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Quantitative and qualitative mutational impact of ionizing radiation on normal cells

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Author(s)
Youk, JeonghwanKwon, Hyun WooLim, JoonohKim, EunjiKim, TaewooKim, RyulPark, SeongyeolYi, KijongNam, Chang HyunJeon, SaraAn, YohanChoi, JinwookNa, HyelinLee, Eon-SeokCho, YoungwonMin, Dong-WookKim, HyoJinKang, Yeong-RokChoi, Si HoBae, Min JiLee, Chang GeunKim, Joon-GoonKim, Young SeoYu, TosolLee, Won-ChulShin, Jong-YeonLee, Dong SooKim, Tae-YouKu, TaeyunKim, Su YeonLee, Joo-HyeonKoo, Bon-KyoungLee, HyunsookYi, On VoxHan, Eon ChulChang, Ji HyunKim, Kyung SuSon, Tae GenJu, Young Seok
Type
Article
Citation
Cell Genomics, v.4, no.2
Issued Date
2024-02
Abstract
The comprehensive genomic impact of ionizing radiation (IR), a carcinogen, on healthy somatic cells remains unclear. Using large-scale whole-genome sequencing (WGS) of clones expanded from irradiated murine and human single cells, we revealed that IR induces a characteristic spectrum of short insertions or deletions (indels) and structural variations (SVs), including balanced inversions, translocations, composite SVs (deletion-insertion, deletion-inversion, and deletion-translocation composites), and complex genomic rearrangements (CGRs), including chromoplexy, chromothripsis, and SV by breakage-fusion-bridge cycles. Our findings suggest that 1 Gy IR exposure causes an average of 2.33 mutational events per Gb genome, comprising 2.15 indels, 0.17 SVs, and 0.01 CGRs, despite a high level of inter-cellular stochasticity. The mutational burden was dependent on total irradiation dose, regardless of dose rate or cell type. The findings were further validated in IR-induced secondary cancers and single cells without clonalization. Overall, our study highlights a comprehensive and clear picture of IR effects on normal mammalian genomes. © 2024 The Author(s)
Publisher
Cell Press
ISSN
2666-979X
DOI
10.1016/j.xgen.2024.100499
URI
https://scholar.gist.ac.kr/handle/local/9713
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