单纯疱疹病毒2型通过将DEAD盒解旋酶3蛋白包装进病毒粒子来消耗细胞中的该蛋白。
Herpes Simplex 2 Virus Depletes Cells of DEAD-Box Helicase 3 Protein by Packaging It into Virions.
作者信息
Piazza Carmen Rita, Lottini Giulia, Quaranta Paola, Perrera Paola, Filippini Fabio, Lai Michele, Di Primio Cristina, Freer Giulia, Pistello Mauro
机构信息
Retrovirus Center, Department of Translational Medicine and New Technologies in Medicine and Surgery, University of Pisa, 56127 Pisa, Italy.
Virology Unit, Pisa University Hospital, 56127 Pisa, Italy.
出版信息
Viruses. 2025 Aug 15;17(8):1124. doi: 10.3390/v17081124.
Human DEAD-box helicase 3 (DDX3) is a multifunctional RNA helicase implicated in mRNA unwinding and the regulation of gene expression. While DDX3 has been extensively studied in the context of RNA virus replication, its role in DNA virus replication remains less understood. In this study, we explore the involvement of DDX3 in the life cycle of Herpes Simplex Virus type 2 (HSV-2), a double-stranded DNA virus. Silencing of DDX3 expression with siRNA significantly impaired HSV-2 replication, indicating that DDX3 supports viral propagation. Unexpectedly, HSV-2 infection led to a marked reduction in cellular DDX3 protein levels during in vitro replication in human cells, particularly at 24 h post-infection, corresponding to the peak of viral production. Notably, this decrease was not accompanied by a reduction in DDX3 mRNA levels, nor was it prevented by proteasome inhibition, suggesting an alternative mechanism of DDX3 depletion. Further analysis revealed substantial amounts of DDX3 protein within HSV-2 virions, supporting the hypothesis that DDX3 is packaged into viral particles during replication. We propose that HSV-2 exploits host DDX3 by incorporating it into progeny virions to facilitate early stages of infection in newly infected cells. However, no evidence linking DDX3 to the assembly process of HSV-2 particles was found. These findings expand the known functional repertoire of DDX3 and highlight its potential as a host factor co-opted by DNA viruses, suggesting a broader relevance in antiviral strategies.
人类DEAD盒解旋酶3(DDX3)是一种多功能RNA解旋酶,参与mRNA解旋和基因表达调控。虽然DDX3在RNA病毒复制方面已得到广泛研究,但其在DNA病毒复制中的作用仍了解较少。在本研究中,我们探究了DDX3在双链DNA病毒单纯疱疹病毒2型(HSV - 2)生命周期中的作用。用小干扰RNA(siRNA)沉默DDX3表达显著损害了HSV - 2复制,表明DDX3支持病毒增殖。出乎意料的是,在人细胞体外复制过程中,HSV - 2感染导致细胞DDX3蛋白水平显著降低,尤其是在感染后24小时,这与病毒产生的峰值相对应。值得注意的是,这种降低并非伴随着DDX3 mRNA水平的下降,蛋白酶体抑制也不能阻止这种降低,这表明存在DDX3消耗的另一种机制。进一步分析发现HSV - 2病毒粒子内有大量DDX3蛋白,支持了DDX3在复制过程中被包装进病毒颗粒的假说。我们提出HSV - 2通过将宿主DDX3纳入子代病毒粒子来利用它,以促进新感染细胞中的早期感染阶段。然而,未发现将DDX3与HSV - 2病毒粒子组装过程联系起来的证据。这些发现扩展了已知的DDX3功能谱,并突出了其作为被DNA病毒利用的宿主因子的潜力,表明其在抗病毒策略中具有更广泛的相关性。
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