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Publication : Signatures of TOP1 transcription-associated mutagenesis in cancer and germline.

First Author  Reijns MAM Year  2022
Journal  Nature Volume  602
Issue  7898 Pages  623-631
PubMed ID  35140396 Mgi Jnum  J:325942
Mgi Id  MGI:7288002 Doi  10.1038/s41586-022-04403-y
Citation  Reijns MAM, et al. (2022) Signatures of TOP1 transcription-associated mutagenesis in cancer and germline. Nature 602(7898):623-631
abstractText  The mutational landscape is shaped by many processes. Genic regions are vulnerable to mutation but are preferentially protected by transcription-coupled repair(1). In microorganisms, transcription has been demonstrated to be mutagenic(2,3); however, the impact of transcription-associated mutagenesis remains to be established in higher eukaryotes(4). Here we show that ID4-a cancer insertion-deletion (indel) mutation signature of unknown aetiology(5) characterized by short (2 to 5 base pair) deletions -is due to a transcription-associated mutagenesis process. We demonstrate that defective ribonucleotide excision repair in mammals is associated with the ID4 signature, with mutations occurring at a TNT sequence motif, implicating topoisomerase 1 (TOP1) activity at sites of genome-embedded ribonucleotides as a mechanistic basis. Such TOP1-mediated deletions occur somatically in cancer, and the ID-TOP1 signature is also found in physiological settings, contributing to genic de novo indel mutations in the germline. Thus, although topoisomerases protect against genome instability by relieving topological stress(6), their activity may also be an important source of mutations in the human genome.
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