| Literature DB >> 29195915 |
Ahmed Abu-Fayyad1, Mohammad M Kamal2, Jennifer L Carroll3, Ana-Maria Dragoi4, Robert Cody5, James Cardelli6, Sami Nazzal7.
Abstract
Vitamin E TPGS is a tocopherol (α-T) based nonionic surfactant that was used in the formulation of the Tocosol™ paclitaxel nanoemulsion, which was withdrawn from phase III clinical trials. Unlike tocopherols, however, the tocotrienol (T3) isomers of vitamin E were found to have innate anticancer activity and were shown to potentiate the antitumor activity of paclitaxel. The primary objective of the present study was therefore to develop a paclitaxel nanoemulsions by substituting α-T oil core of Tocosol™ with γ-T3 in, and vitamin E TPGS with PEGylated γ-T3 as the shell, and test the nanoemulsions against Bx-PC-3 and PANC-1 pancreatic tumor cells. A secondary objective was to test the activity of paclitaxel when directly conjugated with the γ-T3 isomer of vitamin E. The synthesis of the conjugates was confirmed by NMR and mass spectroscopy. Developed nanoemulsions were loaded with free or lipid conjugated paclitaxel. Nanoemulsions droplets were <300 nm with fastest release observed with formulations loaded with free paclitaxel when γ-T3 was used as the core. Substituting α-T with γ-T3 was also found to potentiate the anticancer activity of the nanoemulsions. Although marginal increase in activity was observed when nanoemulsions were loaded with free paclitaxel, a significant increase in activity was observed when lipid conjugates were used. The results from this study suggest that the developed paclitaxel nanoemulsions with either γ-T3, PEGylated γ-T3, or paclitaxel lipid conjugates may represent a more promising option for paclitaxel delivery in cancer chemotherapy.Entities:
Keywords: Cancer chemotherapy; Drug delivery; Nanoemulsion; Nanotechnology; PEGylation; Paclitaxel; Tocotrienol; Vitamin E TPGS
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Year: 2017 PMID: 29195915 PMCID: PMC5803428 DOI: 10.1016/j.ijpharm.2017.11.062
Source DB: PubMed Journal: Int J Pharm ISSN: 0378-5173 Impact factor: 5.875