Abstract
Plasma cholesteryl ester transfer protein (CETP) mediates the transfer of cholesteryl esters (CE) between lipoproteins and was reported to also directly mediate the uptake of high density lipoprotein (HDL) CE by human Hep G2 cells and fibroblasts. The present study investigates that uptake and its relationship to a pathway for "selective uptake" of HDL CE that does not require CETP. HDL3 labeled in both the CE and apoprotein moieties was incubated with Hep G2 cells. During 4-h incubations, CE tracer was selectively taken up from doubly labeled HDL3 in excess of apoA-I tracer, and added CETP did not modify that uptake. However, during 18-20-h incubations, CETP stimulated the uptake of CE tracer more than 4-fold without modifying the uptake of apoA-I tracer. This suggested that secreted products, perhaps lipoproteins, might be required for the CETP effect. Four inhibitors of lipoprotein uptake via low density lipoprotein (LDL) receptors (heparin, monensin, an antibody against the LDL receptor, and antibodies against the receptor binding domains of apoB and apoE) effectively blocked the CETP stimulation of CE tracer uptake. Heparin caused an increase in CE tracer in a d less than 1.063 g/ml fraction of the medium that more than accounted for the heparin blockade of CETP-stimulated CE uptake. CETP did not affect the uptake of doubly labeled HDL3 by human fibroblasts, even at twice plasma levels of activity, and heparin did not modify uptake of HDL3 tracers. Thus the CETP effect on Hep G2 cells can be accounted for by transfer of HDL CE to secreted lipoproteins which are then retaken up, and there is no evidence for a direct effect of CETP on cellular uptake of HDL CE.
Highlights
HDL3labeled in boththe cholesteryl esters (CE) and apoprotein moieties was incubated with Hep G2 cells
The in CE tracer ina d < 1.063 g/ml fraction of the medium conclusion was reached that CETPcan directly interact with that more than accounted for the heparinblockade of cells to deliver high density lipoprotein (HDL) cholesteryl esters to them, it CETP-stimulated CE uptake
The CETP effect on Hep G2 cells can be accounted for by transfer of HDL CEto secreted lipoproteins which are retaken up, and there is no evi-. We have studied another nonendocytotic mechanism by which cells take up HDL cholesteryl esters without HDL particle uptake (4-6)
Summary
Effect on HDL Uptake (6), the difference between total [3H]CEtuptake and “‘1-NMTCapoA-I uptake is taken to represent selective uptake of [3H]CEt, which is expressed in termsof apparent HDL3 particle uptake. Tracer released during the chase incubation andthe subsequent trypsin treatment are summed and designated “reversibly cell-associated HDL3” (12). This too is expressed as apparent cell association of HDL3particles, expressed in terms of HDL3 protein. Data areexpressed as means & S.D. The significance of differences was examined using the Student’s t test for paired data where indicated and for unpaired data in all other cases
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