ABSTRACT
Polymer blends, obtained by polymerization of methyl methacrylate in the presence of poly(propylene glycol), are investigated. Poly(propylene glycol) acts as a plasticizer, significantly lowering poly(methyl methacrylate)'s glass transition temperature and decreasing its elasticity modulus and yield stress. The mixture of methyl methacrylate with poly(propylene glycol) is more stable than its mixture with currently used poly(ethylene glycol), which leads to more uniform distribution and higher possible content of the plasticizer. Unlike low molecular weight plasticizers, poly(propylene glycol) is less prone to migration and exudation during manufacturing process and in use, and has low toxicity. Dynamic mechanical thermal analysis, compression testing and X-ray diffraction were used to investigate how the properties of the material depend on the content and molecular weight of the poly(propylene glycol) in the polymer blend. It was shown that the dependence of the glass transition temperature of methyl methacrylate polymerized in the presence of poly(propylene glycol) on the molar fraction of propylene glycol units is linear, and poly(propylene glycol) with lower molecular weight affects properties of the material stronger than poly(propylene glycol) with higher molecular weight. Therefore, the addition of poly(propylene glycol) allows to control the properties of poly(methyl methacrylate) easily and within wide range.
ABSTRACT
Nonionic amphiphiles and particularly block copolymers of ethylene oxide and propylene oxide (Pluronics) cause pronounced chemosensitization of tumor cells that exhibit multiple resistance to antineoplastic drugs. This effect is due to inhibition of P-glycoprotein (P-gp) responsible for drug efflux. It was suggested that the inhibition of P-gp might be due to changes in its lipid surrounding. Indeed, high dependence of P-gp activity on the membrane microviscosity was demonstrated [Regev et al. (1999) Eur. J. Biochem. 259, 18-24], suggesting that the ability of Pluronics to affect the P-gp activity is mediated by their effect on the membrane structure. We have found recently that adsorption of Pluronics on lipid bilayers induced considerable disturbance of the lipid packing [Krylova et al. (2003) Chemistry 9, 3930-3936]. In the present paper, we studied 19 amphiphilic copolymers, including newly synthesized hyperbranched polyglycerols, Pluronic and Brij surfactants, for their ability to accelerate flip-flop and permeation of antitumor drug doxorubicin (DOX) in liposomes. It was found that not only bulk hydrophobicity but also the chemical microstructure of the copolymer determines its membrane disturbing ability. Copolymers containing polypropylene oxide caused higher acceleration of flip-flop and DOX permeation than polysurfactants containing aliphatic chains. The effects of copolymers containing hyperbranched polyglycerol "corona" were more pronounced, as compared to the copolymers with linear poly(ethylene oxide) chains, indicating that a bulky hydrophilic block induces additional disturbances in the lipid bilayer. A good correlation between the copolymer flippase activity and a linear combination of copolymer bulk hydrophobicity and the van der Waals volume of its hydrophobic block was found. The relationship between the structure of a copolymer and its ability to disturb lipid membranes presented in this paper may be useful for the design of novel amphiphilic copolymers capable of affecting the activity of membrane transporters in living cells.
Subject(s)
Epoxy Compounds/chemistry , Ethylene Oxide/chemistry , Lipid Bilayers/chemistry , Membranes, Artificial , Poloxamer/chemistry , Adsorption , Animals , Cattle , Doxorubicin/chemistry , Free Radicals/chemistry , Glycerol/chemical synthesis , Glycerol/chemistry , Hexanes/chemistry , Liposomes , Permeability , Phosphatidylcholines/chemistry , Polyethylene Glycols/chemistry , Polymers/chemical synthesis , Polymers/chemistry , Structure-Activity Relationship , Water/chemistryABSTRACT
Triblock copolymers of ethylene oxide (EO) and propylene oxide (PO) of EO(n/2)PO(m)EO(n/2) type (Pluronics) demonstrate a variety of biological effects that are mainly due to their interaction with cell membranes. Previously, we have shown that Pluronics can bind to artificial lipid membranes and enhance accumulation of the anti-tumor drug doxorubicin (DOX) inside the pH-gradient liposomes and transmembrane migration (flip-flop) of NBD-labeled phosphatidylethanolamine in the liposomes composed from one component-lecithin. Here, we describe the effects caused by insertion of other natural lipids in lecithin liposomes and the significance of the lipid composition for interaction of Pluronic L61 with the membrane. We used binary liposomes consisting of lecithin and one of the following lipids: cholesterol, phosphatidylethanolamine, ganglioside GM1, sphingomyelin, cardiolipin or phosphatidic acid. The influence of the additives on (1) membrane microviscosity; (2) binding of Pluronic L61; (3) the copolymer effect on lipid flip-flop and membrane permeability towards DOX was studied. The results showed that insertion of sphingomyelin and cardiolipin did not influence membrane microviscosity and effects of Pluronic on the membrane permeability. Addition of phosphatidic acid led to a decrease in microviscosity of the bilayer and provoked its destabilization by the copolymer. On the contrary, cholesterol increased microviscosity of the membrane and decreased binding of Pluronic and its capacity to enhance flip-flop and DOX accumulation. Analogous tendencies were revealed upon incorporation of egg phosphatidylethanolamine or bovine brain ganglioside GM1. Thus, a reverse dependence between the microviscosity of membranes and their sensitivity to Pluronic effects was demonstrated. The described data may be relevant to mechanisms of Pluronic L61 interaction with normal and tumor cells.
