DNA methylation signatures of youth-onset type 2 diabetes and exposure to maternal diabetes

Salama, Ola E.; Hizon, Nikho; Del Vecchio, Melissa; Kolsun, Kurt; Fonseca, Mario A.; Lin, David T. S.; Urtatiz, Oscar; MacIsaac, Julia L.; Kobor, Michael S.; Sellers, Elizabeth A. C.; Dolinsky, Vernon W.; Dart, Allison B.; Jones, Meaghan J.; Wicklow, Brandy A.

DNA methylation signatures of youth-onset type 2 diabetes and exposure to maternal diabetes

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13148_2024_Article_1675.pdf(1.71 MB)

Date

2024-05-13

Authors

Salama, Ola E.

Hizon, Nikho

Del Vecchio, Melissa

Kolsun, Kurt

Fonseca, Mario A.

Lin, David T. S.

Urtatiz, Oscar

MacIsaac, Julia L.

Kobor, Michael S.

Sellers, Elizabeth A. C.

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Abstract

Abstract Objective Youth-onset type 2 diabetes (T2D) is physiologically distinct from adult-onset, but it is not clear how the two diseases differ at a molecular level. In utero exposure to maternal type 2 diabetes (T2D) is known to be a specific risk factor for youth-onset T2D. DNA methylation (DNAm) changes associated with T2D but which differ between youth- and adult-onset might delineate the impacts of T2D development at different ages and could also determine the contribution of exposure to in utero diabetes. Methods We performed an epigenome-wide analysis of DNAm on whole blood from 218 youth with T2D and 77 normoglycemic controls from the iCARE (improving renal Complications in Adolescents with type 2 diabetes through REsearch) cohort. Associations were tested using multiple linear regression models while adjusting for maternal diabetes, sex, age, BMI, smoking status, second-hand smoking exposure, cell-type proportions and genetic ancestry. Results We identified 3830 differentially methylated sites associated with youth T2D onset, of which 3794 were moderately (adjusted p-value < 0.05 and effect size estimate > 0.01) associated and 36 were strongly (adjusted p-value < 0.05 and effect size estimate > 0.05) associated. A total of 3725 of these sites were not previously reported in the EWAS Atlas as associated with T2D, adult obesity or youth obesity. Moreover, three CpGs associated with youth-onset T2D in the PFKFB3 gene were also associated with maternal T2D exposure (FDR < 0.05 and effect size > 0.01). This is the first study to link PFKFB3 and T2D in youth. Conclusion Our findings support that T2D in youth has different impacts on DNAm than adult-onset, and suggests that changes in DNAm could provide an important link between in utero exposure to maternal diabetes and the onset of T2D.

Citation

Clinical Epigenetics. 2024 May 13;16(1):65

URI

https://doi.org/10.1186/s13148-024-01675-1
http://hdl.handle.net/1993/38251

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University of Manitoba Scholarship

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