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Addiction Treatment in Russia: Oral vs. Naltrexone Implant

Addiction Treatment in Russia: Oral and Depot Naltrexone

Status
Completed
Phases
Phase 2Phase 3
Study type
Interventional
Source
ClinicalTrials.gov
Registry ID
NCT00218426
Enrollment
306
Registered
2005-09-22
Start date
2006-07-31
Completion date
2010-11-04
Last updated
2019-03-18

For informational purposes only — not medical advice. Sourced from public registries and may not reflect the latest updates. Terms

Conditions

Heroin Dependence, Opioid-Related Disorders

Brief summary

Heroin addiction is a growing problem in Russia; individuals who enter heroin addiction treatment often relapse. Therefore, effective heroin addiction treatments are necessary to prevent relapse. The purpose of this study is to compare oral naltrexone with a naltrexone implant that provides opioid blockade for two months in preventing relapse to heroin addiction in St. Petersburg, Russia.

Detailed description

The usual treatment of heroin addiction in Russia involves detoxification and 2-4 weeks of rehabilitation with referral to outpatient follow-up. Though most patients complete inpatient treatment, few keep follow-up appointments and relapse rates are high. More effective therapies are needed, especially in view of the epidemic of heroin addiction that has resulted in the spread of HIV and other infectious diseases. A recently-completed study of 52 patients randomized to oral naltrexone (ON) or oral naltrexone placebo (ONP) has shown efficacy in preventing relapse and reducing HIV risk but dropout was a problem with only 44% of ON patients proven to have not relapsed by 6 months (as compared to 16% of ONP patients). A larger study of 280 patients randomized to ON or ONP replicated these results and found some indication that adding an selective serotonin reuptake inhibitor (SSRI) to naltrexone may improve its efficacy in women, probably because they tend to have higher levels of psychiatric symptoms than men. We think that retention and outcome can be improved by using a longer acting naltrexone preparation, and in this study we propose to compare ON with a depot naltrexone implant (DNI) that is manufactured and approved for use in Russia, and provides opioid blockade for 8-10 weeks. We will use a placebo-controlled, double-blind/double-dummy design since a placebo-controlled trial is required by the Russian equivalent of our FDA as a condition for testing a pharmacotherapy. Participants will be male and female heroin addicts who have been detoxified in addiction treatment hospitals or outpatient settings in St. Petersburg and have a family member willing and able to supervise medication adherence and facilitate follow-up. After giving informed consent and confirming the absence of physiologic dependence, 306 patients will be randomly assigned to a 6-month treatment in one of three groups of 102 each: oral naltrexone (ON) + depot naltrexone implant placebo (DNIP); oral naltrexone placebo (ONP) + depot naltrexone implant (DNI); or ONP + DNIP. All patients will receive biweekly clinical management/adherence enhancement counseling. Assessments will be done at baseline, at each biweekly appointment during the 6-months of medication treatment, and at 3 and 6 months following the end of study medication. Primary outcome will be the relapse free proportion at months 1-6; secondary outcomes will be time to dropout, opioid positive urines, HIV risk, use of alcohol and other drugs, psychiatric symptoms, and other measures of overall adjustment. We hypothesize that outcomes will be better with DNI than ON, and that each will be more effective than placebo.

Interventions

DRUGnaltrexone implant

naltrexone implant is 1000 mg naltrexone

DRUGoral naltrexone

oral naltrexone 50 mg/day

DRUGoral placebo naltrexone

oral placebo naltrexone resembles active medication

DRUGplacebo implant

placebo implant resembles active medication

Sponsors

National Institute on Drug Abuse (NIDA)
CollaboratorNIH
St. Petersburg State Pavlov Medical University
CollaboratorOTHER
University of Pennsylvania
Lead SponsorOTHER

Study design

Allocation
RANDOMIZED
Intervention model
PARALLEL
Primary purpose
TREATMENT
Masking
QUADRUPLE (Subject, Caregiver, Investigator, Outcomes Assessor)

