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Journal of Virology, September 2000, p. 8513-8523, Vol. 74, No. 18
Department of Microbiology, University of
Iowa, Iowa City, Iowa 52242
Received 17 March 2000/Accepted 1 June 2000
The direct-repeat elements (dr1) of avian sarcoma virus (ASV) and
leukosis virus have the properties of constitutive transport elements
(CTEs), which facilitate cytoplasmic accumulation of unspliced RNA. It
is thought that these elements represent binding sites for cellular
factors. Previous studies have indicated that in the context of the
avian sarcoma virus genome, precise deletion of both ASV dr1 elements
results in a very low level of virus replication. This is characterized
by a decreased cytoplasmic accumulation of unspliced RNA and a
selective increase in spliced src mRNA. Deletion of either
the upstream or downstream dr1 results in a delayed-replication
phenotype. To determine if the same regions of the dr1 mediate
inhibition of src splicing and unspliced RNA transport,
point mutations in the upstream and downstream elements were studied.
In the context of viral genomes with single dr1 elements, the effects
of the mutations on virus replication and increases in src
splicing closely paralleled the effects of the mutations on CTE
activity. For mutants strongly affecting CTE activity and splicing,
unspliced RNA but not spliced RNA turned over in the nucleus more
rapidly than wild-type RNA. In the context of wild-type virus
containing two dr1 elements, mutations of either element that strongly
affect CTE activity caused a marked delay of virus replication and a
selective increase in src splicing. However, the turnover
of the mutant unspliced RNA as well as the spliced mRNA species did not
differ significantly from that of the wild type. These results suggest
the dr1 elements in ASV act to selectively inhibit src
splicing and that both elements contribute to the fitness of the
wild-type virus. However, a single dr1 element is sufficient to
stabilize unspliced RNA.
0022-538X/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.
Selective Inhibition of Splicing at the Avian Sarcoma Virus
src 3' Splice Site by Direct-Repeat Posttranscriptional
cis Elements
*
Corresponding author. Mailing address: Department of
Microbiology, University of Iowa, Iowa City, IA 52242. Phone: (319)
335-7793. Fax: (319) 335-9006. E-mail:
marty-stoltzfus{at}uiowa.edu.
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