Pharmacological inhibition of KDM1A/LSD1 enhances estrogen receptor beta-mediated tumor suppression in ovarian cancer

Pharmacological inhibition of KDM1A/LSD1 enhances estrogen receptor beta-mediated tumor suppression in ovarian cancer

Ovarian cancer (OCa) is the most lethal gynecologic cancer. Emerging data indicates that estrogen receptor beta (ERβ) functions as a tumor suppressor in OCa. Lysine-specific histone demethylase 1A (KDM1A) is an epigenetic modifier that acts as a coregulator for steroid hormone receptors. However, it...

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Veröffentlicht in:Cancer letters 2023-10, Vol.575, p.216383, Article 216383
Hauptverfasser: Venkata, Prabhakar Pitta, Jayamohan, Sridharan, He, Yi, Alejo, Salvador, Johnson, Jessica D., Palacios, Bridgitte E., Pratap, Uday P., Chen, Yihong, Liu, Zexuan, Zou, Yi, Lai, Zhao, Suzuki, Takayoshi, Viswanadhapalli, Suryavathi, Weintraub, Susan T., Palakurthi, Srinath, Valente, Philip T., Tekmal, Rajeshwar R., Kost, Edward R., Vadlamudi, Ratna K., Sareddy, Gangadhara R.
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Sprache:eng
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Cell Line, Tumor
Combination therapy
Estrogen receptor beta
Estrogen Receptor beta - genetics
Estrogen Receptor beta - metabolism
Estrogens
Female
Genes, Tumor Suppressor
Histone Demethylases
Humans
KDM1A
LSD1
Ovarian cancer
Ovarian Neoplasms - drug therapy
Ovarian Neoplasms - genetics
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container_end_page
container_issue
container_start_page 216383
container_title Cancer letters
container_volume 575
creator Venkata, Prabhakar Pitta
Jayamohan, Sridharan
He, Yi
Alejo, Salvador
Johnson, Jessica D.
Palacios, Bridgitte E.
Pratap, Uday P.
Chen, Yihong
Liu, Zexuan
Zou, Yi
Lai, Zhao
Suzuki, Takayoshi
Viswanadhapalli, Suryavathi
Weintraub, Susan T.
Palakurthi, Srinath
Valente, Philip T.
Tekmal, Rajeshwar R.
Kost, Edward R.
Vadlamudi, Ratna K.
Sareddy, Gangadhara R.
description Ovarian cancer (OCa) is the most lethal gynecologic cancer. Emerging data indicates that estrogen receptor beta (ERβ) functions as a tumor suppressor in OCa. Lysine-specific histone demethylase 1A (KDM1A) is an epigenetic modifier that acts as a coregulator for steroid hormone receptors. However, it remain unknown if KDM1A interacts with ERβ and regulates its expression/functions in OCa. Analysis of TCGA data sets indicated KDM1A and ERβ expression showed an inverse relationship in OCa. Knockout (KO), knockdown (KD), or inhibition of KDM1A increased ERβ isoform 1 expression in established and patient-derived OCa cells. Further, KDM1A interacts with and functions as a corepressor of ERβ, and its inhibition enhances ERβ target gene expression via alterations of histone methylation marks at their promoters. Importantly, KDM1A-KO or -KD enhanced the efficacy of ERβ agonist LY500307, and the combination of KDM1A inhibitor (KDM1Ai) NCD38 with ERβ agonist synergistically reduced the cell viability, colony formation, and invasion of OCa cells. RNA-seq and DIA mass spectrometry analyses showed that KDM1A-KO resulted in enhanced ERβ signaling and that genes altered by KDM1A-KO and ERβ agonist were related to apoptosis, cell cycle, and EMT. Moreover, combination treatment significantly reduced the tumor growth in OCa orthotopic, syngeneic, and patient-derived xenograft models and proliferation in patient-derived explant models. Our results demonstrate that KDM1A regulates ERβ expression/functions, and its inhibition improves ERβ mediated tumor suppression. Overall, our findings suggest that KDM1Ai and ERβ agonist combination therapy is a promising strategy for OCa. •KDM1A knockdown/inhibition increased tumor suppressor ERβ expression via alteration of histone methylation marks.•KDM1A interacts with, and functions as a corepressor of ERβ, and KDM1A knockout enhanced the ERβ agonist-mediated transcriptome.•KDM1A knockdown/inhibition and ERβ agonist combination treatment significantly reduced oncogenic functions of ovarian cancer cells.•KDM1A inhibitor and ERβ agonist combination significantly reduced ovarian tumor growth in mouse xenograft models.
