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Hijacking Oogenesis Enables Massive Propagation of LINE and Retroviral Transposons

机译:劫持ofogyesis使线和逆转录病毒转座的大规模传播

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摘要

Although animals have evolved multiple mechanisms to suppress transposons, "leaky'' mobilizations that cause mutations and diseases still occur. This suggests that transposons employ specific tactics to accomplish robust propagation. By directly tracking mobilization, we show that, during a short and specific time window of oogenesis, retrotransposons achieve massive amplification via a cell-type-specific targeting strategy. Retrotransposons rarely mobilize in undifferentiated germline stem cells. However, as oogenesis proceeds, they utilize supporting nurse cells-which are highly polyploid and eventually undergo apoptosis-as factories to massively manufacture invading products. Moreover, retrotransposons rarely integrate into nurse cells themselves but, instead, via microtubule-mediated transport, they preferentially target the DNA of the interconnected oocytes. Blocking microtubule-dependent intercellular transport from nurse cells significantly alleviates damage to the oocyte genome. Our data reveal that parasitic genomic elements can efficiently hijack a host developmental process to propagate robustly, thereby driving evolutionary change and causing disease.
机译:虽然动物已经进化了多种机制来抑制转座子,但仍然发生突变和疾病的“泄漏”的动员。这表明转座子采用了特定的策略来实现稳健的传播。通过直接跟踪动员,我们展示,在短期和特定的时间窗口窗口,回收朗斯经源通过细胞类型特异性靶向策略实现大规模扩增。Retrotransposons很少在未分化的种系干细胞中动员。然而,随着Oferoisesis进行的,它们利用支持护士细胞 - 这是高度多倍体,最终接受凋亡 - 作为工厂为了大量制造入侵产品。此外,回析骨很少集成到护士细胞中,而是通过微管介导的传输,它们优先靶向相互联系的卵母细胞的DNA。阻断来自护士细胞的微管依赖性细胞间转运显着减轻了对卵母细胞的损伤基因组。我们的数据揭示了寄生基因组元素可以有效地劫持宿主的发育过程以稳健地传播,从而推动进化变化和引起疾病。

著录项

  • 来源
    《Cell》 |2018年第5期|共25页
  • 作者单位

    Carnegie Inst Sci Dept Embryol Baltimore MD 21218 USA;

    Carnegie Inst Sci Dept Embryol Baltimore MD 21218 USA;

    Carnegie Inst Sci Dept Embryol Baltimore MD 21218 USA;

    Carnegie Inst Sci Dept Embryol Baltimore MD 21218 USA;

    Carnegie Inst Sci Dept Embryol Baltimore MD 21218 USA;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 细胞生物学;
  • 关键词

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