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1-硝基芘在A/J小鼠体内的致瘤性与代谢

Tumorigenicity and metabolism of 1-nitropyrene in A/J mice.

作者信息

El-Bayoumy K, Hecht S S, Sackl T, Stoner G D

出版信息

Carcinogenesis. 1984 Nov;5(11):1449-52. doi: 10.1093/carcin/5.11.1449.

Abstract

Four groups of 28-32 male and female A/J mice were given i.p. injections of either trioctanoin or 1-nitropyrene in trioctanoin such that the total doses of 1-nitropyrene were 0.71 mmol/kg, 2.14 mmol/kg, or 6.44 mmol/kg. The mean number of lung tumors/mouse was 1.3 +/- 1.0 in the group treated with 6.44 mmol/kg of 1-nitropyrene compared with 0.3 +/- 0.6 in the trioctanoin group (p less than 0.001). Combined tumor incidence was not significant compared with controls in the two lower dose groups. Cultured explants of A/J mouse lung, and 9000 g supernatant of A/J mouse lung and liver, metabolized [14C]1-nitropyrene to 4,5-dihydro-4,5-dihydroxy-1-nitropyrene and 1-nitrohydroxypyrenes. Substantial amounts of unknown polar metabolites were also produced by cultured lung. Nitro-reduction to 1-aminopyrene was minimal in mouse lung and liver, even under oxygen deficient conditions.

摘要

将28 - 32只雄性和雌性A/J小鼠分为四组,通过腹腔注射三辛酸甘油酯或三辛酸甘油酯中的1 - 硝基芘,使1 - 硝基芘的总剂量分别为0.71 mmol/kg、2.14 mmol/kg或6.44 mmol/kg。与三辛酸甘油酯组(0.3±0.6)相比,接受6.44 mmol/kg 1 - 硝基芘处理的组中,每只小鼠肺部肿瘤的平均数量为1.3±1.0(p<0.001)。在两个较低剂量组中,联合肿瘤发生率与对照组相比无显著差异。A/J小鼠肺的培养外植体以及A/J小鼠肺和肝脏的9000g上清液将[14C]1 - 硝基芘代谢为4,5 - 二氢 - 4,5 - 二羟基 - 1 - 硝基芘和1 - 硝基羟基芘。培养的肺组织也产生了大量未知的极性代谢物。即使在缺氧条件下,小鼠肺和肝脏中1 - 硝基芘向1 - 氨基芘的硝基还原作用也很微弱。

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