MAP: Opioid/Benzodiazepine Polydrug Abuse: Aim 3

Sponsor

Wayne State University (Other)

Overall Status

Recruiting

CT.gov ID

NCT05006079

Collaborator

Henry Ford Health System (Other)

Enrollment

Location

Arms

29.6

Anticipated Duration (Months)

0.8

Patients Per Site Per Month

Study Details

Study Description

Brief Summary

In this study, the investigators will measure affective, neurocognitive and behavioral outcomes related to chronic use of opioids and benzodiazepines (screening phase), and in response to the administration of the opioid morphine, the benzodiazepine alprazolam, morphine then alprazolam, alprazolam then morphine, morphine+alprazolam simultaneously, and placebo (laboratory pharmacology experiment). The latter will enable the investigators to assess the effects of an opioid alone, benzodiazepine alone, concurrent and simultaneous administration of opioid+benzodiazepine, relative to a placebo control.

Condition or Disease	Intervention/Treatment	Phase
Opioid Abuse Benzodiazepine Abuse Polysubstance Abuse	Drug: Morphine Drug: Alprazolam Drug: Placebo	Phase 2

Detailed Description

The investigators propose that benzodiazepine/opioid polysubstance abuse is perpetuated by a dual-deficit in affective/hedonic regulation (difficulties modulating emotional reactions relative to the context and the person's long-term goals). Furthermore, the investigators propose that this dual-deficit biases neurocognition (interferes with executive function) and behaviors (guided by negative reinforcement processes such that polysubstance use acutely blunts aversive states and directs actions away from natural rewards). The scientific premise for this project builds on George Koob's foundational concept that addiction is a 'reward-deficit/stress-surfeit disorder'. There is an urgent need to obtain clinical pharmacology and mechanistic data to test this hypothesis of dual-deficit in affective/hedonic regulation. This study will use human laboratory methods to test affective, neurocognitive and behavioral mechanisms that maintain benzodiazepine/opioid polysubstance abuse.

The screening phase of this human laboratory study will include measures of affective dysregulation related to benzodiazepine/opioid polysubstance use behaviors. These include distress tolerance, pain sensitivity and nocebo responding, and biomarkers (e.g. plasma cortisol). Also, the investigators will include behavioral measures of drug and non-drug reinforcement (e.g. economic simulations of price elasticity of alprazolam and morphine) and neurocognition (e.g. drug attentional bias, response inhibition, cognitive flexibility).

During the pharmacology study the investigators will administer oral placebo, morphine alone and alprazolam doses alone, as well as morphine and alprazolam sequentially (in counterbalanced order) and simultaneously. Following each drug administration, the investigators will measure responses in affective (e.g. anxiety levels, distress tolerance), neurocognitive (e.g. executive function, learning) and behavioral domains (e.g. impulsivity, psychomotor function, reinforcer preferences). The lab study is highly significant because we lack prospective, controlled, dose-response studies that identify whether opioids, benzodiazepines, and their combination modulate core phenotypes that underlie this harmful polysubstance abuse. Testing effects of both sequential and simultaneous benzodiazepine/opioid administration within the same individuals will establish a firm foundation for understanding which phenotypes are sensitive to disruption and may respond to treatment.

Findings from this study will help to focus clinical assessment and identify mechanisms that maintain benzodiazepine/opioid polysubstance abuse, toward the development of novel medication-assisted, evidence-based psychosocial interventions.

Study Design

Study Type:

Interventional

Anticipated Enrollment :

24 participants

Allocation:

Randomized

Intervention Model:

Crossover Assignment

Intervention Model Description:

Repeated measures, placebo-controlled, randomized crossoverRepeated measures, placebo-controlled, randomized crossover

Masking:

Double (Participant, Outcomes Assessor)

Masking Description:

drug doses will be encapsulated, and placebo is included in the design

Primary Purpose:

Basic Science

Official Title:

Opioid/Benzodiazepine Polydrug Abuse: Integrating Research on Mechanisms, Treatment and Policies - Study 3

Actual Study Start Date :

Jun 15, 2022

Anticipated Primary Completion Date :

Aug 1, 2024

Anticipated Study Completion Date :

