DNA methylation as a pharmacodynamic marker of glucocorticoid response and glioma survival

Author:

Wiencke J. K.ORCID,Molinaro Annette M.ORCID,Warrier GayathriORCID,Rice Terri,Clarke JenniferORCID,Taylor Jennie W.ORCID,Wrensch Margaret,Hansen HelenORCID,McCoy LucieORCID,Tang EmilyORCID,Tamaki Stan J.,Tamaki Courtney M.,Nissen EmilyORCID,Bracci Paige,Salas Lucas A.ORCID,Koestler Devin C.,Christensen Brock C.,Zhang ZeORCID,Kelsey Karl T.ORCID

Abstract

AbstractAssessing individual responses to glucocorticoid drug therapies that compromise immune status and affect survival outcomes in neuro-oncology is a great challenge. Here we introduce a blood-based neutrophil dexamethasone methylation index (NDMI) that provides a measure of the epigenetic response of subjects to dexamethasone. This marker outperforms conventional approaches based on leukocyte composition as a marker of glucocorticoid response. The NDMI is associated with low CD4 T cells and the accumulation of monocytic myeloid-derived suppressor cells and also serves as prognostic factor in glioma survival. In a non-glioma population, the NDMI increases with a history of prednisone use. Therefore, it may also be informative in other conditions where glucocorticoids are employed. We conclude that DNA methylation remodeling within the peripheral immune compartment is a rich source of clinically relevant markers of glucocorticoid response.

Funder

U.S. Department of Health & Human Services | National Institutes of Health

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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