Interaction of curcumin with 1,2-dioctadecanoyl-sn-glycero-3-phosphocholine liposomes: Intercalation of rhamnolipids enhances membrane fluidity, permeability and stability of drug molecule
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Elsevier B.V.
Abstract
Stability of curcumin in neutral and alkaline buffer conditions has been a serious concern for its medicinal applications. We demonstrate that the stability of curucmin can be improved in 1,2-Dioctadecanoyl-sn-glycero-3-phosphocholine (DSPC) liposomes. Curcumin strongly partition into liquid crystalline phase compared to solid gel phase of DSPC liposomes. Variation of fluorescence intensity of curcumin associated with liposomes with temperature successfully determines phase transition temperature of DSPC liposomes. However, at higher molar ratio curcumin can influence phase transition temperature by intercalating into deep hydrophobic layer of liposomes and facilitating fusion of two membrane phases. Rhamnolipids (RLs) are recently being applied for various biomedical applications. Here, we have explored new insight on intercalation of rhamnolipids with DSPC liposomes. Intercalation of rhamnolipids exceptionally increases partition of curcumin into solid gel phase of DSPC liposomes, whereas this increase is moderate in liquid crystalline phase. Fluorescence quenching study establishes that permeability and fluidity of the DSPC liposomes are enhanced in the presence of RLs. Membrane permeability and fluidity can be improved further by increasing the percentage of RLs in DSPC liposomes. The phase transition temperature of DSPC liposomes decreases with increase in percentage of RLs in DSPC liposomes by encouraging fusion between solid gel and liquid crystalline phases. Intercalation of RLs is found to further boost stability of drug, curcumin, in DSPC liposomes. Thus, mixing RLs with DSPC liposomes could potentially serve as a good candidate for drug delivery application. © 2016 Elsevier B.V.
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Curcumin, Dspc, Liposomes, Permeability, Phase transition, Rhamnolipids, Decanoates, Drug delivery systems, Drug stability, Hydrophobic and hydrophilic interactions, Kinetics, Lysophosphatidylcholines, Membrane fluidity, Rhamnose, Crystalline materials, Fluidity, Fluorescence, Intercalation, Lipids, Liquids, Mechanical permeability, Medical applications, Phase transitions, Quenching, Stability, Surface active agents, Temperature, 1,2 dioctadecanoyl sn glycero 3 phosphocholine liposome, Liposome, Rhamnolipid, Unclassified drug, Decanoic acid derivative, Lysophosphatidylcholine, Biomedical applications, Drug delivery applications, Fluorescence intensities, Liquid crystalline phase, Liquid-crystalline phasis, Article, Controlled study, Drug delivery system, Drug penetration, Gel, Intercalation complex, Liquid crystal, Molecular interaction, Priority journal, Solid, Analogs and derivatives, Chemical phenomena, Chemistry