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Please use this identifier to cite or link to this item: https://dspace.ffh.bg.ac.rs/handle/123456789/2036
Title: Can Zeolite-Supporting Acridines Boost Their Anticancer Performance?
Authors: Ranković, Maja
Jevremović, Anka 
Janošević Ležaić, Aleksandra
Arsenijević, Aleksandar
Rupar, Jelena
Dobričić, Vladimir
Nedić Vasiljević, Bojana 
Gavrilov, Nemanja 
Bajuk-Bogdanović, Danica 
Milojević-Rakić, Maja 
Keywords: acridine derivatives;anticancer;cytotoxicity;drug release;zeolite
Issue Date: 22-Mar-2023
Journal: Journal of functional biomaterials
Abstract: 
Acridine and its derivatives (9-chloroacridine and 9-aminoacridine) are investigated here, supported on FAU type zeolite Y, as a delivery system of anticancer agents. FTIR/Raman spectroscopy and electron microscopy revealed successful drug loading on the zeolite surface, while spectrofluorimetry was employed for drug quantification. The effects of the tested compounds on cell viability were evaluated using in vitro methylthiazol-tetrazolium (MTT) colorimetric technique against human colorectal carcinoma (cell line HCT-116) and MRC-5 fibroblasts. Zeolite structure remained unchanged during homogeneous drug impregnation with achieved drug loadings in the 18-21 mg/g range. The highest drug release, in the µM concentration range, with favourable kinetics was established for zeolite-supported 9-aminoacridine. The acridine delivery via zeolite carrier is viewed in terms of solvation energy and zeolite adsorption sites. The cytotoxic effect of supported acridines on HCT-116 cells reveals that the zeolite carrier improves toxicity, while the highest efficiency is displayed by zeolite-impregnated 9-aminoacridine. The 9-aminoacridine delivery via zeolite carrier favours healthy tissue preservation while accompanying increased toxicity toward cancer cells. Cytotoxicity results are well correlated with theoretical modelling and release study, providing promising results for applicative purposes.
URI: https://dspace.ffh.bg.ac.rs/handle/123456789/2036
ISSN: 2079-4983
DOI: 10.3390/jfb14030173
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University of Belgrade
Faculty of Physical Chemistry
Studentski trg 12-16
11158 Belgrade 118
PAC 105305
SERBIA
University of Belgrade Faculty of Physical Chemistry