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Increased levels of RNA oxidation enhance the reversion frequency in aging pro-apoptotic yeast mutants

机译:RNA氧化水平的提高提高了衰老促凋亡酵母突变体的回复频率

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摘要

Despite recent advances in understanding the complexity of RNA processes, regulation of the metabolism of oxidized cellular RNAs and the mechanisms through which oxidized ribonucleotides affect mRNA translation, and consequently cell viability, are not well characterized. We show here that the level of oxidized RNAs is markedly increased in a yeast decapping Kllsm4Δ1 mutant, which accumulates mRNAs, ages much faster that the wild type strain and undergoes regulated-cell-death. We also found that in Kllsm4Δ1 cells the mutation rate increases during chronological life span indicating that the capacity to handle oxidized RNAs in yeast declines with aging. Lowering intracellular ROS levels by antioxidants recovers the wild-type phenotype of mutant cells, including reduced amount of oxidized RNAs and lower mutation rate. Since mRNA oxidation was reported to occur in different neurodegenerative diseases, decapping-deficient cells may represent a useful tool for deciphering molecular mechanisms of cell response to such conditions, providing new insights into RNA modification-based pathogenesis.
机译:尽管最近在理解RNA过程的复杂性方面取得了进展,但是对氧化的细胞RNA的代谢的调节以及氧化的核糖核苷酸影响mRNA翻译并因此影响细胞生存力的机制尚不十分清楚。我们在这里显示,在酵母中,使RNA脱帽的Kllsm4Δ1突变体显着增加了氧化RNA的水平,该突变体积累了mRNA,其衰老速度比野生型菌株快得多,并经历了调节性细胞死亡。我们还发现,在Kllsm4Δ1细胞中,随着时间的推移,突变率会增加,这表明随着年龄的增长,处理酵母中氧化RNA的能力会下降。通过抗氧化剂降低细胞内ROS水平可恢复突变细胞的野生型表型,包括减少氧化的RNA量和降低突变率。由于据报道,mRNA氧化发生在不同的神经退行性疾病中,因此,缺乏去皮细胞的细胞可能代表着一种有用的工具,用于破译这种情况下细胞反应的分子机制,从而为基于RNA修饰的发病机理提供了新的见识。

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