HOXA1 Is an Antagonist of ERα in Breast Cancer

Magali Belpaire; Bruno Ewbank; Arnaud Taminiau; Laure Bridoux; Noémie Deneyer; Damien Marchese; Gipsi Lima-Mendez; Jean François Baurain; Dirk Geerts; René Rezsohazy

doi:10.3389/fonc.2021.609521

HOXA1 Is an Antagonist of ERα in Breast Cancer

Magali Belpaire, Bruno Ewbank, Arnaud Taminiau, Laure Bridoux, Noémie Deneyer, Damien Marchese, Gipsi Lima-Mendez, Jean François Baurain, Dirk Geerts, René Rezsohazy

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Abstract

Breast cancer is a heterogeneous disease and the leading cause of female cancer mortality worldwide. About 70% of breast cancers express ERα. HOX proteins are master regulators of embryo development which have emerged as being important players in oncogenesis. HOXA1 is one of them. Here, we present bioinformatic analyses of genome-wide mRNA expression profiles available in large public datasets of human breast cancer samples. We reveal an extremely strong opposite correlation between HOXA1 versus ER expression and that of 2,486 genes, thereby supporting a functional antagonism between HOXA1 and ERα. We also demonstrate in vitro that HOXA1 can inhibit ERα activity. This inhibition is at least bimodal, requiring an intact HOXA1 DNA-binding homeodomain and involving the DNA-binding independent capacity of HOXA1 to activate NF-κB. We provide evidence that the HOXA1-PBX interaction known to be critical for the transcriptional activity of HOXA1 is not involved in the ERα inhibition. Finally, we reveal that HOXA1 and ERα can physically interact but that this interaction is not essential for the HOXA1-mediated inhibition of ERα. Like other HOX oncoproteins interacting with ERα, HOXA1 could be involved in endocrine therapy resistance.

Original language	English
Article number	609521
Journal	Frontiers in Oncology
Volume	11
DOIs	https://doi.org/10.3389/fonc.2021.609521
Publication status	Published - 18 Aug 2021
Externally published	Yes

Keywords

endocrine therapy resistance
estrogen receptor
HOX proteins
NF-κB
PBX

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.3389/fonc.2021.609521

fonc-11-609521Final published version, 7.93 MBLicence: CC BY

Cite this

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title = "HOXA1 Is an Antagonist of ERα in Breast Cancer",

abstract = "Breast cancer is a heterogeneous disease and the leading cause of female cancer mortality worldwide. About 70% of breast cancers express ERα. HOX proteins are master regulators of embryo development which have emerged as being important players in oncogenesis. HOXA1 is one of them. Here, we present bioinformatic analyses of genome-wide mRNA expression profiles available in large public datasets of human breast cancer samples. We reveal an extremely strong opposite correlation between HOXA1 versus ER expression and that of 2,486 genes, thereby supporting a functional antagonism between HOXA1 and ERα. We also demonstrate in vitro that HOXA1 can inhibit ERα activity. This inhibition is at least bimodal, requiring an intact HOXA1 DNA-binding homeodomain and involving the DNA-binding independent capacity of HOXA1 to activate NF-κB. We provide evidence that the HOXA1-PBX interaction known to be critical for the transcriptional activity of HOXA1 is not involved in the ERα inhibition. Finally, we reveal that HOXA1 and ERα can physically interact but that this interaction is not essential for the HOXA1-mediated inhibition of ERα. Like other HOX oncoproteins interacting with ERα, HOXA1 could be involved in endocrine therapy resistance.",

keywords = "endocrine therapy resistance, estrogen receptor, HOX proteins, NF-κB, PBX",

author = "Magali Belpaire and Bruno Ewbank and Arnaud Taminiau and Laure Bridoux and No{\'e}mie Deneyer and Damien Marchese and Gipsi Lima-Mendez and Baurain, {Jean Fran{\c c}ois} and Dirk Geerts and Ren{\'e} Rezsohazy",

note = "Funding Information: MB is a Fonds National de la Recherche Scientifique - FNRS - T{\'e}l{\'e}vie grant holder. This work was supported by the Fonds de la Recherche Scientifique -FNRS under Grants n°7.4555.16 and 7.6513.18 and the Fonds Sp{\'e}ciaux de Recherche from UCLouvain. Funding Information: We thank Han Weidong (Chinese PLA General Hospital, Beijing, China) for the pSG5-hER? expression vector and the 3xERE::luc-TATA reporter vector, Jean-Claude Twizere (Molecular Biology of Diseases, GIGA, ULi?ge, Belgium) for the pENTR-ESR1, and Sylvie Mader (Molecular Targeting in Breast Cancer Treatment Research Unit, Universit? de Montr?al, Montr?al, Canada) for the pGEX2TK-ESR1AB, pGEX2TK-ESR1CDEF, and pGEX2TK-ESR1EF. We also thank Catherine Rasse and Vincent Bremhost (SMCS, UCLouvain, Belgium) for the statistical analyses. Our gratitude goes to Jan Koster and Richard Volckmann for their help in working with the R2 genomics platform. The authors would like to thank Anneke Strietman for her courage and inspiration. Publisher Copyright: {\textcopyright} Copyright {\textcopyright} 2021 Belpaire, Ewbank, Taminiau, Bridoux, Deneyer, Marchese, Lima-Mendez, Baurain, Geerts and Rezsohazy.",

year = "2021",

month = aug,

day = "18",

doi = "10.3389/fonc.2021.609521",

language = "English",

volume = "11",

journal = "Frontiers in Oncology",

publisher = "Frontiers Research Foundation",

}

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T1 - HOXA1 Is an Antagonist of ERα in Breast Cancer

