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NCT03431987 Clinical Trial

Neuroscience of Alcohol and Marijuana Impaired Driving

Alcohol Drinking Clinical Trial

Official title:
Neuroscience of Alcohol and Marijuana Impaired Driving

Clinical Trial Details — Status: Recruiting

Administrative data
NCT number NCT03431987
Other study ID # HHC-2016-0183
Secondary ID
Status Recruiting
Phase
First received
Last updated
Start date July 1, 2018
Est. completion date December 2023

Study information
Verified date August 2022
Source Hartford Hospital
Contact Lindsey Repoli, BS
Phone 860-545-7233
Email lindsey.repoli@hhchealth.org
Is FDA regulated No
Health authority
Study type Observational

Clinical Trial Summary

Alcohol is one of the most widely used intoxicants. The effects of driving while intoxicated are well documented, leading to the laws and regulations behind drunk driving. Marijuana is also a commonly abused drug, whose use is increasing with widespread legalization/decriminalization in many US states and use of medical marijuana. Marijuana use is linked to cognitive impairment and is likely be the cause of intoxication-induced accidents. The effects of marijuana intoxication on driving impairments are less documented than those of alcohol. However, most marijuana users also consume alcohol when smoking cannabis, and preliminary data strongly suggest that driving impairment from both drugs used together is synergistic rather than just additive. This study will aim to investigate the brain and behavior in the same individuals, using a similar design to the current Neuroscience of Marijuana Impaired Driving and the prior Alcohol and Driving Grant, that used similar techniques and measures to quantify drunk automobile driving. We hypothesize that alcohol and marijuana use combined will lead to greater impairment in a simulated driving task, as well as other driving-related cognitive impairments. In a randomized, counterbalanced, double-blind study, we will dose participants with alcohol to a legal level of 0.05% blood alcohol content, then we will administer a moderate inhaled dose of THC marijuana or placebo marijuana, using paced inhalation that employees a vaporizer. Participants will comprise 10 regular alcohol and marijuana consumers aged 21 to 40 years of age; all participants must report smoking marijuana and drinking alcohol together. Of the 10, 5 will be occasional marijuana smokers and 5 frequent marijuana smokers. Following this dosing, we will assess impairment through cognitive testing as well as a simulated driving test through fMRI and neuropsychological tests. Samples of breath, blood and oral fluid will also be collected at multiple time points throughout the study visits to be measured for alcohol and THC concentration and its metabolites. This allows clarification between the relationship of impairment, as well as subjective and objective intoxication, and levels of THC and its metabolites in the users system.

Description:

Alcohol is one of the most widely used intoxicants. The effects of driving while intoxicated are well documented, leading to the laws and regulations behind drunk driving. Marijuana is also a commonly abused drug, whose use is increasing with widespread legalization/decriminalization in many US states and use of medical marijuana. Marijuana use is linked to cognitive impairment and is likely be the cause of intoxication-induced accidents. The effects of marijuana intoxication on driving impairments are less documented than those of alcohol. However, most marijuana users also consume alcohol when smoking cannabis, and preliminary data strongly suggest that driving impairment from both drugs used together is synergistic rather than just additive. Data are being gathered currently in regards to the risk of marijuana-impaired driving from our NIDA-funded Neuroscience of Marijuana Impaired Driving study. Previously we had a grant award from NIAAA that investigated alcohol-impaired driving using a similar design. The current proposed study combines elements of both the NIDA and NIAAA studies, to assess the cognitive and brain impairment due to the simultaneous combination of beverage alcohol and smoked marijuana. Our own prior NIAAA-funded grant, the Brain and Alcohol Research with College Students (BARCS) study, along with epidemiological investigations reveal that most marijuana smokers also consume alcohol when intoxicated. These drugs interact pharmacodynamically and change each other's levels in the user's blood and saliva reference Marilyn study. They both have separate, deleterious effects on driving. These effects are not additive but rather multiplicative. A person using both substances will show more deleterious effects on driving performance than the same individual using just one of these substances. This study will aim to investigate the brain and behavior in the same individuals, using a similar design to the current Neuroscience of Marijuana Impaired Driving and the prior Alcohol and Driving Grant, that used similar techniques and measures to quantify drunk automobile driving. We hypothesize that alcohol and marijuana use combined will lead to greater impairment in a simulated driving task, as well as other driving-related cognitive impairments. In a randomized, counterbalanced, double-blind study, we will dose participants with alcohol to a legal level of 0.05% blood alcohol content, then we will administer a moderate inhaled dose of THC marijuana or placebo marijuana, using paced inhalation that employees a vaporizer. Participants will comprise 10 regular alcohol and marijuana consumers aged 21 to 40 years of age; all participants must report smoking marijuana and drinking alcohol together. Of the 10, 5 will be occasional marijuana smokers and 5 frequent marijuana smokers. Following this dosing, we will assess impairment through cognitive testing as well as a simulated driving test through fMRI and neuropsychological tests. Samples of breath, blood and oral fluid will also be collected at multiple time points throughout the study visits to be measured for alcohol and THC concentration and its metabolites. This allows clarification between the relationship of impairment, as well as subjective and objective intoxication, and levels of THC and its metabolites in the users system.

