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http://dx.doi.org/10.7314/APJCP.2015.16.11.4589

Mutation Analysis of the Dimer Forming Domain of the Caspase 8 Gene in Oral Submucous Fibrosis and Squamous Cell Carcinomas  

Menon, Uthara (Department of Oral Medicine and Radiology, Faculty of Dentistry, SRM University)
Poongodi, V (Department of Oral Medicine and Radiology, Faculty of Dentistry, SRM University)
Raghuram, Pitty Hari (Department of Oral Medicine and Radiology, Faculty of Dentistry, SRM University)
Ashokan, Kannan (Department of Oral Medicine and Radiology, Faculty of Dentistry, SRM University)
Govindarajan, Giri Valanthan Veda (Department of Oral and Maxillofacial Surgery, Faculty of Dentistry, Sri Ramachandra University)
Ramanathan, Arvind (Enable Biolabs, Madurai Meenakshipuram Extension)
Publication Information
Asian Pacific Journal of Cancer Prevention / v.16, no.11, 2015 , pp. 4589-4592 More about this Journal
Abstract
Background: Missense and frame-shift mutations within the dimer forming domain of the caspase 8 gene have been identified in several cancers. However, the genetic status of this region in precancerous lesions, like oral submucous fibrosis (OSMF), and well differentiated oral squamous cell carcinomas (OSCCs) in patients from southern region of India is not known, and hence the present study was designed to address this issue. Materials and Methods: Genomic DNA isolated from biopsy tissues of thirty one oral submucous fibrosis and twenty five OSCC samples were subjected to PCR amplification with intronic primers flanking exon 7 of the caspase 8 gene. The PCR amplicons were subsequently subjected to direct sequencing to elucidate the status of mutation. Results: Sequence analysis identified a frame-shift and a novel missense mutation in two out of twenty five OSCC samples. The frame-shift mutation was due to a two base pair deletion (c.1225_1226delTG), while the missense mutation was due to substitution of wild type cysteine residue with phenylalanine at codon 426 (C426F). The missense mutation, however, was found to be heterozygous as the wild type C426C codon was also present. None of the OSMF samples carried mutations. Conclusions: The identification of mutations in OSCC lesions but not OSMF suggests that dimer forming domain mutations in caspase 8 may be limited to malignant lesions. The absence of mutations in OSMF also suggests that the samples analyzed in the present study may not have acquired transforming potential. To the best of our knowledge this is the first study to have explored and identified frame-shift and novel missense mutations in OSCC tissue samples.
Keywords
Caspase 8 mutation in oral carcinoma; loss of function of caspase 8; caspase 8 mutation in cancer;
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