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Transactivation of E2F-regulated genes by polyomavirus large T antigen: evidence for a two-step mechanism. | LitMetric

Transactivation of E2F-regulated genes by polyomavirus large T antigen: evidence for a two-step mechanism.

Mol Cell Biol

Medical University of Vienna, Department of Medical Biochemistry, Division of Molecular Biology, Vienna Biocenter, Dr. Bohrgasse 9, A-1030 Vienna, Austria.

Published: December 2004

AI Article Synopsis

  • Polyomavirus large T antigen activates genes involved in S phase induction by disrupting E2F-pocket protein complexes.
  • This process requires specific sites on the viral protein for binding pocket proteins and chaperones.
  • The interaction of large T antigen with the CBP/p300-PCAF histone acetyltransferase complex is crucial for gene transactivation, indicating that additional recruitment of this complex is necessary beyond just dissociation of E2F complexes.

Article Abstract

Polyomavirus large T antigen transactivates a variety of genes whose products are involved in S phase induction. These genes are regulated by the E2F family of transcription factors, which are under the control of the pocket protein retinoblastoma protein and its relatives p130 and p107. The viral protein causes a dissociation of E2F-pocket protein complexes that results in transactivation of the genes. This reaction requires the N-terminal binding site for pocket proteins and the J domain that binds chaperones. We found earlier that a mutation of the zinc finger located within the C-terminal domain, a region assumed to function mainly in the replication of viral DNA, also interferes with transactivation. Here we show that binding of the histone acetyltransferase coactivator complex CBP/p300-PCAF to the C terminus correlates with the ability of large T antigen to transactivate genes. This interaction results in promoter-specific acetylation of histones. Inactive mutant proteins with changes within the C-terminal domain were nevertheless able to dissociate the E2F pocket protein complexes, indicating that this dissociation is a necessary but insufficient step in the T antigen-induced transactivation of genes. It has to be accompanied by a second step involving the T antigen-mediated recruitment of a histone acetyltransferase complex.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC533978PMC
http://dx.doi.org/10.1128/MCB.24.24.10986-10994.2004DOI Listing

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