A viral factor, CpBV15 alpha , interacts with a translation initiation factor, eIF2, to suppress host gene expression at a post-transcriptional level.

摘要

An endoparasitoid wasp, Cotesia plutellae, possesses its specific symbiotic virus called C. plutellae bracovirus (CpBV) and parasitizes young larvae of Plutella xylostella. CpBV encodes CpBV15 alpha , which was previously shown to interfere with host protein translation. In vivo transient expression of CpBV15 alpha induced a significant decrease in a storage protein level without its transcriptional level change. In vitro translation assay using rabbit reticulocyte lysate showed that CpBV15 alpha suppressed translation efficiency of mRNAs extracted from fat body of P. xylostella. Transient expression of CpBV15 alpha in nonparasitized P. xylostella suppressed humoral immunity and development to pupal and adult stages. Immunoprecipitation (IP) of CpBV15 alpha co-precipitated eIF2 and eIF2B (a guanine nucleotide exchange factor of eIF2) in parasitized P. xylostella. Additionally, IP of eIF2 co-precipitated CpBV15 alpha as well as eIF2B and eIF5 in parasitized larvae. IP with eIF5 antibody showed that relative amount of eIF2 bound to eIF5 was much decreased in parasitized larvae, while significant amount of eIF2 was bound to CpBV15 alpha . These results suggest that CpBV15 alpha inhibits some host mRNA translation by sequestering eIF2.