首页> 外文期刊>Journal of enzyme inhibition and medicinal chemistry. >Expression of heterologous oxalate decarboxylase in HEK293 cells confers protection against oxalate induced oxidative stress as a therapeutic approach for calcium oxalate stone disease
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Expression of heterologous oxalate decarboxylase in HEK293 cells confers protection against oxalate induced oxidative stress as a therapeutic approach for calcium oxalate stone disease

机译:草酸钙脱羧酶在HEK293细胞中的表达可保护草酸诱导的氧化应激,作为草酸钙结石病的治疗方法

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Abstract Oxalates stimulate alterations in renal epithelial cells and thereby induce calcium oxalate (CaOx) stone formation. Bacillus subtilis YvrK gene encodes for oxalate decarboxylase (OxdC) which degrades oxalate to formate and CO2. The present work is aimed to clone the oxdC gene in a mammalian expression vector pcDNA and transfect into Human Embryonic Kidney 293 (HEK293) cells and evaluate the oxdC expression, cell survival rate and oxalate degrading efficiency. The results indicate cell survival rate of HEK293/pcDNAOXDC cells pre-incubated with oxalate was enhanced by 28%. HEK293/pcDNAOXDC cells expressing OxdC treated with oxalate, significantly restored antioxidant activity, mitochondrial membrane potential and intracellular reactive oxygen species (ROS) generation compared with HEK293/pcDNA. Apoptotic marker caspase 3 downregulation illustrates HEK293/pcDNAOXDC cells were able to survive under oxalate-mediated oxidative stress. The findings suggest HEK293 cells expressing oxdC capable of degrading oxalate protect cells from oxidative damage and thus serve as a therapeutic option for prevention of CaOx stone disease.
机译:摘要草酸盐刺激肾上皮细胞发生改变,从而诱导草酸钙(CaOx)结石形成。枯草芽孢杆菌YvrK基因编码草酸脱羧酶(OxdC),草酸脱羧酶将草酸降解为甲酸和CO 2 。本工作旨在在哺乳动物表达载体pcDNA中克隆oxdC基因,并将其转染到人胚肾293(HEK293)细胞中,并评估oxdC表达,细胞存活率和草酸盐降解效率。结果表明,草酸预孵育的HEK293 / pcDNAOXDC细胞的细胞存活率提高了28%。与HEK293 / pcDNA相比,草酸处理过的表达OxdC的HEK293 / pcDNAOXDC细胞可显着恢复抗氧化活性,线粒体膜电位和细胞内活性氧(ROS)生成。凋亡标记半胱天冬酶3的下调说明HEK293 / pcDNAOXDC细胞能够在草酸盐介导的氧化应激下存活。这些发现表明,表达能够降解草酸盐的oxdC的HEK293细胞可保护细胞免受氧化损伤,因此可作为预防CaOx结石病的治疗选择。

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