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The selective estrogen receptor downregulator GDC-0810 is efficacious in diverse models of ER+ breast cancer

ER-targeted therapeutics provide valuable treatment options for patients with ER+ breast cancer, however, current relapse and mortality rates emphasize the need for improved therapeutic strategies. The recent discovery of prevalent ESR1 mutations in relapsed tumors underscores a sustained reliance o...

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Autores principales: Joseph, James D, Darimont, Beatrice, Zhou, Wei, Arrazate, Alfonso, Young, Amy, Ingalla, Ellen, Walter, Kimberly, Blake, Robert A, Nonomiya, Jim, Guan, Zhengyu, Kategaya, Lorna, Govek, Steven P, Lai, Andiliy G, Kahraman, Mehmet, Brigham, Dan, Sensintaffar, John, Lu, Nhin, Shao, Gang, Qian, Jing, Grillot, Kate, Moon, Michael, Prudente, Rene, Bischoff, Eric, Lee, Kyoung-Jin, Bonnefous, Celine, Douglas, Karensa L, Julien, Jackaline D, Nagasawa, Johnny Y, Aparicio, Anna, Kaufman, Josh, Haley, Benjamin, Giltnane, Jennifer M, Wertz, Ingrid E, Lackner, Mark R, Nannini, Michelle A, Sampath, Deepak, Schwarz, Luis, Manning, Henry Charles, Tantawy, Mohammed Noor, Arteaga, Carlos L, Heyman, Richard A, Rix, Peter J, Friedman, Lori, Smith, Nicholas D, Metcalfe, Ciara, Hager, Jeffrey H
Formato: Online Artículo Texto
Lenguaje:English
Publicado: eLife Sciences Publications, Ltd 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4961458/
https://www.ncbi.nlm.nih.gov/pubmed/27410477
http://dx.doi.org/10.7554/eLife.15828
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author Joseph, James D
Darimont, Beatrice
Zhou, Wei
Arrazate, Alfonso
Young, Amy
Ingalla, Ellen
Walter, Kimberly
Blake, Robert A
Nonomiya, Jim
Guan, Zhengyu
Kategaya, Lorna
Govek, Steven P
Lai, Andiliy G
Kahraman, Mehmet
Brigham, Dan
Sensintaffar, John
Lu, Nhin
Shao, Gang
Qian, Jing
Grillot, Kate
Moon, Michael
Prudente, Rene
Bischoff, Eric
Lee, Kyoung-Jin
Bonnefous, Celine
Douglas, Karensa L
Julien, Jackaline D
Nagasawa, Johnny Y
Aparicio, Anna
Kaufman, Josh
Haley, Benjamin
Giltnane, Jennifer M
Wertz, Ingrid E
Lackner, Mark R
Nannini, Michelle A
Sampath, Deepak
Schwarz, Luis
Manning, Henry Charles
Tantawy, Mohammed Noor
Arteaga, Carlos L
Heyman, Richard A
Rix, Peter J
Friedman, Lori
Smith, Nicholas D
Metcalfe, Ciara
Hager, Jeffrey H
author_facet Joseph, James D
Darimont, Beatrice
Zhou, Wei
Arrazate, Alfonso
Young, Amy
Ingalla, Ellen
Walter, Kimberly
Blake, Robert A
Nonomiya, Jim
Guan, Zhengyu
Kategaya, Lorna
Govek, Steven P
Lai, Andiliy G
Kahraman, Mehmet
Brigham, Dan
Sensintaffar, John
Lu, Nhin
Shao, Gang
Qian, Jing
Grillot, Kate
Moon, Michael
Prudente, Rene
Bischoff, Eric
Lee, Kyoung-Jin
Bonnefous, Celine
Douglas, Karensa L
Julien, Jackaline D
Nagasawa, Johnny Y
Aparicio, Anna
Kaufman, Josh
Haley, Benjamin
Giltnane, Jennifer M
Wertz, Ingrid E
Lackner, Mark R
Nannini, Michelle A
Sampath, Deepak
Schwarz, Luis
Manning, Henry Charles
Tantawy, Mohammed Noor
Arteaga, Carlos L
Heyman, Richard A
Rix, Peter J
Friedman, Lori
Smith, Nicholas D
Metcalfe, Ciara
Hager, Jeffrey H
author_sort Joseph, James D
collection PubMed
description ER-targeted therapeutics provide valuable treatment options for patients with ER+ breast cancer, however, current relapse and mortality rates emphasize the need for improved therapeutic strategies. The recent discovery of prevalent ESR1 mutations in relapsed tumors underscores a sustained reliance of advanced tumors on ERα signaling, and provides a strong rationale for continued targeting of ERα. Here we describe GDC-0810, a novel, non-steroidal, orally bioavailable selective ER downregulator (SERD), which was identified by prospectively optimizing ERα degradation, antagonism and pharmacokinetic properties. GDC-0810 induces a distinct ERα conformation, relative to that induced by currently approved therapeutics, suggesting a unique mechanism of action. GDC-0810 has robust in vitro and in vivo activity against a variety of human breast cancer cell lines and patient derived xenografts, including a tamoxifen-resistant model and those that harbor ERα mutations. GDC-0810 is currently being evaluated in Phase II clinical studies in women with ER+ breast cancer.
