ZEB1 drives epithelial-to-mesenchymal transition in lung cancer

Jill E. Larsen; Vaishnavi Nathan; Jihan K. Osborne; Rebecca K. Farrow; Dhruba Deb; James P. Sullivan; Patrick D. Dospoy; Alexander Augustyn; Suzie K. Hight; Mitsuo Sato; Luc Girard; Carmen Behrens; Ignacio I. Wistuba; Adi F. Gazdar; Nicholas K. Hayward; John D. Minna

doi:10.1172/JCI76725

ZEB1 drives epithelial-to-mesenchymal transition in lung cancer

Jill E. Larsen, Vaishnavi Nathan, Jihan K. Osborne, Rebecca K. Farrow, Dhruba Deb, James P. Sullivan, Patrick D. Dospoy, Alexander Augustyn, Suzie K. Hight, Mitsuo Sato, Luc Girard, Carmen Behrens, Ignacio I. Wistuba, Adi F. Gazdar, Nicholas K. Hayward, John D. Minna

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243 Scopus citations

Abstract

Increased expression of zinc finger E-box binding homeobox 1 (ZEB1) is associated with tumor grade and metastasis in lung cancer, likely due to its role as a transcription factor in epithelial-to-mesenchymal transition (EMT). Here, we modeled malignant transformation in human bronchial epithelial cells (HBECs) and determined that EMT and ZEB1 expression are early, critical events in lung cancer pathogenesis. Specific oncogenic mutations in TP53 and KRAS were required for HBECs to engage EMT machinery in response to microenvironmental (serum/TGF-β) or oncogenetic (MYC) factors. Both TGF-β- and MYC-induced EMT required ZEB1, but engaged distinct TGF-β-dependent and vitamin D receptor-dependent (VDR-dependent) pathways, respectively. Functionally, we found that ZEB1 causally promotes malignant progression of HBECs and tumorigenicity, invasion, and metastases in non-small cell lung cancer (NSCLC) lines. Mechanistically, ZEB1 expression in HBECs directly repressed epithelial splicing regulatory protein 1 (ESRP1), leading to increased expression of a mesenchymal splice variant of CD44 and a more invasive phenotype. In addition, ZEB1 expression in early stage IB primary NSCLC correlated with tumor-node-metastasis stage. These findings indicate that ZEB1-induced EMT and associated molecular changes in ESRP1 and CD44 contribute to early pathogenesis and metastatic potential in established lung cancer. Moreover, TGF-β and VDR signaling and CD44 splicing pathways associated with ZEB1 are potential EMT chemoprevention and therapeutic targets in NSCLC.

Original language	English (US)
Pages (from-to)	3219-3235
Number of pages	17
Journal	Journal of Clinical Investigation
Volume	126
Issue number	9
DOIs	https://doi.org/10.1172/JCI76725
State	Published - Sep 1 2016

ASJC Scopus subject areas

General Medicine

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Larsen, J. E., Nathan, V., Osborne, J. K., Farrow, R. K., Deb, D., Sullivan, J. P., Dospoy, P. D., Augustyn, A., Hight, S. K., Sato, M., Girard, L., Behrens, C., Wistuba, I. I., Gazdar, A. F., Hayward, N. K., & Minna, J. D. (2016). ZEB1 drives epithelial-to-mesenchymal transition in lung cancer. Journal of Clinical Investigation, 126(9), 3219-3235. https://doi.org/10.1172/JCI76725

