Chlorpromazine interaction with glycerophospholipid liposomes studied by magic angle spinning solid state 13C-NMR and differential scanning calorimetry

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Abstract

Phosphatidylserine (PS) extracted from pig brain and synthetic dipalmitoylphosphatidylcholine (DPPC) and dimyristoylphosphatidylcholine (DMPC) were used to make DPPC/DMPC and DPPC/PS large unilamellar liposomes with a diameter of ∼1 μm. Chlorpromazine-HCl (CPZ), an amphipathic cationic psychotropic drug of the phenothiazine group, is known to partition into lipid bilayer membranes of liposomes with partition coefficients depending on the acyl chain length and to alter the bilayer structure in a manner depending on the phospholipid headgroups. The effects of adding CPZ to these membranes were studied by differential scanning calorimetry and proton cross polarization solid state magic angle spinning 13C-nuclear magnetic resonance spectroscopy (CP-MAS-13C-NMR). CP-MAS-13C-NMR spectra of the DPPC (60%)/DMPC (40%) and the DPPC (54%)/DMPC (36%)/CPZ (10%) liposomes, show that CPZ has low or no interaction with the phospholipids of this neutral and densely packed bilayer. Conversely, the DPPC (54%)/PS (36%)/CPZ (10%) bilayer at 25°C demonstrates interaction of CPZ with the phospholipid headgroups (PS). This CPZ interaction causes about 30% of the acyl chains to enter the gauche conformation with low or no CPZ interdigitation among the acyl chains at this temperature (25°C). The DPPC (54%)/PS (36%)/CPZ (10%) bilayer at a sample temperature of 37°C (TC=31.2°C), shows CPZ interdigitation among the phospholipids as deduced from the finding that ∼30% of the phospholipid acyl chains carbon resonances shift low-field by 5–15 ppm.

Keywords

Cross polarization solid state magic angle spinning 13C-nuclear magnetic resonance spectroscopy
Differential scanning calorimetry
DPPC/DMPC liposome
DPPC/PS liposome
Chlorpromazine-HCl interaction

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