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dc.contributor.authorDurmuş, Saliha
dc.contributor.authorYILMAZ AYDOĞAN, Hülya
dc.contributor.authorIşbilen, Murat
dc.contributor.authorÇakir, Tunahan
dc.contributor.authorYAYLIM, İlhan
dc.contributor.authorInal Gültekin, Güldal
dc.contributor.authorTİMİRCİ KAHRAMAN, Özlem
dc.date.accessioned2023-02-21T08:40:32Z
dc.date.available2023-02-21T08:40:32Z
dc.date.issued2022
dc.identifier.citationInal Gültekin G., TİMİRCİ KAHRAMAN Ö., Işbilen M., Durmuş S., Çakir T., YAYLIM İ., YILMAZ AYDOĞAN H., "Six potential biomarkers for bladder cancer: key proteins in cell-cycle division and apoptosis pathways", Journal of the Egyptian National Cancer Institute, cilt.34, sa.1, 2022
dc.identifier.issn1110-0362
dc.identifier.othervv_1032021
dc.identifier.otherav_1fa716c1-920c-4d11-99b1-f6b63ba287eb
dc.identifier.urihttp://hdl.handle.net/20.500.12627/186863
dc.identifier.urihttps://doi.org/10.1186/s43046-022-00153-0
dc.identifier.urihttps://avesis.istanbul.edu.tr/api/publication/1fa716c1-920c-4d11-99b1-f6b63ba287eb/file
dc.description.abstract© 2022, The Author(s).Background: The bladder cancer (BC) pathology is caused by both exogenous environmental and endogenous molecular factors. Several genes have been implicated, but the molecular pathogenesis of BC and its subtypes remains debatable. The bioinformatic analysis evaluates high numbers of proteins in a single study, increasing the opportunity to identify possible biomarkers for disorders. Methods: The aim of this study is to identify biomarkers for the identification of BC using several bioinformatic analytical tools and methods. BC and normal samples were compared for each probeset with T test in GSE13507 and GSE37817 datasets, and statistical probesets were verified with GSE52519 and E-MTAB-1940 datasets. Differential gene expression, hierarchical clustering, gene ontology enrichment analysis, and heuristic online phenotype prediction algorithm methods were utilized. Statistically significant proteins were assessed in the Human Protein Atlas database. GSE13507 (6271 probesets) and GSE37817 (3267 probesets) data were significant after the extraction of probesets without gene annotation information. Common probesets in both datasets (2888) were further narrowed by analyzing the first 100 upregulated and downregulated probesets in BC samples. Results: Among the total 400 probesets, 68 were significant for both datasets with similar fold-change values (Pearson r: 0.995). Protein-protein interaction networks demonstrated strong interactions between CCNB1, BUB1B, and AURKB. The HPA database revealed similar protein expression levels for CKAP2L, AURKB, APIP, and LGALS3 both for BC and control samples. Conclusion: This study disclosed six candidate biomarkers for the early diagnosis of BC. It is suggested that these candidate proteins be investigated in a wet lab to identify their functions in BC pathology and possible treatment approaches.
dc.language.isoeng
dc.subjectOnkoloji
dc.subjectYaşam Bilimleri
dc.subjectSitogenetik
dc.subjectSağlık Bilimleri
dc.subjectTemel Bilimler
dc.subjectKanser Araştırmaları
dc.subjectTıp
dc.subjectDahili Tıp Bilimleri
dc.subjectİç Hastalıkları
dc.subjectBİYOKİMYA VE MOLEKÜLER BİYOLOJİ
dc.subjectONKOLOJİ
dc.subjectMoleküler Biyoloji ve Genetik
dc.subjectKlinik Tıp
dc.subjectYaşam Bilimleri (LIFE)
dc.subjectKlinik Tıp (MED)
dc.titleSix potential biomarkers for bladder cancer: key proteins in cell-cycle division and apoptosis pathways
dc.typeMakale
dc.relation.journalJournal of the Egyptian National Cancer Institute
dc.contributor.departmentOkan Üniversitesi , ,
dc.identifier.volume34
dc.identifier.issue1
dc.contributor.firstauthorID4244857


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