Frontiers in Immunology (Jan 2024)

Alterations in leukocyte DNA methylome are associated to immunosuppression in severe clinical phenotypes of septic patients

  • Jesús Beltrán-García,
  • Jesús Beltrán-García,
  • Jesús Beltrán-García,
  • Jesús Beltrán-García,
  • Germán Casabó-Vallés,
  • Germán Casabó-Vallés,
  • Rebeca Osca-Verdegal,
  • Rebeca Osca-Verdegal,
  • Rebeca Osca-Verdegal,
  • Rebeca Osca-Verdegal,
  • Paula Navarrete-López,
  • María Rodriguez-Gimillo,
  • María Rodriguez-Gimillo,
  • Elena Nacher-Sendra,
  • Elena Nacher-Sendra,
  • Carolina Ferrando-Sánchez,
  • Carolina Ferrando-Sánchez,
  • Eva García-López,
  • Eva García-López,
  • Federico V. Pallardó,
  • Federico V. Pallardó,
  • Federico V. Pallardó,
  • Nieves Carbonell,
  • Nieves Carbonell,
  • Salvador Mena-Mollá,
  • Salvador Mena-Mollá,
  • José Luis García-Giménez,
  • José Luis García-Giménez,
  • José Luis García-Giménez

DOI
https://doi.org/10.3389/fimmu.2023.1333705
Journal volume & issue
Vol. 14

Abstract

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IntroductionSepsis patients experience a complex interplay of host pro- and anti-inflammatory processes which compromise the clinical outcome. Despite considering the latest clinical and scientific research, our comprehension of the immunosuppressive events in septic episodes remains incomplete. Additionally, a lack of data exists regarding the role of epigenetics in modulating immunosuppression, subsequently impacting patient survival.MethodsTo advance the current understanding of the mechanisms underlying immunosuppression, in this study we explored the dynamics of DNA methylation using the Infinium Methylation EPIC v1.0 BeadChip Kit in leukocytes from patients suffering from sepsis, septic shock, and critically ill patients as controls, within the first 24 h after admission in the Intensive Care Unit of a tertiary hospital.Results and discussionEmploying two distinct analysis approaches (DMRcate and mCSEA) in comparing septic shock and critically ill patients, we identified 1,256 differentially methylated regions (DMRs) intricately linked to critical immune system pathways. The examination of the top 100 differentially methylated positions (DMPs) between septic shock and critically ill patients facilitated a clear demarcation among the three patient groups. Notably, the top 6,657 DMPs exhibited associations with organ dysfunction and lactate levels. Among the individual genes displaying significant differential methylation, IL10, TREM1, IL1B, and TNFAIP8 emerged with the most pronounced methylation alterations across the diverse patient groups when subjected to DNA bisulfite pyrosequencing analysis. These findings underscore the dynamic nature of DNA methylation profiles, highlighting the most pronounced alterations in patients with septic shock, and revealing their close association with the disease.

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