Epigenetics of neuroinflammation: Immune response, inflammatory response and cholinergic synaptic involvement evidenced by genome-wide DNA methylation analysis of delirious inpatients

Taku Saito, Hiroyuki Toda, Gabrielle N. Duncan, Sydney S. Jellison, Tong Yu, Mason J. Klisares, Sophia Daniel, Allison J. Andreasen, Lydia R. Leyden, Mandy M. Hellman, Eri Shinozaki, Sangil Lee, Aihide Yoshino, Hyunkeun R. Cho, Gen Shinozaki

Research output: Contribution to journalArticlepeer-review

19 Scopus citations

Abstract

Previously our study has shown that the DNA methylation (DNAm) levels at CpG sites in the pro-inflammatory cytokine gene, TNF-alpha, decrease along with aging, suggesting the potential role of DNAm in aging and heightened inflammatory process leading to increased risk for delirium. However, DNAm differences between delirium cases and non-delirium controls have not been investigated directly. Therefore, we examined genome-wide DNAm differences in blood between patients with delirium and controls to identify useful epigenetic biomarkers for delirium. Data from a total of 87 subjects (43 delirium cases) were analyzed by a genome-wide DNAm case-control association study. A genome-wide significant CpG site near the gene of LDLRAD4 was identified (p = 5.07E-8). In addition, over-representation analysis showed several significant pathways with a false discovery rate adjusted p-value < 0.05. The top pathway with a Gene Ontology term was immune response, and the second top pathway with a Kyoto Encyclopedia of Genes and Genomes term was cholinergic synapse. Significant DNAm differences related to immune/inflammatory response were shown both at gene and pathway levels between patients with delirium and non-delirium controls. This finding indicates that DNAm status in blood has the potential to be used as epigenetic biomarkers for delirium.

Original languageEnglish
Pages (from-to)61-65
Number of pages5
JournalJournal of Psychiatric Research
Volume129
DOIs
StatePublished - Oct 2020

Keywords

  • Aging
  • Delirium
  • Genome-wide DNA methylation
  • Immune response
  • Inflammatory response

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