DUSP4 modulates RIG-I- and STING-mediated IRF3-type I IFN response.
Huipeng JiaoSharmy J JamesChin Wen PngChaoyu CuiHeng LiLiang LiWan Ni ChiaNyo MinWeiyun LiCarla ClaserShanshan W HowlandHongyan WangMark I-Cheng ChenJustin Jang Hann ChuKevin Shyong-Wei TanYinyue DengYongliang ZhangPublished in: Cell death and differentiation (2024)
Detection of cytosolic nucleic acids by pattern recognition receptors, including STING and RIG-I, leads to the activation of multiple signalling pathways that culminate in the production of type I interferons (IFNs) which are vital for host survival during virus infection. In addition to protective immune modulatory functions, type I IFNs are also associated with autoimmune diseases. Hence, it is important to elucidate the mechanisms that govern their expression. In this study, we identified a critical regulatory function of the DUSP4 phosphatase in innate immune signalling. We found that DUSP4 regulates the activation of TBK1 and ERK1/2 in a signalling complex containing DUSP4, TBK1, ERK1/2 and IRF3 to regulate the production of type I IFNs. Mice deficient in DUSP4 were more resistant to infections by both RNA and DNA viruses but more susceptible to malaria parasites. Therefore, our study establishes DUSP4 as a regulator of nucleic acid sensor signalling and sheds light on an important facet of the type I IFN regulatory system.