Exploring the potential of approved drugs for triple-negative breast cancer treatment by targeting casein kinase 2: Insights from computational studies

Triple-negative breast cancer (TNBC) is an aggressive malignancy that requires effective targeted drug therapy. In this study, we employed in silico methods to evaluate the efficacy of seven approved drugs against human ck2 alpha kinase, a significant modulator of TNBC metastasis and invasiveness. M...

Descripción completa

Detalles Bibliográficos
Autores principales: Shoaib, Tagyedeen H., Ibraheem, Walaa, Abdelrahman, Mohammed, Osman, Wadah, Sherif, Asmaa E., Ashour, Ahmed, Ibrahim, Sabrin R. M., Ghazawi, Kholoud F., Miski, Samar F., Almadani, Sara A., ALsiyud, Duaa Fahad, Mohamed, Gamal A., Alzain, Abdulrahim A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10424868/
https://www.ncbi.nlm.nih.gov/pubmed/37578958
http://dx.doi.org/10.1371/journal.pone.0289887
_version_ 1785089753569296384
author Shoaib, Tagyedeen H.
Ibraheem, Walaa
Abdelrahman, Mohammed
Osman, Wadah
Sherif, Asmaa E.
Ashour, Ahmed
Ibrahim, Sabrin R. M.
Ghazawi, Kholoud F.
Miski, Samar F.
Almadani, Sara A.
ALsiyud, Duaa Fahad
Mohamed, Gamal A.
Alzain, Abdulrahim A.
author_facet Shoaib, Tagyedeen H.
Ibraheem, Walaa
Abdelrahman, Mohammed
Osman, Wadah
Sherif, Asmaa E.
Ashour, Ahmed
Ibrahim, Sabrin R. M.
Ghazawi, Kholoud F.
Miski, Samar F.
Almadani, Sara A.
ALsiyud, Duaa Fahad
Mohamed, Gamal A.
Alzain, Abdulrahim A.
author_sort Shoaib, Tagyedeen H.
collection PubMed
description Triple-negative breast cancer (TNBC) is an aggressive malignancy that requires effective targeted drug therapy. In this study, we employed in silico methods to evaluate the efficacy of seven approved drugs against human ck2 alpha kinase, a significant modulator of TNBC metastasis and invasiveness. Molecular docking revealed that the co-crystallized reference inhibitor 108600 achieved a docking score of (-7.390 kcal/mol). Notably, among the seven approved drugs tested, sunitinib, bazedoxifene, and etravirine exhibited superior docking scores compared to the reference inhibitor. Specifically, their respective docking scores were -10.401, -7.937, and -7.743 kcal/mol. Further analysis using MM/GBSA demonstrated that these three top-ranked drugs possessed better binding energies than the reference ligand. Subsequent molecular dynamics simulations identified etravirine, an FDA-approved antiviral drug, as the only repurposed drug that demonstrated a stable and reliable binding mode with the human ck2 alpha protein, based on various analysis measures including RMSD, RMSF, and radius of gyration. Principal component analysis indicated that etravirine exhibited comparable stability of motion as a complex with human ck2 alpha protein, similar to the co-crystallized inhibitor. Additionally, Density functional theory (DFT) calculations were performed on a complex of etravirine and a representative gold atom positioned at different sites relative to the heteroatoms of etravirine. The results of the DFT calculations revealed low-energy complexes that could potentially serve as guides for experimental trials involving gold nanocarriers of etravirine, enhancing its delivery to malignant cells and introducing a new drug delivery route. Based on the results obtained in this research study, etravirine shows promise as a potential antitumor agent targeting TNBC, warranting further investigation through experimental and clinical assessments.
format Online
Article
Text
id pubmed-10424868
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-104248682023-08-15 Exploring the potential of approved drugs for triple-negative breast cancer treatment by targeting casein kinase 2: Insights from computational studies Shoaib, Tagyedeen H. Ibraheem, Walaa Abdelrahman, Mohammed Osman, Wadah Sherif, Asmaa E. Ashour, Ahmed Ibrahim, Sabrin R. M. Ghazawi, Kholoud F. Miski, Samar F. Almadani, Sara A. ALsiyud, Duaa Fahad Mohamed, Gamal A. Alzain, Abdulrahim A. PLoS One Research Article Triple-negative breast cancer (TNBC) is an aggressive malignancy that requires effective targeted drug therapy. In this study, we employed in silico methods to evaluate the efficacy of seven approved drugs against human ck2 alpha kinase, a significant modulator of TNBC metastasis and invasiveness. Molecular docking revealed that the co-crystallized reference inhibitor 108600 achieved a docking score of (-7.390 kcal/mol). Notably, among the seven approved drugs tested, sunitinib, bazedoxifene, and etravirine exhibited superior docking scores compared to the reference inhibitor. Specifically, their respective docking scores were -10.401, -7.937, and -7.743 kcal/mol. Further analysis using MM/GBSA demonstrated that these three top-ranked drugs possessed better binding energies than the reference ligand. Subsequent