Case Presentation
“Ms. B” is a 28-year-old woman with a 4-year history of illicit prescription opioid use by the oral and nasal routes. She began by occasionally sharing pills with friends at parties, then progressed to 1–2 pills a day and steadily increased to an average of 250–350 mg of oxycodone or its equivalent per day but sometimes taking up to 450 mg a day. She sporadically inhaled heroin but denied injecting it, and she was consuming 5–9 drinks (mixed or straight vodka) 6–7 nights per week. She had attended community college for a year but did not graduate, and she was working in a medical office. She obtained opioids by buying them “on the street,” by “doctor shopping” using a vague complaint of back injury with severe pain, or by forging prescriptions, carefully rotating the pharmacies where she filled them to avoid raising pharmacists' suspicions. She debated with herself about quitting because she felt that her life was “ruined and going nowhere,” and she sought treatment because she became frightened after nearly getting caught stealing prescription pads at work. She also reported feeling sad, with crying spells and feelings of hopelessness and self-deprecation, but without suicidal ideation.
Ms. B was addicted to prescription opioids and alcohol and was also depressed; although she acknowledged an opioid problem, she did not initially acknowledge her alcohol problem. The main reason she sought treatment was the anxiety she experienced after nearly getting caught stealing prescription pads. Her acute anxiety was situational, but it was unclear whether her long-standing depression was substance induced or an independent disorder.
Ms. B had heard about buprenorphine from friends, and she agreed to office-based treatment with counseling and pharmacotherapy with a buprenorphine-naloxone preparation. She was started on a daily dose of 8 mg/2 mg, which was increased to 12 mg/3 mg on day 2, to 16 mg/4 mg on day 4, and then, in gradual increments, to 24 mg/6 mg by the third week, at which point she reported that opioid cravings and withdrawal were suppressed for the entire day. She experienced mild alcohol withdrawal shortly after treatment began, with tremulousness and tachycardia that resolved with 200 mg of chlordiazepoxide in divided doses over 2 days. Psychosocial treatment included intensive outpatient group counseling three times a week, individual therapy with a social worker, medication management by an addiction psychiatrist, and encouragement to participate in Narcotics Anonymous (NA).
She was strongly motivated to stop opioids and quickly reduced her use from daily to twice weekly and from many to 1–2 pills a day, and by the fourth week she stopped use altogether. She was ambivalent about abstaining from alcohol, and her belief in her ability to drink in moderation fluctuated; she continued binging with 4–5 drinks at a time, 2–4 nights per week. Therapy focused on encouragement and praise for progress and feedback that highlighted her problematic alcohol and opioid use and the discrepancies between her intentions and her actual behaviors. After 8 weeks, Ms. B was persuaded that she could not limit her drinking, and she stopped altogether and committed to total abstinence.
Ms. B's depressive symptoms continued, and by the second week she agreed to a trial of sertraline. Her initial intention was to take buprenorphine-naloxone for brief detoxification; she expressed disdain for the possibility of becoming dependent on it as a mere “substitute.” But as her opioid use stopped and her depressive symptoms improved, she became more comfortable with continuing buprenorphine-naloxone for an indefinite period and agreed to defer any decision about tapering until she felt “strong enough.” She continued buprenorphine-naloxone, and after 3 months of intensive outpatient group therapy, she stepped down to one group and individual counseling session per week and monthly physician visits.
Around month 4, Ms. B stopped attending group therapy, expressing financial difficulties and the feeling that she no longer needed it. Around month 5, citing personal incompatibility, she stopped seeing her therapist and declined to increase the frequency of physician visits, which was offered as a replacement. At month 6, she began a relationship with a man she met at an NA meeting and began complaining of anorgasmia from sertraline. The sertraline dosage was decreased from 200 to 150 mg/day, and while the anorgasmia improved, depressive symptoms returned despite having maintained opioid and alcohol abstinence. The sertraline dosage was restored to 200 mg, but her depression did not improve, and she was switched to escitalopram, which produced only modest improvement. Augmentation with lithium was tried but stopped after a few doses because it made her feel “weird.”
