
Abstract
Background
Veno‑venous extracorporeal membrane oxygenation (VV‑ECMO) is associated with a high transfusion burden. While trials have concluded that red blood cell (RBC) storage does not impact patient morbidity and mortality in the critically ill or cardiac surgical cohorts, evidence is sparse for ECMO cohorts. A sheep model was to investigate this question. On an underlying injury of smoke inhalation, we compared fresh (< 5 days) or stored (35–42 days) RBC transfusion with no transfusion. Clinically relevant outcomes included pulmonary artery pressure as well as biochemical or histopathological markers of lung, liver, and renal injury.
Methods
Twenty‑four female Merino/Samm Border Leicester Cross sheep were anaesthetised and placed on pressure‑controlled ventilation. They were instrumented for continuous haemodynamic monitoring. They then underwent smoke inhalation injury, followed two hours later by veno‑venous ECMO. Sheep were randomised to three groups: control (no transfusion (n = 8)), fresh RBC (n = 8) and stored RBC (n = 8) transfusion occurring six hours after ECMO initiation. Blood samples were taken regularly, and 24 h post‑ECMO, animals were sacrificed. Post‑mortem samples of lung and kidney were collected for post‑mortem analyses.
Results
Following ECMO initiation and transfusion, pulmonary artery pressure increased in the stored RBC group. Histopathological analysis also demonstrated a significantly elevated lung injury in this group. This lung injury was characterised by greater extravasation of inflammatory cells as well as bronchiole damage and oedema. Renal histopathology showed no significant differences between groups. Alanine aminotransferase, aspartate aminotransferase and bilirubin levels increased in a time dependent manner post‑transfusion but there were no treatment‑associated differences. During experimentation, the coagulation profile changed with firmer clots forming more quickly. Differences were observed between both transfusion groups and controls.
Conclusions
Transfusion of stored RBC elevated pulmonary artery pressure when compared to fresh RBC transfusion and controls. This change was correlated with a greater post‑transfusion lung injury in the stored RBC group. Further
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