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疱疹 B 病毒编码的小 RNA 的鉴定和表达分析。

Identification and expression analysis of herpes B virus-encoded small RNAs.

机构信息

Department of Virology and Immunology, Texas Biomedical Research Institute, P.O. Box 760549, San Antonio, TX 78227, USA.

出版信息

J Virol. 2011 Jul;85(14):7296-311. doi: 10.1128/JVI.00505-11. Epub 2011 May 4.

Abstract

Herpes B virus (BV) naturally infects macaque monkeys and is genetically similar to herpes simplex virus (HSV). Zoonotic infection of humans can cause encephalitis and if untreated has a fatality rate of ∼80%. The frequent use of macaques in biomedical research emphasizes the need to understand the molecular basis of BV pathogenesis with a view toward improving safety for those working with macaques. MicroRNAs (miRNAs) are small noncoding RNAs that regulate the expression of mRNAs bearing complementary target sequences and are employed by viruses to control viral and host gene expression. Using deep sequencing and validation by expression in transfected cells, we identified 12 novel BV-encoded miRNAs expressed in lytically infected cells and 4 in latently infected trigeminal ganglia (TG). Using quantitative reverse transcription-PCR (RT-qPCR), we found that most of the miRNAs exhibited a high level of abundance throughout infection. Further analyses showed that some miRNAs could be generated from multiple transcripts with different kinetic classes, possibly explaining detection throughout infection. Interestingly, miRNAs were detected at early times in the absence of viral gene expression and were present in purified virions. In TG, despite similar amounts of viral DNA per ganglion, it was notable that the relative amount of each miRNA varied between ganglia. The majority of the miRNAs are encoded by the regions that exhibit the most sequence differences between BV and HSV. Additionally, there is no sequence conservation between BV- and HSV-encoded miRNAs, which may be important for the differences in the human diseases caused by BV and HSV.

摘要

单纯疱疹病毒 B 型(BV)自然感染猕猴,与单纯疱疹病毒(HSV)在基因上相似。人类的人畜共患病感染可导致脑炎,如果不治疗,死亡率约为 80%。猕猴在生物医学研究中的频繁使用强调了需要了解 BV 发病机制的分子基础,以期提高与猕猴一起工作的人的安全性。微小 RNA(miRNA)是调节具有互补靶序列的 mRNAs 表达的小非编码 RNA,被病毒用来控制病毒和宿主基因表达。我们使用深度测序和转染细胞中的表达验证,鉴定出 12 种新型在裂解感染细胞中表达的 BV 编码 miRNA 和 4 种在潜伏感染三叉神经节(TG)中表达的 miRNA。使用定量逆转录-PCR(RT-qPCR),我们发现大多数 miRNA 在整个感染过程中表现出高水平的丰度。进一步的分析表明,一些 miRNA 可能来自具有不同动力学类别的多个转录本,这可能解释了在整个感染过程中的检测。有趣的是,miRNA 在没有病毒基因表达的情况下在早期被检测到,并且存在于纯化的病毒粒子中。在 TG 中,尽管每个神经节中的病毒 DNA 量相似,但值得注意的是,每个 miRNA 的相对量在神经节之间存在差异。大多数 miRNA 由 BV 和 HSV 之间序列差异最大的区域编码。此外,BV 和 HSV 编码的 miRNA 之间没有序列保守性,这对于由 BV 和 HSV 引起的人类疾病的差异可能很重要。

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