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This is the abstract of a study selected by Drug and Alcohol Findings as particularly relevant to improving outcomes from drug or alcohol interventions in the United Kingdom. It was not published by Drug and Alcohol Findings. Unless permission has been granted, we are unable to supply full text. Click on the Title to visit the publisher's or other document supplier's web site. Other links to source documents also in blue. Hover mouse over orange text for explanatory notes. Free reprints may be available from the authors - click Request reprint to send or adapt the pre-prepared e-mail message. The abstract is intended to summarise the findings and views expressed in the study. Below are some comments from Drug and Alcohol Findings. and enter e-mail address to be alerted to new studies and reviews Schottenfeld R.S., Chawarski M.C., Mazlan M.Lancet: 2008, 371, p. 2192–2200.
This unique randomised trial tested what would happen if detoxified opiate addicts were
then maintained on a substitute drug, on an opiate-blocking medication, or simply
counselled. The results led to the introduction of methadone prescribing programmes in
Abstract As a follow-on treatment after opiate detoxification, this study compared the
efficacy of the opiate-blocking medication naltrexone, the opiate substitute
buprenorphine, or no treatment other than the drug counselling all patients received. In
Malaysia at the time naltrexone was the main long-term pharmacotherapy and
maintenance substitute prescribing was not permitted.
Between July 2003 and May 2005, 215 people contacted the study of whom 143 heroin
in the study's inpatient clinic. Most of the remaining contacts did not complete the study's initial
assessments; just 12 were excluded due to 126 completed detoxification and started 24 weeks of weekly individual and group drug counselling in
the study's outpatient research clinic. For randomly selected patients, counselling was
buprenorphine, or placebos. In the first week the medications were given daily, then multiple doses were given on Mondays,
Wednesdays and Fridays. All the doses were consumed under supervision at the clinic
and all the patients consumed similar tablets and capsules, either active or placebos
depending on their assignment. Nevertheless, most on the active medications correctly
identified what they were taking, though most on placebos did not. Typically the patients
were poorly educated single men with a history of imprisonment who had been using
heroin for on average 15 years and had used near-daily in the previous month.
Outcomes were assessed mainly by urine tests three times a week while patients were
assumption being made that the few tests missed by
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retained patients would have been positive for heroin, and that patients who dropped out
of treatment had resumed heroin use. When it became apparent that buprenorphine was
clearly the best option, the study was terminated early after 103 patients had completed
Supplementing counselling with naltrexone slightly
improved treatment retention and heroin use
outcomes, but not to a statistically significant degree
according to the study's In contrast, were clearly and universally superior for the buprenorphine patients,
significantly better than placebo, and generally also
significantly better than naltrexone. For example, of the
24 weeks patients could have stayed in treatment, on
buprenorphine they stayed on average for 17 weeks,
naltrexone 12, and placebo 10 chart. Corresponding
figures for retention without a positive/missed test for
heroin use were 7, just over 3, and just under 3 weeks.
For retention without to sustained heroin use, the figures were 11, 9, and just under 6 weeks.
For the authors their findings showed the efficacy of maintenance treatment with
buprenorphine in sustaining abstinence, delaying time to resumption of heroin use and
relapse, and retaining patients in treatment, lending support to the widespread
dissemination of maintenance treatment with buprenorphine as an effective public health
Uniquely the study answered the question: What would happen if continuing
care for patients who completed detoxification consisted of low intensity counselling only
or with attempts to sustain abstinence using naltrexone, versus effectively accepting that
many will relapse and instead prescribing a substitute drug? When these were the only
options available, the answer seemed to be that naltrexone offers no substantial
advantages, but that makes a big difference to how long and how many patients are able to live without regular resort to illegal opiates. Without this, for
most rapid relapse is the norm even after they have been able to complete
detoxification; opiate blocking medication does little to improve the situation.
