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Evaluation of cross-platform compatibility of a DNA methylation-based glucocorticoid response biomarker.

Authors :
Tang, Emily
Tang, Emily
Wiencke, John K
Warrier, Gayathri
Hansen, Helen
McCoy, Lucie
Rice, Terri
Bracci, Paige M
Wrensch, Margaret
Taylor, Jennie W
Clarke, Jennifer L
Koestler, Devin C
Salas, Lucas A
Christensen, Brock C
Kelsey, Karl T
Molinaro, Annette M
Tang, Emily
Tang, Emily
Wiencke, John K
Warrier, Gayathri
Hansen, Helen
McCoy, Lucie
Rice, Terri
Bracci, Paige M
Wrensch, Margaret
Taylor, Jennie W
Clarke, Jennifer L
Koestler, Devin C
Salas, Lucas A
Christensen, Brock C
Kelsey, Karl T
Molinaro, Annette M
Source :
Clinical epigenetics; vol 14, iss 1, 136; 1868-7075
Publication Year :
2022

Abstract

Identifying blood-based DNA methylation patterns is a minimally invasive way to detect biomarkers in predicting age, characteristics of certain diseases and conditions, as well as responses to immunotherapies. As microarray platforms continue to evolve and increase the scope of CpGs measured, new discoveries based on the most recent platform version and how they compare to available data from the previous versions of the platform are unknown. The neutrophil dexamethasone methylation index (NDMI 850) is a blood-based DNA methylation biomarker built on the Illumina MethylationEPIC (850K) array that measures epigenetic responses to dexamethasone (DEX), a synthetic glucocorticoid often administered for inflammation. Here, we compare the NDMI 850 to one we built using data from the Illumina Methylation 450K (NDMI 450). The NDMI 450 consisted of 22 loci, 15 of which were present on the NDMI 850. In adult whole blood samples, the linear composite scores from NDMI 450 and NDMI 850 were highly correlated and had equivalent predictive accuracy for detecting DEX exposure among adult glioma patients and non-glioma adult controls. However, the NDMI 450 scores of newborn cord blood were significantly lower than NDMI 850 in samples measured with both assays. We developed an algorithm that reproduces the DNA methylation glucocorticoid response score using 450K data, increasing the accessibility for researchers to assess this biomarker in archived or publicly available datasets that use the 450K version of the Illumina BeadChip array. However, the NDMI850 and NDMI450 do not give similar results in cord blood, and due to data availability limitations, results from sample types of newborn cord blood should be interpreted with care.

Details

Database :
OAIster
Journal :
Clinical epigenetics; vol 14, iss 1, 136; 1868-7075
Notes :
application/pdf, Clinical epigenetics vol 14, iss 1, 136 1868-7075
Publication Type :
Electronic Resource
Accession number :
edsoai.on1391586128
Document Type :
Electronic Resource