MEDICATIONS: ONCE-A-MONTH INJECTABLE
MEDICATION HELPS TREAT ALCOHOL DEPENDENCE
April 6, 2005 — Because of problems with adherence to a daily oral dose of
naltrexone, the effectiveness found in treating alcohol dependence with a
once-a-month injection of naltrexone could improve long-term treatment outcomes,
according to a study in the April 6 issue of the Journal of the American
Medical Association.
Alcohol dependence is a major public health problem, which worldwide is the
fourth leading cause of disability, according to background information in the
article. Alcohol dependence is present in approximately 4 percent of the U.S.
adult population, is common among primary care patients, and may contribute to
more than 100,000 preventable deaths per year. The drug naltrexone has shown
efficacy for treatment of alcohol dependence. However, adherence to daily oral
doses can be problematic, and clinical acceptance and utility of oral naltrexone
have been limited.
James C. Garbutt, M.D., of the University of North Carolina at Chapel Hill,
N.C., and colleagues conducted a study to determine the efficacy and safety of a
new formulation, which releases naltrexone for one month following a single
injection, for treatment of alcohol dependence.
The six-month, randomized, double-blind, placebo-controlled trial was
conducted between February 2002 and September 2003 at 24 U.S. public hospitals,
private and Veterans Administration clinics, and tertiary care medical centers.
Of the 899 individuals screened, 627 who were diagnosed as being actively
drinking alcohol-dependent adults were randomized to receive treatment and 624
received at least 1 injection. Participants received either an intramuscular
injection of 380 mg. of long-acting naltrexone (n = 205), 190 mg. of long-acting
naltrexone (n = 210), or a matching volume of placebo (n = 209), each
administered monthly and combined with 12 sessions of low-intensity psychosocial
intervention.
The researchers found that compared with placebo, 380 mg. of long-acting
naltrexone resulted in a 25 percent decrease in the event rate of heavy drinking
days and 190 mg. of naltrexone resulted in a 17 percent decrease. Sex and
pretreatment abstinence each showed significant interaction with the medication
group on treatment outcome, with men and those with lead-in abstinence both
exhibiting greater treatment effects. Discontinuation due to adverse events
(e.g. nausea, headache, fatigue) occurred in 14.1 percent in the 380-mg. and 6.7
percent in the 190-mg. group and 6.7 percent in the placebo group. Overall, rate
and time to treatment discontinuation were similar among treatment groups.
"In summary, the results from this trial, with one of the largest samples
ever treated with a medication for alcohol dependence, indicate that long-acting
injectable naltrexone is well tolerated and is associated with a significant
reduction in heavy drinking in a population of actively drinking patients. The
long-acting formulation has the potential to improve intervention strategies for
alcohol dependence by providing a predictable pharmacological foundation for
treatment. In addition to their utility for alcohol dependence, long-acting
formulations may prove to be an important treatment strategy for a variety of
addictive disorders," the authors write.
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