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The antisense strand of small interfering RNAs directs histone methylation and transcriptional gene silencing in human cells.

机译:小干扰RNA的反义链指导人细胞中的组蛋白甲基化和转录基因沉默。

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To determine mechanistically how siRNAs mediate transcriptional gene silencing (TGS) in human cells, we have measured histone methylation at targeted promoters, the dependency on active transcription, and whether or not both strands of the siRNA are required for siRNA-mediated TGS. We report here that siRNA treatment increases both H3K9 and H3K27 methylation of the targeted EF1A promoter and that this increase is dependent on nuclear specific delivery of the siRNA. We also find that TGS can be directed by the antisense strand alone, and requires active transcription by RNA polymerase II in human cells as evidenced by sensitivity to alpha-amanatin. The observation of antisense strand-specific siRNA-mediated TGS of EF1A was substantiated by targeting the U3 region of the HIV-1 LTR/promoter. Furthermore, we show that the antisense strand of siRNA EF52 associates with the transiently expressed Flag-tagged DNMT3A, the targeted EF1A promoter, and trimethylated H3K27. The observations reported here implicate a functional link between siRNA-mediated targeting of genomic regions (promoters), RNA Pol II function, histone methylation, and DNMT3A and support a paradigm in which the antisense strands of siRNAs alone can direct sequence-specific transcriptional gene silencing in human cells.
机译:为了从机械上确定siRNA如何介导人类细胞中的转录基因沉默(TGS),我们测量了靶向启动子处的组蛋白甲基化,对活性转录的依赖性以及siRNA介导的TGS是否需要siRNA的两条链。我们在这里报告,siRNA治疗增加了针对性的EF1A启动子的H3K9和H3K27甲基化,并且这种增加取决于siRNA的核特异性传递。我们还发现,TGS可以仅由反义链控制,并且需要对人类细胞中RNA聚合酶II敏感的RNA聚合酶II主动转录。通过靶向HIV-1 LTR /启动子的U3区,证实了反义链特异性siRNA介导的EF1A TGS的观察。此外,我们显示siRNA EF52的反义链与瞬时表达的带有Flag标签的DNMT3A,靶向的EF1A启动子和三甲基化的H3K27相关。此处报道的观察结果暗示了siRNA介导的基因组区域(启动子)靶向,RNA Pol II功能,组蛋白甲基化和DNMT3A之间的功能联系,并支持一种范式,其中仅siRNA的反义链可以指导序列特异性转录基因沉默在人类细胞中。

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