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用六价铬处理的 lacZ 转基因小鼠的骨髓和肝脏诱变

Bone marrow and liver mutagenesis in lacZ transgenic mice treated with hexavalent chromium.

作者信息

Itoh S, Shimada H

机构信息

Drug Safety Research Laboratory, Daiichi Pharmaceutical Co., Ltd., Tokyo, Japan.

出版信息

Mutat Res. 1998 Jan 13;412(1):63-7. doi: 10.1016/s1383-5718(97)00171-x.

Abstract

The mutagenic effects of the hexavalent chromium compound K2CrO4 in lacZ transgenic mice (Muta Mouse) were investigated at two sampling times. K2CrO4 was administered intraperitoneally to five male mice per treatment group at a single dose of 40 mg/kg. The animals were sacrificed on days 1 and 7 after the treatment. Mutant frequencies in the bone marrow and liver were analyzed by the positive selection method using Escherichia coli C (galE-) strain and phenyl beta-D-galactoside. K2CrO4 induced a significant increase in mutant frequency in the bone marrow on day 1, but not on day 7 after the treatment. In the liver, on the other hand, a significant induction in the mutant frequency was seen on day 7, whereas no induction was observed on day 1. The reason for the different responses to the mutagenic activity of K2CrO4 between these organs may be related to their cell turnover rates. The mutations induced by K2CrO4 in the bone marrow may have occurred in more differentiated cells than stem cells, and the rapid proliferative activity may have caused a rapid decrease in mutated cells by day 7. These results suggest that experiments on mutagenesis should be done with more than one sampling point, a short expression time in addition to a longer one, so as to detect mutations induced in organ with high cell proliferation.

摘要

在两个采样时间点研究了六价铬化合物重铬酸钾(K2CrO4)对lacZ转基因小鼠(Muta Mouse)的致突变作用。每个治疗组给五只雄性小鼠腹腔注射单剂量40mg/kg的K2CrO4。在治疗后的第1天和第7天处死动物。使用大肠杆菌C(galE-)菌株和苯基β-D-半乳糖苷通过阳性选择法分析骨髓和肝脏中的突变频率。K2CrO4在治疗后第1天诱导骨髓中的突变频率显著增加,但在第7天没有。另一方面,在肝脏中,在第7天观察到突变频率有显著诱导,而在第1天未观察到诱导。这些器官对K2CrO4诱变活性的不同反应的原因可能与其细胞更新率有关。K2CrO4在骨髓中诱导的突变可能发生在比干细胞更分化的细胞中,并且快速的增殖活性可能导致到第7天突变细胞迅速减少。这些结果表明,诱变实验应该在多个采样点进行,除了较长的表达时间外还应有较短的表达时间,以便检测在具有高细胞增殖的器官中诱导的突变。

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