An Interventional Left Ventricular Assist System for Cardiogenic Shock

NCT ID: NCT06127927

Last Updated: 2024-07-08

Basic Information

• Recruitment Status: RECRUITING
• Clinical Phase: NA
• Total Enrollment: 60 participants
• Study Classification: INTERVENTIONAL
• Study Start Date: 2023-11-08
• Study Completion Date: 2025-12-08

Brief Summary

Imported Impella The price is relatively expensive and difficult for ordinary patients to afford. In order to better meet the growing clinical needs in China, Anhui Tongling Bionic Technology Co., Ltd. has developed an interventional left ventricular assist system. The test device was tested in preclinical animals It has shown good effectiveness and safety. Through the implementation of this clinical trial, the interventional left ventricular assist system The safety and effectiveness of the system for hemodynamic support in patients with cardiogenic shock have led to further development of this product in the country.

Detailed Description

In recent years, patients with severe heart disease, with coronary heart disease as the main disease spectrum, have been on the rise, and the mortality rate remains high. In routine clinical diagnosis and treatment, inotropic drugs and vasoactive drugs are used to correct shock and maintain blood flow. The cornerstone of mechanical stability, however, there is insufficient evidence that these drugs benefit patients in the long term. Mechanical circulatory support (MCS) is a life support technology that was firstly used clinically in the 1950s. It can replace or partially replace the functions of the heart and/or lungs. And by increasing end-organ and coronary artery perfusion, reducing cardiac volume load, ventricular wall stress and myocardial oxygen consumption, etc. mechanism, quickly and accurately produce a stable hemodynamic effect, ultimately reducing the patient's pulmonary circulation congestion and myocardial ischemia. Reduce blood flow and infarction area and gain valuable time for follow-up treatment, so that patients with severe heart disease can be supported and transitioned to treatment great progress has been made in the treatment of heart diseases, and this technology has been widely used in the field of critical heart disease. 2017 American Heart Association The American Heart Association (AHA) recommends MCS for waiting for recovery of cardiac function or heart transplantation. Interimplantation and definitive treatment of advanced heart failure. Depending on location, MCS is divided into left ventricle Left ventricular assist device (LVAD), right ventricular assist device (Right ventricular assist device (RVAD), biventricular assist device (Biventricular assist device, BVAD) and total artificial heart (TAH). Currently, MCS commonly used in clinical practice mainly includes Intra-aortic balloon pump (IABP), extracorporeal membrane oxygenation (Extracorporeal membrane oxygenation (ECMO), Impella, TandemHeart and RVAD. The Impella system is an LVAD, it is divided into 3 models according to the diameter of the instrument: 12F (Impella 2.5), 14F (Impella CP) and 21F (Impella 5.0), the corresponding maximum output flows are 2.5L/min, 3.0~4.0L/min and 5.0L/min. The working principle of the device is to pump the left heart through the built-in micro axial flow pump at the front end of the catheter.

The oxygenated blood in the ventricle is pumped out through the catheter inlet, and then the axial flow pump is pumped directly into the ascending aorta to establish the left ventricular-ascending aorta. Aortic drainage pathway. Can help increase cardiac output (CO), increase aortic pressure and Coronary perfusion pressure, improve mean arterial pressure, coronary blood flow; while reducing left ventricular preload and pulmonary Pulse wedge pressure reduces ventricular wall tension and myocardial oxygen consumption. Acts as an active mechanical pump and partially replaces left ventricular function able. Impella is commonly used in the clinical treatment of cardiogenic shock. The ISAR-SHOCK study enrolled 26 patients with acute cardiac arrest. Comparing the efficacy of IABP and Impella 2.5 in patients with cardiogenic shock after myocardial infarction, the primary endpoint of the study Changes in cardiac index (CI) 30 minutes after MCS insertion. It was found that Impella A more significant increase in CI than after IABP, with 30-day mortality of 46% in both groups, confirms that Impella 2.5 Safety and feasibility in the treatment of cardiogenic shock after acute myocardial infarction. Two other studies also found that Similar conclusion RECOVER I study is a study that included 16 cases of cardiogenic shock or hypocardia after cardiotomy. A prospective, single-arm study of patients with displacement syndrome, the results of which indicate immediate blood loss after implantation of Impella 5.0 Fluid dynamics indicators improved significantly, and 93% of patients had improved cardiac function at discharge, with all patients at 30 days, 3 months, and 1 year. The survival rates were 94%, 81% and 75% respectively, proving the safety of Impella 5.0 for bridging treatment after cardiac surgery and feasibility. Currently, only Impella produced by the American company Abiomed has been approved by the FDA. However, imported Impella The price is relatively expensive and difficult for ordinary patients to afford. In order to better meet the growing clinical needs in China, Anhui Tongling Bionic Technology Co., Ltd. has developed an interventional left ventricular assist system. The test device was tested in preclinical animals It has shown good effectiveness and safety. Through the implementation of this clinical trial, the interventional left ventricular assist system The safety and effectiveness of the system for hemodynamic support in patients with cardiogenic shock have led to further development of this product in the country.

