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PML Body Component Sp100A Restricts Wild-Type Herpes Simplex Virus 1 Infection

Yilei Ma, Jingjing Li, Hongchang Dong, Zhaoxin Yang, Lingyue Zhou, Pei Xu

2022Journal of Virology19 citationsDOIOpen Access PDF

Abstract

Previous studies show that the PML body component Sp100 protein is immediately targeted by ICP0 of HSV-1 in the nucleus during productive infection. Therefore, extensive studies investigating the interplay of Sp100 isoforms with HSV-1 were conducted using a mutant virus lacking ICP0 or in the absence of infection. The role of Sp100 variants during natural HSV-1 infection remains blurry. Here, we report that Sp100A potently and independently inhibited wild-type HSV-1 and that during HSV-1 infection, cytosolic Sp100 remained stable and was increasingly secreted into the extracellular space, in association with EVs. Furthermore, the Sp100A level in secreting cells positively correlated with its level in EVs and the anti-HSV-1 potency of these EVs in recipient cells. In summary, this study implies an active antiviral role of Sp100A during wild-type HSV-1 infection and reveals a novel mechanism of Sp100A to restrict HSV-1 through extracellular communications.

Topics & Concepts

BiologyHerpes simplex virusVirologySimplexvirusComponent (thermodynamics)VirusHerpesviridaeViral diseaseThermodynamicsPhysicsHerpesvirus Infections and TreatmentsExtracellular vesicles in diseaseVirus-based gene therapy research
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