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Buters, J. ; Quintanilla-Martinez, L. ; Schober, W.* ; Soballa, V.J.* ; Hintermair, J. ; Wolff, T. ; Gonzalez, F.J.* ; Greim, H.*

CYP1B1 determines susceptibility to low doses of 7,12-dimethylbenz[a]anthracene-induced ovarian cancers in mice : Correlation of CYP1B1-mediated DNA adducts with carcinogenicity.

Carcinogenesis 24, 327-334 (2003)
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We showed previously that CYP1B1-null mice developed 10 times less lymphomas than wild-type mice after receiving 7,12-dimethylbenz[a]anthracene (DMBA). In this study a 10-fold lower dose was applied to differentiate between toxicity induced lymphomas (200 μg/mouse/day) and tumor initiation (20 μg/day). DMBA adducts to DNA of organs of mice, or to DNA of V79 cells expressing single mice or human cytochrome P450 isoenzymes were also measured. Mice were dosed three cycles of 5 days/week with DMBA in corn oil orally. Histopathology was determined at intermittent death or 1 year after dosing. DMBA–DNA adducts were assayed by 32P-postlabeling. At 20 μg/day, wild-type mice developed ovary (71%, stromal cells derived), skin (36%), uterus (64%) and lung (14%) hyperplasias. At this dose the CYP1B1-null mice developed no lymphomas, 25% ovary (epithelial cells derived), 8% skin, 58% uterus and 33% lung tumors. Oil control mice (n = 35) developed only eight, mostly different, hyperplasias. Wild-type mice had more DMBA–DNA adducts than the CYP1B1-null mice. The differences were highest in thymus, spleen, ovaries and testes (5–7-fold). Additionally, one specific DMBA–DNA adduct was reduced in CYP1B1-null mice. V79-cells expressed mouse CYP1B1 was 35 times more active than mouse CYP1A1 in forming DMBA–DNA adducts. Human CYP1B1 was 2.5 times less active than mouse CYP1B1 but 2.3-fold more active than human CYP1A1. CYP1B1 is the dominant enzyme in metabolizing DMBA to carcinogenic metabolites at high and low doses in mice, leading to an increased tumor rate of especially the ovaries at low doses of DMBA. Wild-type mice had more DMBA–DNA adducts than CYP1B1-null mice. Additionally, a specific adduct was less present in the CYP1B1-null mice. Human CYP1B1 was less active than mouse CYP1B1, but more active than human CYP1A1 in forming DMBA–DNA adducts. Thus, we expect CYP1B1 to be an important DMBA activating enzyme in humans also.
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Publikationstyp Artikel: Journalartikel
Dokumenttyp Wissenschaftlicher Artikel
Schlagwörter CYP1B1; DNA adducts
Sprache englisch
Veröffentlichungsjahr 2003
HGF-Berichtsjahr 2003
ISSN (print) / ISBN 0143-3334
e-ISSN 1460-2180
Zeitschrift Carcinogenesis
Quellenangaben Band: 24, Heft: 2, Seiten: 327-334 Artikelnummer: , Supplement: ,
Verlag Oxford University Press
Begutachtungsstatus Peer reviewed
Institut(e) Institute of Pathology (PATH)
Institute of Epidemiology (EPI)
Institute of Lung Health and Immunity (LHI)
Institute of Molecular Toxicology and Pharmacology (TOX)
POF Topic(s)
30202 - Environmental Health
30203 - Molecular Targets and Therapies
30504 - Mechanisms of Genetic and Environmental Influences on Health and Disease
Forschungsfeld(er) Enabling and Novel Technologies
PSP-Element(e) FE 70332
FE 73991
G-521200-001
G-505200-002
G-500300-001
DOI 10.1093/carcin/24.2.327
Erfassungsdatum 2003-03-10
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