Bronchiolitis Obliterans Syndrome Clinical Trial
Official title:
Early Detection and Management of Bronchiolitis Obliterans Syndrome Following Pediatric Hematopoietic Stem Cell Transplantation
This study aims to determine whether or not early spirometric detection and management of obstructive lung disease with combined fluticasone/azithromycin/montelukast therapy (FAM) can attenuate declining lung function, prevent the development of bronchiolitis obliterans, and improve patient outcomes following hematopoietic stem cell transplant.
Bronchiolitis obliterans syndrome (BOS) is an inflammatory condition of the lungs that leads
to obstructive physiology, irreversible fibrosis of terminal bronchioles, and obliteration
of the small airways. In both children and adults, the prevalence of BOS is approximately 6%
in those with chronic graft-vs-host disease (cGVHD), although this may be a gross
underestimation given current diagnostic guidelines. Once diagnosed, the prognosis is
extremely unfavorable. BOS carries a mortality rate of approximately 40-60%, with a five
year survival rate of 13%.
Early on, BOS is symptomatically silent. Once symptoms are present, there is a high
likelihood of irreversible disease regardless of the combination of immune suppression used.
Given these circumstances, early diagnosis is of utmost importance, and can be characterized
by an isolated and subclinical decline in lung function. Recent studies have suggested that
early decline in lung function on pulmonary function testing (PFT) may be representative of
developing BOS.
Due to the lack of consistent screening and diagnostic criteria, many patients with evolving
BOS elude a timely diagnosis, thereby jeopardizing their chance of survival. In response,
several experts have recommended frequent PFT screening and a modified, less stringent set
of diagnostic criteria with the goal of establishing earlier diagnosis and timely
intervention.
Traditionally, treatment of BOS has included aggressive immunosuppression, leaving patients
at risk for life-threatening invasive infections, multi-system co-morbidities, and the
threat of lung transplantation. Recent studies have demonstrated that early management with
agents such as inhaled corticosteroids (ICS), macrolides, and leukotriene receptor
antagonists (LTRA) can lead to improvements in both lung function and clinical symptoms.
This study aims to evaluate the utility of frequent and routine pulmonary surveillance in
pediatric patients who have undergone allogenic HSCT. Our prospective study design provides
a novel framework for the implementation of standardized lung function screening every three
months in the first two years following HSCT. With this, we hypothesize that standardized
PFT screening will improve diagnostic sensitivity and allow for earlier intervention in
patients with evolving airway obstruction and BO.
This study also aims to evaluate the efficacy of inhaled fluticasone, azithromycin, and
montelukast (FAM therapy) in the management of early airflow obstruction in pediatric
patients following allogenic HSCT. Early airflow obstruction is defined by pulmonary
function testing (FEV1 decline of ≥10% predicted with a FVC <0.8). With this, we hypothesize
that FAM therapy will attenuate the progression of airflow obstruction and improve lung
function in those with irreversible airflow obstruction at one and two years when compared
to historical controls.
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