Abstract
Background Neutrophil infiltration plays a critical role in the pathogenesis of acute lung injury following liver transplantation (LT). Neutrophil elastase is released from neutrophils during pulmonary polymorphonuclear neutrophil activation and sequestration. The aim of the study was to investigate whether the inhibition of neutrophil elastase could lead to the restoration of pulmonary function following LT. Methods In in vivo experiments, lung tissue and bronchoalveolar lavage fluid (BALF) were collected at 2, 4, 8, and 24 h after rats were subjected to orthotopic autologous LT (OALT), and neutrophil infiltration was detected. Next, neutrophil elastase inhibitors, sivelestat sodium hydrate (exogenous) and serpin family B member 1 (SERPINB1) (endogenous), were administered to rats before OALT, and neutrophil infiltration, pulmonary oxidative stress, and barrier function were measured at 8 h after OALT. Results Obvious neutrophil infiltration occurred from 2 h and peaked at 8 h in the lungs of rats after they were subjected to OALT, as evidenced by an increase in naphthol-positive cells, BALF neutrophil elastase activity, and lung myeloperoxidase activity. Treatment with neutrophil elastase inhibitors, either sivelestat sodium hydrate or SERPINB1, effectively reduced lung naphthol-positive cells and BALF inflammatory cell content, increased expression of lung HO-1 and tight junction proteins ZO-1 and occludin, and increased the activity of superoxide dismutase. Conclusion Neutrophil elastase inhibitors, sivelestat sodium hydrate and SERPINB1, both reduced lung neutrophil infiltration and pulmonary oxidative stress and finally restored pulmonary barrier function.
Highlights
To date, liver transplantation (LT) is the most effective clinical therapy for end-stage liver disease [1, 2]
The results of naphthol esterase staining showed that the infiltration of lung tissue by neutrophils was obvious after LT, and the number of naphthol esterase-positive cells (Figures 1(c) and 1(d)) peaked at 8 h (T8) after orthotopic autologous LT (OALT) and gradually decreased after 24 h (T24) (p < 0:05 vs. sham)
We showed that inflammation and Neutrophil elastase (NE) infiltration were increased in the lung tissues after OALT that were associated with increased oxidative stress and severe lung injury
Summary
Liver transplantation (LT) is the most effective clinical therapy for end-stage liver disease [1, 2]. Wang et al recently found that neutrophils enter the site of liver damage after thermal cauterization using a liver thermal burn model, which leads to the removal of injured blood vessels and rebuilding of new blood vessel channels This group of neutrophils that enters the injury site neither dies nor is swallowed by macrophages but instead returns to the blood vessels and enters the lungs and bone marrow, indicating that neutrophils may play a critical role in the liver-lung axis when the liver is suffering. Neutrophil elastase inhibitors, sivelestat sodium hydrate (exogenous) and serpin family B member 1 (SERPINB1) (endogenous), were administered to rats before OALT, and neutrophil infiltration, pulmonary oxidative stress, and barrier function were measured at 8 h after OALT. Neutrophil elastase inhibitors, sivelestat sodium hydrate and SERPINB1, both reduced lung neutrophil infiltration and pulmonary oxidative stress and restored pulmonary barrier function
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