Simultaneous encapsulation of hydrophilic and lipophilic molecules in liposomes of DSPC

[Display omitted] •DSPC liposomes trap pinocembrin and cholesterol in the lipid bilayer and resazurin in the aqueous center.•Pinocembrin is localized outside of the cooperative zone or between the spaces that cholesterol left.•Pinocembrin tends to aggregate in regions where other molecules were prev...

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Bibliographic Details
Published in:Thermochimica acta 2020-05, Vol.687, p.178462, Article 178462
Main Authors: Romero-Arrieta, Mariana R., Uria-Canseco, Elizabeth, Perez-Casas, Silvia
Format: Article
Language:English
Subjects:
Cancer
DSC
Nanocarrier
Pinocembrin
Resazurin
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Summary:[Display omitted] •DSPC liposomes trap pinocembrin and cholesterol in the lipid bilayer and resazurin in the aqueous center.•Pinocembrin is localized outside of the cooperative zone or between the spaces that cholesterol left.•Pinocembrin tends to aggregate in regions where other molecules were previously hosted.•High amounts of pinocembrin causes domains formation and non-spherical vesicles with different physicochemical properties. This study shows simultaneous incorporation of two hydrophobic molecules and a hydrophilic molecule into distearoylphosphatidylcholine (DSPC) liposomes. Pinocembrin and cholesterol are incorporated in the lipidic membrane while resazurin is encapsulated in the aqueous center. The thermotropic behavior of liposomes as a function of the additives was studied with differential scanning calorimetry and the morphology was observed by SEM. A high percentage of entrapment was found for different concentrations of pinocembrin. Cholesterol does not interfere with the incorporation efficiency of pinocembrin and improves the distribution in the membrane but decreases the dissolution stability of liposomes due to steric hindrance in the bilayer. Encapsulation efficiency of resazurin was close to 50%. This molecule also interacts with the polar heads of the phospholipids. This research offers an alternative formulation by using DSPC liposomes as carrier of molecules with different polarity to evaluate the cytotoxicity of pinocembrin in cancer cell lines.
ISSN:0040-6031
1872-762X
DOI:10.1016/j.tca.2019.178462