Recruitment information / eligibility
Status Recruiting
Enrollment 13
Est. completion date December 2023
Est. primary completion date December 2023
Accepts healthy volunteers Accepts Healthy Volunteers
Gender All
Age group 21 Years to 40 Years
Eligibility Inclusion Criteria: - Must have a current drivers license - Must have used marijuana and alcohol in combination before - Right handed Exclusion Criteria: - Females who are pregnant or breastfeeding - Unable or unsafe to have an MRI - Any serious medical or neurological disorder - Any psychiatric disorder - No major head traumas

Study Design

Related Conditions & MeSH terms

Intervention

Drug:
One day with a dose of placebo cannabis paired with alcohol
Vaporized placebo marijuana with little to no THC paired with drinking alcohol to BrAC of 0.05%
One day with a dose of active THC cannabis paired with alcohol
Vaporized marijuana with active THC paired with drinking alcohol to BrAC of 0.05%

Locations
Country Name City State
United States Olin Neuropsychiatry Research Center, Institute of Living, Hartford Hospital Hartford Connecticut

Sponsors (1)
Lead Sponsor Collaborator
Hartford Hospital

Country where clinical trial is conducted

United States, 

Outcome
Type Measure Description Time frame Safety issue
Primary Change in performance on simulated driving Gap Acceptance Task. The Gap Acceptance Task measures strategic control of the vehicle. Strategic control of the vehicle is measured by size of headway gaps that the participant chooses in pulling out into a stream of traffic. Post Dose: 30 minutes, 2.5 hours, and 5 hours
Primary Change in performance on simulated driving Road Tracking Task. The Road Tracking Task measures operational control of the vehicle. Operational control is measured by standard deviation of lane position from the center point of the lane. Post Dose: 30 minutes, 2.5 hours, and 5 hours
Primary Change in performance on simulated driving Car Following Task. The Car Following Task measures tactical control of the vehicle. Tactical control of the vehicle is measured by following distance from a lead vehicle. Post Dose: 30 minutes, 2.5 hours, and 5 hours
Primary Change in concentration of THC/metabolites in oral fluid tested using Quantisal Oral Fluid Collection devices. Saliva samples will be taken at 3 time points during the day using the Quantisal Oral Fluid Collection devices to assess for changes in concentration of THC and its metabolites. Before Dose and Post Dose: 30 minutes and 2.5 hours
Primary Change in concentration of THC/metabolites in blood samples. Blood samples will be taken at 3 time points during the day to assess for changes in concentration of THC and its metabolites. Before Dose and Post Dose: 30 minutes and 2.5 hours
Primary Marijuana performance changes on the Critical Tracking Task. The Critical Tracking Task assesses visuomotor tracking, it will be administered prior to dosing and at various time points after dosing Post Dose: 2 hours, 4 hours and 6 hours
Primary Intoxication induced performance changes on the Tower of London task. The Tower of London is a task that assesses executive functioning, it will be administered prior to dosing and at various time points after dosing. Post Dose: 2 hours, 4 hours and 6 hours
Primary Intoxication induced performance changes on the Cogstate 1-back/2-back task. The Cogstate 1-back/2-back task assesses working memory, it will be administered prior to dosing and at various time points after dosing. Post Dose: 2 hours, 4 hours and 6 hours
Primary Intoxication induced performance changes on the Cogstate Detection Task. The Cogstate Detection Task assesses processing speed, it will be administered prior to dosing and at various time points after dosing. Post Dose: 2 hours, 4 hours and 6 hours
Primary Intoxication induced performance changes on the Cogstate Set Shifting Task. The Cogstate Set Shifting Task assesses executive functioning, it will be administered prior to dosing and at various time points after dosing. Post Dose: 2 hours, 4 hours and 6 hours
Secondary Change in magnetic resonance spectroscopy scanning. Spectroscopy scanning will be completed to assess the change in chemical concentration of the brain. Post Dose: 2.5 hours
Secondary Change in electroencephalography at rest. EEG will be performed at several time points during the day wearing a Cognionics 4 Channel Quick-20 EEG headset while the participants sits and relaxes. Post Dose: 10 minutes, 1.5 hours, 2.25 hours, 4.5 hours
Secondary Change in electroencephalography while completing the driving simulation. EEG will be performed wearing a Cognionics 4 Channel Quick-20 EEG headset while the participant completes the driving simulation. Post Dose: 5 hours
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