Vivitrol Vs. Suboxone

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Transcription:

Vivitrol Vs. Suboxone

Vivitrol - Naltrexone Indicated for opiate dependence and alcohol withdrawal pure antagonist 380mg once every 4 weeks IM Peak plasma concentration in 2 hrs, followed by a second peak in 2-3 days. Starts declining after about 14 days Metabolized by the liver, non-cytochrome P450 mechanism. Black box warning: Hepatotoxicity Side effects: site reactions, hypersensitivity, eosinophilic PNA, accidental overdose, depression/sucide Can cause pupillary constriction Requires wash out period (~1 week) Does not cause a disulfuram type reaction Reversal regional anesthesia

Suboxone Buprenorphine/Naloxone Indicated for opioid dependence Combination product containing a partial agonist and an antagonist Available in 4 strengths: buprenorphine 2mg/naloxone 0.5mg, 4mg/1mg, 8mg/2mg, 16mg/3mg, respectively Given via sublingual film as a single daily dose Schedule 3 abuse potential Poor bioavailability buprenorphine 10% if swallowed, 30-50% sublingually (vs. IV route). Naloxone 2-5% oral Variable absorption, peak plasma concentrations in 30min 3 hrs

Suboxone Buprenorphine/Naloxone Side effects: headache, N/V, Withdrawal symptoms, elevated LFTs, toungue pain Metabolized bia CYP2D6, CYP3A4 no black box warning Drug interactions! Anti-retrovirals, benzodiazepines. Requires induction period titrated to objective signs of withdrawal Buprenorphine monotherapy recommended for pt s taking long acting opiate

Vivitrol/Suboxone Comparison Study Summary Lee, J. D., Nunes, E. V., Novo, P., Bachrach, K., Bailey, G. L., Bhatt, S., & King, J. (2017). Comparative effectiveness of extended-release naltrexone versus buprenorphine-naloxone for opioid relapse prevention (X: BOT): a multicentre, open-label, randomised controlled trial. The Lancet.

HOW WAS THIS STUDY CONDUCTED? A randomized controlled trial to test Suboxone against Vivitrol in 570 individuals (287 receiving Suboxone and 283 receiving Vivitrol) for 6 months who were attending one of eight inpatient detoxification programs in the U.S. The primary outcome was relapse, measured after the first 3 weeks to prevent against detoxification-related, opioid medication from being counted as opioid use, and defined as one of the following: 4 consecutive weeks of opioid use determined by urine drug test (a missed drug test was counted as positive indicating use) 4 consecutive weeks of opioid use determined by self-report 7 consecutive days of self-reported opioid use Secondary outcomes were failure to initiate the medication, percent days using an opioid during the 6-month study period, and adverse events including overdoses.

HOW WAS THIS STUDY CONDUCTED? All participants had opioid use disorder according to the diagnostic and statistical manual of mental disorders, 5 th edition (DSM-5) and had used opioids in the past 30 days. While the sites differed in terms of how they helped individuals medically withdraw from opioids ( detox ), all were short-term (3-7 days) and part of a community program that provided at least weekly therapy sessions (group or individual) on an outpatient basis during the study. The study was conducted as part of the National Institute on Drug Abuse s Clinical Trials Network, which tests evidence-based treatments for substance use disorder in community settings. Of note, study site and severity in terms of opioid use were taken into account when randomizing patients to receive Suboxone vs. Vivitrol. All patients received medical management at each study visit including psychoeducation about opioid use disorder, an adherence plan, advice to abstain from all substance use, monitoring of side effects, and encouraging attendance at therapy and mutual-help groups. The medical management schedule was the same for both Suboxone vs. Vivitrol weekly for the first month, then every two weeks for the next 3 months, then every month for the final 2 months. Suboxone doses ranged from 8 to 24 mg depending on clinical need. Vivitrol was administered every 28 days, and of course, individuals needed to be abstinent from all opioids for at least 3 days, have a toxicology screen negative for opioids, and pass a naloxone challenge to be sure they would not withdraw from the Vivitrol.

Characteristics of Study Sample? 34 years old, on average, 70% male, 75% White and 10% Black and 13-20% Latino. Most (80%) were heroin users, more than 60% were injection drug users, and 35-40% had prior treatment. Other substance use in the past 30 days was common: 47-57% with stimulant use, 25-32% with sedative use, 42-48% with cannabis use, and 25-27% with heavy drinking, which was not defined by authors but, according to the Substance Abuse and Mental Health Services Administration (SAMHSA), means 5 or more drinks for men or 4 or more for women on the same occasion at least 5 days in the past month. Nearly 70% reported a lifetime history of another psychiatric disorder, and they had mild depressive symptoms, on average, measured by the Hamilton Depression Scale. Individuals were not able to participate in the study if they had serious medical, psychiatric, or substance use disorder as determined by the study physician.

