首页> 外文期刊>Neurochemistry International: The International Journal for the Rapid Publication of Critical Reviews, Preliminary and Original Research Communications in Neurochemistry >Early biochemical and histological alterations in rat corticoencephalic cell cultures following metabolic damage and treatment with modulators of mitochondrial ATP-sensitive potassium channels.
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Early biochemical and histological alterations in rat corticoencephalic cell cultures following metabolic damage and treatment with modulators of mitochondrial ATP-sensitive potassium channels.

机译:代谢损伤和线粒体ATP敏感性钾通道调节剂治疗后大鼠皮质脑细胞培养物中的早期生化和组织学改变。

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摘要

The present study was aimed at characterizing alterations of the nucleotide content and morphological state of rat corticoencephalic cell cultures subjected to metabolic damage and treatment with modulators of mitochondrial ATP-dependent potassium channels (mitoK(ATP)). In a first series of experiments, in vitro ischemic changes of the contents of purine and pyrimidine nucleoside diphosphates and triphosphates were measured by high performance liquid chromatography (HPLC) and the corresponding histological alterations were determined by celestine blue/acid fuchsin staining. As an ischemic stimulus, incubation with a glucose-free medium saturated with argon was used. Ischemia decreased the levels of adenosine, guanine and uridine triphosphate (ATP, GTP, UTP) and increased the levels of the respective dinucleotides ADP and UDP, whereas the GDP content was not changed. Both 5-hydroxydecanoate (5-HD) and diazoxide failed to alter the contents of nucleoside diphosphates and triphosphates, when applied undernormoxic conditions. 5-HD (30 microM) prevented the ischemia-induced changes of nucleotide and nucleoside levels. Diazoxide (300 microM), either alone or in combination with 5-hydroxydecanoate (30 microM) was ineffective. Pyruvate (5 mM) partially reversed the effects of ischemia or ischemia plus 2-deoxyglucose (20mM) in the incubation medium. Diazoxide (300 microM) and 5-HD (30 microM) had no effect in the presence of pyruvate (5mM) and 2-deoxyglucose (20mM). Staining the cells with celestine blue/acid fuchsin in order to classify them as intact, reversibly or profoundly injured, revealed a protective effect of 5-HD. When compared with 5-HD, diazoxide, pyruvate and 2-deoxyglucose had similar but less pronounced effects. In conclusion, these results suggest a protective role of 5-hydroxydecanoate on early corticoencephalic nucleotide and cell viability alterations during ischemia.
机译:本研究旨在表征遭受代谢损伤并用线粒体ATP依赖性钾离子通道(mitoK(ATP))调节剂处理的大鼠皮质脑细胞培养物中核苷酸含量和形态状态的变化。在第一个系列实验中,通过高效液相色谱(HPLC)测量嘌呤和嘧啶核苷二磷酸和三磷酸含量的体外缺血变化,并通过天青蓝/酸性品红染色确定相应的组织学改变。作为缺血刺激,使用与饱和了氩气的无葡萄糖培养基一起孵育。缺血降低了腺苷,鸟嘌呤和尿苷三磷酸(ATP,GTP,UTP)的水平,并增加了各自的二核苷酸ADP和UDP的水平,而GDP含量没有变化。在常氧条件下使用时,5-羟基癸酸酯(5-HD)和二氮嗪均不能改变二磷酸核苷和三磷酸核苷的含量。 5-HD(30 microM)阻止了缺血诱导的核苷酸和核苷水平的变化。单独或与5-羟基癸酸酯(30 microM)组合使用的二氮嗪(300 microM)无效。丙酮酸(5 mM)在培养液中部分逆转了局部缺血或局部缺血加2-脱氧葡萄糖(20mM)的作用。在丙酮酸(5mM)和2-脱氧葡萄糖(20mM)存在下,二氮嗪(300 microM)和5-HD(30 microM)没有作用。为了将细胞分类为完整,可逆或受到严重损伤,用天青蓝/酸性品红将细胞染色,可以发现5-HD具有保护作用。当与5-HD相比时,二氮嗪,丙酮酸和2-脱氧葡萄糖具有相似但不太明显的作用。总之,这些结果表明5-羟基癸酸酯对缺血期间早期皮质脑核苷酸和细胞活力改变的保护作用。

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