Genomic and Nongenomic Effects of Estrogen Signaling in Human Endometrial Cells: Involvement of the Growth Factor Receptor Signaling Downstream AKT Pathway

被引:0
|
作者
Sussane C. J. P. Gielen
Lindy A. M. Santegoets
Liesbeth C. M. Kühne
Wilfred F. J. Van IJcken
Bianca Boers-Sijmons
Payman Hanifi-Moghaddam
Theo J. M. Helmerhorst
Leen J. Blok
Curt W. Burger
机构
[1] Erasmus University Medical Center,Department of Obstetrics and Gynecology
[2] Josephine Nefkens Institute,Department of Reproduction and Development
[3] Eramus University Medical Center,Center for Biomics
[4] Erasmus University Medical Center,Department of Molecular Design and Informatics
[5] Organon NV,undefined
来源
Reproductive Sciences | 2007年 / 14卷
关键词
Estrogen; tamoxifen; insulin-like growth factor receptor; endothelial growth factor receptor; microarray; AKT; amphiregulin;
D O I
暂无
中图分类号
学科分类号
摘要
For the endometrium, estradiol and tamoxifen induce proliferation, and consequently, tamoxifen treatment of breast cancer results in a 2-fold to 7-fold increased risk for endometrial cancer. Here, the role of activation of growth factor receptor signaling in mediating the e fects of estrogen and tamoxifen is determined. Microarray analysis of ECC-1 cells treated with estradiol or tamoxifen indicate that rapid responses to treatment (1 hour) are very distinct from long-term responses (> 24 hours). Furthermore, estradiol and tamoxifen are observed to induce AKT activation. Comparing long-term estrogen- and tamoxifen-regulated genes with genes regulated by insulin-like growth factor 1 and amphiregulin reveals that the late e fects of estrogen and tamoxifen signaling may partly be mediated via activation of growth factor receptor signaling pathways. It is hypothesized that both early and late e fects of estrogen and tamoxifen signaling in the endometrium are partly mediated via the activation of growth factor receptor signaling, putatively at the level of AKT activation.
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页码:646 / 654
页数:8
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