doi_str_mv 10.1016/j.canlet.2023.216383
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Emerging data indicates that estrogen receptor beta (ERβ) functions as a tumor suppressor in OCa. Lysine-specific histone demethylase 1A (KDM1A) is an epigenetic modifier that acts as a coregulator for steroid hormone receptors. However, it remain unknown if KDM1A interacts with ERβ and regulates its expression/functions in OCa. Analysis of TCGA data sets indicated KDM1A and ERβ expression showed an inverse relationship in OCa. Knockout (KO), knockdown (KD), or inhibition of KDM1A increased ERβ isoform 1 expression in established and patient-derived OCa cells. Further, KDM1A interacts with and functions as a corepressor of ERβ, and its inhibition enhances ERβ target gene expression via alterations of histone methylation marks at their promoters. Importantly, KDM1A-KO or -KD enhanced the efficacy of ERβ agonist LY500307, and the combination of KDM1A inhibitor (KDM1Ai) NCD38 with ERβ agonist synergistically reduced the cell viability, colony formation, and invasion of OCa cells. RNA-seq and DIA mass spectrometry analyses showed that KDM1A-KO resulted in enhanced ERβ signaling and that genes altered by KDM1A-KO and ERβ agonist were related to apoptosis, cell cycle, and EMT. Moreover, combination treatment significantly reduced the tumor growth in OCa orthotopic, syngeneic, and patient-derived xenograft models and proliferation in patient-derived explant models. Our results demonstrate that KDM1A regulates ERβ expression/functions, and its inhibition improves ERβ mediated tumor suppression. Overall, our findings suggest that KDM1Ai and ERβ agonist combination therapy is a promising strategy for OCa. •KDM1A knockdown/inhibition increased tumor suppressor ERβ expression via alteration of histone methylation marks.•KDM1A interacts with, and functions as a corepressor of ERβ, and KDM1A knockout enhanced the ERβ agonist-mediated transcriptome.•KDM1A knockdown/inhibition and ERβ agonist combination treatment significantly reduced oncogenic functions of ovarian cancer cells.•KDM1A inhibitor and ERβ agonist combination significantly reduced ovarian tumor growth in mouse xenograft models.</description><identifier>ISSN: 0304-3835</identifier><identifier>ISSN: 1872-7980</identifier><identifier>EISSN: 1872-7980</identifier><identifier>DOI: 10.1016/j.canlet.2023.216383</identifier><identifier>PMID: 37714256</identifier><language>eng</language><publisher>Ireland: Elsevier B.V</publisher><subject>Cell Line, Tumor ; Combination therapy ; Estrogen receptor beta ; Estrogen Receptor beta - genetics ; Estrogen Receptor beta - metabolism ; Estrogens ; Female ; Genes, Tumor Suppressor ; Histone Demethylases ; Humans ; KDM1A ; LSD1 ; Ovarian cancer ; Ovarian Neoplasms - drug therapy ; Ovarian Neoplasms - genetics</subject><ispartof>Cancer letters, 2023-10, Vol.575, p.216383, Article 216383</ispartof><rights>2023 Elsevier B.V.</rights><rights>Copyright © 2023 Elsevier B.V. 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Emerging data indicates that estrogen receptor beta (ERβ) functions as a tumor suppressor in OCa. Lysine-specific histone demethylase 1A (KDM1A) is an epigenetic modifier that acts as a coregulator for steroid hormone receptors. However, it remain unknown if KDM1A interacts with ERβ and regulates its expression/functions in OCa. Analysis of TCGA data sets indicated KDM1A and ERβ expression showed an inverse relationship in OCa. Knockout (KO), knockdown (KD), or inhibition of KDM1A increased ERβ isoform 1 expression in established and patient-derived