AI Article Synopsis

  • Traumatic conditions during surgery can lead to early immune responses, potentially leading to long-lasting changes in leukocyte (white blood cell) activity and increased health risks.
  • A study involving 13 patients undergoing elective cardiac surgery showed significant differences in gene expression in T cells and monocytes before and after surgery, indicating persistent changes in the immune system.
  • Monocytes displayed specific gene expressions related to protein degradation and inflammation over time, suggesting ongoing issues that could affect recovery and health, emphasizing the need for careful clinical consideration post-surgery.

Article Abstract

Traumatic perioperative conditions may trigger early systemic responses, activate leukocytes and reprogram the immune system. We hypothesize that leukocyte activation may not revert to pre-surgical states, and that protracted activation may emerge with increased risks of comorbidities. We tested this concept by examining the transcriptomes of monocytes and T cells in a representative observational cohort of patients (n = 13) admitted for elective cardiac surgery. Transcriptomes in T cells and monocytes were compared from before surgery (t), and monocytes were analyzed longitudinally after acute (t), and convalescent (t) time points. Monocytes and T cells expressed distinct transcriptomes, reflected by statistically significant differential expression of 558 T cell related genes. Monocytes expressed genes related to protein degradation and presented atypical activation of surface markers and cytoplasmic functions over time. Additionally, monocytes exhibited limited transcriptomic heterogeneity prior to surgery, and long-term patterns of gene expression associated with atherosclerosis showed three temporally distinct signatures. These data establish that post-cardiac surgery transcriptomes of monocytes differ even at three months compared to baselines, which may reflect latent ('smoldering') inflammation and persistent progression of tissue degenerative processes that should inform clinical care.

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Source
http://dx.doi.org/10.1016/j.ygeno.2024.110878DOI Listing

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