Scavenger receptor class B type I localizes to a late endosomal compartment

Malika Ahras, Thet Naing and Ruth McPherson¹

Division of Cardiology, University of Ottawa Heart Institute, Ottawa, Canada K1Y 4W7

These studies were supported by a grant from the Canadian Institutesfor Health Research (CIHR) (to R.M.).

Published, JLR Papers in Press, March 29, 2008.

^¹ To whom correspondence should be addressed. e-mail: rmcpherson{at}ottawaheart.ca

Scavenger receptor class B type I (SR-BI) has an establishedrole in mediating the selective uptake of cholesterol from HDLin hepatocytes, steroidogenic cells, and other tissues. SR-BIis present on the plasma membrane but also localizes to stableintracellular compartments of unknown function. Using indirectimmunofluorescence and subcellular fractionation, we have investigatedthe subcellular distribution of SR-BI. We report that red fluorescentprotein-tagged mouse SR-BI (RFP-mSR-BI) colocalizes with thelate endosomal and lysosomal markers, Rab7, LBPA, and Rab9.In addition, endogenous SR-BI is also found on lysosomes andcolocalizes with LAMP-2 in primary hepatocytes. Furthermore,we demonstrate that the trafficking of SR-BI through these compartmentsis Rab7 dependent. Interestingly, filipin staining indicatesaccumulation of lysosomal cholesterol in SR-BI-deficient (^–/–)as compared with wild-type hepatocytes. In addition to its roleas a plasma membrane receptor, SR-BI may function in cholesteroltrafficking from late endosomes/lysosomes.

Supplementary key words cholesterol • selective uptake • late endosomes • lysosomes • intracellular trafficking

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