Tumor‐suppressive microRNA‐223 inhibits cancer cell migration and invasion by targeting ITGA3/ITGB1 signaling in prostate cancer

Analysis of microRNA (miRNA) expression signatures in prostate cancer (PCa) and castration‐resistant PCa has revealed that miRNA‐223 is significantly downregulated in cancer tissues, suggesting that miR‐223 acts as a tumor‐suppressive miRNA by targeting oncogenes. The aim of this study was to invest...

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Autores principales: Kurozumi, Akira, Goto, Yusuke, Matsushita, Ryosuke, Fukumoto, Ichiro, Kato, Mayuko, Nishikawa, Rika, Sakamoto, Shinichi, Enokida, Hideki, Nakagawa, Masayuki, Ichikawa, Tomohiko, Seki, Naohiko
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2015
Materias:
Original Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4724812/
https://www.ncbi.nlm.nih.gov/pubmed/26509963
http://dx.doi.org/10.1111/cas.12842
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author Kurozumi, Akira
Goto, Yusuke
Matsushita, Ryosuke
Fukumoto, Ichiro
Kato, Mayuko
Nishikawa, Rika
Sakamoto, Shinichi
Enokida, Hideki
Nakagawa, Masayuki
Ichikawa, Tomohiko
Seki, Naohiko
author_facet Kurozumi, Akira
Goto, Yusuke
Matsushita, Ryosuke
Fukumoto, Ichiro
Kato, Mayuko
Nishikawa, Rika
Sakamoto, Shinichi
Enokida, Hideki
Nakagawa, Masayuki
Ichikawa, Tomohiko
Seki, Naohiko
author_sort Kurozumi, Akira
collection PubMed
description Analysis of microRNA (miRNA) expression signatures in prostate cancer (PCa) and castration‐resistant PCa has revealed that miRNA‐223 is significantly downregulated in cancer tissues, suggesting that miR‐223 acts as a tumor‐suppressive miRNA by targeting oncogenes. The aim of this study was to investigate the functional roles of miR‐223 and identify downstream oncogenic targets regulated by miR‐223 in PCa cells. Functional studies of miR‐223 were carried out to investigate cell proliferation, migration, and invasion using PC3 and PC3M PCa cell lines. Restoration of miR‐223 significantly inhibited cancer cell migration and invasion in PCa cells. In silico database and genome‐wide gene expression analyses revealed that ITGA3 and ITGB1 were direct targets of miR‐223 regulation. Knockdown of ITGA3 and ITGB1 significantly inhibited cancer cell migration and invasion in PCa cells by regulating downstream signaling. Moreover, overexpression of ITGA3 and ITGB1 was observed in PCa clinical specimens. Thus, our data indicated that downregulation of miR‐223 enhanced ITGA3/ITGB1 signaling and contributed to cancer cell migration and invasion in PCa cells. Elucidation of the molecular pathways modulated by tumor‐suppressive miRNAs provides insights into the mechanisms of PCa progression and metastasis.
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spelling pubmed-47248122016-02-03 Tumor‐suppressive microRNA‐223 inhibits cancer cell migration and invasion by targeting ITGA3/ITGB1 signaling in prostate cancer Kurozumi, Akira Goto, Yusuke Matsushita, Ryosuke Fukumoto, Ichiro Kato, Mayuko Nishikawa, Rika Sakamoto, Shinichi Enokida, Hideki Nakagawa, Masayuki Ichikawa, Tomohiko Seki, Naohiko Cancer Sci Original Articles Analysis of microRNA (miRNA) expression signatures in prostate cancer (PCa) and castration‐resistant PCa has revealed that miRNA‐223 is significantly downregulated in cancer tissues, suggesting that miR‐223 acts as a tumor‐suppressive miRNA by targeting oncogenes. The aim of this study was to investigate the functional roles of miR‐223 and identify downstream oncogenic targets regulated by miR‐223 in PCa cells. Functional studies of miR‐223 were carried out to investigate cell proliferation, migration, and invasion using PC3 and PC3M PCa cell lines. Restoration of miR‐223 significantly inhibited cancer cell migration and invasion in PCa cells. In silico database and genome‐wide gene expression analyses revealed that ITGA3 and ITGB1 were direct targets of miR‐223 regulation. Knockdown of ITGA3 and ITGB1 significantly inhibited cancer cell migration and invasion in PCa cells by regulating downstream signaling. Moreover, overexpression of ITGA3 and ITGB1 was observed in PCa clinical specimens. Thus, our data indicated that downregulation of miR‐223 enhanced ITGA3/ITGB1 signaling and contributed to cancer cell migration and invasion in PCa cells. Elucidation of the molecular pathways modulated by tumor‐suppressive miRNAs provides insights into the mechanisms of PCa progression and metastasis. John Wiley and Sons Inc. 2015-12-05 2016-01 /pmc/articles/PMC4724812/ /pubmed/26509963 http://dx.doi.org/10.1111/cas.12842 Text en © 2015 The Authors. Cancer Science published by Wiley Publishing Asia Pty Ltd on behalf of Japanese Cancer Association. This is an open access article under the terms of the Creative Commons Attribution‐NonCommercial‐NoDerivs (http://creativecommons.org/licenses/by-nc-nd/4.0/) License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non‐commercial and no modifications or adaptations are made.
spellingShingle Original Articles
Kurozumi, Akira
Goto, Yusuke
Matsushita, Ryosuke
Fukumoto, Ichiro
Kato, Mayuko
Nishikawa, Rika
Sakamoto, Shinichi
Enokida, Hideki
Nakagawa, Masayuki
Ichikawa, Tomohiko
Seki, Naohiko
Tumor‐suppressive microRNA‐223 inhibits cancer cell migration and invasion by targeting ITGA3/ITGB1 signaling in prostate cancer
title Tumor‐suppressive microRNA‐223 inhibits cancer cell migration and invasion by targeting ITGA3/ITGB1 signaling in prostate cancer
title_full Tumor‐suppressive microRNA‐223 inhibits cancer cell migration and invasion by targeting ITGA3/ITGB1 signaling in prostate cancer
title_fullStr Tumor‐suppressive microRNA‐223 inhibits cancer cell migration and invasion by targeting ITGA3/ITGB1 signaling in prostate cancer
title_full_unstemmed Tumor‐suppressive microRNA‐223 inhibits cancer cell migration and invasion by targeting ITGA3/ITGB1 signaling in prostate cancer
title_short Tumor‐suppressive microRNA‐223 inhibits cancer cell migration and invasion by targeting ITGA3/ITGB1 signaling in prostate cancer
title_sort tumor‐suppressive microrna‐223 inhibits cancer cell migration and invasion by targeting itga3/itgb1 signaling in prostate cancer
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4724812/
https://www.ncbi.nlm.nih.gov/pubmed/26509963
http://dx.doi.org/10.1111/cas.12842
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