Pharmacophore-Model-Based Virtual-Screening Approaches Identified Novel Natural Molecular Candidates for Treating Human Neuroblastoma

F A Dain Md Opo; Saleh Alkarim; Ghadeer I Alrefaei; Mohammad Habibur Rahman Molla; Nouf H Alsubhi; Faisal Alzahrani; Foysal Ahammad

doi:10.3390/cimb44100329

Pharmacophore-Model-Based Virtual-Screening Approaches Identified Novel Natural Molecular Candidates for Treating Human Neuroblastoma

Curr Issues Mol Biol. 2022 Oct 13;44(10):4838-4858. doi: 10.3390/cimb44100329.

Authors

F A Dain Md Opo^{1

2}, Saleh Alkarim^{1

2

3}, Ghadeer I Alrefaei⁴, Mohammad Habibur Rahman Molla¹, Nouf H Alsubhi⁵, Faisal Alzahrani^{2

3}, Foysal Ahammad^{1

6}

Affiliations

¹ Department of Biological Science, Faculty of Sciences, King Abdulaziz University (KAU), Jeddah 21589, Saudi Arabia.
² Embryonic Stem Cell Research Unit, King Fahd Medical Research Center (KFMRC), King Abdulaziz University (KAU), Jeddah 21589, Saudi Arabia.
³ Embryonic and Cancer Stem Cell Research Group, King Fahd Medical Research Center (KFMRC), King Abdulaziz University (KAU), Jeddah 21589, Saudi Arabia.
⁴ Department of Biology, College of Science, University of Jeddah, Jeddah 21589, Saudi Arabia.
⁵ Department of Biological Sciences, College of Science & Arts, King Abdulaziz University (KAU), Rabigh 21911, Saudi Arabia.
⁶ Division of Biological and Biomedical Sciences (BBS), College of Health and Life Sciences (CHLS), Hamad Bin Khalifa University (HBKU), Doha 122104, Qatar.

Abstract

The mortality of cancer patients with neuroblastoma is increasing due to the limited availability of specific treatment options. Few drug candidates for combating neuroblastoma have been developed, and identifying novel therapeutic candidates against the disease is an urgent issue. It has been found that muc-N protein is amplified in one-third of human neuroblastomas and expressed as an attractive drug target against the disease. The myc-N protein interferes with the bromodomain and extraterminal (BET) family proteins. Pharmacologically inhibition of the protein potently depletes MYCN in neuroblastoma cells. BET inhibitors target MYCN transcription and show therapeutic efficacy against neuroblastoma. Therefore, the study aimed to identify potential inhibitors against the BET family protein, specifically Brd4 (brodamine-containing protein 4), to hinder the activity of neuroblastoma cells. To identify effective molecular candidates against the disease, a structure-based pharmacophore model was created for the binding site of the Brd4 protein. The pharmacophore model generated from the protein Brd4 was validated to screen potential natural active compounds. The compounds identified through the pharmacophore-model-based virtual-screening process were further screened through molecular docking, ADME (absorption, distribution, metabolism, and excretion), toxicity, and molecular dynamics (MD) simulation approach. The pharmacophore-model-based screening process initially identified 136 compounds, further evaluated based on molecular docking, ADME analysis, and toxicity approaches, identifying four compounds with good binding affinity and lower side effects. The stability of the selected compounds was also confirmed by dynamic simulation and molecular mechanics with generalized Born and surface area solvation (MM-GBSA) methods. Finally, the study identified four natural lead compounds, ZINC2509501, ZINC2566088, ZINC1615112, and ZINC4104882, that will potentially inhibit the activity of the desired protein and help to fight against neuroblastoma and related diseases. However, further evaluations through in vitro and in vivo assays are suggested to identify their efficacy against the desired protein and disease.

Keywords: Brd4; MYCN; dynamic simulation; molecular docking; neuroblastoma; pharmacophore model; side effects.

Grants and funding

Grant Number: IFPRC-115-130-2020/King Abdulaziz University