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pri-miRNAs 的细胞质微处理器证据。

Evidence for a cytoplasmic microprocessor of pri-miRNAs.

机构信息

Department of Microbiology, Mount Sinai School of Medicine, New York, New York 10029, USA.

出版信息

RNA. 2012 Jul;18(7):1338-46. doi: 10.1261/rna.032268.112. Epub 2012 May 25.

Abstract

microRNAs (miRNAs) represent a class of noncoding RNAs that fine-tune gene expression through post-transcriptional silencing. While miRNA biogenesis occurs in a stepwise fashion, initiated by the nuclear microprocessor, rare noncanonical miRNAs have also been identified. Here we characterize the molecular components and unique attributes associated with the processing of virus-derived cytoplasmic primary miRNAs (c-pri-miRNAs). RNA in situ hybridization and inhibition of cellular division demonstrated a complete lack of nuclear involvement in c-pri-miRNA cleavage while genetic studies revealed that maturation still relied on the canonical nuclear RNase III enzyme, Drosha. The involvement of Drosha was mediated by a dramatic relocalization to the cytoplasm following virus infection. Deep sequencing analyses revealed that the cytoplasmic localization of Drosha does not impact the endogenous miRNA landscape during infection, despite allowing for robust synthesis of virus-derived miRNAs in the cytoplasm. Taken together, this research describes a unique function for Drosha in the processing of highly structured cytoplasmic RNAs in the context of virus infection.

摘要

微小 RNA(miRNAs)是一类非编码 RNA,通过转录后沉默来精细调控基因表达。虽然 miRNA 的生物发生是通过核微处理器逐步启动的,但也已经鉴定出罕见的非典型 miRNA。在这里,我们描述了与病毒衍生细胞质初级 miRNA(c-pri-miRNA)加工相关的分子成分和独特属性。RNA 原位杂交和细胞分裂抑制实验表明,c-pri-miRNA 切割完全不涉及细胞核,而遗传研究表明,成熟过程仍然依赖于经典的核 RNA 酶 III 酶 Drosha。Drosha 的参与是通过病毒感染后向细胞质的剧烈重定位介导的。深度测序分析表明,Drosha 的细胞质定位在感染过程中不会影响内源性 miRNA 景观,尽管它允许在细胞质中大量合成病毒衍生的 miRNA。总的来说,这项研究描述了 Drosha 在病毒感染背景下加工高度结构化的细胞质 RNA 的独特功能。

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