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人类内源性逆转录病毒K型的基因组灵活性

Genomic flexibility of human endogenous retrovirus type K.

作者信息

Dube Derek, Contreras-Galindo Rafael, He Shirley, King Steven R, Gonzalez-Hernandez Marta J, Gitlin Scott D, Kaplan Mark H, Markovitz David M

机构信息

Department of Internal Medicine, University of Michigan, Ann Arbor, Michigan, USA.

Department of Internal Medicine, University of Michigan, Ann Arbor, Michigan, USA Department of Microbiology and Immunology, University of Michigan, Ann Arbor, Michigan, USA.

出版信息

J Virol. 2014 Sep 1;88(17):9673-82. doi: 10.1128/JVI.01147-14. Epub 2014 Jun 11.

Abstract

UNLABELLED

Human endogenous retrovirus type K (HERV-K) proviruses are scattered throughout the human genome, but as no infectious HERV-K virus has been detected to date, the mechanism by which these viruses replicated and populated the genome remains unresolved. Here, we provide evidence that, in addition to the RNA genomes that canonical retroviruses package, modern HERV-K viruses can contain reverse-transcribed DNA (RT-DNA) genomes. Indeed, reverse transcription of genomic HERV-K RNA into the DNA form is able to occur in three distinct times and locations: (i) in the virus-producing cell prior to viral release, yielding a DNA-containing extracellular virus particle similar to the spumaviruses; (ii) within the extracellular virus particle itself, transitioning from an RNA-containing particle to a DNA-containing particle; and (iii) after entry of the RNA-containing virus into the target cell, similar to canonical retroviruses, such as murine leukemia virus and HIV. Moreover, using a resuscitated HERV-K virus construct, we show that both viruses with RNA genomes and viruses with DNA genomes are capable of infecting target cells. This high level of genomic flexibility historically could have permitted these viruses to replicate in various host cell environments, potentially assisting in their many integration events and resulting in their high prevalence in the human genome. Moreover, the ability of modern HERV-K viruses to proceed through reverse transcription and package RT-DNA genomes suggests a higher level of replication competency than was previously understood, and it may be relevant in HERV-K-associated human diseases.

IMPORTANCE

Retroviral elements comprise at least 8% of the human genome. Of all the endogenous retroviruses, HERV-K viruses are the most intact and biologically active. While a modern infectious HERV-K has yet to be found, HERV-K activation has been associated with cancers, autoimmune diseases, and HIV-1 infection. Thus, determining how this virus family became such a prevalent member of our genome and what it is capable of in its current form are of the utmost importance. Here, we provide evidence that HERV-K viruses currently found in the human genome are able to proceed through reverse transcription and historically utilized a life cycle with a surprising degree of genomic flexibility in which both RNA- and DNA-containing viruses were capable of mediating infection.

摘要

未标注

人类内源性K型逆转录病毒(HERV-K)前病毒散布于整个人类基因组中,但迄今为止尚未检测到具有感染性的HERV-K病毒,这些病毒在基因组中复制和传播的机制仍未明确。在此,我们提供证据表明,除了典型逆转录病毒所包装的RNA基因组外,现代HERV-K病毒还可包含逆转录的DNA(RT-DNA)基因组。实际上,基因组HERV-K RNA逆转录为DNA形式能够在三个不同的时间和位置发生:(i)在病毒释放前的病毒产生细胞中,产生类似于泡沫病毒的含DNA细胞外病毒颗粒;(ii)在细胞外病毒颗粒本身内部,从含RNA颗粒转变为含DNA颗粒;(iii)在含RNA病毒进入靶细胞后,类似于典型逆转录病毒,如鼠白血病病毒和HIV。此外,使用复活的HERV-K病毒构建体,我们表明具有RNA基因组的病毒和具有DNA基因组的病毒均能够感染靶细胞。从历史上看,这种高度的基因组灵活性可能使这些病毒能够在各种宿主细胞环境中复制,潜在地有助于它们发生多次整合事件并导致它们在人类基因组中高度流行。此外,现代HERV-K病毒进行逆转录和包装RT-DNA基因组的能力表明其复制能力比之前所认为的更高,这可能与HERV-K相关的人类疾病有关。

重要性

逆转录病毒元件至少占人类基因组的8%。在所有内源性逆转录病毒中,HERV-K病毒是最完整且具有生物活性的。虽然尚未发现现代具有感染性的HERV-K,但HERV-K的激活与癌症、自身免疫性疾病和HIV-1感染有关。因此,确定这个病毒家族如何成为我们基因组中如此普遍的成员以及它目前的形式能够做什么至关重要。在此,我们提供证据表明,目前在人类基因组中发现的HERV-K病毒能够进行逆转录,并且在历史上利用了一种具有惊人程度基因组灵活性的生命周期,其中含RNA和含DNA的病毒都能够介导感染。

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