NCBP2 and TFRC are novel prognostic biomarkers in oral squamous cell carcinoma

被引:0
|
作者
Rahul Arora
Logan Haynes
Mehul Kumar
Reid McNeil
Jahanshah Ashkani
Steven C. Nakoneshny
T. Wayne Matthews
Shamir Chandarana
Robert D. Hart
Steven J. M. Jones
Joseph C. Dort
Doha Itani
Ayan Chanda
Pinaki Bose
机构
[1] University of Calgary,Department of Biochemistry and Molecular Biology, Cumming School of Medicine
[2] Canada’s Michael Smith Genome Sciences Centre,Ohlson Research Initiative, Arnie Charbonneau Cancer Institute, Cumming School of Medicine
[3] University of Calgary,Department of Surgery, Section of Otolaryngology
[4] University of Calgary,Head & Neck Surgery, Cumming School of Medicine
[5] University of Calgary,Department of Oncology, Cumming School of Medicine
[6] Dalhousie University,Department of Anatomic and Molecular Pathology
来源
Cancer Gene Therapy | 2023年 / 30卷
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摘要
There are few prognostic biomarkers and targeted therapeutics currently in use for the clinical management of oral squamous cell carcinoma (OSCC) and patient outcomes remain poor in this disease. A majority of mutations in OSCC are loss-of-function events in tumour suppressor genes that are refractory to conventional modes of targeting. Interestingly, the chromosomal segment 3q22-3q29 is amplified in many epithelial cancers, including OSCC. We hypothesized that some of the 468 genes located on 3q22-3q29 might be drivers of oral carcinogenesis and could be exploited as potential prognostic biomarkers and therapeutic targets. Our integrative analysis of copy number variation (CNV), gene expression and clinical data from The Cancer Genome Atlas (TCGA), identified two candidate genes: NCBP2, TFRC, whose expression positively correlates with worse overall survival (OS) in HPV-negative OSCC patients. Expression of NCBP2 and TFRC is significantly higher in tumour cells compared to most normal human tissues. High NCBP2 and TFRC protein abundance is associated with worse overall, disease-specific survival, and progression-free interval in an in-house cohort of HPV-negative OSCC patients. Finally, due to a lack of evidence for the role of NCBP2 in carcinogenesis, we tested if modulating NCBP2 levels in human OSCC cell lines affected their carcinogenic behaviour. We found that NCBP2 depletion reduced OSCC cell proliferation, migration, and invasion. Differential expression analysis revealed the upregulation of several tumour-promoting genes in patients with high NCBP2 expression. We thus propose both NCBP2 and TFRC as novel prognostic and potentially therapeutic biomarkers for HPV-negative OSCC.
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页码:752 / 765
页数:13
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