LINE-1 反转录转座子 DNA 在 HIV-1 感染的细胞中积累。
LINE-1 retrotransposable element DNA accumulates in HIV-1-infected cells.
机构信息
Department of Immunology, University of Toronto, Toronto, Ontario, Canada.
出版信息
J Virol. 2013 Dec;87(24):13307-20. doi: 10.1128/JVI.02257-13. Epub 2013 Oct 2.
Abstract
Type 1 long-interspersed nuclear elements (L1s) are autonomous retrotransposable elements that retain the potential for activity in the human genome but are suppressed by host factors. Retrotransposition of L1s into chromosomal DNA can lead to genomic instability, whereas reverse transcription of L1 in the cytosol has the potential to activate innate immune sensors. We hypothesized that HIV-1 infection would compromise cellular control of L1 elements, resulting in the induction of retrotransposition events. Here, we show that HIV-1 infection enhances L1 retrotransposition in Jurkat cells in a Vif- and Vpr-dependent manner. In primary CD4(+) cells, HIV-1 infection results in the accumulation of L1 DNA, at least the majority of which is extrachromosomal. These data expose an unrecognized interaction between HIV-1 and endogenous retrotransposable elements, which may have implications for the innate immune response to HIV-1 infection, as well as for HIV-1-induced genomic instability and cytopathicity.
摘要
1 型长散布核元件(L1s)是自主逆转录转座元件,它们保留了在人类基因组中活跃的潜力,但被宿主因素所抑制。L1 逆转录到染色体 DNA 可导致基因组不稳定,而 L1 在细胞质中的逆转录则有可能激活先天免疫传感器。我们假设 HIV-1 感染会破坏细胞对 L1 元件的控制,导致逆转座事件的诱导。在这里,我们表明 HIV-1 感染以 Vif 和 Vpr 依赖的方式增强 Jurkat 细胞中的 L1 逆转座。在原代 CD4(+)细胞中,HIV-1 感染导致 L1 DNA 的积累,至少其中大部分是染色体外的。这些数据揭示了 HIV-1 与内源性逆转录转座元件之间的一种未被识别的相互作用,这可能对 HIV-1 感染的先天免疫反应以及 HIV-1 诱导的基因组不稳定性和细胞病变性产生影响。
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