Remote Ischemic Conditioning to Enhance Resuscitation (RICE) Pilot

Overview

Following resuscitation from out-of-hospital cardiac arrest (OHCA), reperfusion injury can cause cell damage in the heart and brain. Remote ischemic conditioning (RIC) consists of intermittent application of a device such as a blood pressure cuff to a limb to induce non-lethal ischemia. Studies in animals with cardiac arrest as well as in humans with acute myocardial infarction suggest that RIC before or after restoration of blood flow may reduce injury to the heart and improve outcomes but this has not been proven in humans who have had OHCA. The RICE pilot study is a single-center study to assess the feasibility of application of RIC in the emergency department setting for patients transported to the hospital after resuscitation from OHCA.

Study Type

  • Study Type: Interventional
  • Study Design
    • Allocation: Randomized
    • Intervention Model: Parallel Assignment
    • Primary Purpose: Treatment
    • Masking: Double (Participant, Investigator)
  • Study Primary Completion Date: August 7, 2020

Interventions

  • Device: Active Remote Ischemic Conditioning
    • A standard non-invasive blood pressure cuff (e.g., American Diagnostics Corporation, Hauppauge, NY but any one can be used off the shelf) and disposable plastic clamp (e.g.,Medline Industries Incorporated, Mundelein, IL) can be used to apply RIC in patients resuscitated from OHCA via three cycles of 5-mins. inflation to 200 mmHg followed by 5-mins. deflation of a blood pressure cuff on a upper extremity. The cuff occludes the artery; the clamp maintains pressure in the air bladder of the cuff during the inflation periods.
  • Device: Sham Remote Ischemic Conditioning
    • The control group will have a sham package opened at the bedside as soon as feasible after ED arrival. This will be identical in size, weight and appearance as that in the intervention group, but will contain a sham device. Upon identification that the patient has been randomized to the control group, the care team will proceed with all other resuscitative measures as in the the intervention group.

Arms, Groups and Cohorts

  • Active Comparator: Intervention Group
    • A standard non-invasive blood pressure cuff (e.g., American Diagnostics Corporation, Hauppauge, NY but any one can be used off the shelf) and disposable plastic clamp (e.g.,Medline Industries Incorporated, Mundelein, IL) can be used to apply RIC in patients resuscitated from OHCA via three cycles of 5-mins. inflation to 200 mmHg followed by 5-mins. deflation of a blood pressure cuff on an upper extremity. The cuff occludes the artery; the clamp maintains pressure in the air bladder of the cuff during the inflation periods.
  • Sham Comparator: Control Group
    • The control group will have a sham package opened at the bedside as soon as feasible after ED arrival. This will be identical in size, weight and appearance as that in the intervention group, but will contain a sham device. Upon identification that the patient has been randomized to the control group, the care team will proceed with all other resuscitative measures as in the the intervention group.

Clinical Trial Outcome Measures

Primary Measures

  • Attrition
    • Time Frame: 30 minutes from initiation of study intervention
    • Attrition assessed as the proportion of randomized subjects who do not remain on allocated therapy for the intended study duration among subjects randomly allocated. On therapy for the intended study duration consists of completing three cycles of inflation-deflation.

