Barbara Gzyl-Malcher

Interaction of curcumin with lipid monolayers and liposomal bilayers

Curcumin shows huge potential as an anticancer and anti-inflammatory agent. However, to achieve a satisfactory bioavailability and stability of this compound, its liposomal form is preferable. Our detailed studies on the curcumin interaction with lipid membranes are aimed to obtain better understanding of the mechanism and eventually to improve the efficiency of curcumin delivery to cells. Egg yolk phosphatidylcholine (EYPC) one-component monolayers and bilayers, as well as mixed systems containing additionally dihexadecyl phosphate (DHP) and cholesterol, were studied. Curcumin binding constant to EYPC liposomes was determined based on two different methods: UV/Vis absorption and fluorescence measurements to be 4.26×10(4)M(-1) and 3.79×10(4)M(-1), respectively. The fluorescence quenching experiment revealed that curcumin locates in the hydrophobic region of EYPC liposomal bilayer. It was shown that curcumin impacts the size and stability of the liposomal carriers significantly. Loaded into the EYPC/DPH/cholesterol liposomal bilayer curcumin stabilizes the system proportionally to its content, while the EYPC/DPH system is destabilized upon drug loading. The three-component lipid composition of the liposome seems to be the most promising system for curcumin delivery. An interaction of free and liposomal curcumin with EYPC and mixed monolayers was also studied using Langmuir balance measurements. Monolayer systems were treated as a simple model of cell membrane. Condensing effect of curcumin on EYPC and EYPC/DHP monolayers and loosening influence on EYPC/DHP/chol ones were observed. It was also demonstrated that curcumin-loaded EYPC liposomes are more stable upon interaction with the model lipid membrane than the unloaded ones.

Curcumin-containing liposomes stabilized by thin layers of chitosan derivatives.

Stable vesicles for efficient curcumin encapsulation, delivery and controlled release have been obtained by coating of liposomes with thin layer of newly synthesized chitosan derivatives. Three different derivatives of chitosan were obtained and studied: the cationic (by introduction of the stable, quaternary ammonium groups), the hydrophobic (by attachment of N-dodecyl groups) and cationic-hydrophobic one (containing both quaternary ammonium and N-dodecyl groups). Zeta potential measurements confirmed effective coating of liposomes with all these chitosan derivatives. The liposomes coated with cationic-hydrophobic chitosan derivative are the most promising curcumin carriers; they can easily penetrate cell membrane and release curcumin in a controlled manner. Biological studies indicated that such systems are non-toxic for murine fibroblasts (NIH3T3) while toxic toward murine melanoma (B16F10) cell line.

Effect of selenium on characteristics of rape chloroplasts modified by cadmium.

Selenium appears to be an important protective agent that decreases cadmium-induced toxic effects in animals and plants. The aim of these studies was to investigate the changes of properties of chloroplast membranes obtained from Cd-treated rape seedlings caused by Se additions. Chloroplasts were isolated from leaves of 3-week-old rape plants cultured on Murashige-Skoog media supplied with 2 microM Na(2)SeO(4) and/or 400 microM CdCl(2) under in vitro conditions. The following physicochemical characteristics of chloroplasts were chosen as indicators of Se-effects: average size, zeta potential, ultrastructure, lipid and fatty acid composition and fluidity of envelope membrane. The results suggest that Se can partly counterbalance the destructive effects of Cd. This protective action led to an increase of chloroplast size reduced by Cd treatment and rebuilt, to some extent, the chloroplast ultrastructure. Lipid and fatty acid composition of chloroplast envelopes modified by Cd showed a decrease in digalactosyl-diacylglycerol content and an increase of content of monogalactosyl-diacylglycerol and phospholipid fractions, as well as an increase of fatty acid saturation of all lipids studied. The change in fatty acid saturation correlated well with a decrease of membrane fluidity and with a diminishing of absolute values of zeta potential. The presence of selenium in cultured media caused a partial reversal of the detected changes, which was especially visible in properties related to the hydrophobic part of an envelope, i.e. fatty acid saturation and fluidity.

