Litcius/Paper detail

DDX3X Is Hijacked by Snakehead Vesiculovirus Phosphoprotein To Facilitate Virus Replication via Stabilization of the Phosphoprotein

Congran Bei, Chu Zhang, Hui Wu, Hao Feng, Yong‐An Zhang, Jiagang Tu

2023Journal of Virology15 citationsDOIOpen Access PDF

Abstract

Growing evidence has suggested that DDX3X plays important roles in virus replication. In one respect, DDX3X inhibits the replication of viruses, including hepatitis B virus, influenza A virus, Newcastle disease virus, duck Tembusu virus, and red-spotted grouper nervous necrosis virus. In another respect, DDX3X is required for the replication of viruses, including hepatitis C virus, Japanese encephalitis virus, West Nile virus, murine norovirus, herpes simplex virus, and severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). Because DDX3X has rarely been investigated in rhabdovirus replication, this study aimed at investigating the role of DDX3X in rhabdovirus replication by using the fish rhabdovirus SHVV as a model. We found that DDX3X was required for SHVV replication, with the mechanism that DDX3X interacts with and maintains the stability of SHVV phosphoprotein. Our data provide novel insights into the role of DDX3X in virus replication and will facilitate the design of antiviral drugs against rhabdovirus infection.

Topics & Concepts

BiologyPhosphoproteinViral replicationGene knockdownVirologyReplication factor CSmall interfering RNACell biologyMolecular biologyVirusGeneticsGeneDNA replicationControl of chromosome duplicationTransfectionMosquito-borne diseases and controlViral Infections and Vectorsinterferon and immune responses