Neoadjuvant tamoxifen synchronizes ERα binding and gene expression profiles related to outcome and proliferation

Tesa M. Severson; Ekaterina Nevedomskaya; Justine Peeters; Thomas Kuilman; Oscar Krijgsman; Annelot Van Rossum; Marjolein Droog; Yongsoo Kim; Rutger Koornstra; Inès Beumer; Annuska M. Glas; Daniel Peeper; Jelle Wesseling; Iris M. Simon; Lodewyk Wessels; Sabine C. Linn; Wilbert Zwart

doi:10.18632/oncotarget.8983

Neoadjuvant tamoxifen synchronizes ERα binding and gene expression profiles related to outcome and proliferation

Tesa M. Severson, Ekaterina Nevedomskaya, Justine Peeters, Thomas Kuilman, Oscar Krijgsman, Annelot Van Rossum, Marjolein Droog, Yongsoo Kim, Rutger Koornstra, Inès Beumer, Annuska M. Glas, Daniel Peeper, Jelle Wesseling, Iris M. Simon, Lodewyk Wessels, Sabine C. Linn, Wilbert Zwart^*

^*Corresponding author for this work

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Abstract

Estrogen receptor alpha (ERα)-positive breast cancers are frequently treated with tamoxifen, but resistance is common. It remains elusive how tamoxifen resistance occurs and predictive biomarkers for treatment outcome are needed. Because most biomarker discovery studies are performed using pre-treatment surgical resections, the effects of tamoxifen therapy directly on the tumor cell in vivo remain unexamined. In this study, we assessed DNA copy number, gene expression profiles and ERα/chromatin binding landscapes on breast tumor specimens, both before and after neoadjuvant tamoxifen treatment. We observed neoadjuvant tamoxifen treatment synchronized ERα/chromatin interactions and downstream gene expression, indicating that hormonal therapy reduces inter-tumor molecular variability. ERα-synchronized sites are associated with dynamic FOXA1 action at these sites, which is under control of growth factor signaling. Genes associated with tamoxifen-synchronized sites are capable of differentiating patients for tamoxifen benefit. Due to the direct effects of therapeutics on ERα behavior and transcriptional output, our study highlights the added value of biomarker discovery studies after neoadjuvant drug exposure.

Original language	English
Pages (from-to)	33901-33918
Number of pages	18
Journal	Oncotarget
Volume	7
Issue number	23
DOIs	https://doi.org/10.18632/oncotarget.8983
Publication status	Published - 7 Jun 2016

Keywords

ChIP-seq
Endocrine therapy
Estrogen receptor
Gene expression analysis
Neoadjuvant therapy

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Severson, T. M., Nevedomskaya, E., Peeters, J., Kuilman, T., Krijgsman, O., Van Rossum, A., Droog, M., Kim, Y., Koornstra, R., Beumer, I., Glas, A. M., Peeper, D., Wesseling, J., Simon, I. M., Wessels, L., Linn, S. C., & Zwart, W. (2016). Neoadjuvant tamoxifen synchronizes ERα binding and gene expression profiles related to outcome and proliferation. Oncotarget, 7(23), 33901-33918. https://doi.org/10.18632/oncotarget.8983

@article{c083a39404284f60af042d1d222754ef,

title = "Neoadjuvant tamoxifen synchronizes ERα binding and gene expression profiles related to outcome and proliferation",

abstract = "Estrogen receptor alpha (ERα)-positive breast cancers are frequently treated with tamoxifen, but resistance is common. It remains elusive how tamoxifen resistance occurs and predictive biomarkers for treatment outcome are needed. Because most biomarker discovery studies are performed using pre-treatment surgical resections, the effects of tamoxifen therapy directly on the tumor cell in vivo remain unexamined. In this study, we assessed DNA copy number, gene expression profiles and ERα/chromatin binding landscapes on breast tumor specimens, both before and after neoadjuvant tamoxifen treatment. We observed neoadjuvant tamoxifen treatment synchronized ERα/chromatin interactions and downstream gene expression, indicating that hormonal therapy reduces inter-tumor molecular variability. ERα-synchronized sites are associated with dynamic FOXA1 action at these sites, which is under control of growth factor signaling. Genes associated with tamoxifen-synchronized sites are capable of differentiating patients for tamoxifen benefit. Due to the direct effects of therapeutics on ERα behavior and transcriptional output, our study highlights the added value of biomarker discovery studies after neoadjuvant drug exposure.",

keywords = "ChIP-seq, Endocrine therapy, Estrogen receptor, Gene expression analysis, Neoadjuvant therapy",

