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Vol. 289, Issue 1, 528-534, April 1999
Division of Biopharmaceutics, Photodynamic therapy is a promising new strategy in the treatment of
cardiovascular diseases. Photodynamic therapy for vascular diseases may
be improved by the specific delivery of photosensitizers to the
atherosclerotic lesion. In this study, we studied whether oxidatively
modified low-density lipoprotein (OxLDL) could be used as a specific
carrier for photosensitizers, thereby using the scavenger receptor
expressed on macrophages as a target. The photosensitizer aluminum
phthalocyanine chloride (AlPc) was incorporated into OxLDL, and its
photodynamic effects were studied. Macrophages (RAW 264.7) were
incubated with various concentrations of OxLDL-AlPc for different
periods. After illumination of the cells with red light, cytotoxicity
was observed that was dependent on the time of illumination and
incubation. Macrophages incubated with OxLDL-AlPc that were not
illuminated revealed no cytotoxicity. The uptake of the OxLDL-AlPc
complexes was mediated by scavenger receptors expressed on macrophages.
In the presence of the polyanion polyinosinic acid, a specific ligand
for scavenger receptors, no cytotoxicity could be observed. Serum
incubations of the OxLDL-AlPc complexes revealed that these complexes
stay intact after incubation. No redistribution of AlPc to other plasma
(lipo-) proteins could be detected, and 80-90% of the AlPc remained
associated with the OxLDL particle. These results indicate that OxLDL
may function as a specific delivery system for photosensitizers to the
scavenger receptors expressed on the macrophages in the atherosclerotic lesion, increasing the beneficial effects of photodynamic therapy for
cardiovascular diseases.
0022-3565/99/2891-0528$03.00/0
THE JOURNAL OF PHARMACOLOGY AND EXPERIMENTAL THERAPEUTICS
Copyright © 1999 by The American Society for Pharmacology and Experimental Therapeutics
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