a co-opted dead-box rna helicase enhances tombusvirus plus-strand synthesis谁出局区rna解旋酶提高tombusvirus正链合成.pdfVIP
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a co-opted dead-box rna helicase enhances tombusvirus plus-strand synthesis谁出局区rna解旋酶提高tombusvirus正链合成
A Co-Opted DEAD-Box RNA Helicase Enhances
Tombusvirus Plus-Strand Synthesis
Nikolay Kovalev, Judit Pogany, Peter D. Nagy*
Department of Plant Pathology, University of Kentucky, Lexington, Kentucky, United States of America
Abstract
Replication of plus-strand RNA viruses depends on recruited host factors that aid several critical steps during replication. In
this paper, we show that an essential translation factor, Ded1p DEAD-box RNA helicase of yeast, directly affects replication
of Tomato bushy stunt virus (TBSV). To separate the role of Ded1p in viral protein translation from its putative replication
function, we utilized a cell-free TBSV replication assay and recombinant Ded1p. The in vitro data show that Ded1p plays a
role in enhancing plus-strand synthesis by the viral replicase. We also find that Ded1p is a component of the tombusvirus
replicase complex and Ded1p binds to the 39-end of the viral minus-stranded RNA. The data obtained with wt and ATPase
deficient Ded1p mutants support the model that Ded1p unwinds local structures at the 39-end of the TBSV ( 2)RNA,
rendering the RNA compatible for initiation of (+)-strand synthesis. Interestingly, we find that Ded1p and glyceraldehyde-3-
phosphate dehydrogenase (GAPDH), which is another host factor for TBSV, play non-overlapping functions to enhance (+)-
strand synthesis. Altogether, the two host factors enhance TBSV replication synergistically by interacting with the viral
(2)RNA and the replication proteins. In addition, we have developed an in vitro assay for Flock house virus (FHV), a small
RNA virus of insects, that also demonstrated positive effect on FHV replicase activity by the added Ded1p helicase. Thus,
two small RNA viruses, which do not code for their own helicases, seems to recruit a host RNA helicase to aid their
replication in infected cells.
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