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The somatic piRNA pathway controls germline transposition over generations

机译:体细胞piRNA途径对世代进行树苗转子

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摘要

Transposable elements (TEs) are parasitic DNA sequences that threaten genome integrity by replicative transposition in host gonads. The Piwi-interacting RNAs (piRNAs) pathway is assumed to maintain Drosophila genome homeostasis by downregulating transcriptional and post-transcriptional TE expression in the ovary. However, the bursts of transposition that are expected to follow transposome derepression after piRNA pathway impairment have not yet been reported. Here, we show, at a genome-wide level, that piRNA loss in the ovarian somatic cells boosts several families of the endogenous retroviral subclass of TEs, at various steps of their replication cycle, from somatic transcription to germinal genome invasion. For some of these TEs, the derepression caused by the loss of piRNAs is backed up by another small RNA pathway (siRNAs) operating in somatic tissues at the post transcriptional level. Derepressed transposition during 70 successive generations of piRNA loss exponentially increases the genomic copy number by up to 10-fold.
机译:转座元素(TES)是寄生DNA序列,其通过宿主性腺转置威胁到基因组完整性。假设PIWI相互作用的RNA(PIRNA)途径通过下调卵巢中的转录和转录后转录TE表达来维持果蝇基因组稳态。然而,尚未报告尚未报告PiRNA途径损伤后预期追踪转座体DEREPLACES的转子突发。在这里,我们以基因组 - 宽的水平显示,卵巢体细胞中的piRNA损失促使TES的内源性逆转录病毒亚类的几个家族,以其复制循环的各种步骤,从体细胞转录到发芽基因组侵袭。对于这些TES中的一些,由PIRNA丧失引起的DEREPLACESS由在后转录水平的体细胞组织中操作的另一个小RNA途径(siRNA)来备份。在70种连续几代PiRNA损失期间的大规模转子将基因组拷贝数增加到10倍。

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