The ERα coactivator, HER4/4ICD, regulates progesterone receptor expression in normal and malignant breast epithelium
The HER4 intracellular domain (4ICD) is a potent estrogen receptor (ERα) coactivator with activities in breast cancer and the developing mammary gland that appear to overlap with progesterone receptor (PgR). In fact, 4ICD has recently emerged as an important regulator and predictor of tamoxifen resp...
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| Published in | Molecular cancer Vol. 9; no. 1; p. 150 |
|---|---|
| Main Authors | , , , , , , |
| Format | Journal Article |
| Language | English |
| Published |
London
BioMed Central
15.06.2010
BMC |
| Subjects | |
| Online Access | Get full text |
| ISSN | 1476-4598 1476-4598 |
| DOI | 10.1186/1476-4598-9-150 |
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| Abstract | The HER4 intracellular domain (4ICD) is a potent estrogen receptor (ERα) coactivator with activities in breast cancer and the developing mammary gland that appear to overlap with progesterone receptor (PgR). In fact, 4ICD has recently emerged as an important regulator and predictor of tamoxifen response, a role previously thought to be fulfilled by PgR. Here we investigated the possibility that the 4ICD coactivator regulates PgR expression thereby providing a mechanistic explanation for their partially overlapping activities in breast cancer. We show that 4ICD is both sufficient and necessary to potentiate estrogen stimulation of gene expression. Suppression of HER4/4ICD expression in the MCF-7 breast tumor cell line completely eliminated estrogen stimulated expression of PgR. In addition, the HER4/4ICD negative MCF-7 variant, TamR, failed to express PgR in response to estrogen. Reintroduction of wild-type HER4 but not the γ-secretase processing mutant HER4V673I into the TamR cell line restored PgR expression indicating that 4ICD is an essential PgR coactivator in breast tumor cells. These results were substantiated
in vivo
using two different physiologically relevant experimental systems. In the mouse mammary gland estrogen regulates expression of PgR-A whereas expression of PgR-B is estrogen independent. Consistent with a role for 4ICD in estrogen regulated PgR expression
in vivo
, PgR-A, but not PgR-B, expression was abolished in HER4-null mouse mammary glands during pregnancy. Coexpression of PgR and 4ICD is also commonly observed in ERα positive breast carcinomas. Using quantitative AQUA IHC technology we found that 4ICD potentiated PgR expression in primary breast tumors and the highest levels of PgR expression required coexpression of ERα and the 4ICD coactivator. In summary, our results provide compelling evidence that 4ICD is a physiologically important ERα coactivator and 4ICD cooperates with ERα to potentiate PgR expression in the normal and malignant breast. We propose that direct coupling of these signaling pathways may have important implications for mammary development, breast carcinogenesis, and patient response to endocrine therapy. |
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| AbstractList | The HER4 intracellular domain (4ICD) is a potent estrogen receptor (ERα) coactivator with activities in breast cancer and the developing mammary gland that appear to overlap with progesterone receptor (PgR). In fact, 4ICD has recently emerged as an important regulator and predictor of tamoxifen response, a role previously thought to be fulfilled by PgR. Here we investigated the possibility that the 4ICD coactivator regulates PgR expression thereby providing a mechanistic explanation for their partially overlapping activities in breast cancer. We show that 4ICD is both sufficient and necessary to potentiate estrogen stimulation of gene expression. Suppression of HER4/4ICD expression in the MCF-7 breast tumor cell line completely eliminated estrogen stimulated expression of PgR. In addition, the HER4/4ICD negative MCF-7 variant, TamR, failed to express PgR in response to estrogen. Reintroduction of wild-type HER4 but not the γ-secretase processing mutant HER4V673I into the TamR cell line restored PgR expression indicating that 4ICD is an essential PgR coactivator in breast tumor cells. These results were substantiated
in vivo
using two different physiologically relevant experimental systems. In the mouse mammary gland estrogen regulates expression of PgR-A whereas expression of PgR-B is estrogen independent. Consistent with a role for 4ICD in estrogen regulated PgR expression
in vivo
