Litcius/Paper detail

Potential repurposing of four FDA approved compounds with antiplasmodial activity identified through proteome scale computational drug discovery and in vitro assay

Bakary N’tji Diallo, Tarryn Swart, Heinrich C. Hoppe, Özlem Taştan Bishop, Kevin A. Lobb

2021Scientific Reports23 citationsDOIOpen Access PDF

Abstract

Abstract Malaria elimination can benefit from time and cost-efficient approaches for antimalarials such as drug repurposing. In this work, 796 DrugBank compounds were screened against 36 Plasmodium falciparum targets using QuickVina-W. Hits were selected after rescoring using GRaph Interaction Matching (GRIM) and ligand efficiency metrics: surface efficiency index (SEI), binding efficiency index (BEI) and lipophilic efficiency (LipE). They were further evaluated in Molecular dynamics (MD). Twenty-five protein–ligand complexes were finally retained from the 28,656 (36 × 796) dockings. Hit GRIM scores (0.58 to 0.78) showed their molecular interaction similarity to co-crystallized ligands. Minimum LipE (3), SEI (23) and BEI (7) were in at least acceptable thresholds for hits. Binding energies ranged from −6 to −11 kcal/mol. Ligands showed stability in MD simulation with good hydrogen bonding and favorable protein–ligand interactions energy (the poorest being −140.12 kcal/mol). In vitro testing showed 4 active compounds with two having IC 50 values in the single-digit μM range.

Topics & Concepts

DrugBankRepurposingDrug repositioningComputational biologyLigand (biochemistry)Drug discoveryLigand efficiencyChemistryIn vitroQuantitative structure–activity relationshipProteomeDrugPharmacologyStereochemistryBiologyBiochemistryReceptorEcologyComputational Drug Discovery MethodsMalaria Research and ControlProtein Structure and Dynamics