Epithelial-mesenchymal transition can suppress major attributes of human epithelial tumor-initiating cells

Toni Celià-Terrassa; Óscar Meca-Cortés; Francesca Mateo; Alexia Martínez De Paz; Nuria Rubio; Anna Arnal-Estapé; Brian J. Ell; Raquel Bermudo; Alba Díaz; Marta Guerra-Rebollo; Juan José Lozano; Conchi Estarás; Catalina Ulloa; Daniel Álvarez-Simón; Jordi Milà; Ramón Vilella; Rosanna Paciucci; Marian Martínez-Balbás; Antonio García De Herreros; Roger R. Gomis; Yibin Kang; Jerónimo Blanco; Pedro L. Fernández; Timothy M. Thomson

doi:10.1172/JCI59218

Epithelial-mesenchymal transition can suppress major attributes of human epithelial tumor-initiating cells

Toni Celià-Terrassa
, Óscar Meca-Cortés
, Francesca Mateo
, Alexia Martínez De Paz
, Nuria Rubio
, Anna Arnal-Estapé
, Brian J. Ell
, Raquel Bermudo
, Alba Díaz
, Marta Guerra-Rebollo
, Juan José Lozano
, Conchi Estarás
, Catalina Ulloa
, Daniel Álvarez-Simón
, Jordi Milà
, Ramón Vilella
, Rosanna Paciucci
, Marian Martínez-Balbás
, Antonio García De Herreros
, Roger R. Gomis

Yibin Kang, Jerónimo Blanco, Pedro L. Fernández, Timothy M. Thomson^*

^*Corresponding author for this work

Research output: Indexed journal article › Article › peer-review

403 Citations (Scopus)

Abstract

Malignant progression in cancer requires populations of tumor-initiating cells (TICs) endowed with unlimited self renewal, survival under stress, and establishment of distant metastases. Additionally, the acquisition of invasive properties driven by epithelial-mesenchymal transition (EMT) is critical for the evolution of neoplastic cells into fully metastatic populations. Here, we characterize 2 human cellular models derived from prostate and bladder cancer cell lines to better understand the relationship between TIC and EMT programs in local invasiveness and distant metastasis. The model tumor subpopulations that expressed a strong epithelial gene program were enriched in highly metastatic TICs, while a second subpopulation with stable mesenchymal traits was impoverished in TICs. Constitutive overexpression of the transcription factor Snai1 in the epithelial/ TIC-enriched populations engaged a mesenchymal gene program and suppressed their self renewal and metastatic phenotypes. Conversely, knockdown of EMT factors in the mesenchymal-like prostate cancer cell subpopulation caused a gain in epithelial features and properties of TICs. Both tumor cell subpopulations cooperated so that the nonmetastatic mesenchymal-like prostate cancer subpopulation enhanced the in vitro invasiveness of the metastatic epithelial subpopulation and, in vivo, promoted the escape of the latter from primary implantation sites and accelerated their metastatic colonization. Our models provide new insights into how dynamic interactions among epithelial, self-renewal, and mesenchymal gene programs determine the plasticity of epithelial TICs.

Original language	English
Pages (from-to)	1849-1868
Number of pages	20
Journal	Journal of Clinical Investigation
Volume	122
Issue number	5
DOIs	https://doi.org/10.1172/JCI59218
Publication status	Published - 1 May 2012
Externally published	Yes

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Keywords

Cancer stem-cells
Lymph-node metastasis
E-cadherin
Embryonic stem
Distant metastases
Pancreatic-cancer
Breast-carcinoma
Expression
Growth
Identification

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10.1172/JCI59218

Cite this

Celià-Terrassa, T., Meca-Cortés, Ó., Mateo, F., De Paz, A. M., Rubio, N., Arnal-Estapé, A., Ell, B. J., Bermudo, R., Díaz, A., Guerra-Rebollo, M., Lozano, J. J., Estarás, C., Ulloa, C., Álvarez-Simón, D., Milà, J., Vilella, R., Paciucci, R., Martínez-Balbás, M., De Herreros, A. G., ... Thomson, T. M. (2012). Epithelial-mesenchymal transition can suppress major attributes of human epithelial tumor-initiating cells. Journal of Clinical Investigation, 122(5), 1849-1868. https://doi.org/10.1172/JCI59218

