Differential contributions of pre- And post-EMT tumor cells in breast cancer metastasis

Ana Rita Lourenco; Yi Ban; Michael J. Crowley; Sharrell B. Lee; Divya Ramchandani; Wei Du; Olivier Elemento; Jason T. George; Mohit Kumar Jolly; Herbert Levine; Jianting Sheng; Stephen T. Wong; Nasser K. Altorki; Dingcheng Gao

doi:10.1158/0008-5472.CAN-19-1427

Differential contributions of pre- And post-EMT tumor cells in breast cancer metastasis

Ana Rita Lourenco, Yi Ban, Michael J. Crowley, Sharrell B. Lee, Divya Ramchandani, Wei Du, Olivier Elemento, Jason T. George, Mohit Kumar Jolly, Herbert Levine, Jianting Sheng, Stephen T. Wong, Nasser K. Altorki, Dingcheng Gao

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60 Scopus citations

Abstract

Metastases are responsible for the majority of breast cancer-associated deaths. The contribution of epithelial-to-mesenchymal transition (EMT) in the establishment of metastases is still controversial. To obtain in vivo evidence of EMT in metastasis, we established an EMT lineage tracing (Tri-PyMT) model, in which tumor cells undergoing EMT would irreversibly switch their fluorescent marker from RFP + to GFP + due to mesenchymal-specific Cre expression. Surprisingly, we found that lung metastases were predominantly derived from the epithelial compartment of breast tumors. However, concerns were raised on the fidelity and sensitivity of RFP-to-GFP switch of this model in reporting EMT of metastatic tumor cells. Here, we evaluated Tri-PyMT cells at the single-cell level using single-cell RNA-sequencing and found that the Tri-PyMT cells exhibited a spectrum of EMT phenotypes, with EMT-related genes concomitantly expressed with the activation of GFP. The fluorescent color switch in these cells precisely marked an unequivocal change in EMT status, defining the pre-EMT and post-EMT compartments within the tumor. Consistently, the pre-EMT cells played dominant roles in metastasis, while the post-EMT cells were supportive in promoting tumor invasion and angiogenesis. Importantly, the post-EMT (GFP +) cells in the Tri-PyMT model were not permanently committed to the mesenchymal phenotype; they were still capable of reverting to the epithelial phenotype and giving rise to secondary tumors, suggesting their persistent EMT plasticity. Our study addressed major concerns with the Tri-PyMT EMT lineage tracing model, which provides us with a powerful tool to investigate the dynamic EMT process in tumor biology. SIGNIFICANCE: These findings confirm the fidelity and sensitivity of the EMT lineage tracing (Tri-PyMT) model and highlight the differential contributions of pre- and post-EMT tumor cells in breast cancer metastasis. See related commentary by Bunz, p. 153.

Original language	English (US)
Pages (from-to)	163-169
Number of pages	7
Journal	Cancer research
Volume	80
Issue number	2
DOIs	https://doi.org/10.1158/0008-5472.CAN-19-1427
State	Published - Jan 15 2020

Keywords

Breast Neoplasms
Cell Line, Tumor
Epithelial-Mesenchymal Transition
Humans
Lung Neoplasms
Phenotype

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1158/0008-5472.CAN-19-1427

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@article{6f94519824424738b1132585310be074,

title = "Differential contributions of pre- And post-EMT tumor cells in breast cancer metastasis",

abstract = "Metastases are responsible for the majority of breast cancer-associated deaths. The contribution of epithelial-to-mesenchymal transition (EMT) in the establishment of metastases is still controversial. To obtain in vivo evidence of EMT in metastasis, we established an EMT lineage tracing (Tri-PyMT) model, in which tumor cells undergoing EMT would irreversibly switch their fluorescent marker from RFP + to GFP + due to mesenchymal-specific Cre expression. Surprisingly, we found that lung metastases were predominantly derived from the epithelial compartment of breast tumors. However, concerns were raised on the fidelity and sensitivity of RFP-to-GFP switch of this model in reporting EMT of metastatic tumor cells. Here, we evaluated Tri-PyMT cells at the single-cell level using single-cell RNA-sequencing and found that the Tri-PyMT cells exhibited a spectrum of EMT phenotypes, with EMT-related genes concomitantly expressed with the activation of GFP. The fluorescent color switch in these cells precisely marked an unequivocal change in EMT status, defining the pre-EMT and post-EMT compartments within the tumor. Consistently, the pre-EMT cells played dominant roles in metastasis, while the post-EMT cells were supportive in promoting tumor invasion and angiogenesis. Importantly, the post-EMT (GFP +) cells in the Tri-PyMT model were not permanently committed to the mesenchymal phenotype; they were still capable of reverting to the epithelial phenotype and giving rise to secondary tumors, suggesting their persistent EMT plasticity. Our study addressed major concerns with the Tri-PyMT EMT lineage tracing model, which provides us with a powerful tool to investigate the dynamic EMT process in tumor biology. SIGNIFICANCE: These findings confirm the fidelity and sensitivity of the EMT lineage tracing (Tri-PyMT) model and highlight the differential contributions of pre- and post-EMT tumor cells in breast cancer metastasis. See related commentary by Bunz, p. 153. ",

keywords = "Breast Neoplasms, Cell Line, Tumor, Epithelial-Mesenchymal Transition, Humans, Lung Neoplasms, Phenotype",

author = "Lourenco, {Ana Rita} and Yi Ban and Crowley, {Michael J.} and Lee, {Sharrell B.} and Divya Ramchandani and Wei Du and Olivier Elemento and George, {Jason T.} and Jolly, {Mohit Kumar} and Herbert Levine and Jianting Sheng and Wong, {Stephen T.} and Altorki, {Nasser K.} and Dingcheng Gao",

note = "Funding Information: This work was supported by NIH (5R01CA205418), the Neuberger Berman Foundation Lung Cancer Research Center, and by generous donations to the Division of Thoracic Surgery to N.K. Altorki. J. Sheng and S.T.C. Wong were supported by NIH U01CA-188388, John S Dunn Research Foundation, TT & WF Chao Foundation, and Johnston Estate Endowment. Publisher Copyright: {\textcopyright} 2020 American Association for Cancer Research.",

year = "2020",

month = jan,

day = "15",

doi = "10.1158/0008-5472.CAN-19-1427",

language = "English (US)",

volume = "80",

pages = "163--169",

journal = "Cancer research",

issn = "0008-5472",

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T1 - Differential contributions of pre- And post-EMT tumor cells in breast cancer metastasis

