| Literature DB >> 30626683 |
Shinji Kusakabe1, Tatsuya Suzuki1, Yukari Sugiyama1, Saori Haga1, Kanako Horike1, Makoto Tokunaga1, Junki Hirano1, He Zhang1, David Virya Chen1, Hanako Ishiga1, Yasumasa Komoda1, Chikako Ono1, Takasuke Fukuhara1, Masahiro Yamamoto2, Masahito Ikawa3, Takashi Satoh4, Shizuo Akira4, Tomohisa Tanaka5, Kohji Moriishi5, Moto Fukai6, Akinobu Taketomi6, Sachiyo Yoshio7, Tatsuya Kanto7, Tetsuro Suzuki8, Toru Okamoto9, Yoshiharu Matsuura9.
Abstract
Hepatitis C virus (HCV) utilizes cellular factors for efficient propagation. Ubiquitin is covalently conjugated to the substrate to alter its stability or to modulate signal transduction. In this study, we examined the importance of ubiquitination for HCV propagation. We found that inhibition of deubiquitinating enzymes (DUBs) or overexpression of nonspecific DUBs impaired HCV replication, suggesting that ubiquitination regulates HCV replication. To identify specific DUBs involved in HCV propagation, we set up RNA interference (RNAi) screening against DUBs and successfully identified ubiquitin-specific protease 15 (USP15) as a novel host factor for HCV propagation. Our studies showed that USP15 is involved in translation of HCV RNA and production of infectious HCV particles. In addition, deficiency of USP15 in human hepatic cell lines (Huh7 and Hep3B/miR-122 cells) but not in a nonhepatic cell line (293T cells) impaired HCV propagation, suggesting that USP15 participates in HCV propagation through the regulation of hepatocyte-specific functions. Moreover, we showed that loss of USP15 had no effect on innate immune responses in vitro and in vivo We also found that USP15-deficient Huh7 cells showed reductions in the amounts of lipid droplets (LDs), and the addition of palmitic acids restored the production of infectious HCV particles. Taken together, these data suggest that USP15 participates in HCV propagation by regulating the translation of HCV RNA and the formation of LDs.IMPORTANCE Although ubiquitination has been shown to play important roles in the HCV life cycle, the roles of deubiquitinating enzymes (DUBs), which cleave ubiquitin chains from their substrates, in HCV propagation have not been investigated. Here, we identified USP15 as a DUB regulating HCV propagation. USP15 showed no interaction with viral proteins and no participation in innate immune responses. Deficiency of USP15 in Huh7 cells resulted in suppression of the translation of HCV RNA and reduction in the amounts of lipid droplets, and the addition of fatty acids partially restored the production of infectious HCV particles. These data suggest that USP15 participates in HCV propagation in hepatic cells through the regulation of viral RNA translation and lipid metabolism.Entities:
Keywords: HCV; deubiquitination; innate immunity; lipid; translation
Mesh:
Substances:
Year: 2019 PMID: 30626683 PMCID: PMC6401473 DOI: 10.1128/JVI.01708-18
Source DB: PubMed Journal: J Virol ISSN: 0022-538X Impact factor: 5.103