Secondary Measures

  • Treatment Success
    • Time Frame: 30 minutes from initiation of study intervention
    • Treatment Success assessed as the proportion of intervention group patients who remain alive and on their allocated therapy for the intended study duration.
  • Cardiac Function
    • Time Frame: Within 48 hours of index arrest
    • Cardiac Function assessed as left ventricular ejection fraction (LVEF) using echocardiograms ordered for clinical indications.
  • Cardiogenic Shock
    • Time Frame: Within 48 hours of index arrest
    • Cardiogenic Shock assessed as systolic BP < 80 mmHg during any 6 h period within 48 h of the index arrest not due to a correctable cause, and treated with pressors or inotropes or placement of a mechanical cardiac assist device (e.g. intra-aortic balloon pump). Cardiogenic shock correlates with survival after resuscitation from cardiac arrest.
  • STEMI
    • Time Frame: Within 48 hours of index arrest
    • STEMI assessed as the presence of electrocardiographic (ECG) and biomarker criteria for acute myocardial infarction within 48 h of the index arrest. Note that ST-elevation on the first 12-lead ECG after resuscitation is a poor predictor of acute infarction in this population. These patients often develop infarctions during the subsequent 48 h.
  • Myocardial Injury
    • Time Frame: Within 24 hours of index arrest
    • Myocardial Injury assessed as peak serum troponin in ng/mL at any time point within 24 h of index arrest.
  • Renal Dysfunction
    • Time Frame: Within 24 hours of index arrest
    • Renal Dysfunction assessed using Risk, Injury, Failure, Loss, End Stage criteria.
  • Hospital Free Survival
    • Time Frame: Within 30 days of index arrest
    • Hospital Free Survival (HFS) assessed as number of days alive and permanently out of hospital up to 30 days post arrest
  • Withdrawal of Care
    • Time Frame: Discharge or 30 days after index arrest
    • assessed as the reduction of support (i.e. reducing pressors, lab draws or medications) or withdrawal of support (i.e. extubation, stopping drips/meds, changing to comfort care only) during hospitalization.
  • Favourable Neurologic Status at Discharge
    • Time Frame: Discharge or 30 days after index arrest
    • Favourable Neurologic Status at Discharge assessed using modified Rankin Score (MRS) < 3 at hospital discharge or 30 days after index arrest.
  • Survival to Discharge
    • Time Frame: Dicharge or 30 days after index arrest
    • Survival to Discharge assessed as alive when discharged from hospital to home, nursing facility or rehabilitation. Patients transferred to another acute care facility (e.g. to undergo implantable defibrillator placement) will be considered still hospitalized.
  • Clinical Instability at Discharge
    • Time Frame: Discharge or 30 days after index arrest
    • Clinical Instability at Discharge assessed using the Kosecoff Index measured at discharge based on the presence of nine symptoms and signs associated with increased risk of rehospitalization. Instability will be the presence of any of these.
  • Survival to 30 days after arrest
    • Time Frame: 30 days after index arrest
    • Survival to 30 Days After Cardiac Arrest assessed as alive 30 days after the index cardiac arrest as confirmed by a brief telephone interview.
  • Accrual
    • Time Frame: Through study completion, an average of 6 mos.
    • Accrual is the proportion of eligible subjects who have the study device applied

Participating in This Clinical Trial

Included will be those with: 1. Age 18 years or more; 2. Defibrillation by laypersons or defibrillation and/or chest compressions by EMS providers dispatched to the scene; 3. Non-traumatic etiology of arrest, defined as without concomitant blunt, penetrating, or burn-related injury, or uncontrolled bleeding or exsanguination; 4. Spontaneous circulation upon emergency department arrival; 5. No response to verbal commands; and 6. Ongoing or planned induced hypothermia. Excluded will be those with: 1. STEMI indicated on first 12-lead ECG obtained after restoration of circulation, defined as ST-elevation of ≥2 mm in two or more contiguous ECG leads; 2. Written do not attempt resuscitation (DNAR) reported to providers before randomization; 3. Drowning or hypothermia as cause of arrest; 4. Known prisoner or pregnant; or 5. Dialysis fistula in either upper extremity; or 6. Pre-existing amputation of upper extremity.

Gender Eligibility: All

Minimum Age: 18 Years

Maximum Age: N/A

Are Healthy Volunteers Accepted: No

Investigator Details

  • Lead Sponsor
    • University of Washington
  • Collaborator
    • Kettering Foundation
  • Provider of Information About this Clinical Study
    • Principal Investigator: Graham Nichol, Professor, School of Medicine: Department of Medicine: General Internal Medicine – University of Washington
  • Overall Official(s)
    • Graham Nichol, MD, MPH, Principal Investigator, University of Washington
    • Emilby S Bartlett, MD MS, Principal Investigator, University of Washington
  • Overall Contact(s)
    • Graham Nichol, MD, MPH, 206-521-1722, ricstudy@uw.edu

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