Estrogens, and particularly glucuronides such as ethinylestradiol (EE), have been shown to cause cholestasis in animal studies, by reducing bile acid uptake by hepatocytes. The aim of the present article is to investigate anticholestatic activity of the ethanolic extract of the aerial parts of Jasonia montana against liver cholestasis induced by EE in adult female rats in an attempt to understand its mechanism of action, which may pave the way for possible therapeutic applications. Subcutaneous administration of 100 μg/kg b.w. ethinylestradiol to rats induced hepatocellular cholestasis with a significant decrease in serum cholesterol, bile acids and bilirubin levels as well as in hepatic superoxide dismutase (SOD), glutathione peroxidase (GPx), glutathione reductase (GR) activities and hepatic total, protein-bound and non-protein sulfhydryl groups. Also, treatment with EE produced significant increase in serum Pi-glutathione-s-transferase (Pi-GST), gamma glutamyl transpeptidase (γ-GT) and alpha-glutathione-s-transferase (α-GST) activities as well as serum nitric oxide (NO) and tumor necrosis factor alpha (TNF-α) level and hepatic malondialdehyde (MDA) level as compare to control group. Oral administration of the aerial parts of ethanolic extract at a concentration of 150 mg/kg b.w. daily to rats treated with EE for 15 days showed a significant protection against-induced decrease in serum cholesterol, bile acids and bilirubin levels. The treatment also resulted in a significant increase in hepatic SOD, GPx and GR activities as well as hepatic total, protein-bound and non-protein sulfhydryl groups. In addition, the extract could inhibit serum Pi-GST, γ-GT and α-GST activities as well as reduce serum TNF-α, NO and hepatic MDA as compare to ethinylestradiol treated rats. High content of flavonoids and phenolic compounds was found in ethanolic extract, which may be responsible for free radical activity. The results clearly suggest that the aerial parts of J. montana extract may effectively normalize the impaired antioxidant status in ethinylestradiol (EE)-cholestatic model. Thus the extract may have a therapeutic value in drug-induced biliary cholestasis as well as in hormonal therapy.
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机译:在动物研究中,雌激素,尤其是葡萄糖醛酸苷(如乙炔雌二醇(EE))已被证明可通过减少肝细胞对胆汁酸的吸收而引起胆汁淤积。本文的目的是研究成年雌性大鼠中茉莉花(Jasonia montana)的地上部分乙醇提取物对EE诱发的肝胆汁淤积的抗胆汁抑制作用,以试图了解其作用机理,从而为可能的治疗方法铺平道路。应用程序。皮下给药100μg/ kg体重乙炔雌二醇可导致大鼠肝细胞胆汁淤积,血清胆固醇,胆汁酸和胆红素水平以及肝超氧化物歧化酶(SOD),谷胱甘肽过氧化物酶(GPx),谷胱甘肽还原酶(GR)活性和肝总,蛋白结合和非蛋白质巯基。此外,用EE进行治疗可显着提高血清Pi-谷胱甘肽S-转移酶(Pi-GST),γ-谷氨酰转肽酶(γ-GT)和α-谷胱甘肽S-转移酶(α-GST)的活性以及血清硝酸与对照组相比,氧化氮(NO)和肿瘤坏死因子α(TNF-α)的水平以及肝丙二醛(MDA)的水平。口服乙醇提取物的地上部分,浓度为150 mg / kg b.w.每天对接受EE治疗15天的大鼠显示出显着的保护作用,可防止血清胆固醇,胆汁酸和胆红素水平降低。该治疗还导致肝脏SOD,GPx和GR活性以及肝脏总,蛋白结合和非蛋白巯基的显着增加。此外,与乙炔雌二醇处理的大鼠相比,该提取物可以抑制血清Pi-GST,γ-GT和α-GST活性,并降低血清TNF-α,NO和肝MDA。在乙醇提取物中发现了高含量的类黄酮和酚类化合物,可能与自由基活性有关。结果清楚地表明,山茱J提取物的地上部分可以有效地使乙炔雌二醇(EE)胆汁淤积模型的抗氧化状态正常化。因此,该提取物在药物诱发的胆汁性胆汁淤积以及激素治疗中可能具有治疗价值。
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