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Drug-like Inhibitors of DC-SIGN Based on a Quinolone Scaffold

Hengxi Zhang, Ondřej Daněk, Dmytro Makarov, S. Rádl, Dongyoon Kim, Jiří Ledvinka, Kristýna Vychodilová, Jan Hlaváč, Jonathan Lefèbre, Maxime Denis, Christoph Rademacher, Petra Ménová

2022ACS Medicinal Chemistry Letters17 citationsDOIOpen Access PDF

Abstract

DC-SIGN (dendritic cell-specific intercellular adhesion molecule-3-grabbing non-integrin) is a pattern recognition receptor expressed on immune cells and involved in the recognition of carbohydrate signatures present on various pathogens, including HIV, Ebola, and SARS-CoV-2. Therefore, developing inhibitors blocking the carbohydrate-binding site of DC-SIGN could generate a valuable tool to investigate the role of this receptor in several infectious diseases. Herein, we performed a fragment-based ligand design using 4-quinolone as a scaffold. We synthesized a library of 61 compounds, performed a screening against DC-SIGN using an STD reporter assay, and validated these data using protein-based 1H–15N HSQC NMR. Based on the structure–activity relationship data, we demonstrate that ethoxycarbonyl or dimethylaminocarbonyl in position 2 or 3 is favorable for the DC-SIGN binding activity, especially in combination with fluorine, ethoxycarbonyl, or dimethylaminocarbonyl in position 7 or 8. Furthermore, we demonstrate that these quinolones can allosterically modulate the carbohydrate binding site, which offers an alternative approach toward this challenging protein target.

Topics & Concepts

DC-SIGNHeteronuclear single quantum coherence spectroscopyDrug discoveryChemistryComputational biologyBinding siteScaffoldLigand (biochemistry)ReceptorBiochemistryCell biologyBiologyStereochemistryImmune systemDendritic cellTwo-dimensional nuclear magnetic resonance spectroscopyComputer scienceImmunologyDatabaseImmunotherapy and Immune ResponsesGlycosylation and Glycoproteins ResearchMonoclonal and Polyclonal Antibodies Research
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