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Effect of repeated exposure to aniline nitrobenzene and benzene on liver microsomal metabolism in the rat.

机译:反复接触苯胺硝基苯和苯对大鼠肝脏微粒体代谢的影响。

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摘要

Exposure of rats to aniline at daily doses of 50 mg/kg of body weight over a month stimulated the microsomal metabolism as manifested by (1) acceleration of p-hydroxylation of anilin and N-demethylation of aminopyrine in 9-000 times g postmitochondrial supernatant of the liver, (2) shortening the sleeping time after hexobarbital, and (3) reduction of the antipyretic effect of phenacetin. In the rats exposed to nitrobenzene in a similar manner to aniline, nitroreduction of nitrobenzene and p-hydroxylation of aniline remained unaffected; the antipyretic effect of phenacetin was decreased, whereas hexobarbital sleeping time remained unchanged. Exposure of rats to benzene (50 mg/kg of body weight daily for a month) had no effect on the rate of hydroxylation of benzene and N-demethylation of aminopyrine. In benzene-exposed rats hexobarbital sleeping time was prolonged whereas the antipyretic effect of phenacetin was unaffected. Microsomal metabolism of aniline, nitrobenzene, and benzene was stimulated and inhibited when the rats were pretreated with phenobarbital and SKF 525-A, respectively.
机译:将大鼠每日以50 mg / kg体重的每日剂量苯胺暴露超过一个月可刺激微粒体代谢,其表现为(1)在9-000倍于线粒体后上清液中加速苯胺的p-羟基化和氨基比林的N-去甲基化(2)缩短己烯巴比妥后的睡眠时间,以及(3)降低非那西汀的解热作用。在以与苯胺相似的方式暴露于硝基苯的大鼠中,硝基苯的硝基还原和苯胺的对羟基化仍未受到影响。非那西丁的解热作用降低,而己烯巴比妥的睡眠时间保持不变。大鼠暴露于苯中(每天50 mg / kg体重,持续一个月)对苯的羟基化速率和氨基比林的N-去甲基化速率没有影响。在苯暴露的大鼠中,己烯比巴星的睡眠时间延长,而非那西汀的解热作用不受影响。当分别用苯巴比妥和SKF 525-A预处理大鼠时,苯胺,硝基苯和苯的微粒体代谢受到刺激和抑制。

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