Abstract
Genes containing an interferon (IFN)-stimulated response element (ISRE) can be divided into two groups according to their inducibility by IFN and virus infection: one induced only by IFN and the other induced by both IFN and virus infection. Although it is now clear that IFN regulatory factor 7 (IRF7) is a multifunctional gene essential for induction of type I IFNs, regulation of the IRF7 promoter (IRF7p) is poorly understood. The IRF7 gene includes two IFN responsive elements, an IRF-binding element (IRFE) in the promoter region and an ISRE in the first intron, and is induced by the IFN-triggered Jak-STAT pathway by binding of the IFN-stimulated gene factor 3 (ISGF3) complex to the ISRE. In this study, we demonstrate that IRF3 and IRF7, which with the coactivators CREB-binding protein and P300 form the virus-activated factor (VAF) complex upon Sendai virus infection, bind to the IRF7 ISRE and IRFE and can directly activate IRF7 transcription. Promoter reporter assays show that both the ISRE and IRFE are responsive to activation by IRF7 and IRF3. In cells transiently expressing IRF7 or/and IRF3, the VAF level and binding of VAF are clearly increased after Sendai virus infection. Studies with Jak1 kinase inactive 293 cells that were stably transfected with a Jak1 kinase dead dominant negative construct, and the mutant cell lines SAN (IFNalpha-/beta-), U2A (IRF9-), U4A (Jak1-), and DKO (IRF1-/IRF2-) show that the IRF7 transcription activated directly by VAF is distinct from and independent of the IFN signaling pathway. Thus, IRF7 transcription is autoregulated by binding of the IRF7-containing VAF to its own ISRE and IRFE. The results show two distinct mechanisms for the activation of the IRF7 promoter, by IFN and by virus infection. A regulatory network between type I IFNs and IRF7 is proposed. The distinct pathways may reflect special roles for an efficient antiviral response at different stages of virus infection.
Highlights
In immune and inflammatory responses, virus infection results in activation or direct induction of a set of transcription factors, the interferon (IFN)1 regulatory factors (IRFs), which
We demonstrate that IRF3 and IFN regulatory factor 7 (IRF7), which with the coactivators CREB-binding protein and P300 form the virus-activated factor (VAF) complex upon Sendai virus infection, bind to the IRF7 IFN-stimulated response elements (ISREs) and IRF-binding element (IRFE) and can directly activate IRF7 transcription
In addition to induction by type I IFNs, we demonstrate that IRF7 transcription can be regulated by binding of both IRF7 and IRF3 proteins in the virus-activated factor (VAF) complex to the IRF7 promoter (IRF7p) ISRE and IRFE and that this regulation is independent of the IFN pathway
Summary
In immune and inflammatory responses, virus infection results in activation or direct induction of a set of transcription factors, the interferon (IFN)1 regulatory factors (IRFs), which. In addition to induction by type I IFNs, we demonstrate that IRF7 transcription can be regulated by binding of both IRF7 and IRF3 proteins in the virus-activated factor (VAF) complex to the IRF7p ISRE and IRFE and that this regulation is independent of the IFN pathway.
Sign-in/Register to view highlights & summary Sign-in/Register to access full text options 
Free) 
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a call
