Mannose 6-phosphate receptors, Niemann-Pick C2 protein, and lysosomal cholesterol accumulation

doi:10.1194/jlr.M500131-JLR200

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Mannose 6-phosphate receptors, Niemann-Pick C2 protein, and lysosomal cholesterol accumulation

Marion Willenborg^*, Christine Kathrin Schmidt^*, Peter Braun, Jobst Landgrebe, Kurt von Figura, Paul Saftig¹^,* and Eeva-Liisa Eskelinen¹^,2^,*^,

^* Institute of Biochemistry, University of Kiel, D-24098 Kiel, Germany
Institute of Biochemistry 2, University of Göttingen, D-37075 Göttingen, Germany
Division of Biochemistry, Department of Biological and Environmental Sciences, FI-00014 University of Helsinki, Helsinki, Finland

Published, JLR Papers in Press, September 21, 2005. DOI 10.1194/jlr.M500131-JLR200

^¹ P. Saftig and E-L. Eskelinen contributed equally to this work.

^² To whom correspondence should be addressed. e-mail Eeva-Liisa.Eskelinen{at}Helsinki.Fi

Niemann-Pick disease type C (NPC), caused by mutations in theNPC1 gene or the NPC2 gene, is characterized by the accumulationof unesterified cholesterol and other lipids in endo/lysosomalcompartments. NPC2 is a small, soluble, lysosomal protein thatis targeted to this compartment via a mannose 6-phosphate-inhibitablepathway. To obtain insight into the roles of mannose 6-phosphatereceptors (MPRs) in NPC2 targeting, we here examine the traffickingand function of NPC2 in fibroblast lines deficient in one orboth of the two MPRs, MPR46 and MPR300. We demonstrate thateither MPR alone is sufficient to transport NPC2 to the endo/lysosomalcompartment, although MPR300 seems to be more efficient thanMPR46. In the absence of both MPRs, NPC2 is secreted into theculture medium, and only a small amount of intracellular NPC2can be detected, mainly in the endoplasmic reticulum. This leadsto massive accumulation of unesterified cholesterol in the endo/lysosomalcompartment of the MPR46/300-deficient fibroblasts, a phenotypesimilar to that of the NPC patient fibroblasts. In addition,we observed an upregulation of NPC1 protein and mRNA in theMPR-double-deficient cells.

Taken together, our results suggest that the lysosomal targetingof NPC2 is strictly dependent on MPRs in fibroblasts.

Abbreviations: BMP, bis(monoacylglycero)phosphate; endo H, endoglycosidase H; ER, endoplasmic reticulum; MEF, mouse embryonic fibroblast; MPR, mannose 6-phosphate receptor; NPC, Niemann-Pick type C; PNGase F, peptide N-glycosidase F; TGN, trans Golgi network

Supplementary key words NPC1 • NPC2 • cholesterol • late endosome

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