Discovery of Novel Isoform-Selective Histone Deacetylases 5 and 9 Inhibitors Through Combined Ligand-Based Pharmacophore Modeling, Molecular Mocking, and Molecular Dynamics Simulations for Cancer Treatment

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Date

2021, 2021

Authors

Elmezayen, Ammar D.
Al-Obaidi, Anas
Yelekçi, Kemal

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Volume Title

Publisher

Elsevier

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Green Open Access

No

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Top 10%

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Abstract

Class IIa histone deacetylases (HDACs) 5 and 9 play crucial roles in several human disorders such as cancer, making them important targets for drug design. Continuous research is pursed to overcome the cytotoxicity side effect that comes with the currently available broad-spectrum HDACs inhibitors. Herein, common features of active HDACs inhibitors in clinical trials and use have been calculated to generate the best pharmacophore hypothesis. Guner-Henry scoring system was used to validate the generated hypotheses. Hypo1 of HDAC5 and Hypo2 of HDAC9 exhibited the most statistically significance hypotheses. Compounds with fit value of 3 and more were examined by QuickVina 2 docking tool to calculate their binding affinity toward all class IIa HDACs. A total of 6 potential selective compounds were subjected to 100 molecular dynamics (MD) simulation to examine their binding modes. The free binding energy calculations were computed according to the MM-PBSA method. Proposed selective compounds displayed good stability with their targets and thus they may offer potent leads for the designing of HDAC5 and HDAC9 isoform selective inhibitors.

Description

Keywords

HDAC5, HDAC9, MD simulation, MM-PBSA, Pharmacophore modeling, MD simulation, HDAC5, Molecular Dynamics Simulation, Ligands, Histone Deacetylases, Histone Deacetylase Inhibitors, Molecular Docking Simulation, MM-PBSA, Neoplasms, HDAC9, Humans, Protein Isoforms, Pharmacophore modeling

Fields of Science

0301 basic medicine, 0303 health sciences, 03 medical and health sciences

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OpenCitations Citation Count
3

Source

Journal of Molecular Graphics and Modelling

Volume

106

Issue

Start Page

107937

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CrossRef : 3

Scopus : 4

PubMed : 1

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Mendeley Readers : 12

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4

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3

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10

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151

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3

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