Defined mutations in the 5' nontranslated sequence of Sindbis virus RNA.

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J Virol. 1990 September; 64(9): 4162-4168

Defined mutations in the 5' nontranslated sequence of Sindbis virus RNA.

H G Niesters and J H Strauss

California Institute of Technology, Division of Biology, Pasadena 91125.

ABSTRACT

We have constructed 24 deletion mutants which contain deletionsof from 1 to 15 nucleotides in the 5' nontranslated region ofSindbis virus RNA and tested the effect of these mutations onvirus replication. The results showed that the first 44 nucleotides,which are capable of forming a hairpin structure, are importantfor virus replication, as all deletions tested in this regionwere either lethal or resulted in virus that grew poorly incomparison to the parental virus. Many of these deletions haddifferent effects in mosquito cells than in chicken cells, suggestingthat cellular factors, presumably proteins, bind to this region.This domain may function in at least two processes in viralreplication. It seems likely that in the minus strand, thissequence element is bound by the viral replicase and promotesRNA replication. In the plus strand, this element may modulateinitiation of translation of the nonstructural proteins. Theresults suggest that the hairpin structure itself is important.All deletions within it had deleterious effects on virus replication,and in particular, deletion of one of the G residues at nucleotide7 or 8 or of one of the C residues at nucleotide 36 or 37 whichare theoretically base-paired with these G's resulted in temperature-sensitiveviruses that behaved very similarly. In contrast, large deletionsbetween the 44-nucleotide hairpin and the translation startsite at nucleotides 60 to 62 resulted in virus that grew aswell as or better than the parental virus in both chicken andmosquito cells. The A residue at position 5 of the HRSP strainused was examined in more detail. Deletion of this A was lethal,whereas substitution by G resulted in a virus that grew poorly,despite the fact that G is present at position 5 in the AR339parent of HRSP. U at position 5 resulted in a virus that grewless well than the A5 strain but better than the G5 mutant.

J Virol. 1990 September; 64(9): 4162-4168

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