4.6 Article

Multiple modes of binding enhance the affinity of DC-SIGN for high mannose N-linked glycans found on viral glycoproteins

Journal

JOURNAL OF BIOLOGICAL CHEMISTRY
Volume 282, Issue 6, Pages 4202-4209

Publisher

AMER SOC BIOCHEMISTRY MOLECULAR BIOLOGY INC
DOI: 10.1074/jbc.M609689200

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Funding

  1. NIGMS NIH HHS [GM50569] Funding Source: Medline
  2. Wellcome Trust [075565] Funding Source: Medline

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The dendritic cell surface receptor DC-SIGN and the closely related endothelial cell receptor DC-SIGNR specifically recognize high mannose N-linked carbohydrates on viral pathogens. Previous studies have shown that these receptors bind the outer trimannose branch Man alpha 1-3[Manal-6]Man alpha present in high mannose structures. Although the trimannoside binds to DC-SIGN or DC-SIGNR more strongly than mannose, additional affinity enhancements are observed in the presence of one or more Man alpha 1-2Man alpha moieties on the nonreducing termini of oligomannose structures. The molecular basis of this enhancement has been investigated by determining crystal structures of DC-SIGN bound to a synthetic six-mannose fragment of a high mannose N-linked oligosaccharide, Man alpha 1-2Man alpha 1-3[Man alpha 1-2Man alpha 1-6]Man alpha-6Man and to the disaccharide Man alpha 1-2Man. The structures reveal mixtures of two binding modes in each case. Each mode features typical C-type lectin binding at the principal Ca2+-binding site by one mannose residue. In addition, other sugar residues form contacts unique to each binding mode. These results suggest that the affinity enhancement displayed toward oligosaccharides decorated with the Mana1-2Mana structure is due in part to multiple binding modes at the primary Ca 21 site, which provide both additional contacts and a statistical (entropic) enhancement of binding.

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