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Overexpression of Exportin-5 Overrides the Inhibitory Effect of miRNAs Regulation Control and Stabilize Proteins via Posttranslation Modifications in Prostate Cancer()()

Although XPO5 has been characterized to have tumor-suppressor features in the miRNA biogenesis pathway, the impact of altered expression of XPO5 in cancers is unexplored. Here we report a novel “oncogenic” role of XPO5 in advanced prostate cancer. Using prostate cancer models, we found that excess l...

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Autores principales: Höti, Naseruddin, Yang, Shuang, Aiyetan, Paul, Kumar, Binod, Hu, Yingwei, Clark, David, Eroglu, Arife Unal, Shah, Punit, Johnson, Tamara, Chowdery, Wasim H., Zhang, Hui, Rodriguez, Ronald
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Neoplasia Press 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5587889/
https://www.ncbi.nlm.nih.gov/pubmed/28881308
http://dx.doi.org/10.1016/j.neo.2017.07.008
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author Höti, Naseruddin
Yang, Shuang
Aiyetan, Paul
Kumar, Binod
Hu, Yingwei
Clark, David
Eroglu, Arife Unal
Shah, Punit
Johnson, Tamara
Chowdery, Wasim H.
Zhang, Hui
Rodriguez, Ronald
author_facet Höti, Naseruddin
Yang, Shuang
Aiyetan, Paul
Kumar, Binod
Hu, Yingwei
Clark, David
Eroglu, Arife Unal
Shah, Punit
Johnson, Tamara
Chowdery, Wasim H.
Zhang, Hui
Rodriguez, Ronald
author_sort Höti, Naseruddin
collection PubMed
description Although XPO5 has been characterized to have tumor-suppressor features in the miRNA biogenesis pathway, the impact of altered expression of XPO5 in cancers is unexplored. Here we report a novel “oncogenic” role of XPO5 in advanced prostate cancer. Using prostate cancer models, we found that excess levels of XPO5 override the inhibitory effect of the canoncial miRNA-mRNA regulation, resulting in a global increase in proteins expression. Importantly, we found that decreased expression of XPO5 could promote an increase in proteasome degradation, whereas overexpression of XPO5 leads to altered protein posttranslational modification via hyperglycosylation, resulting in cellular protein stability. We evaluated the therapeutic advantage of targeting XPO5 in prostate cancer and found that knocking down XPO5 in prostate cancer cells suppressed cellular proliferation and tumor development without significantly impacting normal fibroblast cells survival. To our knowledge, this is the first report describing the oncogenic role of XPO5 in overriding the miRNAs regulation control. Furthermore, we believe that these findings will provide an explanation as to why, in some cancers that express higher abundance of mature miRNAs, fail to suppress their potential protein targets.
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spelling pubmed-55878892017-09-15 Overexpression of Exportin-5 Overrides the Inhibitory Effect of miRNAs Regulation Control and Stabilize Proteins via Posttranslation Modifications in Prostate Cancer()() Höti, Naseruddin Yang, Shuang Aiyetan, Paul Kumar, Binod Hu, Yingwei Clark, David Eroglu, Arife Unal Shah, Punit Johnson, Tamara Chowdery, Wasim H. Zhang, Hui Rodriguez, Ronald Neoplasia Original article Although XPO5 has been characterized to have tumor-suppressor features in the miRNA biogenesis pathway, the impact of altered expression of XPO5 in cancers is unexplored. Here we report a novel “oncogenic” role of XPO5 in advanced prostate cancer. Using prostate cancer models, we found that excess levels of XPO5 override the inhibitory effect of the canoncial miRNA-mRNA regulation, resulting in a global increase in proteins expression. Importantly, we found that decreased expression of XPO5 could promote an increase in proteasome degradation, whereas overexpression of XPO5 leads to altered protein posttranslational modification via hyperglycosylation, resulting in cellular protein stability. We evaluated the therapeutic advantage of targeting XPO5 in prostate cancer and found that knocking down XPO5 in prostate cancer cells suppressed cellular proliferation and tumor development without significantly impacting normal fibroblast cells survival. To our knowledge, this is the first report describing the oncogenic role of XPO5 in overriding the miRNAs regulation control. Furthermore, we believe that these findings will provide an explanation as to why, in some cancers that express higher abundance of mature miRNAs, fail to suppress their potential protein targets. Neoplasia Press 2017-09-04 /pmc/articles/PMC5587889/ /pubmed/28881308 http://dx.doi.org/10.1016/j.neo.2017.07.008 Text en © 2017 The Authors http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Original article
Höti, Naseruddin
Yang, Shuang
Aiyetan, Paul
Kumar, Binod
Hu, Yingwei
Clark, David
Eroglu, Arife Unal
Shah, Punit
Johnson, Tamara
Chowdery, Wasim H.
Zhang, Hui
Rodriguez, Ronald
Overexpression of Exportin-5 Overrides the Inhibitory Effect of miRNAs Regulation Control and Stabilize Proteins via Posttranslation Modifications in Prostate Cancer()()
title Overexpression of Exportin-5 Overrides the Inhibitory Effect of miRNAs Regulation Control and Stabilize Proteins via Posttranslation Modifications in Prostate Cancer()()
title_full Overexpression of Exportin-5 Overrides the Inhibitory Effect of miRNAs Regulation Control and Stabilize Proteins via Posttranslation Modifications in Prostate Cancer()()
title_fullStr Overexpression of Exportin-5 Overrides the Inhibitory Effect of miRNAs Regulation Control and Stabilize Proteins via Posttranslation Modifications in Prostate Cancer()()
title_full_unstemmed Overexpression of Exportin-5 Overrides the Inhibitory Effect of miRNAs Regulation Control and Stabilize Proteins via Posttranslation Modifications in Prostate Cancer()()
title_short Overexpression of Exportin-5 Overrides the Inhibitory Effect of miRNAs Regulation Control and Stabilize Proteins via Posttranslation Modifications in Prostate Cancer()()
title_sort overexpression of exportin-5 overrides the inhibitory effect of mirnas regulation control and stabilize proteins via posttranslation modifications in prostate cancer()()
topic Original article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5587889/
https://www.ncbi.nlm.nih.gov/pubmed/28881308
http://dx.doi.org/10.1016/j.neo.2017.07.008
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