Litcius/Paper detail

A conformational selection mechanism of flavivirus NS5 for species-specific STAT2 inhibition

Mahamaya Biswal, Wangyuan Yao, Jiuwei Lu, Jianbin Chen, Juliet Morrison, Rong Hai, Jikui Song

2024Communications Biology20 citationsDOIOpen Access PDF

Abstract

Flaviviruses, including Zika virus (ZIKV) and Dengue virus (DENV), rely on their non-structural protein 5 (NS5) for both replication of viral genome and suppression of host IFN signaling. DENV and ZIKV NS5s were shown to facilitate proteosome-mediated protein degradation of human STAT2 (hSTAT2). However, how flavivirus NS5s have evolved for species-specific IFN-suppression remains unclear. Here we report structure-function characterization of the DENV serotype 2 (DENV2) NS5-hSTAT2 complex. The MTase and RdRP domains of DENV2 NS5 form an extended conformation to interact with the coiled-coil and N-terminal domains of hSTAT2, thereby promoting hSTAT2 degradation in cells. Disruption of the extended conformation of DENV2/ZIKV NS5, but not the alternative compact state, impaired their hSTAT2 binding. Our comparative structural analysis of flavivirus NS5s further reveals a conserved protein-interaction platform with subtle amino-acid variations likely underpinning diverse IFN-suppression mechanisms. Together, this study uncovers a conformational selection mechanism underlying species-specific hSTAT2 inhibition by flavivirus NS5.

Topics & Concepts

FlavivirusDengue virusBiologyDengue feverVirologyViral replicationProtein structureGeneticsVirusBiochemistryMosquito-borne diseases and controlHIV Research and TreatmentStudies on Chitinases and Chitosanases