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Fish novel TRIM protein FTR14 negatively regulates interferon response by targeting TBK1-IRF3.

Authors :
Zhi, Linyong
Yuan, Mengdi
Ma, Yiting
Liu, Shanxing
Qin, Qiwei
Huang, Xiaohong
Huang, Youhua
Source :
Aquaculture. Sep2024, Vol. 590, pN.PAG-N.PAG. 1p.
Publication Year :
2024

Abstract

Growing evidence highlights that tripartite motif (TRIM) family members exert crucial functions in host defense upon infection with microbial pathogens. Of note, the roles of a subfamily of fish-specific TRIM (FTR, also named as finTRIM) which have no true orthologues in mammals were largely unexplored. In this study, a novel FTR gene from grouper (EcFTR14) was identified, and its effects on fish virus infection and host interferon response were investigated. EcFTR14 contained RING, B-Box, and PRY-SPRY domains, and shared 54.81% identity to zebrafish FTR14. The transcription levels of EcFTR14 were markedly induced upon fish virus infection. EcFTR14 was mainly localized in the cytoplasm as small spots or bright aggregates. The overexpression of EcFTR14 could markedly enhance the replication of RGNNV or SGIV. Moreover, overexpression of EcFTR14 reduced the mRNA level of IFN-associated immune signaling molecules, suggesting that the antiviral action of EcFTR14 was due to the negative regulation on IFN response. EcFTR14 was found to interact with EcTBK1, EcIRF3 and EcIRF7, but not with EcSTING. Overexpression of EcFTR14 markedly suppressed the transcription levels of IFN-signaling related molecules evoked by EcSTING and EcTBK1. In addition, overexpression of EcFTR14 could degrade EcTBK1, EcIRF3 and EcIRF7 in a dose-dependent manner, that resulted in the suppression of antiviral effects induced by EcIRF3 and EcTBK1. Collectively, our findings illuminated that EcFTR14, a novel member of FTR family, acted as a pro-viral factor through negatively regulating targeting TBK1-IRF3 activated antviral action. The present study will for the first time shed light on the regulatory roles of FTR14 in innate immune response upon fish virus infection. • EcFTR14 was a novel FTR protein which shared 54.81% identity to zebrafish FTR14. • EcFTR14 were significantly up-regulated upon SGIV and RGNNV infection. • EcFTR14 acted as a pro-viral factor during SGIV and RGNNV infection. • EcFTR14 interacted with EcTBK1, EcIRF3, EcIRF7, and negatively regulated IFN response. • EcFTR14 weakened the antiviral effects induced by EcIRF3 and EcTBK1. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
00448486
Volume :
590
Database :
Academic Search Index
Journal :
Aquaculture
Publication Type :
Academic Journal
Accession number :
177864019
Full Text :
https://doi.org/10.1016/j.aquaculture.2024.741066