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Duchenne muscular dystrophy animal models for high-throughput drug discovery and precision medicine

机译:Duchenne肌肉营养不良动物模型用于高通量药物发现和精密医学

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Introduction: Duchenne muscular dystrophy (DMD) is an X-linked handicapping disease due to the loss of an essential muscle protein dystrophin. Dystrophin-null animals have been extensively used to study disease mechanisms and to develop experimental therapeutics. Despite decades of research, however, treatment options for DMD remain very limited. Areas covered: High-throughput high-content screening and precision medicine offer exciting new opportunities. Here, the authors review animal models that are suitable for these studies. Expert opinion: Nonmammalian models (worm, fruit fly, and zebrafish) are particularly attractive for cost-effective large-scale drug screening. Several promising lead compounds have been discovered using these models. Precision medicine for DMD aims at developing mutation-specific therapies such as exon-skipping and genome editing. To meet these needs, models with patient-like mutations have been established in different species. Models that harbor hotspot mutations are very attractive because the drugs developed in these models can bring mutation-specific therapies to a large population of patients. Humanized hDMD mice carry the entire human dystrophin gene in the mouse genome. Reagents developed in the hDMD mouse-based models are directly translatable to human patients.
机译:介绍:Duchenne肌肉营养不良(DMD)是一种X链接的肌肉蛋白营养不良蛋白损失引起的疾病。 Dystophin-Null动物已被广泛地用于研究疾病机制并开发实验治疗方法。然而,尽管有数十年的研究,但DMD的治疗方案仍然非常有限。所涵盖的区域:高通量高含量筛选和精密医学提供令人兴奋的新机遇。在这里,作者审查适合这些研究的动物模型。专家意见:非含糊性模型(蠕虫,果蝇和斑马鱼)对于具有成本效益的大规模药物筛查特别有吸引力。使用这些模型发现了几种有前途的铅化合物。 DMD的精密药物旨在开发突变特异性疗法,例如外显子跳跃和基因组编辑。为了满足这些需求,已经在不同物种中建立了具有患者样突变的模型。港口热点突变的模型非常有吸引力,因为这些模型中的药物可以将突变特异性疗法带到大群患者。人源化的HDMD小鼠在小鼠基因组中携带整个人营养不良蛋白基因。在基于HDMD鼠标的模型中开发的试剂直接与人类患者翻译。

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