Down-Regulation of eIF4GII by miR-520c-3p Represses Diffuse Large B Cell Lymphoma Development

Deregulation of the translational machinery is emerging as a critical contributor to cancer development. The contribution of microRNAs in translational gene control has been established however; the role of microRNAs in disrupting the cap-dependent translation regulation complex has not been previou...

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Autores principales: Mazan-Mamczarz, Krystyna, Zhao, X. Frank, Dai, Bojie, Steinhardt, James J., Peroutka, Raymond J., Berk, Kimberly L., Landon, Ari L., Sadowska, Mariola, Zhang, Yongqing, Lehrmann, Elin, Becker, Kevin G., Shaknovich, Rita, Liu, Zhenqiu, Gartenhaus, Ronald B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3907297/
https://www.ncbi.nlm.nih.gov/pubmed/24497838
http://dx.doi.org/10.1371/journal.pgen.1004105
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author Mazan-Mamczarz, Krystyna
Zhao, X. Frank
Dai, Bojie
Steinhardt, James J.
Peroutka, Raymond J.
Berk, Kimberly L.
Landon, Ari L.
Sadowska, Mariola
Zhang, Yongqing
Lehrmann, Elin
Becker, Kevin G.
Shaknovich, Rita
Liu, Zhenqiu
Gartenhaus, Ronald B.
author_facet Mazan-Mamczarz, Krystyna
Zhao, X. Frank
Dai, Bojie
Steinhardt, James J.
Peroutka, Raymond J.
Berk, Kimberly L.
Landon, Ari L.
Sadowska, Mariola
Zhang, Yongqing
Lehrmann, Elin
Becker, Kevin G.
Shaknovich, Rita
Liu, Zhenqiu
Gartenhaus, Ronald B.
author_sort Mazan-Mamczarz, Krystyna
collection PubMed
description Deregulation of the translational machinery is emerging as a critical contributor to cancer development. The contribution of microRNAs in translational gene control has been established however; the role of microRNAs in disrupting the cap-dependent translation regulation complex has not been previously described. Here, we established that elevated miR-520c-3p represses global translation, cell proliferation and initiates premature senescence in HeLa and DLBCL cells. Moreover, we demonstrate that miR-520c-3p directly targets translation initiation factor, eIF4GII mRNA and negatively regulates eIF4GII protein synthesis. miR-520c-3p overexpression diminishes cells colony formation and reduces tumor growth in a human xenograft mouse model. Consequently, downregulation of eIF4GII by siRNA decreases translation, cell proliferation and ability to form colonies, as well as induces cellular senescence. In vitro and in vivo findings were further validated in patient samples; DLBCL primary cells demonstrated low miR-520c-3p levels with reciprocally up-regulated eIF4GII protein expression. Our results provide evidence that the tumor suppressor effect of miR-520c-3p is mediated through repression of translation while inducing senescence and that eIF4GII is a key effector of this anti-tumor activity.
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spelling pubmed-39072972014-02-04 Down-Regulation of eIF4GII by miR-520c-3p Represses Diffuse Large B Cell Lymphoma Development Mazan-Mamczarz, Krystyna Zhao, X. Frank Dai, Bojie Steinhardt, James J. Peroutka, Raymond J. Berk, Kimberly L. Landon, Ari L. Sadowska, Mariola Zhang, Yongqing Lehrmann, Elin Becker, Kevin G. Shaknovich, Rita Liu, Zhenqiu Gartenhaus, Ronald B. PLoS Genet Research Article Deregulation of the translational machinery is emerging as a critical contributor to cancer development. The contribution of microRNAs in translational gene control has been established however; the role of microRNAs in disrupting the cap-dependent translation regulation complex has not been previously described. Here, we established that elevated miR-520c-3p represses global translation, cell proliferation and initiates premature senescence in HeLa and DLBCL cells. Moreover, we demonstrate that miR-520c-3p directly targets translation initiation factor, eIF4GII mRNA and negatively regulates eIF4GII protein synthesis. miR-520c-3p overexpression diminishes cells colony formation and reduces tumor growth in a human xenograft mouse model. Consequently, downregulation of eIF4GII by siRNA decreases translation, cell proliferation and ability to form colonies, as well as induces cellular senescence. In vitro and in vivo findings were further validated in patient samples; DLBCL primary cells demonstrated low miR-520c-3p levels with reciprocally up-regulated eIF4GII protein expression. Our results provide evidence that the tumor suppressor effect of miR-520c-3p is mediated through repression of translation while inducing senescence and that eIF4GII is a key effector of this anti-tumor activity. Public Library of Science 2014-01-30 /pmc/articles/PMC3907297/ /pubmed/24497838 http://dx.doi.org/10.1371/journal.pgen.1004105 Text en https://creativecommons.org/publicdomain/zero/1.0/ This is an open-access article distributed under the terms of the Creative Commons Public Domain declaration, which stipulates that, once placed in the public domain, this work may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose.
spellingShingle Research Article
Mazan-Mamczarz, Krystyna
Zhao, X. Frank
Dai, Bojie
Steinhardt, James J.
Peroutka, Raymond J.
Berk, Kimberly L.
Landon, Ari L.
Sadowska, Mariola
Zhang, Yongqing
Lehrmann, Elin
Becker, Kevin G.
Shaknovich, Rita
Liu, Zhenqiu
Gartenhaus, Ronald B.
Down-Regulation of eIF4GII by miR-520c-3p Represses Diffuse Large B Cell Lymphoma Development
title Down-Regulation of eIF4GII by miR-520c-3p Represses Diffuse Large B Cell Lymphoma Development
title_full Down-Regulation of eIF4GII by miR-520c-3p Represses Diffuse Large B Cell Lymphoma Development
title_fullStr Down-Regulation of eIF4GII by miR-520c-3p Represses Diffuse Large B Cell Lymphoma Development
title_full_unstemmed Down-Regulation of eIF4GII by miR-520c-3p Represses Diffuse Large B Cell Lymphoma Development
title_short Down-Regulation of eIF4GII by miR-520c-3p Represses Diffuse Large B Cell Lymphoma Development
title_sort down-regulation of eif4gii by mir-520c-3p represses diffuse large b cell lymphoma development
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3907297/
https://www.ncbi.nlm.nih.gov/pubmed/24497838
http://dx.doi.org/10.1371/journal.pgen.1004105
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