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Liver Protection by Bis(Maltolato)Zinc(II) Complex

机译:双(麦芽糖醇)锌(II)配合物对肝脏的保护

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The aim of this study was to perform screening of a novel drug for treating liver injury. Bis(maltolato)zinc(II) complex [Zn(Mal)_2], which was previously reported to possess insulinomimetic activity, was found to have potency against experimentally induced liver injury both in vitro and in vivo. Cultured rat hepatocytes were treated with bromobenzene for 24 h to induce cellular injury. Zn(Mal)_2 of various concentrations was added along with bromobenzene in order to evaluate the hepatoprotective activity of Zn(Mal)_2 in vitro. The number of viable hepatocytes decreased by 42% in the culture with bromobenzene. However, hepatocyte viability was maintained when Zn(Mal)_2 was added to the bromobenzene culture. The hepatoprotective activity of Zn(Mal)_2 in vivo was investigated using a concanavalin A-induced liver injury model in BALB/c mice. Changes in serum aminotransferase activities and the secretion of several cytokines were measured. The hepatoprotective effect of Zn(Mal)_2 was also demonstrated in vivo by the suppression of serum aspartate aminotransferase and alanine aminotransferase elevation. No significant changes in serum cytokines associated with the induction of hepatic damage were observed in the concanavalin A-induced injury model. However, examination of concanavalin A-treated mouse splenocytes revealed a dose-dependent suppression of cytokine secretions by Zn(Mal)_2. Zn(Mal)_2 possessed hepatoprotective activity and might exert its effect by a number of mechanisms.
机译:这项研究的目的是进行新型药物治疗肝损伤的筛选。以前据报道具有胰岛素模拟活性的Bis(麦芽糖基)锌(II)复合物[Zn(Mal)_2]在体外和体内均可有效抵抗实验性肝损伤。培养的大鼠肝细胞用溴苯处理24小时,以诱导细胞损伤。加入不同浓度的Zn(Mal)_2和溴苯,以评估Zn(Mal)_2的体外肝保护活性。用溴苯培养的存活肝细胞数量减少了42%。但是,将Zn(Mal)_2添加到溴苯培养物中可以保持肝细胞的活力。使用伴刀豆球蛋白A诱导的BALB / c小鼠肝损伤模型,研究了体内Zn(Mal)_2的保肝活性。测量了血清氨基转移酶活性的变化和几种细胞因子的分泌。 Zn(Mal)_2的肝保护作用还通过抑制血清天冬氨酸转氨酶和丙氨酸转氨酶升高而在体内得到证实。在伴刀豆球蛋白A诱导的损伤模型中,未观察到与诱导肝损伤相关的血清细胞因子的显着变化。但是,检查伴刀豆球蛋白A处理的小鼠脾细胞显示Zn(Mal)_2对细胞因子分泌具有剂量依赖性抑制作用。 Zn(Mal)_2具有保肝活性,可能通过多种机制发挥其作用。

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