Ms. B's stressors continued, among them mounting financial difficulties and romantic disappointment when her new boyfriend relapsed to heavy drinking and it took a month for her to break off the relationship. A friend invited her to a party at which she relapsed to drinking, and she soon stopped taking buprenorphine-naloxone and relapsed to opioid use as well. After 2 weeks of intermittent binging on alcohol and prescription opioids, she presented at an urgently scheduled visit saying that she had not been taking her medications, had again stopped using opioids and alcohol for 3 days, was miserable, and wanted to get “back on track.” She was restarted on buprenorphine-naloxone and sertraline; the sertraline was titrated to 300 mg/day, and risperidone, 0.5 mg h.s., was added. With ongoing encouragement, she agreed to reengage in NA, and after a few weeks she started with a new therapist. She maintained abstinence and remission from depression for 6 months.
Opioid Dependence Treatments
Opioid dependence typically has a chronic, relapsing course (
5,
6) that can be interrupted by medication-assisted therapy using naltrexone, methadone, or buprenorphine. Adherence to naltrexone treatment has been poor except in highly motivated patients who are often under strong external pressure (
7), but this situation may be changing with the introduction of extended-release formulations (
8,
9), such as a once-monthly injectable formulation (Vivitrol) that has been approved by the U.S. Food and Drug Administration for preventing relapse to opioid addiction (
10). Methadone has been the mainstay of treatment in the United States and most other countries.
Buprenorphine is a schedule III medication with partial μ-opioid agonist effects. It binds very tightly to receptors, such that it will displace full agonists. Sublingual tablets are available with buprenorphine alone or with buprenorphine and naloxone in a 4:1 combination. Tablets take 3–6 minutes to dissolve and do not work if swallowed, because of first-pass metabolism. The combination product was developed to reduce abuse since naloxone precipitates withdrawal if injected by someone addicted to a full agonist. This strategy appears to be working fairly well (
11–
14), but not for persons abusing only buprenorphine.
As a partial agonist, buprenorphine has a plateau effect such that for most patients, increasing the dosage beyond 16 mg/day increases the duration but not the magnitude of its effects (
15). This property appears to markedly reduce its overdose risk (
16,
17). Buprenorphine dissociates more slowly from μ-opioid receptors than do full agonists, resulting in a less severe withdrawal (
18). However, this property does not seem to reduce relapse rates following detoxification (
6). Buprenorphine can be prescribed by any physician qualified through specialty certification in addiction medicine or addiction psychiatry or completion of at least 8 hours in an approved certification course (
19). The availability of buprenorphine outside the highly controlled methadone system has expanded treatment options for opioid-dependent persons (
20), and the buprenorphine-naloxone combination has been increasingly adopted, with high levels of satisfaction and with positive outcomes (
21,
22).
It is important to administer the first dose of buprenorphine only when the patient is in moderate to severe withdrawal, to avoid precipitating withdrawal. A common starting dose is 4–8 mg, and if this is well tolerated, the usual practice is to make successive 4-mg increases to maintenance levels of 16–32 mg/day over the next 1–14 days. The most conservative approach is to require daily visits for dose adjustments during the first 3–5 days, although some clinicians successfully educate patients to manage their own induction at home (
23,
24). For ongoing treatment, the most common approach is to gradually spread out visits with increasing prescription supplies, with a maximum interval of 1 month.
Comorbid Disorders
Although Ms. B's main problem was prescription opioids, she was also depressed and alcohol dependent—common problems in persons with substance use disorders (
1). It is often difficult to know whether mood symptoms are substance induced or an independent disorder; however, both problems increase the risk of relapse. Substance-induced depression typically clears with abstinence, carries less relapse risk than depression that is independent of the substance use disorder, and is less likely to require additional ongoing psychiatric treatment (
25,
26). DSM-IV-TR guidelines suggest a diagnosis of an independent disorder rather than substance-induced dependence if symptoms persist for more than 4 weeks before the onset of substance use or during 1 month or more of remission or are disproportionate to agonist or withdrawal effects of the substance(s). The timing of treatment initiation is a matter of judgment and, to some degree, of the time available to decide. Ms. B was an outpatient, so decisions about antidepressant treatment had to be made sooner rather than later.
