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Two distinct mechanisms generate endogenous siRNAs from bidirectional transcription in Drosophila melanogaster

机译:两个不同的机制从果蝇的双向转录中产生内源性siRNA。

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Cis-natural antisense transcripts (cis-NATs) have been speculated to be substrates for endogenous RNA interference (RNAi), but little experimental evidence for such a pathway in animals has been reported. Analysis of massive Drosophila melanogaster small RNA data sets now reveals two mechanisms that yield endogenous small interfering RNAs (siRNAs) via bidirectional transcription. First, > 100 cis-NATs with overlapping 3' exons generate 21-nt, Dicer-2 (Dcr-2)-dependent, 3'-end modified siRNAs. The processing of cis-NATs by RNA interference (RNAi) seems to be actively restricted, and the selected loci are enriched for nucleic acid-based functions and include Argonaute-2 (AGO2) itself. Second, we report that extended intervals of the thickveins and klarsicht genes generate exceptionally abundant siRNAs from both strands. These siRNA clusters derive from atypical cis-NAT arrangements involving introns and 5' or internal exons, but their biogenesis is similarly Dcr-2- and AGO2-dependent. These newly recognized siRNA pathways broaden the scope of regulatory networks mediated by small RNAs.
机译:顺式-天然反义转录物(cis-NATs)被认为是内源性RNA干扰(RNAi)的底物,但是在动物中这种途径的实验证据很少。分析大量的果蝇小RNA数据集,现在揭示了两种通过双向转录产生内源性小干扰RNA(siRNA)的机制。首先,> 100个具有重叠3'外显子的顺式NAT产生21-nt,Dicer-2(Dcr-2)依赖性3'末端修饰的siRNA。 RNA干扰(RNAi)对顺式NAT的加工似乎受到积极限制,并且选定的基因座富含基于核酸的功能,并且自身包括Argonaute-2(AGO2)。第二,我们报道了延长的间隔时间间隔的厚静脉和克拉希特基因从两条链产生异常丰富的siRNA。这些siRNA簇源自涉及内含子和5'或内部外显子的非典型顺式NAT排列,但它们的生物发生类似地依赖于Dcr-2-和AGO2。这些新发现的siRNA途径拓宽了由小RNA介导的调控网络的范围。

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