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spelling pubmed-49614582016-07-28 The selective estrogen receptor downregulator GDC-0810 is efficacious in diverse models of ER+ breast cancer Joseph, James D Darimont, Beatrice Zhou, Wei Arrazate, Alfonso Young, Amy Ingalla, Ellen Walter, Kimberly Blake, Robert A Nonomiya, Jim Guan, Zhengyu Kategaya, Lorna Govek, Steven P Lai, Andiliy G Kahraman, Mehmet Brigham, Dan Sensintaffar, John Lu, Nhin Shao, Gang Qian, Jing Grillot, Kate Moon, Michael Prudente, Rene Bischoff, Eric Lee, Kyoung-Jin Bonnefous, Celine Douglas, Karensa L Julien, Jackaline D Nagasawa, Johnny Y Aparicio, Anna Kaufman, Josh Haley, Benjamin Giltnane, Jennifer M Wertz, Ingrid E Lackner, Mark R Nannini, Michelle A Sampath, Deepak Schwarz, Luis Manning, Henry Charles Tantawy, Mohammed Noor Arteaga, Carlos L Heyman, Richard A Rix, Peter J Friedman, Lori Smith, Nicholas D Metcalfe, Ciara Hager, Jeffrey H eLife Cancer Biology ER-targeted therapeutics provide valuable treatment options for patients with ER+ breast cancer, however, current relapse and mortality rates emphasize the need for improved therapeutic strategies. The recent discovery of prevalent ESR1 mutations in relapsed tumors underscores a sustained reliance of advanced tumors on ERα signaling, and provides a strong rationale for continued targeting of ERα. Here we describe GDC-0810, a novel, non-steroidal, orally bioavailable selective ER downregulator (SERD), which was identified by prospectively optimizing ERα degradation, antagonism and pharmacokinetic properties. GDC-0810 induces a distinct ERα conformation, relative to that induced by currently approved therapeutics, suggesting a unique mechanism of action. GDC-0810 has robust in vitro and in vivo activity against a variety of human breast cancer cell lines and patient derived xenografts, including a tamoxifen-resistant model and those that harbor ERα mutations. GDC-0810 is currently being evaluated in Phase II clinical studies in women with ER+ breast cancer. eLife Sciences Publications, Ltd 2016-07-13 /pmc/articles/PMC4961458/ /pubmed/27410477 http://dx.doi.org/10.7554/eLife.15828 Text en © 2016, Joseph et al http://creativecommons.org/licenses/by/4.0/ http://creativecommons.org/licenses/by/4.0/This article is distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use and redistribution provided that the original author and source are credited.
spellingShingle Cancer Biology
Joseph, James D
Darimont, Beatrice
Zhou, Wei
Arrazate, Alfonso
Young, Amy
Ingalla, Ellen
Walter, Kimberly
Blake, Robert A
Nonomiya, Jim
Guan, Zhengyu
Kategaya, Lorna
Govek, Steven P
Lai, Andiliy G
Kahraman, Mehmet
Brigham, Dan
Sensintaffar, John
Lu, Nhin
Shao, Gang
Qian, Jing
Grillot, Kate
Moon, Michael
Prudente, Rene
Bischoff, Eric
Lee, Kyoung-Jin
Bonnefous, Celine
Douglas, Karensa L
Julien, Jackaline D
Nagasawa, Johnny Y
Aparicio, Anna
Kaufman, Josh
Haley, Benjamin
Giltnane, Jennifer M
Wertz, Ingrid E
Lackner, Mark R
Nannini, Michelle A
Sampath, Deepak
Schwarz, Luis
Manning, Henry Charles
Tantawy, Mohammed Noor
Arteaga, Carlos L
Heyman, Richard A
Rix, Peter J
Friedman, Lori
Smith, Nicholas D
Metcalfe, Ciara
Hager, Jeffrey H
The selective estrogen receptor downregulator GDC-0810 is efficacious in diverse models of ER+ breast cancer
title The selective estrogen receptor downregulator GDC-0810 is efficacious in diverse models of ER+ breast cancer
title_full The selective estrogen receptor downregulator GDC-0810 is efficacious in diverse models of ER+ breast cancer
title_fullStr The selective estrogen receptor downregulator GDC-0810 is efficacious in diverse models of ER+ breast cancer
title_full_unstemmed The selective estrogen receptor downregulator GDC-0810 is efficacious in diverse models of ER+ breast cancer
title_short The selective estrogen receptor downregulator GDC-0810 is efficacious in diverse models of ER+ breast cancer
title_sort selective estrogen receptor downregulator gdc-0810 is efficacious in diverse models of er+ breast cancer
topic Cancer Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4961458/
https://www.ncbi.nlm.nih.gov/pubmed/27410477
http://dx.doi.org/10.7554/eLife.15828
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