Delivery of siRNA using cationic rosette nanotubes for gene silencing

Par Conseil national de recherches du Canada

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DOI	Trouver le DOI : https://doi.org/10.1039/D3BM01115A
Auteur	Rechercher : Ho, Uyen¹; Rechercher : El-Bakkari, Mounir¹; Rechercher : Alshamsan, Aws¹; Rechercher : Cho, Jae-Young¹; Rechercher : Yamazaki, Takeshi¹; Rechercher : Hemraz, Usha D.²Identifiant ORCID : https://orcid.org/0000-0001-5151-9484; Rechercher : Fenniri, Hicham³
Affiliation	Conseil national de recherches du Canada. Nanotechnologie Conseil national de recherches du Canada. Thérapeutique en santé humaine Conseil national de recherches du Canada. Technologies de sécurité et de rupture
Bailleur de fonds	Rechercher : National Research Council Canada; Rechercher : Government of Canada; Rechercher : Natural Sciences and Engineering Research Council of Canada; Rechercher : University of Alberta
Format	Texte, Article
Résumé	The quest for new therapeutic treatments for hereditary diseases has led to many advances in RNA interference (RNAi) and gene silencing. While this technique has the potential to address many problems, the key to its continued use is the development of effective delivery strategies that would reduce cellular toxicity and increase silencing efficiency. Rosette nanotubes (RNTs) are biomimetic supramolecular nanostructures formed through the self-assembly of hybrid guanine–cytosine (G∧C) DNA bases. Here, we used bioactive RNTs for siRNA delivery and gene silencing. Fifteen lysine-functionalized twin-G∧C motifs (KnT, n = 1 to 15) were synthesized using solid phase peptide synthesis to produce building blocks that self-assembled to produce cationic RNTs under physiological conditions. The intracellular uptake of siRNA delivered by the oligo-L-lysine RNTs was examined and it was found that the complexation of siRNA was affected by the cationic charges from the lysine residues and the length of RNTs formed, with the higher charged KnT RNTs delivering siRNA to the cells at a faster rate. In addition, by protecting siRNA from serum degradation, KnT RNTs were shown to deliver their cargo to the cells effectively via the endocytic pathway. A reduction in the expression (∼70%) of the target stat3 protein was observed during gene expression analysis in HCT116 and A549 cell lines.
Date de publication	2023-09-21
Maison d’édition	Royal Society of Chemistry
Licence	Creative Commons, Attribution - Pas d’Utilisation Commerciale 3.0 non transposé (CC BY-NC 3.0) https://creativecommons.org/licenses/by-nc/3.0/deed.fr
Dans	Biomaterials Science 11, nº 21 (21 septembre 2023) : 7169–7178.
Langue	anglais
Publications évaluées par des pairs	Oui
Exporter la notice	Exporter en format RIS
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Identificateur de l’enregistrement	5c165d48-d0a4-4114-8301-ab0b3544d82e
Enregistrement créé	2024-04-18
Enregistrement modifié	2024-04-18

Date de modification :: 2024-06-29