CELLULAR CHOLESTEROL EFFLUX MEDIATED BY CYCLODEXTRINS

被引:717
作者
KILSDONK, EPC
YANCEY, PG
STOUDT, GW
BANGERTER, FW
JOHNSON, WJ
PHILLIPS, MC
ROTHBLAT, GH
机构
[1] MED COLL PENN,DEPT BIOCHEM,PHILADELPHIA,PA 19129
[2] HAHNEMANN UNIV,PHILADELPHIA,PA 19129
[3] PFIZER INC,CENT RES,GROTON,CT 06340
关键词
D O I
10.1074/jbc.270.29.17250
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
In this study, we compared cholesterol efflux mediated by either high density lipoproteins (HDL(3)) or beta-cyclodextrins, cyclic oligosaccharides that are able to dis solve lipids in their hydrophobic core. beta-Cyclodextrin, 2-hydroxypropyl-beta-cyclodextrin, and methyl-beta-cyclodextrin at 10 mM induced the release of 50-90% of L-cell [H-3]cholesterol after 8 h of incubation, with a major portion of this cholesterol being released in the first 1-2 h of incubation. The cholesterol efflux kinetics are different if cells are incubated with HDL(3), which induces a relatively constant rate of release of cholesterol throughout an 8-h incubation. Cholesterol efflux to cyclodextrins was much greater than phospholipid release. To test the hypothesis that maximal efflux rate constants for a particular cell are independent of the type of acceptor, we estimated the maximal rate constants for efflux (V-max) of cellular cholesterol from L-cells, Fu5AH cells, and GM3468A fibroblasts. The rate constant for HDL(3)-mediated efflux varied among cell lines in the order Fu5AH > L-cells > fibroblasts. However, these differences were not evident when cyclodextrins were used as cholesterol accepters. The estimated V-max values for cyclodextrin-mediated efflux were 3.5-70-fold greater than for HDL(3) for the three cell lines. The very high efficiency of cyclodextrins in stimulating cell cholesterol efflux suggests that these compounds can be used in two general ways for studies of atherosclerosis: 1) as research tools to probe mechanisms of cholesterol transport and aspects of membrane structure or 2) as potential pharmacological agents that could modify in vivo cholesterol metabolism and influence the development of the atherosclerotic plaque.
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收藏
页码:17250 / 17256
页数:7
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