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首页> 外文期刊>ScientificWorldJournal >Changes in Iron Metabolism and Oxidative Status in STZ-Induced Diabetic Rats Treated with Bis(maltolato) Oxovanadium (IV) as an Antidiabetic Agent
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Changes in Iron Metabolism and Oxidative Status in STZ-Induced Diabetic Rats Treated with Bis(maltolato) Oxovanadium (IV) as an Antidiabetic Agent

机译:STZ诱导糖尿病大鼠铁代谢和氧化地位的变化,用双(麦芽甲醛)氧化钒(IV)作为抗糖尿病药剂治疗

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The role of vanadium as a micronutrient and hypoglycaemic agent has yet to be fully clarified. The present study was undertaken to investigate changes in the metabolism of iron and in antioxidant defences of diabetic STZ rats following treatment with vanadium. Four groups were examined: control; diabetic; diabetic treated with 1 mgV/day; and Diabetic treated with 3 mgV/day. The vanadium was supplied in drinking water as bis(maltolato) oxovanadium (IV) (BMOV). The experiment had a duration of five weeks. Iron was measured in food, faeces, urine, serum, muscle, kidney, liver, spleen, and femur. Superoxide dismutase, catalase, NAD(P)H: quinone-oxidoreductase-1 (NQO1) activity, and protein carbonyl group levels in the liver were determined. In the diabetic rats, higher levels of Fe absorbed, Fe content in kidney, muscle, and femur, and NQO1 activity were recorded, together with decreased catalase activity, in comparison with the control rats. In the rats treated with 3 mgV/day, there was a significant decrease in fasting glycaemia, Fe content in the liver, spleen, and heart, catalase activity, and levels of protein carbonyl groups in comparison with the diabetic group. In conclusion BMOV was a dose-dependent hypoglycaemic agent. Treatment with 3 mgV/day provoked increased Fe deposits in the tissues, which promoted a protein oxidative damage in the liver.
机译:钒作为微量营养素和低血糖剂的作用尚未完全澄清。进行了本研究,以研究钒处理后糖尿病STZ大鼠的铁和抗氧化剂防御的变化。检查四组:控制;糖尿病;糖尿病用1 mgv /天治疗;和糖尿病用3 mgV /天治疗。钒被供应的饮用水作为BIS(麦芽甲咯酸盐)氧化铵(IV)(BMOV)。实验的持续时间为五周。铁以食物,粪便,尿液,血清,肌肉,肾,肝,脾和股骨。超氧化物歧化酶,过氧化氢酶,NAD(P)H:测定肝脏中氧化酶-1(NQO1)活性和蛋白质羰基水平。与对照大鼠相比,在糖尿病大鼠中,记录了肾脏,肌肉和股骨中的肾脏,肌肉和股骨中的Fe含量和NQO1活性。在用3mgV /天处理的大鼠中,与糖尿病组相比,肝脏,脾脏和心脏,过氧化氢酶活性和蛋白质羰基的水平显着降低。结论BMOV是一种剂量依赖性低血糖药。用3 mgV /天的治疗挑起了组织中的加入Fe沉积物,该钙损伤在肝脏中促进蛋白质氧化损伤。

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