Nonphosphorylatable PEA15 mutant inhibits epithelial-mesenchymal transition in triple-negative breast cancer partly through the regulation of IL-8 expression

Jihyun Park; Moises J. Tacam; Gaurav Chauhan; Evan N. Cohen; Maria Gagliardi; Lakesla R. Iles; Naoto T. Ueno; Venkata L. Battula; Yoo Kyoung Sohn; Xiaoping Wang; Hak Sung Kim; Savitri Krishnamurthy; Natalie W. Fowlkes; Morgan M. Green; Geoffrey A. Bartholomeusz; Debu Tripathy; James M. Reuben; Chandra Bartholomeusz

doi:10.1007/s10549-021-06316-2

Nonphosphorylatable PEA15 mutant inhibits epithelial-mesenchymal transition in triple-negative breast cancer partly through the regulation of IL-8 expression

Jihyun Park, Moises J. Tacam, Gaurav Chauhan, Evan N. Cohen, Maria Gagliardi, Lakesla R. Iles, Naoto T. Ueno, Venkata L. Battula, Yoo Kyoung Sohn, Xiaoping Wang, Hak Sung Kim, Savitri Krishnamurthy, Natalie W. Fowlkes, Morgan M. Green, Geoffrey A. Bartholomeusz, Debu Tripathy, James M. Reuben, Chandra Bartholomeusz

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

1 Scopus citations

Abstract

Background: Triple-negative breast cancer (TNBC) is an aggressive breast cancer subtype that lacks targeted therapies. Patients with TNBC have a very poor prognosis because the disease often metastasizes. New treatment approaches addressing drivers of metastasis and tumor growth are crucial to improving patient outcomes. Developing targeted gene therapy is thus a high priority for TNBC patients. PEA15 (phosphoprotein enriched in astrocytes, 15 kDa) is known to bind to ERK, preventing ERK from being translocated to the nucleus and hence blocking its activity. The biological function of PEA15 is tightly regulated by its phosphorylation at Ser104 and Ser116. However, the function and impact of phosphorylation status of PEA15 in the regulation of TNBC metastasis and in epithelial-to-mesenchymal transition (EMT) are not well understood. Methods: We established stable cell lines overexpressing nonphosphorylatable (PEA15-AA) and phospho-mimetic (PEA15-DD) mutants. To dissect specific cellular mechanisms regulated by PEA15 phosphorylation status, we performed RT-PCR immune and metastasis arrays. In vivo mouse models were used to determine the effects of PEA15 phosphorylation on tumor growth and metastasis. Results: We found that the nonphosphorylatable mutant PEA15-AA prevented formation of mammospheres and expression of EMT markers in vitro and decreased tumor growth and lung metastasis in in vivo experiments when compared to control, PEA15-WT and phosphomimetic PEA15-DD. However, phosphomimetic mutant PEA15-DD promoted migration, mesenchymal marker expression, tumorigenesis, and lung metastasis in the mouse model. PEA15-AA-mediated inhibition of breast cancer cell migratory capacity and tumorigenesis was the partial result of decreased expression of interleukin-8 (IL-8). Further, we identified that expression of IL-8 was possibly mediated through one of the ERK downstream molecules, Ets-1. Conclusions: Our results show that PEA15 phosphorylation status serves as an important regulator for PEA15’s dual role as an oncogene or tumor suppressor and support the potential of PEA15-AA as a therapeutic strategy for treatment of TNBC.

Original language	English (US)
Pages (from-to)	333-345
Number of pages	13
Journal	Breast Cancer Research and Treatment
Volume	189
Issue number	2
DOIs	https://doi.org/10.1007/s10549-021-06316-2
State	Published - Sep 2021

Keywords

EMT
Ets-1
IL-8
PEA15
Triple-negative breast cancer

ASJC Scopus subject areas

Oncology
Cancer Research

MD Anderson CCSG core facilities

Research Animal Support Facility

Access to Document

10.1007/s10549-021-06316-2

Cite this

Park, J., Tacam, M. J., Chauhan, G., Cohen, E. N., Gagliardi, M., Iles, L. R., Ueno, N. T., Battula, V. L., Sohn, Y. K., Wang, X., Kim, H. S., Krishnamurthy, S., Fowlkes, N. W., Green, M. M., Bartholomeusz, G. A., Tripathy, D., Reuben, J. M., & Bartholomeusz, C. (2021). Nonphosphorylatable PEA15 mutant inhibits epithelial-mesenchymal transition in triple-negative breast cancer partly through the regulation of IL-8 expression. Breast Cancer Research and Treatment, 189(2), 333-345. https://doi.org/10.1007/s10549-021-06316-2

