Ionizing radiations induce shared epigenomic signatures unraveling adaptive mechanisms of cancerous cell lines with or without methionine dependency.
Youssef SibliniCéline ChéryPierre RouyerJérémie RasoAmélia JulienSébastien HergalantAurélie FrançoisLina BezdetnayaGuillaume VoginJean-Louis GuéantAbderrahim OussalahPublished in: Clinical epigenetics (2021)
IRs generated a variation in the methylation level of a high number of CpG probes with shared biological pathways, including those associated with cell cycle and division, responses to IRs, sustained angiogenesis, tissue invasion, and metastasis. These results provide insight on shared adaptive mechanisms of the epigenome in cancerous cell lines in response to IR. Future experiments should focus on the tryptic association between IRs, the initiation of a radioresistance phenotype, and their interaction with methionine dependency as a hallmark of metabolic adaptation in cancer.
Keyphrases
- cell cycle
- dna methylation
- genome wide
- cell proliferation
- papillary thyroid
- low dose
- endothelial cells
- small molecule
- vascular endothelial growth factor
- squamous cell
- amino acid
- gene expression
- cell migration
- radiation induced
- current status
- fluorescence imaging
- dna damage response
- young adults
- single molecule
- photodynamic therapy
- childhood cancer
- dna damage