A Randomized, Double-blind, Placebo-controlled, Parallel-group Study of Dexmedetomidine (Precedex®), With Lorazepam Rescue, for the Management of Severe Alcohol Withdrawal Syndrome (AWS) and Alcohol Withdrawal Delirium (AWD)
Overview
- Phase
- Phase 4
- Intervention
- Dexmedetomidine
- Conditions
- Alcohol Withdrawal Delirium
- Sponsor
- Denver Health and Hospital Authority
- Enrollment
- 49
- Locations
- 7
- Primary Endpoint
- The Length of ICU Stay Defined as the Time Between Randomization and ICU Transfer Orders.
- Status
- Terminated
- Last Updated
- 8 years ago
Overview
Brief Summary
This is a prospective, randomized, double-blind, placebo-controlled, parallel-group study of dexmedetomidine versus placebo, with lorazepam rescue, for the management of severe alcohol withdrawal syndrome (AWS) and alcohol withdrawal delirium (AWD) in critically ill adults.
The investigators hypothesize that the integration of dexmedetomidine (Precedex®) with usual therapy for the management of severe alcohol withdrawal syndrome (AWS) and alcohol withdrawal delirium/delirium tremens (AWD) in critically ill adult patients will reduce the time to resolution of AWS/AWD, increase the number of delirium-free and ventilator-free days in the first 28 days of hospitalization, reduce the length of ICU and hospital stays, and improve neurocognitive and quality of life scores on hospital discharge.
Detailed Description
Severe alcohol withdrawal syndrome (AWS) and alcohol withdrawal delirium (AWD) are frequent principal indication/s for admission to intensive care units. Additionally, unanticipated alcohol withdrawal complicates other critical illnesses and peri-operative states. Alcohol intoxication and withdrawal syndrome are characterized by classic symptoms of adrenergic activation, psychiatric agitation including seizures, as well as metabolic and respiratory dysfunction. The majority of patients with severe AWS are effectively managed with combinations of benzodiazepine (BZD) sedatives (e.g. lorazepam) and butyrophenone antipsychotics (e.g. haloperidol) and require intensive care admission for 2-3 days. However, almost 25% of patients with SAWS have a prolonged critical care course, often complicated by respiratory failure and associated with excessive sedation and risk for complications such as ventilator-associated pneumonia (VAP). AWS is frequently difficult to manage with usual care including benzodiazepines. Additionally, while intermittent bolus dose sedation is recommended for AWS, high dose BZD alone is associated with excessive respiratory suppression and metabolic acidosis. Such therapy increases the likelihood of respiratory failure with its attendant complications of hospital acquired pneumonia and sepsis. Further, patients with underlying chronic liver disease are at greater risk for prolonged sedative effects of BZD and progression of hepatic encephalopathy. The requirement for mechanical ventilation additionally prolongs the course of treatment for AWD because of the need for prolonged sedation. Strategies to control AWS/AWD that control symptoms but avoid adverse effects of excessive respiratory suppression are anticipated to improve the short and medium-term outcomes of AWS. BZD infusions have also been shown by several investigators to result in excessive and prolonged sedation. However, reasonable alternatives for effective control of psychomotor and adrenergic activation have until recently, been unavailable. The centrally acting alpha-2 receptor agonist, clonidine has been suggested as a useful adjunctive therapy to BZD. However, clonidine is only a mild sedative and can result in significant hemodynamic compromise. By contrast, dexmedetomidine (Precedex), a more potent alpha-2 receptor agonist, is potentially a more effective adjunctive therapy. Precedex is currently marketed in the USA for short-term use as a potent peri-operative sedative and analgesic. This agent has a short circulating half-life and has significantly fewer hemodynamic side effects than clonidine. In addition to its cardiovascular properties, dexmedetomidine possesses anxiolytic, hypnotic/sedative, anesthetic-sparing and analgesic actions and is devoid of significant respiratory depressant effects. Precedex has been shown to be a safe and effective single agent sedative for critically ill medical and surgical patients in prolonged infusions up to thirty days and is associated with significantly lower incidence of delirium than sedation with the benzodiazepine, midazolam. Preclinical experience and case reports suggest anecdotally Precedex may be of particular benefit in patients with SAWS. Measures of sedation and delirium will be assessed with the Minnesota Detoxification Scale (MINDS) derived for use in critically ill adults from the validated Clinical Institute Withdrawal Assessment (CIWA-r) scale.
Investigators
Ivor Douglas
Professor of Medicine
Denver Health and Hospital Authority
Eligibility Criteria
Inclusion Criteria
- •Male or female patients, 18 years or older, with severe AWS or AWD per DSM-IV definitions (below) requiring admission to the ICU for medical management
- •Ability to provide informed consent (via a proxy decision maker or patient).
- •Within 96 hours of ICU admission.
- •Meets DSM-IV diagnostic criteria for 291.8 Alcohol Withdrawal Syndrome:
- •Cessation of (or reduction in) alcohol use that has been heavy and prolonged.
- •Two (or more) of the following, developing within several hours to a few days after Criterion A:
- •autonomic hyperactivity (e.g., sweating or pulse rate greater than 100)
- •increased hand tremor
- •nausea or vomiting
- •transient visual, tactile, or auditory hallucinations or illusions
Exclusion Criteria
- •Age \< 18 years
- •Physician anticipates ICU transfer orders in less than 12 hours from time of consent.
- •Recent traumatic brain injury
- •Active status epilepticus
- •Pregnancy or lactation
- •Known allergy or adverse response to any of the study medications
- •Requiring glucocorticoid therapy for treatment of acute hepatitis or Stage III (advanced) decompensated liver failure and encephalopathy
- •Trauma or burns as admitting diagnoses
- •Neuromuscular blockade other than for intubation
- •Epidural or spinal analgesia
Arms & Interventions
Dexmedetomidine
Dexmedetomidine titrated to achieve predefined goals on selected components of the MINDS score using the minimum amount of medication possible. Blinded study medication will be started at a rate determined by the MINDS score. The maximum infusion rate is 1.4 μg/kg per hour. Uncontrolled SAWS/D symptoms, will be treated with open label lorazepam according to the MINDS score algorithm. Persistent SAWS/D symptoms despite maximum infusion rate of study medication treatment limiting symptoms while receiving higher infusion rates of study medication, ancillary therapies will be administered according to the MINDS score algorithm, at the discretion of the treating physician.
Intervention: Dexmedetomidine
Placebo
Blinded placebo study drug administration in equal volume per hour as active study medication arm.
Intervention: Placebos
Outcomes
Primary Outcomes
The Length of ICU Stay Defined as the Time Between Randomization and ICU Transfer Orders.
Time Frame: up to 28 days in hours
Secondary Outcomes
- Average MINDS Score(up to 28 days)
- The Number of CAM-ICU Negative Days After Randomization.(up to 28 days)
- Scores at Hospital Discharge on the Mini Mental Exam.(up to 28 days)
- Scores at Hospital Discharge on the Beck Depression Inventory.(Up to 28 days.)
- Scores at Hospital Discharge on the Beck Anxiety Inventory(Up to 28 days.)
- Scores at Hospital Discharge on the PTSD Civilian Checklist(Up to 28 days)
- Resource Utilization Costs Associated With This Hospitalization Billed by Physicians.(up to 28 Days)
- Resource Utilization Costs Associated With This Hospitalization Billed by Facility.(Up to 28 days)
- Number of Ventilator Free Days After Randomization.(up to 28 days)
- The Length in Days of the Hospital Stay(up to 28 days)