Literature DB >> 17984090

A novel mechanism for LSECtin binding to Ebola virus surface glycoprotein through truncated glycans.

Alex S Powlesland1, Tanja Fisch, Maureen E Taylor, David F Smith, Bérangère Tissot, Anne Dell, Stefan Pöhlmann, Kurt Drickamer.   

Abstract

LSECtin is a member of the C-type lectin family of glycan-binding receptors that is expressed on sinusoidal endothelial cells of the liver and lymph nodes. To compare the sugar and pathogen binding properties of LSECtin with those of related but more extensively characterized receptors, such as DC-SIGN, a soluble fragment of LSECtin consisting of the C-terminal carbohydrate-recognition domain has been expressed in bacteria. A biotin-tagged version of the protein was also generated and complexed with streptavidin to create tetramers. These forms of the carbohydrate-recognition domain were used to probe a glycan array and to characterize binding to oligosaccharide and glycoprotein ligands. LSECtin binds with high selectivity to glycoproteins terminating in GlcNAcbeta1-2Man. The inhibition constant for this disaccharide is 3.5 microm, making it one of the best low molecular weight ligands known for any C-type lectin. As a result of the selective binding of this disaccharide unit, the receptor recognizes glycoproteins with a truncated complex and hybrid N-linked glycans on glycoproteins. Glycan analysis of the surface glycoprotein of Ebola virus reveals the presence of such truncated glycans, explaining the ability of LSECtin to facilitate infection by Ebola virus. High mannose glycans are also present on the viral glycoprotein, which explains why DC-SIGN also binds to this virus. Thus, multiple receptors interact with surface glycoproteins of enveloped viruses that bear different types of relatively poorly processed glycans.

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Year:  2007        PMID: 17984090      PMCID: PMC2275798          DOI: 10.1074/jbc.M706292200

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  47 in total

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4.  Mechanism of N-acetylgalactosamine binding to a C-type animal lectin carbohydrate-recognition domain.

Authors:  A R Kolatkar; A K Leung; R Isecke; R Brossmer; K Drickamer; W I Weis
Journal:  J Biol Chem       Date:  1998-07-31       Impact factor: 5.157

5.  Mannose receptor-mediated regulation of serum glycoprotein homeostasis.

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6.  Characterization of carbohydrate recognition by langerin, a C-type lectin of Langerhans cells.

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7.  Identification of amino acid residues that determine pH dependence of ligand binding to the asialoglycoprotein receptor during endocytosis.

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8.  Covalent modifications of the ebola virus glycoprotein.

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10.  DC-SIGN and DC-SIGNR bind ebola glycoproteins and enhance infection of macrophages and endothelial cells.

Authors:  Graham Simmons; Jacqueline D Reeves; Case C Grogan; Luk H Vandenberghe; Frédéric Baribaud; J Charles Whitbeck; Emily Burke; Michael J Buchmeier; Elizabeth J Soilleux; James L Riley; Robert W Doms; Paul Bates; Stefan Pöhlmann
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  51 in total

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2.  Different potential of C-type lectin-mediated entry between Marburg virus strains.

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3.  Protein domain histochemistry (PDH): binding of the carbohydrate recognition domain (CRD) of recombinant human glycoreceptor CLEC10A (CD301) to formalin-fixed, paraffin-embedded breast cancer tissues.

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Review 4.  Filovirus entry.

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6.  Identification of cell surface molecules involved in dystroglycan-independent Lassa virus cell entry.

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7.  The primed ebolavirus glycoprotein (19-kilodalton GP1,2): sequence and residues critical for host cell binding.

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8.  Trimeric structure of langerin.

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Journal:  J Biol Chem       Date:  2010-02-24       Impact factor: 5.157

9.  An Ebola Virus-Like Particle-Based Reporter System Enables Evaluation of Antiviral Drugs In Vivo under Non-Biosafety Level 4 Conditions.

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Review 10.  Structural insights into what glycan arrays tell us about how glycan-binding proteins interact with their ligands.

Authors:  Maureen E Taylor; Kurt Drickamer
Journal:  Glycobiology       Date:  2009-06-15       Impact factor: 4.313

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