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Drug repositioning screening identifies etravirine as a potential therapeutic for friedreich's ataxia

机译:药物重新定位筛选将etravirine鉴定为Friedreich Ataxia的潜在治疗方法

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ABSTRACT Background Friedreich's ataxia is an autosomal‐recessive cerebellar ataxia caused by mutation of the frataxin gene, resulting in decreased frataxin expression, mitochondrial dysfunction, and oxidative stress. Currently, no treatment is available for Friedreich's ataxia patients. Given that levels of residual frataxin critically affect disease severity, the main goal of a specific therapy for Friedreich's ataxia is to increase frataxin levels. Objectives With the aim to accelerate the development of a new therapy for Friedreich's ataxia, we took a drug repositioning approach to identify market‐available drugs able to increase frataxin levels. Methods Using a cell‐based reporter assay to monitor variation in frataxin amount, we performed a high‐throughput screening of a library containing 853 U.S. Food and Drug Administration–approved drugs. Results Among the potentially interesting candidates isolated from the screening, we focused our attention on etravirine, an antiviral drug currently in use as an anti–human immunodeficiency virus therapy. Here, we show that etravirine can promote a significant increase in frataxin levels in cells derived from Friedreich's ataxia patients, by enhancing frataxin messenger RNA translation. Importantly, frataxin accumulation in treated patient cell lines is comparable to frataxin levels in unaffected carrier cells, suggesting that etravirine could be therapeutically relevant. Indeed, etravirine treatment restores the activity of the iron‐sulphur cluster containing enzyme aconitase and confers resistance to oxidative stress in cells derived from Friedreich's ataxia patients. Conclusions Considering its excellent safety profile along with its ability to increase frataxin levels and correct some of the disease‐related defects, etravirine represents a promising candidate as a therapeutic for Friedreich's ataxia. ? 2019 International Parkinson and Movement Disorder Society
机译:摘要背景Firedreich的共济失调是由Frataxin基因的突变引起的常染色体隐性小脑共济失调,导致脱脂蛋白表达减少,线粒体功能障碍和氧化应激。目前,Friedreich的Ataxia患者没有任何治疗方法。鉴于残留毒素的水平危重影响疾病严重程度,对Friedreich的共济失调的特异性治疗的主要目标是增加稻草蛋白水平。目标旨在加快开发为弗里德雷希的共济失调的新疗法的发展,我们采取了一种药物排雷方法来识别能够增加脱脂蛋白水平的市场可用药物。方法采用基于细胞的报告检测来监测脱脂量的变化,我们进行了含有853中食品和药物管理批准的药物的文库的高通量筛选。结果在筛选中孤立的潜在有趣的候选者中,我们将注意力集中在etravirine上,是目前用作抗人类免疫缺陷病毒治疗的抗病毒药物。在这里,我们表明etravirine可以通过增强Fratraxin Messenger RNA翻译,促进弗里德莱希亚患者的细胞中的细胞中脱脂蛋白水平的显着增加。重要的是,治疗患者细胞系中的脱脂蛋白积累与未受影响的载体细胞中的脱臼水平相当,表明etravirine可以治疗相关。实际上,埃拉夫林治疗恢复了含有酶穴位酶的铁 - 硫簇的活性,并赋予源自Friedreich Ataxia患者的细胞中的氧化胁迫的抗性。结论考虑其出色的安全性型材以及其增加稻草素水平并纠正一些与疾病相关的缺陷的能力,埃拉夫里林代表了一个有希望的候选人,作为Friedreich Ataxia的治疗方法。还2019年国际帕金森和运动障碍协会

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  • 来源
    《Movement disorders 》 |2019年第3期| 共13页
  • 作者单位

    Laboratory of Signal Transduction Department of Biomedicine and PreventionUniversity of Rome “Tor;

    Laboratory of Signal Transduction Department of Biomedicine and PreventionUniversity of Rome “Tor;

    Laboratory of Signal Transduction Department of Biomedicine and PreventionUniversity of Rome “Tor;

    Laboratory of Molecular Neurobiology Department of Biomedicine and PreventionUniversity of Rome;

    Laboratory of Molecular Neurobiology Department of Biomedicine and PreventionUniversity of Rome;

    Laboratory of Signal Transduction Department of Biomedicine and PreventionUniversity of Rome “Tor;

    Laboratory of Signal Transduction Department of Biomedicine and PreventionUniversity of Rome “Tor;

    Medical Physics Section Department of Biomedicine and PreventionUniversity of Rome “Tor Vergata;

    Laboratory of Signal Transduction Department of Biomedicine and PreventionUniversity of Rome “Tor;

    Laboratory of Signal Transduction Department of Biomedicine and PreventionUniversity of Rome “Tor;

    Laboratory of Molecular Neurobiology Department of Biomedicine and PreventionUniversity of Rome;

    Laboratory of Signal Transduction Department of Biomedicine and PreventionUniversity of Rome “Tor;

    Laboratory of Signal Transduction Department of Biomedicine and PreventionUniversity of Rome “Tor;

    Laboratory of Signal Transduction Department of Biomedicine and PreventionUniversity of Rome “Tor;

    Laboratory of Signal Transduction Department of Biomedicine and PreventionUniversity of Rome “Tor;

    Laboratory of Signal Transduction Department of Biomedicine and PreventionUniversity of Rome “Tor;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 神经病学 ;
  • 关键词

    drug repositioning; etravirine; frataxin; Friedreich's ataxia;

    机译:药物重新定位;etravirine;frataxin;friedreich的共济失调;

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