Proof-of-Concept Study on the Use of Tangerine-Derived Nanovesicles As SiRNA Delivery Vehicles Toward Colorectal Cancer Cell Line SW480

Overview

Journal Int J Mol Sci

Publisher MDPI

Specialties Biochemistry
Chemistry
Molecular Biology

Date 2024 Jan 11

PMID 38203716

Authors

Nima Rabienezhad Ganji

Ornella Urzi

Vincenza Tinnirello

Elisa Costanzo

Giulia Polito

Antonio Palumbo Piccionello

Mauro Manno

Samuele Raccosta

Alessia Gallo

Margot Lo Pinto

Matteo Calligaris

Simone Dario Scilabra

Maria Antonietta Di Bella

Alice Conigliaro

Simona Fontana

Stefania Raimondo

Riccardo Alessandro

Affiliations

Soon will be listed here.

Abstract

In the last years, the field of nanomedicine and drug delivery has grown exponentially, providing new platforms to carry therapeutic agents into the target sites. Extracellular vesicles (EVs) are ready-to-use, biocompatible, and non-toxic nanoparticles that are revolutionizing the field of drug delivery. EVs are involved in cell-cell communication and mediate many physiological and pathological processes by transferring their bioactive cargo to target cells. Recently, nanovesicles from plants (PDNVs) are raising the interest of the scientific community due to their high yield and biocompatibility. This study aims to evaluate whether PDNVs may be used as drug delivery systems. We isolated and characterized nanovesicles from tangerine juice (TNVs) that were comparable to mammalian EVs in size and morphology. TNVs carry the traditional EV marker HSP70 and, as demonstrated by metabolomic analysis, contain flavonoids, organic acids, and limonoids. TNVs were loaded with DDHD1-siRNA through electroporation, obtaining a loading efficiency of 13%. We found that the DDHD1-siRNA complex TNVs were able to deliver DDHD1-siRNA to human colorectal cancer cells, inhibiting the target expression by about 60%. This study represents a proof of concept for the use of PDNVs as vehicles of RNA interference (RNAi) toward mammalian cells.

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