Kinetics of induction of DNA damage and lacZ gene mutations in stomach mucosa of mice treated with beta-propiolactone and N-methyl-N'-nitro-N-nitrosoguanidine, using single-cell gel electrophoresis and MutaMouse models.

Brault D; Renault D; Tombolan F; Thybaud V

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Kinetics of induction of DNA damage and lacZ gene mutations in stomach mucosa of mice treated with beta-propiolactone and N-methyl-N'-nitro-N-nitrosoguanidine, using single-cell gel electrophoresis and MutaMouse models.

机译：使用单细胞凝胶电泳和MutaMouse模型，在用β-丙内酯和N-甲基-N'-硝基-N-亚硝基胍处理的小鼠的胃黏膜中诱导DNA损伤和lacZ基因突变的动力学。

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beta-Propiolactone (BPL) and N-methyl-N'-nitro-N-nitrosoguanidine (MNNG) are two direct alkylating agents that induce multiple genetic lesions and tumors in the rodent stomach. We measured the kinetics of the induction of DNA damage by using the single-cell gel electrophoresis assay (SCGE) and the induction of gene mutations by using the MutaMouse model in the glandular stomach mucosa of mice exposed to a single oral administration of BPL or MNNG. The aims were to determine the optimal sampling time and to investigate the cause-effect relationship between DNA damage and gene mutations. The induction of comets, evaluated in individual cells with the tail moment, was analyzed 1, 2, 4, 24, and 72 hr after a single oral administration of 25 mg/kg BPL or 20 mg/kg MNNG. The effects of both compounds were most intense at the earlier sampling times (1-2 hr), tailing off 4 hr after treatment and becoming undetectable at 72 hr. The lacZ mutant frequency (MF) was measured 3, 7, 14, 28, and 50 days after a single oral administration of 150 mg/kg BPL or 100 mg/kg MNNG, and 3 and 14 days after a single administration of 25 mg/kg BPL or 20 mg/kg MNNG. The MF was strongly enhanced at the highest doses and all sampling times, the most marked effects being observed 14 days (11.1-fold) and 28 days (19.0-fold) after BPL and MNNG administration, respectively. At the lowest doses, only a small increase in MF ( approximately 2.5- to 3.5-fold) was found at both sampling times. Primary DNA damage detected with SCGE shortly after treatment (1-2 hr) was rapidly (3 days) transformed into stable gene mutations that remained detectable for 50 days. These results illustrate the ability and complementarity of the SCGE and MutaMouse models to assess the genotoxicity of direct alkylating agents in the mouse gastric mucosa in vivo. Copyright 1999 Wiley-Liss, Inc.

机译：β-丙内酯（BPL）和N-甲基-N'-硝基-N-亚硝基胍（MNNG）是两种直接的烷基化剂，可在啮齿动物的胃中诱发多种遗传性病变和肿瘤。我们通过使用单细胞凝胶电泳测定（SCGE）和单独使用BPL或MNNG口服暴露的小鼠腺胃黏膜中的MutaMouse模型，通过使用MutaMouse模型测量了DNA损伤诱导的动力学和基因突变的诱导。目的是确定最佳采样时间，并研究DNA损伤与基因突变之间的因果关系。在单次口服25 mg / kg BPL或20 mg / kg MNNG的1、2、4、24和72小时后，对在单个细胞中带有尾矩的彗星诱导进行了分析。两种化合物的作用在更早的采样时间（1-2小时）最为强烈，在处理后4小时逐渐消失，在72小时后变得无法检测到。 lacZ突变体频率（MF）在单次口服150 mg / kg BPL或100 mg / kg MNNG的第3、7、14、28和50天，以及单次口服25 mg的第3和14天后测量/ kg BPL或20 mg / kg MNNG。在最高剂量和所有采样时间下，MF均得到了强烈增强，分别在BPL和MNNG施用后14天（11.1倍）和28天（19.0倍）观察到了最明显的影响。在最低剂量下，两个采样时间的MF仅有少量增加（大约2.5到3.5倍）。用SCGE在治疗后不久（1-2小时）检测到的初级DNA损伤迅速（3天）转化为稳定的基因突变，该突变在50天内仍可检测到。这些结果说明了SCGE和MutaMouse模型评估小鼠体内胃黏膜中直接烷基化剂的遗传毒性的能力和互补性。版权所有1999 Wiley-Liss，Inc.

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《Environmental and molecular mutagenesis.》 |1999年第3期|共8页
作者
Brault D; Renault D; Tombolan F; Thybaud V;
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正文语种 eng
中图分类医学遗传学;
关键词
DNA Damage; Gastric Mucosa; Lac Operon; Methylnitronitrosoguanidine; Mutation; DNA损伤; 胃粘膜; 乳糖操纵子; 甲硝基亚硝胍; 突变; 丙内酯;

机译：DNA Damage;Gastric Mucosa;Lac Operon;Methylnitronitrosoguanidine;Mutation;DNA损伤;胃粘膜;乳糖操纵子;甲硝基亚硝胍;突变;丙内酯;

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1. Kinetics of induction of DNA damage and lacZ gene mutations in stomach mucosa of mice treated with beta-propiolactone and N-methyl-N'-nitro-N-nitrosoguanidine, using single-cell gel electrophoresis and MutaMouse models. [J] . Brault D, Renault D, Tombolan F, Environmental and molecular mutagenesis. . 1999,第2a3期

机译：使用单细胞凝胶电泳和MutaMouse模型，在用β-丙内酯和N-甲基-N'-硝基-N-亚硝基胍处理的小鼠的胃黏膜中诱导DNA损伤和lacZ基因突变的动力学。
2. Induction of glandular stomach cancers in Helicobacter pylori-sensitive Mongolian gerbils treated with N-methyl-N-nitrosourea and N-methyl-N'-nitro-N-nitrosoguanidine in drinking water. [J] . Tatematsu M, Yamamoto M, Shimizu N, Japanese Journal of Cancer Research . 1998,第2期

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3. Comparison of the mutational spectra of the lacZ transgene in four organs of the MutaMouse treated with benzo(a)pyrene: target organ specificity. [J] . Hakura A, Tsutsui Y, Sonoda J, Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects . 2000,第2期

机译：苯并（a）py处理的MutaMouse四个器官中lacZ转基因的突变谱比较：目标器官特异性。
4. Silver Nanoparticles and Carbon Nanotubes Induced DNA Damage in Mice Evaluated by Single Cell Gel Electrophoresis [C] . Kumud Kant Awasthi, Anjali Awasthi, Rajbala Verma International conference on Soft Materials . 2015

机译：银纳米粒子和碳纳米管通过单细胞凝胶电泳评估的小鼠中的DNA损伤诱导
5. Induction of circles of heterogeneous sizes in carcinogen-treated cells: two-dimensional gel analysis of circular DNA molecules. [O] . S Cohen, S Lavi 1996

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6. Detection of gene mutation in skin, stomach and liver of MutaTMMouse following oral or topical treatment with N-methyl-N'-nitro-N-nitrosoguanidine or 1-chloromethylpyrene: some preliminary observations [O] . T. M. Brooks, S. W. Dean 1996

机译：用N-甲基-N'-硝基 - N-硝基胍或1-氯甲基芘的口服或局部处理后皮肤，胃和肝脏皮肤，胃和肝脏的基因突变检测：一些初步观察

Kinetics of induction of DNA damage and lacZ gene mutations in stomach mucosa of mice treated with beta-propiolactone and N-methyl-N'-nitro-N-nitrosoguanidine, using single-cell gel electrophoresis and MutaMouse models.

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