Hemoperfusion Efferon LPS During Cardiac Surgery Using Cardiopulmonary Bypass
- Conditions
- Cardiac DiseaseMultiple Organ Dysfunction Syndrome
- Registration Number
- NCT06659289
- Lead Sponsor
- Efferon JSC
- Brief Summary
More than 1 million people undergo cardiac surgery each year worldwide. Cardiac surgeries still in most cases require cardiopulmonary bypass, use of myocardial protection against aortic clamping and creation of cardioplegic arrest of the heart by injecting cardioplegic solutions into the coronary bed. All of the above is a source of myocardial ischemia-reperfusion injury, which remains the leading cause of acute heart failure in the period after the return of spontaneous circulation and, as a consequence, the development of post-perfusion multiple organ dysfunction syndrome and, in particular, acute kidney injury (AKI). Acute kidney injury typically develops in 7% of all hospitalised patients, 30% of intensive care unit patients and 30% of cardiac surgery patients. Endotoxemia is a major cause of AKI. Septic AKI (compared to non-septic AKI) is associated with a worse prognosis, longer hospital stay and poorer survival.
The use of the Efferon LPS hemoperfusion device, which has proven efficacy in removing not only endotoxin but also cytokines, may be promising in preventing the development of multiple organ dysfunction syndrome and in particular AKI in patients after cardiac surgery with cardiopulmonary bypass.
- Detailed Description
Every year, more than 1 million people around the world undergo heart surgery. Cardiac surgery still requires cardiopulmonary bypass in the majority of cases for a number of reasons. The use of cardiopulmonary bypass in cardiothoracic surgery is a well-known and potent inducer of immune responses due to the contact of whole blood with air and extracorporeal circuit surfaces, ischemia-reperfusion injury, hemolysis and release of free hemoglobin, the effects of surgical trauma itself, and other factors.The activation of immune cells leads to the release of cytokines and inflammatory mediators such as IL-6, IL-8, activated complement and others.
One of the most common post-operative complications associated with the administration of cardiopulmonary bypass during surgery is acute kidney injury (AKI). AKI develops in 30% of patients undergoing cardiac surgery and is associated with high mortality, longer hospital stay, dialysis dependency, high risk of infectious complications and ultimately poor quality of life. Endotoxemia is a major cause of AKI. Septic AKI (compared to non-septic AKI) is associated with a worse prognosis, longer hospital stay and poorer survival.
Currently, hemosorbents based on highly cross-linked styrene/divinylbenzene copolymers can remove endo- and exotoxins in sepsis and acute and chronic renal and hepatic failure, remove intoxication by pharmacological drugs, narcotics and poisons, and remove cytokines produced in excess in systemic inflammatory syndromes of various aetiologies, including systemic inflammatory response syndrome after open-heart surgery with cardiopulmonary bypass.
Hemoperfusion is a method of extracorporeal removal of toxic substances from the blood by adsorption to a porous material. Hemoperfusion can be a good complement or substitute to the classical methods of hemofiltration and hemodialysis when diffusion or convection of toxic substances through the membrane is not efficient enough.
Based on previous studies, the use of the Efferon LPS hemoperfusion device, which has proven efficacy in removing not only endotoxin but also cytokines, may be promising in preventing the development of multiple organ dysfunction syndrome and in particular AKI in patients after cardiac surgery with cardiopulmonary bypass.
Recruitment & Eligibility
- Status
- RECRUITING
- Sex
- All
- Target Recruitment
- 60
- Planned cardiac surgery (aortocoronary bypass, heart valve replacement, etc.) requiring the use of cardiopulmonary bypass
- Emergency nature of cardiac surgery
- Cases in which a surgical procedure is required in addition to an aortocoronary artery bypass graft operation
- History of aortocoronary bypass surgery
- History of hemato-oncology
- Receiving immunosuppressive therapy for cancer and autoimmune diseases
- Sepsis, acute heart failure, acute respiratory failure, acute kidney injury at the time of enrolment
- Chronic kidney disease, stage 5D (requiring continuous hemodialysis)
- Treatment with renal replacement therapy in the past 90 days
- Presence of cirrhosis (>5 Child-Pugh score)
- Acute pulmonary embolism
- Acute myocardial infarction within 3 weeks before elective surgery
- Left ventricular ejection fraction (LVEF) less than 40% according to echocardiography
- Acute cerebrovascular accident within 3 weeks before elective surgery
- Pregnancy
- Any other clinical condition of the patient that, in the opinion of the investigator, precludes inclusion in this study
Study & Design
- Study Type
- INTERVENTIONAL
- Study Design
- PARALLEL
- Primary Outcome Measures
Name Time Method Effect of the hemoperfusion with Efferon LPS device during cardiopulmonary bypass on measures of organ dysfunction 0-72 hours Measured every 24 hours ± 1 hour from the end of cardiopulmonary bypass to 72 hours. The SOFA (Sequential Organ Failure Assessment) index is equal to the sum of six indicators. The higher the score, the greater the insufficiency of the system being assessed. The higher the overall index, the greater the degree of multiorgan dysfunction. Violation of the function of each organ (system) is assessed separately in dynamics against the background of intensive therapy. With a score of no more than 12, multiple organ dysfunctions are assumed, 13-17 points indicate the transition of dysfunction to insufficiency, a score of about 24 indicates a high probability of death. The lower the SOFA index, the less pronounced organ failure and the better the patient's survival prognosis.
- Secondary Outcome Measures
Name Time Method Mean arterial pressure 0-72 hours Mean arterial pressure mmHg (measured every 24 hours ±1 hour)
Duration of vasopressor support 0-72 hours Time (hours) to end of vasopressor support
Pulmonary oxygen metabolic function index 0-72 hours Measuring PaO2 / FiO2 index every 24 hours
Incidence of postperfusion heart failure 0-72 hours Incidence of postperfusion heart failure
Duration of the need for pharmacological and/or mechanical inotropic myocardial support 0-72 hours Duration (number of hours) of the need for pharmacological and/or mechanical inotropic myocardial support from the beginning of the operation to 72 hours.
Duration of ventilation 1-14 days The time (hours) from the start of the operation until you are weaned off the ventilator within 14 days, or are discharged from hospital or transferred from intensive care (if earlier than day 14).
ICU length of stay 1-14 days Time (days) from the end of cardiopulmonary bypass to transfer from the ICU within 14 days or hospital discharge (if earlier than day 14)
Incidence of post-operative acute kidney injury 0-72 hours Incidence of post-operative acute kidney injury is verified by Acute Kidney Injury Network (AKIN) criteria
Renal function 0-72 hours Time (number of hours) to return to normal glomerular filtration rate (GFR)
Duration of renal replacement therapy 1-28 days Duration (hours) of renal replacement therapy in patients with advanced acute kidney injury. The criteria for the end of replacement therapy is the restoration of spontaneous diuresis of more than 50 mL/hour without stimulation of diuresis with drugs or more than 2000 mL/day with stimulation.
28-day mortality Time from randomisation to 28 days from the moment of randomisation The number of trial participants who died in intensive care or in hospital within 28 days of randomisation
Incidence of septic complications 1-14 days The number of patients who were diagnosed with sepsis after the end of cardiopulmonary bypass in the post-operative period according to the Sepsis-3 criteria
Trial Locations
- Locations (1)
Pavlov First Saint Petersburg State Medical University
🇷🇺Saint Petersburg, Russian Federation