Mixed DPPC/DPTAP Monolayers at the Air/Water Interface: Influence of Indolilo-3-acetic Acid and Selenate Ions on the Mono layer Morphology

The interactions of mixed monolayers of two lipids, zwitterionic 1,2-dipalmitoyl-phosphatidylcholine (DPPC) and positively charged 1,2-dipalmitoyl-3-trimethylammonium-propane (DPTAP), with phytohormone indolilo-3-acetic acid (IAA) and selenate anions in the aqueous subphase were studied. For this purpose, isotherms of the surface pressure versus the mean molecular area were recorded. Domain formation was investigated by using Brewster angle microscopy (BAM). The method of grazing incidence X-ray diffraction (GIXD) was also applied for the characterization of the organization of lipid molecules in condensed monolayers. It was found that selenate ions contribute to monolayer condensation by neutralizing the positive net charge of mixed monolayers whereas IAA molecules penetrated the lipid monolayer, causing its expansion/fluidization. When both solutes were introduced into the subphase, a competition between them for interaction with the positively charged lipids in the monolayer was observed.

Interaction of prazosin with model membranes--a Langmuir monolayer study.

In this study, the effect of prazosin on the molecular interactions between cholesterol and 1,2-dipalmitoylphosphatidylcholine (DPPC) within a monolayer at an air-water interface was studied. A mixed cholesterol/DPPC monolayer was employed as a model lipid membrane. From a detailed analysis of surface pressure-area isotherms, it was concluded that DPPC and cholesterol were miscible and formed non-ideal monolayers on prazosin solution. The thermodynamic stability of the mixed monolayers was investigated by analyzing the free energy of mixing. It was found that the mixed monolayers were more stable than the single component monolayers. Monolayers spread over a subphase with prazosin were more compressible than those spread on pure water. To quantify the effect of prazosin on the monolayer stability, the Gibbs free energy due to the presence of prazosin in the water subphase was calculated. It was found that prazosin penetrated and destabilized mixed cholesterol/DPPC monolayers. However, a comparison of the drug penetration into the pure DPPC monolayer and the mixed cholesterol/DPPC monolayer showed that the presence of cholesterol in the DPPC monolayer considerably restricted the drug penetration.

Differences in surface behaviour of galactolipoids originating from different kind of wheat tissue cultivated in vitro

The aim of presented researches was to investigate the physicochemical properties of Langmuir monolayer of galactolipids extracted from two different kinds of plastids: immature embryos and inflorescences. Differences between the physicochemical properties of the plastid membranes may help to explain different physiological processes, such as plant regeneration. Surface pressure (pi) vs. molecular area (A) isotherms of the monogalactosyldiacylglycerol (MGDG)/digalactosyldiacylglycerol (DGDG) monolayers of various molar ratios were measured at 15 degrees C. Galactolipids were extracted from two different types of tissue: inflorescences and embryos. Based on the analysis of the pi-A isotherms, the properties of monolayers, such as collapse pressure (pi(coll)), limiting area (A(lim)), compressibility modulus (C(s)(-1)), excess free energy of mixing (DeltaG(EXC)) and free energy of mixing (DeltaG(MIX)), were calculated. The results show that pure MGDG and DGDG and their mixtures form liquid-expanded monolayers, independently on the kind of tissue. Galactolipids originating from inflorescences produce more compressible films at the air/water interface, with larger limiting area per molecule and lower stability against the collapse process. MGDG and DGDG are miscible and form non-ideal mixed monolayers at the air/water interface. Negative values of DeltaG(EXC) were calculated for the mixture of galactolipids originating from inflorescences, with the content of MGDG, x(MGDG)>0.6. In the case of embryos, the negative values of DeltaG(EXC) were found for x(MGDG) approximately 0.5. Therefore, the attractive interactions between MGDG and DGDG exist in the mixtures of these compositions. As it is shown by negative values of DeltaG(MIX), mixed monolayers are more stable compared with unmixed ones.

Effect of tocopherol on surface properties of plastid lipids originating from wheat calli cultivated in cadmium presence.

