Identification of novel natural drug candidates against BRAF mutated carcinoma; An integrative in-silico structure-based pharmacophore modeling and virtual screening process

The BRAF gene is responsible for transferring signals from outside of the cell to inside of the nucleus by converting a protein namely B-Raf through the RAS/MAPK pathway. This pathway contribute to cell division, proliferation, migration, and apoptotic cell death of human and animal. Mutation in thi...

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Autores principales: Dain Md Opo, F. A., Alsaiari, Ahad Amer, Rahman Molla, Mohammad Habibur, Ahmed Sumon, Md Afsar, Yaghmour, Khaled A., Ahammad, Foysal, Mohammad, Farhan, Simal-Gandara, Jesus
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Chemistry
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9577413/
https://www.ncbi.nlm.nih.gov/pubmed/36267655
http://dx.doi.org/10.3389/fchem.2022.986376
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author Dain Md Opo, F. A.
Alsaiari, Ahad Amer
Rahman Molla, Mohammad Habibur
Ahmed Sumon, Md Afsar
Yaghmour, Khaled A.
Ahammad, Foysal
Mohammad, Farhan
Simal-Gandara, Jesus
author_facet Dain Md Opo, F. A.
Alsaiari, Ahad Amer
Rahman Molla, Mohammad Habibur
Ahmed Sumon, Md Afsar
Yaghmour, Khaled A.
Ahammad, Foysal
Mohammad, Farhan
Simal-Gandara, Jesus
author_sort Dain Md Opo, F. A.
collection PubMed
description The BRAF gene is responsible for transferring signals from outside of the cell to inside of the nucleus by converting a protein namely B-Raf through the RAS/MAPK pathway. This pathway contribute to cell division, proliferation, migration, and apoptotic cell death of human and animal. Mutation in this gene may cause the development of several cancers, including lung, skin, colon, and neuroblastoma. Currently, a few available drugs are being used that has developed by targeting the BRAF mutated protein, and due to the toxic side effects, patients suffer a lot during their treatment. Therefore this study aimed to identify potentially lead compounds that can target and block the expression of BRAF and subsequently inhibit the cancer. The hits were generated through the pharmacophore model-based virtual screening, molecular docking, pharmacohore model validation, ADME (absorption, distribution, metabolism, and excretion) analysis molecular dynamics (MD) simulation to find more suitable candidate against the overexpress BRAF gene. The pharmacophore based screening initially identified 14 k possible hits from online database which were further screened by ligand scout advance software to get hit compound. Based on molecular docking score of ZINC70454679 (-10.6 kcal/mol), ZINC253500968 (-9.4 kcal/mol), ZINC106887736 (-8.6 kcal/mol), and ZINC107434492 (-8.1 kcal/mol), pharmacophore feature and toxicity evaluation, we selected four possible lead compounds. The dynamic simulation with Schrodinger Maestro software was used to determine the stability of the potential lead candidates with target protein (PDB ID: 5VAM). The results showed that the newly obtained four compounds were more stable than the control ligand (Pub Chem ID: 90408826). The current results showed that the ZINC70454679, ZINC253500968, ZINC106887736, and ZINC107434492 compounds may be able to work against several cancers through targeting the BRAF overexpressed gene. To develop a novel drug candidate, however the evaluation of the web lab based experimental work are necessary to evaluate the efficiency of the each compound against the BRAF target gene.
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spelling pubmed-95774132022-10-19 Identification of novel natural drug candidates against BRAF mutated carcinoma; An integrative in-silico structure-based pharmacophore modeling and virtual screening process Dain Md Opo, F. A. Alsaiari, Ahad Amer Rahman Molla, Mohammad Habibur Ahmed Sumon, Md Afsar Yaghmour, Khaled A. Ahammad, Foysal Mohammad, Farhan Simal-Gandara, Jesus Front Chem Chemistry The BRAF gene is responsible for transferring signals from outside of the cell to inside of the nucleus by converting a protein namely B-Raf through the RAS/MAPK pathway. This pathway contribute to cell division, proliferation, migration, and apoptotic cell death of human and animal. Mutation in this gene may cause the development of several cancers, including lung, skin, colon, and neuroblastoma. Currently, a few available drugs are being used that has developed by targeting the BRAF mutated protein, and due to the toxic side effects, patients suffer a lot during their treatment. Therefore this study aimed to identify potentially lead compounds that can target and block the expression of BRAF and subsequently inhibit the cancer. The hits were generated through the pharmacophore model-based virtual screening, molecular docking, pharmacohore model validation, ADME (absorption, distribution, metabolism, and excretion) analysis molecular dynamics (MD) simulation to find more suitable candidate against the overexpress BRAF gene. The pharmacophore based screening initially identified 14 k possible hits from online database which were further screened by ligand scout advance software to get hit compound. Based on molecular docking score of ZINC70454679 (-10.6 kcal/mol), ZINC253500968 (-9.4 kcal/mol), ZINC106887736 (-8.6 kcal/mol), and ZINC107434492 (-8.1 kcal/mol), pharmacophore feature and toxicity evaluation, we selected four possible lead compounds. The dynamic simulation with Schrodinger Maestro software was used to determine the stability of the potential lead candidates with target protein (PDB ID: 5VAM). The results showed that the newly obtained four compounds were more stable than the control ligand (Pub Chem ID: 90408826). The current results showed that the ZINC70454679, ZINC253500968, ZINC106887736, and ZINC107434492 compounds may be able to work against several cancers through targeting the BRAF overexpressed gene. To develop a novel drug candidate, however the evaluation of the web lab based experimental work are necessary to evaluate the efficiency of the each compound against the BRAF target gene. Frontiers Media S.A. 2022-10-04 /pmc/articles/PMC9577413/ /pubmed/36267655 http://dx.doi.org/10.3389/fchem.2022.986376 Text en Copyright © 2022 Dain Md Opo, Alsaiari, Rahman Molla, Ahmed Sumon, Yaghmour, Ahammad, Mohammad and Simal-Gandara. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Chemistry
Dain Md Opo, F. A.
Alsaiari, Ahad Amer
Rahman Molla, Mohammad Habibur
Ahmed Sumon, Md Afsar
Yaghmour, Khaled A.
Ahammad, Foysal
Mohammad, Farhan
Simal-Gandara, Jesus
Identification of novel natural drug candidates against BRAF mutated carcinoma; An integrative in-silico structure-based pharmacophore modeling and virtual screening process
title Identification of novel natural drug candidates against BRAF mutated carcinoma; An integrative in-silico structure-based pharmacophore modeling and virtual screening process
title_full Identification of novel natural drug candidates against BRAF mutated carcinoma; An integrative in-silico structure-based pharmacophore modeling and virtual screening process
title_fullStr Identification of novel natural drug candidates against BRAF mutated carcinoma; An integrative in-silico structure-based pharmacophore modeling and virtual screening process
title_full_unstemmed Identification of novel natural drug candidates against BRAF mutated carcinoma; An integrative in-silico structure-based pharmacophore modeling and virtual screening process
title_short Identification of novel natural drug candidates against BRAF mutated carcinoma; An integrative in-silico structure-based pharmacophore modeling and virtual screening process
title_sort identification of novel natural drug candidates against braf mutated carcinoma; an integrative in-silico structure-based pharmacophore modeling and virtual screening process
topic Chemistry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9577413/
https://www.ncbi.nlm.nih.gov/pubmed/36267655
http://dx.doi.org/10.3389/fchem.2022.986376
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