Abstract
Objective:Epigenetic modifications are gaining focus due to their indirect association with tumorigenesis. DNA methylation plays a prime role in regulation of gene expression. Any aberrations in this gene family may lead to chromosomal instability and increased magnitude of tumour progression. In line with the above fact, the present study has been designed to identify genetic alterations in the genes of the DNMT (DNA methyl-transferase) family among head and neck squamous cell carcinoma patients (HNSCC). Methods:The present study follows an observational design employing computational tools for analysis. The TCGA-Firehose Legacy data was assessed using the cBioportal database. The dataset comprised of 530 samples from HNSCC patients which were assessed for genetic alterations in the DNMT family. Furthermore, the protein stability analysis and pathogenicity of the mutations were assessed using I-Mutant Suite and PROVEAN tools. Results:Almost all genes of the DNMT family harboured gene amplification. The TRDMT1 and DNMT3L genes showed deep deletions. Apart from these several non-synonymous, truncating and splice-site mutations were also documented. Protein stability and pathogenicity analysis revealed that majority of the mutations were found to decrease the stability and impose pathogenicity. Upon probing for reported mutations using gnomAD database, around six reference single nucleotide polymorphisms were identified which were found to exhibit a minor allele frequency less than 0.01. Conclusions:Screening of an exhaustive collection of patient’s samples could provide immense knowledge about the disease pathogenesis and identification of therapeutic leads. The variants identified in the present study could be used as diagnostic markers. However, further experimental analysis through genotyping assay is warranted to validate the present findings.
Highlights
Head and neck squamous cell carcinoma (HNSCC) is the sixth most common type of cancer which is responsible for over 350,000 deaths every year (McDermott and Bowles, 2019)
The dataset comprised of 530 samples from head and neck squamous cell carcinoma patients (HNSCC) patients which were assessed for genetic alterations in the DNMT family
Oncoprint data analysis Submission of user defined query of 5 genes belonging to the family of DNA methyltransferase (Data not shown) returned a window with OncoPrint data which demonstrated the presence of alterations in 5 crucial genes of the DNMT family viz., DNMT1, TRDMT1, DNMT3A and DNMT3B, DNMT3L
Summary
Head and neck squamous cell carcinoma (HNSCC) is the sixth most common type of cancer which is responsible for over 350,000 deaths every year (McDermott and Bowles, 2019). Recent reports by the global cancer observatory, GLOBOCAN, 2018, revealed an increase in the mortality rate due to cancer of the lip and oral cavity especially in males, with a significant proportion of cases arising from south Asian countries (Bray et al, 2018). These two reports have projected a steep increase in the incidence of the disease. Several studies have identified polymorphic variants in DNMT genes with both positive and negative associations with different cancer types. Duan et al, demonstrated that the variants (rs2424913 C/T, rs1569686 G/T, rs6087990 T/C and rs2424908 T/C) were either negatively associated with cancer risk or confer protection against cancer in Asian population
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