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The application of mRNA-based gene transfer in mesenchymal stem cell-mediated cytotoxicity of glioma cells

Since the tumor-oriented homing capacity of mesenchymal stem cells (MSCs) was discovered, MSCs have attracted great interest in the research field of cancer therapy mainly focused on their use as carries for anticancer agents. Differing from DNA-based vectors, the use of mRNA-based antituor gene del...

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Autores principales: Guo, Xing-Rong, Yang, Zhuo-Shun, Tang, Xiang-Jun, Zou, Dan-Dan, Gui, Hui, Wang, Xiao-Li, Ma, Shi-Nan, Yuan, Ya-Hong, Fang, Juan, Wang, Bin, Zhang, Li, Sun, Xu-Yong, Warnock, Garth L., Dai, Long-Jun, Tu, Han-Jun
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5342434/
https://www.ncbi.nlm.nih.gov/pubmed/27487125
http://dx.doi.org/10.18632/oncotarget.10835
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author Guo, Xing-Rong
Yang, Zhuo-Shun
Tang, Xiang-Jun
Zou, Dan-Dan
Gui, Hui
Wang, Xiao-Li
Ma, Shi-Nan
Yuan, Ya-Hong
Fang, Juan
Wang, Bin
Zhang, Li
Sun, Xu-Yong
Warnock, Garth L.
Dai, Long-Jun
Tu, Han-Jun
author_facet Guo, Xing-Rong
Yang, Zhuo-Shun
Tang, Xiang-Jun
Zou, Dan-Dan
Gui, Hui
Wang, Xiao-Li
Ma, Shi-Nan
Yuan, Ya-Hong
Fang, Juan
Wang, Bin
Zhang, Li
Sun, Xu-Yong
Warnock, Garth L.
Dai, Long-Jun
Tu, Han-Jun
author_sort Guo, Xing-Rong
collection PubMed
description Since the tumor-oriented homing capacity of mesenchymal stem cells (MSCs) was discovered, MSCs have attracted great interest in the research field of cancer therapy mainly focused on their use as carries for anticancer agents. Differing from DNA-based vectors, the use of mRNA-based antituor gene delivery benefits from readily transfection and mutagenesis-free. However, it is essential to verify if mRNA transfection interferes with MSCs' tropism and their antitumor properties. TRAIL- and PTEN-mRNAs were synthesized and studied in an in vitro model of MSC-mediated indirect co-culture with DBTRG human glioma cells. The expression of TRAIL and PTEN in transfected MSCs was verified by immunoblotting analysis, and the migration ability of MSCs after anticancer gene transfection was demonstrated using transwell co-cultures. The viability of DBTRG cells was determined with bioluminescence, live/dead staining and real time cell analyzer. An in vivo model of DBTRG cell-derived xenografted tumors was used to verify the antitumor effects of TRAIL- and PTEN-engineered MSCs. With regard to the effect of mRNA transfection on MSCs' migration toward glioma cells, an enhanced migration rate was observed with MSCs transfected with all tested mRNAs compared to non-transfected MSCs (p<0.05). TRAIL- and PTEN-mRNA-induced cytotoxicity of DBTRG glioma cells was proportionally correlated with the ratio of conditioned medium from transfected MSCs. A synergistic action of TRAIL and PTEN was demonstrated in the current co-culture model. The immunoblotting analysis revealed the apoptotic nature of the cells death in the present study. The growth of the xenografted tumors was significantly inhibited by the application of MSC(PTEN) or MSC(TRAIL/PTEN) on day 14 and MSC(TRAIL) on day 28 (p<0.05). The results suggested that anticancer gene-bearing mRNAs synthesized in vitro are capable of being applied for MSC-mediated anticancer modality. This study provides an experimental base for further clinical anticancer studies using synthesized mRNAs.
