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Beta-catenin and epithelial tumors: a study based on 374 oropharyngeal cancers. | LitMetric

Beta-catenin and epithelial tumors: a study based on 374 oropharyngeal cancers.

Biomed Res Int

IRCCS-CROB, Oncological Reference Centre of Basilicata, 85028 Rionero in Vulture, Italy ; Section of Oral Pathology, Department of Clinical and Experimental Medicine, University of Foggia, 71122 Foggia, Italy.

Published: September 2014

Introduction: Although altered regulation of the Wnt pathway via beta-catenin is a frequent event in several human cancers, its potential implications in oral/oropharyngeal squamous cell carcinomas (OSCC/OPSCC) are largely unexplored. Work purpose was to define association between beta-catenin expression and clinical-pathological parameters in 374 OSCCs/OP-SCCs by immunohistochemistry (IHC).

Materials And Methods: Association between IHC detected patterns of protein expression and clinical-pathological parameters was assessed by statistical analysis and survival rates by Kaplan-Meier curves. Beta-catenin expression was also investigated in OSCC cell lines by Real-Time PCR. An additional analysis of the DNA content was performed on 22 representative OSCCs/OPSCCs by DNA-image-cytometric analysis.

Results And Discussion: All carcinomas exhibited significant alterations of beta-catenin expression (P < 0.05). Beta-catenin protein was mainly detected in the cytoplasm of cancerous cells and only focal nuclear positivity was observed. Higher cytoplasmic expression correlated significantly with poor histological differentiation, advanced stage, and worst patient outcome (P < 0.05). By Real-Time PCR significant increase of beta-catenin mRNA was detected in OSCC cell lines and in 45% of surgical specimens. DNA ploidy study demonstrated high levels of aneuploidy in beta-catenin overexpressing carcinomas.

Conclusions: This is the largest study reporting significant association between beta-catenin expression and clinical-pathological factors in patients with OSCCs/OPSCCs.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3912883PMC
http://dx.doi.org/10.1155/2014/948264DOI Listing

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