Publication | Open Access
Human apolipoprotein A-IV binds to apolipoprotein A-I/A-II receptor sites and promotes cholesterol efflux from adipose cells.
214
Citations
36
References
1990
Year
Lipid BiophysicsHyperlipidemiaCholesterol RemovalLipid MovementCellular PhysiologyMolecular PharmacologyMetabolic SyndromeAtherosclerosisCell SignalingDyslipidemiaLipid DisorderHealth SciencesMolecular PhysiologyBiochemistryAdipose CellsMembrane BiologyLipidsPharmacologyA-i/a-ii Receptor SitesA-iv BindsSignal TransductionPhysiologyCholesterol EffluxLipoprotein MetabolismCellular BiochemistryLipid ChemistryMedicineLipid Synthesis
Cholesterol efflux was studied in cultured mouse adipose cells after preloading with low density lipoprotein cholesterol. Exposure to complexes containing human apolipoprotein A-IV and L-alpha-dimyristoylphosphatidylcholine (DMPC) as well as to human lipoprotein particles containing apolipoprotein A-IV but not apolipoprotein A-I and particles containing apolipoproteins A-IV and A-I showed that both artificial and native apolipoprotein A-IV-containing particles were able to promote cholesterol efflux at 37 degrees C as a function of time and concentration. The half-maximal concentration was found to be 0.3 X 10(-6) M for apolipoprotein A-IV.DMPC complexes. Binding experiments performed in intact cells at 4 degrees C with labeled apolipoprotein A-IV.DMPC complexes showed the existence of specific binding sites, with a Kd value of 0.32 x 10(-6) M and a maximal binding capacity of 223,000 sites/cell. By cross-competition experiments with labeled and unlabeled complexes containing apolipoprotein A-IV, A-I, or A-II, it appeared that all three apolipoproteins bind to the same cell-surface recognition sites. It is suggested that apolipoprotein A-IV, which is present in the interstitial fluid surrounding adipose cells in vivo at concentrations similar to those required in vitro for the promotion of cholesterol efflux, plays a critical role in cholesterol removal from peripheral cells.
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