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  2. Heat Shock Protein 90 Ensures the Integrity of Rubella Virus p150 Protein and Supports Viral Replication

Heat Shock Protein 90 Ensures the Integrity of Rubella Virus p150 Protein and Supports Viral Replication

  • J Virol. 2019 Oct 29;93(22):e01142-19. doi: 10.1128/JVI.01142-19.
Masafumi Sakata 1 Hiroshi Katoh 2 Noriyuki Otsuki 2 Kiyoko Okamoto 2 Yuichiro Nakatsu 2 Chang-Kweng Lim 3 Masayuki Saijo 3 Makoto Takeda 2 Yoshio Mori 2
Affiliations

Affiliations

  • 1 Department of Virology 3, National Institute of Infectious Diseases, Tokyo, Japan [email protected].
  • 2 Department of Virology 3, National Institute of Infectious Diseases, Tokyo, Japan.
  • 3 Department of Virology 1, National Institute of Infectious Diseases, Tokyo, Japan.
Abstract

Two viral nonstructural proteins, p150 and p90, are expressed in rubella virus (RUBV)-infected cells and mediate viral genome replication, presumably using various host machineries. Molecular chaperones are critical host factors for the maintenance of cellular proteostasis, and certain Viral Proteins use this chaperone system. The RUBV p150 and p90 proteins are generated from a precursor polyprotein, p200, via processing by the protease activity of its p150 region. This processing is essential for RUBV genome replication. Here we show that heat shock protein 90 (HSP90), a molecular chaperone, is an important host factor for RUBV genome replication. The treatment of RUBV-infected cells with the HSP90 inhibitors 17-allylamino-17-desmethoxygeldanamycin (17-AAG) and ganetespib suppressed RUBV genome replication. HSP90α physically interacted with p150, but not p90. Further analyses into the mechanism of action of the HSP90 inhibitors revealed that HSP90 activity contributes to p150 functional integrity and promotes p200 processing. Collectively, our data demonstrate that RUBV p150 is a client of the HSP90 molecular chaperone and that HSP90 functions as a key host factor for RUBV replication.IMPORTANCE Accumulating evidence indicates that RNA viruses use numerous host factors during replication of their genomes. However, the host factors involved in rubella virus (RUBV) genome replication are largely unknown. In this study, we demonstrate that the HSP90 molecular chaperone is needed for the efficient replication of the RUBV genome. Further, we reveal that HSP90 interacts with RUBV nonstructural protein p150 and its precursor polyprotein, p200. HSP90 contributes to the stability of p150 and the processing of p200 via its protease domain in the p150 region. We conclude that the cellular molecular chaperone HSP90 is a key host factor for functional maturation of nonstructural proteins for RUBV genome replication. These findings provide novel insight into this host-virus interaction.

Keywords

HSP90; Matonaviridae; Togaviridae; alphavirus; genome replication; host factor; rubella virus.

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