Bronchopulmonary Dysplasia Clinical Trial
Official title:
Helping Underdeveloped Lungs With Cells (HULC): Mesenchymal Stromal Cells in Extreme Preterm Infants at Risk of Developing Bronchopulmonary Dysplasia - Phase 1 Study
Verified date | May 2024 |
Source | Ottawa Hospital Research Institute |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
Bronchopulmonary dysplasia (BPD) is a common and chronic lung disease that occurs in preterm infants following ventilator and oxygen therapy and is associated with long-term health consequences. Preclinical research shows that mesenchymal stromal cells (MSCs) can modify a number of pathophysiological processes that are central to the progression of BPD and thus present as a promising new treatment option. The main purpose of this Phase I study is to evaluate the safety of human umbilical cord tissue-derived MSCs in extremely preterm infants at risk of developing BPD.
Status | Active, not recruiting |
Enrollment | 9 |
Est. completion date | November 6, 2033 |
Est. primary completion date | November 6, 2023 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 7 Days to 28 Days |
Eligibility | A participant needs to meet all inclusion criteria between day of life 7-28 to be eligible: Inclusion Criteria: - Admission to The Ottawa Hospital (TOH) NICU - General Campus or Sunnybrook Health Sciences Centre NICU - Gestational age at birth < 28 weeks - Intubated on mechanical ventilation - Fraction of inspired oxygen = 30% - Parents or substitute decision make must provide written informed consent Exclusion Criteria: - Severe congenital anomaly by antenatal ultrasound and physical examination - Ongoing shock and severe sepsis (confirmed by positive blood or cerebrospinal fluid culture) as per attending physician - Severe pulmonary hemorrhage - Active pneumothorax (with chest tube in-situ) - Hemodynamically significant PDA - Participants with caregiver unable to speak English or French - Patient i moribund, not expected to survive - Planned to be extubated in the 24 hours after uc-MSC administration |
Country | Name | City | State |
---|---|---|---|
Canada | The Ottawa Hospital - General Campus | Gloucester | Ontario |
Canada | Sunnybrook Health Sciences Centre | Toronto | Ontario |
Lead Sponsor | Collaborator |
---|---|
Ottawa Hospital Research Institute | Canadian Institutes of Health Research (CIHR), Ontario Institute of Regenerative Medicine (OIRM), Stem Cell Network |
Canada,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Occurrence and rate of dose limiting toxicity | Dose limiting toxicity consists of the following events:
Death occurring within 24 hours of injection; Pulmonary embolism defined as acute increase in right ventricular afterload (identified by serial targeted neonatal echocardiography) and signs of acute increased dead space ventilation (respiratory distress, increased PaCO2, increased minute ventilation) occurring within 24 hours of injection; Hypersensitivity / anaphylactic to uc-MSCs defined as any severe systemic inflammatory response syndrome with negative blood culture not consistent with the overall clinical course of the infant occurring within 72 hours of injection; Any other serious adverse event not expected in this patient population for which there is no alternative explanation but the administration of uc-MSCs, occurring within 1 week of injection. |
Up to 1 week following uc-MSC injection | |
Secondary | Rate of Death | Rate of death until discharge or 40 weeks corrected gestational age, whichever comes first | From enrollment until discharge or 40 weeks corrected gestational age (whichever occurs first) | |
Secondary | Occurrence of Other Severe Complications of Prematurity | Blood culture-proven sepsis
Patent ductus arteriosus (treated medically or surgically) Necrotizing enterocolitis Isolated intestinal perforation Retinopathy of prematurity requiring treatment Severe intraventricular hemorrhage (= grade 3) Cystic periventricular leukomalacia |
From enrollment until discharge or 40 weeks corrected gestational age (whichever occurs first) | |
Secondary | FiO2 and Oxygen Index | Measures of gas exchange | From enrollment until discharge, 40 weeks corrected gestational age, or death (whichever occurs first) | |
Secondary | Need for Ventilatory Support | Time to extubation
Duration of mechanical ventilation Duration of non-invasive positive pressure respiratory support Duration of supplemental oxygen |
From enrollment until discharge, 40 weeks corrected gestational age, or death (whichever occurs first) | |
Secondary | Need for Postnatal Steroids | This is a yes/no measure | From enrollment until discharge, 40 weeks corrected gestational age, or death (whichever occurs first) | |
Secondary | Incidence and Severity of BPD | Measured as mild, moderate, or severe | From enrollment until discharge, 40 weeks corrected gestational age, or death (whichever occurs first) | |
Secondary | Rate of Survival Without (moderate or severe) BPD | Measured according to the physiological definition of BPD (BPD at 36 weeks corrected age) | From enrollment until 36 weeks corrected gestational age | |
Secondary | Changes in Pulmonary Hemodynamics | Targeted neonatal echocardiography to assess pulmonary hypertension using validated parameters | At enrollment, 48 hours following uc-MSC injection, 28 days of life, and 36 weeks corrected gestational age | |
Secondary | Biological Measure of Clinical Improvement | Markers of inflammation will be assessed in patient serum samples | 72-96 hours following uc-MSC injection | |
Secondary | Biological Measure of Lung Improvement | Biomarkers of lung improvement will be assessed in patient tracheal aspirate samples | 72-96 hours following uc-MSC injection | |
Secondary | Feasibility: Cell Administration | Successful recruitment and administration of cells to nine patients in 18 months | Day of life 7-28 | |
Secondary | Feasibility: Recruitment Efficiency | Proportion of potentially eligible patients that are successfully screened
Proportion of participants successfully screened who do not enroll (reason for failure to enroll will be recorded) |
Day of life 7-28 | |
Secondary | Feasibility: Recruitment Timing | Median time from screening to enrollment
Median time from screening to cell administration |
Day of life 7-28 | |
Secondary | Feasibility: Participant Retainment | Proportion of patients that do not complete cell infusion
Proportion of patients enrolled that do not undergo scheduled follow-up |
From enrollment until follow-up at 18-30 months-of-age | |
Secondary | Bayley Scale of Infant and Toddler Development | Assessment of cognitive, language, and motor development | 18-30 months-of-age | |
Secondary | Long-term Safety Follow-Up | Participant's overall health will be assessed through a questionnaire administered over the phone, once a year for 10 years | Ten years following follow-up visit | |
Secondary | Animated Information Video | Characterize parental views of an animated MSC information video through brief semi-structured interviews | Day of life 7-28 |
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