AU - Belpaire, Magali

AU - Ewbank, Bruno

AU - Taminiau, Arnaud

AU - Bridoux, Laure

AU - Deneyer, Noémie

AU - Marchese, Damien

AU - Lima-Mendez, Gipsi

AU - Baurain, Jean François

AU - Geerts, Dirk

AU - Rezsohazy, René

N1 - Funding Information: MB is a Fonds National de la Recherche Scientifique - FNRS - Télévie grant holder. This work was supported by the Fonds de la Recherche Scientifique -FNRS under Grants n°7.4555.16 and 7.6513.18 and the Fonds Spéciaux de Recherche from UCLouvain. Funding Information: We thank Han Weidong (Chinese PLA General Hospital, Beijing, China) for the pSG5-hER? expression vector and the 3xERE::luc-TATA reporter vector, Jean-Claude Twizere (Molecular Biology of Diseases, GIGA, ULi?ge, Belgium) for the pENTR-ESR1, and Sylvie Mader (Molecular Targeting in Breast Cancer Treatment Research Unit, Universit? de Montr?al, Montr?al, Canada) for the pGEX2TK-ESR1AB, pGEX2TK-ESR1CDEF, and pGEX2TK-ESR1EF. We also thank Catherine Rasse and Vincent Bremhost (SMCS, UCLouvain, Belgium) for the statistical analyses. Our gratitude goes to Jan Koster and Richard Volckmann for their help in working with the R2 genomics platform. The authors would like to thank Anneke Strietman for her courage and inspiration. Publisher Copyright: © Copyright © 2021 Belpaire, Ewbank, Taminiau, Bridoux, Deneyer, Marchese, Lima-Mendez, Baurain, Geerts and Rezsohazy.

PY - 2021/8/18

Y1 - 2021/8/18

N2 - Breast cancer is a heterogeneous disease and the leading cause of female cancer mortality worldwide. About 70% of breast cancers express ERα. HOX proteins are master regulators of embryo development which have emerged as being important players in oncogenesis. HOXA1 is one of them. Here, we present bioinformatic analyses of genome-wide mRNA expression profiles available in large public datasets of human breast cancer samples. We reveal an extremely strong opposite correlation between HOXA1 versus ER expression and that of 2,486 genes, thereby supporting a functional antagonism between HOXA1 and ERα. We also demonstrate in vitro that HOXA1 can inhibit ERα activity. This inhibition is at least bimodal, requiring an intact HOXA1 DNA-binding homeodomain and involving the DNA-binding independent capacity of HOXA1 to activate NF-κB. We provide evidence that the HOXA1-PBX interaction known to be critical for the transcriptional activity of HOXA1 is not involved in the ERα inhibition. Finally, we reveal that HOXA1 and ERα can physically interact but that this interaction is not essential for the HOXA1-mediated inhibition of ERα. Like other HOX oncoproteins interacting with ERα, HOXA1 could be involved in endocrine therapy resistance.

AB - Breast cancer is a heterogeneous disease and the leading cause of female cancer mortality worldwide. About 70% of breast cancers express ERα. HOX proteins are master regulators of embryo development which have emerged as being important players in oncogenesis. HOXA1 is one of them. Here, we present bioinformatic analyses of genome-wide mRNA expression profiles available in large public datasets of human breast cancer samples. We reveal an extremely strong opposite correlation between HOXA1 versus ER expression and that of 2,486 genes, thereby supporting a functional antagonism between HOXA1 and ERα. We also demonstrate in vitro that HOXA1 can inhibit ERα activity. This inhibition is at least bimodal, requiring an intact HOXA1 DNA-binding homeodomain and involving the DNA-binding independent capacity of HOXA1 to activate NF-κB. We provide evidence that the HOXA1-PBX interaction known to be critical for the transcriptional activity of HOXA1 is not involved in the ERα inhibition. Finally, we reveal that HOXA1 and ERα can physically interact but that this interaction is not essential for the HOXA1-mediated inhibition of ERα. Like other HOX oncoproteins interacting with ERα, HOXA1 could be involved in endocrine therapy resistance.

KW - endocrine therapy resistance

KW - estrogen receptor

KW - HOX proteins

KW - NF-κB

KW - PBX

UR - http://www.scopus.com/inward/record.url?scp=85114302109&partnerID=8YFLogxK

U2 - 10.3389/fonc.2021.609521

DO - 10.3389/fonc.2021.609521

M3 - Article

AN - SCOPUS:85114302109

VL - 11

JO - Frontiers in Oncology

JF - Frontiers in Oncology

M1 - 609521

ER -

HOXA1 Is an Antagonist of ERα in Breast Cancer

Abstract

Keywords

UN SDGs

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