| Literature DB >> 26813975 |
Dan Li1, Wenping Yang1, Fan Yang1, Huanan Liu1, Zixiang Zhu1, Kaiqi Lian1, Caoqi Lei2, Shu Li2, Xiangtao Liu1, Haixue Zheng3, Hongbing Shu4.
Abstract
Foot-and-mouth disease is a frequently occurring disease of cloven-hoofed animals that is caused by infection with the foot-and-mouth virus (FMDV). FMDV circumvents the type-I IFN response by expressing proteins that antagonize cellular innate immunity, such as leader protease and 3C protease. We identified the FMDV structural protein VP3 as a negative regulator of the virus-triggered IFN-β signaling pathway. Expression of FMDV VP3 inhibited the Sendai virus-triggered activation of IFN regulatory factor-3 and the expression of retinoic acid-inducible gene-I/melanoma differentiation-associated protein-5. Transient transfection and coimmunoprecipitation confirmed that the structural protein VP3 interacts with virus-induced signaling adapter (VISA), which is dependent on the C-terminal aa 111-220 of VP3. In addition, we found that FMDV VP3 inhibits the expression of VISA by disrupting its mRNA. Taken together, our findings reveal a novel strategy used by the structural VP3 protein of FMDV to evade host innate immunity.-Li, D., Yang, W., Yang, F., Liu, H., Zhu, Z., Lian, K., Lei, C., Li, S., Liu, X., Zheng, H., Shu, H. The VP3 structural protein of foot-and-mouth disease virus inhibits the IFN-β signaling pathway. © FASEB.Entities:
Keywords: Aphthovirus; innate immunity; pathogen
Mesh:
Substances:
Year: 2016 PMID: 26813975 DOI: 10.1096/fj.15-281410
Source DB: PubMed Journal: FASEB J ISSN: 0892-6638 Impact factor: 5.191