@article{7f78e5d504524c85bff4905cd1124116,

title = "ZEB1 drives epithelial-to-mesenchymal transition in lung cancer",

abstract = "Increased expression of zinc finger E-box binding homeobox 1 (ZEB1) is associated with tumor grade and metastasis in lung cancer, likely due to its role as a transcription factor in epithelial-to-mesenchymal transition (EMT). Here, we modeled malignant transformation in human bronchial epithelial cells (HBECs) and determined that EMT and ZEB1 expression are early, critical events in lung cancer pathogenesis. Specific oncogenic mutations in TP53 and KRAS were required for HBECs to engage EMT machinery in response to microenvironmental (serum/TGF-β) or oncogenetic (MYC) factors. Both TGF-β- and MYC-induced EMT required ZEB1, but engaged distinct TGF-β-dependent and vitamin D receptor-dependent (VDR-dependent) pathways, respectively. Functionally, we found that ZEB1 causally promotes malignant progression of HBECs and tumorigenicity, invasion, and metastases in non-small cell lung cancer (NSCLC) lines. Mechanistically, ZEB1 expression in HBECs directly repressed epithelial splicing regulatory protein 1 (ESRP1), leading to increased expression of a mesenchymal splice variant of CD44 and a more invasive phenotype. In addition, ZEB1 expression in early stage IB primary NSCLC correlated with tumor-node-metastasis stage. These findings indicate that ZEB1-induced EMT and associated molecular changes in ESRP1 and CD44 contribute to early pathogenesis and metastatic potential in established lung cancer. Moreover, TGF-β and VDR signaling and CD44 splicing pathways associated with ZEB1 are potential EMT chemoprevention and therapeutic targets in NSCLC.",

author = "Larsen, {Jill E.} and Vaishnavi Nathan and Osborne, {Jihan K.} and Farrow, {Rebecca K.} and Dhruba Deb and Sullivan, {James P.} and Dospoy, {Patrick D.} and Alexander Augustyn and Hight, {Suzie K.} and Mitsuo Sato and Luc Girard and Carmen Behrens and Wistuba, {Ignacio I.} and Gazdar, {Adi F.} and Hayward, {Nicholas K.} and Minna, {John D.}",

note = "Funding Information: The authors wish to thank members of the Minna laboratory for their technical assistance, scientific discussion, and manuscript comments; Alex Pertsemlidis (Greehey Children's Cancer Research Institute at the University of Texas Health Science Center, San Antonio, Texas, USA) for scientific discussion; Thomas Brabletz for providing the pSuperRetroPuro-shZEB1 plasmid; Jennifer Richer (University of Colorado Health Sciences Center, Denver, Colorado, USA) for the ZEB1-pCIneo plasmid; and Rolf A. Brekken (University of Texas Southwestern Medical Center) for TGF-β monoclonal antibody (clone 1D11) and control antibody 13C4 monoclonal antibody. This work was supported by the NCI Lung Cancer SPORE (P50CA70907), CTD2N CA176284, NASA NSCOR (NNJ05HD36G), and Cancer Prevention and Research Institute of Texas (CPRIT) (RP120732). JEL was supported by a National Health and Medical Research Council of Australia Overseas-Based Biomedical Training Fellowship (494511), Thoracic Society of Australia and New Zealand/Allen and Hanburys Respiratory Research Fellowship, and Cancer Australia/ Cure Cancer Australia Priority Driven Collaborative Cancer Research Scheme (1070515)",

year = "2016",

month = sep,

day = "1",

doi = "10.1172/JCI76725",

language = "English (US)",

volume = "126",

pages = "3219--3235",

journal = "Journal of Clinical Investigation",

issn = "0021-9738",

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AU - Larsen, Jill E.

AU - Nathan, Vaishnavi

AU - Osborne, Jihan K.

AU - Farrow, Rebecca K.

AU - Deb, Dhruba

AU - Sullivan, James P.

AU - Dospoy, Patrick D.

AU - Augustyn, Alexander

AU - Hight, Suzie K.

AU - Sato, Mitsuo

AU - Girard, Luc

AU - Behrens, Carmen

AU - Wistuba, Ignacio I.

AU - Gazdar, Adi F.

AU - Hayward, Nicholas K.

AU - Minna, John D.

