The influence of viral coding sequences on pestivirus IRES activity reveals further parallels with translation initiation in prokaryotes

被引:47
作者
Fletcher, SP
Ali, IK
Kaminski, A
Digard, P
Jackson, RJ
机构
[1] Univ Cambridge, Dept Biochem, Cambridge CB2 1GA, England
[2] Univ Cambridge, Dept Pathol, Div Virol, Cambridge CB2 1QP, England
关键词
classical swine fever virus (CSFV); eIF4A; hepatitis C virus (HCV); internal initiation of translation; IRES; RNA helicases;
D O I
10.1017/S1355838202023038
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Classical swine fever virus (CSFV) is a member of the pestivirus family, which shares many features in common with hepatitis C virus (HCV). It is shown here that CSFV has an exceptionally efficient cis-acting internal ribosome entry segment (IRES), which, like that of HCV, is strongly influenced by the sequences immediately downstream of the initiation codon, and is optimal with viral coding sequences in this position. Constructs that retained 17 or more codons of viral coding sequence exhibited full IRES activity, but with only 12 codons, activity was similar to66% of maximum. in vitro (though close to maximum in transfected BHK cells), whereas with just 3 codons or fewer, the activity was only similar to15% of maximum. The minimal coding region elements required for high activity were exchanged between HCV and CSFV. Although maximum activity was observed in each case with the homologous combination of coding region and 51 UTR, the heterologous combinations were sufficiently active to rule out a highly specific functional interplay between the 51 UTR and coding sequences. On the other hand, inversion of the coding sequences resulted in low IRES activity, particularly with the HCV coding sequences. RNA structure probing showed that the efficiency of internal initiation of these chimeric constructs correlated most closely with the degree of sing le-strandedness of the region around and immediately downstream of the initiation codon. The low activity IRESs could not be rescued by addition of supplementary eIF4A (the initiation factor with ATP-dependent RNA helicase activity). The extreme sensitivity to secondary structure around the initiation codon is likely to be due to the fact that the eIF4F complex (which has eIF4A as one of its subunits) is not required for and does not participate in initiation on these IRESs.
引用
收藏
页码:1558 / 1571
页数:14
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