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首页> 外文期刊>Molecular cell >A primate herpesvirus uses the integrator complex to generate viral microRNAs.
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A primate herpesvirus uses the integrator complex to generate viral microRNAs.

机译:灵长类疱疹病毒使用整合子复合体产生病毒microRNA。

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摘要

Herpesvirus saimiri (HVS) is a gamma-herpesvirus that expresses Sm class U RNAs (HSURs) in latently infected marmoset T cells. By deep sequencing, we identified six HVS microRNAs (miRNAs) that are derived from three hairpin structures located immediately downstream of the 3' end processing signals of three of the HSURs. The viral miRNAs associate with Ago proteins and are biologically active. We confirmed that the expression of the two classes of viral noncoding RNAs is linked by identifying chimeric HSUR-pre-miRNA transcripts. We show that HVS miRNA biogenesis relies on cis-acting elements specifically required for synthesis and processing of Sm class RNAs. Knockdown of protein components in vivo and processing assays in vitro demonstrated that HVS does not utilize the Microprocessor complex that generates most host miRNAs. Instead, the Integrator complex cleaves to generate the 3' end of the HSUR and the pre-miRNA hairpin. Exportin-5 and Dicer are then required to generate mature viral miRNAs.
机译:saimiri疱疹病毒(HVS)是一种伽马疱疹病毒,在潜伏感染的mar猴T细胞中表达Sm类U RNA(HSUR)。通过深度测序,我们鉴定了六个HVS microRNA(miRNA),它们是从三个HSUR的3'末端加工信号紧接下游的三个发夹结构衍生而来的。病毒miRNA与Ago蛋白结合并具有生物学活性。我们证实,通过识别嵌合HSUR-pre-miRNA转录本,可将两类病毒非编码RNA的表达联系起来。我们表明,HVS miRNA生物发生依赖于Sm类RNA的合成和加工特别需要的顺式作用元件。体内蛋白质组分的敲除和体外加工分析的结果表明,HVS没有利用产生多数宿主miRNA的微处理器复合体。取而代之的是,Integrator复合物裂解产生HSUR的3'末端和pre-miRNA发夹。然后需要Exportin-5和Dicer来生成成熟的病毒miRNA。

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