J. Zwicker et al., The SV40 large T oncoprotein disrupts DNA-binding of the cell cycle-regulated transcriptional repressor CDF, ONCOGENE, 18(11), 1999, pp. 2023-2025
A hallmark of neoplastic transformation by DNA tumor viruses is the deregul
ation of cell cycle genes. At least in some genes, this deregulation appear
s to be due to the oncoprotein-mediated disruption of complexes between E2F
and pocket proteins and the ensuing generation of transcriptionally active
free E2F. In the present study, we have analysed the effect of the SV40 la
rge T oncoprotein (SV-LT) on the function of a different cell cycle-regulat
ed transcriptional repressor, CDF, which is the principal regulator of the
cdc25C, cyclin A and cdc2 genes, As shown by genomic footprinting of sorted
G(1) and G(2) cell populations, transformation by SV-LT completely abrogat
ed protection of the CDF binding site (CDE-CHR) in the cdc25C promoter. In
agreement with this observation, expression of the SV-LT in fibroblasts led
to a dramatic up-regulation of the cdc25C promoter in cells synchronized i
n G(0). These findings indicate that the oncoprotein-mediated dissociation
of the CDF repressor protein from its cognate DNA-binding site is a major m
echanism in virus-induced transcriptional deregulation.