First-in-human, Double Blind, Randomized With Placebo, Open for the 6 First Patients (Dose Ranging) to Evaluate the Safety and Efficacy of Intracoronary Infusion of Allogeneic Human CSCs in Patients With AMI and Left Ventricular Dysfunction
Overview
- Phase
- Phase 1
- Intervention
- Not specified
- Conditions
- Acute Myocardial Infarction
- Sponsor
- Coretherapix
- Enrollment
- 55
- Locations
- 1
- Primary Endpoint
- Safety measured as the number of deaths and number of Major Adverse Cardiac Events (MACE)
- Status
- Completed
- Last Updated
- 8 years ago
Overview
Brief Summary
Development of myocardial reparative therapy for the treatment of acute ischemic cardiac disease, based on the intracoronary administration of allogeneic Cardiac Stem Cells (CSCs) to ameliorate myocardial cell death and promote cardio-regeneration.
The study comprises two phases:
- Initial dose-escalation open-label safety phase comprising 6 patients. Escalation will start with the Maximum Recommended Safe Dose (MRSD) calculated from Non-Observed Adverse Events Level (NOAEL) and it is expected to finish with the target dose (TD). There will be no placebo group for this initial phase.
- Randomized double-blind placebo-controlled safety and efficacy phase in which the TD will be injected if the dose-escalation phase is completed successfully.
Detailed Description
This is a "First in Patient" Clinical Trial to obtain safety and efficacy results about the intracoronary administration of a suspension of allogeneic cardiac stem cells (CSCs) for the treatment of ST elevation Myocardial Infarction (STEMI). This clinical trial will have a first dose-escalation phase in which the safety of 10, 20 and 35 million CSCs administration will be evaluated in 6 patients. A second double-blind randomized and placebo controlled phase will be initiated, if no major safety effects are observed during the first week after cell administration. The 35 million cells dose is the one expected to be used during the randomized phase. Patients with EF\<45% and with infarct sizes \> 25% will be selected by magnetic resonance image (MRI). 49 patients will be included in the randomized phase with the aim of having 38 patients for efficacy analysis at the end of the follow up period (12 months). In this phase, patients will be randomly allocated for receiving CSCs or placebo in a 2:1 scheme. Three bioequivalent cellular batches obtained from different donors will be indistinctly used during the assay. CSCs or placebo treatment will be infused into the coronary artery responsible for the ischemic event. Placebo will be a commercial preparation of human serum albumin 5% in saline solution that will also be used for cell product reconstitution. After treatment, patients will be monitored overnight in a coronary care unit for any toxicity and discharged from hospital 24h after treatment if no adverse events are observed. Subsequent safety follow-up will be done first at day 7 after treatment and then monthly or quarterly thereafter for 12 months. In addition, efficacy evaluations will be performed by MRI and clinical parameters at 1, 6 and 12 months after treatment. Finally, cellular and humoral immunological response (screening for anti-HLA (Human Leukocyte Antigen) class I and class II antibodies, HLA typing, cross-matching between cells and treated patient and cytokine profiling in blood samples) will be analysed during the clinical trial.
Investigators
Eligibility Criteria
Inclusion Criteria
- •Adult patients ≥ 18 years of age and ≤ 80 years.
- •Patients presenting a ST-segment-elevation myocardial infarction (STEMI) according to the universally accepted definition found in the STEMI management guide of the European Society of Cardiology
- •Killip ≤ 2 on admission
- •Successful primary coronary revascularization by Percutaneous Coronary Intervention- PCI - (Thrombolysis In Myocardial Infarction \[TIMI\] = 3) within 12h after the onset of infarct symptoms
- •Bare-metal or drug-eluting stents (DES) of second generation (including new second generation stents, e.g. biolimus, novolimus and bioreabsorbable stents) at coronary revascularization by PCI
- •Ejection Fraction (EF) ≤45% by magnetic resonance imaging (MRI). This MRI will be done between day 3 and day 5 after infarction and will be used as inclusion MRI
- •Infarct size in left ventricle (LV) tested in the screening MRI ≥25% The presence of microvascular obstruction at inclusion MRI is permitted
- •The affected coronary artery is adequate for cells infusion at the administration time. The administration procedure is technically feasible on day 4-7 after coronary revascularization by PCI
- •The patient is stable and in adequate clinical condition to undergo the procedure.
Exclusion Criteria
- •Participation in another clinical trial in the last 30 days
- •Previous allogeneic transplant (blood transfusions are allowed) or treated with cell or gene therapy
- •Previous Q-wave infarction
- •Significant valve disease, relapsing pericarditis, history of cardiac tamponade, cardiomyopathies
- •Severe stenotic lesions (\>90%) in a coronary vessel with size \>2.75 mm not treated by PCI at least 24 hours before the baseline MRI study
- •Previous EF≤45%, NYHA \> 2 (New York Heart Association Functional Classification) or hospital admission for heart failure before STEMI
- •Sustained VT that does not revert with treatment or requires \>6 hours to be controlled in the 48 hours prior to the product administration procedure
- •Complete atrioventricular blockade, or acute left bundle branch block in the 48 hours prior to the product administration procedure
- •History of cardioembolic disease
- •Platelets \<100,000 and/or Hb\<8.5g/dL
Outcomes
Primary Outcomes
Safety measured as the number of deaths and number of Major Adverse Cardiac Events (MACE)
Time Frame: 12 months
The primary objective is to demonstrate the safety of the intra-coronary infusion of allogeneic cardiac stem cells in patients with a 7 days evolution first myocardial infarction and left ventricle dysfunction. Safety will be assessed a) evaluating the number of deaths from any cause within 30 days after cell medicine administration; b) evaluating the number of Major Adverse Cardiac Events (MACE) during the first 30 days (composite endpoint), defined as death from any cause, new Acute Myocardial Infarction (AMI), hospitalization due to Heart Failure (HF), sustained Ventricular Tachycardia (VT), Ventricular Fibrillation (VF), and stroke within 12 months after cell medicine administration.
Secondary Outcomes
- Efficacy measured by MRI as the infarct size change(6 and 12 months)
- Efficacy measured by MRI as the evolution of biomechanical parameters(6 and 12 months)
- Efficacy measured by MRI as the evolution of edema(1 month)