Chemical and Pharmaceutical Bulletin, Volume 70, Issue 6, Pages 420-426 , 01/06/2022

Enhancing Anticancer Potency of a 13-Substituted Berberine Derivative with Cationic Liposomes

Nuttapon Apiratikul, Kanlayanee Sriklung, Kulvadee Dolsophon, Pattamaporn Thamvapee, Ramida Watanapokasin, Boon Ek Yingyongnarongkul, Nattisa Niyomtham, John B. Bremner, Petcharat Watanavetch, Siritron Samosorn

Abstract

Cationic liposomal formulations of the telomeric G-quadruplex stabilizing ligand, 13-(2-naphthylmethoxy)-berberine bromide (1), have been developed with the purpose of delivering 1 into the nucleus of cancer cells for potential telomere targeting. Berberine derivative 1 was encapsulated in various cationic lipids 2–4 by the thin film evaporation method; these lipids are cationic after amine protonation. The most appropriate liposomal berberine formulation was that of 1 and the cholesterol derived cationic lipid 4 in a weight ratio of 1:20 with 76.5% encapsulation efficiency of 1. Cellular uptake studies in the HeLa and HT-29 cancer cells lines showed that the liposomal berberine derivative uptake in the cells was higher and more stable than for berberine derivative 1 alone while free 1 was completely decomposed in the cells within 60min exposure to the cells. Anticancer activity of the liposomal berberine derivative 1 based on 4 was greater than that for the free berberine derivative 1 in the MCF-7, HeLa and HT-29 cell line by 2.3-, 4.9- and 5.3-fold, respectively, and also, interestingly, superior to the anticancer drug doxorubicin against the HT29 cancer cell line.

Document Type

Article

Source Type

Journal

Keywords

cancercationic lipidencapsulationKey words berberine derivativetelomere

ASJC Subject Area

Pharmacology, Toxicology and Pharmaceutics : Drug DiscoveryChemistry : Chemistry (all)


Bibliography


Apiratikul, N., Sriklung, K., Dolsophon, K., Thamvapee, P., Watanapokasin, R., Yingyongnarongkul, B., Niyomtham, N., ... Samosorn, S. (2022). Enhancing Anticancer Potency of a 13-Substituted Berberine Derivative with Cationic Liposomes. Chemical and Pharmaceutical Bulletin, 70(6) 420-426. doi:10.1248/cpb.c21-01049

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