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• W2103608510 endingPage "3454" @default.
• W2103608510 startingPage "3445" @default.
• W2103608510 abstract "Mutations in the adenovirus gene encoding the E1B 19-kilodalton protein (the 19K protein) result in pleiotropic phenotypes that affect the host cell and virus growth. Examination of viral gene expression in HeLa cells infected with E1B 19K mutant viruses revealed synthesis and accumulation of E1A proteins to higher steady-state levels than those proteins synthesized during infection with the wild-type virus. As a consequence of elevated E1A levels, another early gene product, the 72K DNA-binding protein, accumulated earlier in mutant-infected cells. In a 12S E1A cDNA virus background, E1B 19K gene mutations had a more profound effect. Larger amounts of the 12S E1A product were present in E1B mutant-infected cells. A deletion mutation that eliminated expression of the 19K protein was also responsible for a 200-fold increased plaque-forming efficiency of the 12S cDNA virus in HeLa cells and an increased rate of virus production. Therefore, the E1B 19K tumor antigen may function to down-regulate virus replication by repressing E1A-dependent gene transcription. Eliminating expression of the E1A 13S and 12S gene products by substitution of an E1A 9S cDNA gene, however, uncovered a stimulatory effect of the E1B 19K protein on early gene expression and virus replication. An E1A 9S virus with a wild-type gene encoding the E1B 19K protein displayed increased early gene transcription, synthesized more 72K DNA-binding protein, and replicated more efficiently than an E1A 9S virus containing a mutation that eliminated expression of the 19K protein. Therefore, the E1B 19K protein has both positive and negative effects on early gene expression and virus replication. In the presence of functional E1A gene products, the 19K protein repressed E1A-dependent gene expression, but in the absence of E1A, the 19K protein stimulated viral gene expression and DNA synthesis. This raises the possibility that the E1B 19K protein functions to repress transcription by modifying the activity of the E1A proteins. Independent of E1A, however, the E1B 19K protein can increase viral gene expression and DNA synthesis, which then leads to increased virus replication." @default.
• W2103608510 created "2016-06-24" @default.
• W2103608510 creator A5057995235 @default.
• W2103608510 creator A5071437258 @default.
• W2103608510 creator A5074135831 @default.
• W2103608510 date "1988-09-01" @default.
• W2103608510 modified "2023-10-18" @default.
• W2103608510 title "Role of the adenovirus E1B 19,000-dalton tumor antigen in regulating early gene expression" @default.
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• W2103608510 doi "https://doi.org/10.1128/jvi.62.9.3445-3454.1988" @default.
• W2103608510 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/253469" @default.
• W2103608510 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/2969984" @default.
• W2103608510 hasPublicationYear "1988" @default.

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