Anti-hepatitis-C virus activity and QSAR study of certain thiazolidinone and thiazolotriazine derivatives as potential NS5B polymerase inhibitors

Ghaneya S Hassan; Hanan H Georgey; Esraa Z Mohammed; Farghaly A Omar

doi:10.1016/j.ejmech.2019.111747

Anti-hepatitis-C virus activity and QSAR study of certain thiazolidinone and thiazolotriazine derivatives as potential NS5B polymerase inhibitors

Eur J Med Chem. 2019 Dec 15:184:111747. doi: 10.1016/j.ejmech.2019.111747. Epub 2019 Oct 1.

Authors

Ghaneya S Hassan¹, Hanan H Georgey², Esraa Z Mohammed³, Farghaly A Omar³

Affiliations

¹ Pharmaceutical Chemistry Department, Faculty of Pharmacy, Cairo University, Cairo, 11562, Egypt; Pharmaceutical Chemistry Department, Faculty of Pharmacy, Badr University, Cairo, 11829, Egypt.
² Pharmaceutical Chemistry Department, Faculty of Pharmacy, Cairo University, Cairo, 11562, Egypt. Electronic address: hanan.hana@pharma.cu.edu.eg.
³ Pharmaceutical Chemistry Department, Faculty of Pharmacy, October 6 University, Giza, 12585, Egypt.

PMID: 31604164
DOI: 10.1016/j.ejmech.2019.111747

Abstract

The present study reports on evaluation of anti-HCV activity and QSAR of certain arylidenethiazolidinone derivatives as potential inhibitors of HCV-NS5B polymerase. The pursued compounds involving, 5-aryliden-3-arylacetamidothiazolidin-2,4-diones 4-6(a-f), 5-arylidine-2-(N-arylacetamido)-iminothiazolidin-4-one (10) and their rigid counterparts 5-arylidinethiazolotriazines 13-15(a-f), were synthesized and their structures confirmed by spectral and elemental analyses. The results of NS5B polymerase inhibition assay revealed compound 4e, as the most active inhibitor (IC₅₀ = 0.035 μM), which is four folds greater than that of the reference agent, VCH-759, (IC₅₀ = 0.14 μM). Meanwhile, compounds 4b, 4c, 5a, and 5c, and 13b, 14e and 15c displayed equipotency to 2 folds higher activity than VCH-759 (IC₅₀ values: 0.085, 0.14, 0.14, 0.10, 0.12, 0.09 and 0.07 μM, respectively). Assessment of the anti-HCV activity (GT1a) using human hepatoma cell line (Huh-7.5) illustrates superior activity of 4e (EC₅₀ = 3.80 μM) relative to VCH-759 (EC₅₀ = 5.29 μM). Cytotoxicity evaluation on, Transformed normal cell lines (Human Liver Epithelial-2, THLE-2 and Proximal Tubular Epithelial, RPTEC/TERT1), demonstrate enhanced safety profile of 4e (CC₅₀ = 102.77, 161.37 μM, respectively) compared to VCH-759 (CC₅₀ = 61.83, 81.28 μM, respectively). Molecular docking of the synthesized derivatives to NS5B polymerase allosteric site (PDB: 2HWH) showed similar binding modes to that of the co-crystallized ligand. Moreover, QSAR models were established for the studied thiazolidinones and thiazolotriazines to investigate the molecular characteristics contributing to the observed NS5B polymerase inhibition activity. The obtained results inspire further investigations of thiazolidinones and thiazolotriazine aiming at affording more potent, safe and orally active non-nucleoside NS5B polymerase inhibitors as anti-HCV drug candidates.

Keywords: 2D QSAR; Anti-HCV; HCV-NS5B polymerase; Molecular docking; Thiazolidinones; Thiazolotriazines.

MeSH terms

Antiviral Agents / chemical synthesis
Antiviral Agents / chemistry
Antiviral Agents / pharmacology*
Cell Line
Cell Survival / drug effects
Dose-Response Relationship, Drug
Hepacivirus / drug effects*
Hepacivirus / metabolism
Humans
Models, Molecular
Molecular Structure
Protease Inhibitors / chemical synthesis
Protease Inhibitors / chemistry
Protease Inhibitors / pharmacology*
Quantitative Structure-Activity Relationship*
Thiazoles / chemical synthesis
Thiazoles / chemistry
Thiazoles / pharmacology
Thiazolidines / chemical synthesis
Thiazolidines / chemistry
Thiazolidines / pharmacology
Triazines / chemical synthesis
Triazines / chemistry
Triazines / pharmacology
Viral Nonstructural Proteins / antagonists & inhibitors*
Viral Nonstructural Proteins / metabolism

Substances

Antiviral Agents
Protease Inhibitors
Thiazoles
Thiazolidines
Triazines
Viral Nonstructural Proteins
NS-5 protein, hepatitis C virus