Intrinsic apoptotic pathway activation increases response to anti-estrogens in luminal breast cancers article

Michelle M. Williams; Linus Lee; Thomas Werfel; Meghan M.Morrison Joly; Donna J. Hicks; Bushra Rahman; David Elion; Courtney McKernan; Violeta Sanchez; Monica V. Estrada; Suleiman Massarweh; Richard Elledge; Craig Duvall; Rebecca S. Cook

doi:10.1038/s41419-017-0072-x

Intrinsic apoptotic pathway activation increases response to anti-estrogens in luminal breast cancers article

Michelle M. Williams, Linus Lee, Thomas Werfel, Meghan M.Morrison Joly, Donna J. Hicks, Bushra Rahman, David Elion, Courtney McKernan, Violeta Sanchez, Monica V. Estrada, Suleiman Massarweh, Richard Elledge, Craig Duvall, Rebecca S. Cook

Medicine

Research output: Contribution to journal › Article › peer-review

7 Scopus citations

Abstract

Estrogen receptor-α positive (ERα+) breast cancer accounts for approximately 70-80% of the nearly 25,0000 new cases of breast cancer diagnosed in the US each year. Endocrine-targeted therapies (those that block ERα activity) serve as the first line of treatment in most cases. Despite the proven benefit of endocrine therapies, however, ERα+ breast tumors can develop resistance to endocrine therapy, causing disease progression or relapse, particularly in the metastatic setting. Anti-apoptotic Bcl-2 family proteins enhance breast tumor cell survival, often promoting resistance to targeted therapies, including endocrine therapies. Herein, we investigated whether blockade of anti-apoptotic Bcl-2 family proteins could sensitize luminal breast cancers to anti-estrogen treatment. We used long-term estrogen deprivation (LTED) of human ERα+ breast cancer cell lines, an established model of sustained treatment with and acquired resistance to aromatase inhibitors (AIs), in combination with Bcl-2/Bcl-xL inhibition (ABT-263), finding that ABT-263 induced only limited tumor cell killing in LTED-selected cells in culture and in vivo. Interestingly, expression and activity of the Bcl-2-related factor Mcl-1 was increased in LTED cells. Genetic Mcl-1 ablation induced apoptosis in LTED-selected cells, and potently increased their sensitivity to ABT-263. Increased expression and activity of Mcl-1 was similarly seen in clinical breast tumor specimens treated with AI + the selective estrogen receptor downregulator fulvestrant. Delivery of Mcl-1 siRNA loaded into polymeric nanoparticles (MCL1 si-NPs) decreased Mcl-1 expression in LTED-selected and fulvestrant-treated cells, increasing tumor cell death and blocking tumor cell growth. These findings suggest that Mcl-1 upregulation in response to anti-estrogen treatment enhances tumor cell survival, decreasing response to therapeutic treatments. Therefore, strategies blocking Mcl-1 expression or activity used in combination with endocrine therapies would enhance tumor cell death.

Original language	English (US)
Article number	21
Journal	Cell Death and Disease
Volume	9
Issue number	2
DOIs	https://doi.org/10.1038/s41419-017-0072-x
State	Published - Feb 1 2018

ASJC Scopus subject areas

Immunology
Cellular and Molecular Neuroscience
Cell Biology
Cancer Research

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Williams, M. M., Lee, L., Werfel, T., Joly, M. M. M., Hicks, D. J., Rahman, B., Elion, D., McKernan, C., Sanchez, V., Estrada, M. V., Massarweh, S., Elledge, R., Duvall, C., & Cook, R. S. (2018). Intrinsic apoptotic pathway activation increases response to anti-estrogens in luminal breast cancers article. Cell Death and Disease, 9(2), [21]. https://doi.org/10.1038/s41419-017-0072-x

Intrinsic apoptotic pathway activation increases response to anti-estrogens in luminal breast cancers article. / Williams, Michelle M.; Lee, Linus; Werfel, Thomas; Joly, Meghan M.Morrison; Hicks, Donna J.; Rahman, Bushra; Elion, David; McKernan, Courtney; Sanchez, Violeta; Estrada, Monica V.; Massarweh, Suleiman; Elledge, Richard; Duvall, Craig; Cook, Rebecca S.

