Evidence for carbohydrate recognition and homotypic and heterotypic binding by the TIM family

doi:10.1093/intimm/dxm044

International Immunology Advance Access originally published online on May 19, 2007
International Immunology 2007 19(6):763-773; doi:10.1093/intimm/dxm044

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Evidence for carbohydrate recognition and homotypic and heterotypic binding by the TIM family

Peter R. Wilker¹, John R. Sedy¹, Vadim Grigura², Theresa L. Murphy¹ and Kenneth M. Murphy¹^,2

¹ Department of Pathology and Immunology
² Howard Hughes Medical Institute, Washington University School of Medicine, 660 South Euclid Avenue, St Louis, MO 63110, USA

Corresponding to: K. Murphy; E-mail: murphy{at}immunology.wustl.edu

The T cell Ig domain and mucin domain (TIM) proteins form aconserved family of transmembrane cell-surface glycoproteinsexpressed by a variety of tissues. Each TIM protein containsa single V-type Ig domain, a glycosylated mucin-like domain,a transmembrane domain and a cytoplasmic domain. TIM proteinsrecognize a diverse array of ligands, including H-ferritin,galectin-9 as well as other TIM family members. In this study,we demonstrate that the Ig domains of murine TIM-1, -3 and -4display calcium-dependent binding to ligands expressed by murinesplenocytes and several non-murine cell lines, indicating non-species-specificligand recognition. Further, the intrafamilial interaction ofvarious TIM family Ig domains with surface-expressed TIM-1 andTIM-4 requires an intact TIM-1 and TIM-4 glycosylated mucinstalk. Importantly, we also uncovered the previously unrecognizedpotential for homotypic TIM interactions in forming ligand–receptorpairs. Using a glycan array screen, we identified the novelcapacity of the TIM-3 Ig domain to recognize specific carbohydratemoieties, suggesting a role for carbohydrate modification alongwith protein epitopes in TIM ligand recognition. Identificationof the carbohydrate-binding capacity of TIM proteins helps explainthe diversity of ligands recognized by this family and addsto our understanding of homotypic and heterotypic interactionsbetween TIM family members.

Keywords: ligands, tetramers, T lymphocytes

Transmitting editor: J. P. Allison

Received 3 October 2006, accepted 20 March 2007.

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