SREBP2-dependent lipid gene transcription enhances the infection of human dendritic cells by Zika virus.
Emilie BrancheYing-Ting WangKarla M ViramontesJoan M Valls CuevasJialei XieFernanda Ana-Sosa-BatizNorazizah ShafeeSascha H C DuttkeRachel E McMillanAlex E ClarkMichael N NguyenAaron F GarretsonJan J CramesNathan J SpannZhe ZhuJeremy N RichDeborah H SpectorChristopher BennerSujan ShrestaAaron F CarlinPublished in: Nature communications (2022)
The emergence of Zika virus (ZIKV) as a global health threat has highlighted the unmet need for ZIKV-specific vaccines and antiviral treatments. ZIKV infects dendritic cells (DC), which have pivotal functions in activating innate and adaptive antiviral responses; however, the mechanisms by which DC function is subverted to establish ZIKV infection are unclear. Here we develop a genomics profiling method that enables discrete analysis of ZIKV-infected versus neighboring, uninfected primary human DCs to increase the sensitivity and specificity with which ZIKV-modulated pathways can be identified. The results show that ZIKV infection specifically increases the expression of genes enriched for lipid metabolism-related functions. ZIKV infection also increases the recruitment of sterol regulatory element-binding protein (SREBP) transcription factors to lipid gene promoters, while pharmacologic inhibition or genetic silencing of SREBP2 suppresses ZIKV infection of DCs. Our data thus identify SREBP2-activated transcription as a mechanism for promoting ZIKV infection amenable to therapeutic targeting.