OCa cells. Further, KDM1A interacts with and functions as a corepressor of ERβ, and its inhibition enhances ERβ target gene expression via alterations of histone methylation marks at their promoters. Importantly, KDM1A-KO or -KD enhanced the efficacy of ERβ agonist LY500307, and the combination of KDM1A inhibitor (KDM1Ai) NCD38 with ERβ agonist synergistically reduced the cell viability, colony formation, and invasion of OCa cells. RNA-seq and DIA mass spectrometry analyses showed that KDM1A-KO resulted in enhanced ERβ signaling and that genes altered by KDM1A-KO and ERβ agonist were related to apoptosis, cell cycle, and EMT. Moreover, combination treatment significantly reduced the tumor growth in OCa orthotopic, syngeneic, and patient-derived xenograft models and proliferation in patient-derived explant models. Our results demonstrate that KDM1A regulates ERβ expression/functions, and its inhibition improves ERβ mediated tumor suppression. Overall, our findings suggest that KDM1Ai and ERβ agonist combination therapy is a promising strategy for OCa. •KDM1A knockdown/inhibition increased tumor suppressor ERβ expression via alteration of histone methylation marks.•KDM1A interacts with, and functions as a corepressor of ERβ, and KDM1A knockout enhanced the ERβ agonist-mediated transcriptome.•KDM1A knockdown/inhibition and ERβ agonist combination treatment significantly reduced oncogenic functions of ovarian cancer cells.•KDM1A inhibitor and ERβ agonist combination significantly reduced ovarian tumor growth in mouse xenograft models.</description><subject>Cell Line, Tumor</subject><subject>Combination therapy</subject><subject>Estrogen receptor beta</subject><subject>Estrogen Receptor beta - genetics</subject><subject>Estrogen Receptor beta - metabolism</subject><subject>Estrogens</subject><subject>Female</subject><subject>Genes, Tumor Suppressor</subject><subject>Histone Demethylases</subject><subject>Humans</subject><subject>KDM1A</subject><subject>LSD1</subject><subject>Ovarian cancer</subject><subject>Ovarian Neoplasms - drug therapy</subject><subject>Ovarian Neoplasms - genetics</subject><issn>0304-3835</issn><issn>1872-7980</issn><issn>1872-7980</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2023</creationdate><recordtype>article</recordtype><sourceid>EIF</sourceid><recordid>eNp9kEtv1TAQhS0EopfCP0DISza59SNOnA1S1ZaHehFItGtr4kx6fZXEwXYq8e9xlMKyq5GOzjkz8xHynrM9Z7y6OO0tTAOmvWBC7gWvpJYvyI7rWhR1o9lLsmOSlUWW1Rl5E-OJMabKWr0mZ7KueSlUtSPLzyOEEawf_IOzMFA3HV3rkvMT9T29vf7OLy8Ov645xekIk8VIMabgH3CiAS3OyQfaYoJixM5Bwo6mZcxaXOY5YIxrkctdjxAcTNSuHeEtedXDEPHd0zwn959v7q6-FocfX75dXR4KWzKdCmg6oTXYxgJWkoMWsu6hktB1ZVtD20IpwAJTLWurvmk4V31ZlaittVwqJc_Jx613Dv73kg83o4sWhwEm9Es0Qleq1iuhbC03qw0-xoC9mYMbIfwxnJkVuDmZDbhZgZsNeI59eNqwtJnA_9A_wtnwaTNg_vPRYTDROswQOpf5JdN59_yGv24YlWA</recordid><startdate>20231028</startdate><enddate>20231028</enddate><creator>Venkata, Prabhakar Pitta</creator><creator>Jayamohan, Sridharan</creator><creator>He, Yi</creator><creator>Alejo, Salvador</creator><creator>Johnson, Jessica D.</creator><creator>Palacios, Bridgitte E.</creator><creator>Pratap, Uday P.</creator><creator>Chen, Yihong</creator><creator>Liu, Zexuan</creator><creator>Zou, Yi</creator><creator>Lai, Zhao</creator><creator>Suzuki, Takayoshi</creator><creator>Viswanadhapalli, Suryavathi</creator><creator>Weintraub, Susan T.</creator><creator>Palakurthi, Srinath</creator><creator>Valente, Philip T.</creator><creator>Tekmal, Rajeshwar R.</creator><creator>Kost, Edward R.</creator><creator>Vadlamudi, Ratna K.</creator><creator>Sareddy, Gangadhara R.