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Journal of Lipid Research, Vol 36, 714-724, Copyright © 1995 by Lipid Research, Inc.
PM Morganelli, RA Rogers, TJ Kitzmiller and A Bergeron
Macrophage-derived foam cells are important constituents of atheromatous
lesions. In addition to the scavenger receptor pathway, uptake of immune
complexed lipoproteins through IgG Fc receptors (Fc gamma receptors)
represents an additional pathway of macrophage foam cell development that
may be important during atherogenesis. The importance of this mechanism is
suggested by studies showing that the titer of autoantibodies to modified
lipoproteins correlated with the extent of occlusive disease in patients,
and that those antibodies exist in human lesions. Human mononuclear
phagocytes possess three structurally and functionally distinct classes of
Fc gamma receptors, each of which could be associated with a unique pathway
of lipoprotein metabolism. In order to determine whether uptake of an acute
lipid load through each type of Fc gamma receptor was associated with foam
cell development, we used bispecific antibodies consisting of anti-LDL
monoclonal antibodies conjugated to anti-Fc gamma receptor monoclonal
antibodies to study the effects of targeting LDL aggregates to each
specific type of Fc gamma receptor on freshly isolated adherent human
monocytes. Relative to appropriate controls, LDL degradation, cellular
sterol mass, and foam cell development of monocytes were enhanced by
targeting LDL aggregates to Fc gamma RI or Fc gamma RII, and this was
accompanied by an apparent impairment of LDL degradation. Uptake was
specific to the Fc gamma receptors and was not influenced by the presence
of scavenger receptor ligands. Thus, with the bispecific approach, the
functions of each class of Fc gamma receptor can be studied on an
individual basis with respect to several aspects of cellular cholesterol
metabolism. This will be critical for determining which of these receptors
are potentially most important in the clearance of lipoprotein immune
complexes during atherogenesis.
ARTICLES
Enhanced metabolism of LDL aggregates mediated by specific human monocyte IgG Fc receptors
Veteran's Administration Hospital, VT 05009, USA.
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