Abstract

Viruses alter cellular pathways in order to create an environment conducive for the infectious cycle, and to inactivate or escape cellular and systemic anti-viral defense systems. Faced with these challenges, viruses encode proteins or small RNAs to interact with key viral and cellular targets that normally regulate cell growth, death, transcriptional status and communication with systemic anti-viral defenses. DNA tumor viruses, such as simian virus 40 (SV40) have proved to be powerful tools for uncovering pathways that mediate cell proliferation, differentiation, and death. These viruses encode dominantly acting proteins that alter key cellular signal transduction pathways or regulate viral and cellular gene expression. The multifunctional large T antigen encoded by SV40 plays roles in both productive infection and tumorigenesis. T antigen drives cells into S phase by inhibiting the Rb-family of tumor suppressor proteins, and thus activating the expression of genes regulated by the E2F-family of transcription factors. This action requires a functional LXCXE motif that directs the association of T antigen with Rb-E2F complexes, and a J domain, that recruits hsc70. Simultaneously, T antigen binds the tumor suppressor p53 and inhibiting its transcriptional activation activity, and thus blocking p53-dependent cell-cycle arrest and apoptosis. Two key questions are whether the J domain and LXCXE motif of T antigen are sufficient to induce E2F-dependent transcription, and whether the inactivation of Rb and p53 tumor suppressors is the only T antigen functions that contribute to transformation. The regulation of gene expression also plays a role in productive infection. SV40 uses two mechanisms to downregulate early region transcription. First, T antigen binds to the early viral promoter directly inhibiting transcription. In addition, SV40 encodes miRNAs that bind to early mRNA and lower the expression of the viral tumor antigens. Consequently, SV40-infected cells are less susceptible to killing by cytotoxic T cells. In this application we propose to explore the roles played by SV40 control of gene expression in transformation and infection. Specifically we will: 1. determine whether the J domain and LXCXE motif sufficient for T antigen regulation of Rb-E2F interactions. 2. Assess the role of Rb- and p53-independent mechanisms in SV40-mediated transformation. 3. Distinguish the relative roles of the T antigen HR domain and the viral miRNAs in SV40 infection. 4. Determine whether T antigen autoregulation contribute to CTL evasion? ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA040586-23
Application #
7475177
Study Section
Virology - B Study Section (VIRB)
Program Officer
Blair, Donald G
Project Start
1985-07-01
Project End
2011-07-31
Budget Start
2008-08-01
Budget End
2009-07-31
Support Year
23
Fiscal Year
2008
Total Cost
$232,610
Indirect Cost

  Institution

Name
University of Pittsburgh
Department
Biology
Type
Schools of Arts and Sciences
DUNS #
004514360
City
Pittsburgh
State
PA
Country
United States
Zip Code
15213

  Publications

Rathi, Abhilasha V; Cantalupo, Paul G; Sarkar, Saumendra N et al. (2010) Induction of interferon-stimulated genes by Simian virus 40 T antigens. Virology 406:202-11
Cantalupo, Paul G; Sáenz-Robles, Maria Teresa; Rathi, Abhilasha V et al. (2009) Cell-type specific regulation of gene expression by simian virus 40 T antigens. Virology 386:183-91
Pipas, James M (2009) SV40: Cell transformation and tumorigenesis. Virology 384:294-303
Ahuja, Deepika; Rathi, Abhilasha V; Greer, Amy E et al. (2009) A structure-guided mutational analysis of simian virus 40 large T antigen: identification of surface residues required for viral replication and transformation. J Virol 83:8781-8
Wright, Christine M; Chovatiya, Raj J; Jameson, Nora E et al. (2008) Pyrimidinone-peptoid hybrid molecules with distinct effects on molecular chaperone function and cell proliferation. Bioorg Med Chem 16:3291-301
Zhao, Xiaorong; Madden-Fuentes, Ramiro J; Lou, Becky X et al. (2008) Ataxia telangiectasia-mutated damage-signaling kinase- and proteasome-dependent destruction of Mre11-Rad50-Nbs1 subunits in Simian virus 40-infected primate cells. J Virol 82:5316-28
Saenz-Robles, M T; Toma, D; Cantalupo, P et al. (2007) Repression of intestinal drug metabolizing enzymes by the SV40 large T antigen. Oncogene 26:5124-31
Ahuja, Deepika; Saenz-Robles, M Teresa; Pipas, James M (2005) SV40 large T antigen targets multiple cellular pathways to elicit cellular transformation. Oncogene 24:7729-45
Cantalupo, Paul; Doering, Adrienne; Sullivan, Christopher S et al. (2005) Complete nucleotide sequence of polyomavirus SA12. J Virol 79:13094-104
Markovics, Jennifer A; Carroll, Patrick A; Robles, M Teresa Saenz et al. (2005) Intestinal dysplasia induced by simian virus 40 T antigen is independent of p53. J Virol 79:7492-502

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