Mutant Frequency is not Increased in Mice Orally Exposed to Sodium Dichromate.

Food safety (Tokyo, Japan) Pub Date : 2019-03-13 eCollection Date: 2019-03-01 DOI:10.14252/foodsafetyfscj.2018014
Yasunobu Aoki, Michiyo Matsumoto, Michi Matsumoto, Kenichi Masumura, Takehiko Nohmi
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Abstract

The in vivo mutagenicity of hexavalent chromium in the small intestine, the target organ of tumorgenicity, was examined by means of a transgenic mouse gene mutation assay. Sodium dichromate dihydrate was administered orally in drinking water to male gpt delta mice at a dose of 85.7 or 257.4 mg/L for 28 days or at a dose of 8.6, 28.6 or 85.7 mg/L for 90 days. No significant increase in gpt mutant frequency relative to that in control mice was observed in the small intestine in either the 28- or 90-day study, whereas 28-day oral administration of potassium bromate, a positive control substance, increased mutant frequency.

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小鼠口服重铬酸钠不会增加突变频率
通过转基因小鼠基因突变试验,研究了六价铬在小肠这一肿瘤靶器官中的体内致突变性。雄性 gpt delta 小鼠在饮用水中口服二水重铬酸钠,剂量为 85.7 或 257.4 毫克/升,持续 28 天;或剂量为 8.6、28.6 或 85.7 毫克/升,持续 90 天。在 28 天或 90 天的研究中,与对照组小鼠相比,在小肠中未观察到 gpt 突变体频率的明显增加,而口服溴酸钾(一种阳性对照物质)28 天后,突变体频率有所增加。
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