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Conserved Small Nucleotidic Elements at the Origin of Concerted piRNA Biogenesis from Genes and lncRNAs

机译:基因和lncRNA协同piRNA生物发生起源中的保守小核酸元素。

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摘要

PIWI-interacting RNAs (piRNAs) target transcripts by sequence complementarity serving as guides for RNA slicing in animal germ cells. The piRNA pathway is increasingly recognized as critical for essential cellular functions such as germline development and reproduction. In the ovary, as much as 11% of piRNAs map to protein-coding genes. Here, we show that ovarian mRNAs and long non-coding RNAs (lncRNAs) are processed into piRNAs that can direct other transcripts into the piRNA biogenesis pathway. Targeting piRNAs fuel transcripts either into the ping-pong cycle of piRNA amplification or into the machinery of phased piRNA biogenesis, thereby creating networks of inter-regulating transcripts. RNAs of the same network share related genomic repeats. These repeats give rise to piRNAs, which target other transcripts and lead to a cascade of concerted RNA slicing. While ping-pong networks are based on repeats of several hundred nucleotides, networks that rely on phased piRNA biogenesis operate through short ~40-nucleotides long repeats, which we named snetDNAs. Interestingly, snetDNAs are recurring in evolution from insects to mammals. Our study brings to light a new type of conserved regulatory pathway, the snetDNA-pathway, by which short sequences can include independent genes and lncRNAs in the same biological pathway.
机译:PIWI相互作用RNA(piRNA)通过序列互补性靶向转录物,可作为动物生殖细胞中RNA切片的指南。越来越多的人认为piRNA途径对于细胞的基本功能(如种系发育和繁殖)至关重要。在卵巢中,多达11%的piRNA定位于蛋白质编码基因。在这里,我们显示卵巢mRNA和长非编码RNA(lncRNA)被加工成piRNA,可以将其他转录本导入piRNA生物发生途径。靶向piRNA会将转录物加到piRNA扩增的乒乓循环中或阶段性piRNA生物发生的机制中,从而创建相互调控转录物的网络。同一网络的RNA共享相关的基因组重复序列。这些重复产生了piRNA,该piRNA靶向其他转录本,并导致级联一致的RNA切片。乒乓球网络是基于数百个核苷酸的重复序列,而依赖阶段piRNA生物发生的网络通过短的〜40个核苷酸的长重复序列(我们将其称为snetDNAs)进行操作。有趣的是,snetDNA从昆虫到哺乳动物的进化过程中都反复出现。我们的研究揭示了一种新型的保守调控途径,即snetDNA途径,通过该途径,短序列可以在同一生物学途径中包含独立的基因和lncRNA。

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