Pulmonary Disease Clinical Trial
Official title:
The Effect of Autologous Adipose Mesenchymal Stem Cells in Treatment of Airway Injury in Patients Exposed to Sulfur Mustard
Background: Sulfur mustard (SM) is a potent alkylating agent that targets several organs,
especially lung tissue. SM exposure leads to serious changes in morphological structure of
airway system, which is associated with chronic obstructive pulmonary deficiency following
exposure to SM. With extensive progress and achievements in tissue repair through stem cells
therapy, consideration of lung tissue has been increased due to the high prevalence of
pulmonary problems. Several factors such as selection of cell types, required conditions for
growth and proliferation of stem cells, and the process of entering into the body to repair
damaged lung tissue are considered as the most important problems in this issue.
Accumulating studies, both in animals and human with mesenchymal stem cells (MSC) support
the hypothesis of therapeutic effects of these cells in various disorders. In this study
investigators aimed to evaluate safety and potential efficacy of systemic MSC administration
for treatment of chronic lung injuries in SM-exposed patients.
Methods: Patients will receive 100 million MSC cells every two months for three injections
within 6 months. After each injection, parameters including safety, pulmonary function
testing (PFT), quality-of-life indicators, 6 minute walk test (6MWT), and expression of
inflammation and oxidative stress genes will be evaluated.
Patients selection:
In this clinical trial, investigators considered therapeutic effect of MSCs in SM-exposed
male patients.Patients, had a documented encounter with SM during the Iran-Iraq war. The
patients signed informed consent before study. They were selected according to the following
criteria: (a) the severity of lung injury was ranged from moderate 50< forced expiratory
volume in 1 second (FEV1) <65 to severe 40<FEV1<50; (b) absence of contraindications
spirometry (hemoptysis, cerebral arterial aneurysm or aortic, pulmonary embolism,
uncontrolled blood pressure, recent pneumothorax, no doubt surgery/thoracic recent, recent
stroke); and (c) no coagulation. The exclusion criteria for the selection process were as
follow: (a) participate in another study at the same time; (b) smoking habitat; (c) the
existence of pneumonia during the study; (d) the incidence of transfusion reaction; (e)
underlying other diseases (cardiovascular disease, hypertension, diabetes).
Isolation and culture of adipose derived stem cells:
200mL of abdominal adipose tissue was obtained under local anesthesia by liposuction
aspirates protocol. The lipoaspirate was washed with PBS to remove tissue debris. 100mL PBS
containing 0.1% w/v collagenase A type I was added to isolated tissue and then incubated at
37ºC for 60 minutes. Collagenase activity was neutralized using MEM medium along with 10%
fetal bovine serum. Cell pellets were resuspended in culture medium after centrifugation at
2000rpm for 10 min, and then transferred to culture flasks for 72 h at 37ºC in 5% CO2
condition. The culture medium in the flasks was changed every 3 days, and cells were
passaged for two times.
Flow cytometry analysis:
To analyze the cell surface antigen expression, 5×105 fresh cells from third passage were
harvested by trypsin-EDTA. Cells were centrifuged at 100 g for 1 min, resuspended in stain
buffer (PBS, 2% FBS) and then incubated on ice for 10 minutes. Trypsin was neutralized by
centrifuge and isolated cells were washed twice with PBS and finally resuspended in stain
buffer. Cells were incubated in dark environment for 30 minutes. After incubation, the cells
were labeled with anti-human monoclonal antibodies (MAbs) conjugated to fluorochromes. These
antibodies were as follow: anti-CD90-fluorescein isothiocyanate (FITC), CD73-phycoerythrin
(PE), CD11b-FITC, CD34-FITC, CD44-FITC, CD45-PE, CD105-PE. The frequencies of all
immunolabeled cells were analyzed by FACS Canto II flow cytometer, in which approximately
500,000 events were assessed and data were analyzed using FlowJo software (version 10.0).
Karyotype analysis for abnormalities detection:
Standard Giemsa staining procedure was performed and chromosome preparations were obtained
from 80% confluent cells. To stop microtubule formation, the cells were treated with
Colcemid solution. The mitotic arrested cells were then harvested using trypsin-EDTA. The
cells were extracted and then immersed in 75 mmol/l KCl for 30 minute at laboratory
temperature. Finally, they obtained by a centrifugation. The supernatant was replaced with
fixative solution and the suspension was spread over slides for microscopic examination and
imaging. At least, 15 metaphase spreads were analyzed. The karyotypes were considered with
light microscope using a cytovision software.
Freezing and Storage of Adipose-derived Stem Cells:
ADMSCs were harvested at 90% confluence before injection for freezing. To collect cells,
culture medium was removed and replaced with sterile PBS and after three minutes it was
replaced with trypsin-EDTA solution and then incubated at 37°C for 5 minutes. Complete
medium (MEM with 10% FBS) was added to inactivate the trypsin, and centrifuged at 1500 rpm
for 5 minutes. Cell pellet was resuspended in cryopreservation medium (80% FBS, 10%
dimethylsulfoxide and 10% MEM medium) with a final concentration of 5 million cells per
milliliter and aliquoted into cryovials. The vials stored at −80 °C overnight and then
transferred into a liquid nitrogen container for long-term storage.
MSCs injection and Study plan:
Patients received 100×106 cells every 20 day for four injections within 2 months and
screened for 7 times. MSCs were injected intravenously along with 300 ml normal saline to
the patient at a maximum rate of 2×106 cells/min. Each infusion took approximately 30 minute
to be completed. After each injection, patient stayed at hospital for at least 6h as
recovery time. Efficacy of MSCs treatment in these patients were evaluated using the
following parameters: pulmonary functions test (PFTs) [forced expiratory volume in 1 second
(FEV1), Forced vital capacity (FVC), FEV1/FVC], total lung capacity by body plethysmography,
single-breath carbon monoxide diffusing capacity (CO diffusion) , exercise performance
[6-minute walk test (6MWT)], Borg scale dyspnea assessment (BSDA), COPD Assessment Test
(CAT), St. George's Respiratory Questionnaire (SRGQ) and comprehensive safety evaluation.
;
Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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