The Protein Encoded by the UL3.5 Gene of the Duck Plague Virus Affects Viral Secondary Envelopment, Release, and Cell-to-Cell Spread
Huanhuan Cao, Bin Tian, Yanming Tian, Dongjie Cai, Mingshu Wang, Renyong Jia, Shun Chen, Anchun Cheng

TL;DR
This study identifies the UL3.5 gene of duck plague virus as essential for viral replication, specifically in secondary envelopment, release, and cell-to-cell spread.
Contribution
The study reveals the novel role of the DPV UL3.5 gene in viral replication and identifies it as a potential antiviral target.
Findings
UL3.5 encodes an early cytoplasmic protein essential for secondary envelopment and release of the virus.
Deletion of UL3.5 impairs cell-to-cell spread and viral replication.
The gene is classified as an early gene and is highly variable in size and sequence.
Abstract
Duck plague virus (DPV) severely threatens waterfowl, yet the role of its UL3.5 gene remains unknown. This study aimed to define UL3.5’s function by analyzing its protein localization, gene classification, and impact on viral replication. Results show that UL3.5 encodes an early cytoplasmic protein and is essential for viral secondary envelopment, release, and cell-to-cell spread, as its deletion cripples these processes. We conclude that UL3.5 is a key participant in the life cycle of the duck plague virus. These findings unveil a key viral replication mechanism and identify UL3.5 as a potential target for antiviral strategies, offering foundational information for further investigations into the functional characteristics of DPV UL3.5. Duck plague (DP), caused by duck plague virus (DPV), is a highly contagious and fatal disease among waterfowl. UL3.5, an unconserved gene belonging to…
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Taxonomy
TopicsHerpesvirus Infections and Treatments · Toxoplasma gondii Research Studies · interferon and immune responses
