Association of pronounced Elevation of NET formation and Nucleosome Biomarkers with Mortality in Patients with Septic Shock

Author:

Rahimi Muzhda Haem1,Bidar Frank2,Lukaszewicz Anne-Claire1,Garnier Lorna3,Payen-Gay Léa4,Venet Fabienne2,Monneret Guillaume2

Affiliation:

1. Université de Lyon, Université Claude Bernard Lyon_1

2. Hospices Civils de Lyon

3. Hospices Civils de Lyon, CH Lyon-Sud

4. Claude Bernard University Lyon I

Abstract

Abstract Background: Understanding the mechanisms underlying immune dysregulation in sepsis is a major challenge in developing more individualized therapy, as early and persistent inflammation, as well as immunosuppression, play a significant role in pathophysiology. As part of the antimicrobial response, neutrophils can release extracellular traps (NETs) which neutralize and kill microorganisms. However, excessive NETs formation may also contribute to pathogenesis, tissue damage and organ dysfunction. Recently, a novel automated assay has been proposed for the routine measurement of nucleosomes H3.1 (fundamental units of chromatin) that are released during NETs formation. The aim of the present study was to measure nucleosome levels in septic shock patients and to determine association with mortality. Methods: 151 septic shock patients (SEPSIS-3 definition, IMMUNOSEPSIS cohort) were included. Plasma samples were obtained at 3 time-points (day 1-2, 3-4, 6-8 after admission). Nucleosomes H3.1 were measured using a chemiluminescent immunoassay. IL-6 and immunological cellular parameters were concomitantly assessed. Results: The nucleosome H3.1 levels were markedly and significantly elevated at all-time points compared to the control group. Immunological parameters indicated tremendous early inflammation (IL-6 = 1335 pg/mL at day 1-2) along with marked immunosuppression (e.g., mHLA-DR = 3853 AB/C and CD4 = 338 /µL at day 3-4). We found significantly positive correlation between nucleosome levels and organ failure and severity scores, IL-6 concentrations and neutrophil count. Significantly higher values (day 1-2 & 3-4) were measured in non-survivor patients (28-day mortality). This association was still significant after multivariate analysis and was more pronounced with highest concentration. Early (day 1-2) increased nucleosome levels were also independently associated with 5-day mortality. At day 6-8, persistent elevated nucleosome levels were negatively correlated to mHLA-DR values. Conclusions: This study reports a significant elevation of nucleosome in patients during a one-week follow-up. The nucleosome levels showed correlation with neutrophil count, IL-6 and were found to be independently associated with mortality assessed at day 5 or 28. Therefore, nucleosome concentration seems to be a promising biomarker for detecting hyper-inflammatory phenotype upon a patient's admission. Additional investigations are required to evaluate the potential association between sustained elevation of nucleosome and sepsis-induced immunosuppression.

Publisher

Research Square Platform LLC

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