Though this is the verdict from among the range of options on offer in the study, long-
acting forms of naltrexone which last weeks or months might have tipped the balance in
favour of abstinence-based therapy, and seamless entry in to (to the patient) acceptable
forms of residential rehabilitation or intensive day care might have raised outcomes to
the point where the choice of medication was less decisive. In both cases, the caveat is
that compared to substitute prescribing, fewer patients are prepared to accept or can
access these options, and in the case of residential rehabilitation, the are likely to be considerably greater.
The main issue with the study from a UK perspective is its applicability to a country
where these are not the only options available, and where even if they were, patients
would be expected to be allocated to them on an individual basis in the light of what
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seems best for that individual. However, there are parallels. As in the featured study, in
the UK (and elsewhere) failure to complete detoxification or post-detoxification relapse
are the norm, long-acting naltrexone formulations have yet to be licensed and made
widely available, and residential rehabilitation remains in short supply. The relevance of
substitute prescribing is de-emphasised in favour of abstinence-based approaches,
especially if the need for economies forces these to take the form of naltrexone or
counselling rather than intensive, extensive and expensive psychosocial rehabilitation.
of oral naltrexone as a means of providing or reinforcing that support, and the more widespread applicability and more securely
established effectiveness of substitute prescribing using methadone or buprenorphine. It
also provides an argument for maintenance prescribing to be made rapidly available for
the many patients unable to avoid a return to regular opiate use after detoxification.
The implications of the study are supported by other studies of , , though no other study has within itself compared on the study put it, this wider research base indicates that "The preferred oral pharmacological treatment for opioid dependence should be
agonist maintenance with either methadone or buprenorphine." This verdict carefully
limited itself to "pharmacological" treatments and to medications, leaving out more intensive or improved psychosocial approaches or long-acting implanted or injected
In Australia, where polarised opinions favoured substitute prescribing or rejected this in
favour of naltrexone, the federal parliament reacted by conducting a of their respective advantages in the Australian context. The conclusion was that both had their
place, but that place was much greater for substitute prescribing. Oral naltrexone was
seen as a niche option for the minority of opioid-dependent individuals capable of
remaining compliant with the treatment, but for most it had been consistently been
linked with high rates of non-compliance, a greater risk of death and reduced likelihood
of long-term success. In contrast, methadone and other opioid substitution treatments
were seen as widely applicable treatments acknowledged as effective in reducing opioid
dependence and associated health and social problems.
The featured study seems to support this conclusion, but perhaps not as strongly as it
might have done. On one key measure – retention without relapse to sustained heroin
use – buprenorphine's advantage over naltrexone was small (two weeks) and not
statistically significant, possible an artefact of the way Despite its advantages, half the patients on buprenorphine stayed in treatment for six months, less than in other studies possibly due to insufficiently supportive psychosocial
was at the lower end of what is considered effective. It also seems likely that buprenorphine's advantage would have been greater
had patients not been required to complete detoxification in advance, presumably
weeding out those less able or willing to attain abstinence from opiates. On the other
hand, the naltrexone patients might have been disadvantaged by the dosing schedule.
are known to be able to bridge alternate-day dosing schedules, but in studies naltrexone is normally taken daily, providing a daily reminder to
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the patient that any heroin they try will be more or less wasted. Dosing every two or
three days left gaps during which the patients might have been tempted to try heroin.
However, this schedule probably reflects how both drugs are commonly prescribed in
Thanks for their comments on this entry in draft to Brian Kidd of Tayside Drug Problems Service and University of Dundee Medical School, and John Witton of the in London. Commentators bear no responsibility for the text including the interpretations and any remaining errors.Top 10 most closely related documents on this site. For more try a
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Investigación Científica sobre Cerveza y Salud González-Gross M, Lebrón MR, Marcos A. Revisión bibliográfica del consumo moderado de la cerveza sobre la salud. Centro de Información Cerveza y Salud. 2000; E 6. Posadas J. Estudio recopilatorio Cerveza y Salud. Centro de Información Cerveza y Salud. 1998; E 1. Villarino AR, Martínez JR, Posadas P. Biblioteca de publicacio