Growth and metastasis of lung adenocarcinoma is potentiated by BMP4-mediated immunosuppression

Limo Chen; Xiaohui Yi; Sangeeta Goswami; Young Ho Ahn; Jonathon D. Roybal; Yongbin Yang; Lixia Diao; Di Peng; David Peng; Jared J. Fradette; Jing Wang; Lauren A. Byers; Jonathan M. Kurie; Stephen E. Ullrich; F. Xiao Feng Qin; Don L. Gibbons

doi:10.1080/2162402X.2016.1234570

Growth and metastasis of lung adenocarcinoma is potentiated by BMP4-mediated immunosuppression

Limo Chen, Xiaohui Yi, Sangeeta Goswami, Young Ho Ahn, Jonathon D. Roybal, Yongbin Yang, Lixia Diao, Di Peng, David Peng, Jared J. Fradette, Jing Wang, Lauren A. Byers, Jonathan M. Kurie, Stephen E. Ullrich, F. Xiao Feng Qin, Don L. Gibbons

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

22 Scopus citations

Abstract

Cancer cells modulate the recruitment and function of inflammatory cells to create an immunosuppressive microenvironment that favors tumor growth and metastasis. However, the tumor-derived regulatory programs that promote intratumoral immunosuppression remain poorly defined. Here, we show in a Kras^LA1/+p53^R172HΔg/+-based mouse model that bone morphogenetic protein-4 (BMP4) augments the expression of the T cell co-inhibitory receptor ligand PD-L1 in the mesenchymal subset of lung cancer cells, leading to profound CD8⁺ T cell-mediated immunosuppression, producing tumor growth and metastasis. We previously reported in this model that BMP4 functions as a pro-tumorigenic factor regulated by miR-200 via GATA4/6. Thus, BMP4‐mediated immunosuppression is part of a larger miR‐200‐directed gene expression program in tumors that promotes tumor progression, which could have important implications for cancer treatment.

Original language	English (US)
Article number	e1234570
Journal	OncoImmunology
Volume	5
Issue number	11
DOIs	https://doi.org/10.1080/2162402X.2016.1234570
State	Published - Nov 1 2016

Keywords

BMP4
EMT
PD-L1
immunotherapy
lung cancer
miR-200

ASJC Scopus subject areas

Immunology and Allergy
Immunology
Oncology

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10.1080/2162402X.2016.1234570

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Chen, L., Yi, X., Goswami, S., Ahn, Y. H., Roybal, J. D., Yang, Y., Diao, L., Peng, D., Peng, D., Fradette, J. J., Wang, J., Byers, L. A., Kurie, J. M., Ullrich, S. E., Qin, F. X. F., & Gibbons, D. L. (2016). Growth and metastasis of lung adenocarcinoma is potentiated by BMP4-mediated immunosuppression. OncoImmunology, 5(11), Article e1234570. https://doi.org/10.1080/2162402X.2016.1234570

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title = "Growth and metastasis of lung adenocarcinoma is potentiated by BMP4-mediated immunosuppression",

abstract = "Cancer cells modulate the recruitment and function of inflammatory cells to create an immunosuppressive microenvironment that favors tumor growth and metastasis. However, the tumor-derived regulatory programs that promote intratumoral immunosuppression remain poorly defined. Here, we show in a KrasLA1/+p53R172HΔg/+-based mouse model that bone morphogenetic protein-4 (BMP4) augments the expression of the T cell co-inhibitory receptor ligand PD-L1 in the mesenchymal subset of lung cancer cells, leading to profound CD8+ T cell-mediated immunosuppression, producing tumor growth and metastasis. We previously reported in this model that BMP4 functions as a pro-tumorigenic factor regulated by miR-200 via GATA4/6. Thus, BMP4‐mediated immunosuppression is part of a larger miR‐200‐directed gene expression program in tumors that promotes tumor progression, which could have important implications for cancer treatment.",

keywords = "BMP4, EMT, PD-L1, immunotherapy, lung cancer, miR-200",

author = "Limo Chen and Xiaohui Yi and Sangeeta Goswami and Ahn, {Young Ho} and Roybal, {Jonathon D.} and Yongbin Yang and Lixia Diao and Di Peng and David Peng and Fradette, {Jared J.} and Jing Wang and Byers, {Lauren A.} and Kurie, {Jonathan M.} and Ullrich, {Stephen E.} and Qin, {F. Xiao Feng} and Gibbons, {Don L.}",

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doi = "10.1080/2162402X.2016.1234570",

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AU - Yang, Yongbin

AU - Diao, Lixia

AU - Peng, Di

AU - Peng, David

AU - Fradette, Jared J.

AU - Wang, Jing

AU - Byers, Lauren A.

AU - Kurie, Jonathan M.

AU - Ullrich, Stephen E.

AU - Qin, F. Xiao Feng

AU - Gibbons, Don L.

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N2 - Cancer cells modulate the recruitment and function of inflammatory cells to create an immunosuppressive microenvironment that favors tumor growth and metastasis. However, the tumor-derived regulatory programs that promote intratumoral immunosuppression remain poorly defined. Here, we show in a KrasLA1/+p53R172HΔg/+-based mouse model that bone morphogenetic protein-4 (BMP4) augments the expression of the T cell co-inhibitory receptor ligand PD-L1 in the mesenchymal subset of lung cancer cells, leading to profound CD8+ T cell-mediated immunosuppression, producing tumor growth and metastasis. We previously reported in this model that BMP4 functions as a pro-tumorigenic factor regulated by miR-200 via GATA4/6. Thus, BMP4‐mediated immunosuppression is part of a larger miR‐200‐directed gene expression program in tumors that promotes tumor progression, which could have important implications for cancer treatment.

AB - Cancer cells modulate the recruitment and function of inflammatory cells to create an immunosuppressive microenvironment that favors tumor growth and metastasis. However, the tumor-derived regulatory programs that promote intratumoral immunosuppression remain poorly defined. Here, we show in a KrasLA1/+p53R172HΔg/+-based mouse model that bone morphogenetic protein-4 (BMP4) augments the expression of the T cell co-inhibitory receptor ligand PD-L1 in the mesenchymal subset of lung cancer cells, leading to profound CD8+ T cell-mediated immunosuppression, producing tumor growth and metastasis. We previously reported in this model that BMP4 functions as a pro-tumorigenic factor regulated by miR-200 via GATA4/6. Thus, BMP4‐mediated immunosuppression is part of a larger miR‐200‐directed gene expression program in tumors that promotes tumor progression, which could have important implications for cancer treatment.

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Growth and metastasis of lung adenocarcinoma is potentiated by BMP4-mediated immunosuppression

Abstract

Keywords

ASJC Scopus subject areas

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