par Chariot, Alain;Van Lint, Carine 
;Chapelier, M;Gielen, J;Merville, Marie-Paule;Bours, Vincent
Référence Oncogene, 18, 27, page (4007-4014)
Publication Publié, 1999
;Chapelier, M;Gielen, J;Merville, Marie-Paule;Bours, VincentRéférence Oncogene, 18, 27, page (4007-4014)
Publication Publié, 1999
Article révisé par les pairs
| Résumé : | Homeodomain-containing proteins are transcription factors regulating the coordinated expression of multiple target genes involved in development, differentiation and cellular transformation. In this study, we demonstrated that HOXB7, one member of this family, behaved as a transactivator in breast cancer cells. Deletion of either the HOXB7 N-terminal domain or the C-terminal acidic tail abolished this transcriptional effect, suggesting a combination of distinct functional transactivating domains. HOXB7 physically interacted both in vitro and in vivo with the coactivator CREB-binding protein (CBP). This interaction led to an enhanced transactivating potential and required the N-terminal of HOXB7 as well as two domains located at the C-terminal part of CBP. Moreover, trichostatin A, a deacetylase inhibitor, strongly enhanced the transcriptional properties of HOXB7. Our data therefore indicate that HOX proteins can directly interact with CBP and that acetylation/deacetylation may regulate their transcriptional properties. |
