Key Takeaways

  • Naltrexone is an FDA-approved medication for alcohol use disorder that reduces the urge to drink and the reward of drinking — with strong evidence from multiple randomized clinical trials.
  • Despite proven effectiveness, only about 8% of people with alcohol use disorder receive any medication — naltrexone remains severely underutilized.
  • Naltrexone works by blocking opioid receptors, which are involved in the rewarding effects of alcohol. It blunts the euphoria of drinking, making alcohol less appealing over time.
  • Vivitrol, a once-monthly injectable form of naltrexone, eliminates the need for daily pills and significantly improves medication adherence.
  • Naltrexone is most effective when combined with behavioral therapy — particularly the Sinclair Method (targeted naltrexone) and cognitive behavioral therapy.

In This Article

  1. What Is Naltrexone?
  2. How Naltrexone Works for Alcohol
  3. What the Research Says
  4. Oral vs. Injectable (Vivitrol)
  5. The Sinclair Method
  6. Who Benefits Most
  7. Side Effects & Precautions
  8. Naltrexone vs. Other AUD Medications
  9. How to Get Started
  10. FAQs

What Is Naltrexone?

Naltrexone is an opioid antagonist — a medication that blocks opioid receptors in the brain without producing any opioid effects itself. It was originally developed and FDA-approved for opioid use disorder in 1984, and received FDA approval for alcohol use disorder (AUD) in 1994. It is available as a daily oral tablet (ReVia, generic naltrexone) and as a once-monthly injectable formulation (Vivitrol).

According to the National Institute on Alcohol Abuse and Alcoholism (NIAAA), naltrexone is one of three FDA-approved medications for alcohol use disorder — alongside acamprosate and disulfiram — and has among the strongest evidence bases of the three for reducing heavy drinking days. Despite this, it remains dramatically underused: SAMHSA data consistently shows that fewer than 10% of people with AUD receive any pharmacotherapy.

<10%
of people with AUD receive FDA-approved medication (SAMHSA)
30%
reduction in heavy drinking days with naltrexone vs. placebo (meta-analysis)
1994
Year naltrexone received FDA approval for alcohol use disorder

How Naltrexone Works for Alcohol

Alcohol produces many of its rewarding effects — including euphoria, relaxation, and stress reduction — by indirectly stimulating the brain's opioid system. When alcohol is consumed, it triggers the release of endorphins that bind to opioid receptors in the reward circuitry. This opioid activity is a major driver of the pleasurable "buzz" of alcohol and the craving to drink more.

Naltrexone blocks mu-opioid receptors, preventing endorphins released by alcohol consumption from binding to them. The result: drinking produces less euphoria, less of a "buzz," and less reinforcement of the urge to keep drinking. Over time, this pharmacological "extinction" of the alcohol reward reduces cravings and makes it easier to cut down or stop.

Naltrexone Does Not Make You Sick When You Drink

This is a critical point of confusion. Naltrexone is NOT disulfiram (Antabuse), which causes nausea and vomiting if alcohol is consumed. Naltrexone simply reduces the reward of drinking — it has no aversive reaction to alcohol. This makes it safer and often more acceptable to patients who are not yet fully committed to abstinence.

What the Research Says

Naltrexone has been studied in over 50 randomized controlled trials and multiple systematic reviews. The evidence consistently shows clinically meaningful benefits:

  • A landmark Cochrane systematic review of 50 RCTs found naltrexone significantly reduced the rate of return to heavy drinking (relative risk 0.83) and the number of drinking days per month compared to placebo.
  • The COMBINE Study (JAMA, 2006) — the largest AUD medication trial in history with 1,383 participants — found that naltrexone combined with medical management produced significantly better outcomes than placebo on the primary drinking outcome measures.
  • The injectable Vivitrol formulation showed particularly strong results in a pivotal trial published in Archives of General Psychiatry, with a 25% reduction in heavy drinking days compared to placebo, and even stronger results in patients who abstained in the week before starting treatment.
  • A 2014 meta-analysis in JAMA Psychiatry found naltrexone produced a number needed to treat (NNT) of about 12 to prevent one person from returning to heavy drinking — comparable to the NNT of many widely-accepted medical treatments.

