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首页> 外文期刊>Human Molecular Genetics >Combined use of Saccharomyces cerevisiae, Caenorhabditis elegans and patient fibroblasts leads to the identification of clofilium tosylate as a potential therapeutic chemical against POLG-related diseases
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Combined use of Saccharomyces cerevisiae, Caenorhabditis elegans and patient fibroblasts leads to the identification of clofilium tosylate as a potential therapeutic chemical against POLG-related diseases

机译:酿酒酵母,秀丽隐杆线虫和患者成纤维细胞的组合使用可导致鉴定甲苯磺酸clofilium作为潜在的化学疗法,可预防POLG相关疾病

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摘要

Mitochondria are organelles that have their own DNA (mitochondrial DNA, mtDNA) whose maintenance is necessary for the majority of ATP production in eukaryotic cells. Defects in mtDNA maintenance or integrity are responsible for numerous diseases. The DNA polymerase. (POLG) ensures proper mtDNA replication and repair. Mutations in POLG are a major cause of mitochondrial disorders including hepatic insufficiency, Alpers syndrome, progressive external ophthalmoplegia, sensory neuropathy and ataxia. Mutations in POLG are also associated with parkinsonism. To date, no effective therapy is available. Based on the conservation of mitochondrial function from yeast to human, we used Saccharomyces cerevisiae and Caenorhabditis elegans as first pass filters to identify a chemical that suppresses mtDNA instability in cultured fibroblasts of a POLG-deficient patient. We showed that this unsuspected compound, clofilium tosylate (CLO), belonging to a class of anti-arrhythmic agents, prevents mtDNA loss of all yeast mitochondrial polymerase mutants tested, improves behavior and mtDNA content of polg-1-deficient worms and increases mtDNA content of quiescent POLG-deficient fibroblasts. Furthermore, the mode of action of the drug seems conserved as CLO increases POLG steady-state level in yeast and human cells. Two other anti-arrhythmic agents (FDA-approved) sharing common pharmacological properties and chemical structure also show potential benefit for POLG deficiency in C. elegans. Our findings provide evidence of the first mtDNA-stabilizing compound that may be an effective pharmacological alternative for the treatment of POLG-related diseases.
机译:线粒体是具有自己的DNA(线粒体DNA,mtDNA)的细胞器,其维持对于真核细胞中大多数ATP产生是必需的。 mtDNA维持或完整性缺陷导致多种疾病。 DNA聚合酶。 (POLG)可确保正确的mtDNA复制和修复。 POLG中的突变是线粒体疾病的主要原因,包括肝功能不全,Alpers综合征,进行性眼外肌麻痹,感觉神经病和共济失调。 POLG中的突变也与帕金森氏症相关。迄今为止,尚无有效的疗法。基于从酵母到人的线粒体功能的保守性,我们使用酿酒酵母和秀丽隐杆线虫作为首过滤器,以鉴定一种抑制POLG缺乏患者培养的成纤维细胞中mtDNA不稳定性的化学物质。我们证明了这种未被怀疑的化合物,甲苯磺酸clofilium(CLO),属于一类抗心律不齐药物,可防止所有测试的酵母线粒体聚合酶突变体的mtDNA丢失,改善缺乏polg-1的蠕虫的行为和mtDNA含量,并增加mtDNA含量静态POLG缺乏的成纤维细胞。此外,由于CLO增加了酵母和人类细胞中POLG稳态水平,因此该药物的作用方式似乎是保守的。具有共同药理特性和化学结构的其他两种抗心律不齐药(经FDA批准)也显示了秀丽隐杆线虫中POLG缺乏的潜在益处。我们的发现提供了第一个稳定mtDNA的化合物的证据,该化合物可能是治疗POLG相关疾病的有效药理学替代品。

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