Mutagenicity of a unique thymine-thymine dimer or thymine-thymine pyrimidine pyrimidone (6-4) photoproduct in mammalian cells

Gentil, A.; Page, Florence Le; Margot, A.; Lawrence, Christopher W.; Borden, Angela; Sarasin, Alain

doi:10.1093/nar/24.10.1837

Cited by 77 publications

(57 citation statements)

References 27 publications

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“…This is consistent with the results that we have previously obtained with nonreplicating gapped plasmids in mammalian cells (28,41) and with an earlier report using a replicative plasmid (42). A recent study reported that TLS across a TT 6-4 PP in a replicating plasmid is largely accurate (43).…”

Section: Discussionsupporting

confidence: 93%

“…A recent study reported that TLS across a TT 6-4 PP in a replicating plasmid is largely accurate (43). This difference does not stem from a replicative vs. a gapped nonreplicating plasmid as those authors suggested, because an earlier study using a replicative plasmid found that TLS is highly mutagenic (42), like in our study. The reason for the difference is not known yet, but it should be pointed out that the TLS that we have monitored across chromosomal TT 6-4 PP was highly mutagenic.…”

Section: Discussionsupporting

confidence: 78%

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Genomic assay reveals tolerance of DNA damage by both translesion DNA synthesis and homology-dependent repair in mammalian cells

Izhar

Ziv

Cohen

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

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DNA lesions can block replication forks and lead to the formation of single-stranded gaps. These replication complications are mitigated by DNA damage tolerance mechanisms, which prevent deleterious outcomes such as cell death, genomic instability, and carcinogenesis. The two main tolerance strategies are translesion DNA synthesis (TLS), in which low-fidelity DNA polymerases bypass the blocking lesion, and homology-dependent repair (HDR; postreplication repair), which is based on the homologous sister chromatid. Here we describe a unique high-resolution method for the simultaneous analysis of TLS and HDR across defined DNA lesions in mammalian genomes. The method is based on insertion of plasmids carrying defined site-specific DNA lesions into mammalian chromosomes, using phage integrase-mediated integration. Using this method we show that mammalian cells use HDR to tolerate DNA damage in their genome. Moreover, analysis of the tolerance of the UV light-induced 6-4 photoproduct, the tobacco smokeinduced benzo[a]pyrene-guanine adduct, and an artificial trimethylene insert shows that each of these three lesions is tolerated by both TLS and HDR. We also determined the specificity of nucleotide insertion opposite these lesions during TLS in human genomes. This unique method will be useful in elucidating the mechanism of DNA damage tolerance in mammalian chromosomes and their connection to pathological processes such as carcinogenesis.error-prone DNA repair | homologous recombination repair | recombinational repair D NA damage is abundant, caused by both external agents such as sunlight and tobacco smoke and intracellular byproducts of metabolism, amounting to about 50,000 lesions per day per cell (1). Despite the presence of effective DNA repair mechanisms that eliminate lesions and restore the original DNA sequence, DNA replication often encounters unrepaired lesions that have escaped repair. These DNA damages may cause arrest of replication forks and the generation of postreplication gaps (2, 3). To complete replication and prevent the formation of double-strand breaks, which are highly deleterious, cells use DNA damage tolerance (DDT) mechanisms. These include translesion DNA synthesis (TLS) and homology-dependent repair (HDR), which enable bypass of the lesions and completion of replication, without removing the lesions from DNA. HDR uses the sequence from the intact sister chromatid to patch the single-stranded template region carrying the lesion. [We term HDR the pathways of DNA damage tolerance that rely on the homologous sister chromatid, also termed postreplication repair (PRR), damage avoidance, template switch, copy choice recombination, and homologous recombination repair.] This is carried out either by physical transfer of the segment complementary to the damaged template [also termed homologous recombination repair (HRR)] or by copying the complementary strand from the sister chromatid (template switch or postreplication repair). TLS employs specialized low-fidelity DNA polymerases to replicate across ...

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Section: Discussionsupporting

confidence: 93%

Section: Discussionsupporting

confidence: 78%

Genomic assay reveals tolerance of DNA damage by both translesion DNA synthesis and homology-dependent repair in mammalian cells

Izhar

Ziv

Cohen

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

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“…Most notably, an elevated UV-induced skin cancer proneness has been found for XPCÀ/À mice (29), which are TCR proficient and differ from the WT mice by the absence of 6-4PP GGR (20). In this respect, it is worth noting that mutagenic bypass of 6-4PPs in mammalian cells has been reported to be >10 times higher than for CPDs (46). The similar delay in repair of 6-4PPs in both human and mouse cells deficient for DDB2 suggests that the accelerating role of DDB2 in 6-4PP repair might also be important in the protection of humans against UV-induced skin cancer.…”

