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首页> 外文期刊>The Indian journal of medical research >In vivo oxalate degradation by liposome encapsulated oxalate oxidase in rat model of hyperoxaluria
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In vivo oxalate degradation by liposome encapsulated oxalate oxidase in rat model of hyperoxaluria

机译:脂质体包裹草酸氧化酶在高草酸尿大鼠模型中体内草酸的降解

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摘要

Background & objectives: High level of urinary oxalate substantially increases the risk of hyperoxaluria, a significant risk factor for urolithiasis. The primary goal of this study was to reduce urinary oxalate excretion employing liposome encapsulated oxalate oxidase in animal model. Methods: A membrane bound oxalate oxidase was purified from Bougainvillea leaves. The enzyme in its native form was less effective at the physiological pH of the recipient animal. To increase its functional viability, the enzyme was immobilized on to ethylene maleic anhydride (EMA). Rats were injected with liposome encapsulated EMA- oxalate oxidase and the effect was observed on degradation of oxalic acid. Results: The enzyme was purified to apparent homogeneity with 60-fold purification and 31 per cent yield. The optimum pH of EMA-derivative enzyme was 6.0 and it showed 70 per cent of its optimal activity at pH 7.0. The EMA-bound enzyme encapsulated into liposome showed greater oxalate degradation in 15 per cent casein vitamin B 6 deficient fed rats as compared with 30 per cent casein vitamin B 6 deficient fed rats and control rats. Interpretation & conclusions: EMA-oxalate oxidase encapsulated liposome caused oxalate degradation in experimental hyperoxaluria indicating that the enzyme could be used as a therapeutic agent in hyperoxaluria leading to urinary stones.
机译:背景与目的:草酸尿的高水平会大大增加高尿酸尿症的风险,高尿酸尿症是尿路结石的重要危险因素。这项研究的主要目的是在动物模型中使用脂质体包裹的草酸氧化酶来减少尿草酸的排泄。方法:从九重葛叶中纯化膜结合草酸氧化酶。天然形式的酶在受体动物的生理pH下效果较差。为了增加其功能生存力,将酶固定在乙烯马来酸酐(EMA)上。给大鼠注射脂质体包裹的EMA-草酸氧化酶,观察其对草酸降解的影响。结果:该酶被纯化至明显的均一性,纯化了60倍,产率为31%。 EMA衍生物酶的最适pH为6.0,在7.0时显示其最佳活性的70%。封装在脂质体中的与EMA结合的酶在15%酪蛋白缺乏维生素B 6 的大鼠中显示出草酸盐的降解,而30%酪蛋白缺乏维生素B 6 缺乏的大鼠和对照组。解释与结论:EMA-草酸氧化酶包裹的脂质体导致实验性高草酸尿症中草酸盐的降解,表明该酶可以用作高草酸尿症的治疗剂,导致尿结石。

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