Literature DB >> 32687192

Exposure to Gestational Diabetes Enriches Immune-Related Pathways in the Transcriptome and Methylome of Human Amniocytes.

Sara E Pinney1,2,3,4, Apoorva Joshi1, Victoria Yin2, So Won Min2, Cetewayo Rashid5, David E Condon6, Paul Zhipang Wang4,7.   

Abstract

CONTEXT: Gestational diabetes (GDM) has profound effects on the intrauterine metabolic milieu and is linked to obesity and diabetes in offspring, but the mechanisms driving these effects remain largely unknown. Alterations in DNA methylation and gene expression in amniocytes exposed to GDM in utero represent a potential mechanism leading to metabolic dysfunction later in life.
OBJECTIVE: To profile changes in genome-wide DNA methylation and expression in human amniocytes exposed to GDM.
DESIGN: A nested case-control study (n = 14 pairs) was performed in amniocytes matched for offspring sex, maternal race/ethnicity, maternal age, gestational age at amniocentesis, and gestational age at birth. Sex-specific genome-wide DNA methylation analysis and RNA-sequencing were completed and differentially methylated regions (DMRs) and gene expression changes were identified. Ingenuity pathway analysis identified biologically relevant pathways enriched after GDM exposure. In silico high-throughput chromosome conformation capture (Hi-C) analysis identified potential chromatin interactions with DMRs.
RESULTS: Expression of interferon-stimulated genes was increased in GDM amniocytes, accounting for 6 of the top 10 altered genes (q < 0.05). Enriched biological pathways in GDM amniocytes included pathways involving inflammation, the interferon response, fatty liver disease, monogenic diabetes, and atherosclerosis. Forty-two DMRs were identified in male GDM-exposed amniocytes and 20 in female amniocyte analysis (q < 0.05). Hi-C analysis identified interactions between DMRs and 11 genes with significant expression changes in male amniocytes and 9 in female amniocytes (P < .05).
CONCLUSION: In a unique repository of human amniocytes exposed to GDM in utero, transcriptome analysis identified enrichment of inflammation and interferon-related pathways and novel DMRs with potential distal regulatory functions. © Endocrine Society 2020. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.

Entities:  

Keywords:  DNA methylation; epigenetics; fetal programming; gestational diabetes; immune activation; interferon

Mesh:

Substances:

Year:  2020        PMID: 32687192      PMCID: PMC7451504          DOI: 10.1210/clinem/dgaa466

Source DB:  PubMed          Journal:  J Clin Endocrinol Metab        ISSN: 0021-972X            Impact factor:   5.958


  48 in total

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4.  Intrauterine exposure to diabetes conveys risks for type 2 diabetes and obesity: a study of discordant sibships.

Authors:  D Dabelea; R L Hanson; R S Lindsay; D J Pettitt; G Imperatore; M M Gabir; J Roumain; P H Bennett; W C Knowler
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6.  Development of type 2 diabetes following intrauterine growth retardation in rats is associated with progressive epigenetic silencing of Pdx1.

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7.  Gene Expression and DNA Methylation of PPARGC1A in Muscle and Adipose Tissue From Adult Offspring of Women With Diabetes in Pregnancy.

Authors:  Louise Kelstrup; Line Hjort; Azadeh Houshmand-Oeregaard; Tine D Clausen; Ninna S Hansen; Christa Broholm; Liv Borch-Johnsen; Elisabeth R Mathiesen; Allan A Vaag; Peter Damm
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9.  Enhanced reduced representation bisulfite sequencing for assessment of DNA methylation at base pair resolution.

Authors:  Francine E Garrett-Bakelman; Caroline K Sheridan; Thadeous J Kacmarczyk; Jennifer Ishii; Doron Betel; Alicia Alonso; Christopher E Mason; Maria E Figueroa; Ari M Melnick
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10.  Offspring sex impacts DNA methylation and gene expression in placentae from women with diabetes during pregnancy.

Authors:  Jacqueline Alexander; April M Teague; Jing Chen; Christopher E Aston; Yuet-Kin Leung; Steven Chernausek; Rebecca A Simmons; Sara E Pinney
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Review 4.  The link between gestational diabetes and cardiovascular diseases: potential role of extracellular vesicles.

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