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

机译:口服重铬酸钠的小鼠突变频率不会增加

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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.
机译:通过转基因小鼠基因突变测定法检查了六价铬在小肠中的体内诱变性,所述六价铬是致肿瘤性的靶器官。将重铬酸钠二水合物在饮用水中以85.7或257.4mg / L的剂量口服给予雄性gpt delta小鼠28天,或以8.6、28.6或85.7mg / L的剂量口服90天。在28天或90天的研究中,小肠中的gpt突变体频率相对于对照小鼠均没有显着增加,而阳性对照物质溴酸钾的28天口服给药则增加了突变体频率。

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