The behaviour of equimolar mixtures of alpha-tocopherol with monogalactosyldiacylglycerol (MGDG) and digalactosyldiacylglycerol (DGDG) and phospholipids (PL) isolated from wheat calli cultured on media with and without cadmium was investigated at the air-water interface by surface pressure-area (pi-A) measurements established using an automated Langmuir-type film balance. It was found that monolayers of all studied compounds were expanded. The additivity rule was not fulfilled and the collapse pressure of mixtures was different from these recorded for pure components. This can be related with the existence of interactions between molecules in mixed monolayers. Tocopherol diminished the differences between parameters of monolayers formed by lipids extracted from objects cultivated on various media (with and without cadmium).

Influence of Cadmium and Selenate on the Interactions between Hormones and Phospholipids

In this study, the influence of plant hormones, negatively charged indolilo-3-acetic acid (IAA) and positively charged zeatin, on lipid membranes was studied. As models of negatively and positively charged biological membranes, monolayers of 1,2-dimyristoyl-sn-glycero-3-[phospho-l-serine] (DMPS) and 1,2-dipalmitoyl-3-trimethylammonium-propane (DPTAP) at the water/air interface were used, respectively. Additionally, the effect of cadmium and selenium ions on the interactions between hormones and lipids was studied. Surface pressure and surface potential measurements, Brewster angle microscopy (BAM), and grazing incidence X-ray diffraction (GIXD) were used for that purpose. Both IAA and zeatin led to an expansion of the lipid monolayer caused by electrostatic interactions between oppositely charged groups: negatively charged polar group of DMPS and positively charged zeatin or positive DPTAP headgroup and negative IAA. The addition of ions to the subphase containing hormones causes competitive interactions of both solutes with oppositely charged lipid polar heads. The largest effect was observed for IAA. While zeatin does not change the domain shape of DMPS, IAA causes the complete disappearance of characteristic DPTAP domains. Addition of SeO(4)(2-) ions causes restoration of DPTAP domains observed on pure water.

Temperature dependence of the interaction of prazosin with lipid Langmuir monolayers.

The influence of temperature on membrane-prazosin interactions was studied. Prazosin, a quinazoline derivative of 2-furoylpiperazine, is a classic antihypertensive and antiarrhythmic drug. A mixed cholesterol/phospholipid monolayer at the water/air interface was employed as a simplified biomembrane model. Brewster angle microscopy (BAM) was used to visualize the monolayer morphology. It was found that prazosin penetrates Langmuir monolayers and modifies the interactions between membrane components, causing monolayer fluidization. An increase in temperature facilitates penetration of prazosin into the monolayers. Prazosin interacts preferentially with phosphatidylcholine and modifies the morphology of the condensed phase domains of DPPC. In the presence of prazosin, monolayers collapse at lower surface pressures. The difference between the collapse pressures of monolayers on water with and without prazosin increases with temperature.

Influence of polymer–surfactant aggregates on fluid flow

This paper describes the influence of interactions of poly(ethylene oxide) (PEO) with cationic cetyltrimethylammonium bromide (CTAB) micelles on drag reduction. Since the interactions between PEO and CTAB micelles alone are weak, salicylate ions were used as CTAB counterions. They facilitate formation of polymer-micelle aggregates by screening the electrostatic repulsions between the charged surfactant headgroups. The influence of polymer-surfactant interactions on drag reduction is of biomedical engineering importance. Drag reducing additives introduced to blood produce beneficial effects on blood circulation, representing a novel way to treat cardiovascular disorders. PEO is a blood-compatible polymer. However, it quickly mechanically degrades when subjected to high shear stresses. Thus, there is a need to search for other additives able to reduce drag, which would be more mechanically stable, e.g. polymer-surfactant aggregates. Numerical simulations of the flow were performed using the CFX software. Based on the internal structure of the polymer-surfactant solution, a hypothesis explaining the reason of increase of drag reduction and decrease in dynamic viscosity with increasing shear rate was proposed. It was suggested that the probable reason for the abrupt increase in friction factor, observed when the critical Reynolds number was exceeded, was the disappearance of the difference in the dynamic viscosity.