Thermosensitive Drug Delivery System SBA-15-PEI for Controlled Release of Nonsteroidal Anti-Inflammatory Drug Diclofenac Sodium Salt: A Comparative Study

Lubos Zauska; Stefan Bova; Eva Benova; Jozef Bednarcik; Matej Balaz; Vladimir Zelenak; Virginie Hornebecq; Miroslav Almasi

doi:10.3390/ma14081880

Thermosensitive Drug Delivery System SBA-15-PEI for Controlled Release of Nonsteroidal Anti-Inflammatory Drug Diclofenac Sodium Salt: A Comparative Study

Materials (Basel). 2021 Apr 9;14(8):1880. doi: 10.3390/ma14081880.

Authors

Lubos Zauska¹, Stefan Bova², Eva Benova¹, Jozef Bednarcik³, Matej Balaz⁴, Vladimir Zelenak¹, Virginie Hornebecq⁵, Miroslav Almasi¹

Affiliations

¹ Department of Inorganic Chemistry, Faculty of Science, P. J. Šafárik University, Moyzesova 11, SK-041 01 Košice, Slovakia.
² BovaChem s.r.o, Garbiarska 1919/14, SK-048 01 Rožňava, Slovakia.
³ Institute of Experimental Physics, Slovak Academy of Sciences, Watsonova 47, SK-040 01 Košice, Slovakia.
⁴ Institute of Geotechnics, Slovak Academy of Sciences, Watsonova 45, SK-040 01 Košice, Slovakia.
⁵ Madirel Laboratory, CNRS, MADIREL, Aix-Marseille University, F-133 97 Marseille, France.

Abstract

Mesoporous SBA-15 silica material was prepared by the sol-gel method and functionalized with thermosensitive polyethylenimine polymers with different molecular weight (g·mol^-1): 800 (SBA-15(C)-800), 1300 (SBA-15(C)-1300) and 2000 (SBA-15(C)-2000). The nonsteroidal anti-inflammatory drug (NSAID) diclofenac sodium was selected as a model drug and encapsulated into the pores of prepared supports. Materials were characterized by the combination of infrared spectroscopy (IR), atomic force microscopy (AFM), transmission electron microscopy (TEM), photon cross-correlation spectroscopy (PCCS), nitrogen adsorption/desorption analysis, thermogravimetry (TG), differential scanning calorimetry (DSC) and small-angle X-ray diffraction (SA-XRD) experiments. The drug release from prepared matrixes was realized in two model media differing in pH, namely small intestine environment/simulated body fluid (pH = 7.4) and simulated gastric fluid (pH = 2), and at different temperatures, namely normal body temperature (T = 37 °C) and inflammatory temperature (T = 42 °C). The process of drug loading into the pores of prepared materials from the diclofenac sodium salt solutions with different concentrations and subsequent quantitative determination of released drugs was analyzed by UV-VIS spectroscopy. Analysis of prepared SBA-15 materials modified with polyethylenimines in solution showed a high ability to store large amounts of the drug, up to 230 wt.%. Experimental results showed their high drug release into the solution at pH = 7.4 for both temperatures, which is related to the high solubility of diclofenac sodium in a slightly alkaline environment. At pH = 2, a difference in drug release rate was observed between both temperatures. Indeed, at a higher temperature, the release rates and the amount of released drug were 2-3 times higher than those observed at a lower temperature. Different kinetic models were used to fit the obtained drug release data to determine the drug release rate and its release mechanism. Moreover, the drug release properties of prepared compounds were compared to a commercially available medicament under the same experimental conditions.

Keywords: diclofenac sodium; kinetic models; mesoporous silica; polyethylenimines; surface modification; temperature and pH.

Abstract

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