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Volume 150, Issue 4
21 August 2000
Journal of Cell Biology Cover Image for Volume 150, Issue 4
Article Contents
Report| August 21 2000

Cyclin E as a Coactivator of the Androgen Receptor

Ayako Yamamoto,
Ayako Yamamoto
aInstitute of Molecular and Cellular Biosciences, University of Tokyo, Tokyo 113, Japan
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Yoshihiro Hashimoto,
Yoshihiro Hashimoto
bDepartment of Geriatric Research, National Institute for Longevity Sciences, Obu, Aichi 474-8522, Japan
cDepartment of Urology, Nagoya City University Medical School, Nagoya 467-8601, Japan
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Kenjiro Kohri,
Kenjiro Kohri
cDepartment of Urology, Nagoya City University Medical School, Nagoya 467-8601, Japan
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Etsuro Ogata,
Etsuro Ogata
eCancer Institute Hospital, Japanese Foundation for Cancer Research, Tokyo 170-8455, Japan
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Shige-aki Kato,
Shige-aki Kato
aInstitute of Molecular and Cellular Biosciences, University of Tokyo, Tokyo 113, Japan
fCREST, Japan Science and Technology Corporation, Saitama 332, Japan
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Kyoji Ikeda,
Kyoji Ikeda
bDepartment of Geriatric Research, National Institute for Longevity Sciences, Obu, Aichi 474-8522, Japan
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Makoto Nakanishi
Makoto Nakanishi
bDepartment of Geriatric Research, National Institute for Longevity Sciences, Obu, Aichi 474-8522, Japan
dDepartment of Biochemistry, Nagoya City University Medical School, Nagoya 467-8601, Japan
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Author and Article Information
Ayako Yamamoto
aInstitute of Molecular and Cellular Biosciences, University of Tokyo, Tokyo 113, Japan
Yoshihiro Hashimoto
bDepartment of Geriatric Research, National Institute for Longevity Sciences, Obu, Aichi 474-8522, Japan
cDepartment of Urology, Nagoya City University Medical School, Nagoya 467-8601, Japan
Kenjiro Kohri
cDepartment of Urology, Nagoya City University Medical School, Nagoya 467-8601, Japan
Etsuro Ogata
eCancer Institute Hospital, Japanese Foundation for Cancer Research, Tokyo 170-8455, Japan
Shige-aki Kato
aInstitute of Molecular and Cellular Biosciences, University of Tokyo, Tokyo 113, Japan
fCREST, Japan Science and Technology Corporation, Saitama 332, Japan
Kyoji Ikeda
bDepartment of Geriatric Research, National Institute for Longevity Sciences, Obu, Aichi 474-8522, Japan
Makoto Nakanishi
bDepartment of Geriatric Research, National Institute for Longevity Sciences, Obu, Aichi 474-8522, Japan
dDepartment of Biochemistry, Nagoya City University Medical School, Nagoya 467-8601, Japan

Ayako Yamamoto and Yoshihiro Hashimoto contributed equally to this work.

Abbreviations used in this paper: AR, androgen receptor; ARE, androgen response element; CAT, chloramphenicol acetyltransferase; Cdk, cyclin-dependent kinase; DBD, DNA-binding domain; DHT, dihydrotestosterone; ERα, estrogen receptor α; GR, glucocorticoid receptor; GST, glutathione S-transferase; 5-OH-F, 5-hydroxyflutamide; PR, progesterone receptor; PSA, prostate-specific antigen.

Received: April 25 2000
Revision Requested: June 29 2000
Accepted: July 03 2000
Online ISSN: 1540-8140
Print ISSN: 0021-9525
© 2000 The Rockefeller University Press
2000
The Rockefeller University Press
J Cell Biol (2000) 150 (4): 873–880.
https://doi.org/10.1083/jcb.150.4.873
Article history
Received:
April 25 2000
Revision Requested:
June 29 2000
Accepted:
July 03 2000

Androgens play an important role in the growth of prostate cancer, but the molecular mechanism that underlies development of resistance to antiandrogen therapy remains unknown. Cyclin E has now been shown to increase the transactivation activity of the human androgen receptor (AR) in the presence of its ligand dihydrotestosterone. The enhancement of AR activity by cyclin E was resistant to inhibition by the antiandrogen 5-hydroxyflutamide. Cyclin E was shown to bind directly to the COOH terminus portion of the AB domain of the AR, and to enhance its AF-1 transactivation function. These results suggest that cyclin E functions as a coactivator of the AR, and that aberrant expression of cyclin E in tumors may contribute to persistent activation of AR function, even during androgen ablation therapy.

© 2000 The Rockefeller University Press
2000
The Rockefeller University Press
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