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首页> 外文期刊>Toxicology Letters: An International Journal Providing a Forum for Original and Pertinent Contributions in Toxicology Research >Investigation of testicular toxicity of nefiracetam, a neurotransmission enhancer, in rats.
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Investigation of testicular toxicity of nefiracetam, a neurotransmission enhancer, in rats.

机译:神经传递增强剂奈非西坦对大鼠睾丸毒性的研究。

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摘要

Testicular toxicity of nefiracetam (N-(2,6-dimethylphenyl)-2-(2-oxo-1-pyrrolidinyl) acetamide), a neurotransmission enhancer, was investigated in male Slc:SD rats. Nefiracetam was orally administered daily at 1500 mg/kg for 4 weeks, and the animals were killed sequentially during the course of administration to determine testicular histopathological changes and sperm head counts (SHC), and hormonal changes. Retention of step 19 spermatids, sporadic degeneration of pachytene spermatocytes and step 7 spermatids in the stage VII seminiferous tubules, and a decrease in SHC were seen as earliest changes after 1 week of administration. These changes gradually advanced up to atrophy of seminiferous tubules with multinucleated-giant-cell formation after 4-week administration. Serum and testicular testosterone levels were decreased, but recovered to the control levels within a day following a single administration, and the decreases were repeated after 1-week administration. These results suggest that nefiracetam-induced earliest changes could be caused by the decreased level of testicular testosterone.
机译:在雄性Slc:SD大鼠中研究了奈非西坦(N-(2,6-二甲基苯基)-2-(2-氧代-1-吡咯烷基)乙酰胺)的睾丸毒性,这是一种神经传递增强剂。奈非西坦每天1500 mg / kg口服给药,持续4周,在给药过程中依次杀死动物,以确定睾丸的组织病理学变化,精子头数(SHC)和激素变化。第七阶段的曲细精管中保留了第19步精子,偶尔出现的粗线精子细胞变性和第7步精子,以及SHC的降低是给药1周后的最早变化。这些变化在给药4周后逐渐发展到具有多核巨细胞形成的曲细精管萎缩。血清和睾丸睾丸激素水平降低,但在单次给药后一天之内恢复到对照水平,并且在给药1周后重复下降。这些结果表明,奈非西坦引起的最早变化可能是睾丸睾丸激素水平降低所致。

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