Analysis of the status of the novel estrogen receptor α (ERα) coactivator p72 in endometrial cancer and its cross talk with erbB-2 in the transactivation of ERα

  • Authors:
    • Lin Zhao
    • Michiko Watanabe
    • Tetsu Yano
    • Junn Yanagisawa
    • Shunsuke Nakagawa
    • Hajime Oishi
    • Osamu Wada-Hiraike
    • Katsutoshi Oda
    • Takeo Minaguchi
    • Toshiharu Yasugi
    • Shigeaki Kato
    • Yuji Taketani
  • View Affiliations

  • Published online on: May 1, 2008     https://doi.org/10.3892/mmr.1.3.387
  • Pages: 387-390
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Abstract

To determine how estrogens are involved in the growth of endometrial cancer with varying degrees of differentiation, we investigated the status of p72, a novel specific coactivator for estrogen receptor α (ERα) activation function-1 (AF-1), AIB1, a steroid receptor coactivator amplified in breast cancer 1, erbB-2, a receptor tyrosine kinase, and ERα in endometrial cancer. Gene expression of ERα, p72, AIB1 and erbB-2 was measured in 26 samples of primary endometrial cancers by real-time RT-PCR, and their in vivo cellular effects on the transactivation function of ERα were examined by a transient expression assay. The mRNA levels of erbB-2 increased and those of ERα, p72 and AIB1 decreased with the loss of histological differentiation. Transient expression of p72, AIB1 and erbB-2 in human embryonic kidney 293T cells led to a synergistic promotion of the transactivation function of ERα in the presence of 17α-estradiol or 4-hydroxytamoxifen, an ERα AF-1 agonist/AF-2 antagonist, as a ligand. In conclusion, estrogen action through ERα AF-1 might be exerted by the increased expression of the coactivators p72 and AIB1, together with cross talk between erbB-2 and p72, to accelerate the transactivation of ERα AF-1 in endometrial cancer. These findings also suggest that the cooperative transactivation of ERα AF-1 by the overexpression of p72, AIB1 and erbB-2 might be involved in tamoxifen-stimulated growth of endometrial cancer.

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May-June 2008
Volume 1 Issue 3

Print ISSN: 1791-2997
Online ISSN:1791-3004

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Spandidos Publications style
Zhao L, Watanabe M, Yano T, Yanagisawa J, Nakagawa S, Oishi H, Wada-Hiraike O, Oda K, Minaguchi T, Yasugi T, Yasugi T, et al: Analysis of the status of the novel estrogen receptor α (ERα) coactivator p72 in endometrial cancer and its cross talk with erbB-2 in the transactivation of ERα. Mol Med Rep 1: 387-390, 2008.
APA
Zhao, L., Watanabe, M., Yano, T., Yanagisawa, J., Nakagawa, S., Oishi, H. ... Taketani, Y. (2008). Analysis of the status of the novel estrogen receptor α (ERα) coactivator p72 in endometrial cancer and its cross talk with erbB-2 in the transactivation of ERα. Molecular Medicine Reports, 1, 387-390. https://doi.org/10.3892/mmr.1.3.387
MLA
Zhao, L., Watanabe, M., Yano, T., Yanagisawa, J., Nakagawa, S., Oishi, H., Wada-Hiraike, O., Oda, K., Minaguchi, T., Yasugi, T., Kato, S., Taketani, Y."Analysis of the status of the novel estrogen receptor α (ERα) coactivator p72 in endometrial cancer and its cross talk with erbB-2 in the transactivation of ERα". Molecular Medicine Reports 1.3 (2008): 387-390.
Chicago
Zhao, L., Watanabe, M., Yano, T., Yanagisawa, J., Nakagawa, S., Oishi, H., Wada-Hiraike, O., Oda, K., Minaguchi, T., Yasugi, T., Kato, S., Taketani, Y."Analysis of the status of the novel estrogen receptor α (ERα) coactivator p72 in endometrial cancer and its cross talk with erbB-2 in the transactivation of ERα". Molecular Medicine Reports 1, no. 3 (2008): 387-390. https://doi.org/10.3892/mmr.1.3.387