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Dicer-Independent Primal RNAs Trigger RNAi and Heterochromatin Formation

机译:不依赖切酶的原始RNA触发RNAi和异染色质形成

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摘要

Assembly of fission yeast pericentromeric heterochromatin and generation of small interfering RNAs (siRNAs) from noncoding centromeric transcripts are mutually dependent processes. How this interdependent positive feedback loop is first triggered is a fundamental unanswered question. Here, we show that two distinct Argonaute (Ago1)-dependent pathways mediate small RNA generation. RNAdependent RNA polymerase complex (RDRC) and Dicer act on specific noncoding RNAs to generate siRNAs by a mechanism that requires the slicer activity of Ago1 but is independent of pre-existing heterochromatin. In the absence of RDRC or Dicer, a distinct class of small RNAs, called primal small RNAs (priRNAs), associates with Ago1. priRNAs are degradation products of abundant transcripts, which bind to Ago1 and target antisense transcripts that result from bidirectional transcription of DNA repeats. Our results suggest that a transcriptome surveillance mechanism based on random association of RNA degradation products with Argonaute triggers siRNA amplification and heterochromatin assembly within DNA repeats.
机译:裂变酵母的着丝粒着丝粒异染色质的组装和从非编码着丝粒的转录本产生小干扰RNA(siRNA)是相互依赖的过程。首先如何触发这个相互依存的正反馈回路是一个根本未解决的问题。在这里,我们显示了两个不同的Argonaute(Ago1)依赖途径介导小RNA的产生。 RNA依赖性RNA聚合酶复合物(RDRC)和Dicer通过需要Ago1的切片机活性但不依赖于先前存在的异染色质的机制作用于特定的非编码RNA,以生成siRNA。在没有RDRC或Dicer的情况下,一类独特的小RNA被称为原始小RNA(priRNA)与Ago1结合。 priRNA是大量转录物的降解产物,可与Ago1结合并靶向由DNA重复序列的双向转录产生的反义转录物。我们的结果表明,基于RNA降解产物与Argonaute的随机关联的转录组监视机制可触发siRNA扩增和DNA重复序列中的异染色质组装。

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