Performance of Pyridylthiourea‐Polyethylenimine Polyplex for siRNA‐Mediated Liver Cancer Therapy in Cell Monolayer, Spheroid, and Tumor Xenograft Models

Medical application of siRNAs relies on methods for delivering nucleic acids into the cytosol. Synthetic carriers, which assemble with nucleic acids into delivery systems, show promises for cancer therapy but efficiency remains to be improved. In here, the effectiveness of pyridylthiourea‐polyethyle...

Descripción completa

Detalles Bibliográficos
Autores principales: Gossart, Jean Baptiste, Pascal, Etienne, Meyer, Florent, Heuillard, Emilie, Gonçalves, Mathieu, Gossé, Francine, Robinet, Eric, Frisch, Benoît, Seguin, Cendrine, Zuber, Guy
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2017
Materias:
Full Papers
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6607116/
https://www.ncbi.nlm.nih.gov/pubmed/31565271
http://dx.doi.org/10.1002/gch2.201700013
_version_ 1783432029041328128
author Gossart, Jean Baptiste
Pascal, Etienne
Meyer, Florent
Heuillard, Emilie
Gonçalves, Mathieu
Gossé, Francine
Robinet, Eric
Frisch, Benoît
Seguin, Cendrine
Zuber, Guy
author_facet Gossart, Jean Baptiste
Pascal, Etienne
Meyer, Florent
Heuillard, Emilie
Gonçalves, Mathieu
Gossé, Francine
Robinet, Eric
Frisch, Benoît
Seguin, Cendrine
Zuber, Guy
author_sort Gossart, Jean Baptiste
collection PubMed
description Medical application of siRNAs relies on methods for delivering nucleic acids into the cytosol. Synthetic carriers, which assemble with nucleic acids into delivery systems, show promises for cancer therapy but efficiency remains to be improved. In here, the effectiveness of pyridylthiourea‐polyethylenimine (πPEI), a siRNA carrier that favors both polyplex disassembly and endosome rupture upon sensing the acidic endosomal environment, in 3 experimental models of hepatocellular cancer is tested. The πPEI‐assisted delivery of a siRNA targeting the polo‐like kinase 1 into Huh‐7 monolayer produces a 90% cell death via a demonstrated RNA interference mechanism. Incubation of polyplex with Huh‐7 spheroids leads to siRNA delivery into the superficial first cell layer and a 60% reduction in spheroid growth compared to untreated controls. Administration of polyplexes into mice bearing subcutaneous implanted Huh‐7Luc tumors results in a reduced tumor progression, similar to the one observed in the spheroid model. Altogether, these results support the in vivo use of synthetic and dedicated polymers for increasing siRNA‐mediated gene knockdown, and their clinical promise in cancer therapeutics.
format Online
Article
Text
id pubmed-6607116
institution National Center for Biotechnology Information
language English
publishDate 2017
publisher John Wiley and Sons Inc.
record_format MEDLINE/PubMed
spelling pubmed-66071162019-09-27 Performance of Pyridylthiourea‐Polyethylenimine Polyplex for siRNA‐Mediated Liver Cancer Therapy in Cell Monolayer, Spheroid, and Tumor Xenograft Models Gossart, Jean Baptiste Pascal, Etienne Meyer, Florent Heuillard, Emilie Gonçalves, Mathieu Gossé, Francine Robinet, Eric Frisch, Benoît Seguin, Cendrine Zuber, Guy Glob Chall Full Papers Medical application of siRNAs relies on methods for delivering nucleic acids into the cytosol. Synthetic carriers, which assemble with nucleic acids into delivery systems, show promises for cancer therapy but efficiency remains to be improved. In here, the effectiveness of pyridylthiourea‐polyethylenimine (πPEI), a siRNA carrier that favors both polyplex disassembly and endosome rupture upon sensing the acidic endosomal environment, in 3 experimental models of hepatocellular cancer is tested. The πPEI‐assisted delivery of a siRNA targeting the polo‐like kinase 1 into Huh‐7 monolayer produces a 90% cell death via a demonstrated RNA interference mechanism. Incubation