An in vivo analysis of MMC-induced DNA damage and its repair

doi:10.1093/carcin/bgi254

Carcinogenesis Advance Access originally published online on October 29, 2005
Carcinogenesis 2006 27(3):446-453; doi:10.1093/carcin/bgi254

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An in vivo analysis of MMC-induced DNA damage and its repair

Young-Ju Lee¹, Su-Jung Park^1,³, Samantha L.M. Ciccone², Chong-Rak Kim⁴ and Suk-Hee Lee^1,^3,^*

¹ Department of Biochemistry and Molecular Biology, ² Microbiology and ³ Walther Oncology Center, Indiana University School of Medicine, Indianapolis, IN 46202, USA and ⁴ Inje University, Kimhae, Korea

^* To whom correspondence should be addressed at: 1044 W. Walnut Street Room 153, Indiana University Cancer Research Institute, Indianapolis, IN 46202, USA. Tel: +1 317 278 3464; Fax: +1 317 274 8046; Email: slee{at}iupui.edu

Mitomycin C (MMC) induces various types of DNA damages thatcause significant cytotoxicity to cells. Accordingly, repairof MMC-induced damages involves multiple repair pathways suchas nucleotide excision repair, homologous recombination repairand translesion bypass repair pathways. Nonetheless, repairof the MMC-induced DNA damages in mammals have not been fullydelineated. In this study, we investigated potential roles forXeroderma pigmentosum (XP) proteins in the repair of MMC-inducedDNA damages using an assay that detects the ssDNA patches generatedfollowing treatment with MMC or 8'-methoxy-psoralen (8-MOP)+ UVA (ultraviolet light A). Human wild-type cells formed distinctivessDNA foci following treatment with MMC or 8-MOP + UVA, butnot with those inducing alkylation damage, oxidative damageor strand-break damage, suggesting that the foci represent ssDNApatches formed during the crosslink repair. In contrast to wild-typecells, mutant defective in XPE orXPG did not form the ssDNAfoci following MMC treatment, while XPF mutant cells showeda significantly delayed response in forming the foci. A positiverole for XPG in the repair of MMC-induced DNA damages was furthersupported by observations that cells treated with MMC induceda tight association of XPG with chromatin, and a targeted inhibitionof XPG abolished MMC-induced ssDNA foci formation, renderingcells hypersensitive to MMC. Together, our results suggest thatXPG along with XPE and XPF play unique role(s) in the repairof MMC-induced DNA damages.

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