Oral Naltrexone vs. Vivitrol (Injectable)

FeatureOral Naltrexone (ReVia)Injectable Naltrexone (Vivitrol)
Dose50mg tablet, once daily380mg injection, once monthly
AdherenceRequires daily pill-taking; easy to skipOnce-monthly; eliminates daily adherence problem
CostLower — generics widely availableHigher — but often covered by insurance
Best forMotivated patients with good daily routinePatients with adherence challenges or severe AUD
FlexibilityCan stop any day; Sinclair Method-compatibleLess flexible — 28-day commitment per injection

The Sinclair Method

The Sinclair Method (TSM) is a specific protocol for naltrexone use developed by Finnish researcher David Sinclair, PhD. Rather than requiring abstinence before and during treatment, TSM instructs patients to take naltrexone one hour before every drinking occasion — and to allow themselves to drink as usual after taking the medication.

The theory: by repeatedly experiencing drinking without the opioid-mediated reward, the brain gradually "unlearns" the association between alcohol and pleasure through pharmacological extinction. Over months, most patients find their craving for alcohol decreasing naturally, and many achieve significant reduction or abstinence without being forced into immediate abstinence.

TSM Research Results

A Finnish study of TSM published in Alcohol and Alcoholism found that 78% of patients achieved either controlled drinking or complete abstinence after 3 years of TSM use. The Sinclair Method is particularly appealing to patients who are not ready to commit to immediate abstinence, as it works with drinking rather than against it — at least initially.

Who Benefits Most from Naltrexone

Research has identified several patient characteristics associated with stronger responses to naltrexone:

  • Family history of alcoholism: Patients with a positive family history of AUD show larger reductions in alcohol craving and consumption on naltrexone — possibly reflecting genetic differences in opioid receptor density or function.
  • High craving: Patients who report intense cravings for alcohol tend to respond better to naltrexone than those whose drinking is more habitual and less craving-driven.
  • OPRM1 gene variant (A118G): Research suggests that patients carrying the Asn40Asp variant of the mu-opioid receptor gene (OPRM1) may respond more strongly to naltrexone. Pharmacogenomic testing is available but not yet standard of care.
  • Early abstinence before starting: Patients who achieve even a brief period of abstinence before starting injectable Vivitrol tend to have better outcomes.

Interested in Naltrexone or Other AUD Treatment?

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Side Effects & Precautions

Naltrexone is generally well-tolerated, with most side effects mild and transient:

  • Common: Nausea (most common, especially in first week), headache, fatigue, anxiety, insomnia, decreased appetite
  • Injection site reactions (Vivitrol): Pain, tenderness, swelling at the injection site — occasionally severe with tissue necrosis in rare cases
  • Mood effects: Some patients report dysphoria or "emotional blunting" — particularly relevant for patients with co-occurring depression

Critical precautions:

  • Liver toxicity: Naltrexone can cause dose-dependent liver damage at very high doses. Liver function tests should be checked before starting and periodically during treatment. Naltrexone is contraindicated in acute hepatitis or liver failure.
  • Opioid use: Naltrexone is absolutely contraindicated in patients who are physically dependent on opioids — it will immediately precipitate severe withdrawal. Patients must be opioid-free for 7–10 days before starting naltrexone (longer for methadone). Always perform a naloxone challenge test before initiating in patients with recent opioid use.
  • Pain management: Naltrexone blocks opioid analgesia. Patients on naltrexone needing surgery or pain management must inform their medical team.

