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Preclinical pharmaco-toxicological screening of biomimetic melanin-like nanoparticles as a potential therapeutic strategy for cutaneous melanoma

Affiliation
Faculty of Pharmacy ,“Victor Babes” University of Medicine and Pharmacy from Timisoara ,Timisoara ,Romania
Marcovici, Iasmina;
Affiliation
Faculty of Medicine ,“Victor Babes” University of Medicine and Pharmacy from Timisoara ,Timisoara ,Romania
Chioibas, Raul;
Affiliation
Faculty of Pharmacy ,University of Szeged ,Szeged ,Hungary
Zupko, Istvan;
Affiliation
Faculty of Pharmacy ,“Victor Babes” University of Medicine and Pharmacy from Timisoara ,Timisoara ,Romania
Pinzaru, Iulia;
Affiliation
Faculty of Pharmacy ,“Victor Babes” University of Medicine and Pharmacy from Timisoara ,Timisoara ,Romania
Moaca, Alina;
Affiliation
Faculty of Pharmacy ,“Victor Babes” University of Medicine and Pharmacy from Timisoara ,Timisoara ,Romania
Ledeti, Adriana;
Affiliation
Electron Microscopy Laboratory “Prof. C. Craciun” ,Faculty of Biology and Geology ,“Babes-Bolyai” University ,Cluj-Napoca ,Romania
Barbu-Tudoran, Lucian;
Affiliation
Faculty of Pharmacy ,“Victor Babes” University of Medicine and Pharmacy from Timisoara ,Timisoara ,Romania
Geamantan, Andreea;
Affiliation
Faculty of Pharmacy ,“Victor Babes” University of Medicine and Pharmacy from Timisoara ,Timisoara ,Romania
Predescu, Iasmina;
Affiliation
Faculty of Pharmacy ,“Victor Babes” University of Medicine and Pharmacy from Timisoara ,Timisoara ,Romania
Dehelean, Cristina Adriana

Introduction Despite its rarity, cutaneous melanoma (CM) represents the deadliest skin cancer with a high mortality rate, an incidence on the rise, and limited therapeutic options at present. Melanin is a polymeric pigment naturally produced within melanocytes and CM cells that gained a noteworthy attention due to its pharmacological properties, and potential for the design of nanoplatforms with biomedical applications. Up to date, the utilization of melanin-like nanoparticles (MEL-NPs) in cancer treatment has been well-documented, although their efficacy in CM therapy remains scarcely investigated. The current study presents the preclinical evaluation of MEL-NPs as a potential nanomedicine for CM management. Methods MEL-NPs were produced through the oxidative polymerization of dopamine and characterized via electron microscopy and UV-VIS spectroscopy. The antioxidant activity was determined by using the DPPH method. The cytotoxic, anti-migratory, anti-clonogenic, pro-oxidant and pro-apoptotic properties of MEL-NPs were investigated in vitro by applying the MTT viability test, bright-field and immunofluorescence microscopy, DCFDA/H2DCFDA test, scratch assay, colony formation assay, and RT-qPCR. The irritant and anti-angiogenic effects were assessed in ovo on the vascularized chorioallantoic membrane (CAM). Results The as-made MEL-NPs presented a spherical morphology, an average size of 85.61 nm, a broad UV-VIS absorption spectrum, and a strong antioxidant activity. After a 24 h treatment, MEL-NPs exerted a selective cytotoxicity in SH-4 and B164A5 CM cells compared to HEMa, HaCaT, and JB6 Cl 41-5a healthy skin cells, except for the concentration of 100 µg/mL, at which their viability declined under 70%. Additionally, MEL-NPs accumulated within the intracellular space of CM cells, forming a perinuclear coating, inhibited their motility and clonogenic potential, increased intracellular oxidative stress, targeted the epithelial-to-mesenchymal transition, and induced apoptosis by altering cell morphology, nuclear aspect, F-actin and tubulin distribution, and by modulating the expression of pro- and anti-apoptotic markers. In ovo , MEL-NPs lacked irritant and vascular toxic effects, while exerting an angio-suppressive activity. Conclusion MEL-NPs demonstrated promising anti-melanoma properties, showing a selective cytotoxicity, a strong anti-invasive effect and a pro-apoptotic activity in CM cells, while inhibiting CAM angiogenesis, these novel findings contributing to future research on the potential application of this nanoplatform in CM therapy.

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License Holder: Copyright © 2025 Marcovici, Chioibas, Zupko, Pinzaru, Moaca, Ledeti, Barbu-Tudoran, Geamantan, Predescu and Dehelean.

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