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Intracellular trafficking of recycling apolipoprotein E in Chinese hamster ovary cells
Authors:Braun Nicole A  Mohler Peter J  Weisgraber Karl H  Hasty Alyssa H  Linton MacRae F  Yancey Patricia G  Su Yan Ru  Fazio Sergio  Swift Larry L
Affiliation:Department of Pathology, Vanderbilt University School of Medicine, Nashville, TN 37232, USA.
Abstract:We have investigated apolipoprotein E (apoE) recycling in Chinese hamster ovary (CHO) cells, a peripheral cell that does not produce lipoproteins or express apoE. Using a pulse-chase protocol in which cells were pulsed with 125I-apoE-VLDL and chased for different periods, approximately 30% of the apoE internalized during the pulse was resecreted within a 4 h chase in a relatively lipid-free state. The addition of lysosomotropic agents or brefeldin A had no effect on apoE recycling. Unlike previous results with hepatocytes and macrophages, neither apoA-I nor upregulation of ABCA1 stimulated apoE recycling. However, cyclodextrin, which extracts cholesterol from plasma membrane lipid rafts, increased recycling. Confocal studies revealed that apoE, internalized during a 1 h pulse, colocalizes with early endosomal antigen-1, Rab5, Rab11a, and lysobisphosphatidic acid but not with lysosomal-associated membrane protein-1. Colocalization of apoE and Rab11a persisted even after cells had been chased for 1 h, suggesting a pool of apoE within the endosomal recycling compartment (ERC). Our data suggest that apoE recycling in CHO cells is linked to cellular cholesterol removal via the ERC and phospholipid-containing acceptors in a pathway alternative to the ABCA1-apoA-I axis.
Keywords:cholesterol efflux  recycling endosomes  Rab5  Rab11a  early endosomes  β-cyclodextrin  ATP binding cassette transporter A1
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