AN OPEN RANDOMIZED STUDY COMPARING DISULFIRAM AND ACAMPROSATE IN THE TREATMENT OF ALCOHOL DEPENDENCE

AVINASH DE SOUSA* and ALAN DE SOUSA

Get Well Clinic And Nursing Home, 33rd Road, Off Linking Road, Bandra, Mumbai 400050, Maharashtra State, India

* Author to whom correspondence should be addressed: Tel.: +91 22 26460785; E-mail: avinashdes999{at}yahoo.co.uk

(Received 11 March 2005; first review notified 6 June 2005; in final revised form 21 June 2005; accepted 2 July 2005)


    ABSTRACT
 TOP
 ABSTRACT
 INTRODUCTION
 SUBJECTS and METHODS
 RESULTS
 DISCUSSION
 LIMITATIONS
 REFERENCES
 
Aims: To compare the efficacy of acamprosate (ACP) and disulfiram (DSF) for preventing alcoholic relapse in routine clinical practice. Methods: One hundred alcoholic men with family members who would encourage medication compliance and accompany them for follow-up were randomly allocated to 8 months of treatment with DSF or ACP. Weekly group psychotherapy was also available. The psychiatrist, patient, and family member were aware of the treatment prescribed. Alcohol consumption, craving, and adverse events were recorded weekly for 3 months and then fortnightly. Serum gamma glutamyl transferase was measured at the start and the end of the study. Results: At the end of the trial, 93 patients were still in contact. Relapse (the consumption of >5 drinks/40 g of alcohol) occurred at a mean of 123 days with DSF compared to 71 days with ACP (P = 0.0001). Eighty-eight per cent of patients on DSF remained abstinent compared to 46% with ACP (P = 0.0002). However, patients allocated to ACP had lower craving than those on DSF (P = 0.002). Conclusion: DSF is superior to ACP for preventing relapse in alcohol-dependent men with good family support. Further comparisons between these two drugs in different treatment settings and populations are warranted.


    INTRODUCTION
 TOP
 ABSTRACT
 INTRODUCTION
 SUBJECTS and METHODS
 RESULTS
 DISCUSSION
 LIMITATIONS
 REFERENCES
 
Two anti-craving agents, acamprosate (ACP) and naltrexone (NTX) are now widely available for the long-term management of alcoholism. However, they are more expensive than older alcohol-deterrent drugs like disulfiram (DSF) and few studies comparing the effectiveness of the two classes of medication have been done.

Pooled analysis of ACP trials confirms its efficacy in the maintenance of abstinence in alcohol dependence (Lesch et al., 2001Go; Slattery et al., 2003Go; Mann et al., 2004Go; Verheul et al., 2004Go) (www.docs.scottishmedicines.org/docs/pdf/Alcohol%20Report.pdf). However, this efficacy is relatively modest with an average effect size of only 0.26 (Berglund et al., 2003Go) and some subsequent studies have not shown efficacy (e.g. Namkoong et al., 2003Go). ACP reduces the severity of relapse in alcoholics undergoing abstinence-oriented treatment (Chick et al., 2003Go), and may even be effective in the management of alcohol-dependent adolescents (Niederhofer and Staffen, 2003Go). It is the only anti-craving agent so far with good cost effectiveness ratings in the management of alcoholism (Schadlich and Brecht, 1998Go; Foster and McClellan, 1999Go).

DSF is an alcohol deterrent that inhibits acetaldehyde dehydrogenase. The resulting increase in acetaldehyde levels in the body leads to the characteristic DSF–ethanol reaction that includes a sense of uneasiness, flushing, nausea, and vomiting (Savas and Gullu, 1997Go). Several reviews support the efficacy of DSF, if supervised, in the treatment of alcohol dependence (Brewer, 1992Go; 1995Go; Berglund et al., 2003Go; Slattery et al., 2003Go).

We reported a comparison of DSF and NTX and found DSF considerably more effective in reducing the frequency and severity of relapse (De Sousa and De Sousa, 2004Go). However, there have been no studies so far comparing DSF and ACP, though Besson et al. (1998)Go found that, in a study where there was random allocation to placebo or ACP, patients who had chosen to take DSF did particularly well compared to patients who had not chosen DSF whether on placebo or ACP. The aim of this study was to compare DSF and ACP in patients with pure alcohol dependence. As with our comparison of DSF and NTX, an open trial design was chosen, partly because it would have been difficult to maintain compliance and blinding in a long trial and partly because the patients' awareness that they are taking DSF is an important factor in DSF's effectiveness.


