Overview

Efficacy and Safety Evaluating Study of Odelepran for the Use in Patient With Alcohol Dependence

Status:
Completed

Trial end date:
2016-05-14

Target enrollment:
0

Participant gender:
All

Summary

The purpose of this study was to assess efficacy and safety of the study drug Odelepran, 125 mg as compared to placebo in the treatment of alcohol dependence in adult outpatients.

Phase:

Phase 3

Accepts Healthy Volunteers?

Details

Lead Sponsor:

R-Pharm

Collaborator:

Synergy Research Inc.

Treatments:

Ethanol

Criteria

Inclusion Criteria:

- Signed and dated informed consent.

- Outpatients (not hospitalized by the moment of randomization).

- Average alcohol consumption during 30 days prior to screening higher than a medium
drinking risk level (men: > 4 drinks/day or 14 drinks/week; women > 3 drinks/day or 7
drinks/week) according to the National Institute on Alcohol Abuse and Alcoholism
(NIAAA) criteria.

- Patients diagnosed with alcohol dependence according to the International
Classification of Diseases (ICD)-10, assessed with the Mini-International
Neuropsychiatric Interview (MINI).

- Abstaining from alcohol during 3 days prior to screening and 3 days before
randomization confirmed by the test for alcohol in exhaled air (less than 0,02 %).

- For women retaining childbearing potential - negative pregnancy test and consent to
use reliable contraception methods (as well as for men) throughout the study period,
including the study follow up period.

- Patients able to comply with study protocol as per investigator's opinion.

- Availability of a patient's trustee who reside with the patient. A trustee is defined
here as a person who spends with the patient at least 4 hours a day. The trustee must
give his/her consent for participation in the study as the patient's representative.

- Study drug monotherapy must be acceptable for the patient as per investigator's
opinion.

Exclusion Criteria:

- Hypersensitivity to Odelepran or to any excipient of the study drug (including lactose
intolerance).

- Binge drinking (more than 5 day consecutive days of heavy drinking) during 30 days
prior to screening. Heavy drinking is considered as 5 or more drinks per day for men
and 4 or more drinks per day for women.

- Ever diagnosed schizophrenia, schizoaffective disorder, bipolar mood disorder or any
other psychiatric disorder, except for alcohol dependence. History of alcohol induced
psychosis.

- Anxiety or depressive disorder present at enrollment into the study. Montgomery-Asberg
Depression Rating Scale (MADRS) score higher than 15.

- High suicidal risk confirmed by MINI.

- Previous use of opioid antagonists implants less than 3 months prior to screening; use
of long-acting naltrexone injections (e,g, Vivitrol) less than 4 weeks after the first
injection and 3 months after the second and the following injections; use of cyanamide
(Kolme) less than 2 weeks prior to screening, use of oral opioid antagonists or
disulfiram during 2 weeks prior to screening.

- Psychotherapeutic "coding" (a method when the patient is induced a misbelief that
alcohol consumption would lead to death, expected to result from undisclosed
pharmacological manipulation) that took place during less than 3 months prior to
screening.

- Use of psychotropic medication less than 3 weeks before the screening (for long-acting
and 'depot' formulations) or 1 week before the screening (for other formulations)
except for those used to treat alcohol withdrawal syndrome.

- Severe alcohol withdrawal syndrome (severity of alcohol withdrawal more than 10 on
Clinical Institute Withdrawal Assessment of Alcohol (CIWA-Ar) scale).

- History of seizures (excepting febrile seizers). Severe brain injury, history of
intracranial neoplasms and/or intracranial haemorrhages or any conditions that impose
the risk of seizures. History of anticonvulsive therapy.

- Any clinical condition affecting cognitive or other psychoneurological functioning
(verified for head injury with the loss of consciousness that lasted more than 1 hour,
or resulted in cognitive or behavioral impairment, stroke, encephalopathy, dementia,
neurodegenerative disorder, etc). Except for mild cognitive impairment.

- Mental retardation of syndromes of severe organic brain injury.

- Use of drugs of abuse (opioids, cannabinoids, amphetamines, etc.) or diagnoses of
substance addiction/dependence at the moment of screening or positive urine drug
screen test.

- Significant liver function impairment (aspartate aminotransferase (AST) and alanine
aminotransferase (ALT) higher than 3 upper limits of normal range or diagnosis of
hepatic failure, class B or C by Child Pugh).

- Severe renal failure (creatinine clearance calculated at the screening less than 30
ml/min or renal replacement therapy).

- Severe cardiovascular system disorders: unstable angina, poorly controlled arrhythmia,
cardiac failure of III or IV class by New-York Heart Association (NYHA), acute
myocardial infarction within the past 6 months.

- HIV-infection, hepatitis B or C.

- Decompensated diabetes mellitus (determined glycated hemoglobin HbAc1 level more than
7,5%)

- Other concomitant disorders and conditions that, as per investigator's opinion, put
the patient's safety under risk or that could affect the analysis of safety data.

- Any diagnosed or suspected malignancy.

- Pregnancy, breast feeding.

- Participation in any other clinical study during 30 days or 6 periods of half life
(depending on what is longer) prior to screening.

- Patients that need treatment with drugs prohibited by the study protocol (opioid
antagonists, psychotropic medications, opioid analgesics, anticonvulsants, central
muscle relaxants, antineoplastic drugs, glucocorticoids).