Data from case series and large retrospective trials suggest that the early treatment of cardiogenic shock AMI patients with the association of VA-ECMO and IABP may significantly decrease mortality, which is still unacceptably high nowadays (40-50% at 30 days). An important benefit for the patients randomized to the ECMO arm is expected and the risk-to-benefit ratio is expected to be in favor of the experimental treatment arm.
Scientific background \- Venoarterial extracorporeal membrane oxygenation (VA-ECMO) is used more and more frequently in patients with acute myocardial infarction (AMI) and refractory cardiogenic shock despite the absence of high level scientific evidence to recommend the use of temporary circulatory support devices (TCS) in this setting.TCS support may also benefit to cardiogenic shock patients not initially refractory to conventional medical management since their mortality exceeds 40% and most of deaths are due to the development of refractory cardiogenic shock and multiple organ failure. The ANCHOR trial is therefore designed to test the hypothesis that VA-ECMO support associated with IABP results in improved outcomes in comparison with optimal medical treatment alone in patients with AMI and cardiogenic shock. An ethical rescue option to VA-ECMO will however be provided to control patients with cardiogenic shock refractory to conventional medical treatment since recent data suggested survival up-to 50% with ECMO support in this setting. Main objective - To determine if early VA-ECMO combined with IABP support and optimal medical treatment would improve the outcomes of patients with acute myocardial infarction complicated by cardiogenic shock as compared with optimal medical treatment alone. Scope of the study \- Patients satisfying all of the Inclusion and Exclusion Criteria will be classified as 'Eligible'. Consent to research will be obtained from a close relative or surrogate for all eligible patients prior to randomization. Should such a person be absent, eligible patients will be randomized according to the specifications of emergency consent and the patient will be asked to give his/her consent for the continuation of the trial when his/her condition will allow. Randomization will be possible in centers with robust experience in the management of AMI and cardiogenic shock but no on-site ECMO capability providing that an ECMO retrieval team from the nearest ECMO center can establish ECMO no later than 2 hours after randomization. Before randomization, physicians at the non-ECMO center will check that the ECMO team is immediately available and that an ICU/CCU bed is available at the ECMO center. Thereafter, if the patient is randomized to the ECMO arm, the mobile ECMO retrieval team will travel to the center, initiate VA-ECMO and will rapidly transfer the patient on VA-ECMO to the ECMO center. Description of experimental ECMO + IABP Arm * Protocolized conventional management of cardiogenic shock * VA-ECMO will be started as soon as possible * For patients randomized at non-ECMO centers, a mobile ECMO team will initiate ECMO at the non-ECMO center and transport the patient to the ECMO center immediately * IABP inserted in the contralateral femoral artery (unless technically not possible) * ECMO management according to protocol * ECMO weaning according to protocol Description of conventional treatment Arm * Protocolized conventional management of cardiogenic shock * IABP not recommended. No other TCS device (e.g., ECMO, Impella, Thoratec PHP, TandemHeart) permitted * Rescue VA-ECMO only if one of 1 or 2 or 3 applies: * 1\. Refractory cardiogenic shock defined as 1. Cardiac index \<1.2 l/min/m² or VTI \<6 cm AND 2. Assessment and correction of hypovolemia AND 3. (dobutamine ≥15 microg/kg/min + norepinephrine ≥1.5 microg/kg/min) OR epinephrine ≥ 0.75 microg/kg/min 4. Serum lactate \>5 mmol/L or serum lactate increased \>50% in the last 6 hours * 2\. Uncontrolled lethal arrhythmia despite K \>4.5 mmol/l AND Mg \>1.0 mmol/l AND Intubation and mechanical ventilation with deep sedation AND IV Loading of amiodarone AND IV xylocaine * 3\. Refractory cardiac arrest Mandatory validation of rescue VA-ECMO by an independent adjudicator.
* The ECMO device will be the CardioHelp (MAQUET, GETINGE, Orléans, France) using the veno-arterial setting and percutaneous femoro-femoral cannulation with MAQUET GETINGE HLS cannulae. * Intraortic balloon pump will be MEGA 50 cc or 40cc, (MAQUET, GETINGE, Orléans, France).
Hôpital Pitié Salpétrière
Paris, France
RECRUITINGTreatment failure at Day 30
Death in the ECMO group and death OR rescue ECMO in the control group
Time frame: At day 30
Mortality at Day 30
All-cause mortality at day 30
Time frame: At day 30
Major Adverse Cardiovascular Events
Major Adverse Cardiovascular Events are defined as death, stroke (any new neurological symptoms in association with signs of ischemia or hemorrhage in a cranial CT or MRI), recurrent myocardial infarction, need for repeat revascularization (PCI and/or CABG), renal replacement therapy, re-hospitalization for heart failure, escalation to permanent left ventricular assist device (LVAD) or total artificial heart, cardiac transplant.
