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Antitumor efficiency of the natural alkaloid berberine complexed with C60 fullerene in Lewis lung carcinoma in vitro and in vivo

小檗碱 体内 刘易斯肺癌 体外 MTT法 化学 细胞毒性 细胞凋亡 流式细胞术 药理学 分子生物学 生物化学 癌症 医学 生物 内科学 生物技术 转移
作者
Anna Grebinyk,Svitlana Prylutska,Sergii Grebinyk,Maxim P. Evstigneev,Iryna Krysiuk,T. D. Skaterna,I. R. Horak,Yanfang Sun,Л. Б. Дробот,Olga Matyshevska,Yu. І. Prylutskyy,Uwe Ritter,Marcus Frohme
出处
期刊:Cancer Nanotechnology [BioMed Central]
卷期号:12 (1) 被引量:19
标识
DOI:10.1186/s12645-021-00096-6
摘要

Abstract Background Berberine (Ber) is a herbal alkaloid with pharmacological activity in general and a high anticancer potency in particular. However, due to its low bioavailability, the difficulty in reaching a target and choosing the right dose, there is a need to improve approaches of Ber use in anticancer therapy. In this study, Ber, noncovalently bound to a carbon nanostructure C 60 fullerene (C 60 ) at various molar ratios of the components, was explored against Lewis lung carcinoma (LLC). Methods C 60 –Ber noncovalent nanocomplexes were synthesized in 1:2, 1:1 and 2:1 molar ratios. Ber release from the nanocomplexes was studied after prolonged incubation at different pH with the liquid chromatography–mass spectrometry analysis of free Ber content. Biological effects of the free and C 60 -complaxated Ber were studied in vitro towards LLC cells with phase-contrast and fluorescence microscopy, flow cytometry, MTT reduction, caspase activity and wound closure assays. The treatment with C 60 –Ber nanocomplex was evaluated in vivo with the LLC-tumored C57Bl mice. The mice body weight, tumor size, tumor weight and tumor weight index were assessed for four groups, treated with saline, 15 mg C 60 /kg, 7.5 mg Ber/kg or 2:1 C 60 -Ber nanocomplex (15 mg C 60 /kg, 7.5 mg Ber/kg). Results Ber release from C 60 –Ber nanocomplexes was promoted with medium acidification. LLC cells treatment with C 60 –Ber nanocomplexes was followed by enhanced Ber intracellular uptake as compared to free Ber. The cytotoxicity of the studied agents followed the order: free Ber < 1:2 < 1:1 < 2:1 C 60 –Ber nanocomplex. The potency of cytotoxic effect of 2:1 C 60 –Ber nanocomplex was confirmed by 21.3-fold decrease of IC 50 value (0.8 ± 0.3 µM) compared to IC 50 for free Ber (17 ± 2 µM). C 60 –Ber nanocomplexes induced caspase 3/7 activation and suppressed the migration activity of LLC cells. The therapeutic potency of 2:1 C 60 –Ber nanocomplex was confirmed in a mouse model of LLC. The tumor growth in the group treated with 2:1 C 60 –Ber nanocomplex is suppressed by approximately 50% at the end of experiment, while in the tumor-bearing group treated with free Ber no therapeutic effect was detected. Conclusions This study indicates that complexation of natural alkaloid Ber with C 60 may be a novel therapeutic strategy against lung carcinoma. Graphical abstract
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