Vaccinia virus induces cellular mRNA degradation.
AUTOR(ES)
Rice, A P
RESUMO
The infection of mouse L cells with vaccinia virus induced a rapid inhibition of cellular polypeptide synthesis and a diversion of protein synthesis to the exclusive production of viral polypeptides. This shutoff of cell-specific protein synthesis was achieved by a novel mechanism by which the virus induced the rapid degradation of cellular mRNAs. Concurrent with the degradation of cellular mRNA, the virus proceeds in the orderly temporal expression of its own genetic information. The effect of vaccinia virus infection upon two abundant L-cell mRNAs was assessed by using the highly conserved cDNA sequences that encode chicken beta-actin and rat alpha-tubulin. Hybridization analyses demonstrated that throughout infection there is a rapid and progressive degradation of both of these mRNAs. In fact, after 3 h of infection they are reduced to less than 50% of their concentration in uninfected L cells, and between 8 to 10 h they are almost entirely degraded. This observation explains in part the mechanism by which vaccinia virus inhibits host cell protein synthesis.
ACESSO AO ARTIGO
http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=255294Documentos Relacionados
- Premature translation termination mediates triosephosphate isomerase mRNA degradation.
- Histone mRNA concentrations are regulated at the level of transcription and mRNA degradation.
- Physical evidence for cotranslational regulation of beta-tubulin mRNA degradation.
- Degradation of cellular mRNA during infection by herpes simplex virus.
- Double-stranded RNA induces mRNA degradation in Trypanosoma brucei