Buprenorphine is compatible with most psychiatric medications. However, a handful of deaths have been linked to concurrent abuse of benzodiazepines (
17,
27,
28). This has led to concern about buprenorphine use in patients abusing benzodiazepines or taking them for anxiety disorders or alcohol detoxification. Because overdose deaths have generally been associated with injection of high doses of buprenorphine and benzodiazepines, the risk-benefit ratio of clinically appropriate doses in medically supervised detoxification from alcohol or benzodiazepines is probably favorable, but careful monitoring is recommended.
There are a few case reports of elevated liver enzymes associated with buprenorphine, but its role is unclear. Periodic monitoring of liver enzymes is advisable in patients with clinically significant liver disease but is not needed otherwise. Compared to methadone, buprenorphine has few clinically significant interactions with antiretroviral medications (
29) and is less likely to prolong QTc intervals (
30–
32). In pregnant patients, use of the buprenorphine-only product is recommended because of uncertainty about the effects of naloxone on the fetus.
Treatment Components and Duration
Counseling, psychotherapy, and urine testing are essential components of treatment and increase the impact of pharmacotherapy for many patients. Office-based opioid treatment providers often refer their patients to substance abuse counselors, social workers, psychologists, or nurses for counseling, but physicians also can provide counseling as a component of medication management. Many clinicians recommend weekly urine testing early in treatment, expecting that patients will have some ongoing use, which can be addressed using prescription interval as a contingency to encourage an improving trajectory to abstinence.
As with methadone, high relapse rates have been seen after dosage tapering in buprenorphine studies (
6,
19) and longer treatment duration has been associated with better outcomes (
33). Early reports of outcomes in general medical settings have been favorable, with retention in buprenorphine treatment ranging from 40% to 70% at 6 months (
34–
36) and 38% to 52% at 18–24 months (
33,
37).
Many patients want to transition off buprenorphine-naloxone as soon as possible and ask about treatment duration at the outset, often because of concerns about becoming “dependent” on medication. One way to address such concerns is to avoid the sometimes-charged term “maintenance” and encourage “extended stabilization” until opioid and other drug use stops before discussing tapering. Another strategy is to emphasize a “functional clock,” asking patients to plan on continuing medication until they have not only stopped drug use but also accomplished important goals in the domains of work, school, family, or criminal justice system involvement. After discontinuation of medication, practitioners often recommend continuing involvement in counseling and/or 12-step groups and encourage patients to restart buprenorphine promptly in the event of a relapse.
Conclusions
Buprenorphine is an effective treatment for opioid dependence when used as directed, and if diverted or abused, it carries less risk of overdose than methadone or other full agonists. The combination product is recommended (except during pregnancy) because it appears to have lower abuse liability than the monotherapy product. It can be prescribed in specialized addiction treatment programs or through office-based treatment by certified physicians in any medical practice, including addiction medicine, psychiatry, and primary care. It may not work as well as methadone for some patients, but it has made agonist treatment more accessible to patients who needed it but were unwilling or unable to participate. It may assist with engaging patients in an array of ongoing complementary treatments. The case presented here reviews its use to treat a patient who was addicted to prescription opioids and alcohol, had comorbid depression, was ambivalent about stopping alcohol use, and felt demoralized by interpersonal problems. The treatment course was not always smooth, but through coordinated pharmacological and psychosocial interventions over several months, the case of Ms. B depicts characteristic positive outcomes. Buprenorphine as part of a comprehensive medication-assisted recovery approach—combined, for example, with counseling, treatment of additional nonopioid substance use disorders, and treatment of comorbid psychiatric illness—provides an important tool for relapse prevention and should be a mainstay of the standard repertoire for treating opioid dependence.