Correlation between Neutrophil Extracellular Traps (NETs) Expression and Primary Graft Dysfunction Following Human Lung Transplantation

Author:

Bonneau Steven,Landry Caroline,Bégin Stéphanie,Adam Damien,Villeneuve Louis,Clavet-Lanthier Marie-Élaine,Dasilva Ariane,Charles Elcha,Dumont Benjamin L.,Neagoe Paul-Eduard,Brochiero Emmanuelle,Menaouar Ahmed,Nasir Basil,Stevens Louis-Mathieu,Ferraro Pasquale,Noiseux Nicolas,Sirois Martin G.ORCID

Abstract

Primary graft dysfunction (PGD) is characterized by alveolar epithelial and vascular endothelial damage and inflammation, lung edema and hypoxemia. Up to one-third of recipients develop the most severe form of PGD (Grade 3; PGD3). Animal studies suggest that neutrophils contribute to the inflammatory process through neutrophil extracellular traps (NETs) release (NETosis). NETs are composed of DNA filaments decorated with granular proteins contributing to vascular occlusion associated with PGD. The main objective was to correlate NETosis in PGD3 (n = 9) versus non-PGD3 (n = 27) recipients in an exploratory study. Clinical data and blood samples were collected from donors and recipients pre-, intra- and postoperatively (up to 72 h). Inflammatory inducers of NETs’ release (IL-8, IL-6 and C-reactive protein [CRP]) and components (myeloperoxidase [MPO], MPO-DNA complexes and cell-free DNA [cfDNA]) were quantified by ELISA. When available, histology, immunohistochemistry and immunofluorescence techniques were performed on lung biopsies from donor grafts collected during the surgery to evaluate the presence of activated neutrophils and NETs. Lung biopsies from donor grafts collected during transplantation presented various degrees of vascular occlusion including neutrophils undergoing NETosis. Additionally, in recipients intra- and postoperatively, circulating inflammatory (IL-6, IL-8) and NETosis biomarkers (MPO-DNA, MPO, cfDNA) were up to 4-fold higher in PGD3 recipients compared to non-PGD3 (p = 0.041 to 0.001). In summary, perioperative elevation of NETosis biomarkers is associated with PGD3 following human lung transplantation and these biomarkers might serve to identify recipients at risk of PGD3 and initiate preventive therapies.

Funder

Université de Montréal studentship

Canadian Institutes of Health Research

Fonds de recherche du Québec-Santé

Thoracic Surgery Research Foundation of Montreal

Montreal Heart Institute Foundation

Quebec Respiratory Health Research Network

Publisher

MDPI AG

Subject

General Medicine

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