Molecular Interaction of a Kinase Inhibitor Midostaurin with Anticancer Drug Targets, S100A8 and EGFR: Transcriptional Profiling and Molecular Docking Study for Kidney Cancer Therapeutics

The S100A8 and epidermal growth factor receptor (EGFR) proteins are proto-oncogenes that are strongly expressed in a number of cancer types. EGFR promotes cellular proliferation, differentiation, migration and survival by activating molecular pathways. Involvement of proinflammatory S100A8 in tumor...

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Autores principales: Mirza, Zeenat, Schulten, Hans-Juergen, Farsi, Hasan Ma, Al-Maghrabi, Jaudah A., Gari, Mamdooh A., Chaudhary, Adeel Ga, Abuzenadah, Adel M., Al-Qahtani, Mohammed H., Karim, Sajjad
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4366044/
https://www.ncbi.nlm.nih.gov/pubmed/25789858
http://dx.doi.org/10.1371/journal.pone.0119765
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author Mirza, Zeenat
Schulten, Hans-Juergen
Farsi, Hasan Ma
Al-Maghrabi, Jaudah A.
Gari, Mamdooh A.
Chaudhary, Adeel Ga
Abuzenadah, Adel M.
Al-Qahtani, Mohammed H.
Karim, Sajjad
author_facet Mirza, Zeenat
Schulten, Hans-Juergen
Farsi, Hasan Ma
Al-Maghrabi, Jaudah A.
Gari, Mamdooh A.
Chaudhary, Adeel Ga
Abuzenadah, Adel M.
Al-Qahtani, Mohammed H.
Karim, Sajjad
author_sort Mirza, Zeenat
collection PubMed
description The S100A8 and epidermal growth factor receptor (EGFR) proteins are proto-oncogenes that are strongly expressed in a number of cancer types. EGFR promotes cellular proliferation, differentiation, migration and survival by activating molecular pathways. Involvement of proinflammatory S100A8 in tumor cell differentiation and progression is largely unclear and not studied in kidney cancer (KC). S100A8 and EGFR are potential therapeutic biomarkers and anticancer drug targets for KC. In this study, we explored molecular mechanisms of interaction profiles of both molecules with potential anticancer drugs. We undertook transcriptional profiling in Saudi KCs using Affymetrix HuGene 1.0 ST arrays. We identified 1478 significantly expressed genes, including S100A8 and EGFR overexpression, using cut-off p value <0.05 and fold change ≥2. Additionally, we compared and confirmed our findings with expression data available at NCBI’s GEO database. A significant number of genes associated with cancer showed involvement in cell cycle progression, DNA repair, tumor morphology, tissue development, and cell survival. Atherosclerosis signaling, leukocyte extravasation signaling, notch signaling, and IL-12 signaling were the most significantly disrupted signaling pathways. The present study provides an initial transcriptional profiling of Saudi KC patients. Our analysis suggests distinct transcriptomic signatures and pathways underlying molecular mechanisms of KC progression. Molecular docking analysis revealed that the kinase inhibitor "midostaurin" has amongst the selected drug targets, the best ligand properties to S100A8 and EGFR, with the implication that its binding inhibits downstream signaling in KC. This is the first structure-based docking study for the selected protein targets and anticancer drug, and the results indicate S100A8 and EGFR as attractive anticancer targets and midostaurin with effective drug properties for therapeutic intervention in KC.
