Hepatoprotective activity of Livshis, a polyherbal formulation in CCl4-induced hepatotoxic male Wistar rats: A toxicity screening approach

Tushar Kanti Bera , Kausik Chatterjee , Debasis De , Kazi Monjur Ali , Kishalay Jana , Soumyajit Maiti , Debidas Ghosh
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引用次数: 13

Abstract

This study investigated the hepatoprotective activity of the polyherbal formulation Livshis in CCl4-induced hepatotoxic male albino rats, and included an assessment of the toxicity of the formulation. Male Wistar albino rats (140 ± 10 g) were divided into five groups (n = 6). Liver necrosis was induced by intraperitoneal injection of CCl4 (1 mL/kg body weight, 50% v/v with olive oil). Antioxidant enzyme activities, such as lipid peroxidation, and liver function test biosensors were assessed. Hematological and renotoxicity markers were evaluated to assess the general toxicity of the formulation. For acute toxicity evaluation of Livshis, the formulation was administered orally at doses ranging from 25 to 3200 mg/kg body weight. Hepatic antioxidant enzyme activities diminished significantly, and hepatic lipid peroxidation rates were elevated in CCl4-treated animals that were pretreated with distilled water (Group II). The activities of serum toxicity marker enzymes and serum liver function test biosensors increased significantly in Group II animals, whereas these biosensors were significantly protected in Livshis pretreated, CCl4-treated animals. Group V animals, treated with Livshis alone, did not exhibit any significant variation in levels of hematological and renotoxicity markers compared to controls. In an acute toxicity study, there were no toxic symptoms up to the dose level of 3200 mg/kg body weight. We conclude that Livshis is safe for long-term treatment for hepatic protection at doses of 50 mg/kg body weight.

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复方利夫氏对ccl4诱导的雄性Wistar大鼠肝毒性的保护作用:毒性筛选方法
本研究考察了复方利氏对ccl4诱导的肝毒性雄性白化大鼠的肝保护作用,并对其毒性进行了评估。将雄性Wistar白化大鼠(140±10 g)分为5组(n = 6),腹腔注射CCl4 (1 mL/kg体重,50% v/v橄榄油)诱导肝坏死。抗氧化酶活性,如脂质过氧化和肝功能测试生物传感器进行了评估。评估血液学和肾毒性指标,以评估制剂的一般毒性。对于Livshis的急性毒性评估,该制剂的口服剂量范围为25至3200mg /kg体重。经蒸馏水预处理(II组)的ccl4处理动物肝脏抗氧化酶活性显著降低,肝脏脂质过氧化率升高。血清毒性标记酶和血清肝功能测试生物传感器活性在II组动物中显著升高,而这些生物传感器在经ccl4预处理的Livshis动物中受到显著保护。与对照组相比,单独给予Livshis治疗的V组动物在血液学和肾毒性标志物水平上没有表现出任何显著变化。在一项急性毒性研究中,在3200mg /kg体重的剂量水平下没有出现中毒症状。我们得出结论,在50 mg/kg体重的剂量下,Livshis对肝脏保护的长期治疗是安全的。
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