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Literature DB >> 20471330

XRCC1 deficiency influences the cytotoxicity and the genomic instability induced by Me-lex, a specific inducer of N3-methyladenine.

Debora Russo¹, Gilberto Fronza, Laura Ottaggio, Paola Monti, Chiara Perfumo, Alberto Inga, Prema Iyer, Barry Gold, Paola Menichini.

Abstract

Me-lex is a sequence-specific alkylating agent synthesized to preferentially (>90%) generate N3-methyladenine (3-mA) in the minor groove of double-strand DNA, in A-T rich regions. In this paper we investigated the effect of XRCC1 deficiency in the processing of 3-mA adducts generated by Me-lex, through the molecular analysis of the Hprt mutations and the evaluation of cytogenetic end points such as sister chromatid exchanges (SCEs), micronuclei (MN) and nucleus fragmentation. EM-C11 cells, deficient in XRCC1 activity, showed a 2.5-fold higher sensitivity to the toxicity of Me-lex compared to the DNA repair proficient parental CHO-9 cells, but were not hyper mutable. The spontaneous mutation spectrum at the Hprt locus generated in EM-C11 cells revealed a high percentage of genomic deletions. After Me-lex treatment, the percentage of genomic deletions did not increase, but a class of mutations which appeared to target regulatory regions of the gene significantly increased (p=0.0277), suggesting that non-coding Hprt genomic sequences represent a strong target for the rare mutations induced by Me-lex. The number of SCEs per chromosome increased 3-fold above background in 50mucapital EM, Cyrillic Me-lex treated CHO-9 cells, while at higher Me-lex concentrations a sharp increase in the percentage of MN and fragmented nuclei was observed. In EM-C11 cells the background level of SCEs (0.939+/-0.182) was approximately 10-fold higher than in CHO-9 (0.129+/-0.027) and higher levels of multinucleated cells and MN were also found. In EM-C11, even low doses of Me-lex (25microM) led to a significant increase in genomic damage. These results indicate that XRCC1 deficiency can lead to genomic instability even in the absence of an exogenous genotoxic insult and low levels of Me-lex-induced lesions, i.e., 3-mA and/or a BER intermediate, can exacerbate this instability. 2010 Elsevier B.V. All rights reserved.

Entities: CellLine Chemical Disease Gene Species

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Year: 2010 PMID： 20471330 PMCID： PMC2893271 DOI： 10.1016/j.dnarep.2010.03.016

Source DB: PubMed Journal: DNA Repair (Amst) ISSN： 1568-7856

41 in total

Review 1. XRCC1 keeps DNA from getting stranded.

Authors: L H Thompson; M G West
Journal: Mutat Res Date: 2000-02-16 Impact factor: 2.433

2. Evidence in Escherichia coli that N3-methyladenine lesions induced by a minor groove binding methyl sulfonate ester can be processed by both base and nucleotide excision repair.

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Journal: Biochemistry Date: 2001-02-13 Impact factor: 3.162

3. Mutagenicity of N3-methyladenine: a multi-translesion polymerase affair.

Authors: Paola Monti; Ilaria Traverso; Laura Casolari; Paola Menichini; Alberto Inga; Laura Ottaggio; Debora Russo; Prema Iyer; Barry Gold; Gilberto Fronza
Journal: Mutat Res Date: 2010-01-05 Impact factor: 2.433

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Journal: Mutat Res Date: 2000-11-20 Impact factor: 2.433

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Authors: Debora Russo; Gilberto Fronza; Laura Ottaggio; Paola Monti; Alberto Inga; Prema Iyer; Barry Gold; Paola Menichini
Journal: Mutat Res Date: 2009-09-01 Impact factor: 2.433

Review 9. Mechanisms and consequences of methylating agent-induced SCEs and chromosomal aberrations: a long road traveled and still a far way to go.

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Journal: EMBO J Date: 1984-11 Impact factor: 11.598

1 in total

Review 1. Variant base excision repair proteins: contributors to genomic instability.

Authors: Antonia A Nemec; Susan S Wallace; Joann B Sweasy
Journal: Semin Cancer Biol Date: 2010-10-16 Impact factor: 15.707

1 in total