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绵羊疱疹病毒 2 编码的 microRNAs 靶向参与病毒潜伏的病毒基因。

Ovine herpesvirus-2-encoded microRNAs target virus genes involved in virus latency.

机构信息

The Roslin Institute & Royal (Dick) School of Veterinary Studies, University of Edinburgh, Easter Bush Veterinary Campus, Roslin, Midlothian EH25 9RG, UK.

出版信息

J Gen Virol. 2014 Feb;95(Pt 2):472-480. doi: 10.1099/vir.0.059303-0. Epub 2013 Oct 30.

Abstract

Herpesviruses encode microRNAs (miRNAs) that target both virus and host genes; however, their role in herpesvirus biology is understood poorly. We identified previously eight miRNAs encoded by ovine herpesvirus-2 (OvHV-2), the causative agent of malignant catarrhal fever (MCF), and have now investigated the role of these miRNAs in regulating expression of OvHV-2 genes that play important roles in virus biology. ORF20 (cell cycle inhibition), ORF50 (reactivation) and ORF73 (latency maintenance) each contain predicted targets for several OvHV-2 miRNAs. Co-transfection of miRNA mimics with luciferase reporter constructs containing the predicted targets showed the 5' UTRs of ORF20 and ORF73 contain functional targets for ovhv-miR-2 and ovhv2-miR-8, respectively, and the 3' UTR of ORF50 contains a functional target for ovhv2-miR-5. Transfection of BJ1035 cells (an OvHV-2-infected bovine T-cell line) with the relevant miRNA mimic resulted in a significant decrease in ORF50 and a smaller but non-significant decrease in ORF20. However, we were unable to demonstrate a decrease in ORF73. MCF is a disease of dysregulated lymphocyte proliferation; miRNA inhibition of ORF20 expression may play a role in this aberrant lymphocyte proliferation. The proteins encoded by ORF50 and ORF73 play opposing roles in latency. It has been hypothesized that miRNA-induced inhibition of virus genes acts to ensure that fluctuations in virus mRNA levels do not result in reactivation under conditions that are unfavourable for viral replication and our data supported this hypothesis.

摘要

疱疹病毒编码靶向病毒和宿主基因的 microRNAs(miRNAs);然而,它们在疱疹病毒生物学中的作用知之甚少。我们之前已经鉴定出绵羊疱疹病毒 2(OvHV-2)编码的八种 miRNAs,OvHV-2 是恶性卡他热(MCF)的病原体,现在我们研究了这些 miRNAs 调节病毒生物学中重要基因表达的作用。ORF20(细胞周期抑制)、ORF50(再激活)和 ORF73(潜伏期维持)每个都包含几个 OvHV-2 miRNAs 的预测靶标。miRNA 模拟物与包含预测靶标的荧光素酶报告基因构建体的共转染表明,ORF20 和 ORF73 的 5'UTR 分别包含 OvHV-2-miR-2 和 OvHV2-miR-8 的功能靶标,而 ORF50 的 3'UTR 包含 OvHV2-miR-5 的功能靶标。用相关 miRNA 模拟物转染 BJ1035 细胞(感染 OvHV-2 的牛 T 细胞系)导致 ORF50 的显著减少,而 ORF20 的减少较小但无统计学意义。然而,我们无法证明 ORF73 的减少。MCF 是一种淋巴细胞增殖失调的疾病;ORF20 表达的 miRNA 抑制可能在这种异常淋巴细胞增殖中发挥作用。ORF50 和 ORF73 编码的蛋白质在潜伏期发挥相反的作用。据推测,miRNA 诱导的病毒基因抑制作用可确保病毒 mRNA 水平的波动不会在不利于病毒复制的条件下导致再激活,我们的数据支持这一假设。

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本文引用的文献

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