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曲通(利沃松)对Wistar大鼠氧化DNA损伤的保护作用及其对各种肝毒性剂的肝保护潜力。

Protective effect of Tritone (Livosone) on oxidative DNA damage and its hepatoprotective potential against various hepatotoxic agent in wistar rats.

作者信息

Medhekar Sheetal Kashinath, Jadhav Tejas Pandurang, Sasane Vishal Sadashiv, Shende Vikas Suresh, Aloorkar Nagesh Hanmantrao, Chincholkar Anjali Baburao, Soman Girish Sudhakar, Kulkarni Ajit Shankarrao

机构信息

Department of Pharmacology, Satara College of Pharmacy, Degaon, Satara, MH, India.

R & D center, Nisarga Biotech Pvt Ltd, Satara, MH, India.

出版信息

Exp Toxicol Pathol. 2017 Mar 2;69(3):153-161. doi: 10.1016/j.etp.2016.12.005. Epub 2017 Jan 4.

Abstract

AIM

To evaluate antioxidant activity, DNA damage inhibition and hepatoprotecitve potential of polyherbal formulation Tritone (Livosone).

METHODS

In vitro antioxidant activity of Tritone formulation was performed by using DPPH assay. Hepatoprotecitve potential of Tritone was evaluated against various hepatotoxic agents including Paracetamol (2g/kg b. wt p.o. single dose on 15th day), Galactosamine (400mg/kg b. wt. i.p. single dose on 8th day) and Alcohol (30% p.o.1ml/100g of rat for 15days). Tritone formulation at the doses of (40.5, 81 and 162mg/kg) and standard silymarin (100mg/kg) and Liv52 (270mg/kg) were administered p.o. The hepatoprotective assessment was done by estimating biochemical parameters: SGOT, SGPT, ALP and Total Bilirubin total protein and ChE levels. Additionally histopathological and DNA fragmentation study of Tritone was also performed.

RESULT

Administration of hepatotoxins (paracetamol, D-GaiN and alcohol) in experimental animals showed significant biochemical, histological deterioration and DNA fragmentation. Pretreatment with Tritone (Livosone) shows significant reduction in serum SGOT, SGPT, ALP and total bilirubin levels and shows significant elevation in total protein and cholinesterase (ChE) levels compared to groups treated with hepatotoxic agents. Histopathological observations of rat liver pretreated with Tritone (Livosone) shows significant protection against hepatic damage. Inhibition of DNA fragmentation by Tritone indicates protective effect of formulation on liver at molecular level. Finally all the results were compared with standard drugs Silymarin and Liv52.

CONCLUSION

Correlation of antioxidant activity, biochemical results, histopathological changes and inhibition of DNA damage after treatment with Tritone shows maximum hepatoprotective potential at dose 81mg/kg and 162mg/kg.

摘要

目的

评估多草药配方制剂Tritone(利沃松)的抗氧化活性、DNA损伤抑制作用及肝脏保护潜力。

方法

采用DPPH法检测Tritone制剂的体外抗氧化活性。通过给予多种肝毒性药物来评估Tritone的肝脏保护潜力,这些肝毒性药物包括对乙酰氨基酚(第15天口服单剂量2g/kg体重)、半乳糖胺(第8天腹腔注射单剂量400mg/kg体重)和酒精(15天内每天口服30%的溶液,1ml/100g大鼠体重)。分别以(40.5、81和162mg/kg)的剂量口服给予Tritone制剂、标准药物水飞蓟素(100mg/kg)和利维52(270mg/kg)。通过检测生化指标:谷草转氨酶(SGOT)、谷丙转氨酶(SGPT)、碱性磷酸酶(ALP)、总胆红素、总蛋白和胆碱酯酶(ChE)水平来进行肝脏保护评估。此外,还对Tritone进行了组织病理学和DNA片段化研究。

结果

给实验动物施用肝毒性药物(对乙酰氨基酚、D-氨基半乳糖和酒精)后,出现了明显的生化、组织学恶化及DNA片段化。与用肝毒性药物处理的组相比,用Tritone(利沃松)预处理后,血清中的SGOT、SGPT、ALP和总胆红素水平显著降低,总蛋白和胆碱酯酶(ChE)水平显著升高。对用Tritone(利沃松)预处理的大鼠肝脏进行组织病理学观察,显示出对肝损伤有显著的保护作用。Tritone对DNA片段化的抑制表明该制剂在分子水平上对肝脏有保护作用。最后,将所有结果与标准药物水飞蓟素和利维52进行比较。

结论

Tritone处理后的抗氧化活性、生化结果、组织病理学变化及DNA损伤抑制之间的相关性表明,在81mg/kg和162mg/kg剂量下具有最大的肝脏保护潜力。

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