DNA base adducts in urine andwhite blood cells of cancer patients receiving combination chemotherapies which include<i>N</i>-methyl-<i>N</i>-nitrosourea

Virginie Prévost(Centre International de Recherche sur le Cancer), Alexei J. Likhachev(Institute of Oncology NN Petrov), N. Loktionova(Institute of Oncology NN Petrov), Helmut Bartsch(Centre International de Recherche sur le Cancer), Christopher P. Wild(Centre International de Recherche sur le Cancer), O. I. Kazanova(Institute of Oncology NN Petrov), Alexei Arkhipov(Centre International de Recherche sur le Cancer), М Л Гершанович(Centre International de Recherche sur le Cancer), David E. G. Shuker(Centre International de Recherche sur le Cancer)
Biomarkers
January 1, 1996
Cited by 8

Abstract

Abstract Urinary 3-methyladenine (3-MeAde) excretion andlymphocyte DNA adduct formation was studied in 15 patients receiving methylnitrosourea (MNU) at several dose levels (250 mg, 300 mg and600 mg total dose, 143-385 mg m(-2)) as part of various combination chemotherapies for advanced tumours (malignant melanoma, lymphoblastic lymphosarcorna andHodgkin's disease). Urinary 3-MeAde levels were significantly increased over background in patients at all dose levels (p < 0.001) andthe increases were dose-dependent (r = 0.77, p < 0.01). There were large interindividual variations in the excretion of 3-MeAde at each dose of MNU. In a subset of patients, N7-methyl-2-deoxyguanosine (7-MedG) andO(6)-methyl-2'-deoxyguanosine (O(6)-WedG) levels in DNA from blood leucocytes showed dose-dependent increases, however there were no simple relationships between urinary methylated DNA bases andleucocyte DNA adducts. Levels of adducts in leucocyte DNA (7-MedG, < 17-217 μmol mol(-1) dG; O(6)-WedG, < 1.6-35 μmol mol(-1) dG) were comparable with those reported for other methylating chemotherapeutic drugs. Leucocyte DNA andurinary methyl adducts may be useful markers of individual responses to treatment with methylating drugs.


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