Dec 1, 2024

Arms and Interventions

Arm	Intervention/Treatment
Placebo Comparator: Placebo drug Lactose, administered both at 9:30 am and 12:00 pm	Drug: Placebo Lactose
Active Comparator: Morphine alone 15mg immediate-release oral morphine, administered both at 9:30 am and 12:00 pm	Drug: Morphine immediate release oral 15mg dose
Active Comparator: Alprazolam alone 0.25mg oral alprazolam, administered at both 9:30 am and 12:00 pm	Drug: Alprazolam oral 0.25mg dose
Active Comparator: Morphine then alprazolam 15mg oral morphine administered at 9:30 am, then 0.25mg oral alprazolam administered at 12:00 pm	Drug: Morphine immediate release oral 15mg dose Drug: Alprazolam oral 0.25mg dose
Active Comparator: Alprazolam then morphine 0.25mg oral alprazolam administered at 9:30 am, then 15mg oral morphine administered at 12:00 pm	Drug: Morphine immediate release oral 15mg dose Drug: Alprazolam oral 0.25mg dose
Active Comparator: Morphine+alprazolam simultaneously morphine 15mg + 0.25mg alprazolam at 9:30 am, then morphine 15mg + 0.25mg alprazolam at 12:00 pm	Drug: Morphine immediate release oral 15mg dose Drug: Alprazolam oral 0.25mg dose

Outcome Measures

Primary Outcome Measures

State anxiety [within-session peak change from pre-drug baseline to 15-120 min post-drug 1 and 15-240 min post-drug 2 administration; measured in each of the 6 laboratory sessions over about 3 weeks]
State Trait Anxiety Inventory - state anxiety scale total score
Positive affect [within-session peak change from baseline to 15-120 min post-drug 1 and 15-240 min post-drug 2 administration; measured in each of the 6 laboratory sessions over about 3 weeks]
Positive and Negative Affect Scale-Short Form (PANAS-SF) positive affect scale score
Negative affect [within-session peak change from baseline to 15-120 min post-drug 1 and 15-240 min post-drug 2 administration; measured in each of the 6 laboratory sessions over about 3 weeks]
Positive and Negative Affect Scale-Short Form (PANAS-SF) negative affect scale score

Secondary Outcome Measures

Symbol matching performance task [difference from placebo condition, measured within each session at 15-240 min post-drug 2 administration; measured in each of the 6 laboratory sessions over about 3 weeks]
Digit Symbol Substitution Task (DSST) symbol matching total score
Impulsivity performance task accuracy [difference from placebo condition, measured within each session at 15-240 min post-drug 2 administration; measured in each of the 6 laboratory sessions over about 3 weeks]
Go/No task percentage of trials correct
Cognitive flexibility performance task [difference from placebo condition, measured within each session at 15-240 min post-drug 2 administration; measured in each of the 6 laboratory sessions over about 3 weeks]
Wisconsin Card Sorting Task (WCST) percentage of trials correct
Cognitive inhibition performance task [difference from placebo condition, measured within each session at 15-240 min post-drug 2 administration; measured in each of the 6 laboratory sessions over about 3 weeks]
Addiction Stroop Task, reaction time to drug vs. neutral words presented in different colors
Vigilance performance task [difference from placebo condition, measured within each session at 15-240 min post-drug 2 administration; measured in each of the 6 laboratory sessions over about 3 weeks]
Psychomotor Vigilance Task (PVT) average reaction time
Hypothetical drug purchasing questionnaire [difference from placebo condition, measured within each session at 15-240 min post-drug 2 administration; measured in each of the 6 laboratory sessions over about 3 weeks]
Intensity and elasticity of drug demand. This is measured by having the participant make a series of independent choices as to how many drug units s/he will purchase across a range of (low to high) unit prices. Demand intensity is the drug purchase amount at the lowest non-zero price. Demand intensity is the calculated point on the price/purchasing curve where the slope (in log/log space) equals -1 (i.e. 'tipping point' where purchasing decreases more rapidly than the rate of increase in drug price).
Preference for natural reinforcement choice procedure [difference from placebo condition, measured within each session at 15-240 min post-drug 2 administration; measured in each of the 6 laboratory sessions over about 3 weeks]
Number of choices for money vs. avoiding listening to soundtrack of crying babies
Monetary delay discounting questionnaire [difference from placebo condition, measured within each session at 15-240 min post-drug 2 administration; measured in each of the 6 laboratory sessions over about 3 weeks]
Participants are asked to make a series of independent choices (preferences) for delayed larger amounts of money vs. smaller immediate amounts of money. The outcome is the rate at which future choice value is discounted, measured by area under the time-delay curve
Respiration rate [within-session peak change from baseline to 15-120 min post-drug 1 and 15-240 min post-drug 2 administration; measured in each of the 6 laboratory sessions over about 3 weeks]
Breaths per minute, measured by behavioral observation
Oxygen saturation [within-session peak change from baseline to 15-120 min post-drug 1 and 15-240 min post-drug 2 administration; measured in each of the 6 laboratory sessions over about 3 weeks]
Percentage oxygen saturation, measured by photoplethysmograph
Heart rate [within-session peak change from baseline to 15-120 min post-drug 1 and 15-240 min post-drug 2 administration; measured in each of the 6 laboratory sessions over about 3 weeks]
Pulse rate (beats per minute), measured by photoplethysmograph
Blood pressure [within-session peak change from baseline to 15-120 min post-drug 1 and 15-240 min post-drug 2 administration; measured in each of the 6 laboratory sessions over about 3 weeks]
Systolic and diastolic blood pressure (mm Hg)
Pupil diameter [within-session peak change from baseline to 15-120 min post-drug 1 and 15-240 min post-drug 2 administration; measured in each of the 6 laboratory sessions over about 3 weeks]
Pupil size (mm), measured by digital photography
Drug effect visual analog scale (VAS) ratings [within-session peak change from baseline to 15-120 min post-drug 1 and 15-240 min post-drug 2 administration; measured in each of the 6 laboratory sessions over about 3 weeks]
0-100 scale ratings of alert, difficulty concentrating, clumsy, confused, forgetful, blurred vision, dizzy, heaviness in limbs, mellow, yawning, stimulated, sedated, sleepy, tired, energetic, self-confident, dreamy, floating, sluggish, tingling, high, liking, good drug effect, bad drug effect
Drug craving visual analog scale (VAS) ratings [within-session peak change from baseline to 15-120 min post-drug 1 and 15-240 min post-drug 2 administration; measured in each of the 6 laboratory sessions over about 3 weeks]
0-100 scale rating of "want to take drug again", "desire to use", and "craving" for opioids, sedatives, alcohol, cigarettes, marihuana, and cocaine
Sleep efficiency [difference from placebo condition, measured on an outpatient basis during the evening after each laboratory drug administration; measured after each of the 6 laboratory sessions over about 3 weeks]
Percentage of sleep time (time asleep divided by time in bed), measured using WatchPat device

