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Defects of mitochondrial RNA turnover lead to the accumulation of double-stranded RNA in vivo

机译:线粒体RNA更新的缺陷导致体内双链RNA的积累

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摘要

The RNA helicase SUV3 and the polynucleotide phosphorylase PNPase are involved in the degradation of mitochondrial mRNAs but their roles in vivo are not fully understood. Additionally, upstream processes, such as transcript maturation, have been linked to some of these factors, suggesting either dual roles or tightly interconnected mechanisms of mitochondrial RNA metabolism. To get a better understanding of the turn-over of mitochondrial RNAs in vivo, we manipulated the mitochondrial mRNA degrading complex in Drosophila melanogaster models and studied the molecular consequences. Additionally, we investigated if and how these factors interact with the mitochondrial poly(A) polymerase, MTPAP, as well as with the mitochondrial mRNA stabilising factor, LRPPRC. Our results demonstrate a tight interdependency of mitochondrial mRNA stability, polyadenylation and the removal of antisense RNA. Furthermore, disruption of degradation, as well as polyadenylation, leads to the accumulation of double-stranded RNAs, and their escape out into the cytoplasm is associated with an altered immune-response in flies. Together our results suggest a highly organised and inter-dependable regulation of mitochondrial RNA metabolism with far reaching consequences on cellular physiology.
机译:RNA解旋酶SUV3和多核苷酸磷酸化酶PNPase参与线粒体mRNA的降解,但它们在体内的作用尚不完全清楚。另外,上游过程,例如转录物成熟,已经与这些因素中的一些联系在一起,表明线粒体RNA代谢的双重作用或紧密联系的机制。为了更好地了解体内线粒体RNA的转换,我们在果蝇模型中处理了线粒体mRNA降解复合物,并研究了分子后果。此外,我们调查了这些因素是否以及如何与线粒体多聚(A)聚合酶MTPAP以及线粒体mRNA稳定因子LRPPRC相互作用。我们的研究结果表明线粒体mRNA稳定性,聚腺苷酸化和反义RNA的去除之间紧密相关。此外,降解的破坏以及聚腺苷酸化会导致双链RNA的积累,而它们逃逸进入细胞质与果蝇中免疫反应的改变有关。我们的研究结果共同表明线粒体RNA代谢的高度组织化和相互依赖的调节对细胞生理学具有深远的影响。

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