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Animal: DNA Viruses |
International Centre for Genetic Engineering and Biotechnology, Padriciano 99, I-34012 Trieste, Italy1
Author for correspondence: Lawrence Banks. Fax +39 040 226555. e-mail banks{at}icgeb.trieste.it
Previous studies have shown that the human papillomavirus type 16 (HPV-16) E6 protein binds to p300/CBP and abrogates its transcriptional co-activator function. However, there is little information on the biological consequences of this interaction and discrepancy as to whether the interaction is high-risk E6 specific or not. We performed a series of studies to compare the interactions of HPV-18 and HPV-11 E6 with p300, and showed that both high- and low- risk E6 proteins bind p300. In addition, using a transformation-deficient mutant of adenovirus E1a, which cannot interact with p300, we demonstrated that HPV-16, HPV-18 and, to a lesser extent, HPV-11 E6, can complement this mutant in cell transformation assays. In contrast, a mutant of HPV-16 E6 which does not bind p300 failed to rescue the E1a mutant. These results suggest that the E6–p300 interaction may be important for the ability of HPV E6 to contribute towards cell transformation.
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  J. M. Routes, K. Morris, M. C. Ellison, and S. Ryan Macrophages Kill Human Papillomavirus Type 16 E6-Expressing Tumor Cells by Tumor Necrosis Factor Alpha- and Nitric Oxide-Dependent Mechanisms J. Virol., January 1, 2005; 79(1): 116 - 123. [Abstract] [Full Text] [PDF]
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