Time frame: At day 30
Stroke
Any new neurological symptoms in association with signs of ischemia or hemorrhage in a cranial CT or MRI
Time frame: At day 30
Recurrent myocardial infarction
Recurrent myocardial infarction
Time frame: At day 30
Need for repeat revascularization with PCI and/or CABG
Need for repeat revascularization (PCI and/or CABG)
Time frame: At day 30
Need for renal replacement therapy
Need for renal replacement therapy
Time frame: At day 30
Re-hospitalization for heart failure
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Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
NONE
Enrollment
400
re-hospitalization for heart failure
Time frame: At day 30
Escalation to LVAD or total artificial heart
Escalation to permanent left ventricular assist device or total artificial heart
Time frame: At day 30
Cardiac transplantation
Cardiac transplantation
Time frame: At day 30
Major bleeding
Major bleeding (TIMI definition): Any intracranial bleeding (excluding microhemorrhages \<10 mm evident only on gradient-echo MRI) OR Clinically overt signs of hemorrhage associated with a drop in hemoglobin of ≥5 g/dL or a ≥15% absolute decrease in hematocrit OR Fatal bleeding (bleeding that directly results in death within 7 d)
Time frame: At day 30
Red blood cells transfused
Number of packed red blood cells transfused
Time frame: At day 30
Serum lactate
Time to serum lactate normalization
Time frame: At day 30
Number of days alive without organ failure at day 30
Number of days alive without organ failure(s) defined with the SOFA score, catecholamine support, mechanical ventilation and renal replacement therapy
Time frame: At day 30
Durations of ICU stay and hospitalization
Durations of ICU stay and of hospitalization
Time frame: At day 30
LV function
LV function assessed with Doppler echocardiography or magnetic resonance imaging
Time frame: At day 30
NYHA/INTERMACS status
NYHA/INTERMACS status
Time frame: At day 30
ECMO-related complications
ECMO-related complications (infection at VA-ECMO cannulation sites requiring antibiotics, hemorrhage, limb ischemia requiring surgery, cannula or circuit thrombosis, overt pulmonary edema, thrombocytopenia, gaseous emboli and hemolysis).
Time frame: At day 30
Treatment failure at one year
Treatment failure defined as death (all-cause) in the ECMO group and death (all-cause) OR rescue ECMO in the control group.
Time frame: At one year
Mortality at one year
All-cause mortality
Time frame: At one year
Major Adverse Cardiovascular at one year
MACE, Major Adverse Cardiovascular Events are defined as death, stroke (any new neurological symptoms in association with signs of ischemia or hemorrhage in a cranial CT or MRI), recurrent myocardial infarction, need for repeat revascularization (PCI and/or CABG), renal replacement therapy, re-hospitalization for heart failure, escalation to permanent left ventricular assist device (LVAD) or total artificial heart, cardiac transplant.
Time frame: At one year
Stroke at one year
Stroke (any new neurological symptoms in association with signs of ischemia or hemorrhage in a cranial CT or MRI),
Time frame: At one year
Recurrent myocardial infarction at one year
Recurrent myocardial infarction between randomization and one year
Time frame: At one year
PCI and/or CABG at one year
Repeat revascularization (PCI and/or CABG) between randomization and one year
Time frame: At one year
Renal replacement therapy at one year
Need for renal replacement therapy between randomization and one year
Time frame: At one year
Re-hospitalization for heart failure
Re-hospitalization for heart failure between randomization and one year
Time frame: At one year
LVAD at one year
Escalation to permanent left ventricular assist device (LVAD) or total artificial heart
Time frame: At one year
Cardiac transplant at one year
Cardiac transplantation
Time frame: At one year
Major bleeding at one year
Major bleeding (TIMI definition): Any intracranial bleeding (excluding microhemorrhages \<10 mm evident only on gradient-echo MRI) OR Clinically overt signs of hemorrhage associated with a drop in hemoglobin of ≥5 g/dL or a ≥15% absolute decrease in hematocrit OR Fatal bleeding (bleeding that directly results in death within 7 d)
Time frame: At one year
NYHA/INTERMACS status at one year
NYHA/INTERMACS status
Time frame: At one year
Returned to work at one year
Rate of patients who returned to work if previously active
Time frame: At one year
LV ejection fraction at one year
Latest LV ejection fraction
Time frame: At one year
Short Form 36 (SF-36) questionnaire at one year
Quality of life assessed using the Short Form 36 (SF-36) Health Survey questionnaire
Time frame: At one year