AU - Lourenco, Ana Rita

AU - Ban, Yi

AU - Crowley, Michael J.

AU - Lee, Sharrell B.

AU - Ramchandani, Divya

AU - Du, Wei

AU - Elemento, Olivier

AU - George, Jason T.

AU - Jolly, Mohit Kumar

AU - Levine, Herbert

AU - Sheng, Jianting

AU - Wong, Stephen T.

AU - Altorki, Nasser K.

AU - Gao, Dingcheng

N1 - Funding Information: This work was supported by NIH (5R01CA205418), the Neuberger Berman Foundation Lung Cancer Research Center, and by generous donations to the Division of Thoracic Surgery to N.K. Altorki. J. Sheng and S.T.C. Wong were supported by NIH U01CA-188388, John S Dunn Research Foundation, TT & WF Chao Foundation, and Johnston Estate Endowment. Publisher Copyright: © 2020 American Association for Cancer Research.

PY - 2020/1/15

Y1 - 2020/1/15

N2 - Metastases are responsible for the majority of breast cancer-associated deaths. The contribution of epithelial-to-mesenchymal transition (EMT) in the establishment of metastases is still controversial. To obtain in vivo evidence of EMT in metastasis, we established an EMT lineage tracing (Tri-PyMT) model, in which tumor cells undergoing EMT would irreversibly switch their fluorescent marker from RFP + to GFP + due to mesenchymal-specific Cre expression. Surprisingly, we found that lung metastases were predominantly derived from the epithelial compartment of breast tumors. However, concerns were raised on the fidelity and sensitivity of RFP-to-GFP switch of this model in reporting EMT of metastatic tumor cells. Here, we evaluated Tri-PyMT cells at the single-cell level using single-cell RNA-sequencing and found that the Tri-PyMT cells exhibited a spectrum of EMT phenotypes, with EMT-related genes concomitantly expressed with the activation of GFP. The fluorescent color switch in these cells precisely marked an unequivocal change in EMT status, defining the pre-EMT and post-EMT compartments within the tumor. Consistently, the pre-EMT cells played dominant roles in metastasis, while the post-EMT cells were supportive in promoting tumor invasion and angiogenesis. Importantly, the post-EMT (GFP +) cells in the Tri-PyMT model were not permanently committed to the mesenchymal phenotype; they were still capable of reverting to the epithelial phenotype and giving rise to secondary tumors, suggesting their persistent EMT plasticity. Our study addressed major concerns with the Tri-PyMT EMT lineage tracing model, which provides us with a powerful tool to investigate the dynamic EMT process in tumor biology. SIGNIFICANCE: These findings confirm the fidelity and sensitivity of the EMT lineage tracing (Tri-PyMT) model and highlight the differential contributions of pre- and post-EMT tumor cells in breast cancer metastasis. See related commentary by Bunz, p. 153.

AB - Metastases are responsible for the majority of breast cancer-associated deaths. The contribution of epithelial-to-mesenchymal transition (EMT) in the establishment of metastases is still controversial. To obtain in vivo evidence of EMT in metastasis, we established an EMT lineage tracing (Tri-PyMT) model, in which tumor cells undergoing EMT would irreversibly switch their fluorescent marker from RFP + to GFP + due to mesenchymal-specific Cre expression. Surprisingly, we found that lung metastases were predominantly derived from the epithelial compartment of breast tumors. However, concerns were raised on the fidelity and sensitivity of RFP-to-GFP switch of this model in reporting EMT of metastatic tumor cells. Here, we evaluated Tri-PyMT cells at the single-cell level using single-cell RNA-sequencing and found that the Tri-PyMT cells exhibited a spectrum of EMT phenotypes, with EMT-related genes concomitantly expressed with the activation of GFP. The fluorescent color switch in these cells precisely marked an unequivocal change in EMT status, defining the pre-EMT and post-EMT compartments within the tumor. Consistently, the pre-EMT cells played dominant roles in metastasis, while the post-EMT cells were supportive in promoting tumor invasion and angiogenesis. Importantly, the post-EMT (GFP +) cells in the Tri-PyMT model were not permanently committed to the mesenchymal phenotype; they were still capable of reverting to the epithelial phenotype and giving rise to secondary tumors, suggesting their persistent EMT plasticity. Our study addressed major concerns with the Tri-PyMT EMT lineage tracing model, which provides us with a powerful tool to investigate the dynamic EMT process in tumor biology. SIGNIFICANCE: These findings confirm the fidelity and sensitivity of the EMT lineage tracing (Tri-PyMT) model and highlight the differential contributions of pre- and post-EMT tumor cells in breast cancer metastasis. See related commentary by Bunz, p. 153.

KW - Breast Neoplasms

KW - Cell Line, Tumor

KW - Epithelial-Mesenchymal Transition

KW - Humans

KW - Lung Neoplasms

KW - Phenotype

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Differential contributions of pre- And post-EMT tumor cells in breast cancer metastasis

Abstract

Keywords

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