Model Affitin and PEG modifications onto siRNA lipid nanocapsules: cell uptake and in vivo biodistribution improvements

Malignant melanoma is an aggressive tumor, associated with the presence of local and/or distant metastases. The development of gene therapy by the use of small interfering RNA (siRNA) represents a promising new treatment. However, the protection of this biomolecule is necessary in order for it to be...

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Autores principales: Resnier, Pauline, Lepeltier, Elise, Emina, Anthea Lucrezia, Galopin, Natacha, Bejaud, Jérôme, David, Stephanie, Ballet, Caroline, Benvegnu, Thierry, Pecorari, Frédéric, Chourpa, Igor, Benoit, Jean-Pierre, Passirani, Catherine
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Royal Society of Chemistry 2019
Materias:
Chemistry
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9070605/
https://www.ncbi.nlm.nih.gov/pubmed/35529231
http://dx.doi.org/10.1039/c9ra03668g
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author Resnier, Pauline
Lepeltier, Elise
Emina, Anthea Lucrezia
Galopin, Natacha
Bejaud, Jérôme
David, Stephanie
Ballet, Caroline
Benvegnu, Thierry
Pecorari, Frédéric
Chourpa, Igor
Benoit, Jean-Pierre
Passirani, Catherine
author_facet Resnier, Pauline
Lepeltier, Elise
Emina, Anthea Lucrezia
Galopin, Natacha
Bejaud, Jérôme
David, Stephanie
Ballet, Caroline
Benvegnu, Thierry
Pecorari, Frédéric
Chourpa, Igor
Benoit, Jean-Pierre
Passirani, Catherine
author_sort Resnier, Pauline
collection PubMed
description Malignant melanoma is an aggressive tumor, associated with the presence of local and/or distant metastases. The development of gene therapy by the use of small interfering RNA (siRNA) represents a promising new treatment. However, the protection of this biomolecule is necessary in order for it to be intravenously administrated, for example via its incorporation into nanomedicines. In parallel to the passive targeting usually obtained by pegylation, various studies have aimed at developing “smart” nanomedicines to efficiently deliver the drug to tumor sites. In this work, siRNA loaded lipid nanocapsules (LNCs) were modified with DSPE-polyethylene glycol (DSPE-PEG), tetraether-PEG (TE-PEG) and/or with an Affitin model, to assay multiple targeting strategies. The uptake of fluorescently labelled LNCs, nanocarrier integrity and siRNA release into human SK-Mel28 melanoma cells were studied by flow cytometry, conventional confocal microscopy and by confocal spectral imaging in a Förster Resonance Energy Transfer (FRET) mode. Surface modified siRNA LNCs were followed after human plasma incubation and after intravenous injection, in order to compare the stealth properties. Finally, the biodistribution of the different siRNA LNCs in healthy and melanoma tumor bearing mice models was assessed by in vivo biofluorescence imaging (BFI), to evaluate the potential tumor targeting ability. The post-insertion of DSPE-PEG induced a strong decrease of the internalization into melanoma cells compared to TE-PEG modification. Both PEG polymer decorations induced a great plasma protection of siRNA but only DSPE-PEG led to stealth properties, even at low concentration (5 mM). The Affitin grafting by thiolation of DSPE-PEG was validated on siRNA LNCs. DSPE-PEG-Affitin LNCs were not detected in this melanoma tumor model but did not show unspecific accumulation in organs. DSPE-PEG and TE-PEG LNCs induced a significant intratumoral accumulation of modified LNCs.
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spelling pubmed-90706052022-05-05 Model Affitin and PEG modifications onto siRNA lipid nanocapsules: cell uptake and in vivo biodistribution improvements Resnier, Pauline Lepeltier, Elise Emina, Anthea Lucrezia Galopin, Natacha Bejaud, Jérôme David, Stephanie Ballet, Caroline Benvegnu, Thierry Pecorari, Frédéric Chourpa, Igor Benoit, Jean-Pierre Passirani, Catherine RSC Adv Chemistry Malignant melanoma is an aggressive tumor, associated with the presence of local and/or distant metastases. The development of gene therapy by the use of small interfering RNA (siRNA) represents a promising new treatment. However, the protection of this biomolecule is necessary in order for it to be intravenously administrated, for example via its incorporation into nanomedicines. In parallel to the passive targeting usually obtained by pegylation, various studies have aimed at developing “smart” nanomedicines to efficiently deliver the drug to tumor sites. In this work, siRNA loaded lipid nanocapsules (LNCs) were modified with DSPE-polyethylene glycol (DSPE-PEG), tetraether-PEG (TE-PEG) and/or with an Affitin model, to assay multiple targeting strategies. The uptake of fluorescently labelled LNCs, nanocarrier integrity and siRNA release into human SK-Mel28 melanoma cells were studied by flow cytometry, conventional confocal microscopy and by confocal spectral imaging in a Förster Resonance Energy Transfer (FRET) mode. Surface modified siRNA LNCs were followed after human plasma incubation and after intravenous injection, in order to compare the stealth properties. Finally, the biodistribution of the different siRNA LNCs in healthy and melanoma tumor bearing mice models was assessed by in vivo biofluorescence imaging (BFI), to evaluate the potential tumor targeting ability. The post-insertion of DSPE-PEG induced a strong decrease of the internalization into melanoma cells compared to TE-PEG modification. Both PEG polymer decorations induced a great plasma protection of siRNA but only DSPE-PEG led to stealth properties, even at low concentration (5 mM). The Affitin grafting by thiolation of DSPE-PEG was validated on siRNA LNCs. DSPE-PEG-Affitin LNCs were not detected in this melanoma tumor model but did not show unspecific accumulation in organs. DSPE-PEG and TE-PEG LNCs induced a significant intratumoral accumulation of modified LNCs. The Royal Society of Chemistry 2019-08-30 /pmc/articles/PMC9070605/ /pubmed/35529231 http://dx.doi.org/10.1039/c9ra03668g Text en This journal is © The Royal Society of Chemistry https://creativecommons.org/licenses/by-nc/3.0/
spellingShingle Chemistry
Resnier, Pauline
Lepeltier, Elise
Emina, Anthea Lucrezia
Galopin, Natacha
Bejaud, Jérôme
David, Stephanie
Ballet, Caroline
Benvegnu, Thierry
Pecorari, Frédéric
Chourpa, Igor
Benoit, Jean-Pierre
Passirani, Catherine
Model Affitin and PEG modifications onto siRNA lipid nanocapsules: cell uptake and in vivo biodistribution improvements
title Model Affitin and PEG modifications onto siRNA lipid nanocapsules: cell uptake and in vivo biodistribution improvements
title_full Model Affitin and PEG modifications onto siRNA lipid nanocapsules: cell uptake and in vivo biodistribution improvements
title_fullStr Model Affitin and PEG modifications onto siRNA lipid nanocapsules: cell uptake and in vivo biodistribution improvements
title_full_unstemmed Model Affitin and PEG modifications onto siRNA lipid nanocapsules: cell uptake and in vivo biodistribution improvements
title_short Model Affitin and PEG modifications onto siRNA lipid nanocapsules: cell uptake and in vivo biodistribution improvements
title_sort model affitin and peg modifications onto sirna lipid nanocapsules: cell uptake and in vivo biodistribution improvements
topic Chemistry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9070605/
https://www.ncbi.nlm.nih.gov/pubmed/35529231
http://dx.doi.org/10.1039/c9ra03668g
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