苜蓿银纹夜蛾核型多角体病毒编码的微小RNA(AcMNPV-miR-1)在杆状病毒复制中的功能调控
Functional Regulation of an Autographa californica Nucleopolyhedrovirus-Encoded MicroRNA, AcMNPV-miR-1, in Baculovirus Replication.
作者信息
Zhu Mengxiao, Wang Jinwen, Deng Riqiang, Wang Xunzhang
机构信息
School of Life Science, Sun Yat-Sen University, Guangzhou, China.
School of Life Science, Sun Yat-Sen University, Guangzhou, China
出版信息
J Virol. 2016 Jun 24;90(14):6526-6537. doi: 10.1128/JVI.00165-16. Print 2016 Jul 15.
UNLABELLED
An Autographa californica nucleopolyhedrovirus-encoded microRNA (miRNA), AcMNPV-miR-1, downregulates the ac94 gene, reducing the production of infectious budded virions and accelerating the formation of occlusion-derived virions. In the current study, four viruses that constitutively overexpress AcMNPV-miR-1 were constructed to further explore the function of the miRNA. In addition to the ac94 gene, two new viral gene targets (ac18 and ac95) of AcMNPV-miR-1 were identified, and the possible interacting proteins were verified and tested. In the context of AcMNPV-miR-1 overexpression, ac18 was slightly upregulated, and ac95 was downregulated. Several interacting proteins were identified, and a functional pathway for AcMNPV-miR-1 was deduced. AcMNPV-miR-1 overexpression decreased budded virus infectivity, reduced viral DNA replication, accelerated polyhedron formation, and promoted viral infection efficiency in Trichoplusia ni larvae, suggesting that AcMNPV-miR-1 restrains virus infection of cells but facilitates virus infection of larvae.
IMPORTANCE
Recently, microRNAs (miRNAs) have been widely reported as moderators or regulators of mammalian cellular processes, especially disease-related pathways in humans. However, the roles played by miRNAs encoded by baculoviruses, which infect numerous beneficial insects and agricultural pests, have rarely been described. To explore the actions of virus-encoded miRNAs, we investigated an miRNA encoded by Autographa californica nucleopolyhedrovirus (AcMNPV-miR-1). We previously identified this miRNA through the exogenous addition of AcMNPV-miR-1 mimics. In the current study, we constitutively overexpressed AcMNPV-miR-1 and analyzed the resultant effects to more comprehensively assess what is indeed the function of this miRNA during viral infection. In addition, we widely explored the target genes for the miRNA in the viral and host genomes and proposed a possible functional network for AcMNPV-miR-1, which provides a better general understanding of virus-encoded miRNAs. In brief, our study implied that AcMNPV-miR-1 constrains viral replication and cellular infection but enhances larval infection.
未标记
苜蓿银纹夜蛾核型多角体病毒(Autographa californica nucleopolyhedrovirus,AcMNPV)编码的一种微小RNA(miRNA),即AcMNPV-miR-1,可下调ac94基因,减少感染性出芽病毒粒子的产生,并加速多角体衍生病毒粒子的形成。在本研究中,构建了四种组成型过表达AcMNPV-miR-1的病毒,以进一步探索该miRNA的功能。除ac94基因外,还鉴定出AcMNPV-miR-1的两个新的病毒基因靶点(ac18和ac95),并对可能的相互作用蛋白进行了验证和测试。在AcMNPV-miR-1过表达的情况下,ac18略有上调,ac95下调。鉴定出了几种相互作用蛋白,并推导了AcMNPV-miR-1的功能途径。AcMNPV-miR-1过表达降低了出芽病毒的感染性,减少了病毒DNA复制,加速了多角体形成,并提高了在粉纹夜蛾(Trichoplusia ni)幼虫中的病毒感染效率,这表明AcMNPV-miR-1抑制病毒对细胞的感染,但促进病毒对幼虫的感染。
重要性
最近,微小RNA(miRNAs)作为哺乳动物细胞过程的调节因子或调控因子已被广泛报道,尤其是在人类与疾病相关的途径中。然而,感染众多有益昆虫和农业害虫的杆状病毒编码的miRNAs所起的作用却鲜有描述。为了探索病毒编码的miRNAs的作用,我们研究了苜蓿银纹夜蛾核型多角体病毒(AcMNPV)编码的一种miRNA(AcMNPV-miR-1)。我们之前通过外源添加AcMNPV-miR-1模拟物鉴定出了这种miRNA。在本研究中,我们组成型过表达AcMNPV-miR-1并分析其产生的影响,以更全面地评估该miRNA在病毒感染过程中的实际功能。此外,我们广泛探索了该miRNA在病毒和宿主基因组中的靶基因,并提出了AcMNPV-miR-1可能的功能网络,这为更好地全面理解病毒编码的miRNAs提供了帮助。简而言之,我们的研究表明AcMNPV-miR-1抑制病毒复制和细胞感染,但增强幼虫感染。
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