Complex N-glycans are the major ligands for galectin-1, -3, and -8 on Chinese hamster ovary cells

doi:10.1093/glycob/cwj063

Glycobiology Advance Access originally published online on November 29, 2005
Glycobiology 2006 16(4):305-317; doi:10.1093/glycob/cwj063

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Complex N-glycans are the major ligands for galectin-1, -3, and -8 on Chinese hamster ovary cells

Santosh Kumar Patnaik², Barry Potvin², Susanne Carlsson³, David Sturm², Hakon Leffler³ and Pamela Stanley¹^,2

² Department of Cell Biology, Albert Einstein College of Medicine, New York, NY 10461; and ³ Section MIG (Microbiology, Immunology, Glycobiology), Institute of Laboratory Medicine, Lund University, PO Box 124, SE-221 00, Lund, Sweden

¹ To whom correspondence should be addressed; e-mail: stanley{at}aecom.yu.edu

Received on August 18, 2005; revised on November 10, 2005; accepted on November 15, 2005

Galectins are implicated in a large variety of biological functions,many of which depend on their carbohydrate-binding ability.Fifteen members of the family have been identified in vertebratesbased on binding to galactose (Gal) that is mediated by oneor two, evolutionarily conserved, carbohydrate-recognition domains(CRDs). Variations in glycan structures expressed on glycoconjugatesat the cell surface may, therefore, affect galectin bindingand functions. To identify roles for different glycans in thebinding of the three types of mammalian galectins to cells,we performed fluorescence cytometry at 4deg;C with recombinantrat galectin-1, human galectin-3, and three forms of human galectin-8,to Chinese hamster ovary (CHO) cells and 12 different CHO glycosylationmutants. All galectin species bound to parent CHO cells andbinding was inhibited >90% by 0.2 M lactose. Galectin-8 isoformswith either a long or a short inter-CRD linker bound similarlyto CHO cells. However, a truncated form of galectin-8 containingonly the N-terminal CRD bound only weakly to CHO cells and theC-terminal galectin-8 CRD exhibited extremely low binding. Bindingof the galectins to the different CHO glycosylation mutantsrevealed that complex N-glycans are the major ligands for eachgalectin except the N-terminal CRD of galectins-8, and alsoidentified some fine differences in glycan recognition. Interestingly,increased binding of galectin-1 at 4deg;C correlated with increasedpropidium iodide (PI) uptake, whereas galectin-3 or -8 bindingdid not induce permeability to PI. The CHO glycosylation mutantswith various repertoires of cell surface glycans are a usefultool for investigating galectin–cell interactions as theypresent complex and simple glycans in a natural mixture of multivalentprotein and lipid glycoconjugates anchored in a cell membrane.

Key words: CHO / galectin / glycan recognition / glycosylation mutants / lectin

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