DDX56 cooperates with FMDV 3A to enhance FMDV replication by inhibiting the phosphorylation of IRF3

The components of foot-and-mouth disease virus (FMDV) interact with host cellular proteins to promote self-replication and evade the host immune response. Previous studies have shown that FMDV 3A, 2C and 2B proteins interact with host cellular proteins involved in FMDV replication. However, whether...

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Bibliographic Details
Published in:Cellular signalling 2019-12, Vol.64, p.109393-109393, Article 109393
Main Authors: Fu, Shao-zu, Yang, Wen-ping, Ru, Yi, Zhang, Ke-shan, Wang, Yong, Liu, Xiang-tao, Li, Dan, Zheng, Hai-xue
Format: Article
Language:English
Subjects:
DDX56
FMDV 3A
IRF3
Phosphorylation
Replication
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Summary:The components of foot-and-mouth disease virus (FMDV) interact with host cellular proteins to promote self-replication and evade the host immune response. Previous studies have shown that FMDV 3A, 2C and 2B proteins interact with host cellular proteins involved in FMDV replication. However, whether the other host proteins have an impact on FMDV replication is less understood. In this study, we identified DDX56 as a positive regulator of FMDV replication. DDX56 overexpression increased FMDV replication, whereas DDX56 knockdown had the opposite effect. DDX56 interacted and cooperated with FMDV 3A to inhibit the type I interferon by reducing the phosphorylation of IRF3. Moreover, the D166 site of DDX56 played a role in increasing FMDV replication and cooperating with FMDV 3A to inhibit the phosphorylation of IRF3. Additionally, knockdown of DDX56 or FMDV 3A results also showed that DDX56 cooperated with FMDV 3A to inhibit the phosphorylation of IRF3. These results suggest that the interaction between FMDV 3A protein and the host protein DDX56 is critical for FMDV replication. •DDX56 interacts with FMDV 3A.•DDX56 cooperates with FMDV 3A to inhibit the type I interferon.•DDX56 potentiates FMDV replication.•DDX56 cooperates with FMDV 3A to inhibit the phosphorylation of IRF3.
ISSN:0898-6568
1873-3913
DOI:10.1016/j.cellsig.2019.109393