A potential mechanism for selective control of cap-independent translation by a viral RNA sequence in cis and in trans

dc.contributor.author Wang, Shanping
dc.contributor.author Guo, Liang
dc.contributor.author Allen, Edwards
dc.contributor.author Miller, W. Allen
dc.contributor.department Plant Pathology and Microbiology
dc.date 2018-02-17T04:29:27.000
dc.date.accessioned 2020-06-30T06:23:37Z
dc.date.available 2020-06-30T06:23:37Z
dc.date.copyright Fri Jan 01 00:00:00 UTC 1999
dc.date.issued 1999
dc.description.abstract <p>Highly efficient cap-independent translation initiation at the 5'- proximal AUG is facilitated by the 3' translation enhancer sequence (3'TE) located near the 3' end of barley yellow dwarf virus (BYDV) genomic RNA. The role of the 3'TE in regulating viral translation was examined. The 3'TE is required for translation and thus replication of the genomic RNA that lacks a 5' cap (Allen et al., 1999, Virology 253:139-144). Here we show that the 3'TE also mediates translation of uncapped viral subgenomic mRNAs (sgRNA1 and sgRNA2). A 109-nt viral sequence is sufficient for 3'TE activity in vitro, but additional viral sequence is necessary for cap-independent translation in vivo. The 5' extremity of the sequence required in the 3' untranslated region (UTR) for cap-independent translation in vivo coincides with the 5' end of sgRNA2. Thus, sgRNA2 has the 3'TE in its 5' UTR. Competition studies using physiological ratios of viral RNAs showed that, in trans, the 109-nt 3'TE alone, or in the context of 869-nt sgRNA2, inhibited translation of genomic RNA much more than it inhibited translation of sgRNA1. The divergent 5' UTRs of genomic RNA and sgRNA1 contribute to this differential susceptibility to inhibition. We propose that sgRNA2 serves as a novel regulatory RNA to carry out the switch from early to late gene expression. Thus, this new mechanism for temporal control of translation control involves a sequence that stimulates translation in cis and acts in trans to selectively inhibit translation of viral mRNA.</p>
dc.description.comments <p>This article is from <em>RNA</em> 5 (1999): 728, doi: <a href="http://dx.doi.org/10.1017/S1355838299981979" target="_blank">10.1017/S1355838299981979</a>. Posted with permission.</p>
dc.format.mimetype application/pdf
dc.identifier archive/lib.dr.iastate.edu/plantpath_pubs/39/
dc.identifier.articleid 1041
dc.identifier.contextkey 7774089
dc.identifier.s3bucket isulib-bepress-aws-west
dc.identifier.submissionpath plantpath_pubs/39
dc.identifier.uri https://dr.lib.iastate.edu/handle/20.500.12876/57756
dc.language.iso en
dc.source.bitstream archive/lib.dr.iastate.edu/plantpath_pubs/39/1999_MillerWA_PotentialMechanismSelective.pdf|||Fri Jan 14 23:54:48 UTC 2022
dc.source.uri 10.1017/S1355838299981979
dc.subject.disciplines Agricultural Science
dc.subject.disciplines Genetics
dc.subject.disciplines Plant Pathology
dc.subject.keywords 3' untranslated region
dc.subject.keywords barley yellow dwarf virus
dc.subject.keywords subgenomic RNA
dc.subject.keywords translational switch
dc.subject.keywords Genetics and MCDB Programs
dc.title A potential mechanism for selective control of cap-independent translation by a viral RNA sequence in cis and in trans
dc.type article
dc.type.genre article
dspace.entity.type Publication
relation.isAuthorOfPublication 4ad3ad12-430c-43b9-8f3c-3a920e00b28c
relation.isOrgUnitOfPublication a26b5928-54bb-4a0b-a973-95d649d1ad83
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