Eligibility

Sex/Gender
ALL
Age
18 Years to 50 Years
Healthy volunteers
No

Inclusion criteria

* Current opioid dependence * Recently completed opioid detoxification

Exclusion criteria

* Serious medical or psychiatric condition requiring immediate hospitalization or that would make participation in the study hazardous * Planning to leave the study area within the 12 months following study entry * Imminent incarceration * Pregnancy

Design outcomes

Primary

MeasureTime frameDescription
Retention Without Relapse to Heroin Addiction (Measured at Month 6)6 monthsSurvival analysis (Kaplan-Meier survival functions with log-rank Cox-Mantel criteria for group comparison was used to determine the primary outcome of retention, defined as not missing 2 consecutive counseling sessions and not having a relapse. Because this outcome combined patients who failed to keep appointments with those who kept appointments but relapsed, the proportion of non-survivors attributable to proven relapse.

Secondary

MeasureTime frameDescription
Positive Opioid Urine Test6 monthsmissed urine tests were imputed to be positive for opiates
Use of Alcohol6 monthsuse of alcohol grams per day
Composite Score of Psychiatric Problems6 monthscomposite score is a decimal score; with 0 = no problems, 1 = the most problems based on the Addiction Severity Index composite score of 11 indexed questions.
HIV Risk (Baseline)baselineThe Risk Assessment Behavior (RAB), is an HIV risk Scale. The Total Score is scored by adding the values that correspond to the responses selected by the subject for the items asked. This highest total score is 40 (highest risk), and the lowest score = 0 (no risk). This assessment has 2 Subsections: 1) Drug Risk = 8 questions (lowest Drug Risk score = 0 (no risk), and highest drug risk score = 22 =(greatest risk), 2) 10 Sex Risk questions: scores are 0 = no risk, and 18 = highest risk). Total RAB Score = Drug Risk Total + Sex Risk Total (0 = no risk, 40 = highest). See: Risk Assessment Battery (RAB) Scoring System, https://www.med.upenn.edu/hiv/assets/user-content/.../RABScoringv2.112.21.95.doc
Number of Subjects Who Dropped Out of Treatment6 monthsKaplan-Meier survival curves for the event of subjects who dropped out of treatment
Amphetamine Drug UsebaselineNumber of subjects who used Amphetamine in the past 90 days at baseline as measured by the TimeLine Follow-back Form (TLFB) . The TLFB is an instrument that assesses substance use over a specified period of time (Sobel & Sobel, 1992).
Cocaine Drug UsebaselineNumber of subjects with cocaine drug use in the past 90 days at baseline as measured by the TimeLine Follow-back Form (TLFB) . The TLFB is an instrument that assesses substance use over a specified period of time (Sobel & Sobel, 1992).
Marijuana Drug UsebaselineNumber of subjects with Marijuana use in the past 90 days at baseline as measured by the TimeLine Follow-back Form (TLFB) . The TLFB is an instrument that assesses substance use over a specified period of time (Sobel & Sobel, 1992).
Benzodiazepine Drug UsebaselineNumber of subjects with benzodiazepine drug use in the past 90 days at baseline as measured by the TimeLine Follow-back Form (TLFB) . The TLFB is an instrument that assesses substance use over a specified period of time (Sobel & Sobel, 1992).
Global Assessment Form (GAF)baselineAssessment of overall psychiatric function comprises Axis V in the DSM-IV (DSM-IV, 1994). GAF scores range from 0 to 100. A reasonably well-functioning person will score above 70; serious impairment is below 50.

Countries

Russia, United States

Participant flow

Recruitment details

Subjects (SS) are from Leningrad Regional Alcoholism and Substance Abuse Treatment Center, Leningrad Region; and St. Petersburg City Alcoholism and Substance Abuse Treatment Center, screened for detoxification and if met study criteria and interested were referred to study on day of discharge. First SS admitted on 7/31/06, last visit was 1/4/09.

Pre-assignment details

SS were opioid dependent with physiological features for at least 1 year, negative urine for opioids, had ability to give informed consent, not on psychotropic medication, if female, not pregnant, could provide at least 1 relative contact, no significant lab abnormality, and not major psych disorder.