Conditions

Cardiogenic Shock

Study Design

• Allocation Method: NON_RANDOMIZED
• Intervention Model: SINGLE_GROUP
• Primary Study Purpose: TREATMENT
• Blinding Strategy: NONE

Study Groups

Interventional Left Ventricular Assist System Pre-trial

The design of the first phase pre-trial clinical study will involve a total of 6 subjects. The survival rate of subjects before discharge or 30 days after weaning was the main effectiveness evaluation indicator, and the safety and effectiveness of the test device were preliminarily evaluated. All SAE events during the study will be reviewed by CEC experts. According to the expert review opinions, if no unexpected serious complications and product defects are found, the Formal Research phase will be started.

Group Type: EXPERIMENTAL

Interventional Left Ventricular Assist System

Intervention Type: DEVICE

Interventional left ventricular assist system for cardiogenic shock patients

Interventional Left Ventricular Assist System Formal Research

A formal clinical trial to evaluate the effectiveness and safety of interventional left ventricular assist system for hemodynamic support in patients with cardiogenic shock through a prospective, multicenter, single-group target value study.The total number of patients enrolled in this study is planned to be 54. This sample size is calculated according to statistical principles, combining the research hypothesis and the estimate of the expected level of efficacy. The sample size calculation is based on the main efficacy index and the main safety index. Since it is set according to the common evaluation index, the sample size is calculated for the two main evaluation indicators separately, and the largest one is used as the final sample size of this trial.

Group Type: EXPERIMENTAL

Interventional Left Ventricular Assist System

Intervention Type: DEVICE

Interventional left ventricular assist system for cardiogenic shock patients

Interventions

Interventional Left Ventricular Assist System

Interventional left ventricular assist system for cardiogenic shock patients

Intervention Type: DEVICE

Eligibility Criteria

Inclusion Criteria

1. Age 18-75 years old;

2. Refractory cardiogenic shock as determined by the cardiac MDT expert group; The criteria for refractory cardiogenic shock are: despite adequate doses of two vasoactive drugs and treatment of the underlying cause, there is still evidence of tissue hypoperfusion;

3. The subject can understand the purpose of the trial, voluntarily participate and sign the written informed consent form reviewed and approved by the ethics committee; the subject agrees to complete the follow-up in accordance with the protocol requirements.

1. Age 18-75 years old;

2. Low cardiac output syndrome or increased filling pressure after regular continuous pumping of 1 high-dose or 2 medium-dose inotropic drugs within 48 hours after cardiopulmonary bypass was removed during cardiac surgery. The specific criteria are as follows;

The drugs, doses and time of 1 high-dose or 2 medium-dose inotropic drugs are as follows:

Epinephrine: medium dose (<0.03 μg/kg/min), continuous pumping ≥15 minutes High dose (≥0.03 μg/kg/min), continuous pumping ≥15 minutes; Dobutamine: medium dose (<5μg/kg/min), continuous pumping ≥15 minutes High dose (≥5μg/kg/min), continuous pumping ≥15 minutes; Milrinone: medium dose (<0.3 μg/kg/min), continuous pumping ≥120 minutes High dose (≥0.3 μg/kg/min), continuous pumping ≥120 minutes; Low cardiac output syndrome: cardiac index 1.3≤CI≤2.2 L/min/m2;

Increased filling pressure: pulmonary capillary wedge pressure:

20≤PCWP≤30mmHg or pulmonary artery systolic pressure: 25≤PAP≤35mmHg 3) The subject can understand the purpose of the trial, voluntarily participate and sign the informed consent form reviewed and approved by the ethics committee; the subject agrees to complete the follow-up in accordance with the protocol requirements.

Exclusion Criteria

1. Right heart failure that meets any of the following conditions:

a Central venous pressure-capillary wedge pressure ≥10mmHg; b Central venous pressure-pulmonary artery diastolic pressure ≥10mmHg; c Cardiac tamponade.

