Phase behavior of cholesteryl ester dispersions which model the inclusions of foam cells.

In order to understand the phase behavior of the approximately 1-micron-diameter droplets which occur in the cytoplasm of cholesterol-enriched cells, differential scanning calorimetry has been utilized to elucidate the factors controlling the rate of crystallization of cholesteryl esters. The kinetics of the thermotropic transitions between liquid, liquid-crystal, and crystal states which occur in mixtures of cholesteryl oleate and cholesteryl palmitate present in monodisperse, phospholipid-stabilized, emulsion droplets have been determined and are compared to the characteristics of these transitions in bulk mixtures. Cholesteryl palmitate is observed to crystallize in undercooled phospholipid-stabilized dispersions of cholesteryl palmitate/cholesteryl oleate (50/50 w/w) at temperatures up to 50 degrees C lower than it does in bulk mixtures of the same cholesteryl ester composition. It is postulated that this difference between crystallization temperatures is due primarily to the presence of impurities present in bulk mixtures which act as catalysts that promote crystallization. It is suggested that phospholipid-stabilized dispersions of cholesteryl palmitate/cholesteryl oleate are more appropriate models than bulk mixtures of these cholesteryl esters for studying the kinetic and thermodynamic basis of the phase behavior in cholesteryl ester rich inclusions characteristic of foam cells and atherosclerotic plaque. The thermotropic phase behavior of these dispersions can be satisfactorily analyzed by using the equations of homogeneous nucleation theory. The interfacial tension between the crystal nucleus and the surrounding fluid cholesteryl ester is about 10 erg/cm2.(ABSTRACT TRUNCATED AT 250 WORDS)