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首页> 外文期刊>Chemico-biological interactions >Garlic oil and DDB, comprised in a pharmaceutical composition for the treatment of patients with viral hepatitis, prevents acute liver injuries potentiated by glutathione deficiency in rats.
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Garlic oil and DDB, comprised in a pharmaceutical composition for the treatment of patients with viral hepatitis, prevents acute liver injuries potentiated by glutathione deficiency in rats.

机译:包含在治疗病毒性肝炎患者的药物组合物中的大蒜油和DDB可防止大鼠中的谷胱甘肽缺乏症引起的急性肝损伤。

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摘要

A pharmaceutical composition PENNEL comprising garlic oil (GO) and dimethyl-4,4'-dimethoxy-5,6,5',6'-dimethylene dioxybiphenyl-2,2'-dicarboxylate (DDB) as ingredients active for phase II enzyme induction and liver protection, respectively, has been used as a curative preparation for patients with acute or chronic viral hepatitis. In spite of the wide clinical use of PENNEL in Asian and Middle Eastern countries, whether GO+DDB treatment synergistically protects the liver from injuries potentiated by GSH deficiency compared to the individual treatment has not been determined. This study investigated the effects of GO+DDB in comparison with each ingredient alone on chemical-induced liver injury potentiated by a GSH depleting agent. Rats that had been daily pretreated with GO+DDB, GO, DDB, ursodesoxycholic acid or silymarin for 6 days were exposed to buthionine sulfoximine (BSO) and then injected with a single dose of CCl4. The effects of the agents on acute liver toxicities induced by BSO, CCl4 or BSO+CCl4 were assessed by blood biochemistry and histopathology. GO+DDB pretreatment effectively prevented increases in plasma aminotransferases or lactate dehydrogenase activities in rats exposed to BSO+CCl4, compared to GO or DDB treatment alone. Whereas BSO potentiated CCl4-induced liver injuries as evidenced by elevations in central necrosis, hepatocyte degeneration and inflammation, pretreatment with GO+DDB abrogated BSO+CCl4-induced liver injuries more efficaciously than did that with GO or DDB. The hepatoprotective effect of GO+DDB was superior to that of ursodesoxycholic acid or silymarin. Also, blood biochemistry indicated that GO+DDB pretreatment prevented increases in plasma triglyceride contents in rats insulted with CCl4 or BSO+CCl4. The present study demonstrated that GO+DDB, when daily pretreated for six consecutive days, exerted synergistic protection of the liver from chemical-induced injury potentiated by the condition of GSH deficiency, and has additional advantages in lowering the plasma lipids.
机译:药物组合物PENNEL,其包含大蒜油(GO)和二甲基-4,4'-二甲氧基-5,6,5',6'-二亚甲基二氧基联苯-2,2'-二羧酸盐(DDB)作为对II期酶诱导有效的成分肝和肝保护分别被用作治疗急性或慢性病毒性肝炎的药物。尽管PENNEL在亚洲和中东国家广泛使用,但与单独治疗相比,GO + DDB治疗是否能协同保护肝脏免受GSH缺乏所致的伤害,目前尚无定论。这项研究调查了GO + DDB与单独使用每种成分相比对GSH消耗剂加强的化学性肝损伤的作用。每天用GO + DDB,GO,DDB,熊去氧胆酸或水飞蓟素预处理的大鼠暴露于丁硫氨酸亚砜亚胺(BSO),然后注射单剂量的CCl4。通过血液生化和组织病理学评估了这些药物对BSO,CCl4或BSO + CCl4诱导的急性肝毒性的影响。与单独进行GO或DDB处理相比,GO + DDB预处理可有效防止暴露于BSO + CCl4的大鼠血浆氨基转移酶或乳酸脱氢酶活性的增加。 BSO增强了CCl4诱导的肝损伤,如中央坏死,肝细胞变性和炎症的升高所证明,而GO + DDB预处理比BGO + DDB更加有效地消除了BSO + CCl4诱导的肝损伤。 GO + DDB的肝保护作用优于熊去氧胆酸或水飞蓟素。此外,血液生物化学表明,GO + DDB预处理可防止CCl4或BSO + CCl4损伤的大鼠血浆甘油三酸酯含量增加。本研究表明,GO + DDB在连续六天每天进行预处理时,可对肝脏产生协同保护作用,使其免受GSH缺乏症加重的化学诱导损伤的影响,并且在降低血浆脂质方面具有其他优势。

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