Park, J, Tacam, MJ, Chauhan, G, Cohen, EN, Gagliardi, M, Iles, LR, Ueno, NT, Battula, VL, Sohn, YK, Wang, X, Kim, HS, Krishnamurthy, S , Fowlkes, NW, Green, MM, Bartholomeusz, GA, Tripathy, D, Reuben, JM & Bartholomeusz, C 2021, 'Nonphosphorylatable PEA15 mutant inhibits epithelial-mesenchymal transition in triple-negative breast cancer partly through the regulation of IL-8 expression', Breast Cancer Research and Treatment, vol. 189, no. 2, pp. 333-345. https://doi.org/10.1007/s10549-021-06316-2

@article{cfaaf4a7be464a669926d8d7dec71d1d,

title = "Nonphosphorylatable PEA15 mutant inhibits epithelial-mesenchymal transition in triple-negative breast cancer partly through the regulation of IL-8 expression",

abstract = "Background: Triple-negative breast cancer (TNBC) is an aggressive breast cancer subtype that lacks targeted therapies. Patients with TNBC have a very poor prognosis because the disease often metastasizes. New treatment approaches addressing drivers of metastasis and tumor growth are crucial to improving patient outcomes. Developing targeted gene therapy is thus a high priority for TNBC patients. PEA15 (phosphoprotein enriched in astrocytes, 15 kDa) is known to bind to ERK, preventing ERK from being translocated to the nucleus and hence blocking its activity. The biological function of PEA15 is tightly regulated by its phosphorylation at Ser104 and Ser116. However, the function and impact of phosphorylation status of PEA15 in the regulation of TNBC metastasis and in epithelial-to-mesenchymal transition (EMT) are not well understood. Methods: We established stable cell lines overexpressing nonphosphorylatable (PEA15-AA) and phospho-mimetic (PEA15-DD) mutants. To dissect specific cellular mechanisms regulated by PEA15 phosphorylation status, we performed RT-PCR immune and metastasis arrays. In vivo mouse models were used to determine the effects of PEA15 phosphorylation on tumor growth and metastasis. Results: We found that the nonphosphorylatable mutant PEA15-AA prevented formation of mammospheres and expression of EMT markers in vitro and decreased tumor growth and lung metastasis in in vivo experiments when compared to control, PEA15-WT and phosphomimetic PEA15-DD. However, phosphomimetic mutant PEA15-DD promoted migration, mesenchymal marker expression, tumorigenesis, and lung metastasis in the mouse model. PEA15-AA-mediated inhibition of breast cancer cell migratory capacity and tumorigenesis was the partial result of decreased expression of interleukin-8 (IL-8). Further, we identified that expression of IL-8 was possibly mediated through one of the ERK downstream molecules, Ets-1. Conclusions: Our results show that PEA15 phosphorylation status serves as an important regulator for PEA15{\textquoteright}s dual role as an oncogene or tumor suppressor and support the potential of PEA15-AA as a therapeutic strategy for treatment of TNBC.",

keywords = "EMT, Ets-1, IL-8, PEA15, Triple-negative breast cancer",

author = "Jihyun Park and Tacam, {Moises J.} and Gaurav Chauhan and Cohen, {Evan N.} and Maria Gagliardi and Iles, {Lakesla R.} and Ueno, {Naoto T.} and Battula, {Venkata L.} and Sohn, {Yoo Kyoung} and Xiaoping Wang and Kim, {Hak Sung} and Savitri Krishnamurthy and Fowlkes, {Natalie W.} and Green, {Morgan M.} and Bartholomeusz, {Geoffrey A.} and Debu Tripathy and Reuben, {James M.} and Chandra Bartholomeusz",

note = "Publisher Copyright: {\textcopyright} 2021, The Author(s).",

year = "2021",

month = sep,

doi = "10.1007/s10549-021-06316-2",

language = "English (US)",

volume = "189",

pages = "333--345",

journal = "Breast Cancer Research and Treatment",

issn = "0167-6806",

publisher = "Springer New York",

number = "2",

}

TY - JOUR

T1 - Nonphosphorylatable PEA15 mutant inhibits epithelial-mesenchymal transition in triple-negative breast cancer partly through the regulation of IL-8 expression

AU - Park, Jihyun

AU - Tacam, Moises J.

AU - Chauhan, Gaurav

AU - Cohen, Evan N.

AU - Gagliardi, Maria

AU - Iles, Lakesla R.

AU - Ueno, Naoto T.

AU - Battula, Venkata L.

AU - Sohn, Yoo Kyoung

AU - Wang, Xiaoping

AU - Kim, Hak Sung

AU - Krishnamurthy, Savitri

AU - Fowlkes, Natalie W.

AU - Green, Morgan M.

AU - Bartholomeusz, Geoffrey A.

AU - Tripathy, Debu

AU - Reuben, James M.

