Identification of an Imidazopyridine-based Compound as an Oral Selective Estrogen Receptor Degrader for Breast Cancer Therapy

The pro-oncogenic activities of estrogen receptor alpha (ERα) drive breast cancer pathogenesis. Endocrine therapies that impair the production of estrogen or the action of the ERα are therefore used to prevent primary disease metastasis. Although recent successes with ERα degraders have been reporte...

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Autores principales: Pan, Mengwu, Solozobova, Valeria, Kuznik, Nane C., Jung, Nicole, Gräßle, Simone, Gourain, Victor, Heneka, Yvonne M., Cramer von Clausbruch, Christina A., Fuhr, Olaf, Munuganti, Ravi S. N., Maddalo, Danilo, Blattner, Christine, Neeb, Antje, Sharp, Adam, Cato, Laura, Weiss, Carsten, Jeselsohn, Rinath M., Orian-Rousseau, Veronique, Bräse, Stefan, Cato, Andrew C. B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Association for Cancer Research 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10373600/
https://www.ncbi.nlm.nih.gov/pubmed/37520743
http://dx.doi.org/10.1158/2767-9764.CRC-23-0111
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author Pan, Mengwu
Solozobova, Valeria
Kuznik, Nane C.
Jung, Nicole
Gräßle, Simone
Gourain, Victor
Heneka, Yvonne M.
Cramer von Clausbruch, Christina A.
Fuhr, Olaf
Munuganti, Ravi S. N.
Maddalo, Danilo
Blattner, Christine
Neeb, Antje
Sharp, Adam
Cato, Laura
Weiss, Carsten
Jeselsohn, Rinath M.
Orian-Rousseau, Veronique
Bräse, Stefan
Cato, Andrew C. B.
author_facet Pan, Mengwu
Solozobova, Valeria
Kuznik, Nane C.
Jung, Nicole
Gräßle, Simone
Gourain, Victor
Heneka, Yvonne M.
Cramer von Clausbruch, Christina A.
Fuhr, Olaf
Munuganti, Ravi S. N.
Maddalo, Danilo
Blattner, Christine
Neeb, Antje
Sharp, Adam
Cato, Laura
Weiss, Carsten
Jeselsohn, Rinath M.
Orian-Rousseau, Veronique
Bräse, Stefan
Cato, Andrew C. B.
author_sort Pan, Mengwu
collection PubMed
description The pro-oncogenic activities of estrogen receptor alpha (ERα) drive breast cancer pathogenesis. Endocrine therapies that impair the production of estrogen or the action of the ERα are therefore used to prevent primary disease metastasis. Although recent successes with ERα degraders have been reported, there is still the need to develop further ERα antagonists with additional properties for breast cancer therapy. We have previously described a benzothiazole compound A4B17 that inhibits the proliferation of androgen receptor–positive prostate cancer cells by disrupting the interaction of the cochaperone BAG1 with the AR. A4B17 was also found to inhibit the proliferation of estrogen receptor—positive (ER(+)) breast cancer cells. Using a scaffold hopping approach, we report here a group of small molecules with imidazopyridine scaffolds that are more potent and efficacious than A4B17. The prototype molecule X15695 efficiently degraded ERα and attenuated estrogen-mediated target gene expression as well as transactivation by the AR. X15695 also disrupted key cellular protein–protein interactions such as BAG1–mortalin (GRP75) interaction as well as wild-type p53–mortalin or mutant p53–BAG2 interactions. These activities together reactivated p53 and resulted in cell-cycle block and the induction of apoptosis. When administered orally to in vivo tumor xenograft models, X15695 potently inhibited the growth of breast tumor cells but less efficiently the growth of prostate tumor cells. We therefore identify X15695 as an oral selective ER degrader and propose further development of this compound for therapy of ER(+) breast cancers. SIGNIFICANCE: An imidazopyridine that selectively degrades ERα and is orally bioavailable has been identified for the development of ER(+) breast cancer therapeutics. This compound also activates wild-type p53 and disrupts the gain-of-function tumorigenic activity of mutant p53, resulting in cell-cycle arrest and the induction of apoptosis.
