Structure-based virtual screening of unbiased and RNA-focused libraries to identify new ligands for the HCV IRES model system

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structurebased_virtual_screen-20250109100351715.pdf (1.37 MB)

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2024

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CC-BY-4.0
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Item type: Item , ZeitschriftenaufsatzAccess status: Open Access ,

Abstract

Targeting RNA including viral RNAs with small molecules is an emerging field. The hepatitis C virus internal ribosome entry site (HCV IRES) is a potential target for translation inhibitor development to raise drug resistance mutation preparedness. Using RNA-focused and unbiased molecule libraries, a structure-based virtual screening (VS) by molecular docking and pharmacophore analysis was performed against the HCV IRES subdomain IIa. VS hits were validated by a microscale thermophoresis (MST) binding assay and a Förster resonance energy transfer (FRET) assay elucidating ligand-induced conformational changes. Ten hit molecules were identified with potencies in the high to medium micromolar range proving the suitability of structure-based virtual screenings against RNA-targets. Hit compounds from a 2-guanidino-quinazoline series, like the strongest binder, compound 8b with an EC50 of 61 μM, show low molecular weight, moderate lipophilicity and reduced basicity compared to previously reported IRES ligands. There

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http://doi.org/10.25358/openscience-11203

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https://openscience.ub.uni-mainz.de/handle/20.500.12030/11224

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RSC medicinal chemistry, 15, Royal Society of Chemistry, Cambridge, 2024, https://doi.org/10.1039/d3md00696d

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