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在病毒传播之前,受感染细胞发出信号,远程激活未感染细胞中的宿主细胞DNA合成。

Remote Activation of Host Cell DNA Synthesis in Uninfected Cells Signaled by Infected Cells in Advance of Virus Transmission.

作者信息

Schmidt Nora, Hennig Thomas, Serwa Remigiusz A, Marchetti Magda, O'Hare Peter

机构信息

Section of Virology, St. Mary's Medical School, Imperial College, London, United Kingdom.

Section of Virology, St. Mary's Medical School, Imperial College, London, United Kingdom Department of Chemistry, Imperial College London, London, United Kingdom.

出版信息

J Virol. 2015 Nov;89(21):11107-15. doi: 10.1128/JVI.01950-15. Epub 2015 Aug 26.

Abstract

UNLABELLED

Viruses modulate cellular processes and metabolism in diverse ways, but these are almost universally studied in the infected cell itself. Here, we study spatial organization of DNA synthesis during multiround transmission of herpes simplex virus (HSV) using pulse-labeling with ethynyl nucleotides and cycloaddition of azide fluorophores. We report a hitherto unknown and unexpected outcome of virus-host interaction. Consistent with the current understanding of the single-step growth cycle, HSV suppresses host DNA synthesis and promotes viral DNA synthesis in spatially segregated compartments within the cell. In striking contrast, during progressive rounds of infection initiated at a single cell, we observe that infection induces a clear and pronounced stimulation of cellular DNA replication in remote uninfected cells. This induced DNA synthesis was observed in hundreds of uninfected cells at the extended border, outside the perimeter of the progressing infection. Moreover, using pulse-chase analysis, we show that this activation is maintained, resulting in a propagating wave of host DNA synthesis continually in advance of infection. As the virus reaches and infects these activated cells, host DNA synthesis is then shut off and replaced with virus DNA synthesis. Using nonpropagating viruses or conditioned medium, we demonstrate a paracrine effector of uninfected cell DNA synthesis in remote cells continually in advance of infection. These findings have significant implications, likely with broad applicability, for our understanding of the ways in which virus infection manipulates cell processes not only in the infected cell itself but also now in remote uninfected cells, as well as of mechanisms governing host DNA synthesis.

IMPORTANCE

We show that during infection initiated by a single particle with progressive cell-cell virus transmission (i.e., the normal situation), HSV induces host DNA synthesis in uninfected cells, mediated by a virus-induced paracrine effector. The field has had no conception that this process occurs, and the work changes our interpretation of virus-host interaction during advancing infection and has implications for understanding controls of host DNA synthesis. Our findings demonstrate the utility of chemical biology techniques in analysis of infection processes, reveal distinct processes when infection is examined in multiround transmission versus single-step growth curves, and reveal a hitherto-unknown process in virus infection, likely relevant for other viruses (and other infectious agents) and for remote signaling of other processes, including transcription and protein synthesis.

摘要

未标记

病毒以多种方式调节细胞过程和代谢,但这些几乎都是在受感染的细胞本身中进行研究的。在这里,我们使用乙炔基核苷酸脉冲标记和叠氮荧光团的环加成反应,研究单纯疱疹病毒(HSV)多轮传播过程中DNA合成的空间组织。我们报告了一个迄今为止未知且出乎意料的病毒-宿主相互作用结果。与目前对单步生长周期的理解一致,HSV在细胞内空间隔离的区室中抑制宿主DNA合成并促进病毒DNA合成。与之形成鲜明对比的是,在由单个细胞引发的渐进性感染轮次中,我们观察到感染会在远处未感染的细胞中诱导明显且显著的细胞DNA复制刺激。在进展性感染范围之外的扩展边界处,数百个未感染的细胞中观察到了这种诱导的DNA合成。此外,使用脉冲追踪分析,我们表明这种激活得以维持,导致宿主DNA合成的传播波持续在感染之前出现。当病毒到达并感染这些被激活的细胞时,宿主DNA合成随后被关闭并被病毒DNA合成所取代。使用非传播性病毒或条件培养基,我们证明了在感染之前,未感染细胞的DNA合成在远处细胞中存在旁分泌效应器。这些发现对于我们理解病毒感染不仅在受感染细胞本身而且在远处未感染细胞中操纵细胞过程的方式以及控制宿主DNA合成的机制具有重要意义,可能具有广泛的适用性。

重要性

我们表明,在由单个病毒颗粒引发并伴有渐进性细胞间病毒传播(即正常情况)的感染过程中,HSV通过病毒诱导的旁分泌效应器在未感染细胞中诱导宿主DNA合成。该领域此前并不知道这个过程的发生,这项工作改变了我们对进展性感染期间病毒-宿主相互作用的解释,并对理解宿主DNA合成的控制具有重要意义。我们的发现证明了化学生物学技术在分析感染过程中的实用性,揭示了在多轮传播与单步生长曲线中检查感染时的不同过程,并揭示了病毒感染中一个迄今为止未知的过程,这可能与其他病毒(以及其他传染因子)以及包括转录和蛋白质合成在内的其他过程的远程信号传导有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5e4b/4621119/35197b19a97e/zjv9990909350001.jpg

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