Naltrexone vs. Other FDA-Approved AUD Medications

MedicationHow It WorksBest ForKey Limitation
NaltrexoneBlocks opioid reward of alcoholReducing heavy drinking; patients with cravingsContraindicated with opioid use
AcamprosateReduces glutamate-driven craving after abstinencePatients committed to abstinence; post-detoxMust be abstinent; less effective for active drinkers
Disulfiram (Antabuse)Causes aversive reaction when alcohol consumedHighly motivated, externally monitored patientsDangerous cardiac/respiratory reactions if alcohol consumed; compliance issues

How to Get Started on Naltrexone

Naltrexone is available by prescription from any licensed physician, including primary care physicians, psychiatrists, and addiction medicine specialists. It does not require a special license to prescribe (unlike buprenorphine for opioid use disorder). Here are the steps:

  • Medical evaluation: Your provider will review your medical history, check liver function tests, and screen for opioid use to confirm naltrexone is safe for you.
  • Insurance verification: Most insurance plans cover oral naltrexone. Vivitrol requires prior authorization from most insurers but is usually covered. Our specialists can verify your benefits at no cost.
  • Treatment program: Naltrexone is most effective when combined with counseling. MAT programs, outpatient treatment, and IOP all incorporate naltrexone as part of comprehensive AUD treatment.

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Frequently Asked Questions

Yes. Multiple randomized controlled trials and meta-analyses confirm that naltrexone significantly reduces heavy drinking days, the rate of return to heavy drinking, and alcohol craving compared to placebo. It is FDA-approved for alcohol use disorder and endorsed by NIAAA, SAMHSA, and ASAM as a first-line treatment.
Not necessarily — unlike acamprosate, naltrexone can be initiated while someone is still drinking. The Sinclair Method specifically involves taking naltrexone before drinking occasions. However, for injectable Vivitrol, research shows better outcomes for patients who achieve even brief abstinence before the first injection.
No. Naltrexone is absolutely contraindicated in patients who are physically dependent on opioids. It will immediately precipitate severe opioid withdrawal. Patients must be completely opioid-free for at least 7–10 days (longer for methadone) before starting naltrexone.
Research suggests longer treatment produces better outcomes. Most guidelines recommend at least 3–6 months of naltrexone treatment, with many experts recommending 12 months or longer for patients with severe AUD. Naltrexone is generally continued as long as it is helping and the patient wishes to continue.
Yes — naltrexone carries a black box warning about hepatotoxicity (liver damage) at high doses. At standard doses for AUD (50mg oral or 380mg injectable monthly), liver toxicity is uncommon in patients with normal baseline liver function. Liver function tests should be monitored before and during treatment.
Yes. Vivitrol is the brand name for extended-release injectable naltrexone. It contains the same active ingredient as oral naltrexone but is formulated as a microsphere injection that releases naltrexone slowly over 28 days, eliminating the need for daily pills.

Sources

  1. NIAAA. (2023). Treatment of Alcohol Problems: Finding and Getting Help. niaaa.nih.gov
  2. Anton RF, et al. (2006). Combined Pharmacotherapies and Behavioral Interventions for Alcohol Dependence (COMBINE). JAMA, 295(17), 2003–2017.
  3. Rösner S, et al. (2010). Opioid antagonists for alcohol dependence. Cochrane Database of Systematic Reviews.
  4. Garbutt JC, et al. (2005). Efficacy and tolerability of long-acting injectable naltrexone for alcohol dependence. JAMA, 293(13), 1617–1625.
  5. SAMHSA. (2023). Medication for the Treatment of Alcohol Use Disorder. samhsa.gov
  6. ASAM. (2023). National Practice Guideline for the Treatment of Opioid Use Disorder. asam.org

Dr. James Whitfield, MD

Board-Certified Addiction Medicine Specialist

Dr. Whitfield is a board-certified addiction medicine physician with over 15 years of experience treating substance use disorders and co-occurring psychiatric conditions. He completed his fellowship at Johns Hopkins University School of Medicine and serves as a clinical advisor for addiction treatment facilities across the southeastern United States.

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