N-Nitrosodi- n-propylamine induces organ specific mutagenesis with specific expression times in lacZ transgenic mice

N-Nitrosodi- n-propylamine induces organ specific mutagenesis with specific expression times in lacZ transgenic mice

The mutagenic and clastogenic effects of N-nitrosodi- n-propylamine (NDPA) in lacZ transgenic mice (Muta™Mouse) were investigated as a part of the second collaborative study of the transgenic mouse mutation assay by a subgroup of the Mammalian Mutagenesis Study Group, a suborganization of the Enviro...

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Veröffentlicht in:Mutation research 1999-08, Vol.444 (2), p.309-319
Hauptverfasser: Itoh, Satoru, Miura, Miki, Itoh, Toshiaki, Miyauchi, Yoshiteru, Suga, Miho, Takahashi, Yukimi, Kasahara, Yoshinori, Yamamura, Eiji, Hirono, Haruyoshi, Shimada, Hiroyasu
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Sprache:eng
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Animals
Biological and medical sciences
Carcinogens - toxicity
Chemical mutagenesis
Lac Operon
lacZ
lacZ gene
Male
Medical sciences
Mice
Mice, Transgenic
Micronucleus Tests
Mutagenesis
Mutagenicity
Mutagens - toxicity
Muta™Mouse
N-Nitrosodi- n-propylamine
Nitrosamines - toxicity
Organ Specificity
Toxicology
Transgenic mouse
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container_end_page 319
container_issue 2
container_start_page 309
container_title Mutation research
container_volume 444
creator Itoh, Satoru
Miura, Miki
Itoh, Toshiaki
Miyauchi, Yoshiteru
Suga, Miho
Takahashi, Yukimi
Kasahara, Yoshinori
Yamamura, Eiji
Hirono, Haruyoshi
Shimada, Hiroyasu
description The mutagenic and clastogenic effects of N-nitrosodi- n-propylamine (NDPA) in lacZ transgenic mice (Muta™Mouse) were investigated as a part of the second collaborative study of the transgenic mouse mutation assay by a subgroup of the Mammalian Mutagenesis Study Group, a suborganization of the Environmental Mutagen Society of Japan. Male Muta™Mouse mice were administered NDPA intraperitoneally at a dose of 250 mg/kg, which is half of the LD 50 of the compound. The clastogenicity of NDPA was examined by the peripheral blood micronucleus test just before and at 24, 48 and 72 h after the treatment. The mutant frequencies in the bone marrow, liver, lung, kidney and urinary bladder were examined by the positive selection method for lacZ mutations on days 7, 14 and 28 after treatment and in the testis on day 28. NDPA did not cause a significant increase in micronucleated reticulocytes in peripheral blood. In the mutation assay, NDPA showed a statistically significant increase in mutant frequencies in the liver, lung and kidney. No biologically meaningful increase in mutant frequency was observed in the bone marrow, urinary bladder or testis. The mutant frequency in the liver increased in a time-dependent manner, whereas in the lung and kidney the mutant frequencies on days 14 and 28 were almost equal. The order of mutagenic potency of NDPA was liver>lung> kidney. These findings demonstrate that NDPA induces organ-specific mutagenesis with specific expression times, and that the mutagenicity of NDPA in lacZ transgenic mice is consistent with its carcinogenicity.
doi_str_mv 10.1016/S1383-5718(99)00062-5
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Male Muta™Mouse mice were administered NDPA intraperitoneally at a dose of 250 mg/kg, which is half of the LD 50 of the compound. The clastogenicity of NDPA was examined by the peripheral blood micronucleus test just before and at 24, 48 and 72 h after the treatment. The mutant frequencies in the bone marrow, liver, lung, kidney and urinary bladder were examined by the positive selection method for lacZ mutations on days 7, 14 and 28 after treatment and in the testis on day 28. NDPA did not cause a significant increase in micronucleated reticulocytes in peripheral blood. In the mutation assay, NDPA showed a statistically significant increase in mutant frequencies in the liver, lung and kidney. No biologically meaningful increase in mutant frequency was observed in the bone marrow, urinary bladder or testis. The mutant frequency in the liver increased in a time-dependent manner, whereas in the lung and kidney the mutant frequencies on days 14 and 28 were almost equal. 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Male Muta™Mouse mice were administered NDPA intraperitoneally at a dose of 250 mg/kg, which is half of the LD 50 of the compound. The clastogenicity of NDPA was examined by the peripheral blood micronucleus test just before and at 24, 48 and 72 h after the treatment. The mutant frequencies in the bone marrow, liver, lung, kidney and urinary bladder were examined by the positive selection method for lacZ mutations on days 7, 14 and 28 after treatment and in the testis on day 28. NDPA did not cause a significant increase in micronucleated reticulocytes in peripheral blood. In the mutation assay, NDPA showed a statistically significant increase in mutant frequencies in the liver, lung and kidney. No biologically meaningful increase in mutant frequency was observed in the bone marrow, urinary bladder or testis. The mutant frequency in the liver increased in a time-dependent manner, whereas in the lung and kidney the mutant frequencies on days 14 and 28 were almost equal. 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Male Muta™Mouse mice were administered NDPA intraperitoneally at a dose of 250 mg/kg, which is half of the LD 50 of the compound. The clastogenicity of NDPA was examined by the peripheral blood micronucleus test just before and at 24, 48 and 72 h after the treatment. The mutant frequencies in the bone marrow, liver, lung, kidney and urinary bladder were examined by the positive selection method for lacZ mutations on days 7, 14 and 28 after treatment and in the testis on day 28. NDPA did not cause a significant increase in micronucleated reticulocytes in peripheral blood. In the mutation assay, NDPA showed a statistically significant increase in mutant frequencies in the liver, lung and kidney. No biologically meaningful increase in mutant frequency was observed in the bone marrow, urinary bladder or testis. The mutant frequency in the liver increased in a time-dependent manner, whereas in the lung and kidney the mutant frequencies on days 14 and 28 were almost equal. The order of mutagenic potency of NDPA was liver&gt;lung&gt; kidney. These findings demonstrate that NDPA induces organ-specific mutagenesis with specific expression times, and that the mutagenicity of NDPA in lacZ transgenic mice is consistent with its carcinogenicity.</abstract><cop>Amsterdam</cop><pub>Elsevier B.V</pub><pmid>10521671</pmid><doi>10.1016/S1383-5718(99)00062-5</doi><tpages>11</tpages></addata></record>
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identifier ISSN: 1383-5718
ispartof Mutation research, 1999-08, Vol.444 (2), p.309-319
issn 1383-5718
0027-5107
1879-3592
language eng
recordid cdi_proquest_miscellaneous_17411247
source MEDLINE; Access via ScienceDirect (Elsevier)
subjects Animals
Biological and medical sciences
Carcinogens - toxicity
Chemical mutagenesis
Lac Operon
lacZ
lacZ gene
Male
Medical sciences
Mice
Mice, Transgenic
Micronucleus Tests
Mutagenesis
Mutagenicity
Mutagens - toxicity
Muta™Mouse
N-Nitrosodi- n-propylamine
Nitrosamines - toxicity
Organ Specificity
Toxicology
Transgenic mouse
title N-Nitrosodi- n-propylamine induces organ specific mutagenesis with specific expression times in lacZ transgenic mice
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