    SUBJECTS and METHODS
 TOP
 ABSTRACT
 INTRODUCTION
 SUBJECTS and METHODS
 RESULTS
 DISCUSSION
 LIMITATIONS
 REFERENCES
 
The setting of this open, randomised study was typical of routine clinical practice in India. The subjects were alcohol-dependent men undergoing detoxification in a private psychiatric hospital in the large city of Mumbai. The list for randomisation was provided by a qualified statistician. Treatment was allocated by the clinic's staff according to the serial number on the list.

Inclusion criteria

  1. Age between 18 and 65 years.
  2. DSM-IV criteria for alcohol dependence.
  3. Patients were required to have a stable family environment so that the family could ensure to maximize treatment compliance and provide regular follow-up information.

Exclusion criteria

  1. Presence of other substance abuse disorders (excluding nicotine dependence).
  2. Presence of any co-morbid psychiatric disorder.
  3. Any medical condition present that would interfere with treatment compliance or be a contraindication to ACP or DSF.
  4. Any of the routine liver function test values more than three times above the normal value.
  5. Previous treatment with DSF and/or ACP.
After completing detoxification, either in hospital or as an out patient, subjects were informed about the objectives and duration of the study and the nature of the two drugs. Their mechanisms of action, side effects, and the importance of maintaining compliance were discussed. Patients were also told that the drug given to them would be chosen at random but they would know which drug they were receiving. They were told that relapse or non-compliance would lead to their exclusion from the trial, as would the absence of regular follow-up with a family member. They were free to leave the study at any time.

Assessment procedure
After signing the informed consent declaration, subjects completed:

  1. The Addiction Severity Index (McLellan et al., 1980Go).
  2. The Severity of Alcohol Dependence Scale (Stockwell et al., 1983Go).
  3. A scale to measure the three parameters of craving i.e. frequency, duration, and intensity (Anton et al., 1995Go).

They were given a calendar to record any alcohol consumption during the follow-up. Baseline aspartate aminotransferase (AST), alanine aminotransferase (ALT), gamma glutamyl transferase (GGT), and serum bilirubin were done.

Following randomisation, patients received either 250 mg of DSF or 1998 mg of ACP per day. DSF was given as a single daily dose after breakfast while ACP was given as 666 mg thrice daily after meals. The importance of family members observing patients when they took medication to enhance compliance was emphasised. Only the non-dispersible form of DSF is available in India.

Patients were followed up weekly for the first 3 months and then fortnightly until the end of the trial. At each follow-up, they were assessed for craving and adverse effects along with compliance and alcohol consumption. Self-reports were checked against reports of family members. All patients were offered weekly supportive group psychotherapy during the trial. It was probably less structured than in classical treatment programmes. Abstinence was positively reinforced. Patients also received symptomatic treatment for depression (escitalopram 10 mg/day) or insomnia (zolpidem 5–10 mg at night), when required. Benzodiazepines were not prescribed.

Outcome measures
The following outcome measures were assessed:

  1. Accumulated days of abstinence.
  2. Days until the first relapse (defined as the consumption of >5 alcoholic drinks/40 g of alcohol in 24 h.
  3. Number of drinks consumed per typical week.
  4. Number of drinks consumed per typical occasion.
  5. Craving measures.
  6. GGT measured every 3 months.
  7. Discontinuation of treatment.
  8. Drop out from the study.
To improve the consistency and independence of the ratings the final outcomes were rated by a psychologist independent of the study. Since she was on the staff of the clinic, she was not blinded to the treatment group in all cases.

Statistical analysis
Chi square test and Student's t-test were used in the statistical analysis. All outcome analyses were conducted on an ‘intention to treat’ principle. Drop-outs were considered as relapses. The number of drinks consumed per week, number of drinks consumed at a time, and the serum GGT were analysed using the analysis of covariance (ANCOVA).


