In silico assessment of DNA damage response gene variants associated with head and neck cancer

Raima Das; Sharbadeb Kundu; Shaheen Laskar; Yashmin Choudhury; Sankar Kumar Ghosh

doi:10.1080/07391102.2022.2027817

In silico assessment of DNA damage response gene variants associated with head and neck cancer

J Biomol Struct Dyn. 2023 Apr;41(6):2090-2107. doi: 10.1080/07391102.2022.2027817. Epub 2022 Jan 17.

Authors

Raima Das¹, Sharbadeb Kundu², Shaheen Laskar¹, Yashmin Choudhury¹, Sankar Kumar Ghosh¹

Affiliations

¹ Department of Biotechnology, Assam University, Silchar, India.
² Genome Science, School of Interdisciplinary Studies, University of Kalyani, Nadia, West India.

PMID: 35037836
DOI: 10.1080/07391102.2022.2027817

Abstract

Head and neck cancer (HNC), the sixth most common cancer globally, stands first in India, especially Northeast India, where tobacco usage is predominant, which introduces various carcinogens leading to malignancies by accumulating DNA damages. Consequently, the present work aimed to predict the impact of significant germline variants in DNA repair and Tumour Suppressor genes on HNC development. WES in Ion Proton^TM platform on 'discovery set' (n = 15), followed by recurrence assessment of the observed variants on 'confirmation set' (n = 40) using Sanger Sequencing was performed on the HNC-prevalent NE Indian populations. Initially, 53 variants were identified, of which seven HNC-linked DNA damage response gene variants were frequent in the studied populations. Different tools ascertained the biological consequences of these variants, of which the non-coding variants viz. EXO1_rs4150018, RAD52_rs6413436, CHD5_rs2746066, HACE1_rs6918700 showed risk, while FLT3_rs2491227 and BMPR1A_rs7074064 conferred protection against HNC by affecting transcriptional regulation and splicing mechanism. Molecular Dynamics Simulation of the full-length p53 model predicted that the observed coding TP53_rs1042522 variant conferred HNC-risk by altering the structural dynamics of the protein, which displayed difficulty in the transition between active and inactive conformations due to high-energy barrier. Subsequent pathway and gene ontology analysis revealed that EXO1, RAD52 and TP53 variants affected the Double-Strand Break Repair pathway, whereas CHD5 and HACE1 variants inactivated DNA repair cascade, facilitating uncontrolled cell proliferation, impaired apoptosis and malignant transformation. Conversely, FLT3 and BMPR1A variants protected against HNC by controlling tumorigenesis, which requires experimental validation. These findings may serve as prognostic markers for developing preventive measures against HNC.

Keywords: DNA damage response; HNC; cancer-causing genes; full-length p53 model; germline variants; in silico assessment; molecular dynamics simulation; transcriptional regulation.

MeSH terms

DNA Damage / genetics
DNA Helicases / genetics
DNA Repair / genetics
Genetic Predisposition to Disease*
Head and Neck Neoplasms* / genetics
Humans
Nerve Tissue Proteins / genetics
Polymorphism, Single Nucleotide
Ubiquitin-Protein Ligases / genetics

Substances

CHD5 protein, human
DNA Helicases
Nerve Tissue Proteins
HACE1 protein, human
Ubiquitin-Protein Ligases