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Yeast as a system for modeling mitochondrial disease mechanisms and discovering therapies

机译:酵母作为模拟线粒体疾病机制和发现疗法的系统

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Mitochondrial diseases are severe and largely untreatable. Owing to the many essential processes carried out by mitochondria and the complex cellular systems that support these processes, these diseases are diverse, pleiotropic, and challenging to study. Much of our current understanding of mitochondrial function and dysfunction comes from studies in the baker's yeast Saccharomyces cerevisiae. Because of its good fermenting capacity, S. cerevisiae can survive mutations that inactivate oxidative phosphorylation, has the ability to tolerate the complete loss of mitochondrial DNA (a property referred to as ‘petite-positivity’), and is amenable to mitochondrial and nuclear genome manipulation. These attributes make it an excellent model system for studying and resolving the molecular basis of numerous mitochondrial diseases. Here, we review the invaluable insights this model organism has yielded about diseases caused by mitochondrial dysfunction, which ranges from primary defects in oxidative phosphorylation to metabolic disorders, as well as dysfunctions in maintaining the genome or in the dynamics of mitochondria. Owing to the high level of functional conservation between yeast and human mitochondrial genes, several yeast species have been instrumental in revealing the molecular mechanisms of pathogenic human mitochondrial gene mutations. Importantly, such insights have pointed to potential therapeutic targets, as have genetic and chemical screens using yeast.
机译:线粒体疾病很严重,而且基本上无法治愈。由于线粒体执行了许多基本过程,并且复杂的细胞系统支持了这些过程,因此这些疾病是多种多样的,多效的,并且难以研究。我们目前对线粒体功能和功能障碍的大部分了解来自面包酵母啤酒酵母的研究。由于其良好的发酵能力,酿酒酵母可以幸免于灭活氧化磷酸化的突变,具有耐受线粒体DNA完全丧失的能力(一种称为“小正性”的特性),并且适合线粒体和核基因组操纵。这些属性使其成为研究和解决众多线粒体疾病分子基础的优秀模型系统。在这里,我们回顾了这种模式生物对线粒体功能障碍引起的疾病的宝贵见解,其范围从氧化磷酸化的主要缺陷到代谢紊乱,以及基因组或线粒体动力学的功能障碍。由于酵母和人类线粒体基因之间的功能保守性很高,因此几种酵母菌在揭示致病性人类线粒体基因突变的分子机制中发挥了作用。重要的是,这些见解指出了潜在的治疗目标,使用酵母的基因和化学筛选也是如此。

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