@article{23fde4c4e22e49edacc384492e65bc27,

title = "Epithelial-mesenchymal transition can suppress major attributes of human epithelial tumor-initiating cells",

abstract = "Malignant progression in cancer requires populations of tumor-initiating cells (TICs) endowed with unlimited self renewal, survival under stress, and establishment of distant metastases. Additionally, the acquisition of invasive properties driven by epithelial-mesenchymal transition (EMT) is critical for the evolution of neoplastic cells into fully metastatic populations. Here, we characterize 2 human cellular models derived from prostate and bladder cancer cell lines to better understand the relationship between TIC and EMT programs in local invasiveness and distant metastasis. The model tumor subpopulations that expressed a strong epithelial gene program were enriched in highly metastatic TICs, while a second subpopulation with stable mesenchymal traits was impoverished in TICs. Constitutive overexpression of the transcription factor Snai1 in the epithelial/ TIC-enriched populations engaged a mesenchymal gene program and suppressed their self renewal and metastatic phenotypes. Conversely, knockdown of EMT factors in the mesenchymal-like prostate cancer cell subpopulation caused a gain in epithelial features and properties of TICs. Both tumor cell subpopulations cooperated so that the nonmetastatic mesenchymal-like prostate cancer subpopulation enhanced the in vitro invasiveness of the metastatic epithelial subpopulation and, in vivo, promoted the escape of the latter from primary implantation sites and accelerated their metastatic colonization. Our models provide new insights into how dynamic interactions among epithelial, self-renewal, and mesenchymal gene programs determine the plasticity of epithelial TICs.",

keywords = "Cancer stem-cells, Lymph-node metastasis, E-cadherin, Embryonic stem, Distant metastases, Pancreatic-cancer, Breast-carcinoma, Expression, Growth, Identification",

author = "Toni Celi{\`a}-Terrassa and {\'O}scar Meca-Cort{\'e}s and Francesca Mateo and \{De Paz\}, \{Alexia Mart{\'i}nez\} and Nuria Rubio and Anna Arnal-Estap{\'e} and Ell, \{Brian J.\} and Raquel Bermudo and Alba D{\'i}az and Marta Guerra-Rebollo and Lozano, \{Juan Jos{\'e}\} and Conchi Estar{\'a}s and Catalina Ulloa and Daniel {\'A}lvarez-Sim{\'o}n and Jordi Mil{\`a} and Ram{\'o}n Vilella and Rosanna Paciucci and Marian Mart{\'i}nez-Balb{\'a}s and \{De Herreros\}, \{Antonio Garc{\'i}a\} and Gomis, \{Roger R.\} and Yibin Kang and Jer{\'o}nimo Blanco and Fern{\'a}ndez, \{Pedro L.\} and Thomson, \{Timothy M.\}",

year = "2012",

month = may,

day = "1",

doi = "10.1172/JCI59218",

language = "English",

volume = "122",

pages = "1849--1868",

journal = "Journal of Clinical Investigation",

issn = "0021-9738",

publisher = "American Society for Clinical Investigation",

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}

Celià-Terrassa, T, Meca-Cortés, Ó, Mateo, F, De Paz, AM, Rubio, N, Arnal-Estapé, A, Ell, BJ, Bermudo, R, Díaz, A, Guerra-Rebollo, M, Lozano, JJ, Estarás, C, Ulloa, C, Álvarez-Simón, D, Milà, J, Vilella, R, Paciucci, R, Martínez-Balbás, M, De Herreros, AG, Gomis, RR, Kang, Y, Blanco, J, Fernández, PL & Thomson, TM 2012, 'Epithelial-mesenchymal transition can suppress major attributes of human epithelial tumor-initiating cells', Journal of Clinical Investigation, vol. 122, no. 5, pp. 1849-1868. https://doi.org/10.1172/JCI59218

TY - JOUR

T1 - Epithelial-mesenchymal transition can suppress major attributes of human epithelial tumor-initiating cells

AU - Celià-Terrassa, Toni

AU - Meca-Cortés, Óscar

AU - Mateo, Francesca

AU - De Paz, Alexia Martínez

AU - Rubio, Nuria

AU - Arnal-Estapé, Anna

AU - Ell, Brian J.

