DNA damage response profile distinguishes poor-acting gliomas with shared methylome signatures
Nalin Leelatian, Charu Singh, Richard Bouffard, Ranjini K Sundaram, Kirsten E Diggins, William Sullivan, Sateja Paradkar, Zeynep Erson Omay, Bret C Mobley, Susan E Gueble, Juan C Vasquez, Ranjit S Bindra

TL;DR
This study shows that DNA damage response patterns in gliomas can predict poor outcomes and may help guide treatment strategies.
Contribution
The study introduces DDR epigenetic and transcriptional signatures as novel biomarkers for glioma prognosis and treatment.
Findings
Two DDR methylation groups correlate with IDH mutation status and molecular glioma subtypes.
High DDR transcription across pathways is linked to poor survival independent of IDH or MGMT status.
Intratumoral DDR diversity and high DDR protein expression in proliferative cells associate with worse outcomes.
Abstract
Therapies for diffuse glioma induce DNA damage response (DDR), and strategies to exploit DDR defects are active areas of investigation. While global DNA methylation profiling effectively classifies gliomas into subtypes, the epigenetic and gene expression patterns of DDR genes, and their contribution to tumor classification and outcomes, have yet to be fully elucidated. Thus, dissecting the DDR epigenetics, gene expression, and single-cell heterogeneity may reveal key molecular characteristics, refine prognosis, and identify novel treatment strategies and resistance mechanisms. We characterized DDR epigenetics and gene expression of TCGA glioblastomas (GBM) and low-grade gliomas (LGG). Single-cell protein analysis by imaging mass cytometry (IMC) was performed on a separate cohort of 118 diffuse gliomas. Analysis of TCGA cohorts revealed two DDR methylation groups that correlated with…
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Taxonomy
TopicsGlioma Diagnosis and Treatment · Chromatin Remodeling and Cancer · Cancer Genomics and Diagnostics
