Evaluation of the Xpa-Deficient Transgenic Mouse Model for Short-Term Carcinogenicity Testing: 9-Month Studies with Haloperidol, Reserpine, Phenacetin, and D-Mannitol
article
As part of the international evaluation program coordinated by ILSI/HESI, the potential of DNA repair deficient Xpa-/- mice and the double knockout Xpa-/-.p53+/- mice for short term carcinogenicity assays was evaluated. For comparison also wild-type C57BL/6 mice (WT) were included in these studies. Four test compounds were administered to groups of 15 male and 15 female Xpa-/- mice, Xpa -/-.p53+/- mice and WT mice for 39 weeks. The model compounds investigated were haloperidol, reserpine (nongenotoxic rodent carcinogens, putative human noncarcinogens), phenacetin (genotoxic rodent carcinogen, suspected human carcinogen), and D-mannitol (noncarcinogen in rodents and humans). The test compounds were administered as admixture to rodent diet at levels up to 25 mg/kg diet for haloperidol, 7.5 mg/kg diet for reserpine, 0.75% for phenacetin, and 10% for D-mannitol. These levels included the maximum tolerable dose (MTD). Survival was not affected with any of the test compounds. Haloperidol, reserpine and D-mannitol were negative in the carcinogenicity assay with Xpa-/- and Xpa-/-.p53 +/- mice, showing low and comparable tumor incidences in controls and high-dose animals. The results obtained with phenacetin may be designated equivocal in Xpa-/-.p53+/- mice, based on the occurrence of a single rare tumor in the target organ (kidney) accompanied by a low incidence of hyperplastic renal lesions and a high incidence of karyomegaly. These results are in agreement with the currently known carcinogenic potential of the 4 test compounds in humans.
Topics
Toxicology and Applied PharmacologyCarcinogenicity testingCarcinogensDNA repair deficientKnockout miceXpaXpa/p53HaloperidolMannitolPhenacetinReserpineAnimal experimentAnimal tissueCancer incidenceCarcinogen testingControlled studyDNA repairEvaluationFemaleHyperplasiaKidney tumorKnockout mouseMaleMaximum tolerated doseMouseNonhumanPriority journalRare diseaseSurvivalTarget organTransgenic mouseAdministration, OralAnimalsCarcinogenicity TestsDietDisease Models, AnimalDNA-Binding ProteinsDose-Response Relationship, DrugHaloperidolMannitolMiceMice, Inbred C57BLMice, KnockoutMice, TransgenicNeoplasms, ExperimentalPhenacetinReproducibility of ResultsReserpineTime FactorsXeroderma Pigmentosum Group A ProteinAnimaliaMus musculusRodentia
TNO Identifier
237631
ISSN
01926233
Source
Toxicologic Pathology, 32(2), pp. 192-201.
Pages
192-201
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