Abstract

The second exon of adenovirus EIA negatively modulates in vitro cell transformation, tumorigenesis and tumor metastasis. These activities of exon 2 are encoded within a short region located near the C-terminus of BIA. Mutations within this region confer a hyper-transforming phenotype on EIA. The oncogenesis restraining activities of the C-terminal region of EIA correlate with the interaction of a 48 kDa cellular nuclear protein, CtBP. CtBP is a transcriptional co-repressor. Through mutational analysis, we will determine if the oncogenesis modulating activity of CtBP is linked to its transcriptional repressor activity. CtBP also interacts with a cellular protein CtIP via a CtBP-binding motif, PLDLS. Our hypothesis predicts that interaction of CtIP with CtBP antagonizes the activities of CtBP and that the C-termninus of EIA may suppress tumorigenesis by disrupting the CtBP/CIIP complex. We hypothesize that the activity of a cellular repressor that functions through the CtBP corepressor may be altered by CtIP or E1A exon 2. We will determine the effects of overexpression of CtIP or EtA on the activity of a model human cellular repressor ZEB. CtBP is a phosphoprotein. We will identify the phosphorylation sites and investigate the role of phosphorylation on CtBP functions. In preliminary studies, we have observed that CtBP interacts with the p70 subunit of DNA-dependent protein kinase (DNA-PK). We will determine if CtBP is a target for DNA-PK. Our hypothesis predicts that an oncogenic stimulus would enhance complex formation between CtBP and CtIP. We will test this hypothesis by analyzing the CtBP/CtIP complex by coimmunoprecipitation analysis in cells expressing EtA exon 1. CtIP also interacts with pRb-family tumor suppressor proteins (pRb, p107 and p130) through an Rb-binding site (LXCXE). We hypothesize that the CR2 region ofElA promotes oncogenesis through a novel pathway (in addition to the previously known pRb/E2F pathway) by disrupting complexes of CtIP and pRb-famity proteins. We propose to investigate if the CR2 region of E1A disrupts the pRb/CtIP complex in vivo and leads to oncogenic transformation in cooperation with E2F-l. Thus, our proposed studies should illuminate how a viral oncoprotein, adenovirus EtA, modulates oncogenesis novel pathways that involve cellular proteins CtBP and CtIP.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA084941-02
Application #
6514350
Study Section
Virology Study Section (VR)
Program Officer
Daschner, Phillip J
Project Start
2001-03-01
Project End
2006-02-28
Budget Start
2002-03-01
Budget End
2003-02-28
Support Year
2
Fiscal Year
2002
Total Cost
$226,699
Indirect Cost

  Institution

Name
Saint Louis University
Department
Microbiology/Immun/Virology
Type
Schools of Medicine
DUNS #
City
Saint Louis
State
MO
Country
United States
Zip Code
63103

  Publications

Vijayalingam, S; Subramanian, T; Zhao, Ling-Jun et al. (2016) The Cellular Protein Complex Associated with a Transforming Region of E1A Contains c-MYC. J Virol 90:1070-9
Zhao, Ling-Jun; Subramanian, T; Vijayalingam, S et al. (2014) CtBP2 proteome: Role of CtBP in E2F7-mediated repression and cell proliferation. Genes Cancer 5:31-40
Vijayalingam, S; Kuppusamy, Mohan; Subramanian, T et al. (2014) Evaluation of apoptogenic adenovirus type 5 oncolytic vectors in a Syrian hamster head and neck cancer model. Cancer Gene Ther 21:228-237
Subramanian, T; Zhao, Ling-Jun; Chinnadurai, G (2013) Interaction of CtBP with adenovirus E1A suppresses immortalization of primary epithelial cells and enhances virus replication during productive infection. Virology 443:313-20
Kuppuswamy, Mohan; Subramanian, T; Kostas-Polston, Elizabeth et al. (2013) Functional similarity between E6 proteins of cutaneous human papillomaviruses and the adenovirus E1A tumor-restraining module. J Virol 87:7781-6
Vijayalingam, S; Chinnadurai, G (2013) Adenovirus L-E1A activates transcription through mediator complex-dependent recruitment of the super elongation complex. J Virol 87:3425-34
Chinnadurai, G (2011) Opposing oncogenic activities of small DNA tumor virus transforming proteins. Trends Microbiol 19:174-83
Zhao, Ling-Zun; Chinnadurai, G (2010) Incapacitating CtBP to kill cancer. Cell Cycle 9:3645-6
Komorek, Jessica; Kuppuswamy, Mohan; Subramanian, T et al. (2010) Adenovirus type 5 E1A and E6 proteins of low-risk cutaneous beta-human papillomaviruses suppress cell transformation through interaction with FOXK1/K2 transcription factors. J Virol 84:2719-31
Chinnadurai, G (2009) Joint surveillance of the replication foci by PCNA and CtIP. Cell Cycle 8:1306-1307

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