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Covalent Activation of the C‐type Lectin DC‐SIGN

  • Jonathan Lefèbre
  • , Maurice Besch
  • , Noémi Csorba
  • , Kristóf Garami
  • , Zoltán Orgován
  • , Gitta Schlosser
  • , Iris Bermejo
  • , Péter Ábrányi‐Balogh
  • , György M. Keserű (Corresponding author)
  • , Christoph Rademacher (Corresponding author)

Publications: Contribution to journalArticlePeer Reviewed

Abstract

Dendritic cell-specific intercellular adhesion molecule-3-grabbing non-integrin (DC-SIGN) is a C-type lectin receptor expressed on antigen-presenting cells, crucial for pathogen recognition and immune modulation. The shallow and polar carbohydrate binding site of DC-SIGN presents challenges for ligand design. Here, we explored covalent modification targeting specific lysine residues as a novel strategy to modulate DC-SIGN function. Screening a lysine-targeted electrophilic fragment library using orthogonal functional assays identified two potent activators. Structural analyses via NMR spectroscopy, mass spectrometry and computational modeling confirmed structural perturbations of the carbohydrate recognition domain (CRD) and revealed distinct mechanisms of activation. While both activators significantly enhanced DC-SIGN's affinity for monosaccharide ligands, one compound induced oligomerization via covalent coupling and non-covalent secondary site interactions, whereas the other selectively modified lysine K373 directly within the primary carbohydrate binding site. These findings demonstrate the potential of lysine-targeted covalent compounds as a novel therapeutic strategy for modulating DC-SIGN function and potentially C-type lectins in general.

Original languageEnglish
Article numbere20594
JournalAngewandte Chemie International Edition
Volume65
Issue number3
Early online date24 Nov 2025
DOIs
Publication statusPublished - 16 Jan 2026

Austrian Fields of Science 2012

  • 106002 Biochemistry
  • 106006 Biophysics
  • 104004 Chemical biology
  • 106041 Structural biology

Keywords

  • Lectins, C-Type/chemistry
  • Cell Adhesion Molecules/chemistry
  • Receptors, Cell Surface/chemistry
  • Humans
  • Binding Sites
  • Lysine/chemistry
  • Ligands

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