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Loss of the RNA helicase SKIV2L2 impairs mitotic progression and replication-dependent histone mRNA turnover in murine cell lines

机译:RNA Helicase Skiv2L2的丧失损害鼠细胞系中的有丝分裂进展和复制依赖性组蛋白mRNA果实

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RNA surveillance via the nuclear exosome requires cofactors such as the helicase SKIV2L2 to process and degrade certain noncoding RNAs. This research aimed to characterize the phenotype associated with RNAi knockdown of Skiv2I2 in two murine cancer cell lines: Neuro2A and P19. SKIV2L2 depletion in Neuro2A and P19 cells induced changes in gene expression indicative of cell differentiation and reduced cellular proliferation by 30%. Propidium iodide-based cell-cycle analysis of Skiv2I2 knockdown cells revealed defective progression through the G2/M phase and an accumulation of mitotic cells, suggesting SKIV2L2 contributes to mitotic progression. Since SKIV2L2 targets RNAs to the nuclear exosome for processing and degradation, we identified RNA targets elevated in cells depleted of SKIV2L2 that could account for the observed twofold increase in mitotic cells. Skiv2I2 knockdown cells accumulated replication-dependent histone mRNAs, among other RNAs, that could impede mitotic progression and indirectly trigger differentiation.
机译:通过核外泌体的RNA监测需要辅助粘液剂,例如螺旋酶SKIV2L2来处理和降解某些非编码RNA。该研究旨在表征与两只小鼠癌细胞系中Skiv2i2的RNAi敲低相关的表型:Neuro2a和P19。 Neuro2a和P19细胞中的Skiv2L2耗竭诱导指示细胞分化的基因表达的变化,降低细胞增殖30%。 Skiv2i2敲低细胞的碘化钛基细胞循环分析通过G2 / M相显示出缺陷的进展和有丝分裂细胞的积累,表明Skiv2L2有助于有丝分裂进展。由于Skiv2L2靶向RNA以核外泌体进行加工和降解,因此我们鉴定了在Skiv2L2的细胞中升高的RNA靶标,这可能考虑在有丝分裂细胞中观察到的双重增加。 Skiv2i2敲低细胞累积复制依赖性组蛋白MRNA,其中rNA可以妨碍有丝分裂进展和间接触发分化。

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