ErbB3 downregulation enhances luminal breast tumor response to antiestrogens

Meghan M. Morrison; Katherine Hutchinson; Michelle M. Williams; Jamie C. Stanford; Justin M. Balko; Christian Young; Maria G. Kuba; Violeta Sánchez; Andrew J. Williams; Donna J. Hicks; Carlos L. Arteaga; Aleix Prat; Charles M. Perou; H. Shelton Earp; Suleiman Massarweh; Rebecca S. Cook

doi:10.1172/JCI66764

ErbB3 downregulation enhances luminal breast tumor response to antiestrogens

Meghan M. Morrison, Katherine Hutchinson, Michelle M. Williams, Jamie C. Stanford, Justin M. Balko, Christian Young, Maria G. Kuba, Violeta Sánchez, Andrew J. Williams, Donna J. Hicks, Carlos L. Arteaga, Aleix Prat, Charles M. Perou, H. Shelton Earp, Suleiman Massarweh, Rebecca S. Cook

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

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Abstract

Aberrant regulation of the erythroblastosis oncogene B (ErbB) family of receptor tyrosine kinases (RTKs) and their ligands is common in human cancers. ErbB3 is required in luminal mammary epithelial cells (MECs) for growth and survival. Since breast cancer phenotypes may reflect biological traits of the MECs from which they originate, we tested the hypothesis that ErbB3 drives luminal breast cancer growth. We found higher ERBB3 expression and more frequent ERBB3 gene copy gains in luminal A/B breast cancers compared with other breast cancer subtypes. In cell culture, ErbB3 increased growth of luminal breast cancer cells. Targeted depletion of ErbB3 with an anti-ErbB3 antibody decreased 3D colony growth, increased apoptosis, and decreased tumor growth in vivo. Treatment of clinical breast tumors with the antiendocrine drug fulvestrant resulted in increased ErbB3 expression and PI3K/mTOR signaling. Depletion of ErbB3 in fulvestrant-treated tumor cells reduced PI3K/mTOR signaling, thus decreasing tumor cell survival and tumor growth. Fulvestrant treatment increased phosphorylation of all ErbB family RTKs; however, phospho-RTK upregulation was not seen in tumors treated with both fulvestrant and anti-ErbB3. These data indicate that upregulation of ErbB3 in luminal breast cancer cells promotes growth, survival, and resistance to fulvestrant, thus suggesting ErbB3 as a target for breast cancer treatment.

Original language	English (US)
Pages (from-to)	4329-4343
Number of pages	15
Journal	Journal of Clinical Investigation
Volume	123
Issue number	10
DOIs	https://doi.org/10.1172/JCI66764
State	Published - Oct 1 2013

ASJC Scopus subject areas

General Medicine

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Morrison, M. M., Hutchinson, K., Williams, M. M., Stanford, J. C., Balko, J. M., Young, C., Kuba, M. G., Sánchez, V., Williams, A. J., Hicks, D. J., Arteaga, C. L., Prat, A., Perou, C. M., Shelton Earp, H., Massarweh, S., & Cook, R. S. (2013). ErbB3 downregulation enhances luminal breast tumor response to antiestrogens. Journal of Clinical Investigation, 123(10), 4329-4343. https://doi.org/10.1172/JCI66764

Morrison, MM, Hutchinson, K, Williams, MM, Stanford, JC, Balko, JM, Young, C, Kuba, MG, Sánchez, V, Williams, AJ, Hicks, DJ, Arteaga, CL, Prat, A, Perou, CM, Shelton Earp, H, Massarweh, S & Cook, RS 2013, 'ErbB3 downregulation enhances luminal breast tumor response to antiestrogens', Journal of Clinical Investigation, vol. 123, no. 10, pp. 4329-4343. https://doi.org/10.1172/JCI66764

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title = "ErbB3 downregulation enhances luminal breast tumor response to antiestrogens",

abstract = "Aberrant regulation of the erythroblastosis oncogene B (ErbB) family of receptor tyrosine kinases (RTKs) and their ligands is common in human cancers. ErbB3 is required in luminal mammary epithelial cells (MECs) for growth and survival. Since breast cancer phenotypes may reflect biological traits of the MECs from which they originate, we tested the hypothesis that ErbB3 drives luminal breast cancer growth. We found higher ERBB3 expression and more frequent ERBB3 gene copy gains in luminal A/B breast cancers compared with other breast cancer subtypes. In cell culture, ErbB3 increased growth of luminal breast cancer cells. Targeted depletion of ErbB3 with an anti-ErbB3 antibody decreased 3D colony growth, increased apoptosis, and decreased tumor growth in vivo. Treatment of clinical breast tumors with the antiendocrine drug fulvestrant resulted in increased ErbB3 expression and PI3K/mTOR signaling. Depletion of ErbB3 in fulvestrant-treated tumor cells reduced PI3K/mTOR signaling, thus decreasing tumor cell survival and tumor growth. Fulvestrant treatment increased phosphorylation of all ErbB family RTKs; however, phospho-RTK upregulation was not seen in tumors treated with both fulvestrant and anti-ErbB3. These data indicate that upregulation of ErbB3 in luminal breast cancer cells promotes growth, survival, and resistance to fulvestrant, thus suggesting ErbB3 as a target for breast cancer treatment.",

