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Journal of Lipid Research, Vol 29, 729-743, Copyright © 1988 by Lipid Research, Inc.
Y Kleinman, ES Krul, M Burnes, W Aronson, B Pfleger and G Schonfeld
To assess the effects of perturbing the surface of low density lipoprotein
(LDL) on the conformation of apoB-100, LDL (d 1.030-1.050 g/ml) isolated
from normal subjects were treated with phospholipase A2 (PL-A2) for 0.5 to
15 min. The resulting P-LDL and concurrent control LDL (C-LDL) incubated
without PL-A2 were isolated by gel permeation chromatography. Approximately
50% of LDL-phosphatidylcholine was hydrolyzed in 2 min and approximately
85% in 5 min. Lysophosphatidylcholine compounds (LPC) and free fatty acids
(FFA) accumulated during lipolysis but most of the LPC and all of FFA could
be removed by adding FFA-free albumin to the lipolysis mixtures.
Immunoreactivities of P-LDL and C-LDL were evaluated in competitive
radioimmunoassays, using a library of anti-human LDL monoclonal antibodies
directed against the major regions of apoB-100 (the T4, T3, and T2 thrombin
fragments). One epitope defined by monoclonal antibody 465B6C3 and
localized near the carboxyl end of the apoB-100 molecule became less
immunoreactive (ED 50s increased); three other epitopes on the T2 fragment
near the LDL receptor recognition site and four epitopes localized towards
the middle (T3) and amino terminal (T4) regions did not change. Altered
immunoreactivities were not related to LPC and FFA contents. Thus, the
conformation of apoB-100 was selectively altered by phospholipolysis. The
interactions of P-LDL with cultured fibroblasts were grossly altered: P-LDL
were bound nonspecifically to fibroblasts of both normal and homozygous
familial hypercholesterolemic subjects and P-LDL were not degraded. LPC and
FFA retained in LDL did not explain these alterations, nor did changes of
epitope expression near the LDL receptor recognition site. It is likely
that the apoB-100 aberrant cell interaction is due to loss of surface
phospholipids and "uncovering" of core lipids that react nonspecifically
with cell surface components.
ARTICLES
Lipolysis of LDL with phospholipase A2 alters the expression of selected apoB-100 epitopes and the interaction of LDL with cells
Department of Medicine, Washington University School of Medicine, St. Louis, MO 63110.
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