Affiliation:
1. Department of Microbiology and Immunology
2. The Cancer Center, University of Rochester, Rochester, New York 14642
Abstract
ABSTRACT
Essential to the oncogenic properties of human papillomavirus type 16 (HPV-16) are the activities encoded by the early gene product E7. HPV-16 E7 (E7.16) binds to cellular factors involved in cell cycle regulation and differentiation. These include the retinoblastoma tumor suppressor protein (Rb) and histone deacetylase (HDAC) complexes. While the biological significance of these interactions remains unclear, E7 is believed to help maintain cells in a proliferative state, thus establishing an environment that is conducive to viral replication. Most pathways that govern cell growth converge on downstream effectors. Among these is the cdc25A tyrosine phosphatase. cdc25A is required for G
1
/S transition, and its deregulation is associated with carcinogenesis. Considering the importance of cdc25A in cell cycle progression, it represents a relevant target for viral oncoproteins. Accordingly, the present study focuses on the putative deregulation of cdc25A by E7.16. Our results indicate that E7.16 can impede growth arrest induced during serum starvation and keratinocyte differentiation. Importantly, these E7-specific phenotypes correlate with elevated cdc25A steady-state levels. Reporter assays performed with NIH 3T3 cell lines and human keratinocytes indicate that E7 can transactivate the
cdc25A
promoter. In addition, transcriptional activation by E7.16 requires the distal E2F site within the
cdc25A
promoter. We further demonstrate that the ability of E7 to abrogate cell cycle arrest, activate
cdc25A
transcription, and increase cdc25A protein levels requires intact Rb and HDAC-1 binding domains. Finally, by using the cdk inhibitor roscovitine, we reveal that E7 activates the
cdc25A
promoter independently of cell cycle progression and cdk activity. Consequently, we propose that E7.16 can directly target
cdc25A
transcription and maintains
cdc25A
gene expression by disrupting Rb/E2F/HDAC-1 repressor complexes.
Publisher
American Society for Microbiology
Subject
Virology,Insect Science,Immunology,Microbiology
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