Abstract
Much of the cholesterol that accumulates in atherosclerotic plaques is found within monocyte-macrophages transforming these cells into "foam cells." Native low density lipoprotein (LDL) does not cause foam cell formation. Treatment of LDL with cholesterol esterase converts LDL into cholesterol-rich liposomes having >90% cholesterol in unesterified form. Similar cholesterol-rich liposomes are found in early developing atherosclerotic plaques surrounding foam cells. We now show that cholesterol-rich liposomes produced from cholesterol esterase-treated LDL can cause human monocyte-macrophage foam cell formation inducing a 3-5-fold increase in macrophage cholesterol content of which >60% is esterified. Although cytochalasin D inhibited LDL liposome-induced macrophage cholesteryl ester accumulation, LDL liposomes did not enter macrophages by phagocytosis. Rather, the LDL liposomes induced and entered surface-connected compartments within the macrophages, a unique endocytic pathway in these cells that we call patocytosis. LDL liposome apoB rather than LDL liposome lipid mediated LDL liposome uptake by macrophages. This was shown by the findings that: 1) protease treatment of the LDL liposomes prevented macrophage cholesterol accumulation; 2) liposomes prepared from LDL lipid extracts did not cause macrophage cholesterol accumulation; and 3) purified apoB induced and accumulated within macrophage surface-connected compartments. Although apoB mediated the macrophage uptake of LDL liposomes, this uptake did not occur through LDL, LDL receptor-related protein, or scavenger receptors. Also, LDL liposome uptake was not sensitive to treatment of macrophages with trypsin or heparinase. Cholesterol esterase-mediated transformation of LDL into cholesterol-rich liposomes is an LDL modification that: 1) stimulates uptake of LDL cholesterol by apoB-dependent endocytosis into surface-connected compartments, and 2) causes human monocyte-macrophage foam cell formation.
Highlights
Much of the cholesterol that accumulates in atherosclerotic plaques is found within monocyte-macrophages transforming these cells into “foam cells.” Native low density lipoprotein (LDL) does not cause foam cell formation
When LDL was converted to liposomes did LDL induce substantial cholesterol accumulation in the macrophages
We showed that microcrystalline cholesterol and aggregated LDL enter surface-connected membrane bound compartments (SCC) that form in human monocytemacrophages during incubation with these lipid particles [22]
Summary
Much of the cholesterol that accumulates in atherosclerotic plaques is found within monocyte-macrophages transforming these cells into “foam cells.” Native low density lipoprotein (LDL) does not cause foam cell formation. The LDL liposomes induced and entered surface-connected compartments within the macrophages, a unique endocytic pathway in these cells that we call patocytosis. Cholesterol esterase-mediated transformation of LDL into cholesterol-rich liposomes is an LDL modification that: 1) stimulates uptake of LDL cholesterol by apoB-dependent endocytosis into surface-connected compartments, and 2) causes human monocyte-macrophage foam cell formation. We showed that LDL aggregated through vortexing or treatment with phospholipase C caused its uptake by a unique endocytic pathway in monocyte-macrophages [9]. These aggregated LDLs induced and entered a labyrinth of surface-connected membrane bound compartments (SCC) within the macrophage. We report that cholesterol esterase mediated conversion of LDL into liposomes is an LDL modification that stimulates patocytosis and foam cell formation
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