The ligand-binding profile of HARE: hyaluronan and chondroitin sulfates A, C, and D bind to overlapping sites distinct from the sites for heparin, acetylated low-density lipoprotein, dermatan sulfate, and CS-E

doi:10.1093/glycob/cwn045

Glycobiology Advance Access originally published online on May 22, 2008
Glycobiology 2008 18(8):638-648; doi:10.1093/glycob/cwn045

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The ligand-binding profile of HARE: hyaluronan and chondroitin sulfates A, C, and D bind to overlapping sites distinct from the sites for heparin, acetylated low-density lipoprotein, dermatan sulfate, and CS-E

Edward N. Harris and Paul H. Weigel¹

Department of Biochemistry and Molecular Biology and The Oklahoma Center for Medical Glycobiology, University of Oklahoma Health Sciences Center, Oklahoma City, OK 73190, USA

¹ To whom correspondence should be addressed: Tel: +1-405-271-1288; Fax: +1-405-271-3092; e-mail: paul-weigel{at}ouhsc.edu

Received on April 11, 2008; revised on May 16, 2008; accepted on May 18, 2008

The hyaluronic acid receptor for endocytosis (HARE)/ Stabilin-2is the primary systemic scavenger receptor for hyaluronan (HA),the chondroitin sulfates (CS), dermatan sulfate (DS), and nonglycosaminoglycan(GAG) ligands such as acetylated low-density lipoprotein (AcLDL),pro-collagen propeptides, and advanced glycation end products.We recently discovered that HARE is also a systemic scavengerreceptor for heparin (Hep) (Harris EN, Weigel JA, Weigel PH.2008. The human hyaluronan receptor for endocytosis [HARE/Stabilin-2]is a systemic clearance receptor for heparin. J Biol Chem. 283:17341–17350).Our goal was to map the binding sites of eight different ligandswithin HARE. We used biotinylated GAGs and radio-iodinated streptavidinor AcLDL to assess the binding activities of ligands directlyor indirectly (by competition with unlabeled ligands) in endocytosisassays using stable cell lines expressing the 315 or 190 kDaHA receptor for endocytosis (315- or 190-HARE) isoforms, andELISA-like assays, with purified recombinant soluble 190-HAREecto-domain. For example, Hep binding to HARE was competed byDS, CS-E, AcLDL, and dextran sulfate, but not by other CS types,HA, dextran, or heparosan. ¹²⁵I-AcLDL binding to HARE was partiallycompeted by Hep and dextran sulfate, but not competed by HA.Two ligands, DS and CS-E, competed with both Hep and HA to somedegree. Hep and HA binding or endocytosis is mutually inclusive;binding of these two GAGs occurs with functionally separate,noncompetitive, and apparently noninteracting domains. Thus,HARE binds to HA and Hep simultaneously. Although the domain(s)responsible for Hep binding remains unknown, the Link domainwas required for HARE binding to HA, CS-A, CS-C, and CS-D. Theseresults enable us to outline, for the first time, a bindingactivity map for multiple ligands of HARE.

Key words: chondroitin sulfate / endocytosis / glycosaminoglycan turnover / heparin / Stabilin-2

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