Downregulation of IFNG in CD4(+) T Cells in Lung Cancer through Hypermethylation: A Possible Mechanism of Tumor-Induced Immunosuppression

Tumor survival is significantly correlated with the immune response of patients. IFNG plays an important role in the tumor host response and decreased IFNG expression is often observed in lung cancer. Studies have shown that CpG island hypermethylation plays a critical role in transcriptional silenc...

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Autores principales: Wang, Fang, Xu, Jian, Zhu, Quan, Qin, Xuejun, Cao, Yan, Lou, Jiangfang, Xu, Yuqiao, Ke, Xing, Li, Qing, Xie, Erfu, Zhang, Lixia, Sun, Ruihong, Chen, Liang, Fang, Bingliang, Pan, Shiyang
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3823966/
https://www.ncbi.nlm.nih.gov/pubmed/24244422
http://dx.doi.org/10.1371/journal.pone.0079064
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author Wang, Fang
Xu, Jian
Zhu, Quan
Qin, Xuejun
Cao, Yan
Lou, Jiangfang
Xu, Yuqiao
Ke, Xing
Li, Qing
Xie, Erfu
Zhang, Lixia
Sun, Ruihong
Chen, Liang
Fang, Bingliang
Pan, Shiyang
author_facet Wang, Fang
Xu, Jian
Zhu, Quan
Qin, Xuejun
Cao, Yan
Lou, Jiangfang
Xu, Yuqiao
Ke, Xing
Li, Qing
Xie, Erfu
Zhang, Lixia
Sun, Ruihong
Chen, Liang
Fang, Bingliang
Pan, Shiyang
author_sort Wang, Fang
collection PubMed
description Tumor survival is significantly correlated with the immune response of patients. IFNG plays an important role in the tumor host response and decreased IFNG expression is often observed in lung cancer. Studies have shown that CpG island hypermethylation plays a critical role in transcriptional silencing of IFNG gene expression. However, there is limited understanding regarding the molecular mechanisms of altered methylation, and whether the tumor microenvironment has any effect on DNA methylation and IFNG production. In the current study, we demonstrate that plasma and intra-cellular IFNG levels are significantly lower in lung cancer patients. Hypermethylation of the IFNG promoter in CD4(+) T cells and plasma IFNG was negatively correlated. CD4(+) T cells from healthy individuals co-cultured with SPC-A1 cells generated lower levels of IFNG after activation, elevated expression of DNA methyltransferases (DNMTs), and exhibited hypermethylation of the IFNG promoter. In conclusion, decreased IFNG expression of CD4(+) T cells co-cultured with lung cancer cell is associated with IFNG promoter hypermethylation. Our study suggests that interaction between lung cancer cells and CD4(+) T cells induces DNMT expression and IFNG promoter hypermethylation in CD4(+) T cell, which may serve as an important mechanism of tumor-induced immunosuppression.
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spelling pubmed-38239662013-11-15 Downregulation of IFNG in CD4(+) T Cells in Lung Cancer through Hypermethylation: A Possible Mechanism of Tumor-Induced Immunosuppression Wang, Fang Xu, Jian Zhu, Quan Qin, Xuejun Cao, Yan Lou, Jiangfang Xu, Yuqiao Ke, Xing Li, Qing Xie, Erfu Zhang, Lixia Sun, Ruihong Chen, Liang Fang, Bingliang Pan, Shiyang PLoS One Research Article Tumor survival is significantly correlated with the immune response of patients. IFNG plays an important role in the tumor host response and decreased IFNG expression is often observed in lung cancer. Studies have shown that CpG island hypermethylation plays a critical role in transcriptional silencing of IFNG gene expression. However, there is limited understanding regarding the molecular mechanisms of altered methylation, and whether the tumor microenvironment has any effect on DNA methylation and IFNG production. In the current study, we demonstrate that plasma and intra-cellular IFNG levels are significantly lower in lung cancer patients. Hypermethylation of the IFNG promoter in CD4(+) T cells and plasma IFNG was negatively correlated. CD4(+) T cells from healthy individuals co-cultured with SPC-A1 cells generated lower levels of IFNG after activation, elevated expression of DNA methyltransferases (DNMTs), and exhibited hypermethylation of the IFNG promoter. In conclusion, decreased IFNG expression of CD4(+) T cells co-cultured with lung cancer cell is associated with IFNG promoter hypermethylation. Our study suggests that interaction between lung cancer cells and CD4(+) T cells induces DNMT expression and IFNG promoter hypermethylation in CD4(+) T cell, which may serve as an important mechanism of tumor-induced immunosuppression. Public Library of Science 2013-11-11 /pmc/articles/PMC3823966/ /pubmed/24244422 http://dx.doi.org/10.1371/journal.pone.0079064 Text en © 2013 Wang et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Wang, Fang
Xu, Jian
Zhu, Quan
Qin, Xuejun
Cao, Yan
Lou, Jiangfang
Xu, Yuqiao
Ke, Xing
Li, Qing
Xie, Erfu
Zhang, Lixia
Sun, Ruihong
Chen, Liang
Fang, Bingliang
Pan, Shiyang
Downregulation of IFNG in CD4(+) T Cells in Lung Cancer through Hypermethylation: A Possible Mechanism of Tumor-Induced Immunosuppression
title Downregulation of IFNG in CD4(+) T Cells in Lung Cancer through Hypermethylation: A Possible Mechanism of Tumor-Induced Immunosuppression
title_full Downregulation of IFNG in CD4(+) T Cells in Lung Cancer through Hypermethylation: A Possible Mechanism of Tumor-Induced Immunosuppression
title_fullStr Downregulation of IFNG in CD4(+) T Cells in Lung Cancer through Hypermethylation: A Possible Mechanism of Tumor-Induced Immunosuppression
title_full_unstemmed Downregulation of IFNG in CD4(+) T Cells in Lung Cancer through Hypermethylation: A Possible Mechanism of Tumor-Induced Immunosuppression
title_short Downregulation of IFNG in CD4(+) T Cells in Lung Cancer through Hypermethylation: A Possible Mechanism of Tumor-Induced Immunosuppression
title_sort downregulation of ifng in cd4(+) t cells in lung cancer through hypermethylation: a possible mechanism of tumor-induced immunosuppression
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3823966/
https://www.ncbi.nlm.nih.gov/pubmed/24244422
http://dx.doi.org/10.1371/journal.pone.0079064
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