Participants by arm

ArmCount
ONP + DNI
Oral naltrexone placebo + Depot Naltrexone Implant 1000 mg naltrexone implant: depot implant is 1000 mg naltrexone placebo oral tablet: placebo oral tablet resembles active medication
102
ON + DNIP
Oral naltrexone 50 mg + Depot Naltrexone placebo Implant oral naltrexone: oral naltrexone 50 mg/day depot placebo implant: placebo implant resembles active medication
102
ONP + DNIP
Oral placebo naltrexone + placebo naltrexone implant placebo oral tablet: placebo oral tablet resembles active medication depot placebo implant: placebo implant resembles active medication
102
Total306

Baseline characteristics

CharacteristicONP + DNION + DNIPONP + DNIPTotal
Age, Categorical
<=18 years
0 Participants0 Participants0 Participants0 Participants
Age, Categorical
>=65 years
0 Participants0 Participants0 Participants0 Participants
Age, Categorical
Between 18 and 65 years
102 Participants102 Participants102 Participants306 Participants
Age, Continuous28.0 years27.9 years28.7 years28.2 years
Ethnicity (NIH/OMB)
Hispanic or Latino
0 Participants0 Participants0 Participants0 Participants
Ethnicity (NIH/OMB)
Not Hispanic or Latino
102 Participants102 Participants102 Participants306 Participants
Ethnicity (NIH/OMB)
Unknown or Not Reported
0 Participants0 Participants0 Participants0 Participants
Race (NIH/OMB)
American Indian or Alaska Native
0 Participants0 Participants0 Participants0 Participants
Race (NIH/OMB)
Asian
0 Participants0 Participants0 Participants0 Participants
Race (NIH/OMB)
Black or African American
0 Participants0 Participants0 Participants0 Participants
Race (NIH/OMB)
More than one race
0 Participants0 Participants0 Participants0 Participants
Race (NIH/OMB)
Native Hawaiian or Other Pacific Islander
0 Participants0 Participants0 Participants0 Participants
Race (NIH/OMB)
Unknown or Not Reported
0 Participants0 Participants0 Participants0 Participants
Race (NIH/OMB)
White
102 Participants102 Participants102 Participants306 Participants
Region of Enrollment
Russia
102 participants102 participants102 participants360 participants
Sex: Female, Male
Female
28 Participants28 Participants28 Participants84 Participants
Sex: Female, Male
Male
74 Participants74 Participants74 Participants222 Participants

Adverse events

Event typeEG000
affected / at risk
EG001
affected / at risk
EG002
affected / at risk
deaths
Total, all-cause mortality
0 / 1020 / 1020 / 102
other
Total, other adverse events
6 / 10217 / 1023 / 102
serious
Total, serious adverse events
0 / 1020 / 1021 / 102

Outcome results

Primary

Retention Without Relapse to Heroin Addiction (Measured at Month 6)

Survival analysis (Kaplan-Meier survival functions with log-rank Cox-Mantel criteria for group comparison was used to determine the primary outcome of retention, defined as not missing 2 consecutive counseling sessions and not having a relapse. Because this outcome combined patients who failed to keep appointments with those who kept appointments but relapsed, the proportion of non-survivors attributable to proven relapse.

Time frame: 6 months

Population: Subjects who remained in treatment without relapse. remaining in treatment = 6 months manualized clinical counseling, plus medication.

ArmMeasureValue (COUNT_OF_PARTICIPANTS)
ON + DNIP, Oral Naltrexone + Depot Placebo Naltrexone ImplantRetention Without Relapse to Heroin Addiction (Measured at Month 6)54 Participants
DNI + ONP , Naltrexone Implant + Oral Naltrexone PlaceboRetention Without Relapse to Heroin Addiction (Measured at Month 6)16 Participants
ONP + DNIP, Oral Placebo Naltrexone and Depot Placebo ImplantRetention Without Relapse to Heroin Addiction (Measured at Month 6)11 Participants
Secondary

Amphetamine Drug Use

Number of subjects who used Amphetamine in the past 90 days at baseline as measured by the TimeLine Follow-back Form (TLFB) . The TLFB is an instrument that assesses substance use over a specified period of time (Sobel & Sobel, 1992).

