DNA methylation and gene expression of TXNIP in adult offspring of women with diabetes in pregnancy.

DNA methylation and gene expression of TXNIP in adult offspring of women with diabetes in pregnancy.

Fetal exposure to maternal diabetes increases the risk of type 2 diabetes (T2DM), possibly mediated by epigenetic mechanisms. Low blood TXNIP DNA methylation has been associated with elevated glucose levels and risk of T2DM, and increased skeletal muscle TXNIP gene expression was reported in subject...

Full description

Bibliographic Details
Main Authors: Azadeh Houshmand-Oeregaard, Line Hjort, Louise Kelstrup, Ninna S Hansen, Christa Broholm, Linn Gillberg, Tine D Clausen, Elisabeth R Mathiesen, Peter Damm, Allan Vaag
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2017-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC5659766?pdf=render
id doaj-3b0ab48dd793492296252cd892c80fc8
record_format Article
spelling doaj-3b0ab48dd793492296252cd892c80fc82020-11-25T01:45:20ZengPublic Library of Science (PLoS)PLoS ONE1932-62032017-01-011210e018703810.1371/journal.pone.0187038DNA methylation and gene expression of TXNIP in adult offspring of women with diabetes in pregnancy.Azadeh Houshmand-OeregaardLine HjortLouise KelstrupNinna S HansenChrista BroholmLinn GillbergTine D ClausenElisabeth R MathiesenPeter DammAllan VaagFetal exposure to maternal diabetes increases the risk of type 2 diabetes (T2DM), possibly mediated by epigenetic mechanisms. Low blood TXNIP DNA methylation has been associated with elevated glucose levels and risk of T2DM, and increased skeletal muscle TXNIP gene expression was reported in subjects with impaired glucose metabolism or T2DM. Subcutaneous adipose tissue (SAT) and skeletal muscle play a key role in the control of whole body glucose metabolism and insulin action. The extent to which TXNIP DNA methylation levels are decreased and/or gene expression levels increased in SAT or skeletal muscle of a developmentally programmed at-risk population is unknown.The objective of this study was to investigate TXNIP DNA methylation and gene expression in SAT and skeletal muscle, and DNA methylation in blood, from adult offspring of women with gestational diabetes (O-GDM, n = 82) or type 1 diabetes (O-T1DM, n = 67) in pregnancy compared with offspring of women from the background population (O-BP, n = 57).SAT TXNIP DNA methylation was increased (p = 0.032) and gene expression decreased (p = 0.001) in O-GDM, but these differences were attenuated after adjustment for confounders. Neither blood/muscle TXNIP DNA methylation nor muscle gene expression differed between groups.We found no evidence of decreased TXNIP DNA methylation or increased gene expression in metabolic target tissues of offspring exposed to maternal diabetes. Further studies are needed to confirm and understand the paradoxical SAT TXNIP DNA methylation and gene expression changes in O-GDM subjects.http://europepmc.org/articles/PMC5659766?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Azadeh Houshmand-Oeregaard
Line Hjort
Louise Kelstrup
Ninna S Hansen
Christa Broholm
Linn Gillberg
Tine D Clausen
Elisabeth R Mathiesen
Peter Damm
Allan Vaag
spellingShingle Azadeh Houshmand-Oeregaard
Line Hjort
Louise Kelstrup
Ninna S Hansen
Christa Broholm
Linn Gillberg
Tine D Clausen
Elisabeth R Mathiesen
Peter Damm
Allan Vaag
DNA methylation and gene expression of TXNIP in adult offspring of women with diabetes in pregnancy.
PLoS ONE
author_facet Azadeh Houshmand-Oeregaard
Line Hjort
Louise Kelstrup
Ninna S Hansen
Christa Broholm
Linn Gillberg
Tine D Clausen
Elisabeth R Mathiesen
Peter Damm
Allan Vaag
author_sort Azadeh Houshmand-Oeregaard
title DNA methylation and gene expression of TXNIP in adult offspring of women with diabetes in pregnancy.
title_short DNA methylation and gene expression of TXNIP in adult offspring of women with diabetes in pregnancy.
title_full DNA methylation and gene expression of TXNIP in adult offspring of women with diabetes in pregnancy.
title_fullStr DNA methylation and gene expression of TXNIP in adult offspring of women with diabetes in pregnancy.
title_full_unstemmed DNA methylation and gene expression of TXNIP in adult offspring of women with diabetes in pregnancy.
title_sort dna methylation and gene expression of txnip in adult offspring of women with diabetes in pregnancy.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2017-01-01
description Fetal exposure to maternal diabetes increases the risk of type 2 diabetes (T2DM), possibly mediated by epigenetic mechanisms. Low blood TXNIP DNA methylation has been associated with elevated glucose levels and risk of T2DM, and increased skeletal muscle TXNIP gene expression was reported in subjects with impaired glucose metabolism or T2DM. Subcutaneous adipose tissue (SAT) and skeletal muscle play a key role in the control of whole body glucose metabolism and insulin action. The extent to which TXNIP DNA methylation levels are decreased and/or gene expression levels increased in SAT or skeletal muscle of a developmentally programmed at-risk population is unknown.The objective of this study was to investigate TXNIP DNA methylation and gene expression in SAT and skeletal muscle, and DNA methylation in blood, from adult offspring of women with gestational diabetes (O-GDM, n = 82) or type 1 diabetes (O-T1DM, n = 67) in pregnancy compared with offspring of women from the background population (O-BP, n = 57).SAT TXNIP DNA methylation was increased (p = 0.032) and gene expression decreased (p = 0.001) in O-GDM, but these differences were attenuated after adjustment for confounders. Neither blood/muscle TXNIP DNA methylation nor muscle gene expression differed between groups.We found no evidence of decreased TXNIP DNA methylation or increased gene expression in metabolic target tissues of offspring exposed to maternal diabetes. Further studies are needed to confirm and understand the paradoxical SAT TXNIP DNA methylation and gene expression changes in O-GDM subjects.
url http://europepmc.org/articles/PMC5659766?pdf=render
work_keys_str_mv AT azadehhoushmandoeregaard dnamethylationandgeneexpressionoftxnipinadultoffspringofwomenwithdiabetesinpregnancy
AT linehjort dnamethylationandgeneexpressionoftxnipinadultoffspringofwomenwithdiabetesinpregnancy
AT louisekelstrup dnamethylationandgeneexpressionoftxnipinadultoffspringofwomenwithdiabetesinpregnancy
AT ninnashansen dnamethylationandgeneexpressionoftxnipinadultoffspringofwomenwithdiabetesinpregnancy
AT christabroholm dnamethylationandgeneexpressionoftxnipinadultoffspringofwomenwithdiabetesinpregnancy
AT linngillberg dnamethylationandgeneexpressionoftxnipinadultoffspringofwomenwithdiabetesinpregnancy
AT tinedclausen dnamethylationandgeneexpressionoftxnipinadultoffspringofwomenwithdiabetesinpregnancy
AT elisabethrmathiesen dnamethylationandgeneexpressionoftxnipinadultoffspringofwomenwithdiabetesinpregnancy
AT peterdamm dnamethylationandgeneexpressionoftxnipinadultoffspringofwomenwithdiabetesinpregnancy
AT allanvaag dnamethylationandgeneexpressionoftxnipinadultoffspringofwomenwithdiabetesinpregnancy
_version_ 1725023463627816960

Similar Items