AU - Bermudo, Raquel

AU - Díaz, Alba

AU - Guerra-Rebollo, Marta

AU - Lozano, Juan José

AU - Estarás, Conchi

AU - Ulloa, Catalina

AU - Álvarez-Simón, Daniel

AU - Milà, Jordi

AU - Vilella, Ramón

AU - Paciucci, Rosanna

AU - Martínez-Balbás, Marian

AU - De Herreros, Antonio García

AU - Gomis, Roger R.

AU - Kang, Yibin

AU - Blanco, Jerónimo

AU - Fernández, Pedro L.

AU - Thomson, Timothy M.

PY - 2012/5/1

Y1 - 2012/5/1

N2 - Malignant progression in cancer requires populations of tumor-initiating cells (TICs) endowed with unlimited self renewal, survival under stress, and establishment of distant metastases. Additionally, the acquisition of invasive properties driven by epithelial-mesenchymal transition (EMT) is critical for the evolution of neoplastic cells into fully metastatic populations. Here, we characterize 2 human cellular models derived from prostate and bladder cancer cell lines to better understand the relationship between TIC and EMT programs in local invasiveness and distant metastasis. The model tumor subpopulations that expressed a strong epithelial gene program were enriched in highly metastatic TICs, while a second subpopulation with stable mesenchymal traits was impoverished in TICs. Constitutive overexpression of the transcription factor Snai1 in the epithelial/ TIC-enriched populations engaged a mesenchymal gene program and suppressed their self renewal and metastatic phenotypes. Conversely, knockdown of EMT factors in the mesenchymal-like prostate cancer cell subpopulation caused a gain in epithelial features and properties of TICs. Both tumor cell subpopulations cooperated so that the nonmetastatic mesenchymal-like prostate cancer subpopulation enhanced the in vitro invasiveness of the metastatic epithelial subpopulation and, in vivo, promoted the escape of the latter from primary implantation sites and accelerated their metastatic colonization. Our models provide new insights into how dynamic interactions among epithelial, self-renewal, and mesenchymal gene programs determine the plasticity of epithelial TICs.

AB - Malignant progression in cancer requires populations of tumor-initiating cells (TICs) endowed with unlimited self renewal, survival under stress, and establishment of distant metastases. Additionally, the acquisition of invasive properties driven by epithelial-mesenchymal transition (EMT) is critical for the evolution of neoplastic cells into fully metastatic populations. Here, we characterize 2 human cellular models derived from prostate and bladder cancer cell lines to better understand the relationship between TIC and EMT programs in local invasiveness and distant metastasis. The model tumor subpopulations that expressed a strong epithelial gene program were enriched in highly metastatic TICs, while a second subpopulation with stable mesenchymal traits was impoverished in TICs. Constitutive overexpression of the transcription factor Snai1 in the epithelial/ TIC-enriched populations engaged a mesenchymal gene program and suppressed their self renewal and metastatic phenotypes. Conversely, knockdown of EMT factors in the mesenchymal-like prostate cancer cell subpopulation caused a gain in epithelial features and properties of TICs. Both tumor cell subpopulations cooperated so that the nonmetastatic mesenchymal-like prostate cancer subpopulation enhanced the in vitro invasiveness of the metastatic epithelial subpopulation and, in vivo, promoted the escape of the latter from primary implantation sites and accelerated their metastatic colonization. Our models provide new insights into how dynamic interactions among epithelial, self-renewal, and mesenchymal gene programs determine the plasticity of epithelial TICs.

KW - Cancer stem-cells

KW - Lymph-node metastasis

KW - E-cadherin

KW - Embryonic stem

KW - Distant metastases

KW - Pancreatic-cancer

KW - Breast-carcinoma

KW - Expression

KW - Growth

KW - Identification

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U2 - 10.1172/JCI59218

DO - 10.1172/JCI59218

M3 - Article

C2 - 22505459

AN - SCOPUS:84860578009

SN - 0021-9738

VL - 122

SP - 1849

EP - 1868

JO - Journal of Clinical Investigation

JF - Journal of Clinical Investigation

IS - 5

ER -

Epithelial-mesenchymal transition can suppress major attributes of human epithelial tumor-initiating cells

Abstract

UN SDGs

Keywords

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