Drug Repurposing of FDA Compounds against α-Glucosidase for the Treatment of Type 2 Diabetes: Insights from Molecular Docking and Molecular Dynamics Simulations

Rebwar Saeed M. Rashid; Selin Temurlu; Arwa Abourajab; Pelin Karsili; Meltem Dinleyici; Basma Al-Khateeb; Huriye Icil

doi:10.3390/ph16040555

Pharmaceuticals (Apr 2023)

Drug Repurposing of FDA Compounds against α-Glucosidase for the Treatment of Type 2 Diabetes: Insights from Molecular Docking and Molecular Dynamics Simulations

Rebwar Saeed M. Rashid,
Selin Temurlu,
Arwa Abourajab,
Pelin Karsili,
Meltem Dinleyici,
Basma Al-Khateeb,
Huriye Icil

Affiliations

Rebwar Saeed M. Rashid: Department of Chemistry, Faculty of Arts and Science, Eastern Mediterranean University, Famagusta 99628, Northern Cyprus, Mersin 10, Turkey
Selin Temurlu: Department of Chemistry, Faculty of Arts and Science, Eastern Mediterranean University, Famagusta 99628, Northern Cyprus, Mersin 10, Turkey
Arwa Abourajab: Department of Chemistry, Faculty of Arts and Science, Eastern Mediterranean University, Famagusta 99628, Northern Cyprus, Mersin 10, Turkey
Pelin Karsili: Department of Chemistry, Faculty of Arts and Science, Eastern Mediterranean University, Famagusta 99628, Northern Cyprus, Mersin 10, Turkey
Meltem Dinleyici: Department of Chemistry, Faculty of Arts and Science, Eastern Mediterranean University, Famagusta 99628, Northern Cyprus, Mersin 10, Turkey
Basma Al-Khateeb: Department of Chemistry, Faculty of Arts and Science, Eastern Mediterranean University, Famagusta 99628, Northern Cyprus, Mersin 10, Turkey
Huriye Icil: Department of Chemistry, Faculty of Arts and Science, Eastern Mediterranean University, Famagusta 99628, Northern Cyprus, Mersin 10, Turkey

DOI: https://doi.org/10.3390/ph16040555
Journal volume & issue: Vol. 16, no. 4
p. 555

Abstract

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Type 2 diabetes mellitus is a chronic health problem that can be controlled by slowing one’s carbohydrate metabolism by inhibiting α-glucosidase, an enzyme responsible for carbohydrate degradation. Currently, drugs for type 2 diabetes have limitations in terms of safety, efficiency, and potency, while cases are rapidly increasing. For this reason, the study planned and moved towards drug repurposing by utilizing food and drug administration (FDA)-approved drugs against α-glucosidase, and investigated the molecular mechanisms. The target protein was refined and optimized by introducing missing residues, and minimized to remove clashes to find the potential inhibitor against α-glucosidase. The most active compounds were selected after the docking study to generate a pharmacophore query for the virtual screening of FDA-approved drug molecules based on shape similarity. The analysis was performed using Autodock Vina (ADV)—based on binding affinities (−8.8 kcal/mol and −8.6 kcal/mol) and root-mean-square-deviation (RMSD) values (0.4 Å and 0.6 Å). Two of the most potent lead compounds were selected for a molecular dynamics (MD) simulation to determine the stability and specific interactions between receptor and ligand. The docking score, RMSD values, pharmacophore studies, and MD simulations revealed that two compounds, namely Trabectedin (ZINC000150338708) and Demeclocycline (ZINC000100036924), are potential inhibitors for α-glucosidase compared to standard inhibitors. These predictions showed that the FDA-approved molecules Trabectedin and Demeclocycline are potential suitable candidates for repurposing against type 2 diabetes. The in vitro studies showed that trabectedin was significantly effective with an IC50 of 1.263 ± 0.7 μM. Further investigation in the laboratory is needed to justify the safety of the drug to be used in vivo.

Published in Pharmaceuticals

ISSN: 1424-8247 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Medicine: Pharmacy and materia medica
Website: http://www.mdpi.com/journal/pharmaceuticals/

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