Mutational signatures in tumours induced by high and low energy radiation in Trp53 deficient mice

Ionising radiation (IR) is a recognised carcinogen responsible for cancer development in patients previously treated using radiotherapy, and in individuals exposed as a result of accidents at nuclear energy plants. However, the mutational signatures induced by distinct types and doses of radiation a...

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Veröffentlicht in:Nature communications 2020-01, Vol.11 (1), p.394-15, Article 394
Hauptverfasser: Rose Li, Yun, Halliwill, Kyle D., Adams, Cassandra J., Iyer, Vivek, Riva, Laura, Mamunur, Rashid, Jen, Kuang-Yu, del Rosario, Reyno, Fredlund, Erik, Hirst, Gillian, Alexandrov, Ludmil B., Adams, David, Balmain, Allan
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Sprache:eng
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Zusammenfassung:Ionising radiation (IR) is a recognised carcinogen responsible for cancer development in patients previously treated using radiotherapy, and in individuals exposed as a result of accidents at nuclear energy plants. However, the mutational signatures induced by distinct types and doses of radiation are unknown. Here, we analyse the genetic architecture of mammary tumours, lymphomas and sarcomas induced by high ( 56 Fe-ions) or low (gamma) energy radiation in mice carrying Trp53 loss of function alleles. In mammary tumours, high-energy radiation is associated with induction of focal structural variants, leading to genomic instability and Met amplification. Gamma-radiation is linked to large-scale structural variants and a point mutation signature associated with oxidative stress. The genomic architecture of carcinomas, sarcomas and lymphomas arising in the same animals are significantly different. Our study illustrates the complex interactions between radiation quality, germline Trp53 deficiency and tissue/cell of origin in shaping the genomic landscape of IR-induced tumours. Mutational signatures induced by ionising radiation remain largely unexplored. Here in TP53 mutant mice, the authors characterise the genomic landscape of tumours induced by high- and low-energy radiation.
ISSN:2041-1723
2041-1723
DOI:10.1038/s41467-019-14261-4