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spelling pubmed-103736002023-07-28 Identification of an Imidazopyridine-based Compound as an Oral Selective Estrogen Receptor Degrader for Breast Cancer Therapy Pan, Mengwu Solozobova, Valeria Kuznik, Nane C. Jung, Nicole Gräßle, Simone Gourain, Victor Heneka, Yvonne M. Cramer von Clausbruch, Christina A. Fuhr, Olaf Munuganti, Ravi S. N. Maddalo, Danilo Blattner, Christine Neeb, Antje Sharp, Adam Cato, Laura Weiss, Carsten Jeselsohn, Rinath M. Orian-Rousseau, Veronique Bräse, Stefan Cato, Andrew C. B. Cancer Res Commun Research Article The pro-oncogenic activities of estrogen receptor alpha (ERα) drive breast cancer pathogenesis. Endocrine therapies that impair the production of estrogen or the action of the ERα are therefore used to prevent primary disease metastasis. Although recent successes with ERα degraders have been reported, there is still the need to develop further ERα antagonists with additional properties for breast cancer therapy. We have previously described a benzothiazole compound A4B17 that inhibits the proliferation of androgen receptor–positive prostate cancer cells by disrupting the interaction of the cochaperone BAG1 with the AR. A4B17 was also found to inhibit the proliferation of estrogen receptor—positive (ER(+)) breast cancer cells. Using a scaffold hopping approach, we report here a group of small molecules with imidazopyridine scaffolds that are more potent and efficacious than A4B17. The prototype molecule X15695 efficiently degraded ERα and attenuated estrogen-mediated target gene expression as well as transactivation by the AR. X15695 also disrupted key cellular protein–protein interactions such as BAG1–mortalin (GRP75) interaction as well as wild-type p53–mortalin or mutant p53–BAG2 interactions. These activities together reactivated p53 and resulted in cell-cycle block and the induction of apoptosis. When administered orally to in vivo tumor xenograft models, X15695 potently inhibited the growth of breast tumor cells but less efficiently the growth of prostate tumor cells. We therefore identify X15695 as an oral selective ER degrader and propose further development of this compound for therapy of ER(+) breast cancers. SIGNIFICANCE: An imidazopyridine that selectively degrades ERα and is orally bioavailable has been identified for the development of ER(+) breast cancer therapeutics. This compound also activates wild-type p53 and disrupts the gain-of-function tumorigenic activity of mutant p53, resulting in cell-cycle arrest and the induction of apoptosis. American Association for Cancer Research 2023-07-27 /pmc/articles/PMC10373600/ /pubmed/37520743 http://dx.doi.org/10.1158/2767-9764.CRC-23-0111 Text en © 2023 The Authors; Published by the American Association for Cancer Research https://creativecommons.org/licenses/by/4.0/This open access article is distributed under the Creative Commons Attribution 4.0 International (CC BY 4.0) license.
spellingShingle Research Article
Pan, Mengwu
Solozobova, Valeria
Kuznik, Nane C.
Jung, Nicole
Gräßle, Simone
Gourain, Victor
Heneka, Yvonne M.
Cramer von Clausbruch, Christina A.
Fuhr, Olaf
Munuganti, Ravi S. N.
Maddalo, Danilo
Blattner, Christine
Neeb, Antje
Sharp, Adam
Cato, Laura
Weiss, Carsten
Jeselsohn, Rinath M.
Orian-Rousseau, Veronique
Bräse, Stefan
Cato, Andrew C. B.
Identification of an Imidazopyridine-based Compound as an Oral Selective Estrogen Receptor Degrader for Breast Cancer Therapy
title Identification of an Imidazopyridine-based Compound as an Oral Selective Estrogen Receptor Degrader for Breast Cancer Therapy
title_full Identification of an Imidazopyridine-based Compound as an Oral Selective Estrogen Receptor Degrader for Breast Cancer Therapy
title_fullStr Identification of an Imidazopyridine-based Compound as an Oral Selective Estrogen Receptor Degrader for Breast Cancer Therapy
title_full_unstemmed Identification of an Imidazopyridine-based Compound as an Oral Selective Estrogen Receptor Degrader for Breast Cancer Therapy
title_short Identification of an Imidazopyridine-based Compound as an Oral Selective Estrogen Receptor Degrader for Breast Cancer Therapy
title_sort identification of an imidazopyridine-based compound as an oral selective estrogen receptor degrader for breast cancer therapy
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10373600/
https://www.ncbi.nlm.nih.gov/pubmed/37520743
http://dx.doi.org/10.1158/2767-9764.CRC-23-0111
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