ZEB1 collaborates with ELK3 to repress e-cadherin expression in triple-negative breast cancer cells

Hyeon Ju Cho; Nuri Oh; Ji Hoon Park; Kwang Soo Kim; Hyung Keun Kim; Eunbyeol Lee; Sohyun Hwang; Seong Jin Kim; Kyung Soon Park

doi:10.1158/1541-7786.MCR-19-0380

ZEB1 collaborates with ELK3 to repress e-cadherin expression in triple-negative breast cancer cells

Hyeon Ju Cho, Nuri Oh, Ji Hoon Park, Kwang Soo Kim, Hyung Keun Kim, Eunbyeol Lee, Sohyun Hwang, Seong Jin Kim, Kyung Soon Park^*

^*Corresponding author for this work

Neurological Surgery

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

27 Scopus citations

Abstract

ZEB1 has intrinsic oncogenic functions that control the epithelial-to-mesenchymal transition (EMT) of cancer cells, impacting tumorigenesis from its earliest stages. By integrating microenvironment signals and being implicated in feedback regulatory loops, ZEB1 appears to be a central switch that determines EMT and metastasis of cancer cells. Here, we found that ZEB1 collaborates with ELK3, a ternary complex factor belonging to the ETS family, to repress E-cadherin expression. ZEB1 functions as a transcriptional activator of ELK3. We first identified that ELK3 and ZEB1 have a positively correlated expression in breast cancer cells by using multiple databases for correlation analysis. Molecular analysis revealed that ZEB1 functions as a transcriptional activator of ELK3 expression. GST pull-down assay and coimmunoprecipitation analysis of wild-type or domain deletion mutants of ZEB1 and ELK3 showed that these 2 proteins directly bound each other. Furthermore, we demonstrated that ZEB1 and ELK3 collaborate to repress the expression of E-cadherin, a representative protein that initiates EMT. Our finding suggested that ELK3 is a novel factor of the ZEB1/E-cadherin axis in triple-negative breast cancer cells.

Original language	English (US)
Pages (from-to)	2257-2266
Number of pages	10
Journal	Molecular Cancer Research
Volume	17
Issue number	11
DOIs	https://doi.org/10.1158/1541-7786.MCR-19-0380
State	Published - 2019

Funding

This research was supported by the Ministry of Education, Science, and Technology (NRF-2019R1A2C1003581) and by Basic Science Research Program through the National Research Foundation of Korea (NRF) funded by the Ministry of Education (2019R1A6A1A03032888).

ASJC Scopus subject areas

General Medicine

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10.1158/1541-7786.MCR-19-0380

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title = "ZEB1 collaborates with ELK3 to repress e-cadherin expression in triple-negative breast cancer cells",

abstract = "ZEB1 has intrinsic oncogenic functions that control the epithelial-to-mesenchymal transition (EMT) of cancer cells, impacting tumorigenesis from its earliest stages. By integrating microenvironment signals and being implicated in feedback regulatory loops, ZEB1 appears to be a central switch that determines EMT and metastasis of cancer cells. Here, we found that ZEB1 collaborates with ELK3, a ternary complex factor belonging to the ETS family, to repress E-cadherin expression. ZEB1 functions as a transcriptional activator of ELK3. We first identified that ELK3 and ZEB1 have a positively correlated expression in breast cancer cells by using multiple databases for correlation analysis. Molecular analysis revealed that ZEB1 functions as a transcriptional activator of ELK3 expression. GST pull-down assay and coimmunoprecipitation analysis of wild-type or domain deletion mutants of ZEB1 and ELK3 showed that these 2 proteins directly bound each other. Furthermore, we demonstrated that ZEB1 and ELK3 collaborate to repress the expression of E-cadherin, a representative protein that initiates EMT. Our finding suggested that ELK3 is a novel factor of the ZEB1/E-cadherin axis in triple-negative breast cancer cells.",

author = "Cho, {Hyeon Ju} and Nuri Oh and Park, {Ji Hoon} and Kim, {Kwang Soo} and Kim, {Hyung Keun} and Eunbyeol Lee and Sohyun Hwang and Kim, {Seong Jin} and Park, {Kyung Soon}",

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doi = "10.1158/1541-7786.MCR-19-0380",

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AU - Cho, Hyeon Ju

AU - Oh, Nuri

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AU - Kim, Kwang Soo

AU - Kim, Hyung Keun

AU - Lee, Eunbyeol

AU - Hwang, Sohyun

AU - Kim, Seong Jin

AU - Park, Kyung Soon

PY - 2019

Y1 - 2019

N2 - ZEB1 has intrinsic oncogenic functions that control the epithelial-to-mesenchymal transition (EMT) of cancer cells, impacting tumorigenesis from its earliest stages. By integrating microenvironment signals and being implicated in feedback regulatory loops, ZEB1 appears to be a central switch that determines EMT and metastasis of cancer cells. Here, we found that ZEB1 collaborates with ELK3, a ternary complex factor belonging to the ETS family, to repress E-cadherin expression. ZEB1 functions as a transcriptional activator of ELK3. We first identified that ELK3 and ZEB1 have a positively correlated expression in breast cancer cells by using multiple databases for correlation analysis. Molecular analysis revealed that ZEB1 functions as a transcriptional activator of ELK3 expression. GST pull-down assay and coimmunoprecipitation analysis of wild-type or domain deletion mutants of ZEB1 and ELK3 showed that these 2 proteins directly bound each other. Furthermore, we demonstrated that ZEB1 and ELK3 collaborate to repress the expression of E-cadherin, a representative protein that initiates EMT. Our finding suggested that ELK3 is a novel factor of the ZEB1/E-cadherin axis in triple-negative breast cancer cells.

AB - ZEB1 has intrinsic oncogenic functions that control the epithelial-to-mesenchymal transition (EMT) of cancer cells, impacting tumorigenesis from its earliest stages. By integrating microenvironment signals and being implicated in feedback regulatory loops, ZEB1 appears to be a central switch that determines EMT and metastasis of cancer cells. Here, we found that ZEB1 collaborates with ELK3, a ternary complex factor belonging to the ETS family, to repress E-cadherin expression. ZEB1 functions as a transcriptional activator of ELK3. We first identified that ELK3 and ZEB1 have a positively correlated expression in breast cancer cells by using multiple databases for correlation analysis. Molecular analysis revealed that ZEB1 functions as a transcriptional activator of ELK3 expression. GST pull-down assay and coimmunoprecipitation analysis of wild-type or domain deletion mutants of ZEB1 and ELK3 showed that these 2 proteins directly bound each other. Furthermore, we demonstrated that ZEB1 and ELK3 collaborate to repress the expression of E-cadherin, a representative protein that initiates EMT. Our finding suggested that ELK3 is a novel factor of the ZEB1/E-cadherin axis in triple-negative breast cancer cells.

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ZEB1 collaborates with ELK3 to repress e-cadherin expression in triple-negative breast cancer cells

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