Natural Compounds in Liposomal Nanoformulations of Potential Clinical Application in Glioblastoma

Author:

Piwowarczyk LudwikaORCID,Mlynarczyk Dariusz T.ORCID,Krajka-Kuźniak ViolettaORCID,Majchrzak-Celińska AleksandraORCID,Budzianowska AnnaORCID,Tomczak SzymonORCID,Budzianowski JaromirORCID,Woźniak-Braszak Aneta,Pietrzyk Rafał,Baranowski MikołajORCID,Goslinski TomaszORCID,Jelinska Anna

Abstract

Glioblastoma (GBM) is the most common malignant neoplasm in adults among all CNS gliomas, with the 5-year survival rate being as low as 5%. Among nanocarriers, liposomal nanoformulations are considered as a promising tool for precise drug delivery. The herein presented study demonstrates the possibility of encapsulating four selected natural compounds (curcumin, bisdemethoxycurcumin, acteoside, and orientin) and their mixtures in cationic liposomal nanoformulation composed of two lipid types (DOTAP:POPC). In order to determine the physicochemical properties of the new drug carriers, specific measurements, including particle size, Zeta Potential, and PDI index, were applied. In addition, NMR and EPR studies were carried out for a more in-depth characterization of nanoparticles. Within biological research, the prepared formulations were evaluated on T98G and U-138 MG glioblastoma cell lines in vitro, as well as on a non-cancerous human lung fibroblast cell line (MRC-5) using the MTT test to determine their potential as anticancer agents. The highest activity was exhibited by liposome-entrapped acteoside towards the T98G cell line with IC50 equal 2.9 ± 0.9 µM after 24 hours of incubation. Noteworthy, curcumin and orientin mixture in liposomal formulation exhibited a synergistic effect against GBM. Moreover, the impact on the expression of apoptosis-associated proteins (p53 and Caspase-3) of acteoside as well as curcumin and orientin mixture, as the most potent agents, was assessed, showing nearly 40% increase as compared to control U-138 MG and T98G cells. It should be emphasized that a new and alternative method of extrusion of the studied liposomes was developed.

Funder

National Science Center

Publisher

MDPI AG

Subject

Cancer Research,Oncology

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