    RESULTS
 TOP
 ABSTRACT
 INTRODUCTION
 SUBJECTS and METHODS
 RESULTS
 DISCUSSION
 LIMITATIONS
 REFERENCES
 
A total of 167 patients were screened and 104 met the criteria. Of these, the first 100 (in serial order) were chosen for the study. Fifty patients were randomized to each group. During the study, three dropped out of the ACP group due to irregular attendance while four dropped out of the DSF group—three due to side effects (neuropathy) and one due to stoppage of medication.

Table 1 shows that there were no significant differences between the treatment groups in terms of baseline socio-demographic or clinical variables.


View this table:
[in this window]
[in a new window]
 
Table 1. Variables at the entry into the study

 
All the six patients who dropped out from the study did so in the first month. Table 2 shows that by the end of this 8-month study, 88% of DSF group had not relapsed, compared with 46% in the ACP group (P = 0.0001). Mean survival time until the first relapse was significantly greater with DSF (123 days) than with ACP (71 days) (P = 0.0001). Craving scores of patients on ACP were lower than for those on DSF.


View this table:
[in this window]
[in a new window]
 
Table 2. Outcomes at the end of 8 months

 
Only two patients received escitalopram. Zolpidem was given to 28 patients for insomnia. Side effects were uncommon. Nausea was experienced equally in both groups (ACP 3%, DSF 4%), but side effects abated in the first week of the study.


    DISCUSSION
 TOP
 ABSTRACT
 INTRODUCTION
 SUBJECTS and METHODS
 RESULTS
 DISCUSSION
 LIMITATIONS
 REFERENCES
 
Compared with ACP, DSF was associated with a large and significantly greater reduction in relapse and significantly more abstinent days. This study adds to the evidence that supervised DSF is a very effective component of alcoholism treatment and is significantly more effective than either ACP or NTX. It does not seem to be sufficiently recognized that DSF generally has no specific effect unless it is monitored and supervised by family members or professionals (Brewer, 1986Go; Fuller and Gordis, 2004Go). It is of theoretical and practical interest that although ACP reduced craving significantly more than DSF, there were no comparable reductions in relapse or alcohol intake. This is the first published comparison between these two drugs in a relatively large number of patients but even larger studies in diverse treatment settings are clearly needed. Family support is typically strong in India. Wives monitored medication in ~90% of subjects. In the remainder, parents monitored it. Another point of importance in an Indian context is that DSF is cheaper than ACP and much cheaper than NTX. We nominated one family member to take responsibility for monitoring and encouraging compliance and the same person was invited to accompany the patient at follow-up.


    LIMITATIONS
 TOP
 ABSTRACT
 INTRODUCTION
 SUBJECTS and METHODS
 RESULTS
 DISCUSSION
 LIMITATIONS
 REFERENCES
 
This was an open study and the investigators were not blinded. At the start of the study, the investigators had no firm indication as to which treatment would be more effective but as the study progressed, better outcomes were noted with DSF. This may have resulted in the investigators making more efforts to ensure better compliance in this group and could have introduced some bias. The assessment of compliance was based on family reports. It would have been helpful if more use had been made of laboratory markers. Most patients in this study had supportive families. This may partly account for the low drop-out rate compared with many other studies. Nevertheless, we conclude from this study that DSF is more effective than ACP for preventing relapse in alcohol dependence.


    ACKNOWLEDGEMENTS
 
We owe thanks to Clinical Psychologist Dr Jyoti Jagtap and Statistician, Mr O. P. Nayar.


    REFERENCES
 TOP
 ABSTRACT
 INTRODUCTION
 SUBJECTS and METHODS
 RESULTS
 DISCUSSION
 LIMITATIONS
 REFERENCES
 
Anton, R. F., Moak, D. H. and Latham, P. (1995) The obsessive compulsive drinking scale—a self rated instrument for the quantification of thoughts about alcohol and drinking behaviour. Alcoholism: Clinical and Experimental Research 19, 92–99.[ISI][Medline]

Berglund, M., Thelander, S. and Jonsson, E. (eds) (2003) Treating Alcohol and Drug Abuse. An Evidence Based Review. WILEY-VCH Verlag GmbH and Co. KGaA, Weinheim.

