Lung Transplantation Clinical Trial
Bronchiolitis obliterable syndrome (BOS) is the most common cause of death in long-term
survivors after lung transplantation and refractory to most interventions. Many risk factor
for BOS were identified in previous studies such as acute cellular rejection, lymphocytic
bronchiolitis, cytomegalovirus (CMV) and non-CMV respiratory infections, injury to the
allograft or airways, Primary graft dysfunction, HLA mismatching, and organizing pneumonia.
(Belperio JA. et al.). Neutrophils and their released products may be involved in the
development of BOS. Neutrophilia was repeatedly observed in the bronchoalveolar lavage fluid
of patients after lung transplantation. In addition, infiltration of neutrophils into the
bronchial epithelium has been detected in patients with higher degrees of active airway
damage. Neutrophils are capable of causing severe damage to the lung tissue by releasing
toxic proteases and reactive oxygen species if not counterbalanced by the antiprotease/
antioxidant screen of the lung. Based on this background, a causal relationship between
neutrophilia and the development of BOS has been proposed. (Hirsch J. et al.) Detection of
unopposed Neutrophile elastase (NE) activity in BAL appears to correlate with poor outcome
due to refractory BOS. Unopposed NE in these subjects may not only serve as a marker of
evolving graft dysfunction but also participate in damaging the airways of the allograft and
inhibit adequate bacterial clearance. Prevention of neutrophil sequestration or inhibition
of NE may prevent or attenuate airway damage and improve bacterial clearance mechanisms.
(Nutley D et al.) These data demonstrate the importance of neutrophils and unopposed NE in
the pathogenesis of BOS and call for new approach to prevent or modulate BOS targeting this
mechanism.
AAT is the main inhibitor of neutrophil elastase in the lower airways and patients with AAT
deficiency have low concentrations of the protein in this region of the lung. This explains
the proteinase/antiproteinase theory of the development of emphysema in deficient patients
in which the amount of elastase released in the lung exceeds the amount of AAT. The net
result is persistence of elastase activity leading to lung destruction and the pathological
changes of emphysema. (Abusriwil H. et al.) The administration of the AAT is to address
proteinase/antiproteinase imbalance.
Administration of AAT will help to prevent further destruction of the lung architecture and
reduce the inflammatory dysregulation that causes pulmonary dysfunction. It is expected that
by attacking a specific and previously untreated key component part of the
pathophysiological cycle of BOS, AAT therapy would decrease the prevalence of BOS in lung
transplant recipients and prolong life expectancy of these patients.
n/a
Allocation: Non-Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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