比较吡哆醇和 N-乙酰半胱氨酸对扑热息痛诱导的大鼠肝中毒的保护作用

Ghazala Bibi, Arooj Javed, Hira Siyar, Haji Bahadar
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摘要

扑热息痛是一种常见的非处方药。扑热息痛引起的肝中毒每年导致 30 多万人住院治疗,占所有急性肝衰竭病例的 42%。N-乙酰半胱氨酸(NAC)是控制扑热息痛毒性的潜在解毒剂。研究目的研究吡哆醇单独或与 NAC 联合使用对雄性威斯特大鼠扑热息痛所致肝损伤的修复效果。研究方法给 Wistar 大鼠口服单剂量扑热息痛(650 毫克/千克)以诱导肝中毒。使用标准肝功能测试、组织病理学和血清谷胱甘肽水平评估了剂量为 300 毫克/千克的 NAC 和吡哆醇(200 毫克/千克)的肝脏保护作用。结果显示服用吡哆醇和 NAC 后,谷草转氨酶(AST)、谷丙转氨酶(ALT)和总胆红素水平显著下降,组织病理学变化也得到逆转。相反,联合使用 NAC 和吡哆醇会产生除谷胱甘肽水平外的其他显著变化。结论研究得出结论,在扑热息痛诱导的肝毒性中,吡哆醇可作为一种潜在的保肝药物。在与 NAC 联用时,吡哆醇对扑热息痛诱导的肝毒性有保护作用。
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A Comparison of the Protective Effect of Pyridoxine and N-Acetylcysteine in Paracetamol Induced Hepatotoxicity in Rats
Paracetamol is a common over the counter drug. Paracetamol-induced hepatotoxicity results in over 300,000 hospitalizations each year and accounts for up to 42% of all cases of acute liver failure. N-acetylcysteine (NAC) is a potential antidote to manage paracetamol toxicity. Objective: To investigate the effects of pyridoxine, alone and in combination with NAC in repairing paracetamol-induced liver damage in male Wister rats. Methods: A single oral dose of paracetamol (650 mg/kg) was administered to Wistar rats to induce hepatotoxicity. The hepato-protective effects of NAC at a dose 300 mg/kg, and pyridoxine (200 mg/kg) were evaluated using standard liver function tests and histopathological along with serum glutathione levels. Results: The administration of pyridoxine and NAC resulted in a significant decrease in AST, ALT, and total bilirubin levels and the reversal of histopathological changes. Conversely, administering NAC and pyridoxine in combination yielded significant changes except for the glutathione level. Conclusions: The study concluded that pyridoxine may be used as a potential hepatoprotective drug in paracetamol-induced hepatotoxicity. In combination with NAC, it showed protective effects in paracetamol-induced hepatoxicity. 
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