Targeting undruggable carbohydrate recognition sites through focused fragment library design

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Shanina, Elena | Kuhaudomlarp, Sakonwan | Siebs, Eike | Fuchsberger, Felix | Denis, Maxime | da Silva Figueiredo Celestino Gomes, Priscila | Clausen, Mads | Seeberger, Peter | Rognan, Didier | Titz, Alexander | Imberty, Anne | Rademacher, Christoph

Edité par CCSD ; Nature Research -

International audience. Carbohydrate-protein interactions are key for cell-cell and host-pathogen recognition and thus, emerged as viable therapeutic targets. However, their hydrophilic nature poses major limitations to the conventional development of drug-like inhibitors. To address this shortcoming, four fragment libraries were screened to identify metal-binding pharmacophores (MBPs) as novel scaffolds for inhibition of Ca 2+ -dependent carbohydrate-protein interactions. Here, we show the effect of MBPs on the clinically relevant lectins DC-SIGN, Langerin, LecA and LecB. Detailed structural and biochemical investigations revealed the specificity of MBPs for different Ca 2+ -dependent lectins. Exploring the structure-activity relationships of several fragments uncovered the functional groups in the MBPs suitable for modification to further improve lectin binding and selectivity. Selected inhibitors bound efficiently to DC-SIGN-expressing cells. Altogether, the discovery of MBPs as a promising class of Ca 2+ -dependent lectin inhibitors creates a foundation for fragment-based ligand design for future drug discovery campaigns.

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