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Double-stranded DNA-dependent ATPase Irc3p is directly involved in mitochondrial genome maintenance

机译:双链依赖DNA的ATPase Irc3p直接参与线粒体基因组的维持

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Nucleic acid-dependent ATPases are involved in nearly all aspects of DNA and RNA metabolism. Previous studies have described a number of mitochondrial helicases. However, double-stranded DNA-dependent ATPases, including translocases or enzymes remodeling DNA-protein complexes, have not been identified in mitochondria of the yeast Saccha-romyces cerevisae. Here, we demonstrate that Irc3p is a mitochondrial double-stranded DNA-dependent ATPase of the Superfamily II. In contrast to the other mitochondrial Superfamily II enzymes Mss116p, Suv3p and Mrh4p, which are RNA helicases, Irc3p has a direct role in mitochondrial DNA (mtDNA) maintenance. Specific Irc3p-dependent mtDNA metabolic intermediates can be detected, including high levels of double-stranded DNA breaks that accumulate in irc3 Delta mutants. irc3 Delta-related topology changes in rho-mtDNA can be reversed by the deletion of mitochondrial RNA polymerase RPO41, suggesting that Irc3p counterbalances adverse effects of transcription on mitochondrial genome stability.
机译:核酸依赖性ATP酶几乎涉及DNA和RNA代谢的所有方面。先前的研究已经描述了许多线粒体解旋酶。但是,尚未在酵母酿酒酵母的线粒体中鉴定出双链DNA依赖性ATP酶,包括转位酶或重塑DNA-蛋白质复合物的酶。在这里,我们证明Irc3p是超家族II的线粒体双链DNA依赖性ATPase。与其他线粒体超家族II酶Mss116p,Suv3p和Mrh4p(RNA解旋酶)相反,Irc3p在线粒体DNA(mtDNA)维护中具有直接作用。可以检测到特定的Irc3p依赖型mtDNA代谢中间体,包括在irc3 Delta突变体中积累的高水平双链DNA断裂。 rh-mtDNA的irc3 Delta相关拓扑变化可以通过线粒体RNA聚合酶RPO41的缺失来逆转,这表明Irc3p平衡了转录对线粒体基因组稳定性的不利影响。

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