The sequence and context of the 5′ splice site govern the nuclear stability of polyoma virus late RNAs

The sequence and context of the 5′ splice site govern the nuclear stability of polyoma virus late RNAs

We have examined the influence of splicing signals on the stability of polyoma virus late RNAs in the nucleus. Late primary transcripts contain a single 5′ splice site and three alternative 3′ splice sites. In earlier work we showed that the presence of introns was not required for late RNA accumula...

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Bibliographic Details
Published in:Nucleic acids research Vol. 23; no. 23; pp. 4812 - 4817
Main Authors: Barrett, Nancy L., Li, Xiaotong, Carmichael, Gorden G.
Format: Journal Article
Language:English
Published: England Oxford University Press 11-12-1995
Subjects:
3T3 Cells
Animals
Base Sequence
Cell Nucleus - metabolism
Exons - genetics
Genetic Vectors
Introns
Mice
Molecular Sequence Data
Mutation - genetics
Polyomavirus - genetics
RNA Splicing - genetics
RNA, Messenger - metabolism
RNA, Viral - genetics
RNA, Viral - metabolism
Transcription, Genetic
Transfection
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Summary:We have examined the influence of splicing signals on the stability of polyoma virus late RNAs in the nucleus. Late primary transcripts contain a single 5′ splice site and three alternative 3′ splice sites. In earlier work we showed that the presence of introns was not required for late RNA accumulation, however, the 5′ splice site was essential, as removal of only the 5′ splice site was sufficient to destabilize late RNAs up to 100-fold when compared with early RNAs. A complementary clone which retained the 5′ splice site but which carried small deletions of all late region 3′ splice sites produced wild-type levels of unspliced late RNA. In order to extend this work we have constructed additional types of mutants. Point mutations in the 5′ splice site confirmed its importance for RNA stability. Other mutants Included constructs in which the spacing between the 5′ splice site and the late promoter was altered and 5′ splice site insertion mutants where a 58 bp fragment containing the 5′ splice site sequence was inserted separately at various restriction sites in the late region. Both types of mutants lacked all of the late 3′ splice sites and had only a single 5′ splice site. RNase protection analyses of late and early RNAs from these constructs revealed that moving the 5′ splice site away from the late promoter (or from its normal context) destabilized late RNAs >10-fold relative to the wild-type. We conclude that both 5′ splice site integrity and its proximity to the late promoter play important roles in the nuclear stability of polyoma virus late RNAs.
Bibliography:istex:8F6D73F1B74954ABC63492E4028CB29FCC8B58E2
ArticleID:23.23.4812
Prescnt address: Epidemiology Program, Department of Public Health. Hartford, CT 06106, USA
To whom correspondence should be addressed
ark:/67375/HXZ-8QM21FCX-F
ObjectType-Article-2
SourceType-Scholarly Journals-1
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content type line 23
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ISSN:0305-1048
1362-4962
DOI:10.1093/nar/23.23.4812