Besson, J., Aeby, F., Kasas, A. et al. (1998) Combined efficacy of acamprosate and disulfiram in the treatment of alcoholism—a controlled study. Alcoholism: Clinical and Experimental Research 22, 573–579.[ISI][Medline]

Brewer, C. (1986) Patterns of compliance and evasion in treatment programs that include supervised disulfiram. Alcohol and Alcoholism 21, 385–388.[ISI][Medline]

Brewer, C. (1992) Controlled trials of antabuse in alcoholism—importance of supervision and adequate dosage. Acta Psychiatrica Scandanavica 69(3), 51–58.

Brewer, C. (1995) Recent developments in disulfiram treatment. Alcohol and Alcoholism 28, 385–393.

Chick, J., Lehert, P. and Landron, F. (2003) Does acamprosate improve reduction of drinking as well as aiding abstinence. Journal of Psychopharmacology 17, 397–402.[CrossRef][ISI][Medline]

De Sousa, A. and De Sousa, A. (2004) A one-year pragmatic trial of naltrexone versus disulfiram in the treatment of alcohol dependence. Alcohol and Alcoholism 39, 528–531.[Abstract/Free Full Text]

Foster, R. H. and McClellan, K. J. (1999) Acamprosate—pharmacoeconomics and implications of therapy. Pharmacoeconomics 16, 743–755.[ISI][Medline]

Fuller, R. K. and Gordis, E. (2004) Does disulfiram have a role in alcoholism treatment today? Addiction 99, 21–24.

Lesch, O. M., Riegler, A., Gutierrez, K. et al. (2001) The European acamprosate trials—conclusions for research and therapy. Journal of Biomedical Sciences 8, 89–95.[CrossRef]

Mann, K., Lehert, P. and Morgan, M. Y. (2004) The efficacy of acamprosate in the maintenance of abstinence of alcohol dependence patients—a meta analysis. Alcoholism: Clinical and Experimental Research 28, 51–63.[ISI][Medline]

McLellan, A., Luborsky, L., O'Brien, C. et al. (1980) An improved instrument for assessing alcoholic patients—the Addiction Severity Index. Journal of Nervous and Mental Disease 168, 26–33.[ISI][Medline]

Namkoong, K., Lee, B. O., Lee, P. G. et al. (2003) Acamprosate in Korean alcohol dependence patients—a multicenter randomized double blind placebo controlled study. Alcohol and Alcoholism 38, 135–141.[Abstract/Free Full Text]

Niederhofer, H. and Staffen, W. (2003) Acamprosate and its efficacy in treating alcohol dependent adolescents. European Child and Adolescent Psychiatry 12, 144–148.[CrossRef][ISI][Medline]

Savas, M. C. and Gullu, I. H. (1997) Disulfiram-ethanol reaction—the significance of supervision. Annals of Pharmacotherapy 31, 374–375.[ISI][Medline]

Schadlich, P. K. and Brecht, J. G. (1998) The cost effectiveness of acamprosate in the treatment of alcoholism in Germany. Economic evaluation of the prevention of relapse with acamprosate in the management of alcoholism. The PRAMA study. Pharmacoeconomics 13, 719–730.[ISI][Medline]

Slattery, J., Chick, J., Craig, J. et al. (2003) Prevention of Relapse in Alcohol Dependence. Health Technology Assessment Report 3. Health Technology Board for Scotland, Glasgow.

Stockwell, T., Murphy, D. and Hodgson, R. (1983) The severity of alcohol dependence questionnaire—its use, reliability and validity. British Journal of Addiction 78, 145–155.[ISI][Medline]

Verheul, R., Lehert, P., Geerlings, P. J. et al. (2004) Predictors of acamprosate efficacy—results from a pooled analysis of seven European trials including 1485 alcohol dependence patients. Psychopharmacology (Berlin) 178, 167–173.[ISI][Medline]





This Article
Abstract
Full Text (PDF)
All Versions of this Article:
40/6/545    most recent
agh187v1
Alert me when this article is cited
Alert me if a correction is posted
Services
Email this article to a friend
Similar articles in this journal
Similar articles in ISI Web of Science
Similar articles in PubMed
Alert me to new issues of the journal
Add to My Personal Archive
Download to citation manager
Request Permissions
Google Scholar
Articles by DE SOUSA, A.
Articles by DE SOUSA, A.
PubMed
PubMed Citation
Articles by DE SOUSA, A.
Articles by DE SOUSA, A.