In: Cell Death and Disease, Vol. 9, No. 2, 21, 01.02.2018.

Research output: Contribution to journal › Article › peer-review

Williams, Michelle M. ; Lee, Linus ; Werfel, Thomas ; Joly, Meghan M.Morrison ; Hicks, Donna J. ; Rahman, Bushra ; Elion, David ; McKernan, Courtney ; Sanchez, Violeta ; Estrada, Monica V. ; Massarweh, Suleiman ; Elledge, Richard ; Duvall, Craig ; Cook, Rebecca S. / Intrinsic apoptotic pathway activation increases response to anti-estrogens in luminal breast cancers article. In: Cell Death and Disease. 2018 ; Vol. 9, No. 2.

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title = "Intrinsic apoptotic pathway activation increases response to anti-estrogens in luminal breast cancers article",

abstract = "Estrogen receptor-α positive (ERα+) breast cancer accounts for approximately 70-80% of the nearly 25,0000 new cases of breast cancer diagnosed in the US each year. Endocrine-targeted therapies (those that block ERα activity) serve as the first line of treatment in most cases. Despite the proven benefit of endocrine therapies, however, ERα+ breast tumors can develop resistance to endocrine therapy, causing disease progression or relapse, particularly in the metastatic setting. Anti-apoptotic Bcl-2 family proteins enhance breast tumor cell survival, often promoting resistance to targeted therapies, including endocrine therapies. Herein, we investigated whether blockade of anti-apoptotic Bcl-2 family proteins could sensitize luminal breast cancers to anti-estrogen treatment. We used long-term estrogen deprivation (LTED) of human ERα+ breast cancer cell lines, an established model of sustained treatment with and acquired resistance to aromatase inhibitors (AIs), in combination with Bcl-2/Bcl-xL inhibition (ABT-263), finding that ABT-263 induced only limited tumor cell killing in LTED-selected cells in culture and in vivo. Interestingly, expression and activity of the Bcl-2-related factor Mcl-1 was increased in LTED cells. Genetic Mcl-1 ablation induced apoptosis in LTED-selected cells, and potently increased their sensitivity to ABT-263. Increased expression and activity of Mcl-1 was similarly seen in clinical breast tumor specimens treated with AI + the selective estrogen receptor downregulator fulvestrant. Delivery of Mcl-1 siRNA loaded into polymeric nanoparticles (MCL1 si-NPs) decreased Mcl-1 expression in LTED-selected and fulvestrant-treated cells, increasing tumor cell death and blocking tumor cell growth. These findings suggest that Mcl-1 upregulation in response to anti-estrogen treatment enhances tumor cell survival, decreasing response to therapeutic treatments. Therefore, strategies blocking Mcl-1 expression or activity used in combination with endocrine therapies would enhance tumor cell death.",

author = "Williams, {Michelle M.} and Linus Lee and Thomas Werfel and Joly, {Meghan M.Morrison} and Hicks, {Donna J.} and Bushra Rahman and David Elion and Courtney McKernan and Violeta Sanchez and Estrada, {Monica V.} and Suleiman Massarweh and Richard Elledge and Craig Duvall and Cook, {Rebecca S.}",

note = "Funding Information: This work was supported by Specialized Program of Research Excellence (SPORE) grant NIH P50 CA098131 (VICC), Cancer Center Support grant NIH P30 CA68485 (VICC), NIH F31 CA195989-01 (MMW) and CTSA UL1TR000445 from the National Center for Advancing Translational Sciences.",

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AU - Werfel, Thomas

AU - Joly, Meghan M.Morrison

AU - Hicks, Donna J.

AU - Rahman, Bushra

AU - Elion, David

AU - McKernan, Courtney

AU - Sanchez, Violeta

AU - Estrada, Monica V.

AU - Massarweh, Suleiman

AU - Elledge, Richard

AU - Duvall, Craig

AU - Cook, Rebecca S.

