Abstract

The breast is an estrogen responsive tissue, and most breast tumors appear to be, at least initially, estrogen dependent. Furthermore, the estrogen receptor (ER) is overexpressed not only in breast tumors but even in early premalignant breast lesions as compared with normal breast epithelium, so that it may be associated with progression toward cancer. We have also recently found in several early lesions a unique ER mutant which is hypersensitive to estrogen. In many breast tumors we have found enhanced expression of ER splice variants, particularly an exon 5 deletion variant which is active even without estrogen and confers tamoxifen resistance. Thus it seems likely that derangements in the expression level or structure of ER may well play roles both in the development of breast cancer and in the failure of hormone responsiveness during treatment. We now propose to investigate how ER overexpression arises during early progression of breast lesions, how the appearance of certain variants may contribute to the biological behavior of primary breast tumors, particularly tamoxifen resistance, and whether further ER alterations may be associated with the development of metastases.
Our Aims are: 91) To determine the molecular basis for elevated ER expression in hyperplastic breast lesion and breast tumors as compared to adjacent normal breast epithelium, by analysis of the promoter region of the ER and by analysis of the cell-specific ER transactivating factors present which are responsible for the inappropriate activation of ER expression in these lesions. (2) To discover whether expression of the truncated exon 5 ER deletion variant in primary breast cancer is associated with clinical tamoxifen resistance, using tamoxifen-treated patients in the San Antonio Tumor Bank and in a large randomized Swedish adjuvant trial. (3) To study ER alterations in metastatic breast cancers which might be associated with tumor progression, by both direct DNA sequencing and SSCP analyses of paired primary and metastatic tumor specimens. Identified ER alterations will be characterized using our series of unique estrogen-inducible ERE reporters. Cell migration, invasion, and metastatic behavior will also be determined in stable breast cancer cell line transfectants to correlate these features with expression of specific ER alterations. We will also correlate levels of individual ER variants isolated from metastatic breast lesions with clinical outcome. We have already made important discoveries on the occurrence of variant forms of the estrogen receptor and regulation of the receptor in clinical breast cancer. The proposed work should now shed light on the role of Er in early breast lesions. It should also indicate whether the appearance of higher levels of the truncated exon 5 deletion ER splice variant in breast cancer is related to the clinically ominous development of tamoxifen resistance, and suggest which ER variants or mutations presage metastasis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA030195-21
Application #
6479420
Study Section
Project Start
2001-08-01
Project End
2002-12-31
Budget Start
Budget End
Support Year
21
Fiscal Year
2001
Total Cost
Indirect Cost

  Institution

Name
Baylor College of Medicine
Department
Type
DUNS #
074615394
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

Park, Jun Hyoung; Vithayathil, Sajna; Kumar, Santosh et al. (2016) Fatty Acid Oxidation-Driven Src Links Mitochondrial Energy Reprogramming and Oncogenic Properties in Triple-Negative Breast Cancer. Cell Rep 14:2154-2165
Pathiraja, Thushangi N; Nayak, Shweta R; Xi, Yuanxin et al. (2014) Epigenetic reprogramming of HOXC10 in endocrine-resistant breast cancer. Sci Transl Med 6:229ra41
Zhang, Yi; Tseng, Chun-Chih; Tsai, Yuan-Li et al. (2013) Cancer cells resistant to therapy promote cell surface relocalization of GRP78 which complexes with PI3K and enhances PI(3,4,5)P3 production. PLoS One 8:e80071
Machado, Heather L; Kittrell, Frances S; Edwards, David et al. (2013) Separation by cell size enriches for mammary stem cell repopulation activity. Stem Cells Transl Med 2:199-203
Zhang, Xiaomei; Claerhout, Sofie; Prat, Aleix et al. (2013) A renewable tissue resource of phenotypically stable, biologically and ethnically diverse, patient-derived human breast cancer xenograft models. Cancer Res 73:4885-97
Boone, David N; Lee, Adrian V (2012) Targeting the insulin-like growth factor receptor: developing biomarkers from gene expression profiling. Crit Rev Oncog 17:161-73
Casa, Angelo J; Potter, Adam S; Malik, Simeen et al. (2012) Estrogen and insulin-like growth factor-I (IGF-I) independently down-regulate critical repressors of breast cancer growth. Breast Cancer Res Treat 132:61-73
Creighton, Chad J (2012) Molecular classification and drug response prediction in cancer. Curr Drug Targets 13:1488-94
Pathiraja, Thushangi N; Shetty, Priya B; Jelinek, Jaroslav et al. (2011) Progesterone receptor isoform-specific promoter methylation: association of PRA promoter methylation with worse outcome in breast cancer patients. Clin Cancer Res 17:4177-86
Heckman-Stoddard, B M; Vargo-Gogola, T; Herrick, M P et al. (2011) P190A RhoGAP is required for mammary gland development. Dev Biol 360:1-10

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