EWI2 prevents EGFR from clustering and endocytosis to reduce tumor cell movement and proliferation

Chenying Fu; Jie Wang; Sandeep Pallikkuth; Yingjun Ding; Junxiong Chen; Jonathan D. Wren; Yuchao Yang; Kwong Kwok Wong; Hiroyasu Kameyama; Muralidharan Jayaraman; Anupama Munshi; Takemi Tanaka; Keith A. Lidke; Xin A. Zhang

doi:10.1007/s00018-022-04417-9

EWI2 prevents EGFR from clustering and endocytosis to reduce tumor cell movement and proliferation

Chenying Fu, Jie Wang, Sandeep Pallikkuth, Yingjun Ding, Junxiong Chen, Jonathan D. Wren, Yuchao Yang, Kwong Kwok Wong, Hiroyasu Kameyama, Muralidharan Jayaraman, Anupama Munshi, Takemi Tanaka, Keith A. Lidke, Xin A. Zhang

Gynecological Oncology & Reproductive Medicine

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

2 Scopus citations

Abstract

EWI2 is a transmembrane immunoglobulin superfamily (IgSF) protein that physically associates with tetraspanins and integrins. It inhibits cancer cells by influencing the interactions among membrane molecules including the tetraspanins and integrins. The present study revealed that, upon EWI2 silencing or ablation, the elevated movement and proliferation of cancer cells in vitro and increased cancer metastatic potential and malignancy in vivo are associated with (i) increases in clustering, endocytosis, and then activation of EGFR and (ii) enhancement of Erk MAP kinase signaling. These changes in signaling make cancer cells (i) undergo partial epithelial-to-mesenchymal (EMT) for more tumor progression and (ii) proliferate faster for better tumor formation. Inhibition of EGFR or Erk kinase can abrogate the cancer cell phenotypes resulting from EWI2 removal. Thus, to inhibit cancer cells, EWI2 prevents EGFR from clustering and endocytosis to restrain its activation and signaling.

Original language	English (US)
Article number	389
Journal	Cellular and Molecular Life Sciences
Volume	79
Issue number	7
DOIs	https://doi.org/10.1007/s00018-022-04417-9
State	Published - Jul 2022

Keywords

And integrin
Clathrin-mediated endocytosis
Epithelial-to-mesenchymal transition
MAPK signaling
Membrane spatial heterogeneity

ASJC Scopus subject areas

Molecular Medicine
Molecular Biology
Pharmacology
Cellular and Molecular Neuroscience
Cell Biology

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Fu, C., Wang, J., Pallikkuth, S., Ding, Y., Chen, J., Wren, J. D., Yang, Y., Wong, K. K., Kameyama, H., Jayaraman, M., Munshi, A., Tanaka, T., Lidke, K. A., & Zhang, X. A. (2022). EWI2 prevents EGFR from clustering and endocytosis to reduce tumor cell movement and proliferation. Cellular and Molecular Life Sciences, 79(7), Article 389. https://doi.org/10.1007/s00018-022-04417-9

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title = "EWI2 prevents EGFR from clustering and endocytosis to reduce tumor cell movement and proliferation",

abstract = "EWI2 is a transmembrane immunoglobulin superfamily (IgSF) protein that physically associates with tetraspanins and integrins. It inhibits cancer cells by influencing the interactions among membrane molecules including the tetraspanins and integrins. The present study revealed that, upon EWI2 silencing or ablation, the elevated movement and proliferation of cancer cells in vitro and increased cancer metastatic potential and malignancy in vivo are associated with (i) increases in clustering, endocytosis, and then activation of EGFR and (ii) enhancement of Erk MAP kinase signaling. These changes in signaling make cancer cells (i) undergo partial epithelial-to-mesenchymal (EMT) for more tumor progression and (ii) proliferate faster for better tumor formation. Inhibition of EGFR or Erk kinase can abrogate the cancer cell phenotypes resulting from EWI2 removal. Thus, to inhibit cancer cells, EWI2 prevents EGFR from clustering and endocytosis to restrain its activation and signaling.",

keywords = "And integrin, Clathrin-mediated endocytosis, Epithelial-to-mesenchymal transition, MAPK signaling, Membrane spatial heterogeneity",

author = "Chenying Fu and Jie Wang and Sandeep Pallikkuth and Yingjun Ding and Junxiong Chen and Wren, {Jonathan D.} and Yuchao Yang and Wong, {Kwong Kwok} and Hiroyasu Kameyama and Muralidharan Jayaraman and Anupama Munshi and Takemi Tanaka and Lidke, {Keith A.} and Zhang, {Xin A.}",

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year = "2022",

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doi = "10.1007/s00018-022-04417-9",

language = "English (US)",

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T1 - EWI2 prevents EGFR from clustering and endocytosis to reduce tumor cell movement and proliferation

AU - Fu, Chenying

AU - Wang, Jie

AU - Pallikkuth, Sandeep

AU - Ding, Yingjun

AU - Chen, Junxiong

AU - Wren, Jonathan D.

AU - Yang, Yuchao

AU - Wong, Kwong Kwok

AU - Kameyama, Hiroyasu

AU - Jayaraman, Muralidharan

AU - Munshi, Anupama

AU - Tanaka, Takemi

AU - Lidke, Keith A.

AU - Zhang, Xin A.

PY - 2022/7

Y1 - 2022/7

N2 - EWI2 is a transmembrane immunoglobulin superfamily (IgSF) protein that physically associates with tetraspanins and integrins. It inhibits cancer cells by influencing the interactions among membrane molecules including the tetraspanins and integrins. The present study revealed that, upon EWI2 silencing or ablation, the elevated movement and proliferation of cancer cells in vitro and increased cancer metastatic potential and malignancy in vivo are associated with (i) increases in clustering, endocytosis, and then activation of EGFR and (ii) enhancement of Erk MAP kinase signaling. These changes in signaling make cancer cells (i) undergo partial epithelial-to-mesenchymal (EMT) for more tumor progression and (ii) proliferate faster for better tumor formation. Inhibition of EGFR or Erk kinase can abrogate the cancer cell phenotypes resulting from EWI2 removal. Thus, to inhibit cancer cells, EWI2 prevents EGFR from clustering and endocytosis to restrain its activation and signaling.

AB - EWI2 is a transmembrane immunoglobulin superfamily (IgSF) protein that physically associates with tetraspanins and integrins. It inhibits cancer cells by influencing the interactions among membrane molecules including the tetraspanins and integrins. The present study revealed that, upon EWI2 silencing or ablation, the elevated movement and proliferation of cancer cells in vitro and increased cancer metastatic potential and malignancy in vivo are associated with (i) increases in clustering, endocytosis, and then activation of EGFR and (ii) enhancement of Erk MAP kinase signaling. These changes in signaling make cancer cells (i) undergo partial epithelial-to-mesenchymal (EMT) for more tumor progression and (ii) proliferate faster for better tumor formation. Inhibition of EGFR or Erk kinase can abrogate the cancer cell phenotypes resulting from EWI2 removal. Thus, to inhibit cancer cells, EWI2 prevents EGFR from clustering and endocytosis to restrain its activation and signaling.

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KW - Epithelial-to-mesenchymal transition

KW - MAPK signaling

KW - Membrane spatial heterogeneity

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EWI2 prevents EGFR from clustering and endocytosis to reduce tumor cell movement and proliferation

Abstract

Keywords

ASJC Scopus subject areas

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