molecular dynamics simulations identified etravirine, an FDA-approved antiviral drug, as the only repurposed drug that demonstrated a stable and reliable binding mode with the human ck2 alpha protein, based on various analysis measures including RMSD, RMSF, and radius of gyration. Principal component analysis indicated that etravirine exhibited comparable stability of motion as a complex with human ck2 alpha protein, similar to the co-crystallized inhibitor. Additionally, Density functional theory (DFT) calculations were performed on a complex of etravirine and a representative gold atom positioned at different sites relative to the heteroatoms of etravirine. The results of the DFT calculations revealed low-energy complexes that could potentially serve as guides for experimental trials involving gold nanocarriers of etravirine, enhancing its delivery to malignant cells and introducing a new drug delivery route. Based on the results obtained in this research study, etravirine shows promise as a potential antitumor agent targeting TNBC, warranting further investigation through experimental and clinical assessments. Public Library of Science 2023-08-14 /pmc/articles/PMC10424868/ /pubmed/37578958 http://dx.doi.org/10.1371/journal.pone.0289887 Text en © 2023 Shoaib et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Shoaib, Tagyedeen H.
Ibraheem, Walaa
Abdelrahman, Mohammed
Osman, Wadah
Sherif, Asmaa E.
Ashour, Ahmed
Ibrahim, Sabrin R. M.
Ghazawi, Kholoud F.
Miski, Samar F.
Almadani, Sara A.
ALsiyud, Duaa Fahad
Mohamed, Gamal A.
Alzain, Abdulrahim A.
Exploring the potential of approved drugs for triple-negative breast cancer treatment by targeting casein kinase 2: Insights from computational studies
title Exploring the potential of approved drugs for triple-negative breast cancer treatment by targeting casein kinase 2: Insights from computational studies
title_full Exploring the potential of approved drugs for triple-negative breast cancer treatment by targeting casein kinase 2: Insights from computational studies
title_fullStr Exploring the potential of approved drugs for triple-negative breast cancer treatment by targeting casein kinase 2: Insights from computational studies
title_full_unstemmed Exploring the potential of approved drugs for triple-negative breast cancer treatment by targeting casein kinase 2: Insights from computational studies
title_short Exploring the potential of approved drugs for triple-negative breast cancer treatment by targeting casein kinase 2: Insights from computational studies
title_sort exploring the potential of approved drugs for triple-negative breast cancer treatment by targeting casein kinase 2: insights from computational studies
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10424868/
https://www.ncbi.nlm.nih.gov/pubmed/37578958
http://dx.doi.org/10.1371/journal.pone.0289887
work_keys_str_mv AT shoaibtagyedeenh exploringthepotentialofapproveddrugsfortriplenegativebreastcancertreatmentbytargetingcaseinkinase2insightsfromcomputationalstudies
AT ibraheemwalaa exploringthepotentialofapproveddrugsfortriplenegativebreastcancertreatmentbytargetingcaseinkinase2insightsfromcomputationalstudies
AT abdelrahmanmohammed exploringthepotentialofapproveddrugsfortriplenegativebreastcancertreatmentbytargetingcaseinkinase2insightsfromcomputationalstudies
AT osmanwadah exploringthepotentialofapproveddrugsfortriplenegativebreastcancertreatmentbytargetingcaseinkinase2insightsfromcomputationalstudies
AT sherifasmaae exploringthepotentialofapproveddrugsfortriplenegativebreastcancertreatmentbytargetingcaseinkinase2insightsfromcomputationalstudies
AT ashourahmed exploringthepotentialofapproveddrugsfortriplenegativebreastcancertreatmentbytargetingcaseinkinase2insightsfromcomputationalstudies
AT ibrahimsabrinrm exploringthepotentialofapproveddrugsfortriplenegativebreastcancertreatmentbytargetingcaseinkinase2insightsfromcomputationalstudies
AT ghazawikholoudf exploringthepotentialofapproveddrugsfortriplenegativebreastcancertreatmentbytargetingcaseinkinase2insightsfromcomputationalstudies
AT miskisamarf exploringthepotentialofapproveddrugsfortriplenegativebreastcancertreatmentbytargetingcaseinkinase2insightsfromcomputationalstudies
AT almadanisaraa exploringthepotentialofapproveddrugsfortriplenegativebreastcancertreatmentbytargetingcaseinkinase2insightsfromcomputationalstudies
AT alsiyudduaafahad exploringthepotentialofapproveddrugsfortriplenegativebreastcancertreatmentbytargetingcaseinkinase2insightsfromcomputationalstudies
AT mohamedgamala exploringthepotentialofapproveddrugsfortriplenegativebreastcancertreatmentbytargetingcaseinkinase2insightsfromcomputationalstudies
AT alzainabdulrahima exploringthepotentialofapproveddrugsfortriplenegativebreastcancertreatmentbytargetingcaseinkinase2insightsfromcomputationalstudies

Ejemplares similares