Clinical Trial Details
— Status: Withdrawn
Administrative data
| NCT number |
NCT00655967 |
| Other study ID # |
HRRC# 06-318 |
| Secondary ID |
CMP-MD-11 |
| Status |
Withdrawn |
| Phase |
Phase 4
|
| First received |
|
| Last updated |
|
| Start date |
December 2006 |
| Est. completion date |
December 2006 |
Study information
| Verified date |
July 2023 |
| Source |
University of New Mexico |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
Alcohol abuse and dependence are very prevalent and result in significant morbidity,
mortality and cost to society (Harwood 2000). Pharmacotherapies to assist with alcohol
dependence consist of disulfiram, naltrexone and acamprosate. Of these, acamprosate is unique
in that it is not metabolized by the liver, but rather completely excreted renally. In
contrast, naltrexone is metabolized by the CYP450 system of the liver and less than 2% is
excreted unchanged and can cause liver damage (PDR 2005). Multiple cases of hepatitis,
including both cholestatic and fulminant hepatitis, as well as hepatic failure resulting in
transplantation or death, have been reported with administration of disulfiram (PDR 2005).
The incidence of liver disease among alcoholics is high and increases with age and years of
drinking and this may preclude the use of antabuse or naltrexone to help alcohol dependent
patients with liver disease or that are elderly . Thus acamprosate has a unique safety
profile that would make it ideally suited for treating alcohol dependence in the elderly,
even in the presence of hepatic impairment. The current study is to evaluate the safety
profile of acamprosate in elderly patients with alcohol dependence.
Acamprosate, calcium acetyl homotaurinate, has been approved in most European countries and
the U.S. for the maintenance of abstinence in recently detoxified alcoholics. The mechanism
of action involves primarily the restoration of a normal N-methyl- D -aspartate (NMDA)
receptor tone in glutamatergic systems (Rammes et al 2001). Several trials of acamprosate
confirm its efficacy in the maintenance of abstinence in alcohol dependence (Lesch et al.
2001; Slattery et al. 2003; Mann et al. 2004; Verheul et al. 2004). It also reduces the
severity of relapse in alcoholics in abstinence based treatment programs (Chick et al. 2003).
There is limited data on the safety of acamprosate in the elderly (PDR 2005).
For the purposes of this study, elderly will be defined as 60 years or older.
STUDY OBJECTIVE: To determine the short-term safety of Acamprosate in the treatment of
alcohol dependence in the elderly.
Description:
STUDY DESIGN: This trial will be conducted as an open-label, fixed dose design for safety of
Acamprosate in the elderly. Subjects will receive Acamprosate for 12 weeks. The schedule of
visits will include screening, baseline and three monthly follow-up visits at days 30, 60 and
90. We will recruit 25 subjects in the total study period of 15 month.
Regarding the number of subjects, chi-squared analysis of the total number of side effects
(61%, i.e. 1230 out of 2018 subjects in prior studies) and the possible number of subjects in
the study with side effects (from 0 to 25), indicates that a significant (alpha=0.05)
difference from the previously observed rate would occur if less than 11 (p<=0.05) or more
than 20 (p<=0.025) subjects report side effects. Side effects in 11 to 20 subjects would be
nonsignificantly different from the previously published rates. Thus 25 subjects are
sufficient to detect significant deviation in frequency of overall side effects in this
sample compared to the subjects in prior studies. Total number of side effects was used for
this calculation because there is no single common or significant side effect that would lend
itself as an appropriate surrogate for the side effects overall.
During the course of the study subjects will be supplied with 333mg tablets of Acamprosate
provided by the Sponsor. The study medication will be administered at a dose of 666mg (=two
tablets) three times a day for subjects with a creatinine clearance >50. The dose will be
333mg three times a day for subjects with a creatinine clearance in the range of 30-50.
Safety will be monitored by subject's report of adverse events at all treatment visits
throughout both, open label and double blind phases of the Trial. The report of adverse
events or new symptoms by the subject will be reviewed and summarized. This may also include
any clinically significant changes in the vital signs (blood pressure and pulse readings,
weight, temperature), physical examinations, laboratory evaluations (blood chemistry,
hematology, urinalysis, EKG) and recording of concomitant treatment. A DSMB plan has been set
up.
Treatment compliance will be monitored by counts of returned medication, and subjects are to
be counseled if they do not adhere, or if they are thought to be at risk for not adhering to
the medication regimen.
