百里醌改善丙硫脲嘧啶所致幼年大鼠甲状腺功能减退的肝肾毒性。

Y. Baghcheghi, Amin Mokhtari-Zaer, M. Hosseini, A. Anaeigoudari, H. Salmani, F. Beheshti
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引用次数: 3

摘要

越来越多的研究表明,甲状腺功能减退可能导致肝肾毒性。本研究考察了黑草主要活性成分百里醌(TQ)对幼年期大鼠甲状腺功能减退肝肾毒性的抑制作用。方法雄性大鼠随机分为对照组、丙硫脲嘧啶组(PTU)、PTU- tq 5 mg/kg、PTU- tq 10 mg/kg 4组(n = 7)。将PTU以0.05%的浓度溶解于饮用水中,给药6周。在PTU- tq5和PTU- tq10组中,动物分别接受PTU加5 mg/kg和10 mg/kg TQ (i.p),持续6周。通过测定血清肝肾功能指标及肝肾组织氧化应激生物标志物对TQ治疗后大鼠进行评价。结果TQ(5和10 mg/kg)可降低甲状腺功能减退大鼠肝脏和肾脏组织氧化应激损伤,提高肝脏和肾脏匀浆中抗氧化酶活性,降低MDA。此外,TQ治疗显著抑制了与肝肾毒性相关的肝肾功能血清生化指标的升高。结论TQ对甲状腺功能减退所致大鼠肝肾毒性的保护作用可能与其降低肝、肾组织氧化应激有关。然而,建议进行更多的研究来研究TQ对人类甲状腺功能减退患者肝肾预后影响的确切机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Thymoquinone Ameliorate Hepatorenal Toxicity Associated With Propylthiouracil-Induced Hypothyroidism in Juvenile Rats.
Background An increasing number of studies suggest that hypothyroidism may lead to hepatorenal toxicity. This study examined whether thymoquinone (TQ), the main active Nigella sativa constituent, could prevent the detrimental influences of hepatorenal toxicity of hypothyroidism during the juvenile period in rats. Methods The male rats were randomly divided into four groups (n = 7), including control, propylthiouracil (PTU), PTU-TQ 5 mg/kg, and PTU-TQ 10 mg/kg. PTU was dissolved in drinking water at a concentration of 0.05% and administered for six weeks. In the PTU-TQ5 and PTU-TQ10 groups, animals received PTU plus 5 mg/kg and 10 mg/kg of the TQ (i.p.) for six weeks, respectively. The rats were evaluated after TQ treatment by measuring serum markers of liver and kidney function tests as well as oxidative stress biomarkers in liver and kidney tissues. Results Administration of TQ (5 and 10 mg/kg) decreased oxidative stress damage in liver and kidney tissue in hypothyroidism rats with improvement in activities of antioxidant enzymes and a decrease in MDA in both liver and kidney homogenates. Furthermore, TQ treatment significantly inhibited the elevation of serum biochemical markers of liver and kidney function associated with this hepatorenal toxicity. Conclusion These results suggest that the protective effect of TQ in hypothyroidism-induced hepatorenal toxicity in rats is attributed to its ability to reduce oxidative stress in hepatic and renal tissues. However, more studies are recommended to investigate the exact mechanism (s) for the effect of TQ on hepatorenal outcomes of hypothyroidism in human subjects.
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