Opioid-Related Disorders Clinical Trial
Official title:
Clonidine for Relapse Prevention in Buprenorphine-Maintenance Patients
Background:
- Though the drug buprenorphine effectively treats dependence on opioids like heroin, some
abstinent patients relapse to use during treatment. This relapse may be triggered by
stress or stressful situations, and buprenorphine probably has no specific protective
effect in these situations. Buprenorphine probably also has no specific effect on
relapse to cocaine use.
- Research has shown that clonidine, a drug originally prescribed to treat high blood
pressure and some symptoms of opioid withdrawal, can help block stress-induced relapse
to heroin and cocaine seeking in rats. Researchers are interested in studying whether a
combination of clonidine and buprenorphine may be more effective in preventing drug
relapse than administering one of the medications alone.
Objectives:
- To determine whether clonidine, given to abstinent patients maintained on buprenorphine, is
more effective than placebo in preventing relapse to heroin or cocaine use.
Eligibility:
- Individuals between 18 and 50 years of age who are current cocaine or heroin users seeking
treatment.
Design:
- The study will last up to 36 weeks, with four phases of treatment and a follow-up
evaluation. Three times a week, participants will be asked to report illicit drug use
and provide urine and breath samples. Throughout the study, participants will receive
individual counseling in weekly 40 60 minute sessions. Other samples and tests will be
scheduled as required by the study researchers.
- Patients will be stabilized on daily buprenorphine over the first 14 days of the study.
- Weeks 1 8: Participants will receive vouchers for regular substance-free urine samples.
Those who successfully complete this phase will continue to the next part of the study.
- Weeks 7 9: Participants will receive either clonidine or placebo along with the
buprenorphine. The dose of clonidine will be stabilized during this time.
- Weeks 9 22: Participants will continue to receive either clonidine or placebo along with
the buprenorphine. During this part of the study, participants will keep electronic
diaries to record drug use or craving and to record data on mood, stress levels, and
activity.
- Weeks 23 28: Participants will stop taking the clonidine or placebo, but will continue
the buprenorphine treatment. Participants will continue to keep electronic diaries.
- Weeks 29 36: Participants will have the choice of transferring to a community clinic
transfer or gradually reducing doses of buprenorphine to end the study.
- Participants will return for a follow-up visit and urine sample 6 months after the end
of the study.
Background. Though buprenorphine effectively treats opioid dependence, some abstinent
patients relapse to maladaptive use of opioids during treatment. Relapse may be triggered by
stress. Rodent studies have demonstrated that stress can induce relapse to heroin and cocaine
use (Erb, et al., 1996; Shaham, et al., 1996; Shaham and Stewart, 1995). In a rodent model,
stress-induced relapse to heroin and cocaine seeking is blocked by the alpha-2 adrenergic
agonist clonidine. In this study, clonidine will be compared to placebo in preventing relapse
to opioid abuse in opioid maintained patients who have achieved abstinence while on
buprenorphine and contingency management.
Scientific goals. To determine whether clonidine, given to abstinent patients maintained on
buprenorphine, prevents relapse to opioid use more effectively than placebo.
Participant population. 300 opioid-dependent outpatients (120 evaluable). Target enrollment
will include 40 persent women and 60 percent minorities (mostly African-American).
Experimental design and methods. The study will be a randomized double-blind clinical trial.
Two treatment groups will be studied (60/group), one receiving clonidine and the other
receiving placebo. Assignment to treatment group will be randomized. All patients will
receive buprenorphine daily (8 mg to 24 mg SL) and individual counseling weekly throughout 28
weeks of treatment. In order to establish abstinence prior to clonidine induction, after one
week of stabilization on buprenorphine, they will receive contingent vouchers for
opioid-negative urine specimens for 8 weeks (weeks 1-8). Patients who are abstinent from
illicit opioids during weeks 5 and 6 will be randomized to receive clonidine (0.3 mg oral
dose) or clonidine placebo from weeks 9 through 20. Participants who are not abstinent will
be switched to methadone for four weeks (usual dose from 50 mg to 100 mg) followed by an
eight week methadone taper. Assignment to clonidine or placebo will be double-blind. Weeks 21
and 22 will include a clonidine taper to avoid rebound hypertension. From weeks 23-28,
participants will receive buprenorphine and counseling only, and then will be offered
assistance to transfer to another program; those who do not transfer will undergo an 8-week
buprenorphine taper. The primary outcome measures will be longest duration of opioid
abstinence, time to relapse, and the proportion of opioid-negative urine specimens over time
during the Intervention phase. In addition, fluctuations in drug use, drug craving, stress,
and HIV-risk behaviors such as injection drug use will be assessed via ecological momentary
assessment (EMA).
Benefits to participants and/or society. Participants will receive buprenorphine, drug
counseling, and contingency-management therapy. The buprenorphine and voucher interventions
are likely to reduce participants' use of opioids. Counseling will include reduction of HIV
risk behaviors.
Risks to participants. Participants may experience side effects from clonidine,
buprenorphine, or methadone and discomfort during withdrawal from each drug. In particular,
discontinuation of clonidine may cause rebound hypertension. The EMA component of the study
may generate some assessment burden.
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