author = "Severson, {Tesa M.} and Ekaterina Nevedomskaya and Justine Peeters and Thomas Kuilman and Oscar Krijgsman and {Van Rossum}, Annelot and Marjolein Droog and Yongsoo Kim and Rutger Koornstra and In{\`e}s Beumer and Glas, {Annuska M.} and Daniel Peeper and Jelle Wesseling and Simon, {Iris M.} and Lodewyk Wessels and Linn, {Sabine C.} and Wilbert Zwart",

year = "2016",

month = jun,

day = "7",

doi = "10.18632/oncotarget.8983",

language = "English",

volume = "7",

pages = "33901--33918",

journal = "Oncotarget",

issn = "1949-2553",

publisher = "Impact Journals",

number = "23",

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Severson, TM, Nevedomskaya, E, Peeters, J, Kuilman, T, Krijgsman, O, Van Rossum, A, Droog, M, Kim, Y, Koornstra, R, Beumer, I, Glas, AM, Peeper, D, Wesseling, J, Simon, IM, Wessels, L, Linn, SC & Zwart, W 2016, 'Neoadjuvant tamoxifen synchronizes ERα binding and gene expression profiles related to outcome and proliferation', Oncotarget, vol. 7, no. 23, pp. 33901-33918. https://doi.org/10.18632/oncotarget.8983

TY - JOUR

T1 - Neoadjuvant tamoxifen synchronizes ERα binding and gene expression profiles related to outcome and proliferation

AU - Severson, Tesa M.

AU - Nevedomskaya, Ekaterina

AU - Peeters, Justine

AU - Kuilman, Thomas

AU - Krijgsman, Oscar

AU - Van Rossum, Annelot

AU - Droog, Marjolein

AU - Kim, Yongsoo

AU - Koornstra, Rutger

AU - Beumer, Inès

AU - Glas, Annuska M.

AU - Peeper, Daniel

AU - Wesseling, Jelle

AU - Simon, Iris M.

AU - Wessels, Lodewyk

AU - Linn, Sabine C.

AU - Zwart, Wilbert

PY - 2016/6/7

Y1 - 2016/6/7

N2 - Estrogen receptor alpha (ERα)-positive breast cancers are frequently treated with tamoxifen, but resistance is common. It remains elusive how tamoxifen resistance occurs and predictive biomarkers for treatment outcome are needed. Because most biomarker discovery studies are performed using pre-treatment surgical resections, the effects of tamoxifen therapy directly on the tumor cell in vivo remain unexamined. In this study, we assessed DNA copy number, gene expression profiles and ERα/chromatin binding landscapes on breast tumor specimens, both before and after neoadjuvant tamoxifen treatment. We observed neoadjuvant tamoxifen treatment synchronized ERα/chromatin interactions and downstream gene expression, indicating that hormonal therapy reduces inter-tumor molecular variability. ERα-synchronized sites are associated with dynamic FOXA1 action at these sites, which is under control of growth factor signaling. Genes associated with tamoxifen-synchronized sites are capable of differentiating patients for tamoxifen benefit. Due to the direct effects of therapeutics on ERα behavior and transcriptional output, our study highlights the added value of biomarker discovery studies after neoadjuvant drug exposure.

AB - Estrogen receptor alpha (ERα)-positive breast cancers are frequently treated with tamoxifen, but resistance is common. It remains elusive how tamoxifen resistance occurs and predictive biomarkers for treatment outcome are needed. Because most biomarker discovery studies are performed using pre-treatment surgical resections, the effects of tamoxifen therapy directly on the tumor cell in vivo remain unexamined. In this study, we assessed DNA copy number, gene expression profiles and ERα/chromatin binding landscapes on breast tumor specimens, both before and after neoadjuvant tamoxifen treatment. We observed neoadjuvant tamoxifen treatment synchronized ERα/chromatin interactions and downstream gene expression, indicating that hormonal therapy reduces inter-tumor molecular variability. ERα-synchronized sites are associated with dynamic FOXA1 action at these sites, which is under control of growth factor signaling. Genes associated with tamoxifen-synchronized sites are capable of differentiating patients for tamoxifen benefit. Due to the direct effects of therapeutics on ERα behavior and transcriptional output, our study highlights the added value of biomarker discovery studies after neoadjuvant drug exposure.

KW - ChIP-seq

KW - Endocrine therapy

KW - Estrogen receptor

KW - Gene expression analysis

KW - Neoadjuvant therapy

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U2 - 10.18632/oncotarget.8983

DO - 10.18632/oncotarget.8983

M3 - Article

C2 - 27129152

AN - SCOPUS:84973596133

SN - 1949-2553

VL - 7

SP - 33901

EP - 33918

JO - Oncotarget

JF - Oncotarget

IS - 23

ER -

Neoadjuvant tamoxifen synchronizes ERα binding and gene expression profiles related to outcome and proliferation

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