N1 - Funding Information: This work was supported by Specialized Program of Research Excellence (SPORE) grant NIH P50 CA098131 (VICC), Cancer Center Support grant NIH P30 CA68485 (VICC), NIH F31 CA195989-01 (MMW) and CTSA UL1TR000445 from the National Center for Advancing Translational Sciences.

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N2 - Estrogen receptor-α positive (ERα+) breast cancer accounts for approximately 70-80% of the nearly 25,0000 new cases of breast cancer diagnosed in the US each year. Endocrine-targeted therapies (those that block ERα activity) serve as the first line of treatment in most cases. Despite the proven benefit of endocrine therapies, however, ERα+ breast tumors can develop resistance to endocrine therapy, causing disease progression or relapse, particularly in the metastatic setting. Anti-apoptotic Bcl-2 family proteins enhance breast tumor cell survival, often promoting resistance to targeted therapies, including endocrine therapies. Herein, we investigated whether blockade of anti-apoptotic Bcl-2 family proteins could sensitize luminal breast cancers to anti-estrogen treatment. We used long-term estrogen deprivation (LTED) of human ERα+ breast cancer cell lines, an established model of sustained treatment with and acquired resistance to aromatase inhibitors (AIs), in combination with Bcl-2/Bcl-xL inhibition (ABT-263), finding that ABT-263 induced only limited tumor cell killing in LTED-selected cells in culture and in vivo. Interestingly, expression and activity of the Bcl-2-related factor Mcl-1 was increased in LTED cells. Genetic Mcl-1 ablation induced apoptosis in LTED-selected cells, and potently increased their sensitivity to ABT-263. Increased expression and activity of Mcl-1 was similarly seen in clinical breast tumor specimens treated with AI + the selective estrogen receptor downregulator fulvestrant. Delivery of Mcl-1 siRNA loaded into polymeric nanoparticles (MCL1 si-NPs) decreased Mcl-1 expression in LTED-selected and fulvestrant-treated cells, increasing tumor cell death and blocking tumor cell growth. These findings suggest that Mcl-1 upregulation in response to anti-estrogen treatment enhances tumor cell survival, decreasing response to therapeutic treatments. Therefore, strategies blocking Mcl-1 expression or activity used in combination with endocrine therapies would enhance tumor cell death.

AB - Estrogen receptor-α positive (ERα+) breast cancer accounts for approximately 70-80% of the nearly 25,0000 new cases of breast cancer diagnosed in the US each year. Endocrine-targeted therapies (those that block ERα activity) serve as the first line of treatment in most cases. Despite the proven benefit of endocrine therapies, however, ERα+ breast tumors can develop resistance to endocrine therapy, causing disease progression or relapse, particularly in the metastatic setting. Anti-apoptotic Bcl-2 family proteins enhance breast tumor cell survival, often promoting resistance to targeted therapies, including endocrine therapies. Herein, we investigated whether blockade of anti-apoptotic Bcl-2 family proteins could sensitize luminal breast cancers to anti-estrogen treatment. We used long-term estrogen deprivation (LTED) of human ERα+ breast cancer cell lines, an established model of sustained treatment with and acquired resistance to aromatase inhibitors (AIs), in combination with Bcl-2/Bcl-xL inhibition (ABT-263), finding that ABT-263 induced only limited tumor cell killing in LTED-selected cells in culture and in vivo. Interestingly, expression and activity of the Bcl-2-related factor Mcl-1 was increased in LTED cells. Genetic Mcl-1 ablation induced apoptosis in LTED-selected cells, and potently increased their sensitivity to ABT-263. Increased expression and activity of Mcl-1 was similarly seen in clinical breast tumor specimens treated with AI + the selective estrogen receptor downregulator fulvestrant. Delivery of Mcl-1 siRNA loaded into polymeric nanoparticles (MCL1 si-NPs) decreased Mcl-1 expression in LTED-selected and fulvestrant-treated cells, increasing tumor cell death and blocking tumor cell growth. These findings suggest that Mcl-1 upregulation in response to anti-estrogen treatment enhances tumor cell survival, decreasing response to therapeutic treatments. Therefore, strategies blocking Mcl-1 expression or activity used in combination with endocrine therapies would enhance tumor cell death.

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