author = "Morrison, {Meghan M.} and Katherine Hutchinson and Williams, {Michelle M.} and Stanford, {Jamie C.} and Balko, {Justin M.} and Christian Young and Kuba, {Maria G.} and Violeta S{\'a}nchez and Williams, {Andrew J.} and Hicks, {Donna J.} and Arteaga, {Carlos L.} and Aleix Prat and Perou, {Charles M.} and {Shelton Earp}, H. and Suleiman Massarweh and Cook, {Rebecca S.}",

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AU - Morrison, Meghan M.

AU - Hutchinson, Katherine

AU - Williams, Michelle M.

AU - Stanford, Jamie C.

AU - Balko, Justin M.

AU - Young, Christian

AU - Kuba, Maria G.

AU - Sánchez, Violeta

AU - Williams, Andrew J.

AU - Hicks, Donna J.

AU - Arteaga, Carlos L.

AU - Prat, Aleix

AU - Perou, Charles M.

AU - Shelton Earp, H.

AU - Massarweh, Suleiman

AU - Cook, Rebecca S.

PY - 2013/10/1

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N2 - Aberrant regulation of the erythroblastosis oncogene B (ErbB) family of receptor tyrosine kinases (RTKs) and their ligands is common in human cancers. ErbB3 is required in luminal mammary epithelial cells (MECs) for growth and survival. Since breast cancer phenotypes may reflect biological traits of the MECs from which they originate, we tested the hypothesis that ErbB3 drives luminal breast cancer growth. We found higher ERBB3 expression and more frequent ERBB3 gene copy gains in luminal A/B breast cancers compared with other breast cancer subtypes. In cell culture, ErbB3 increased growth of luminal breast cancer cells. Targeted depletion of ErbB3 with an anti-ErbB3 antibody decreased 3D colony growth, increased apoptosis, and decreased tumor growth in vivo. Treatment of clinical breast tumors with the antiendocrine drug fulvestrant resulted in increased ErbB3 expression and PI3K/mTOR signaling. Depletion of ErbB3 in fulvestrant-treated tumor cells reduced PI3K/mTOR signaling, thus decreasing tumor cell survival and tumor growth. Fulvestrant treatment increased phosphorylation of all ErbB family RTKs; however, phospho-RTK upregulation was not seen in tumors treated with both fulvestrant and anti-ErbB3. These data indicate that upregulation of ErbB3 in luminal breast cancer cells promotes growth, survival, and resistance to fulvestrant, thus suggesting ErbB3 as a target for breast cancer treatment.

AB - Aberrant regulation of the erythroblastosis oncogene B (ErbB) family of receptor tyrosine kinases (RTKs) and their ligands is common in human cancers. ErbB3 is required in luminal mammary epithelial cells (MECs) for growth and survival. Since breast cancer phenotypes may reflect biological traits of the MECs from which they originate, we tested the hypothesis that ErbB3 drives luminal breast cancer growth. We found higher ERBB3 expression and more frequent ERBB3 gene copy gains in luminal A/B breast cancers compared with other breast cancer subtypes. In cell culture, ErbB3 increased growth of luminal breast cancer cells. Targeted depletion of ErbB3 with an anti-ErbB3 antibody decreased 3D colony growth, increased apoptosis, and decreased tumor growth in vivo. Treatment of clinical breast tumors with the antiendocrine drug fulvestrant resulted in increased ErbB3 expression and PI3K/mTOR signaling. Depletion of ErbB3 in fulvestrant-treated tumor cells reduced PI3K/mTOR signaling, thus decreasing tumor cell survival and tumor growth. Fulvestrant treatment increased phosphorylation of all ErbB family RTKs; however, phospho-RTK upregulation was not seen in tumors treated with both fulvestrant and anti-ErbB3. These data indicate that upregulation of ErbB3 in luminal breast cancer cells promotes growth, survival, and resistance to fulvestrant, thus suggesting ErbB3 as a target for breast cancer treatment.

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JO - Journal of Clinical Investigation

JF - Journal of Clinical Investigation

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ER -

ErbB3 downregulation enhances luminal breast tumor response to antiestrogens

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