, PgR-A, but not PgR-B, expression was abolished in HER4-null mouse mammary glands during pregnancy. Coexpression of PgR and 4ICD is also commonly observed in ERα positive breast carcinomas. Using quantitative AQUA IHC technology we found that 4ICD potentiated PgR expression in primary breast tumors and the highest levels of PgR expression required coexpression of ERα and the 4ICD coactivator. In summary, our results provide compelling evidence that 4ICD is a physiologically important ERα coactivator and 4ICD cooperates with ERα to potentiate PgR expression in the normal and malignant breast. We propose that direct coupling of these signaling pathways may have important implications for mammary development, breast carcinogenesis, and patient response to endocrine therapy. Abstract The HER4 intracellular domain (4ICD) is a potent estrogen receptor (ERα) coactivator with activities in breast cancer and the developing mammary gland that appear to overlap with progesterone receptor (PgR). In fact, 4ICD has recently emerged as an important regulator and predictor of tamoxifen response, a role previously thought to be fulfilled by PgR. Here we investigated the possibility that the 4ICD coactivator regulates PgR expression thereby providing a mechanistic explanation for their partially overlapping activities in breast cancer. We show that 4ICD is both sufficient and necessary to potentiate estrogen stimulation of gene expression. Suppression of HER4/4ICD expression in the MCF-7 breast tumor cell line completely eliminated estrogen stimulated expression of PgR. In addition, the HER4/4ICD negative MCF-7 variant, TamR, failed to express PgR in response to estrogen. Reintroduction of wild-type HER4 but not the γ-secretase processing mutant HER4V673I into the TamR cell line restored PgR expression indicating that 4ICD is an essential PgR coactivator in breast tumor cells. These results were substantiated in vivo using two different physiologically relevant experimental systems. In the mouse mammary gland estrogen regulates expression of PgR-A whereas expression of PgR-B is estrogen independent. Consistent with a role for 4ICD in estrogen regulated PgR expression in vivo, PgR-A, but not PgR-B, expression was abolished in HER4-null mouse mammary glands during pregnancy. Coexpression of PgR and 4ICD is also commonly observed in ERα positive breast carcinomas. Using quantitative AQUA IHC technology we found that 4ICD potentiated PgR expression in primary breast tumors and the highest levels of PgR expression required coexpression of ERα and the 4ICD coactivator. In summary, our results provide compelling evidence that 4ICD is a physiologically important ERα coactivator and 4ICD cooperates with ERα to potentiate PgR expression in the normal and malignant breast. We propose that direct coupling of these signaling pathways may have important implications for mammary development, breast carcinogenesis, and patient response to endocrine therapy. |
| ArticleNumber | 150 |
| Author | Wansbury, Olivia Giltnane, Jennifer M Howard, Beatrice A Rimm, David L Jones, Frank E Rokicki, Jerzy Das, Partha M |
| AuthorAffiliation | 1 Department of Cell and Molecular Biology, Tulane University, New Orleans, Louisiana, 70118, USA 3 The Breakthrough Breast Cancer Research Centre, The Institute of Cancer Research, London, SW36JB, UK 2 Department of Pathology, Yale University School of Medicine, New Haven, Connecticut, 06520, USA |
| AuthorAffiliation_xml | – name: 1 Department of Cell and Molecular Biology, Tulane University, New Orleans, Louisiana, 70118, USA – name: 3 The Breakthrough Breast Cancer Research Centre, The Institute of Cancer Research, London, SW36JB, UK – name: 2 Department of Pathology, Yale University School of Medicine, New Haven, Connecticut, 06520, USA |
| Author_xml | – sequence: 1 givenname: Jerzy surname: Rokicki fullname: Rokicki, Jerzy organization: Department of Cell and Molecular Biology, Tulane University – sequence: 2 givenname: Partha M surname: Das fullname: Das, Partha M organization: Department of Cell and Molecular Biology, Tulane University – sequence: 3 givenname: Jennifer M surname: Giltnane fullname: Giltnane, Jennifer M organization: Department of Pathology, Yale University School of Medicine – sequence: 4 givenname: Olivia surname: Wansbury fullname: Wansbury, Olivia organization: The Breakthrough Breast Cancer Research Centre, The Institute of Cancer Research – sequence: 5 givenname: David L surname: Rimm fullname: Rimm, David L organization: Department of Pathology, Yale University School of Medicine – sequence: 6 givenname: Beatrice A surname: Howard fullname: Howard, Beatrice A organization: The Breakthrough Breast Cancer Research Centre, The Institute of Cancer Research – sequence: 7 givenname: Frank E surname: Jones fullname: Jones, Frank E email: fjones3@tulane.edu organization: Department of Cell and Molecular Biology, Tulane University |
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| Copyright | Rokicki et al; licensee BioMed Central Ltd. 2010 This article is published under license to BioMed Central Ltd. This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited. Copyright ©2010 Rokicki et al; licensee BioMed Central Ltd. 2010 Rokicki et al; licensee BioMed Central Ltd. |
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| Title | The ERα coactivator, HER4/4ICD, regulates progesterone receptor expression in normal and malignant breast epithelium |
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