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Molecular and Cellular Biology, March 2005, p. 2419-2430, Vol. 25, No. 6
0270-7306/05/$08.00+0     doi:10.1128/MCB.25.6.2419-2430.2005
Copyright © 2005, American Society for Microbiology. All Rights Reserved.

p21^WAF1/CIP1 Selectively Controls the Transcriptional Activity of Estrogen Receptor

Asmaà Fritah,¹ Cécile Saucier,¹ Jan Mester,¹ Gérard Redeuilh,¹ and Michèle Sabbah^1*

Institut National de la Santé et de la Recherche Médicale U482, Hôpital Saint-Antoine, Paris, France¹

Received 13 May 2004/ Returned for modification 11 June 2004/ Accepted 21 December 2004

Estrogen receptors (ER) are ligand-dependent transcription factors that regulate growth, differentiation, and maintenance of cellular functions in a wide variety of tissues. We report here that p21^WAF1/CIP1, a cyclin-dependent kinase (Cdk) inhibitor, cooperates with CBP to regulate the ER-mediated transcription of endogenous target genes in a promoter-specific manner. The estrogen-induced expression of the progesterone receptor and WISP-2 mRNA transcripts in MCF-7 cells was enhanced by p21^WAF1/CIP1, whereas that of the cyclin D1 mRNA was reduced and the pS2 mRNA was not affected. Chromatin immunoprecipitation assays revealed that p21^WAF1/CIP1 was recruited simultaneously with ER and CBP to the endogenous progesterone receptor gene promoter in an estrogen-dependent manner. Experiments in which the p21^WAF1/CIP1 protein was knocked down by RNA interference showed that the induction of the expression of the gene encoding the progesterone receptor required p21^WAF1/CIP1, in contrast with that of the cyclin D1 and pS2 genes. p21^WAF1/CIP1 induced not only cell cycle arrest in breast cancer cells but also milk fat globule protein and lipid droplets, indicators of the differentiated phenotype, as well as cell flattening and increase of the volume of the cytoplasm. These results indicate that p21^WAF1/CIP1, in addition to its Cdk-regulatory role, behaves as a transcriptional coactivator in a gene-specific manner implicated in cell differentiation.

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* Corresponding author. Mailing address: INSERM U482, Hôpital Saint-Antoine, 184 rue du Faubourg Saint-Antoine, 75571 Paris Cedex 12, France. Phone: (33) 1 49 28 46 12/93. Fax: (33) 1 44 74 93 18. E-mail: sabbah{at}st-antoine.inserm.fr.

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Molecular and Cellular Biology, March 2005, p. 2419-2430, Vol. 25, No. 6
0022-538X/05/$08.00+0     doi:10.1128/MCB.25.6.2419-2430.2005
Copyright © 2005, American Society for Microbiology. All Rights Reserved.

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