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CuATSM efficacy is independently replicated in a SOD1 mouse model of ALS while unmetallated ATSM therapy fails to reveal benefits

机译:CuATSM功效可在ALS的SOD1小鼠模型中独立复制而未金属化的ATSM疗法无法显示其益处

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摘要

A copper chelator known as diacetylbis(N(4)-methylthiosemicarbazonato) copper II (CuATSM), has been reported to be efficacious in multiple transgenic SOD1 models of amyotrophic lateral sclerosis (ALS), a fatal neurodegenerative disorder affecting motor neurons. Here we report that we also observed CuATSM efficacy on disease onset and progression in a standardized litter-matched and gender-balanced efficacy study using B6SJL-SOD1G93A/1Gur mice. We also report improved survival trends with CuATSM treatment. In addition, we report a lack of efficacy by unmetallated ATSM in the same model using the same standardized study design. These results add to existing evidence supporting an efficacious role for copper delivery using chaperone molecules in mouse models of ALS.
机译:铜螯合剂称为二乙酰基双(N(4)-甲硫基氨基甲酸铜)铜II(CuATSM),据报道在肌萎缩性侧索硬化症(ALS)的多种转基因SOD1模型中有效,后者是一种影响运动神经元的致命性神经退行性疾病。在这里,我们报告说,我们还在使用B6SJL-SOD1G93A / 1Gur小鼠的标准化产仔匹配和性别平衡功效研究中观察到了CuATSM对疾病发作和进展的功效。我们还报告了CuATSM治疗改善了生存趋势。此外,我们报告了使用相同标准化研究设计的相同模型中非金属化ATSM缺乏疗效。这些结果增加了现有证据,支持在伴侣的ALS小鼠模型中使用分子伴侣分子对铜的有效递送。

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