Section: Ddb2 Protects Mice From Uv-induced Skin Cancermentioning

confidence: 99%

Enhanced DDB2 Expression Protects Mice from Carcinogenic Effects of Chronic UV-B Irradiation

et al. 2005

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UV-damaged DNA-binding protein (UV-DDB) is essential for global genome repair (GGR) of UV-induced cyclobutane pyrimidine dimers (CPD). Unlike human cells, rodent epidermal cells are deficient in GGR of CPDs and express a subunit of UV-DDB, DDB2, at a low level. In this study, we generated mice (K14-DDB2) ectopically expressing mouse DDB2 at elevated levels. Enhanced expression of DDB2 both delayed the onset of squamous cell carcinoma and decreased the number of tumors per mouse in chronically UV-B light-exposed hairless mice. Enhanced expression of DDB2 improved repair of both CPDs and pyrimidine(6-4)pyrimidone photoproducts (6-4PP) in dermal fibroblasts. However, GGR of CPDs in K14-DDB2 mice did not reach the level of efficiency of human cells, suggesting that another repair protein may become rate limiting when DDB2 is abundantly present. To complement these studies, we generated mice in which the DDB2 gene was disrupted. DDB2À/À and DDB2+/À mice were found to be hypersensitive to UV-induced skin carcinogenesis. On the cellular level, we detected a delay in the repair of 6-4PPs in DDB2À/À dermal fibroblasts. Neither the absence nor the enhanced expression of DDB2 affected the levels of UV-induced apoptosis in epidermal keratinocytes or cultured dermal fibroblasts. Our results show an important role for DDB2 in the protection against UVinduced cancer and indicate that this protection is most likely mediated by accelerating the repair of photolesions. (Cancer Res 2005; 65(22): 10298-306)

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“…2). However, most of the UV-induced mutations at TT sequences are T-A-to-C-G transitions at the 3Ј T-A base pair (19,32). Therefore, in addition to the 5Ј T-G mismatches in our TϽϾT compound lesions, we wished to use 3Ј T-G-associated compound lesions to ascertain that the preferential repair of compound TϽϾT lesions contributes to UV mutagenesis.…”

Section: Fig 1 Incision/excision Of Tͻͼt and T[6-4]t Photoproducts mentioning

confidence: 99%

Recognition and Repair of Compound DNA Lesions (Base Damage and Mismatch) by Human Mismatch Repair and Excision Repair Systems

Tursun

Duckett

et al. 1997

Molecular and Cellular Biology

184

133

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Nucleotide excision repair and the long-patch mismatch repair systems correct abnormal DNA structures arising from DNA damage and replication errors, respectively. DNA synthesis past a damaged base (translesion replication) often causes misincorporation at the lesion site. In addition, mismatches are hot spots for DNA damage because of increased susceptibility of unpaired bases to chemical modification. We call such a DNA lesion, that is, a base damage superimposed on a mismatch, a compound lesion. To learn about the processing of compound lesions by human cells, synthetic compound lesions containing UV photoproducts or cisplatin 1,2-d(GpG) intrastrand cross-link and mismatch were tested for binding to the human mismatch recognition complex hMutS␣ and for excision by the human excision nuclease. No functional overlap between excision repair and mismatch repair was observed. The presence of a thymine dimer or a cisplatin diadduct in the context of a G-T mismatch reduced the affinity of hMutS␣ for the mismatch. In contrast, the damaged bases in these compound lesions were excised three-to fourfold faster than simple lesions by the human excision nuclease, regardless of the presence of hMutS␣ in the reaction. These results provide a new perspective on how excision repair, a cellular defense system for maintaining genomic integrity, can fix mutations under certain circumstances.Mismatches in DNA resulting from replication errors, and base damage caused by physical (UV light) and chemical (polyaromatic hydrocarbons) agents, are responsible for the majority of human cancers (18). Although certain mismatches and base lesions can be eliminated from DNA by the base excision repair pathway initiated by glycosylases with narrow substrate ranges, in human cells there exists a general mismatch repair system and a general damage repair system of wide substrate range. The mismatch repair system removes the mismatched base as a nucleotide (44), and the excision repair system excises the damaged base(s) in an oligonucleotide (52, 67).The general mismatch repair system (long-patch mismatch repair) corrects all eight single-base mismatches as well as small insertion sequence loops with comparable efficiencies (31, 44). The general nucleotide excision repair (excision repair) system (8) not only is the sole repair pathway for bulky lesions such as thymine dimers (TϽϾT) and cisplatin-guanine adducts but also repairs a wide variety of nonbulky lesions such as O 6 -methylguanine (O 6 -meG) at physiologically relevant rates (52). Thus, it appears that both repair systems recognize many dissimilar non-B DNA forms rather than a specific lesion structure.Given the wide substrate ranges of both systems, it is not unreasonable to expect overlaps between the two substrate spectra, or that one repair system may facilitate the function of the other. Indeed, it has been shown that the excision repair system recognizes mismatches and removes the mismatched base in a manner identical to the removal of damaged bases (27). Since a DNA lesion, by de...

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Mutagenicity of a unique thymine-thymine dimer or thymine-thymine pyrimidine pyrimidone (6-4) photoproduct in mammalian cells

Cited by 77 publications

References 27 publications

Genomic assay reveals tolerance of DNA damage by both translesion DNA synthesis and homology-dependent repair in mammalian cells

Genomic assay reveals tolerance of DNA damage by both translesion DNA synthesis and homology-dependent repair in mammalian cells

Enhanced DDB2 Expression Protects Mice from Carcinogenic Effects of Chronic UV-B Irradiation

Recognition and Repair of Compound DNA Lesions (Base Damage and Mismatch) by Human Mismatch Repair and Excision Repair Systems

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