Increasing the number of tandem estrogen response elements increases the estrogenic activity of a tamoxifen analogue

W. H. Catherino; V. C. Jordan

doi:10.1016/0304-3835(95)03755-L

Increasing the number of tandem estrogen response elements increases the estrogenic activity of a tamoxifen analogue

W. H. Catherino, V. C. Jordan

Research output: Contribution to journal › Article › peer-review

68 Scopus citations

Abstract

There have been several reports of women who have tumor relapse while on tamoxifen therapy, followed by tumor regression after tamoxifen withdrawal. In such apparently tamoxifen-stimulated tumors, there is likely a genetic change which increases the estrogenicity of tamoxifen. In this study, we determine if increasing the number of estrogen response elements (EREs) in the promotor region of a reporter gene can alter the agonistic activity of fixed-ring 4-hydroxytamoxifen. We show that increasing the number of EREs in the promotor region increases the transcriptional response of the reporter plasmid to estradiol. We also find that while fixed-ring 4-hydroxytamoxifen is unable to stimulate transcription when one ERE is present, transcriptional activation can occur with multiple EREs. These results demonstrate that ERE amplification could explain the agonistic properties of tamoxifen, and suggests a novel mechanism to explain tamoxifen-stimulated breast cancer growth.

Original language	English (US)
Pages (from-to)	39-47
Number of pages	9
Journal	Cancer Letters
Volume	92
Issue number	1
DOIs	https://doi.org/10.1016/0304-3835(95)03755-L
State	Published - May 25 1995
Externally published	Yes

Keywords

Breast cancer
Estradiol
Estrogen response element
Tamoxifen
Transfection

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1016/0304-3835(95)03755-L

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title = "Increasing the number of tandem estrogen response elements increases the estrogenic activity of a tamoxifen analogue",

abstract = "There have been several reports of women who have tumor relapse while on tamoxifen therapy, followed by tumor regression after tamoxifen withdrawal. In such apparently tamoxifen-stimulated tumors, there is likely a genetic change which increases the estrogenicity of tamoxifen. In this study, we determine if increasing the number of estrogen response elements (EREs) in the promotor region of a reporter gene can alter the agonistic activity of fixed-ring 4-hydroxytamoxifen. We show that increasing the number of EREs in the promotor region increases the transcriptional response of the reporter plasmid to estradiol. We also find that while fixed-ring 4-hydroxytamoxifen is unable to stimulate transcription when one ERE is present, transcriptional activation can occur with multiple EREs. These results demonstrate that ERE amplification could explain the agonistic properties of tamoxifen, and suggests a novel mechanism to explain tamoxifen-stimulated breast cancer growth.",

keywords = "Breast cancer, Estradiol, Estrogen response element, Tamoxifen, Transfection",

author = "Catherino, {W. H.} and Jordan, {V. C.}",

note = "Funding Information: Special thanks for the technical support of J. Holsen and M. Bong. We also thank Dr. Raymond McCague for providing us with fixed-ring 4-hydroxytamoxifen, and Dr. Alan Wakeling for providing us with ICI 182 780. These studies were supported by Public Health Service grant CA-56143, the Commonwealth Foundation of the National Medical Fellowships, and the M.D./{\textquoteright} Ph.D. integrated degree program at the University of Wisconsin-Madison.",

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doi = "10.1016/0304-3835(95)03755-L",

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AU - Catherino, W. H.

AU - Jordan, V. C.

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PY - 1995/5/25

Y1 - 1995/5/25

N2 - There have been several reports of women who have tumor relapse while on tamoxifen therapy, followed by tumor regression after tamoxifen withdrawal. In such apparently tamoxifen-stimulated tumors, there is likely a genetic change which increases the estrogenicity of tamoxifen. In this study, we determine if increasing the number of estrogen response elements (EREs) in the promotor region of a reporter gene can alter the agonistic activity of fixed-ring 4-hydroxytamoxifen. We show that increasing the number of EREs in the promotor region increases the transcriptional response of the reporter plasmid to estradiol. We also find that while fixed-ring 4-hydroxytamoxifen is unable to stimulate transcription when one ERE is present, transcriptional activation can occur with multiple EREs. These results demonstrate that ERE amplification could explain the agonistic properties of tamoxifen, and suggests a novel mechanism to explain tamoxifen-stimulated breast cancer growth.

AB - There have been several reports of women who have tumor relapse while on tamoxifen therapy, followed by tumor regression after tamoxifen withdrawal. In such apparently tamoxifen-stimulated tumors, there is likely a genetic change which increases the estrogenicity of tamoxifen. In this study, we determine if increasing the number of estrogen response elements (EREs) in the promotor region of a reporter gene can alter the agonistic activity of fixed-ring 4-hydroxytamoxifen. We show that increasing the number of EREs in the promotor region increases the transcriptional response of the reporter plasmid to estradiol. We also find that while fixed-ring 4-hydroxytamoxifen is unable to stimulate transcription when one ERE is present, transcriptional activation can occur with multiple EREs. These results demonstrate that ERE amplification could explain the agonistic properties of tamoxifen, and suggests a novel mechanism to explain tamoxifen-stimulated breast cancer growth.

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KW - Transfection

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Increasing the number of tandem estrogen response elements increases the estrogenic activity of a tamoxifen analogue

Abstract

Keywords

ASJC Scopus subject areas

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