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首页> 外文期刊>Environmental and molecular mutagenesis. >Induction of lacZ mutations in MutaMouse primary hepatocytes.
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Induction of lacZ mutations in MutaMouse primary hepatocytes.

机译:MutaMouse原代肝细胞中lacZ突变的诱导。

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摘要

We have developed an in vitro mutation assay using primary hepatocytes from the transgenic MutaMouse. Primary hepatocytes were isolated using a two-step perfusion method with purification by Percoll, cultured, and treated with benzo[a]pyrene (BaP), 2-amino-1-methyl-6-phenyl- imidazo[4,5-b]pyridine (PhIP), 3-nitrobenzoanthrone (3-NBA), and cigarette smoke condensate (CSC). The mean lacZ mutant frequency (MF) for the solvent control was approximately twofold greater than the spontaneous MF observed in liver tissue. A concentration-dependent increase in MF (up to 3.7-fold above control) was observed following exposure to BaP. Fourfold and twofold increases in mutant frequency were observed for 3-NBA and PhIP exposures, respectively, without the addition of any exogenous metabolic activation. A slight but statistically significant increase in lacZ MF was observed for CSC, but only at the lowest concentration. This is the first report demonstrating that mutations can be detected in cultured primary hepatocytes from MutaMouse. The preliminary results presented suggest that the MutaMouse primary hepatocyte mutagenicity assay can be used as a cost-effective tool for screening of environmental mutagens and therapeutic products.
机译:我们已经开发了一种使用来自转基因MutaMouse的原代肝细胞的体外突变测定方法。用两步灌注法分离原代肝细胞,并通过Percoll纯化,培养,并用苯并[a] py(BaP),2-氨基-1-甲基-6-苯基咪唑[4,5-b]处理吡啶(PhIP),3-硝基苯并蒽酮(3-NBA)和香烟烟雾冷凝物(CSC)。溶剂对照的平均lacZ突变频率(MF)大约是在肝组织中观察到的自发MF的两倍。暴露于BaP后,观察到MF的浓度依赖性增加(比对照高多达3.7倍)。对于3-NBA和PhIP暴露,突变频率分别增加了4倍和2倍,而没有添加任何外源性代谢激活。观察到CSC的lacZ MF略有增加,但具有统计学意义,但仅在最低浓度下增加。这是第一个证明可以在MutaMouse的培养的原代肝细胞中检测到突变的报告。提出的初步结果表明,MutaMouse原代肝细胞致突变性测定可用作筛选环境诱变剂和治疗产品的经济有效工具。

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