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CHF: a novel factor binding to cyclin A CHR corepressor element

Abstract

Cell cycle modulation of cyclin A expression is due to the periodic relief of a transcriptional repression mediated by a bipartite negative DNA regulatory region. The 5′ element (Cell Cycle Responsive Element: CCRE; cell Cycle Dependent Element: CDE) is clearly occupied in a cyclic manner in vivo, whereas the 3′ element, whose sequence is shared by B-myb, cdc25C and cdc2 genes (cell Cycle gene Homology Region: CHR), is involved in more subtle interactions. Mutation of either element results in complete deregulation of cyclin A promoter activity. Whereas some reports claim that E2F/DP can bind to the CCRE/CDE, the nature of the protein(s) interacting with the CHR is unknown. In the present work we have characterized an activity present in quiescent cells and absent in cells blocked in S phase, which binds specifically to cyclin A CHR, but not to B-myb, or to cdc25C, or to cdc2 CHRs. A 90 kD protein, named CHF (cyclin A CHR binding factor), has been identified through preparative electrophoresis and UV crosslinking experiments. In order to address in more functional terms the binding of CHF to cyclin A CHR, we developed in vitro and in vivo oligonucleotide competition assays. Both in vitro transcription and in vivo microinjection experiments demonstrate that a functional difference exists between the composite CCRE/CDE-CHR repressor regions of cell cycle regulated genes such as cyclin A and cdc25C.

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Acknowledgements

We thank A Fernandez for her interest in this work and help with photomicroscopy. We are grateful to R Hipskind, C Sardet and ML Vignais for discussions around this work, which was supported by grants from the CNRS, the BIOMED2 program, the ARC and the Ligue Nationale contre le Cancer.

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Philips, A., Chambeyron, S., Lamb, N. et al. CHF: a novel factor binding to cyclin A CHR corepressor element. Oncogene 18, 6222–6232 (1999). https://doi.org/10.1038/sj.onc.1203017

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