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首页> 外文期刊>Experimental Neurology >The efficacy of trientine or ascorbate alone compared to that of the combined treatment with these two agents in familial amyotrophic lateral sclerosis model mice.
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The efficacy of trientine or ascorbate alone compared to that of the combined treatment with these two agents in familial amyotrophic lateral sclerosis model mice.

机译:在家族性肌萎缩性侧索硬化模型小鼠中,单独使用曲恩汀或抗坏血酸的疗效与使用这两种药物联合治疗的疗效相比。

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摘要

One of the hypotheses regarding the pathogenesis of familial ALS (FALS) is a copper-mediated oxidative toxicity derived from the mutant Cu, Zn-superoxide dismutase (SOD1). We have previously demonstrated the efficacy of the combined treatment with a copper chelator (trientine) and an antioxidant (ascorbate) on the disease expression of the FALS-linked mutated SOD1 transgenic mice. Here, we investigated the efficacy of trientine or ascorbate alone on FALS mice when administered before or after the onset of the disease. The mice with a high dose of trientine or ascorbate administered before the onset survived significantly longer than the control. In the combined treatment with a high dose of trientine and ascorbate initiated before the onset, survival lengthened and the motor function of the mice remained more significantly than the control. None of the treatments affected the mean age of the onset, and none of the agents administered after the onset prolonged survival. These findings suggest that better outcomes may be expected by the administration of these agents at the preonset stage of the disease, and the combination of the agents acting on different sites might be useful in preserving the motor performance in FALS.
机译:关于家族性ALS(FALS)发病机理的一种假设是铜介导的氧化毒性,其源自突变型铜,锌超氧化物歧化酶(SOD1)。我们以前已经证明了与铜螯合剂(曲恩汀)和抗氧化剂(抗坏血酸)联合治疗对FALS连锁突变SOD1转基因小鼠的疾病表达的功效。在这里,我们研究了曲坦汀或抗坏血酸单独治疗FALS小鼠在疾病发作之前或之后的功效。在发作前给予高剂量曲汀或抗坏血酸的小鼠存活时间明显长于对照组。在发作前开始用高剂量曲汀和抗坏血酸的联合治疗,小鼠的存活期延长,运动功能仍比对照组明显。没有一种疗法会影响发作的平均年龄,并且在发作后施用的任何药物都不会延长生存期。这些发现表明,在疾病的发病前阶段施用这些药物可能会带来更好的结果,并且作用在不同部位的药物组合可能有助于保持FALS的运动功能。

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