柚皮苷抗邻苯二甲酸二正丁酯(DBP)诱导的雄性大鼠睾丸氧化损伤的细胞保护效力

Anis Anis, Sameh H. El-Nady, Hany A. Amer, Hamed T. Elbaz, Ahmed E. Elweza, Nermeen Borai El-Borai, Salah S. El-Ballal
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摘要

本研究旨在探讨柚皮苷(NG)对邻苯二甲酸二丁酯(DBP)致大鼠睾丸损伤和精子发生障碍的保护作用。雄性Wistar白化大鼠42只,随机分为6组,口服治疗,每周3次,连续8周。对照组给予橄榄油,柚皮素处理组给予NG (80 mg/kg), dbp250和dbp500中毒组分别给予DBP (250 mg/kg)和(500 mg/kg), NG + dbp250和NG + dbp500组在dbp250和500给药前1 h给予NG。结果显示,舒张压引起剂量依赖性男性生殖功能障碍,包括血清睾酮水平显著降低,同时精子数量、活力和总活动力显著降低。同时,DBP显著提高睾丸丙二醛水平,显著降低谷胱甘肽含量和过氧化氢酶活性。在病理组织学上,DBP引起精子缺失,精管细胞层退行性改变,精管上皮厚度明显减少。相反,在DBP 250或500中毒前1小时同时使用NG可减轻DBP引起的剂量依赖性生殖功能障碍,这可以通过血清睾酮水平、精子活力、计数和活力显著增加以及氧化/抗氧化状态和睾丸组织结构显著改善来证明。综上所述,本研究结果证明,NG可减轻dbp诱导的睾丸损伤和精子发生障碍,提示NG主要通过其强大的抗氧化活性,作为一种天然的保护和治疗药物,缓解生殖功能障碍,提高生殖性能。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Cytoprotective potency of naringin against di-n-butylphthalate (DBP)-induced oxidative testicular damage in male rats

Cytoprotective potency of naringin against di-n-butylphthalate (DBP)-induced oxidative testicular damage in male rats

The present study aimed to investigate the protective potential of naringin (NG) against di-n-butyl phthalate (DBP)- induced testicular damage and impairment of spermatogenesis in rats. Forty-two male Wistar albino rats were divided into six equal groups, and treated orally, 3 times weekly for 8 successive weeks. Control vehicle group was administrated olive oil, naringin-treated group was administered NG (80 mg/kg), DBP 250- and DBP 500- intoxicated groups received DBP (250 mg/kg) and (500 mg/kg), respectively, NG + DBP 250 and NG + DBP 500 groups received NG, an hour prior to DBP 250 and 500 administration. The results revealed that DBP induced dose-dependent male reproductive dysfunctions, included a significant decrease in the serum testosterone level concomitantly with significant decreases in the sperm count, viability, and total motility. Meanwhile, DBP significantly increased the testicular malondialdehyde level with significant reductions of glutathione content and catalase activity. Histopathologically, DBP provoked absence of spermatozoa, degenerative changes in the cell layers of seminiferous tubules and a significant decrease in the thickness of the seminiferous tubules epithelium. Conversely, the concomitant treatment with NG, one hour before DBP 250 or 500- intoxication mitigated the dose-dependent reproductive dysfunctions induced by DBP, evidenced by significant increases of serum testosterone level, sperm motility, count and viability along with marked improvement of the oxidant/antioxidant status and testicular histoarchitecture. In conclusion, the findings recorded herein proved that NG could mitigate DBP-induced testicular damage and impairment of spermatogenesis, suggesting the perspective of using NG as a natural protective and therapeutic agent for alleviating the reproductive dysfunctions and improving reproductive performance, mainly via its potent antioxidant activity.

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