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某些抗精神病药物在显性致死突变试验中无有害作用。

Absence of noxious effects of selected neuroleptics in dominant-lethal mutagenesis assay.

作者信息

Sýkora I, Gandalovicová D, Rezábek K

出版信息

Mutat Res. 1979 Mar;66(3):291-9.

PMID:35745
Abstract

In a dominant-lethal assay in mice the following tricyclic neuroleptics were tested: prothiaden, imipramine, oxyprothepin decanoate and docloxythepin. No dominant-lethal effect was induced by these neuroleptics, even when administered at doses many times as great as clinical doses. The reduced percentages of pregnancies, in females who had copulated with males receiving docloxythepin, observed during and immediately after its administration, were directly connected with marked sedation induced in the males by this neuroleptic.

摘要

在一项针对小鼠的显性致死试验中,对以下三环类抗精神病药物进行了测试:丙硫异烟胺、丙咪嗪、癸酸羟丙硫蒽和多氯氧硫蒽。即使以比临床剂量高出许多倍的剂量给药,这些抗精神病药物也未诱导出显性致死效应。在给药期间及给药后立即观察到,与接受多氯氧硫蒽的雄性小鼠交配的雌性小鼠怀孕率降低,这与该抗精神病药物在雄性小鼠中引起的明显镇静作用直接相关。

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