Polymer-functionalized magnetic nanoparticles for targeted quercetin delivery: a potential strategy for colon cancer treatment
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Nanoparticle-based drug delivery systems improve
pharmacokinetic aspects, including controlled release and drug targeting, increasing thera peutic efficacy, and reducing toxicity in conventional colon cancer treatment. The super paramagnetism of magnetic nanoparticles (MNP) appears to be a potential alternative for
magnetothermal therapy, inducing tumor cell death by an external magnetic field. There fore, this study aimed to develop chitosan (CS) and folate-chitosan (FA-CS)-coated MNP to
improve the stability and targeting of the system for quercetin (Q) delivery. Methods: After
FA-CS synthesis and 32
factorial design, polymer-functionalized MNPs were produced
for quercetin loading, characterized, and evaluated by drug dissolution and cytotoxicity
assay. Results: The factorial design indicated the positive influence of CS on MNPs’ Zeta
potential, followed by the CS–temperature interaction. Optimized formulations had hydro dynamic diameters of 122.32 ± 8.56 nm, Zeta potentials of +30.78 ± 0.8 mV, and loading
efficiencies of 80.45% (MNP-CS-Q) and 54.4% (MNP-FA-CS-Q). The 24 h drug release was
controlled in MNP-CS-Q (up to 6.4%) and MNP-FA-CS-Q (up to 7.7%) in a simulated tumor
medium, with Fickian diffusion release mechanism correlated to the Korsmeyer–Peppas
model (R > 0.99). The cytotoxicity assay in HCT-116 showed a higher (p < 0.001) dose dependent antitumor effect of quercetin-loaded MNP compared to free drug, with IC50s
of 1.46 (MNP-CS) and 1.30 µg·mL−1
(MNP-FA-CS). Conclusions: Therefore, this study
contributes to the development of biomedical nanotechnology and the magnetic debate by
highlighting the antitumor potential of quercetin magnetic nanoparticles. The experimental
design allows the discussion of critical manufacturing variables and the determination of
optimal parameters for the formulations.
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MACEDO, Júlia Borges de et al. Polymer-functionalized magnetic nanoparticles for targeted quercetin delivery: a potential strategy for colon cancer treatment. Pharmaceutics, Basel, v. 17, n. 4, e467, 2025. DOI: 10.3390/pharmaceutics17040467. Disponível em: https://www.mdpi.com/1999-4923/17/4/467. Acesso em: 20 ago. 2025.