High-throughput analysis of the mutagenic and cytotoxic properties of DNA lesions by next-generation sequencing

Yuan, Bi-Feng; Wang, Jianshuang; Cao, Huachuan; Sun, Ruobai; Wang, Yinsheng

doi:10.1093/nar/gkr159

Cited by 60 publications

(117 citation statements)

References 37 publications

Supporting

Mentioning

107

Contrasting

Order By: Relevance

“…This method enables the examination of the types and frequencies of lesion-induced errors generated by specific DNA polymerases. Although next-generation sequencing technology has previously been used to assess the mutagenic properties of carboxymethylated DNA lesions (22), only mutations opposite the lesion site were analyzed. In contrast, our design provides sequencing information for at least 10 template positions upstream and downstream from the DNA lesion site.…”

Section: Introductionmentioning

confidence: 99%

A high-throughput and quantitative method to assess the mutagenic potential of translesion DNA synthesis

Taggart¹,

Camerlengo²,

Harrison³

et al. 2013

Nucleic Acids Research

View full text Add to dashboard Cite

Cellular genomes are constantly damaged by endogenous and exogenous agents that covalently and structurally modify DNA to produce DNA lesions. Although most lesions are mended by various DNA repair pathways in vivo, a significant number of damage sites persist during genomic replication. Our understanding of the mutagenic outcomes derived from these unrepaired DNA lesions has been hindered by the low throughput of existing sequencing methods. Therefore, we have developed a cost-effective high-throughput short oligonucleotide sequencing assay that uses next-generation DNA sequencing technology for the assessment of the mutagenic profiles of translesion DNA synthesis catalyzed by any error-prone DNA polymerase. The vast amount of sequencing data produced were aligned and quantified by using our novel software. As an example, the high-throughput short oligonucleotide sequencing assay was used to analyze the types and frequencies of mutations upstream, downstream and at a site-specifically placed cis–syn thymidine–thymidine dimer generated individually by three lesion-bypass human Y-family DNA polymerases.

show abstract

Section: Introductionmentioning

confidence: 99%

A high-throughput and quantitative method to assess the mutagenic potential of translesion DNA synthesis

Taggart¹,

Camerlengo²,

Harrison³

et al. 2013

Nucleic Acids Research

View full text Add to dashboard Cite

show abstract

“…The cdA and cdG lesions have been found in γ-irradiated human cultured cells, 48, 49 and in humans. 50 The cyclopurine adducts are highly mutagenic 51, 52 and their accumulation in cellular DNA may contribute to the etiology of cancer and other diseases. 49, 53–55 The guanine – thymine tandem lesions, G[8-5m]T are formed by the addition of 5-(uracilyl) methyl radicals to the C8 position of guanine to form a radical adduct that is rapidly oxidized by traces of oxygen or other weak oxidants 56–60 .…”

Section: Resultsmentioning

confidence: 99%

Generation of guanine–amino acid cross-links by a free radical combination mechanism

Uvaydov

Geacintov

Shafirovich

2014

Phys. Chem. Chem. Phys.

View full text Add to dashboard Cite

A direct method has been developed for the in vitro synthesis of stable DNA – protein cross-links (DPC’s) between guanine and amino acids (lysine, arginine). This method employs the combination of guanine neutral radicals, G(-H)•, and side-chain C-centered amino acid radicals. The latter were generated indirectly after first causing the selective photoionization of 2-aminopurine (2AP) embedded in the oligonucleotide, 5’-d(CC[2AP]TCGCTACC) by intense nanosecond 308 nm excimer laser pulses. The 2AP radical cation deprotonates rapidly to form the 2AP(-H)• neutral radical which, in turn, oxidizes the nearby guanine to form the neutral guanine G(-H)• radical, as described previously (Shafirovich et al. J. Phys. Chem. B, 2001, 105, 8431). In parallel, the hydrated electrons generated by the photoionization of 2AP, are scavenged by nitrous oxide to generate hydroxyl radicals. In the presence of a large excess of the amino acids, the hydroxyl radicals oxidize the latter to produce C-centered amino acid radicals that combine with the G(-H)• radicals to form the guanine-amino acid cross-linked oligonucleotide product. Analogous products were generated by photoionizing the free nucleoside, 2’,3’,5’-tri-O-acetylguanoise, (tri-O-Ac-Guo) using intense nanosecond 266 nm Nd: Yag laser pulse irradiation. The guanine – amino acid cross-links thus produced either site-specifically positioned in oligonucleotides, or in the free nucleoside tri-O-Ac-Guo were isolated by HPLC methods and identified by high resolution LC-TOF/MS and LC-MS/MS methods. The possibility is discussed that analogous guanine-amino acid cross-linked products could be formed in vivo under single hit radical generation mechanisms during oxidative stress.

show abstract

“…Identification of different patterns of mutagenesis may provide insight into causal mechanisms behind the mutagenic process [26,43,[132][133][134] These data suggested an odds ratio of approximately 26 for developing SJS in individuals that are carriers of the HLA-A*3101 allele. Considering the effect size of this variant, it would likely be of value clinically to perform genotyping of patients prior to the administration of carbamazepine in order to limit the risk of SJS.…”

Section: Genomics Examplementioning

confidence: 99%

The Application of Omics Technologies to the Study of Mammalian Toxicology

Auerbach¹,

Merrick²

2015

Mammalian Toxicology

View full text Add to dashboard Cite

High-throughput analysis of the mutagenic and cytotoxic properties of DNA lesions by next-generation sequencing

Cited by 60 publications

References 37 publications

A high-throughput and quantitative method to assess the mutagenic potential of translesion DNA synthesis

A high-throughput and quantitative method to assess the mutagenic potential of translesion DNA synthesis

Generation of guanine–amino acid cross-links by a free radical combination mechanism

The Application of Omics Technologies to the Study of Mammalian Toxicology

Contact Info

Product

Resources

About