At early times in Mammalian Orthoreovirus (MRV) infection, cytoplasmic inclusions termed stress granules (SGs) are formed as a component of the innate immune response, however, at later times they are no longer present despite continued immune signaling. To investigate the roles of MRV proteins in SG modulation we examined non-structural protein mu NS localization relative to SGs in infected and transfected cells. Using a series of mutant plasmids, we mapped the necessary mu NS residues for SG localization to amino acids 78 and 79. We examined the capacity of a mu NS(78-79) mutant to associate with known viral protein binding partners of [INS and found that it loses association with viral core protein lambda 2. Finally, we show that while this mutant cannot support de novo viral replication, it is able to rescue replication following siRNA knockdown of [INS. These data suggest that mu NS association with SGs, lambda 2, or both play roles in MRV replication.

• 出版日期2014-1-5