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Publication : Transcriptional control of the ERBB2 amplicon by ERRalpha and PGC-1beta promotes mammary gland tumorigenesis.

First Author  Deblois G Year  2010
Journal  Cancer Res Volume  70
Issue  24 Pages  10277-87
PubMed ID  20961995 Mgi Jnum  J:167180
Mgi Id  MGI:4867373 Doi  10.1158/0008-5472.CAN-10-2840
Citation  Deblois G, et al. (2010) Transcriptional control of the ERBB2 amplicon by ERRalpha and PGC-1beta promotes mammary gland tumorigenesis. Cancer Res 70(24):10277-87
abstractText  Overexpression of ERBB2 and its neighboring genes on chromosome 17 occurs in approximately 25% of breast tumors and is associated with poor prognosis. While amplification of the 17q12-21 chromosomal region often correlates with an increase in the transcriptional rates of the locus, the molecular mechanisms and the factors involved in the coordinated expression of genes residing within the ERBB2 amplicon remain largely unknown. Here we demonstrate that estrogen-related receptor alpha (ERRalpha, NR3B1) and its coregulator PGC-1beta are key effectors in this process. Using a mouse model of ERBB2-initiated mammary tumorigenesis, we first show that ablation of ERRalpha significantly delays ERBB2-induced tumor development and lowers the levels of amplicon transcripts. Chromosome 17q-wide binding site location analyses in human breast cancer cells show preferential recruitment of ERRalpha to DNA segments associated with the ERBB2 amplicon. Furthermore, ERRalpha directs the co-recruitment of the coactivator PGC-1beta to segments in the 17q12 region and the recruitment of RNA polymerase II to the promoters of the ERBB2 and coamplified genes. ERRalpha and PGC-1beta also participate in the de-repression of ERBB2 expression through competitive genomic cross-talk with estrogen receptor alpha (ERalpha) and, as a consequence, influence tamoxifen sensitivity in breast cancer cells. Taken together, our results suggest that ERRalpha and PGC-1beta are key players in the etiology of malignant breast cancer by coordinating the transcriptional regulation of genes located in the 17q12 region, a process that also involves interference with the repressive function of ERalpha on ERBB2 expression.
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