Nanoparticles codelivering mRNA and SiRNA for simultaneous restoration and silencing of gene/protein expression in vitro and in vivo

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DOI	Trouver le DOI : https://doi.org/10.1021/acsnanoscienceau.4c00040
Auteur	Rechercher : Manturthi, Shireesha; Rechercher : El-Sahli, Sara; Rechercher : Bo, Yuxia; Rechercher : Durocher, Emma; Rechercher : Kirkby, Melanie; Rechercher : Popatia, Alyanna; Rechercher : Mediratta, Karan; Rechercher : Daniel, Redaet; Rechercher : Lee, Seung-Hwan; Rechercher : Iqbal, Umar¹Identifiant ORCID : https://orcid.org/0009-0007-8326-0455; Rechercher : Côté, Marceline Identifiant ORCID : https://orcid.org/0000-0002-4664-4325; Rechercher : Wang, Lisheng; Rechercher : Gadde, Suresh Identifiant ORCID : https://orcid.org/0000-0001-9102-3029
Affiliation	Conseil national de recherches Canada. Thérapeutique en santé humaine
Bailleur de fonds	Rechercher : National Research Council Canada; Rechercher : Canadian Institutes of Health Research; Rechercher : Natural Sciences and Engineering Research Council of Canada
Format	Texte, Article
Sujet	nanoparticles; siRNA; mRNA; codelivery; gene; protein; restoration and knockdown
Résumé	RNA-based agents (siRNA, miRNA, and mRNA) can selectively manipulate gene expression/proteins and are set to revolutionize a variety of disease treatments. Nanoparticle (NP) platforms have been developed to deliver functional mRNA or siRNA inside cells to overcome their inherent limitations. Recent studies have focused on siRNA to knock down proteins causing drug resistance or mRNA technology to introduce tumor suppressors. However, cancer needs multitargeted approaches to selectively manipulate multiple gene expressions/proteins. In this proof-of-concept study, we developed NPs containing Luc-mRNA and siRNA-GFP as model agents ((M+S)-NPs) and showed that NPs can simultaneously deliver functional mRNA and siRNA and impact the expression of two genes/proteins in vitro. Additionally, after in vivo administration, (M+S)-NPs successfully knocked down GFP while introducing luciferase into a TNBC mouse model, indicating that our NPs have the potential to develop RNA-based anticancer therapeutics. These studies pave the way to develop RNA-based, multitargeted approaches for complex diseases like cancer.
Date de publication	2024-11-15
Maison d’édition	American Chemical Society
Licence	Creative Commons, Attribution - Pas d’utilisation commerciale – Pas de modification 4.0 International (CC BY-NC-ND 4.0) https://creativecommons.org/licenses/by-nc-nd/4.0/deed.fr
Dans	ACS Nanoscience Au 4, nº 6 (15 novembre 2024) : 416–425.
Langue	anglais
Publications évaluées par des pairs	Oui
Exporter la notice	Exporter en format RIS
Signaler une correction	Signaler une correction (s'ouvre dans un nouvel onglet)
Identificateur de l’enregistrement	d819e293-bce6-45b2-9c12-a5c3f7dd28cb
Enregistrement créé	2025-04-02
Enregistrement modifié	2025-11-03

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