Keith Humphreys, a drug policy expert at Stanford who was involved in the Lancet study, summarized the findings: If you get on the medication, both are equally effective, but it s harder to get on naltrexone because you need the detoxification first. WHAT DID THIS STUDY FIND? 15 patients assigned to Vivitrol had an overdose (two fatal) and eight assigned to Suboxone had an overdose (three fatal). In other words, 23 of the 570 patients in the entire trial had an overdose, five of whom died, during the study period less than 1%

WHAT DID THIS STUDY FIND? In the Suboxone group, 57% relapsed during the study, significantly less than the 65% who relapsed in the Vivitrol group (i.e., unlikely due to chance a reliably large difference). As seen in the figures below, out of 24 weekly tox screens, Suboxone individuals had 10 negative opioid tox screens, and Vivitrol individuals had four negative opioid tox screens, on average. Out of 144 days, by self-report Suboxone individuals had 81 opioid abstinent days and Vivitrol 39 abstinent days. The Suboxone group also had a significantly longer time until they relapsed, on average (14 weeks vs. 8 weeks). More specifically, in any given week, if one person was abstinent in the Suboxone group and a similar person was abstinent in the Vivitrol group, the person in the Suboxone group had a 36% higher odds of avoiding relapse that week. The good and the bad news: If you can t start it, it isn t equal

WHAT DID THIS STUDY FIND? One noteworthy nuance from this study is that the advantage of Suboxone occurred early in the first 6 weeks. For those who make it past 6 weeks, Vivitrol begins to show an advantage. Another distinction is that the advantage for Suboxone appears to come from the tougher time that individuals experienced who were assigned to Vivitrol when getting started on the medication 94% of individuals assigned to Suboxone were successfully started (also called induction ) while only 72% of those assigned to Vivitrol were successfully started on the medication. When only the individuals successfully started on medication were analyzed, the Suboxone and Vivitrol outcomes were similar. Also, Vivitrol individuals were more likely to be successfully started on the medication if entered the study more than 3 days after the last opioid use compared to less than 3 days after their last opioid use (84% started vs 53%, respectively). So having at least a few days abstinent made a difference for Vivitrol patients

BOTTOM LINE For scientists: In this multisite randomized controlled trial comparing Suboxone to Vivitrol on relapse risk (i.e., 4 consecutive weeks of opioid use) over 6 months among individuals recently entering detoxification with a plan to transition to outpatient treatment, Suboxone outperformed Vivitrol, primarily because more individuals assigned to Suboxone were able to get started on the medication right away. While there are many potential next steps, primary among these are investigations of medication moderators, as well as how to boost medication outcomes given that even in this highly rigorous trial, more than half of the Suboxone group relapsed.

BOTTOM LINE For policy makers: Suboxone and Vivitrol both help reduce craving and protect against relapse. Vivitrol, however, is harder to start as it requires a period of at least a few days of opioid abstinence. Policies to increase the dissemination of these evidence-based medications for opioid use disorder would likely decrease the health, criminal justice, and financial burdens attributable to the opioid overdose epidemic and opioid use more broadly. More than half of individuals relapsed during the 6 month trial, even in the highly rigorous and controlled circumstances of a clinical trial as was the case here.

BOTTOM LINE For treatment professionals and treatment systems: Suboxone and Vivitrol both help reduce craving and protect against relapse. If choosing between one or the other to reduce opioid use: Suboxone is the better choice in outpatient settings, while Suboxone and Vivitrol will fare similarly, on average, in an inpatient setting, where programs have the benefit of an extended detoxification if needed. More research is needed to further improve outcomes for individuals with opioid use disorder. For example, research on what types of other clinical and recovery support services can be integrated with medication to potentially improve outcomes is needed. Also, studies that investigate which individuals, in particular, may be more or less likely to benefit the most from each specific medication are needed.

BOTTOM LINE The research is clear: Medication-assisted treatment works The key with medication-assisted treatment is that while it does involve continued drug use (dope substitution), it turns that drug use into a much safer habit. So instead of stealing to get heroin or using painkillers so much that he puts his life at risk, a patient on medication-assisted treatment can simply use methadone or buprenorphine to meet his physical cravings and otherwise go about his day going to school, work, or any other obligations. The fight over medication-assisted treatment is really about how we see addiction As Stanford psychiatrist and author Anna Lembke put it, If you see somebody who continues to use despite their lives being totally destroyed losing their jobs, losing loved ones, ending up in jail nobody would choose that. Nobody anywhere would ever choose that life. So clearly it is beyond this individual s control on some level.

BOTTOM LINE The research backs this up: Various studies, including systematic reviews of the research, have found that medication-assisted treatment can cut the all-cause mortality rate among addiction patients by half or more. Just imagine if a medication came out for any other disease and, yes, health experts consider addiction a disease that cuts mortality by half; it would be a momentous discovery.

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