Time frame: baseline

ArmMeasureValue (COUNT_OF_PARTICIPANTS)
ON + DNIP, Oral Naltrexone + Depot Placebo Naltrexone ImplantAmphetamine Drug Use6 Participants
DNI + ONP , Naltrexone Implant + Oral Naltrexone PlaceboAmphetamine Drug Use12 Participants
ONP + DNIP, Oral Placebo Naltrexone and Depot Placebo ImplantAmphetamine Drug Use18 Participants
Secondary

Benzodiazepine Drug Use

Number of subjects with benzodiazepine drug use in the past 90 days at baseline as measured by the TimeLine Follow-back Form (TLFB) . The TLFB is an instrument that assesses substance use over a specified period of time (Sobel & Sobel, 1992).

Time frame: baseline

ArmMeasureValue (COUNT_OF_PARTICIPANTS)
ON + DNIP, Oral Naltrexone + Depot Placebo Naltrexone ImplantBenzodiazepine Drug Use10 Participants
DNI + ONP , Naltrexone Implant + Oral Naltrexone PlaceboBenzodiazepine Drug Use15 Participants
ONP + DNIP, Oral Placebo Naltrexone and Depot Placebo ImplantBenzodiazepine Drug Use9 Participants
Secondary

Cocaine Drug Use

Number of subjects with cocaine drug use in the past 90 days at baseline as measured by the TimeLine Follow-back Form (TLFB) . The TLFB is an instrument that assesses substance use over a specified period of time (Sobel & Sobel, 1992).

Time frame: baseline

ArmMeasureValue (COUNT_OF_PARTICIPANTS)
ON + DNIP, Oral Naltrexone + Depot Placebo Naltrexone ImplantCocaine Drug Use0 Participants
DNI + ONP , Naltrexone Implant + Oral Naltrexone PlaceboCocaine Drug Use0 Participants
ONP + DNIP, Oral Placebo Naltrexone and Depot Placebo ImplantCocaine Drug Use0 Participants
Secondary

Composite Score of Psychiatric Problems

composite score is a decimal score; with 0 = no problems, 1 = the most problems based on the Addiction Severity Index composite score of 11 indexed questions.

Time frame: 6 months

Population: mean of composite score

ArmMeasureValue (MEAN)Dispersion
ON + DNIP, Oral Naltrexone + Depot Placebo Naltrexone ImplantComposite Score of Psychiatric Problems0.19 composite scoreStandard Deviation 0.02
DNI + ONP , Naltrexone Implant + Oral Naltrexone PlaceboComposite Score of Psychiatric Problems0.15 composite scoreStandard Deviation 0.02
ONP + DNIP, Oral Placebo Naltrexone and Depot Placebo ImplantComposite Score of Psychiatric Problems0.18 composite scoreStandard Deviation 0.02
Secondary

Global Assessment Form (GAF)

Assessment of overall psychiatric function comprises Axis V in the DSM-IV (DSM-IV, 1994). GAF scores range from 0 to 100. A reasonably well-functioning person will score above 70; serious impairment is below 50.

Time frame: baseline

ArmMeasureValue (MEAN)Dispersion
ON + DNIP, Oral Naltrexone + Depot Placebo Naltrexone ImplantGlobal Assessment Form (GAF)62.8 score on a scaleStandard Deviation 0.7
DNI + ONP , Naltrexone Implant + Oral Naltrexone PlaceboGlobal Assessment Form (GAF)64.7 score on a scaleStandard Deviation 0.8
ONP + DNIP, Oral Placebo Naltrexone and Depot Placebo ImplantGlobal Assessment Form (GAF)62.5 score on a scaleStandard Deviation 0.9
Secondary

HIV Risk (Baseline)

