芦荟-大黄素醌预处理可降低四氯化碳致急性肝损伤。

B Arosio, N Gagliano, L M Fusaro, L Parmeggiani, J Tagliabue, P Galetti, D De Castri, C Moscheni, G Annoni
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引用次数: 140

摘要

芦荟含有几种活性化合物,包括芦荟素,一种c -糖苷,可以在肠道中水解形成芦荟大黄素蒽酮,而蒽酮又被自动氧化成醌芦荟大黄素。基于一些蒽醌类药物声称的肝保护活性,我们在四氯化碳中毒大鼠模型中研究了芦荟大黄素,因为这种外源性药物在自由基产生后通过脂质过氧化诱导急性肝损伤。12只大鼠腹腔注射CCl4 (3 mg/kg), 6只大鼠腹腔注射两次芦荟大黄素(50 mg/kg;亚兰+芦荟大黄素);另外6只大鼠只注射芦荟大黄素(芦荟大黄素),6只不给药(对照组)。肝脏组织学检查显示,与单独使用CCl4治疗的大鼠相比,CCl4+芦荟-大黄素治疗的大鼠肝脏病变较少,血清l -天冬氨酸-2-氧葡萄糖-转氨酶水平证实了这一点(CCl4组为394+/-38.6 UI/l, CCl4+芦荟-大黄素组为280+/-24.47 UI/l;P
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Aloe-Emodin quinone pretreatment reduces acute liver injury induced by carbon tetrachloride.

Aloe contains several active compounds including aloin, a C-glycoside that can be hydrolyzed in the gut to form aloe-emodin anthrone which, in turn, is auto-oxidized to the quinone aloe-emodin. On the basis of the claimed hepatoprotective activity of some antraquinones, we studied aloe-emodin in a rat model of carbon tetrachloride (CCl4) intoxication, since this xenobiotic induces acute liver damage by lipid peroxidation subsequent to free radical production. Twelve rats were treated with CCl4 (3 mg/kg) intraperitoneally and six were protected with two intraperitoneally injections of aloe-emodin (50 mg/kg; CCl4+aloe-emodin); six other rats were only aloe-emodin injected (aloe-emodin) and six were untreated (control). Histological examination of the livers showed less marked lesions in the CCl4+aloe-emodin rats than in those treated with CCl4 alone, and this was confirmed by the serum levels of L-aspartate-2-oxoglutate-aminotransferase (394+/-38.6 UI/l in CCl4, 280+/-24.47 UI/l in CCl4+aloe-emodin rats; P<0.05). We also quantified changes in hepatic albumin and tumour necrosis factor-alpha mRNAs. Albumin mRNA expression was significantly lower only in the liver of CCl4 rats (P<0.05 versus control) and was only slightly reduced in the CCl4+aloe-emodin rats. In contrast tumour necrosis factor-alpha mRNA was significantly higher (P<0.05) in the CCl4 than the control rats and almost equal in the CCl4+aloe-emodin, aloe-emodin and control groups. In conclusion, aloe-emodin appears to have some protective effect not only against hepatocyte death but also on the inflammatory response subsequent to lipid peroxidation.

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