Eligibility Criteria

Criteria

Ages Eligible for Study:

18 Years to 60 Years

Sexes Eligible for Study:

All

Accepts Healthy Volunteers:

Inclusion Criteria:

must self-report past 5-year experience taking opioid and sedative drugs (for therapeutic or non-therapeutic reasons), but not necessarily at the same time, and may have current mild- or moderate-severity Opioid Use Disorder or current mild- or moderate-severity Sedative Use Disorder;
must not be seeking treatment for their substance use problems;
must be in current good overall health

Exclusion Criteria:

meet DSM-5 criteria for current psychosis, bipolar disorder, or severe depression (i.e. severe psychiatric disorder);
meet DSM-5 criteria for severe substance use disorder for any substance (e.g. Sedative, Opioid, Alcohol);
past-month benzodiazepine or opioid prescription (which would suggest daily use, tolerance, or withdrawal upon cessation);
report of past-year any-drug overdose or suicide attempt/ideation;
exhibit cognitive impairment (IQ < 80 on the Shipley Institute of Living Scale);
neurological, cardiovascular, pulmonary, or systemic diseases (see specific exclusionary conditions under Protection of Human Subjects);
body mass index > 32 kg/m2;
females who are pregnant (urine), lactating or heterosexually active (self-report) and not using medically approved birth control;
treatment with methadone, buprenorphine or naltrexone;
past 30-day use of contraindicated medications;
alcohol-positive breath sample (>.02% breath alcohol concentration);
urine sample positive for methadone, cocaine, amphetamines, or barbiturates (<300 ng/ml)

Contacts and Locations

Locations

	Site	City	State	Country	Postal Code
1	Tolan Park Medical Building	Detroit	Michigan	United States	48201

Sponsors and Collaborators

Wayne State University
Henry Ford Health System

Investigators

Principal Investigator: Mark K Greenwald, PhD, Wayne State University

Study Documents (Full-Text)

None provided.

More Information

Publications

None provided.

Responsible Party:

Mark Greenwald, PhD, Professor of Psychiatry and Behavioral Neurosciences; and Director, Substance Abuse Research Division, Wayne State University

ClinicalTrials.gov Identifier:

NCT05006079

Other Study ID Numbers:

IRB-21-07-3844

First Posted:

Aug 16, 2021

Last Update Posted:

Jun 29, 2022

Last Verified:

Jun 1, 2022

Individual Participant Data (IPD) Sharing Statement:

Plan to Share IPD:

Studies a U.S. FDA-regulated Drug Product:

Yes

Studies a U.S. FDA-regulated Device Product:

Product Manufactured in and Exported from the U.S.:

Yes

Additional relevant MeSH terms:

Opioid-Related Disorders

Morphine

Alprazolam

Study Results

No Results Posted as of Jun 29, 2022