Nucleotide excision repair modulates the cytotoxic and mutagenic effects of N-n-butyl-N-nitrosourea in cultured mammalian cells as well as in mouse splenocytes in vivo

doi:10.1093/mutage/14.3.317

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Mutagenesis, Vol. 14, No. 3, 317-322, May 1999
© 1999 UK Environmental Mutagen Society/Oxford University Press

Nucleotide excision repair modulates the cytotoxic and mutagenic effects of N-n-butyl-N-nitrosourea in cultured mammalian cells as well as in mouse splenocytes in vivo

Sandra A.M. Bol¹, Harry van Steeg², Conny Th.M. van Oostrom², Ad D. Tates¹^,3, Harry Vrieling¹^,3, Anton J.L. de Groot¹^,3, Leon H.F. Mullenders¹^,3^,4, Albert A. van Zeeland¹^,3 and Jacob G. Jansen¹

¹ MGC–Department of Radiation Genetics and Chemical Mutagenesis, Leiden University, PO Box 9503, 2300 RA Leiden, ² National Institute of Public Health and the Environment, Department of Carcinogenesis, Mutagenesis and Genetics, Bilthoven and ³ J.A.Cohen Institute, Interuniversity Research Institute for Radiopathology and Radiation Protection, Leiden, The Netherlands

The butylating agent N-n-butyl-N-nitrosourea (BNU) was employedto study the role of nucleotide excision repair (NER) in protectingmammalian cells against the genotoxic effects of monofunctionalalkylating agents. The direct acting agent BNU was found tobe mutagenic in normal and XPA mouse splenocytes after a singlei.p. treatment in vivo. After 25 and 35 mg/kg BNU, but not after75 mg/kg, 2- to 3-fold more hprt mutants were detected in splenocytesfrom XPA mice than from normal mice. Using O⁶-alkylguanine-DNAalkyltransferase (AGT)-deficient hamster cells, it was foundthat NER-deficient CHO UV5 cells carrying a mutation in theERCC-2 gene were 40% more mutable towards lesions induced byBNU when compared with parental NER-proficient CHO AA8 cells.UV5 cells were 1.4-fold more sensitive to the cytotoxic effectsof BNU compared with AA8 cells. To investigate whether thisincreased sensitivity of NER-deficient cells is modulated byAGT activity, cell survival studies were performed in humanand mouse primary fibroblasts as well. BNU was 2.7-fold moretoxic for mouse XPA fibroblasts compared with normal mouse fibroblasts.Comparable results were found for human fibroblasts. Taken togetherthese data indicate that the role of NER in protecting rodentcells against the mutagenic and cytotoxic effects of the alkylatingagent BNU depends on AGT.

⁴ To whom correspondence should be addressed. Tel: +31 71 5276126;Fax: +31 71 5221615; Email: mullenders{at}rullf2.medfac.leidenuniv.nl

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