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Literature DB >> 3003386

Properties of the simian virus 40 (SV40) large T antigens encoded by SV40 mutants with deletions in gene A.

Abstract

The biochemical properties of the large T antigens encoded by simian virus 40 (SV40) mutants with deletions at DdeI sites in the SV40 A gene were determined. Mutant large T antigens containing only the first 138 to 140 amino acids were unable to bind to the SV40 origin of DNA replication as were large T antigens containing at their COOH termini 96 or 97 amino acids encoded by the long open reading frame located between 0.22 and 0.165 map units (m.u.). All other mutant large T antigens were able to bind to the SV40 origin of replication. Mutants with in-phase deletions at 0.288 and 0.243 m.u. lacked ATPase activity, but ATPase activity was normal in mutants lacking origin-binding activity. The 627-amino acid large T antigen encoded by dlA2465, with a deletion at 0.219 m.u., was the smallest large T antigen displaying ATPase activity. Mutant large T antigens with the alternate 96- or 97-amino acid COOH terminus also lacked ATPase activity. All mutant large T antigens were found in the nuclei of infected cells; a small amount of large T with the alternate COOH terminus was also located in the cytoplasm. Mutant dlA2465 belonged to the same class of mutants as dlA2459. It was unable to form plaques on CV-1p cells at 37 or 32 degrees C but could form plaques on BSC-1 monolayers at 37 degrees C but not at 32 degrees C. It was positive for viral DNA replication and showed intracistronic complementation with any group A mutant whose large T antigen contained a normal carboxyl terminus. These findings and those of others suggest that both DNA binding and ATPase activity are required for the viral DNA replication function of large T antigen, that these two activities must be located on the same T antigen monomer, and that these two activities are performed by distinct domains of the polypeptide. These domains are distinct and separable from the domain affected by the mutation of dlA2465 and indicate that SV40 large T antigen is made up of at least three separate functional domains.

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Year: 1986 PMID： 3003386 PMCID： PMC252767

Source DB: PubMed Journal: J Virol ISSN： 0022-538X Impact factor: 5.103

40 in total

6. Monoclonal antibodies as probes for a function of large T antigen during the elongation process of simian virus 40 DNA replication.

Authors: M Wiekowski; P Dröge; H Stahl
Journal: J Virol Date: 1987-02 Impact factor: 5.103

7. Large T-antigen mutants define multiple steps in the initiation of simian virus 40 DNA replication.

Authors: I J Mohr; M P Fairman; B Stillman; Y Gluzman
Journal: J Virol Date: 1989-10 Impact factor: 5.103

8. Simian virus 40 host range/helper function mutations cause multiple defects in viral late gene expression.

Authors: T Stacy; M Chamberlain; C N Cole
Journal: J Virol Date: 1989-12 Impact factor: 5.103

9. Linker insertion mutants of simian virus 40 large T antigen that show trans-dominant interference with wild-type large T antigen map to multiple sites within the T-antigen gene.

Authors: J Y Zhu; C N Cole
Journal: J Virol Date: 1989-11 Impact factor: 5.103

10. Simian virus 40 large T antigen host range domain functions in virion assembly.

Authors: S L Spence; J M Pipas
Journal: J Virol Date: 1994-07 Impact factor: 5.103

Properties of the simian virus 40 (SV40) large T antigens encoded by SV40 mutants with deletions in gene A.

1. Mutational analysis of the simian virus 40 replicon: pseudorevertants of mutants with a defective replication origin.

2. The binding site on SV40 DNA for a T antigen-related protein.

3. DNA binding and sedimentation properties of SV40 T antigens synthesized in vivo and in vitro.

4. Sequencing end-labeled DNA with base-specific chemical cleavages.

5. Pyrimidine-specific chemical reactions useful for DNA sequencing.

6. Simian virus 40 mutants with deletions at the 3' end of the early region are defective in adenovirus helper function.

7. A poly(dT)-stimulated ATPase activity associated with simian virus 40 large T antigen.

8. Characterization of a fused protein specified by the adenovirus type 2-simian virus 40 hybrid Ad2+ND1 dp2.

9. Physical and genetic characterization of deletion mutants of simian virus 40 constructed in vitro.

10. Characterization of the autoregulation of simian virus 40 gene A.

1. Functional characterization of temperature-sensitive mutants of simian virus 40 large T antigen.

2. trans-Dominant and non-trans-dominant mutant simian virus 40 large T antigens show distinct responses to ATP.

3. Mapping of helicase and helicase substrate-binding domains on simian virus 40 large T antigen.

Review 4. Viral proteins containing the purine NTP-binding sequence pattern.

5. T-antigen-DNA polymerase alpha complex implicated in simian virus 40 DNA replication.

6. Monoclonal antibodies as probes for a function of large T antigen during the elongation process of simian virus 40 DNA replication.

7. Large T-antigen mutants define multiple steps in the initiation of simian virus 40 DNA replication.

8. Simian virus 40 host range/helper function mutations cause multiple defects in viral late gene expression.

9. Linker insertion mutants of simian virus 40 large T antigen that show trans-dominant interference with wild-type large T antigen map to multiple sites within the T-antigen gene.

10. Simian virus 40 large T antigen host range domain functions in virion assembly.