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Published Online: 1 July 2011

Adapting Treatment to Patient Problems

Alcoholism is a complex disorder with multifaceted symptoms involving multiple neural-behavioral systems. Thus, it is not surprising that multiple treatment approaches have been reported to improve outcomes. Evidence is accumulating that matching treatment to patient problems leads to better outcomes. This was shown in a prospective randomized study (1) in which treatment was applied to specific problems measured at intake by the Addiction Severity Index (2). Unfortunately, most treatment programs provide the same treatment to all patients, even though their program advertisements might say otherwise (3).
Adapting treatment to specific problems can also be approached by selection of medication. Last year in the Journal, Pettinati and colleagues (4) reported on combining medications for patients suffering from both alcoholism and major depression. This is a very common combination of problems, and it has been approached with different kinds of antidepressant medication. In a placebo-controlled trial, Pettinati et al. tried a combination of two medications, one for heavy drinking (naltrexone) and the other for depression (sertraline). The patients receiving the combination showed significantly more clinical improvement both in depression and in drinking behavior than those receiving either medication alone.
In this issue, Anton and colleagues (5), again acknowledging the multifaceted symptoms of alcoholism, report the effect of adding gabapentin to naltrexone in the postdetoxification period. The naltrexone-gabapentin combination makes excellent pharmacological sense, and it is likely to be safe because naltrexone has no significant interactions with any class of drugs other than opioids. During the immediate postdetoxification period, symptoms that can be described as “protracted withdrawal” are prominent in many patients and may cause treatment dropout or relapse to drinking. Naltrexone has not been found to have any effect on such symptoms. Clinicians have always been tempted to add other medications for symptomatic treatment of irritability, insomnia, and anxiety early in alcoholism treatment, and gabapentin seems to be a logical choice. It has already been shown to reduce the symptoms of acute alcohol withdrawal in a controlled study (6).
But Anton et al. went beyond the usual open clinical experimentation. They tested their hypothesis in a double-blind trial with the addition of either gabapentin or placebo to naltrexone. During the first 6 weeks of the study, the addition of gabapentin to naltrexone produced a longer delay to relapse, fewer drinks per drinking day, and a decrease in alcohol craving. As expected, the gabapentin group reported fewer sleep problems than the other two groups, which is consistent with reports of gabapentin's benefits for alcohol withdrawal.
The Anton et al. study is a fine example of clinical research guided by clinical experience and shows that medication combinations can indeed be objectively evaluated. Their study deserves replication, perhaps adding a gabapentin-alone treatment arm, as the authors suggest. Another variable to be considered in a replication study is the dosage of naltrexone. The recommended daily dose of 50 mg was arrived at in 1983 by convenience, as this was the dosage used in the treatment of heroin addiction. More recent studies, such as Project COMBINE (7) and the above-cited study using an antidepressant and naltrexone (4), have used 100 mg per day.
Most importantly, the Anton et al. study provides guidance to clinicians who are faced with a patient who has multiple chronic withdrawal complaints during the course of naltrexone treatment for alcoholism. This is an important problem that often leads to dropout and relapse to heavy drinking. Clinicians are known to add medications for symptomatic treatment in the absence of controlled data. While a single study does not provide adequate proof, the high quality of Anton and colleagues' study provides support to desperate clinicians seeking a way to retain the patient in treatment. We can also hope that a replication study is already in the planning stage.

Footnote

Editorial accepted for publication April 2011.

References

1.
McLellan AT, Grissom GR, Zanis D, Randall M, Brill P, O'Brien CP: Problem-service “matching” in addiction treatment: a prospective study in 4 programs. Arch Gen Psychiatry 1997; 54:730–735
2.
McLellan AT, Luborsky L, Woody GE, O'Brien CP: An improved diagnostic evaluation instrument for substance abuse patients: the Addiction Severity Index. J Nerv Ment Dis 1980; 168:26–33
3.
McLellan AT: The status of the United States treatment system: implications for evidence based treatments, in Rethinking Substance Abuse: What the Science Shows and What We Should Do About It . Edited by, Miller WR, Carroll KM. New York, Guilford, 2005, pp 146–157
4.
Pettinati HM, Oslin DW, Kampman KM, Dundon WD, Xie H, Gallis TL, Dackis C, O'Brien CP: A double-blind, placebo-controlled trial combining sertraline and naltrexone for treating co-occurring depression and alcohol dependence. Am J Psychiatry 2010; 167:668–675
5.
Anton RF, Myrick H, Wright TM, Latham PK, Baros AM, Waid LR, Randall PK: Gabapentin combined with naltrexone for the treatment of alcohol dependence. Am J Psychiatry 2011; 168:709–717
6.
Myrick H, Malcolm R, Randall PK, Boyle E, Anton RF, Becker HC, Randall CL: A double-blind trial of gaba-pentin versus lorazepam in the treatment of alcohol withdrawal. Alcohol Clin Exp Res 2009; 33:1582–1588
7.
Anton RF, O'Malley SS, Ciraulo DA, Cisler RA, Couper D, Donovan DM, Gastfriend DR, Hosking JD, Johnson BA, LoCastro JS, Longabaugh R, Mason BJ, Mattson ME, Miller WR, Pettinati HM, Randall CL, Swift R, Weiss RD, Williams LD, Zweben A; COMBINE Study Research Group: Combined pharmacotherapies and behavioral interventions for alcohol dependence: the COMBINE study: a randomized controlled trial. JAMA 2006; 295:2003–2017

Information & Authors

Information

Published In

Go to American Journal of Psychiatry
Go to American Journal of Psychiatry
American Journal of Psychiatry
Pages: 670 - 671
PubMed: 21724671

History

Accepted: April 2011
Published online: 1 July 2011
Published in print: July 2011

Authors

Details

Charles P. O'Brien, M.D., Ph.D.

Notes

Address correspondence and reprint requests to Dr. O'Brien ([email protected]).

Funding Information

Dr. O'Brien has worked as a consultant for Alkermes and Gilead. Dr. Freedman has reviewed this editorial and found no evidence of influence from these relationships.

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