首页> 外文期刊>Scientific reports. >Induced pluripotent stem cells-derived neurons from patients with Friedreich ataxia exhibit differential sensitivity to resveratrol and nicotinamide
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Induced pluripotent stem cells-derived neurons from patients with Friedreich ataxia exhibit differential sensitivity to resveratrol and nicotinamide

机译:来自Friedreich Ataxia患者的诱导多能干细胞衍生的神经元对白藜芦醇和烟酰胺具有差异敏感性

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Translation of pharmacological results from in vitro cell testing to clinical trials is challenging. One of the causes that may underlie these discrepant results is the lack of the phenotypic or species-specific relevance of the tested cells; today, this lack of relevance may be reduced by relying on cells differentiated from human pluripotent stem cells. To analyse the benefits provided by this approach, we chose to focus on Friedreich ataxia, a neurodegenerative condition for which the recent clinical testing of two compounds was not successful. These compounds, namely, resveratrol and nicotinamide, were selected because they had been shown to stimulate the expression of frataxin in fibroblasts and lymphoblastoid cells. Our results indicated that these compounds failed to do so in iPSC-derived neurons generated from two patients with Friedreich ataxia. By comparing the effects of both molecules on different cell types that may be considered to be non-relevant for the disease, such as fibroblasts, or more relevant to the disease, such as neurons differentiated from iPSCs, a differential response was observed; this response suggests the importance of developing more predictive in vitro systems for drug discovery. Our results demonstrate the value of utilizing human iPSCs early in drug discovery to improve translational predictability.
机译:来自体外细胞测试对临床试验的药理学结果的翻译是挑战性的。这些差异结果可能提出的原因之一是缺乏测试细胞的表型或物种的特异性;如今,通过依赖于从人多能干细胞分化的细胞可以减少这种缺乏相关性。为了分析这种方法所提供的福利,我们选择专注于Friedreich Ataxia,一种神经变性病症,最近对两种化合物的临床检测不成功。选择这些化合物,即白藜芦醇和烟酰胺,因为它们已被证明刺激成纤维细胞和淋巴细胞细胞中脱脂蛋白的表达。我们的结果表明,这些化合物未能在来自两名Friedreich Ataxia的两名患者产生的IPSC衍生的神经元中。通过比较两种分子对不同细胞类型的影响,这些不同细胞类型对于对疾病的疾病(例如成纤维细胞)或与疾病的更相关的不同细胞类型,例如从IPSC分化的神经元,观察到差异反应;这种反应表明为制定更预测的体外系统进行药物发现的重要性。我们的结果表明,在药物发现早期利用人IPSC的价值,以提高平移可预测性。

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