Cannabimimetic N-Stearoylethanolamine as “Double-Edged Sword” in Anticancer Chemotherapy: Proapoptotic Effect on Tumor Cells and Suppression of Tumor Growth versus Its Bio-Protective Actions in Complex with Polymeric Carrier on General Toxicity of Doxorubicin In Vivo

Author:

Panchuk Rostyslav12ORCID,Skorokhyd Nadiya1ORCID,Chumak Vira1ORCID,Lehka Lilya1,Kosiakova Halyna3,Horid’ko Tetyana3ORCID,Hudz Iehor3,Hula Nadiya3,Riabtseva Anna4,Mitina Nataliya4ORCID,Zaichenko Alexander45,Heffeter Petra2ORCID,Berger Walter2ORCID,Stoika Rostyslav1ORCID

Affiliation:

1. Institute of Cell Biology National Academy of Sciences of Ukraine, Drahomanov Str., 14/16, 79005 Lviv, Ukraine

2. Center for Cancer Research and Comprehensive Cancer Center, Medical University of Vienna, Borschkegasse 8a, 1090 Vienna, Austria

3. Palladin Institute of Biochemistry National Academy of Sciences of Ukraine, Leontovycha Str. 9, 01030 Kyiv, Ukraine

4. Department of Organic Chemistry, Lviv Polytechnic National University, S. Bandera Str. 12, 79013 Lviv, Ukraine

5. Department of Applied Physics and Nanomaterial Science, Lviv Polytechnic National University, S. Bandera Str. 12, 79013 Lviv, Ukraine

Abstract

This study reports a dose-dependent pro-apoptotic action of synthetic cannabimimetic N-stearoylethanolamine (NSE) on diverse cancer cell lines, including multidrug-resistant models. No antioxidant or cytoprotective effects of NSE were found when it was applied together with doxorubicin. A complex of NSE with the polymeric carrier poly(5-(tert-butylperoxy)-5-methyl-1-hexen-3-yn-co-glycidyl methacrylate)-graft-PEG was synthesized. Co-immobilization of NSE and doxorubicin on this carrier led to a 2-10-fold enhancement of the anticancer activity, particularly, against drug-resistant cells overexpressing ABCC1 and ABCB1. This effect might be caused by accelerated nuclear accumulation of doxorubicin in cancer cells, which led to the activation of the caspase cascade, revealed by Western blot analysis. The NSE-containing polymeric carrier was also able to significantly enhance the therapeutic activity of doxorubicin in mice with implanted NK/Ly lymphoma or L1210 leukemia, leading to the complete eradication of these malignancies. Simultaneously, loading to the carrier prevented doxorubicin-induced elevation of AST and ALT as well as leukopenia in healthy Balb/c mice. Thus, a unique bi-functionality of the novel pharmaceutical formulation of NSE was revealed. It enhanced doxorubicin-induced apoptosis in cancer cells in vitro and promoted its anticancer activity against lymphoma and leukemia models in vivo. Simultaneously, it was very well tolerated preventing frequently observed doxorubicin-associated adverse effects.

Funder

OEAD

National Academy of Sciences of Ukraine

West-Ukrainian Biomedical Research Center

Austrian Science Fund

JESH-Ukraine fellowship

Publisher

MDPI AG

Subject

Pharmaceutical Science

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