPC tissues and its expression was positively associated with survival of CRPC patients. In vitro studies showed that miR‐200a overexpression in CRPC cells markedly suppressed cellular proliferation and facilitated apoptosis. In vivo studies indicated that overexpression of miR‐200a inhibited growth and metastasis of prostate cancer. The luciferase reporter assay demonstrated that BRD4 is a direct target gene of miR‐200a and it could reverse miR‐200a‐mediated biological effects in prostate cancer cells. Most importantly, our findings indicated that miR‐200a suppresses the progression of CRPC by inhibiting the activation of BRD4‐mediated AR signaling. This finding provides the foundation for the development of more personalized therapeutic approaches for CRPC patients.https://doi.org/10.1002/cam4.2029androgen receptorBRD4miRNAprostate cancersignaling pathway |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Han Guan Zonghao You Can Wang Fang Fang Rui Peng Likai Mao Bin Xu Ming Chen |
spellingShingle |
Han Guan Zonghao You Can Wang Fang Fang Rui Peng Likai Mao Bin Xu Ming Chen MicroRNA‐200a suppresses prostate cancer progression through BRD4/AR signaling pathway Cancer Medicine androgen receptor BRD4 miRNA prostate cancer signaling pathway |
author_facet |
Han Guan Zonghao You Can Wang Fang Fang Rui Peng Likai Mao Bin Xu Ming Chen |
author_sort |
Han Guan |
title |
MicroRNA‐200a suppresses prostate cancer progression through BRD4/AR signaling pathway |
title_short |
MicroRNA‐200a suppresses prostate cancer progression through BRD4/AR signaling pathway |
title_full |
MicroRNA‐200a suppresses prostate cancer progression through BRD4/AR signaling pathway |
title_fullStr |
MicroRNA‐200a suppresses prostate cancer progression through BRD4/AR signaling pathway |
title_full_unstemmed |
MicroRNA‐200a suppresses prostate cancer progression through BRD4/AR signaling pathway |
title_sort |
microrna‐200a suppresses prostate cancer progression through brd4/ar signaling pathway |
publisher |
Wiley |
series |
Cancer Medicine |
issn |
2045-7634 |
publishDate |
2019-04-01 |
description |
Abstract Prostate cancer is still considered a significant health care challenge worldwide due in part to the distinct transformation of androgen‐dependent prostate cancer (ADPC) into treatment‐refractory castration‐resistant prostate cancer (CRPC). Consequently, there is an urgent need to explore novel molecular mechanisms underlying treatment resistance in ADPC. Although numerous studies have alluded to the role of miR‐200a in several cancers, the biological significance of miR‐200a in prostate cancer remains unknown. After performing microarray analysis and reanalysis of the publicly available Memorial Sloan Kettering Cancer Center dataset, miR‐200a expression was found higher in ADPC tissues and its expression was positively associated with survival of CRPC patients. In vitro studies showed that miR‐200a overexpression in CRPC cells markedly suppressed cellular proliferation and facilitated apoptosis. In vivo studies indicated that overexpression of miR‐200a inhibited growth and metastasis of prostate cancer. The luciferase reporter assay demonstrated that BRD4 is a direct target gene of miR‐200a and it could reverse miR‐200a‐mediated biological effects in prostate cancer cells. Most importantly, our findings indicated that miR‐200a suppresses the progression of CRPC by inhibiting the activation of BRD4‐mediated AR signaling. This finding provides the foundation for the development of more personalized therapeutic approaches for CRPC patients. |
topic |
androgen receptor BRD4 miRNA prostate cancer signaling pathway |
url |
https://doi.org/10.1002/cam4.2029 |
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