The Risk Assessment Behavior (RAB), is an HIV risk Scale. The Total Score is scored by adding the values that correspond to the responses selected by the subject for the items asked. This highest total score is 40 (highest risk), and the lowest score = 0 (no risk). This assessment has 2 Subsections: 1) Drug Risk = 8 questions (lowest Drug Risk score = 0 (no risk), and highest drug risk score = 22 =(greatest risk), 2) 10 Sex Risk questions: scores are 0 = no risk, and 18 = highest risk). Total RAB Score = Drug Risk Total + Sex Risk Total (0 = no risk, 40 = highest). See: Risk Assessment Battery (RAB) Scoring System, https://www.med.upenn.edu/hiv/assets/user-content/.../RABScoringv2.112.21.95.doc

Time frame: baseline

ArmMeasureValue (MEAN)Dispersion
ON + DNIP, Oral Naltrexone + Depot Placebo Naltrexone ImplantHIV Risk (Baseline)8.1 score on a scaleStandard Deviation 0.44
DNI + ONP , Naltrexone Implant + Oral Naltrexone PlaceboHIV Risk (Baseline)8.0 score on a scaleStandard Deviation 0.47
ONP + DNIP, Oral Placebo Naltrexone and Depot Placebo ImplantHIV Risk (Baseline)8.7 score on a scaleStandard Deviation 0.49
Secondary

Marijuana Drug Use

Number of subjects with Marijuana use in the past 90 days at baseline as measured by the TimeLine Follow-back Form (TLFB) . The TLFB is an instrument that assesses substance use over a specified period of time (Sobel & Sobel, 1992).

Time frame: baseline

ArmMeasureValue (COUNT_OF_PARTICIPANTS)
ON + DNIP, Oral Naltrexone + Depot Placebo Naltrexone ImplantMarijuana Drug Use22 Participants
DNI + ONP , Naltrexone Implant + Oral Naltrexone PlaceboMarijuana Drug Use35 Participants
ONP + DNIP, Oral Placebo Naltrexone and Depot Placebo ImplantMarijuana Drug Use25 Participants
Secondary

Number of Subjects Who Dropped Out of Treatment

Kaplan-Meier survival curves for the event of subjects who dropped out of treatment

Time frame: 6 months

ArmMeasureValue (NUMBER)
ON + DNIP, Oral Naltrexone + Depot Placebo Naltrexone ImplantNumber of Subjects Who Dropped Out of Treatment54 participants
DNI + ONP , Naltrexone Implant + Oral Naltrexone PlaceboNumber of Subjects Who Dropped Out of Treatment16 participants
ONP + DNIP, Oral Placebo Naltrexone and Depot Placebo ImplantNumber of Subjects Who Dropped Out of Treatment11 participants
Secondary

Positive Opioid Urine Test

missed urine tests were imputed to be positive for opiates

Time frame: 6 months

Population: missing = positive; results negative for opioids

ArmMeasureValue (NUMBER)
ON + DNIP, Oral Naltrexone + Depot Placebo Naltrexone ImplantPositive Opioid Urine Test.427 urine tests
DNI + ONP , Naltrexone Implant + Oral Naltrexone PlaceboPositive Opioid Urine Test.636 urine tests
ONP + DNIP, Oral Placebo Naltrexone and Depot Placebo ImplantPositive Opioid Urine Test.341 urine tests
Secondary

Use of Alcohol

use of alcohol grams per day

Time frame: 6 months

ArmMeasureValue (MEAN)Dispersion
ON + DNIP, Oral Naltrexone + Depot Placebo Naltrexone ImplantUse of Alcohol10.2 grams per dayStandard Deviation 1.7
DNI + ONP , Naltrexone Implant + Oral Naltrexone PlaceboUse of Alcohol9.0 grams per dayStandard Deviation 1.7
ONP + DNIP, Oral Placebo Naltrexone and Depot Placebo ImplantUse of Alcohol9.6 grams per dayStandard Deviation 1.6

Source: ClinicalTrials.gov · Data processed: Feb 4, 2026