The Chinese hamster FANCG/XRCC9 mutant NM3 fails to express the monoubiquitinated form of the FANCD2 protein, is hypersensitive to a range of DNA damaging agents and exhibits a normal level of spontaneous sister chromatid exchange

doi:10.1093/carcin/22.12.1939

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Carcinogenesis, Vol. 22, No. 12, 1939-1946, December 2001
© 2001 Oxford University Press

CANCER BIOLOGY

The Chinese hamster FANCG/XRCC9 mutant NM3 fails to express the monoubiquitinated form of the FANCD2 protein, is hypersensitive to a range of DNA damaging agents and exhibits a normal level of spontaneous sister chromatid exchange

James B. Wilson¹, Mark A. Johnson¹^,5, Anna P. Stuckert², Kelly L. Trueman¹, Simon May¹^,6, Peter E. Bryant³, Raymond E. Meyn⁴, Alan D. D'Andrea² and Nigel J. Jones¹^,7

¹ Mammalian DNA Repair Laboratory, School of Biological Sciences, Donnan Laboratories, University of Liverpool, Liverpool, L69 7ZD, UK,
² Department of Pediatric Oncology, Dana-Farber Cancer Institute and Department of Pediatrics, Children's Hospital, Harvard Medical School, 44 Binney Street, Boston, MA 02115, USA,
³ School of Biomedical Sciences, University of St. Andrews, St Andrews, KY16 9TS, UK
⁴ Department Experimental Radiation Oncology, MD Anderson Cancer Centre, 1515 Holcombe Boulevard, Box 066, Houston, Texas 77030, USA

Fanconi anemia (FA) is a human autosomal disorder characterizedby cancer susceptibility and cellular sensitivity to DNA crosslinkingagents such as mitomycin C and diepoxybutane. Six FA genes havebeen cloned including a gene designated XRCC9 (for X-ray RepairCross Complementing), isolated using a mitomycin C-hypersensitiveChinese hamster cell mutant termed UV40, and subsequently foundto be identical to FANCG. A nuclear complex containing the FANCA,FANCC, FANCE, FANCF and FANCG proteins is needed for the activationof a sixth FA protein FANCD2. When monoubiquitinated, the FANCD2protein co-localizes with the breast cancer susceptibility proteinBRCA1 in DNA damage induced foci. In this study, we have assignedNM3, a nitrogen mustard-hypersensitive Chinese hamster mutantto the same genetic complementation group as UV40. NM3, likehuman FA cell lines (but unlike UV40) exhibits a normal spontaneouslevel of sister chromatid exchange. We show that both NM3 andUV40 are also hypersensitive to other DNA crosslinking agents(including diepoxybutane and chlorambucil) and to non-crosslinkingDNA damaging agents (including bleomycin, streptonigrin andEMS), and that all these sensitivities are all corrected upontransfection of the human FANCG/XRCC9 cDNA. Using immunoblotting,NM3 and UV40 were found not to express the active monoubiquitinatedisoform of the FANCD2 protein, although expression of the FANCD-Lisoform was restored in the FANCG cDNA transformants, correlatingwith the correction of mutagen-sensitivity. These data indicatethat cellular resistance to these DNA damaging agents requiresFANCG and that the FA gene pathway, via its activation of FANCD2and that protein's subsequent interaction with BRCA1, is involvedin maintaining genomic stability in response not only to DNAinterstrand crosslinks but also a range of other DNA damagesincluding DNA strand breaks. NM3 and other `FA-like' Chinesehamster mutants should provide an important resource for thestudy of these processes in mammalian cells.

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