Abstract
Human monocyte-derived macrophages can efflux accumulated cholesterol without exogenously added cholesterol acceptors (Kruth, H. S., Skarlatos, S. I., Gaynor, P. M., and Gamble, W. (1994) J. Biol. Chem. 269, 24511-24518). Most of the effluxed cholesterol accumulates in the medium as apolipoprotein E-discoidal lipid particles. In the current study, we determined whether and to what degree cholesterol efflux from human monocyte-macrophages depended on apolipoprotein E secretion. Unexpectedly, 2-week-old differentiated monocyte-macrophages secreted similar amounts of apolipoprotein E without or with cholesterol enrichment. Apolipoprotein E mRNA levels in these macrophages were not increased by cholesterol enrichment and were comparable with levels in HepG2 cells. Without cholesterol enrichment, monocyte-macrophages secreted lipid-poor apolipoprotein E with a density >1.21 g/ml. By contrast, cholesterol enrichment of monocyte-macrophages induced the association of apoE with phospholipid and cholesterol to form discoidal particles that floated at densities of 1.08-1.10 g/ml. An anti-apolipoprotein E monoclonal antibody added to the culture medium significantly inhibited cholesterol and phospholipid efflux from the monocyte-macrophages. This showed that apolipoprotein E was required for most of the cholesterol efflux, and that apolipoprotein E did not leave macrophages with lipid but rather associated with lipid after it was secreted. Thus, 1) apolipoprotein E was constitutively secreted by differentiated human monocyte-macrophages, 2) apolipoprotein E only formed discoidal particles following macrophage cholesterol enrichment, 3) apolipoprotein E was necessary for cholesterol efflux to occur in the absence of added cholesterol acceptors and, in addition 4) the level of macrophage unesterified cholesterol was not rate-limiting for this cholesterol efflux, and 5) net phospholipid synthesis occurred in macrophages secondary to apoE-mediated loss of macrophage phospholipid. In conclusion, apolipoprotein E functions in an autocrine pathway that mediates cholesterol efflux from human monocyte-derived macrophages.
Highlights
Human monocyte-derived macrophages can efflux accumulated cholesterol without exogenously added cholesterol acceptors
We have observed that differentiated human monocyte-macrophages efflux accumulated cholesterol even when these macrophages are incubated in basal medium without any added serum components or high density lipoprotein (HDL) that could function as cholesterol acceptors [7]
Human monocyte-macrophages (2week-old cultures) incubated with acetylated low density lipoprotein (AcLDL) (100 g/ml) for 3 days showed no significant difference in their secretion of apoE compared with monocyte-macrophages that were not incubated with AcLDL (Table I)
Summary
Human monocyte-derived macrophages can efflux accumulated cholesterol without exogenously added cholesterol acceptors We have observed that differentiated human monocyte-macrophages efflux accumulated cholesterol even when these macrophages are incubated in basal medium without any added serum components or HDL that could function as cholesterol acceptors [7]. Most of this effluxed cholesterol accumulates in the medium within apoE-discoidal lipoprotein particles. It has not been determined whether and to what degree cholesterol efflux depends on apoE secretion by human monocyte-macrophages. The purpose of this study was 1) to determine the importance of apoE in mediating cholesterol efflux from these cells, and 2) to determine the relationship between apoE secretion and production of apoEdiscoidal particles
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