AU - Bartholomeusz, Chandra

PY - 2021/9

Y1 - 2021/9

N2 - Background: Triple-negative breast cancer (TNBC) is an aggressive breast cancer subtype that lacks targeted therapies. Patients with TNBC have a very poor prognosis because the disease often metastasizes. New treatment approaches addressing drivers of metastasis and tumor growth are crucial to improving patient outcomes. Developing targeted gene therapy is thus a high priority for TNBC patients. PEA15 (phosphoprotein enriched in astrocytes, 15 kDa) is known to bind to ERK, preventing ERK from being translocated to the nucleus and hence blocking its activity. The biological function of PEA15 is tightly regulated by its phosphorylation at Ser104 and Ser116. However, the function and impact of phosphorylation status of PEA15 in the regulation of TNBC metastasis and in epithelial-to-mesenchymal transition (EMT) are not well understood. Methods: We established stable cell lines overexpressing nonphosphorylatable (PEA15-AA) and phospho-mimetic (PEA15-DD) mutants. To dissect specific cellular mechanisms regulated by PEA15 phosphorylation status, we performed RT-PCR immune and metastasis arrays. In vivo mouse models were used to determine the effects of PEA15 phosphorylation on tumor growth and metastasis. Results: We found that the nonphosphorylatable mutant PEA15-AA prevented formation of mammospheres and expression of EMT markers in vitro and decreased tumor growth and lung metastasis in in vivo experiments when compared to control, PEA15-WT and phosphomimetic PEA15-DD. However, phosphomimetic mutant PEA15-DD promoted migration, mesenchymal marker expression, tumorigenesis, and lung metastasis in the mouse model. PEA15-AA-mediated inhibition of breast cancer cell migratory capacity and tumorigenesis was the partial result of decreased expression of interleukin-8 (IL-8). Further, we identified that expression of IL-8 was possibly mediated through one of the ERK downstream molecules, Ets-1. Conclusions: Our results show that PEA15 phosphorylation status serves as an important regulator for PEA15’s dual role as an oncogene or tumor suppressor and support the potential of PEA15-AA as a therapeutic strategy for treatment of TNBC.

AB - Background: Triple-negative breast cancer (TNBC) is an aggressive breast cancer subtype that lacks targeted therapies. Patients with TNBC have a very poor prognosis because the disease often metastasizes. New treatment approaches addressing drivers of metastasis and tumor growth are crucial to improving patient outcomes. Developing targeted gene therapy is thus a high priority for TNBC patients. PEA15 (phosphoprotein enriched in astrocytes, 15 kDa) is known to bind to ERK, preventing ERK from being translocated to the nucleus and hence blocking its activity. The biological function of PEA15 is tightly regulated by its phosphorylation at Ser104 and Ser116. However, the function and impact of phosphorylation status of PEA15 in the regulation of TNBC metastasis and in epithelial-to-mesenchymal transition (EMT) are not well understood. Methods: We established stable cell lines overexpressing nonphosphorylatable (PEA15-AA) and phospho-mimetic (PEA15-DD) mutants. To dissect specific cellular mechanisms regulated by PEA15 phosphorylation status, we performed RT-PCR immune and metastasis arrays. In vivo mouse models were used to determine the effects of PEA15 phosphorylation on tumor growth and metastasis. Results: We found that the nonphosphorylatable mutant PEA15-AA prevented formation of mammospheres and expression of EMT markers in vitro and decreased tumor growth and lung metastasis in in vivo experiments when compared to control, PEA15-WT and phosphomimetic PEA15-DD. However, phosphomimetic mutant PEA15-DD promoted migration, mesenchymal marker expression, tumorigenesis, and lung metastasis in the mouse model. PEA15-AA-mediated inhibition of breast cancer cell migratory capacity and tumorigenesis was the partial result of decreased expression of interleukin-8 (IL-8). Further, we identified that expression of IL-8 was possibly mediated through one of the ERK downstream molecules, Ets-1. Conclusions: Our results show that PEA15 phosphorylation status serves as an important regulator for PEA15’s dual role as an oncogene or tumor suppressor and support the potential of PEA15-AA as a therapeutic strategy for treatment of TNBC.

KW - EMT

KW - Ets-1

KW - IL-8

KW - PEA15

KW - Triple-negative breast cancer

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U2 - 10.1007/s10549-021-06316-2

DO - 10.1007/s10549-021-06316-2

M3 - Article

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AN - SCOPUS:85109952263

SN - 0167-6806

VL - 189

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EP - 345

JO - Breast Cancer Research and Treatment

JF - Breast Cancer Research and Treatment

IS - 2

ER -

Nonphosphorylatable PEA15 mutant inhibits epithelial-mesenchymal transition in triple-negative breast cancer partly through the regulation of IL-8 expression

Abstract

Keywords

ASJC Scopus subject areas

MD Anderson CCSG core facilities

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