ARID2 suppression promotes tumor progression and upregulates cytokeratin 8, 18 and β-4 integrin expression in TP53-mutated tobacco-related oral cancer and has prognostic implications
Mutations in ARID2 and TP53 genes are found to be implicated in the tobacco related tumorigeneses. However, the effect of loss of ARID2 in the TP53 mutated background in tobacco related cancer including oral cancer has not been investigated yet. Hence, in this study we knockdown ARID2 using shRNA me...
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Veröffentlicht in: | Cancer gene therapy 2022-12, Vol.29 (12), p.1908-1917 |
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Zusammenfassung: | Mutations in
ARID2
and
TP53
genes are found to be implicated in the tobacco related tumorigeneses. However, the effect of loss of ARID2 in the
TP53
mutated background in tobacco related cancer including oral cancer has not been investigated yet. Hence, in this study we knockdown ARID2 using shRNA mediated knockdown strategy in
TP53
mutated oral squamous cell carcinoma (OSCC) cell line and studied its tumorigenic role. Our study revealed that suppression of ARID2 in
TP53
mutated oral cancer cells increases cell motility and invasion, induces drastic morphological changes and leads to a marked increase in the expression levels of cytokeratins, and integrins, CK8, CK18 and β4-Integrin, markers of cell migration/invasion in oral cancer. ARID2 suppression also showed early onset and increased tumorigenicity in-vivo. Interestingly, transcriptome profiling revealed differentially expressed genes associated with migration and invasion in oral cancer cells including
AKR1C2, NCAM2, NOS1, ADAM23
and genes of
S100A
family in ARID2 knockdown
TP53
mutated oral cancer cells. Pathway analysis of differentially regulated genes identified “cancer pathways” and “PI3K/AKT Pathway” to be significantly dysregulated upon suppression of ARID2 in
TP53
mutated OSCC cells. Notably, decreased ARID2 expression and increased CK8, CK18 expression leads to poor prognosis in Head and Neck cancer (HNSC) patients as revealed by Pan-Cancer TCGA data analysis. To conclude, our study is the first to demonstrate tumor suppressor role of ARID2 in
TP53
mutated background indicating their cooperative role in OSCC, and also highlights its prognostic implications suggesting ARID2 as an important therapeutic target in OSCC. |
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ISSN: | 0929-1903 1476-5500 1476-5500 |
DOI: | 10.1038/s41417-022-00505-x |