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spelling pubmed-53424342017-03-22 The application of mRNA-based gene transfer in mesenchymal stem cell-mediated cytotoxicity of glioma cells Guo, Xing-Rong Yang, Zhuo-Shun Tang, Xiang-Jun Zou, Dan-Dan Gui, Hui Wang, Xiao-Li Ma, Shi-Nan Yuan, Ya-Hong Fang, Juan Wang, Bin Zhang, Li Sun, Xu-Yong Warnock, Garth L. Dai, Long-Jun Tu, Han-Jun Oncotarget Research Paper Since the tumor-oriented homing capacity of mesenchymal stem cells (MSCs) was discovered, MSCs have attracted great interest in the research field of cancer therapy mainly focused on their use as carries for anticancer agents. Differing from DNA-based vectors, the use of mRNA-based antituor gene delivery benefits from readily transfection and mutagenesis-free. However, it is essential to verify if mRNA transfection interferes with MSCs' tropism and their antitumor properties. TRAIL- and PTEN-mRNAs were synthesized and studied in an in vitro model of MSC-mediated indirect co-culture with DBTRG human glioma cells. The expression of TRAIL and PTEN in transfected MSCs was verified by immunoblotting analysis, and the migration ability of MSCs after anticancer gene transfection was demonstrated using transwell co-cultures. The viability of DBTRG cells was determined with bioluminescence, live/dead staining and real time cell analyzer. An in vivo model of DBTRG cell-derived xenografted tumors was used to verify the antitumor effects of TRAIL- and PTEN-engineered MSCs. With regard to the effect of mRNA transfection on MSCs' migration toward glioma cells, an enhanced migration rate was observed with MSCs transfected with all tested mRNAs compared to non-transfected MSCs (p<0.05). TRAIL- and PTEN-mRNA-induced cytotoxicity of DBTRG glioma cells was proportionally correlated with the ratio of conditioned medium from transfected MSCs. A synergistic action of TRAIL and PTEN was demonstrated in the current co-culture model. The immunoblotting analysis revealed the apoptotic nature of the cells death in the present study. The growth of the xenografted tumors was significantly inhibited by the application of MSC(PTEN) or MSC(TRAIL/PTEN) on day 14 and MSC(TRAIL) on day 28 (p<0.05). The results suggested that anticancer gene-bearing mRNAs synthesized in vitro are capable of being applied for MSC-mediated anticancer modality. This study provides an experimental base for further clinical anticancer studies using synthesized mRNAs. Impact Journals LLC 2016-07-25 /pmc/articles/PMC5342434/ /pubmed/27487125 http://dx.doi.org/10.18632/oncotarget.10835 Text en Copyright: © 2016 Guo et al. http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Guo, Xing-Rong
Yang, Zhuo-Shun
Tang, Xiang-Jun
Zou, Dan-Dan
Gui, Hui
Wang, Xiao-Li
Ma, Shi-Nan
Yuan, Ya-Hong
Fang, Juan
Wang, Bin
Zhang, Li
Sun, Xu-Yong
Warnock, Garth L.
Dai, Long-Jun
Tu, Han-Jun
The application of mRNA-based gene transfer in mesenchymal stem cell-mediated cytotoxicity of glioma cells
title The application of mRNA-based gene transfer in mesenchymal stem cell-mediated cytotoxicity of glioma cells
title_full The application of mRNA-based gene transfer in mesenchymal stem cell-mediated cytotoxicity of glioma cells
title_fullStr The application of mRNA-based gene transfer in mesenchymal stem cell-mediated cytotoxicity of glioma cells
title_full_unstemmed The application of mRNA-based gene transfer in mesenchymal stem cell-mediated cytotoxicity of glioma cells
title_short The application of mRNA-based gene transfer in mesenchymal stem cell-mediated cytotoxicity of glioma cells
title_sort application of mrna-based gene transfer in mesenchymal stem cell-mediated cytotoxicity of glioma cells
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5342434/
https://www.ncbi.nlm.nih.gov/pubmed/27487125
http://dx.doi.org/10.18632/oncotarget.10835
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