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Journal of Lipid Research, Vol 37, 1897-1906, Copyright © 1996 by Lipid Research, Inc.
E Campos, S Jackle, G Chi Chen and RJ Havel
We have isolated two fractions of very low density lipoprotein particles in
human plasma that lack apolipoprotein (apo) E by combined anti-apoE and
heparin affinity chromatography of whole plasma followed by
ultracentrifugation. The two fractions are distinguished by their ability
to bind to heparin. Each of these fractions, designated "B" particles to
distinguish them from very low density lipoproteins that contain apoE
("B,E" particles), comprises an appreciable fraction of total particles in
very low density lipoproteins of normolipidemic and hypertriglyceridemic
subjects. The heparin-unbound B particles, which have been reported
previously by others, are larger and have negligible affinity for low
density lipoprotein receptors. The heparin-bound B particles are smaller
and do bind to low density lipoprotein receptors, albeit with much lower
affinity than B,E particles. No differences in accessibility to limited
protease digestion were found between apoB-100 in the two types of B
particles. Our data indicate that a substantial fraction of human very low
density lipoproteins lacks apoE, the principal ligand for lipoprotein
receptors that mediate the terminal catabolism of these lipoproteins.
Whereas the B particles that fail to bind to heparin are likely to
represent a form of nascent lipoprotein, the origin of those B particles
that bind to heparin remains to be determined.
ARTICLES
Isolation and characterization of two distinct species of human very low density lipoproteins lacking apolipoprotein E
Cardiovascular Research Institute, University of California, San Francisco, 94143-0130, USA.
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