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人疱疹病毒6型编码的小非编码RNA定义了病毒再激活的一个中期和早期阶段。

HHV-6 encoded small non-coding RNAs define an intermediate and early stage in viral reactivation.

作者信息

Prusty Bhupesh K, Gulve Nitish, Chowdhury Suvagata Roy, Schuster Michael, Strempel Sebastian, Descamps Vincent, Rudel Thomas

机构信息

1Biocenter, Chair of Microbiology, University of Würzburg, Würzburg, Germany.

Present Address: Institute for Virology and Immunobiology, Versbacher Str. 7, 97078 Würzburg, Germany.

出版信息

NPJ Genom Med. 2018 Sep 5;3:25. doi: 10.1038/s41525-018-0064-5. eCollection 2018.

Abstract

Human herpesvirus 6A and 6B frequently acquires latency. HHV-6 activation has been associated with various human diseases. Germ line inheritance of chromosomally integrated HHV-6 makes viral DNA-based analysis difficult for determination of early stages of viral activation. We characterized early stages of HHV-6 activation using high throughput transcriptomics studies and applied the results to understand virus activation under clinical conditions. Using a latent HHV-6A cell culture model in U2OS cells, we identified an early stage of viral reactivation, which we define as transactivation that is marked by transcription of several viral small non-coding RNAs (sncRNAs) in the absence of detectable increase in viral replication and proteome. Using deep sequencing approaches, we detected previously known as well as a new viral sncRNAs that characterized viral transactivation and differentiated it from latency. Here we show changes in human transcriptome upon viral transactivation that reflect multiple alterations in mitochondria-associated pathways, which was supported by observation of increased mitochondrial fragmentation in virus reactivated cells. Furthermore, we present here a unique clinical case of DIHS/DRESS associated death where HHV-6 sncRNA-U14 was abundantly detected throughout the body of the patient in the presence of low viral DNA. In this study, we have identified a unique and early stage of viral activation that is characterized by abundant transcription of viral sncRNAs, which can serve as an ideal biomarker under clinical conditions.

摘要

人类疱疹病毒6A和6B经常进入潜伏状态。HHV-6激活与多种人类疾病有关。染色体整合的HHV-6的种系遗传使得基于病毒DNA的分析难以确定病毒激活的早期阶段。我们使用高通量转录组学研究对HHV-6激活的早期阶段进行了表征,并将结果应用于了解临床条件下的病毒激活情况。利用U2OS细胞中的潜伏性HHV-6A细胞培养模型,我们确定了病毒重新激活的早期阶段,我们将其定义为反式激活,其特征是在病毒复制和蛋白质组未检测到增加的情况下,几种病毒小非编码RNA(sncRNA)转录。使用深度测序方法,我们检测到了先前已知的以及一种新的病毒sncRNA,它们表征了病毒反式激活并将其与潜伏状态区分开来。在这里,我们展示了病毒反式激活后人转录组的变化,这些变化反映了线粒体相关途径的多种改变,病毒重新激活的细胞中线粒体碎片化增加的观察结果支持了这一点。此外,我们在此展示了一例与DIHS/DRESS相关死亡的独特临床病例,在病毒DNA含量较低的情况下,患者全身大量检测到HHV-6 sncRNA-U14。在这项研究中,我们确定了一个独特的病毒激活早期阶段,其特征是病毒sncRNA大量转录,这在临床条件下可作为理想的生物标志物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/46da/6125432/529335c91266/41525_2018_64_Fig1_HTML.jpg

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