Glycidamide-induced hypermutation in yeast single-stranded DNA reveals a ubiquitous clock-like mutational motif in humans

Author:

Hudson Kathleen M1,Klimczak Leszek J2ORCID,Sterling Joan F1,Burkholder Adam B3,Kazanov Marat D45ORCID,Saini Natalie6ORCID,Mieczkowski Piotr A7,Gordenin Dmitry A1ORCID

Affiliation:

1. Genome Integrity and Structural Biology Laboratory, National Institute of Environmental Health Sciences, US National Institutes of Health , Durham , NC 27709, USA

2. Integrative Bioinformatics Support Group, National Institute of Environmental Health Sciences, US National Institutes of Health , Durham , NC 27709, USA

3. Office of Environmental Science Cyberinfrastructure, National Institute of Environmental Health Sciences, US National Institutes of Health , Durham , NC 27709, USA

4. Faculty of Engineering and Natural Sciences, Sabanci University , Istanbul , 34956, Turkey

5. Skolkovo Institute of Science and Technology , Moscow 121205,  Russia

6. Department of Biochemistry & Molecular Biology, Medical University of South Carolina , Charleston , SC, 29425 , USA

7. Department of Genetics, School of Medicine, University of North Carolina , Chapel Hill, NC 27599, USA

Abstract

Abstract Mutagens often prefer specific nucleotides or oligonucleotide motifs that can be revealed by studying the hypermutation spectra in single-stranded (ss) DNA. We utilized a yeast model to explore mutagenesis by glycidamide, a simple epoxide formed endogenously in humans from the environmental toxicant acrylamide. Glycidamide caused ssDNA hypermutation in yeast predominantly in cytosines and adenines. The most frequent mutations in adenines occurred in the nAt→nGt trinucleotide motif. Base substitutions A→G in this motif relied on Rev1 translesion polymerase activity. Inactivating Rev1 did not alter the nAt trinucleotide preference, suggesting it may be an intrinsic specificity of the chemical reaction between glycidamide and adenine in the ssDNA. We found this mutational motif enriched in published sequencing data from glycidamide-treated mouse cells and ubiquitous in human cancers. In cancers, this motif was positively correlated with the single base substitution (SBS) smoking-associated SBS4 signature, with the clock-like signatures SBS1, SBS5, and was strongly correlated with smoking history and with age of tumor donors. Clock-like feature of the motif was also revealed in cells of human skin and brain. Given its pervasiveness, we propose that this mutational motif reflects mutagenic lesions to adenines in ssDNA from a potentially broad range of endogenous and exogenous agents.

Funder

National Institutes of Health

NIH

Publisher

Oxford University Press (OUP)

Subject

Genetics

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