A Phase II, Randomized, Double-Blind Pilot Trial of VIVITROL® (Naltrexone for Extended-Release Injectable Suspension) for the Treatment of Cocaine and Alcohol Dependence
Overview
- Phase
- Phase 2
- Intervention
- VIVITROL (Naltrexone extended-release injectable suspension)
- Conditions
- Cocaine Dependence
- Sponsor
- University of Pennsylvania
- Enrollment
- 80
- Locations
- 1
- Primary Endpoint
- Urine Assay for Benzoylecgonine (BE), the Primary Metabolite of Cocaine.
- Status
- Completed
- Last Updated
- 8 years ago
Overview
Brief Summary
To evaluate the efficacy of VIVITROL (naltrexone for extended-release injectable suspension) for the treatment of co-occurring cocaine and alcohol dependence
Detailed Description
This is a Phase II double-blind randomized controlled clinical pilot study. The exploratory objectives in the proposed study will be examined with a 2-group design to assess the efficacy of naltrexone extended-release injectable suspension (VIVITROL™) as compared to placebo. Safety measures will be collected weekly through medical management (MM) by medical practitioners, including adverse events and concomitant meds. The psychosocial treatment will be Cognitive Behavioral Coping Skills Therapy (CBT). Subjects will be 80 men and women with current DSM-IV diagnoses of alcohol dependence and cocaine dependence that will be randomized to receive either VIVITROL or placebo (40 subjects per group). All subjects will receive weekly sessions of CBT and MM. The study length for each subject is comprised of 1-3 weeks of screening, an 8-week double-blind, placebo-controlled trial with MM and CBT (medication phase), and an end of medication visit. Primary Exploratory Objectives: * To compare medication groups' rates of cocaine abstinence, as determined by urine assay for benzoylecgonine (BE), the primary metabolite of cocaine. This will be cross-checked against participants' self-reports of cocaine use through Time-Line Follow Back (TLFB)(Sobell \& Sobell, 1992). * To compare medication groups' rates of abstinence from drinking, and of clinically significant drinking, as measured by the TLFB. Secondary Exploratory Objectives: * To evaluate medication groups' reports of craving for cocaine and alcohol, as measured by scores on the Penn Alcohol Craving Scale and the Minnesota Cocaine Craving Scale during the medication treatment phase. * To compare women's reports of medication tolerance of naltrexone extended-release injectable suspension versus high dose oral naltrexone that was reported in our recently published pilot trial of high dose naltrexone for dual cocaine and alcohol dependence (Pettinati et al., 2008).
Investigators
Kyle Kampman
Principal Investigator
University of Pennsylvania
Eligibility Criteria
Inclusion Criteria
- Not provided
Exclusion Criteria
- •Positive urine drug screen and/or current DSM-IV diagnosis of any psychoactive substance dependence other than cocaine, alcohol, or nicotine dependence, as determined by the SCID.
- •Concomitant treatment with psychotropic medications, including opioid analgesics.
- •Patients mandated to treatment based upon a legal decision or as a condition of employment.
- •Current severe psychiatric symptoms, e.g., psychosis, dementia, suicidal or homicidal ideation, mania or depression requiring antidepressant therapy in the opinion of the Principal Investigator (PI).
- •Taken any investigational medication within the past 30 days.
- •History within the six months prior to randomization of significant heart disease (an arrhythmia which required medication, Wolff-Parkinson-White Syndrome, angina pectoris, documented history of myocardial infarction, heart failure). These are to be reviewed on a case-by-case basis: EKG 1st degree heart block, sinus tachycardia, left axis deviation, and nonspecific ST or T wave changes are allowed; liver function tests \[LFTs\] \<3 x ULN are acceptable).
- •Known hypersensitivity to naltrexone, PLG, carboxymethylcellulose, or any other components of the diluent.
- •Subjects with a BMI of 40 and above, as determined by the Body Mass Index Table, or that have distribution of adipose tissue such that they would be at greater risk of serious injection site reaction, based on clinical judgment. Participants with a BMI over 30 will have additional screening procedures conducted to determine inclusion in the study. These procedures include an additional screening measurement of waist-hip ratio for those participants with a BMI over
- •Males with a waist to hip ratio of \>0.9 and females with a waist to hip ratio of \>0.85 will be referred to the investigator for final decision of study inclusion. If the ratio is \<0.9 for men or \<0.85 for women they will be eligible for study inclusion without further action.
- •Patients with any serious illnesses that may require hospitalization during the study.
Arms & Interventions
1
VIVITROL (Naltrexone extended-release injectable suspension), 380 mg injection at the start of weeks 2 and 6
Intervention: VIVITROL (Naltrexone extended-release injectable suspension)
2
Placebo injection, 380 mg injection at the start of weeks 2 and 6.
Intervention: Placebo
Outcomes
Primary Outcomes
Urine Assay for Benzoylecgonine (BE), the Primary Metabolite of Cocaine.
Time Frame: 8 week medication phase
Percentage of subjects with no cocaine use for at least 3 weeks
Time Line Follow Back -Reported Days of Abstinence From Drinking
Time Frame: 8 week medication phase
Percentage of participants who were abstinent from drinking