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N-亚硝基-3,5-二甲基哌啶异构体的致癌作用。

Carcinogenesis by isomers of N-nitroso-3,5-dimethylpiperidine.

作者信息

Lijinsky W, Reuber M D, Singer S S, Singer G M

出版信息

J Natl Cancer Inst. 1982 Jun;68(6):989-91.

PMID:6953279
Abstract

The cis- and trans-isomers of N-nitroso-3,5-dimethylpiperidine were administered separately in drinking water solution to groups of 20 female F344 rats for 50 weeks. The concentrations of the solutions were 0.72 m M for the cis-isomer and 0.14 mM for the trans-isomer. In both groups the animals died with tumors of the upper gastrointestinal (GI) tract, mainly carcinomas of the esophagus, at about the same time. A third group of animals was given a mixture of the two isomers in the ratio of 5 cis:1 trans, and these animals died more rapidly with the same upper GI tumors. The trans-isomer appeared to be a more potent carcinogen than the cis-isomer. The 3,5-dimethyl derivative is a less potent carcinogen than nitrosopiperidine.

摘要

将N-亚硝基-3,5-二甲基哌啶的顺式和反式异构体分别以饮用水溶液的形式给予每组20只雌性F344大鼠,持续50周。顺式异构体溶液的浓度为0.72 mM,反式异构体溶液的浓度为0.14 mM。在两组中,动物大约在同一时间死于上消化道(GI)肿瘤,主要是食管癌。第三组动物给予两种异构体比例为5顺式:1反式的混合物,这些动物因相同的上消化道肿瘤死亡得更快。反式异构体似乎比顺式异构体更具致癌性。3,5-二甲基衍生物的致癌性比亚硝基哌啶弱。

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