Adrenergic Blockade After Subarachnoid Hemorrhage
Overview
- Phase
- Not Applicable
- Intervention
- Esmolol
- Conditions
- Subarachnoid Hemorrhage
- Sponsor
- University of Michigan
- Locations
- 1
- Primary Endpoint
- Change in high sensitivity troponin
- Status
- Withdrawn
- Last Updated
- 11 years ago
Overview
Brief Summary
The purpose of this study is to evaluate the clinical effect of esmolol treatment on cardiac function and electrophysiology; to assess the effects of esmolol treatment on serum adrenergic and cardiac biomarkers; to explore the safety of esmolol treatment shortly after subarachnoid hemorrhage (SAH). Patients will be followed for a maximum of 1 month after the index SAH. The primary outcome will be change in systolic function - ejection fraction by Simpson's rule (baseline versus Day 7 +/- 2 after SAH).
Detailed Description
Subarachnoid hemorrhage (SAH) remains one of the most devastating forms of stroke. Over 25% of all stroke related potential years of life lost are from SAH. Outcomes are adversely affected by secondary ischemia from cerebral vasospasm, along with cardiac complications. Trials performed in patients with SAH have demonstrated benefit after the administration of beta blockers - reducing mortality nearly in half; but concerns over diminishing cerebral perfusion inhibited the widespread adoption of this therapy. Our specific aims are as follows: 1. To evaluate the clinical effect of esmolol treatment on cardiac systolic and diastolic function, along with cardiac electrophysiology; 2. To assess the effects of esmolol treatment on serum adrenergic and cardiac biomarkers; 3. To explore the safety of esmolol shortly after SAH. The primary outcome will be change in systolic function - ejection fraction by Simpson's rule (baseline versus Day 7 +/- 2 after SAH).
Investigators
William J Meurer
Assistant Professor
University of Michigan
Eligibility Criteria
Inclusion Criteria
- •Subarachnoid hemorrhage presumed to be the result of ruptured aneurysm
- •Age 18 years old or greater
- •Able to enroll within 24 hours of onset of symptoms
- •Systolic blood pressure over 140 mm Hg OR administration of antihypertensives after presentation
Exclusion Criteria
- •Withdrawal of life support imminent (within six hours)
- •Known heart failure or cardiomyopathy AND ejection fraction 35% or below
- •Prisoner or pregnant female
- •Ongoing vasopressor administration to maintain SBP, or clinical suspicion of left ventricular failure
- •Clinically important arrhythmias (history of cardiac arrest or ventricular arrhythmias), conduction abnormalities (Mobitz Type 2, 3rd degree AV block, or symptomatic Mobitz 1 without pacemaker), clinical cardiogenic shock, or overt clinical heart failure
- •Active bronchospastic disease (ongoing bronchospasm after SAH presentation or current treatment with oral corticosteroids for asthma or obstructive lung disease)
- •End stage renal disease
Arms & Interventions
esmolol
Esmolol will be used preferentially to control hypertension.
Intervention: Esmolol
Outcomes
Primary Outcomes
Change in high sensitivity troponin
Time Frame: Peak to nadir within 7 days
Secondary Outcomes
- Proportion with depressed ejection fraction on initial echocardiogram 36 - 49%(Baseline (within 24 hours of presentation for index SAH))
- Proportion with life-threatening arrhythmias or cardiac arrest(Measured through end of index hospitalization (approximately 30 days maximum))
- Change in serum troponin and BNP levels from peak to nadir(baseline through end of hospitalization)
- Proportion with abnormal 30-day echocardiogram(30 days post index SAH)
- Proportion with symptomatic cerebral vasospasm(baseline until end of hospitalization)
- Proportion with radiographic cerebral vasospasm(baseline until end of hospitalization)
- Change in systolic function - ejection fraction by Simpson's rule (baseline vs Day 7 +/- 2)(5-7 days)
- Mean difference in time weighted average amount of cerebral perfusion pressure below 60 mmHg.(Measured for 4 days from index SAH)
- Proportion experiencing serious adverse event: hypotension requiring vasopressor (excluding during anesthesia), neurological deterioration, serious bronchospasm, and in hospital case fatality.(Measured during index hospitalization or first 30 days from index SAH)
- Disability (30 days +/-7).(30 days from index SAH)
- Change in serum norepinephrine level from peak to nadir(Baseline versus 4th day after index SAH)
- Change in corrected QT interval(First week after presentation for index SAH)
- Proportion with echocardiographic wall motion abnormalities at baseline and day 7 +- 2(First week after presentation.)
- Proportion with electrocardiographic abnormalities cumulative through day 7(Baseline, and at first week after presentation.)