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首页> 外文期刊>Mutagenesis >A colony color method identifies the vulnerability of mitochondria to oxidative damage.
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A colony color method identifies the vulnerability of mitochondria to oxidative damage.

机译:菌落颜色法可识别线粒体对氧化损伤的脆弱性。

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摘要

Mitochondrial dysfunction is a profound feature of cancer cells and is also known to cause several mitochondrial diseases. Mutations in mitochondrial DNA (mtDNA) have been reported frequently in these diseases. Although many environmental agents are known to cause damage to mitochondria, rapid methods need to be developed for testing agents that cause mitochondrial dysfunction and are involved in the development of mitochondrial and other diseases. Using Saccharomyces cerevisiae, we describe the development of a colorimetric method that identifies both physical and chemical agents that cause mitochondrial dysfunction and mutation of the mitochondrial genome. This method utilizes the previously reported ade2 mutant of S.cerevisiae that produces red colonies. However, when they lose mitochondrial function the colonies turn white. This colorimetric method has helped quantify the vulnerability of mtDNA to oxidative agents. Our study reveals that the oxidative agent adriamycin causes both mutation and extensive damage to mtDNA, which leads to loss of mtDNA. Our study also reveals that the lost mtDNA fragments migrate to the nucleus and integrate into the nuclear genome. Furthermore, our analysis reveals that loss of mtDNA leads to resistance to oxidative agents. The method described in this paper should aid in the rapid identification of environmental and other agents that cause mitochondrial dysfunction and mutagenesis, agents that may be involved in the development of mitochondrial and other diseases.
机译:线粒体功能障碍是癌细胞的重要特征,并且还已知会引起多种线粒体疾病。在这些疾病中,线粒体DNA(mtDNA)的突变已被频繁报道。尽管已知许多环境因子会破坏线粒体,但需要开发快速方法来检测导致线粒体功能障碍并参与线粒体和其他疾病发展的试剂。使用酿酒酵母,我们描述了比色法的发展,该比色法可识别引起线粒体功能障碍和线粒体基因组突变的物理和化学试剂。该方法利用先前报道的酿酒酵母的ade2突变体,该突变体产生红色菌落。但是,当它们失去线粒体功能时,菌落变成白色。这种比色方法有助于量化mtDNA对氧化剂的脆弱性。我们的研究表明,氧化剂阿霉素会引起mtDNA突变和广泛损伤,从而导致mtDNA丢失。我们的研究还揭示了丢失的mtDNA片段迁移到细胞核并整合到核基因组中。此外,我们的分析表明,mtDNA的丢失会导致对氧化剂的抗性。本文所述的方法应有助于快速识别导致线粒体功能障碍和诱变的环境因素和其他因素,以及可能与线粒体疾病和其他疾病的发展有关的因素。

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