of polyplex with Huh‐7 spheroids leads to siRNA delivery into the superficial first cell layer and a 60% reduction in spheroid growth compared to untreated controls. Administration of polyplexes into mice bearing subcutaneous implanted Huh‐7Luc tumors results in a reduced tumor progression, similar to the one observed in the spheroid model. Altogether, these results support the in vivo use of synthetic and dedicated polymers for increasing siRNA‐mediated gene knockdown, and their clinical promise in cancer therapeutics. John Wiley and Sons Inc. 2017-05-19 /pmc/articles/PMC6607116/ /pubmed/31565271 http://dx.doi.org/10.1002/gch2.201700013 Text en © 2017 The Authors. Published by WILEY‐VCH Verlag GmbH & Co. KGaA, Weinheim This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Full Papers
Gossart, Jean Baptiste
Pascal, Etienne
Meyer, Florent
Heuillard, Emilie
Gonçalves, Mathieu
Gossé, Francine
Robinet, Eric
Frisch, Benoît
Seguin, Cendrine
Zuber, Guy
Performance of Pyridylthiourea‐Polyethylenimine Polyplex for siRNA‐Mediated Liver Cancer Therapy in Cell Monolayer, Spheroid, and Tumor Xenograft Models
title Performance of Pyridylthiourea‐Polyethylenimine Polyplex for siRNA‐Mediated Liver Cancer Therapy in Cell Monolayer, Spheroid, and Tumor Xenograft Models
title_full Performance of Pyridylthiourea‐Polyethylenimine Polyplex for siRNA‐Mediated Liver Cancer Therapy in Cell Monolayer, Spheroid, and Tumor Xenograft Models
title_fullStr Performance of Pyridylthiourea‐Polyethylenimine Polyplex for siRNA‐Mediated Liver Cancer Therapy in Cell Monolayer, Spheroid, and Tumor Xenograft Models
title_full_unstemmed Performance of Pyridylthiourea‐Polyethylenimine Polyplex for siRNA‐Mediated Liver Cancer Therapy in Cell Monolayer, Spheroid, and Tumor Xenograft Models
title_short Performance of Pyridylthiourea‐Polyethylenimine Polyplex for siRNA‐Mediated Liver Cancer Therapy in Cell Monolayer, Spheroid, and Tumor Xenograft Models
title_sort performance of pyridylthiourea‐polyethylenimine polyplex for sirna‐mediated liver cancer therapy in cell monolayer, spheroid, and tumor xenograft models
topic Full Papers
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6607116/
https://www.ncbi.nlm.nih.gov/pubmed/31565271
http://dx.doi.org/10.1002/gch2.201700013
work_keys_str_mv AT gossartjeanbaptiste performanceofpyridylthioureapolyethyleniminepolyplexforsirnamediatedlivercancertherapyincellmonolayerspheroidandtumorxenograftmodels
AT pascaletienne performanceofpyridylthioureapolyethyleniminepolyplexforsirnamediatedlivercancertherapyincellmonolayerspheroidandtumorxenograftmodels
AT meyerflorent performanceofpyridylthioureapolyethyleniminepolyplexforsirnamediatedlivercancertherapyincellmonolayerspheroidandtumorxenograftmodels
AT heuillardemilie performanceofpyridylthioureapolyethyleniminepolyplexforsirnamediatedlivercancertherapyincellmonolayerspheroidandtumorxenograftmodels
AT goncalvesmathieu performanceofpyridylthioureapolyethyleniminepolyplexforsirnamediatedlivercancertherapyincellmonolayerspheroidandtumorxenograftmodels
AT gossefrancine performanceofpyridylthioureapolyethyleniminepolyplexforsirnamediatedlivercancertherapyincellmonolayerspheroidandtumorxenograftmodels
AT robineteric performanceofpyridylthioureapolyethyleniminepolyplexforsirnamediatedlivercancertherapyincellmonolayerspheroidandtumorxenograftmodels
AT frischbenoit performanceofpyridylthioureapolyethyleniminepolyplexforsirnamediatedlivercancertherapyincellmonolayerspheroidandtumorxenograftmodels
AT seguincendrine performanceofpyridylthioureapolyethyleniminepolyplexforsirnamediatedlivercancertherapyincellmonolayerspheroidandtumorxenograftmodels
AT zuberguy performanceofpyridylthioureapolyethyleniminepolyplexforsirnamediatedlivercancertherapyincellmonolayerspheroidandtumorxenograftmodels

Ejemplares similares