Thermoresponsive M1 macrophage-derived hybrid nanovesicles for improved in vivo tumor targeting

Author:

Barone AntonellaORCID,Zimbo Anna MariaORCID,d’Avanzo NicolaORCID,Tolomeo Anna MariaORCID,Ruga StefanoORCID,Cardamone AntonioORCID,Celia ChristianORCID,Scalise MariangelaORCID,Torella DanieleORCID,La Deda MassimoORCID,Iaccino EnricoORCID,Paolino DonatellaORCID

Abstract

AbstractDespite the efforts and advances done in the last few decades, cancer still remains one of the main leading causes of death worldwide. Nanomedicine and in particular extracellular vesicles are one of the most potent tools to improve the effectiveness of anticancer therapies. In these attempts, the aim of this work is to realize a hybrid nanosystem through the fusion between the M1 macrophages-derived extracellular vesicles (EVs-M1) and thermoresponsive liposomes, in order to obtain a drug delivery system able to exploit the intrinsic tumor targeting capability of immune cells reflected on EVs and thermoresponsiveness of synthetic nanovesicles. The obtained nanocarrier has been physicochemically characterized, and the hybridization process has been validated by cytofluorimetric analysis, while the thermoresponsiveness was in vitro confirmed through the use of a fluorescent probe. Tumor targeting features of hybrid nanovesicles were in vivo investigated on melanoma-induced mice model monitoring the accumulation in tumor site through live imaging and confirmed by cytofluorimetric analysis, showing higher targeting properties of hybrid nanosystem compared to both liposomes and native EVs. These promising results confirmed the ability of this nanosystem to combine the advantages of both nanotechnologies, also highlighting their potential use as effective and safe personalized anticancer nanomedicine. Graphical Abstract

Funder

Università degli studi "Magna Graecia" di Catanzaro

Publisher

Springer Science and Business Media LLC

Subject

Pharmaceutical Science

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