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Aging-dependent DNA hypermethylation and gene expression of GSTM1 involved in T cell differentiation

This study investigated whether aging was associated with epigenetic changes of DNA hypermethylation on immune gene expression and lymphocyte differentiation. We screened CG sites of methylation in blood leukocytes from different age populations, picked up genes with age-related increase of CG methy...

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Autores principales: Yeh, Shu-Hui, Liu, Cheng-Ling, Chang, Ren-Chieh, Wu, Chih-Chiang, Lin, Chia-Hsueh, Yang, Kuender D.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5564710/
https://www.ncbi.nlm.nih.gov/pubmed/28596482
http://dx.doi.org/10.18632/oncotarget.18109
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author Yeh, Shu-Hui
Liu, Cheng-Ling
Chang, Ren-Chieh
Wu, Chih-Chiang
Lin, Chia-Hsueh
Yang, Kuender D.
author_facet Yeh, Shu-Hui
Liu, Cheng-Ling
Chang, Ren-Chieh
Wu, Chih-Chiang
Lin, Chia-Hsueh
Yang, Kuender D.
author_sort Yeh, Shu-Hui
collection PubMed
description This study investigated whether aging was associated with epigenetic changes of DNA hypermethylation on immune gene expression and lymphocyte differentiation. We screened CG sites of methylation in blood leukocytes from different age populations, picked up genes with age-related increase of CG methylation content more than 15%, and validated immune related genes with CG hypermethylation involved in lymphocyte differentiation in the aged population. We found that 12 genes (EXHX1、 IL-10、 TSP50、 GSTM1、SLC5A5、SPI1、F2R、LMO2、PTPN6、FGFR2、MMP9、MET) were associated with promoter or exon one DNA hypermethylation in the aged group. Two immune related genes, GSTM1 and LMO2, were chosen to validate its aging-related CG hypermethylation in different leukocytes. We are the first to validate that GSTM1_P266 and LMO2_E128 CG methylation contents in T lymphocytes but not polymorphonuclear cells (PMNs) or mononuclear cells (MNCs) were significantly increased in the aged population. The GSTM1 mRNA expression in T lymphocytes but not PMNs or MNCs was inversely associated with the GSTM1 CG hypermethylation levels in the aged population studied. Further studies showed that lower GSTM1 CG methylation content led to the higher GSTM1 mRNA expression in T cells and knockdown of GSTM1 mRNA expression decreased type 1 T helper cell (Th1) differentiation in Jurkat T cells and normal adult CD4 T cells. The GSTM1_P266 hypermethylation in the aged population associated with lower GSTM1 mRNA expression was involved in Th1 differentiation, highlighting that modulation of aging-associated GSTM1 methylation may be able to enhance T helper cell immunity in the elders.
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spelling pubmed-55647102017-08-23 Aging-dependent DNA hypermethylation and gene expression of GSTM1 involved in T cell differentiation Yeh, Shu-Hui Liu, Cheng-Ling Chang, Ren-Chieh Wu, Chih-Chiang Lin, Chia-Hsueh Yang, Kuender D. Oncotarget Research Paper: Gerotarget (Focus on Aging) This study investigated whether aging was associated with epigenetic changes of DNA hypermethylation on immune gene expression and lymphocyte differentiation. We screened CG sites of methylation in blood leukocytes from different age populations, picked up genes with age-related increase of CG methylation content more than 15%, and validated immune related genes with CG hypermethylation involved in lymphocyte differentiation in the aged population. We found that 12 genes (EXHX1、 IL-10、 TSP50、 GSTM1、SLC5A5、SPI1、F2R、LMO2、PTPN6、FGFR2、MMP9、MET) were associated with promoter or exon one DNA hypermethylation in the aged group. Two immune related genes, GSTM1 and LMO2, were chosen to validate its aging-related CG hypermethylation in different leukocytes. We are the first to validate that GSTM1_P266 and LMO2_E128 CG methylation contents in T lymphocytes but not polymorphonuclear cells (PMNs) or mononuclear cells (MNCs) were significantly increased in the aged population. The GSTM1 mRNA expression in T lymphocytes but not PMNs or MNCs was inversely associated with the GSTM1 CG hypermethylation levels in the aged population studied. Further studies showed that lower GSTM1 CG methylation content led to the higher GSTM1 mRNA expression in T cells and knockdown of GSTM1 mRNA expression decreased type 1 T helper cell (Th1) differentiation in Jurkat T cells and normal adult CD4 T cells. The GSTM1_P266 hypermethylation in the aged population associated with lower GSTM1 mRNA expression was involved in Th1 differentiation, highlighting that modulation of aging-associated GSTM1 methylation may be able to enhance T helper cell immunity in the elders. Impact Journals LLC 2017-05-23 /pmc/articles/PMC5564710/ /pubmed/28596482 http://dx.doi.org/10.18632/oncotarget.18109 Text en Copyright: © 2017 Yeh et al. http://creativecommons.org/licenses/by/3.0/ This article is distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/3.0/) (CC-BY), which permits unrestricted use and redistribution provided that the original author and source are credited.
spellingShingle Research Paper: Gerotarget (Focus on Aging)
Yeh, Shu-Hui
Liu, Cheng-Ling
Chang, Ren-Chieh
Wu, Chih-Chiang
Lin, Chia-Hsueh
Yang, Kuender D.
Aging-dependent DNA hypermethylation and gene expression of GSTM1 involved in T cell differentiation
title Aging-dependent DNA hypermethylation and gene expression of GSTM1 involved in T cell differentiation
title_full Aging-dependent DNA hypermethylation and gene expression of GSTM1 involved in T cell differentiation
title_fullStr Aging-dependent DNA hypermethylation and gene expression of GSTM1 involved in T cell differentiation
title_full_unstemmed Aging-dependent DNA hypermethylation and gene expression of GSTM1 involved in T cell differentiation
title_short Aging-dependent DNA hypermethylation and gene expression of GSTM1 involved in T cell differentiation
title_sort aging-dependent dna hypermethylation and gene expression of gstm1 involved in t cell differentiation
topic Research Paper: Gerotarget (Focus on Aging)
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5564710/
https://www.ncbi.nlm.nih.gov/pubmed/28596482
http://dx.doi.org/10.18632/oncotarget.18109
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