| Literature DB >> 31812350 |
Yukang Yuan1, Ying Miao1, Liping Qian1, Yang Zhang2, Chao Liu3, Jin Liu1, Yibo Zuo1, Qian Feng1, Tingting Guo1, Liting Zhang1, Xiangjie Chen1, Lincong Jin1, Fan Huang1, Hongguang Zhang1, Wei Zhang4, Wei Li3, Guoqiang Xu2, Hui Zheng5.
Abstract
Mutation and prevalence of pathogenic viruses prompt the development of broad-spectrum antiviral strategies. Viperin is a potent antiviral protein that inhibits a broad range of viruses. Unexpectedly, we found that Viperin protein production in epithelium is defective in response to both viruses and interferons (IFNs). We further revealed that viruses and IFNs stimulate expression of the acetyltransferase HAT1, which induces Lys197-acetylation on Viperin. Viperin acetylation in turn recruits UBE4A that stimulates K6-linked polyubiquitination at Lys206 of Viperin, leading to Viperin protein degradation. Importantly, UBE4A deficiency restores Viperin protein production in epithelium. We then designed interfering peptides (IPs) to inhibit UBE4A binding with Viperin. We found that VIP-IP3 rescues Viperin protein production in epithelium and therefore enhances cellular antiviral activity. VIP-IP3 renders mice more resistant to viral infection. These findings could provide strategies for both enhancing host broad-spectrum antiviral response and improving the efficacy of IFN-based antiviral therapy.Entities:
Keywords: HAT1; UBE4A; Viperin; acetylation; antiviral response; epithelial cells; interferon; ubiquitination; viral infection
Year: 2019 PMID: 31812350 DOI: 10.1016/j.molcel.2019.11.003
Source DB: PubMed Journal: Mol Cell ISSN: 1097-2765 Impact factor: 17.970