Frontiers in Immunology (Sep 2021)

Whole-Blood Mitochondrial DNA Copies Are Associated With the Prognosis of Acute Respiratory Distress Syndrome After Sepsis

  • Tamara Hernández-Beeftink,
  • Tamara Hernández-Beeftink,
  • Beatriz Guillen-Guio,
  • Héctor Rodríguez-Pérez,
  • Itahisa Marcelino-Rodríguez,
  • Jose M. Lorenzo-Salazar,
  • Almudena Corrales,
  • Almudena Corrales,
  • Miryam Prieto-González,
  • Aurelio Rodríguez-Pérez,
  • Aurelio Rodríguez-Pérez,
  • Demetrio Carriedo,
  • Jesús Blanco,
  • Jesús Blanco,
  • Alfonso Ambrós,
  • Elena González-Higueras,
  • Nancy G. Casanova,
  • Manuel González-Garay,
  • Elena Espinosa,
  • Arturo Muriel,
  • David Domínguez,
  • Abelardo García de Lorenzo,
  • José M. Añón,
  • José M. Añón,
  • Marina Soro,
  • Javier Belda,
  • Joe G. N. Garcia,
  • Jesús Villar,
  • Jesús Villar,
  • Carlos Flores,
  • Carlos Flores,
  • Carlos Flores

DOI
https://doi.org/10.3389/fimmu.2021.737369
Journal volume & issue
Vol. 12

Abstract

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Acute respiratory distress syndrome (ARDS) is an inflammatory process of the lungs that develops primarily in response to pulmonary or systemic sepsis, resulting in a disproportionate death toll in intensive care units (ICUs). Given its role as a critical activator of the inflammatory and innate immune responses, previous studies have reported that an increase of circulating cell-free mitochondrial DNA (mtDNA) is a biomarker for fatal outcome in the ICU. Here we analyzed the association of whole-blood mtDNA (wb-mtDNA) copies with 28-day survival from sepsis and sepsis-associated ARDS. We analyzed mtDNA data from 687 peripheral whole-blood samples within 24 h of sepsis diagnosis from unrelated Spanish patients with sepsis (264 with ARDS) included in the GEN-SEP study. The wb-mtDNA copies were obtained from the array intensities of selected probes, with 100% identity with mtDNA and with the largest number of mismatches with the nuclear sequences, and normalized across the individual-probe intensities. We used Cox regression models for testing the association with 28-day survival. We observed that wb-mtDNA copies were significantly associated with 28-day survival in ARDS patients (hazard ratio = 3.65, 95% confidence interval = 1.39–9.59, p = 0.009) but not in non-ARDS patients. Our findings support that wb-mtDNA copies at sepsis diagnosis could be considered an early prognostic biomarker in sepsis-associated ARDS patients. Future studies will be needed to evaluate the mechanistic links of this observation with the pathogenesis of ARDS.

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