Exploring the Novel Computational Drug Target and Associated Key Pathways of Oral Cancer

Oral cancer (OC) is a serious health concern that has a high fatality rate. The oral cavity has seven kinds of OC, including the lip, tongue, and floor of the mouth, as well as the buccal, hard palate, alveolar, retromolar trigone, and soft palate. The goal of this study is to look into new biomarke...

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Autores principales: Akhter, Fatema, Kahtani, Fawzia Haif Al, Sambawa, Zainah Mohammed, Alhassan, Deema Abdulrahman, AlSaif, Reema Abdulaziz, Haque, Tahsinul, Alam, Mohammad Khursheed, Hasan, Md. Tanvir, Islam, Md. Rakibul, Ahmed, Kawsar, Basri, Rehana
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9406749/
https://www.ncbi.nlm.nih.gov/pubmed/36005140
http://dx.doi.org/10.3390/cimb44080244
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author Akhter, Fatema
Kahtani, Fawzia Haif Al
Sambawa, Zainah Mohammed
Alhassan, Deema Abdulrahman
AlSaif, Reema Abdulaziz
Haque, Tahsinul
Alam, Mohammad Khursheed
Hasan, Md. Tanvir
Islam, Md. Rakibul
Ahmed, Kawsar
Basri, Rehana
author_facet Akhter, Fatema
Kahtani, Fawzia Haif Al
Sambawa, Zainah Mohammed
Alhassan, Deema Abdulrahman
AlSaif, Reema Abdulaziz
Haque, Tahsinul
Alam, Mohammad Khursheed
Hasan, Md. Tanvir
Islam, Md. Rakibul
Ahmed, Kawsar
Basri, Rehana
author_sort Akhter, Fatema
collection PubMed
description Oral cancer (OC) is a serious health concern that has a high fatality rate. The oral cavity has seven kinds of OC, including the lip, tongue, and floor of the mouth, as well as the buccal, hard palate, alveolar, retromolar trigone, and soft palate. The goal of this study is to look into new biomarkers and important pathways that might be used as diagnostic biomarkers and therapeutic candidates in OC. The publicly available repository the Gene Expression Omnibus (GEO) was to the source for the collection of OC-related datasets. GSE74530, GSE23558, and GSE3524 microarray datasets were collected for analysis. Minimum cut-off criteria of |log fold-change (FC)| > 1 and adjusted p < 0.05 were applied to calculate the upregulated and downregulated differential expression genes (DEGs) from the three datasets. After that only common DEGs in all three datasets were collected to apply further analysis. Gene ontology (GO) and pathway analysis were implemented to explore the functional behaviors of DEGs. Then protein–protein interaction (PPI) networks were built to identify the most active genes, and a clustering algorithm was also implemented to identify complex parts of PPI. TF-miRNA networks were also constructed to study OC-associated DEGs in-depth. Finally, top gene performers from PPI networks were used to apply drug signature analysis. After applying filtration and cut-off criteria, 2508, 3377, and 670 DEGs were found for GSE74530, GSE23558, and GSE3524 respectively, and 166 common DEGs were found in every dataset. The GO annotation remarks that most of the DEGs were associated with the terms of type I interferon signaling pathway. The pathways of KEGG reported that the common DEGs are related to the cell cycle and influenza A. The PPI network holds 88 nodes and 492 edges, and CDC6 had the highest number of connections. Four clusters were identified from the PPI. Drug signatures doxorubicin and resveratrol showed high significance according to the hub genes. We anticipate that our bioinformatics research will aid in the definition of OC pathophysiology and the development of new therapies for OC.
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spelling pubmed-94067492022-08-26 Exploring the Novel Computational Drug Target and Associated Key Pathways of Oral Cancer Akhter, Fatema Kahtani, Fawzia Haif Al Sambawa, Zainah Mohammed Alhassan, Deema Abdulrahman AlSaif, Reema Abdulaziz Haque, Tahsinul Alam, Mohammad Khursheed Hasan, Md. Tanvir Islam, Md. Rakibul Ahmed, Kawsar Basri, Rehana Curr Issues Mol Biol Article Oral cancer (OC) is a serious health concern that has a high fatality rate. The oral cavity has seven kinds of OC, including the lip, tongue, and floor of the mouth, as well as the buccal, hard palate, alveolar, retromolar trigone, and soft palate. The goal of this study is to look into new biomarkers and important pathways that might be used as diagnostic biomarkers and therapeutic candidates in OC. The publicly available repository the Gene Expression Omnibus (GEO) was to the source for the collection of OC-related datasets. GSE74530, GSE23558, and GSE3524 microarray datasets were collected for analysis. Minimum cut-off criteria of |log fold-change (FC)| > 1 and adjusted p < 0.05 were applied to calculate the upregulated and downregulated differential expression genes (DEGs) from the three datasets. After that only common DEGs in all three datasets were collected to apply further analysis. Gene ontology (GO) and pathway analysis were implemented to explore the functional behaviors of DEGs. Then protein–protein interaction (PPI) networks were built to identify the most active genes, and a clustering algorithm was also implemented to identify complex parts of PPI. TF-miRNA networks were also constructed to study OC-associated DEGs in-depth. Finally, top gene performers from PPI networks were used to apply drug signature analysis. After applying filtration and cut-off criteria, 2508, 3377, and 670 DEGs were found for GSE74530, GSE23558, and GSE3524 respectively, and 166 common DEGs were found in every dataset. The GO annotation remarks that most of the DEGs were associated with the terms of type I interferon signaling pathway. The pathways of KEGG reported that the common DEGs are related to the cell cycle and influenza A. The PPI network holds 88 nodes and 492 edges, and CDC6 had the highest number of connections. Four clusters were identified from the PPI. Drug signatures doxorubicin and resveratrol showed high significance according to the hub genes. We anticipate that our bioinformatics research will aid in the definition of OC pathophysiology and the development of new therapies for OC. MDPI 2022-08-09 /pmc/articles/PMC9406749/ /pubmed/36005140 http://dx.doi.org/10.3390/cimb44080244 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Akhter, Fatema
Kahtani, Fawzia Haif Al
Sambawa, Zainah Mohammed
Alhassan, Deema Abdulrahman
AlSaif, Reema Abdulaziz
Haque, Tahsinul
Alam, Mohammad Khursheed
Hasan, Md. Tanvir
Islam, Md. Rakibul
Ahmed, Kawsar
Basri, Rehana
Exploring the Novel Computational Drug Target and Associated Key Pathways of Oral Cancer
title Exploring the Novel Computational Drug Target and Associated Key Pathways of Oral Cancer
title_full Exploring the Novel Computational Drug Target and Associated Key Pathways of Oral Cancer
title_fullStr Exploring the Novel Computational Drug Target and Associated Key Pathways of Oral Cancer
title_full_unstemmed Exploring the Novel Computational Drug Target and Associated Key Pathways of Oral Cancer
title_short Exploring the Novel Computational Drug Target and Associated Key Pathways of Oral Cancer
title_sort exploring the novel computational drug target and associated key pathways of oral cancer
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9406749/
https://www.ncbi.nlm.nih.gov/pubmed/36005140
http://dx.doi.org/10.3390/cimb44080244
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