2. Any peripheral vascular disease that prevents the placement of the trial device;

3. Left or right ventricular thrombus;

4. Aortic valve regurgitation, echocardiographic grade ≥2+;

5. Aortic valve stenosis, valve area ≤1.5cm2;

6. Aortic valve calcification;

7. Presence of mechanical aortic valve;

8. Hypertrophic or obstructive cardiomyopathy;

9. Untreated ventricular septal or atrial septal defect;

10. Patent foramen ovale;

11. Mechanical complications of acute myocardial infarction;

12. Presence of hereditary spherocytosis, hereditary elliptocytosis, autoimmune hemolytic anemia or other diseases that cause hemolysis;

13. Cardiopulmonary resuscitation lasting more than 15 minutes within 24 hours before catheter pump implantation;

14. Ventricular tachycardia or ventricular fibrillation is ineffective with drug treatment;

15. Renal failure, serum creatinine ≥309.4umol/l or blood urea nitrogen ★ ≥35.7mmol/l);

16. Liver failure (total bilirubin ≥85.5umol/l);

17. Allergy or intolerance to heparin;

18. Presence of any cardiac assist device;

19. Presence of active systemic infection;

20. Refusing to sign the informed consent form or failing to complete follow-up as required by the protocol;

21. Pregnant or lactating women, female subjects with potential fertility but unable or unwilling to use effective contraceptive measures during the study;

22. Subjects who have participated in other clinical trials within 3 months or are currently participating in other clinical trials;

23. Other situations that the investigator believes are not suitable for clinical trials.

For Formal Research Phase

1. Right heart failure that meets any of the following conditions:

1. Central venous pressure-capillary wedge pressure ≥10mmHg;

2. Central venous pressure-pulmonary artery diastolic pressure ≥10mmHg;

3. Cardiac ascites.

2. Any peripheral vascular disease that prevents the placement of the trial device;

3. Left or right ventricular thrombus;

4. Aortic valve regurgitation, echocardiographic grade ≥2+;

5. Aortic valve stenosis, valve area ≤1.5cm2;

6. Presence of mechanical aortic valve;

7. Hypertrophic or obstructive cardiomyopathy;

8. Untreated ventricular septal or atrial septal defect;

9. Patent foramen ovale;

10. Mechanical complications of acute myocardial infarction;

11. Suffering from diseases that cause increased blood cell fragility or hemolysis;

12. Cardiopulmonary resuscitation lasting more than 15 minutes within 24 hours before catheter pump implantation;

13. Sustained or non-sustained ventricular tachycardia or ventricular fibrillation that is unresponsive to drug treatment;

14. Renal failure, serum creatinine ≥3.5mg/dl or blood urea nitrogen ≥100mg/dl;

15. Liver failure, total bilirubin ≥5mg/dl;

16. Allergy or intolerance to heparin;

17. Other cardiac assist devices other than IABP have been implanted;

18. Active systemic infection;

19. Refuse to sign the informed consent form or fail to complete follow-up as required by the protocol;

20. Pregnant or lactating women, female subjects with potential fertility but unable or unwilling to use effective contraceptive measures during the study;

21. Subjects who are participating in other clinical trials and have not yet reached the endpoints of the trial;

22. Other situations that the investigator believes are not suitable for clinical trials.

• Minimum Eligible Age: 18 Years
• Maximum Eligible Age: 75 Years
• Eligible Sex: ALL
• Accepts Healthy Volunteers: No

Sponsors

Fujian Medical University

OTHER

Sponsor Role: lead

Responsible Party

Liang-Wan Chen MD

Chief

Responsibility Role: PRINCIPAL_INVESTIGATOR

Principal Investigators

Liang-wan Chen, M.D Ph.D

Role: STUDY_CHAIR

Fujian Medical University Union Hospital

Locations

Department of Cardiovascular Surgery

Fuzhou, Fujian, China

Site Status: RECRUITING

Fujian Medical University Union Hospital

Fuzhou, Fujian, China

Site Status: RECRUITING

Countries

China

Central Contacts

Liang-wan Chen, M.D Ph.D

Role: CONTACT

chenliangwan@tom.com

+8613358255333

Facility Contacts

Liang-Wan Chen, M.D, Ph.D

Role: primary

daixiaofu719@hotmail.com

86 13358255333

E Lin, M.D

Role: backup

1470054258@qq.com

86 13365912195

Liang-wan Chen, PhD MD

Role: primary

chenliangwan@tom.com

13358255333

Other Identifiers

A202301

Identifier Type: -

Identifier Source: org_study_id