Mutagenic activity of N-chloropiperidine.

M A Bempong, F E Scully
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Abstract

The toxicity and mutagenicity of N-chloropiperidine (NCP) and piperidine (PD) were tested in C57Bl/J6 mice and in Salmonella tester strains. Toxicity studies, based on single intraperitoneal administration of the test compounds, revealed that while the toxic effect of PD in aqueous solution decreased with time, the toxicity of aqueous solution of NCP increased on standing at room temperature for 24 or more hr. Direct incorporation assay of NCP and PD for mutagenic activity, using Salmonella tester strains as the test system, showed that the number of revertants induced by NCP was about 2.4 fold of that induced by PD. The results further indicated that TA100 and TA1535 were the most sensitive strains. A modified host-mediated assay, involving the analysis of urine, peritoneal fluid and faecal material from control and NCP-treated mice, indicated that peritoneal fluid from treated animals generated more revertants; moderate levels of revertants were produced by faecal material and urinary and urinary preparations produced the least number of revertants.

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n -氯哌啶的致突变活性。
研究了n -氯哌啶(NCP)和哌啶(PD)对C57Bl/J6小鼠和沙门氏菌试验菌株的毒性和致突变性。单次腹腔给药的毒性研究表明,PD在水溶液中的毒性作用随着时间的推移而降低,而NCP水溶液在室温下放置24小时或更长时间后毒性增加。以沙门菌试验菌株为试验系统,将NCP与PD直接掺入试验,结果表明NCP诱导的回变菌数量约为PD诱导的2.4倍。结果进一步表明,TA100和TA1535是最敏感的菌株。一项改进的宿主介导试验,包括对对照小鼠和ncp治疗小鼠的尿液、腹膜液和粪便物质进行分析,表明治疗小鼠的腹膜液产生更多的逆转物;粪便物质产生中等水平的还原物,尿液和尿液制剂产生最少数量的还原物。
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