</creator><general>Elsevier B.V</general><scope>CGR</scope><scope>CUY</scope><scope>CVF</scope><scope>ECM</scope><scope>EIF</scope><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><scope>7X8</scope><orcidid>https://orcid.org/0000-0001-9977-3932</orcidid><orcidid>https://orcid.org/0000-0002-8430-0881</orcidid><orcidid>https://orcid.org/0000-0002-1475-2217</orcidid></search><sort><creationdate>20231028</creationdate><title>Pharmacological inhibition of KDM1A/LSD1 enhances estrogen receptor beta-mediated tumor suppression in ovarian cancer</title><author>Venkata, Prabhakar Pitta ; 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Emerging data indicates that estrogen receptor beta (ERβ) functions as a tumor suppressor in OCa. Lysine-specific histone demethylase 1A (KDM1A) is an epigenetic modifier that acts as a coregulator for steroid hormone receptors. However, it remain unknown if KDM1A interacts with ERβ and regulates its expression/functions in OCa. Analysis of TCGA data sets indicated KDM1A and ERβ expression showed an inverse relationship in OCa. Knockout (KO), knockdown (KD), or inhibition of KDM1A increased ERβ isoform 1 expression in established and patient-derived OCa cells. Further, KDM1A interacts with and functions as a corepressor of ERβ, and its inhibition enhances ERβ target gene expression via alterations of histone methylation marks at their promoters. Importantly, KDM1A-KO or -KD enhanced the efficacy of ERβ agonist LY500307, and the combination of KDM1A inhibitor (KDM1Ai) NCD38 with ERβ agonist synergistically reduced the cell viability, colony formation, and invasion of OCa cells. RNA-seq and DIA mass spectrometry analyses showed that KDM1A-KO resulted in enhanced ERβ signaling and that genes altered by KDM1A-KO and ERβ agonist were related to apoptosis, cell cycle, and EMT. Moreover, combination treatment significantly reduced the tumor growth in OCa orthotopic, syngeneic, and patient-derived xenograft models and proliferation in patient-derived explant models. Our results demonstrate that KDM1A regulates ERβ expression/functions, and its inhibition improves ERβ mediated tumor suppression. Overall, our findings suggest that KDM1Ai and ERβ agonist combination therapy is a promising strategy for OCa. •KDM1A knockdown/inhibition increased tumor suppressor ERβ expression via alteration of histone methylation marks.•KDM1A interacts with, and functions as a corepressor of ERβ, and KDM1A knockout enhanced the ERβ agonist-mediated transcriptome.•KDM1A knockdown/inhibition and ERβ agonist combination treatment significantly reduced oncogenic functions of ovarian cancer cells.•KDM1A inhibitor and ERβ agonist combination significantly reduced ovarian tumor growth in mouse xenograft models.</abstract><cop>Ireland</cop><pub>Elsevier B.V</pub><pmid>37714256</pmid><doi>10.1016/j.canlet.2023.216383</doi><orcidid>https://orcid.org/0000-0001-9977-3932</orcidid><orcidid>https://orcid.org/0000-0002-8430-0881</orcidid><orcidid>https://orcid.org/0000-0002-1475-2217</orcidid><oa>free_for_read</oa></addata></record>
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subjects Cell Line, Tumor
Combination therapy
Estrogen receptor beta
Estrogen Receptor beta - genetics
Estrogen Receptor beta - metabolism
Estrogens
Female
Genes, Tumor Suppressor
Histone Demethylases
Humans
KDM1A
LSD1
Ovarian cancer
Ovarian Neoplasms - drug therapy
Ovarian Neoplasms - genetics
title Pharmacological inhibition of KDM1A/LSD1 enhances estrogen receptor beta-mediated tumor suppression in ovarian cancer
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