首页> 外文期刊>Central European journal of public health >Effects of kojic acid on oxidative damage and on iron and trace element level in iron-overloaded mice and rats.
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Effects of kojic acid on oxidative damage and on iron and trace element level in iron-overloaded mice and rats.

机译:曲酸对铁超载小鼠和大鼠氧化损伤以及铁和微量元素水平的影响。

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摘要

Since members of hydroxypyrone series posses iron chelating properties, kojic acid (KA), 5-hydroxy-2-(hydroxymethyl)-4H-pyran-one, a fungal metabolite of natural origin, has been suggested to might play a role in iron-overload diseases and in oxidative stress conditions involving transition metal. In our experiments in vivo models of iron-overload were used to study iron-chelating properties of KA and its effect on oxidative damage in mice and rats. The treatment of iron-preloaded rats (25 mg Fe x kg(-1) b.w., i.p., daily for five days) with 0.5% KA in drinking water for four weeks did not lower the iron concentration accumulated in the liver, neither diminished the induced hepatic lipid peroxidation in iron-loaded rats. The GSH level decreased in KA-treated group. Similarly, in iron-loaded mice model experiment, the following oral treatment with KA (100 mg x kg(-1)) daily for 7 days did not decrease the level of Fe accumulated in the liver and the lipid peroxidation even enhanced after KA treatment. Though in our experiments in vivo the ability of kojic acid to affect iron kinetics in the organism could not be proved, kojic acid as a molecule of natural origin may serve as a template for the preparation of new biologically active derivatives possessing capability of chelating iron.
机译:由于羟基吡喃酮系列的成员具有铁螯合特性,因此有人提出曲酸(KA),5-羟基-2-(羟甲基)-4H-吡喃酮一(一种天然来源的真菌代谢物)可能在铁-超载疾病和涉及过渡金属的氧化应激条件。在我们的实验中,铁超载的体内模型用于研究KA的铁螯合特性及其对小鼠和大鼠氧化损伤的影响。用饮用水中含0.5%KA的铁预载大鼠(25 mg Fe x kg(-1)bw,ip,每天ip,连续5天)治疗4周没有降低肝脏中积累的铁浓度,也没有降低肝脏中的铁浓度。诱导铁负荷大鼠肝脂质过氧化。 KA治疗组GSH水平降低。同样,在铁负载的小鼠模型实验中,每天口服KA(100 mg x kg(-1))连续7天进行以下口服治疗不会降低肝脏中铁的累积水平,并且在KA处理后脂质过氧化作用甚至会增强。尽管在我们的体内实验中不能证明曲酸影响生物体内铁动力学的能力,但曲酸作为天然来源的分子可以作为制备具有螯合铁能力的新型生物活性衍生物的模板。

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