N1 - Funding Information: The authors wish to thank members of the Minna laboratory for their technical assistance, scientific discussion, and manuscript comments; Alex Pertsemlidis (Greehey Children's Cancer Research Institute at the University of Texas Health Science Center, San Antonio, Texas, USA) for scientific discussion; Thomas Brabletz for providing the pSuperRetroPuro-shZEB1 plasmid; Jennifer Richer (University of Colorado Health Sciences Center, Denver, Colorado, USA) for the ZEB1-pCIneo plasmid; and Rolf A. Brekken (University of Texas Southwestern Medical Center) for TGF-β monoclonal antibody (clone 1D11) and control antibody 13C4 monoclonal antibody. This work was supported by the NCI Lung Cancer SPORE (P50CA70907), CTD2N CA176284, NASA NSCOR (NNJ05HD36G), and Cancer Prevention and Research Institute of Texas (CPRIT) (RP120732). JEL was supported by a National Health and Medical Research Council of Australia Overseas-Based Biomedical Training Fellowship (494511), Thoracic Society of Australia and New Zealand/Allen and Hanburys Respiratory Research Fellowship, and Cancer Australia/ Cure Cancer Australia Priority Driven Collaborative Cancer Research Scheme (1070515)

PY - 2016/9/1

Y1 - 2016/9/1

N2 - Increased expression of zinc finger E-box binding homeobox 1 (ZEB1) is associated with tumor grade and metastasis in lung cancer, likely due to its role as a transcription factor in epithelial-to-mesenchymal transition (EMT). Here, we modeled malignant transformation in human bronchial epithelial cells (HBECs) and determined that EMT and ZEB1 expression are early, critical events in lung cancer pathogenesis. Specific oncogenic mutations in TP53 and KRAS were required for HBECs to engage EMT machinery in response to microenvironmental (serum/TGF-β) or oncogenetic (MYC) factors. Both TGF-β- and MYC-induced EMT required ZEB1, but engaged distinct TGF-β-dependent and vitamin D receptor-dependent (VDR-dependent) pathways, respectively. Functionally, we found that ZEB1 causally promotes malignant progression of HBECs and tumorigenicity, invasion, and metastases in non-small cell lung cancer (NSCLC) lines. Mechanistically, ZEB1 expression in HBECs directly repressed epithelial splicing regulatory protein 1 (ESRP1), leading to increased expression of a mesenchymal splice variant of CD44 and a more invasive phenotype. In addition, ZEB1 expression in early stage IB primary NSCLC correlated with tumor-node-metastasis stage. These findings indicate that ZEB1-induced EMT and associated molecular changes in ESRP1 and CD44 contribute to early pathogenesis and metastatic potential in established lung cancer. Moreover, TGF-β and VDR signaling and CD44 splicing pathways associated with ZEB1 are potential EMT chemoprevention and therapeutic targets in NSCLC.

AB - Increased expression of zinc finger E-box binding homeobox 1 (ZEB1) is associated with tumor grade and metastasis in lung cancer, likely due to its role as a transcription factor in epithelial-to-mesenchymal transition (EMT). Here, we modeled malignant transformation in human bronchial epithelial cells (HBECs) and determined that EMT and ZEB1 expression are early, critical events in lung cancer pathogenesis. Specific oncogenic mutations in TP53 and KRAS were required for HBECs to engage EMT machinery in response to microenvironmental (serum/TGF-β) or oncogenetic (MYC) factors. Both TGF-β- and MYC-induced EMT required ZEB1, but engaged distinct TGF-β-dependent and vitamin D receptor-dependent (VDR-dependent) pathways, respectively. Functionally, we found that ZEB1 causally promotes malignant progression of HBECs and tumorigenicity, invasion, and metastases in non-small cell lung cancer (NSCLC) lines. Mechanistically, ZEB1 expression in HBECs directly repressed epithelial splicing regulatory protein 1 (ESRP1), leading to increased expression of a mesenchymal splice variant of CD44 and a more invasive phenotype. In addition, ZEB1 expression in early stage IB primary NSCLC correlated with tumor-node-metastasis stage. These findings indicate that ZEB1-induced EMT and associated molecular changes in ESRP1 and CD44 contribute to early pathogenesis and metastatic potential in established lung cancer. Moreover, TGF-β and VDR signaling and CD44 splicing pathways associated with ZEB1 are potential EMT chemoprevention and therapeutic targets in NSCLC.

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ZEB1 drives epithelial-to-mesenchymal transition in lung cancer

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