Graft vs Host Disease Clinical Trial
Official title:
Phase II Trial of Cyclosporine Inhalation Solution (CIS) in Lung Transplant and Hematopoietic Stem Cell Transplant Recipients for Treatment of Bronchiolitis Obliterans Syndrome
Background:
- Bronchiolitis obliterans or bronchiolitis obliterans syndrome is a lung disorder that
occurs as a complication of either lung transplantation or bone marrow/blood stem cell
transplantation. One of the complications of transplant is the occurrence of graft versus
host disease (in hematopoietic stem cell transplants) and host versus graft disease (in lung
transplantation). In these diseases, the cells attack the lungs and cause irreversible small
airway fibrosis referred to as bronchiolitis obliterans syndrome. When a patient develops
fibrosis of the lungs or bronchioles, the lungs no longer work properly, which causes
difficulties with breathing that lead to a diminished quality of life and an increased risk
of death. Treatment typically involves immunosuppressive therapy such as oral cyclosporine or
steroid therapy, but these treatments are only marginally effective and can cause significant
toxicities and increase the risk of infections. Inhaled cyclosporine (CIS) achieves higher
concentrations of cyclosporine in the lungs and lower concentrations of cyclosporine in the
blood than oral cyclosporine. Therefore, it could have advantages over conventional oral
immunosuppressive therapies used to treat this disorder. Researchers are interested in
testing whether inhaled cyclosporine therapy could be used as a safe and effective treatment
for bronchiolitis obliterans or bronchiolitis obliterans syndrome occurring after bone
marrow/blood stem cell or lung transplants.
Objectives:
- To evaluate whether inhaled cyclosporine (CIS) can improve or stabilize lung function and
quality of life in individuals with bronchiolitis obliterans.
Eligibility:
- Individuals between 10 and 80 years of age who have been diagnosed with bronchiolitis
obliterans or bronchiolitis obliterans syndrome after blood or lung transplants.
Design:
- Participants will be screened with a full medical history and physical examination, as
well as blood and urine tests, lung function tests, imaging studies, bronchoalveolar
lavage samples, and quality of life questionnaires.
- Participants will take cyclosporine inhalation solution through a nebulizer. The
nebulizer generates a mist of cyclosporine inhalation solution (CIS), which is then
breathed in through a mouthpiece. The process takes approximately 20 minutes. The
solution will be provided in single-use vials.
- Participants will continue to take all medications for post-transplant care as required
by their doctor and the study researchers. Attempts will be made to reduce the doses and
types of immunosuppressants given to participants on the study, as long as the treatment
continues to produce improved or stable lung function.
- Participants will have study visits every 3 weeks with blood and urine tests, lung
function tests, and imaging studies. Participants will undergo repeat bronchoalveolar
sample at week 9 and 18. Participants will also complete quality of life questionnaires
as directed. Treatment will continue for a minimum of 18 weeks, followed by a final
follow-up visit 2 weeks after the end of the study.
- Participants who benefit from the inhaled cyclosporine (CIS) may continue to receive
further therapy with inhaled cyclosporine at the end of the study by participation in a
separate study extension.
Bronchiolitis Obliterans (BO) is an obstructive lung disease that can affect individuals that
have undergone a lung or hematopoietic stem cell transplant. BO has been studied most
extensively in lung transplant recipients, where it is considered to represent chronic lung
rejection. It is the leading cause of death after lung transplant, with mortality rates up to
55%. In hematopoietic stem cell transplantation, BO is thought to be a manifestation of
chronic graft-vs-host disease (GVHD). Up to 45% of patients undergoing hematopoietic stem
cell transplantation at the NHLBI develop a decline in pulmonary function. Conventional
therapy for patients who develop BO consists of augmentation of systemic immunosuppressants.
Systemic immunosuppression has limited efficacy for BO and is associated with deleterious
consequences including increased risk of infections and decreased graft-versus tumor/leukemia
effects.
Recently, cyclosporine inhalation solution (CIS) in solution with propylene glycol has been
shown to improve overall survival and chronic rejection-free survival in lung transplant
patients. These findings suggest targeted delivery of immunosuppressive therapy to the
diseased organ warrants further investigation as this may minimize the morbidity associated
with systemic immunosuppression. However, there currently exists limited data regarding the
overall efficacy of inhaled cyclosporine to treat established BO following lung
transplantation. Furthermore, inhaled cyclosporine has not been studied in the treatment of
BO following hematopoietic stem cell transplantation.
Here, we propose to evaluate the safety, efficacy, and pharmacodynamics of inhaled
cyclosporine for the treatment of BO. Two distinct patient populations will be offered
enrollment in this protocol: hematopoietic transplant recipients with BO (group A) and lung
transplant recipients with BO (group B). Study participants will receive CIS at an initial
dose of 150mg, three times weekly. Patients will undergo dose titration to a maximum dose of
300mg, three times weekly. Drug deposition and pharmacokinetic analyses will be performed at
the initiation of treatment. Clinical parameters, including pulmonary function tests, will be
measured in addition to laboratory markers of the anti-inflammatory response to CIS. Adverse
events associated with treatment will be recorded.
The primary objective is to 1) assess the safety and efficacy of inhaled cyclosporine as a
new therapy in hematopoietic transplant patients and lung transplant patients with
established BO. Additionally, we seek to promote a better understanding of the pathogenesis
of BO in these two transplant groups and to assess the anti-inflammatory effects of inhaled
cyclosporine in patients that develop this complication.
The primary endpoint of each study group is the best response, FEV1 improvement or
stabilization from study baseline at week 18 for two successive measures, at least 1 week
apart, no more than 2 weeks apart. Secondary endpoints include the toxicity profile as
measured by CTCAE criteria (safety), the study of pharmacokinetics and lung deposition
characteristics of inhaled cyclosporine, improvement in high resolution chest CT images,
results of peripheral blood and bronchoalveolar cytokine arrays to assess secondary markers
of inflammation, and functional capacity measurements using a six-minute walk test.
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