Self-assembling drug delivery systems have drawn attention over recent decades thanks to their versatility and easy preparation processes. Of the various nanocarriers available, micelles are able to self-assemble from an amphiphilic molecule in an aqueous solution, making them simple to prepare. In this work, 1,2-distearoyl-sn-glycero-3-phosphoethanolamine-N-[methoxy(polyethylene glycol)-2000] (PEG-DSPE) was utilized to prepare lipid-based micelles for the encapsulation of a gemcitabine prodrug, GemC18, with the aim of improving its anticancer activity. Furthermore, an active targeting strategy was achieved by preparing Gem-C18-loaded PEG-DSPE micelles in the presence of a hyaluronic acid (4800 or 14,800 Da) (HA)-phospholipid conjugate (HA-DPPE) to provide actively targeted mixed micelles. This study presents the characterization of the mixed micelles, from basic characteristics (size, PDI, and zeta potential) to complex molecular structure (FESEM, X-ray diffraction, SAXS), and demonstrates that the presence of the HA-conjugate does not alter the physicochemical properties of the PEG-DSPE micelles. The mixed micelles display a size of below 100 nm, a negative zeta potential of −30 mV, and a high encapsulation efficiency (above 90 %). Finally, their preferential uptake, and consequently their cytotoxicity on cancer cell lines that overexpress the HA-specific receptor (CD44), has been assessed and confirmed using competition assays.
Andreana, I., Bincoletto, V., Ricci, C., Salaroglio, I.c., Manzoli, M., Zurletti, B., et al. (2025). Smart hyaluronated micelles to enhance a gemcitabine prodrug efficacy. JOURNAL OF DRUG DELIVERY SCIENCE AND TECHNOLOGY, 104 [10.1016/j.jddst.2024.106518].
Smart hyaluronated micelles to enhance a gemcitabine prodrug efficacy
Matricardi, Pietro;
2025-01-01
Abstract
Self-assembling drug delivery systems have drawn attention over recent decades thanks to their versatility and easy preparation processes. Of the various nanocarriers available, micelles are able to self-assemble from an amphiphilic molecule in an aqueous solution, making them simple to prepare. In this work, 1,2-distearoyl-sn-glycero-3-phosphoethanolamine-N-[methoxy(polyethylene glycol)-2000] (PEG-DSPE) was utilized to prepare lipid-based micelles for the encapsulation of a gemcitabine prodrug, GemC18, with the aim of improving its anticancer activity. Furthermore, an active targeting strategy was achieved by preparing Gem-C18-loaded PEG-DSPE micelles in the presence of a hyaluronic acid (4800 or 14,800 Da) (HA)-phospholipid conjugate (HA-DPPE) to provide actively targeted mixed micelles. This study presents the characterization of the mixed micelles, from basic characteristics (size, PDI, and zeta potential) to complex molecular structure (FESEM, X-ray diffraction, SAXS), and demonstrates that the presence of the HA-conjugate does not alter the physicochemical properties of the PEG-DSPE micelles. The mixed micelles display a size of below 100 nm, a negative zeta potential of −30 mV, and a high encapsulation efficiency (above 90 %). Finally, their preferential uptake, and consequently their cytotoxicity on cancer cell lines that overexpress the HA-specific receptor (CD44), has been assessed and confirmed using competition assays.| File | Dimensione | Formato | |
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