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spelling pubmed-43660442015-03-23 Molecular Interaction of a Kinase Inhibitor Midostaurin with Anticancer Drug Targets, S100A8 and EGFR: Transcriptional Profiling and Molecular Docking Study for Kidney Cancer Therapeutics Mirza, Zeenat Schulten, Hans-Juergen Farsi, Hasan Ma Al-Maghrabi, Jaudah A. Gari, Mamdooh A. Chaudhary, Adeel Ga Abuzenadah, Adel M. Al-Qahtani, Mohammed H. Karim, Sajjad PLoS One Research Article The S100A8 and epidermal growth factor receptor (EGFR) proteins are proto-oncogenes that are strongly expressed in a number of cancer types. EGFR promotes cellular proliferation, differentiation, migration and survival by activating molecular pathways. Involvement of proinflammatory S100A8 in tumor cell differentiation and progression is largely unclear and not studied in kidney cancer (KC). S100A8 and EGFR are potential therapeutic biomarkers and anticancer drug targets for KC. In this study, we explored molecular mechanisms of interaction profiles of both molecules with potential anticancer drugs. We undertook transcriptional profiling in Saudi KCs using Affymetrix HuGene 1.0 ST arrays. We identified 1478 significantly expressed genes, including S100A8 and EGFR overexpression, using cut-off p value <0.05 and fold change ≥2. Additionally, we compared and confirmed our findings with expression data available at NCBI’s GEO database. A significant number of genes associated with cancer showed involvement in cell cycle progression, DNA repair, tumor morphology, tissue development, and cell survival. Atherosclerosis signaling, leukocyte extravasation signaling, notch signaling, and IL-12 signaling were the most significantly disrupted signaling pathways. The present study provides an initial transcriptional profiling of Saudi KC patients. Our analysis suggests distinct transcriptomic signatures and pathways underlying molecular mechanisms of KC progression. Molecular docking analysis revealed that the kinase inhibitor "midostaurin" has amongst the selected drug targets, the best ligand properties to S100A8 and EGFR, with the implication that its binding inhibits downstream signaling in KC. This is the first structure-based docking study for the selected protein targets and anticancer drug, and the results indicate S100A8 and EGFR as attractive anticancer targets and midostaurin with effective drug properties for therapeutic intervention in KC. Public Library of Science 2015-03-19 /pmc/articles/PMC4366044/ /pubmed/25789858 http://dx.doi.org/10.1371/journal.pone.0119765 Text en © 2015 Mirza et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Mirza, Zeenat
Schulten, Hans-Juergen
Farsi, Hasan Ma
Al-Maghrabi, Jaudah A.
Gari, Mamdooh A.
Chaudhary, Adeel Ga
Abuzenadah, Adel M.
Al-Qahtani, Mohammed H.
Karim, Sajjad
Molecular Interaction of a Kinase Inhibitor Midostaurin with Anticancer Drug Targets, S100A8 and EGFR: Transcriptional Profiling and Molecular Docking Study for Kidney Cancer Therapeutics
title Molecular Interaction of a Kinase Inhibitor Midostaurin with Anticancer Drug Targets, S100A8 and EGFR: Transcriptional Profiling and Molecular Docking Study for Kidney Cancer Therapeutics
title_full Molecular Interaction of a Kinase Inhibitor Midostaurin with Anticancer Drug Targets, S100A8 and EGFR: Transcriptional Profiling and Molecular Docking Study for Kidney Cancer Therapeutics
title_fullStr Molecular Interaction of a Kinase Inhibitor Midostaurin with Anticancer Drug Targets, S100A8 and EGFR: Transcriptional Profiling and Molecular Docking Study for Kidney Cancer Therapeutics
title_full_unstemmed Molecular Interaction of a Kinase Inhibitor Midostaurin with Anticancer Drug Targets, S100A8 and EGFR: Transcriptional Profiling and Molecular Docking Study for Kidney Cancer Therapeutics
title_short Molecular Interaction of a Kinase Inhibitor Midostaurin with Anticancer Drug Targets, S100A8 and EGFR: Transcriptional Profiling and Molecular Docking Study for Kidney Cancer Therapeutics
title_sort molecular interaction of a kinase inhibitor midostaurin with anticancer drug targets, s100a8 and egfr: transcriptional profiling and molecular docking study for kidney cancer therapeutics
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4366044/
https://www.ncbi.nlm.nih.gov/pubmed/25789858
http://dx.doi.org/10.1371/journal.pone.0119765
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