Binge Drinking Clinical Trial
Official title:
The Brain, the Bug, and the Binge: a Double-blind, Randomized Controlled Trial Investigating the Interplay Between Binge Drinking, Gut Microbiota and Brain Functioning
Adolescence and youth are periods of significant maturational changes which seems to involve greater susceptibility to disruptive events in the brain such as binge drinking (BD). This prevalent pattern of consumption -characterized by repeated alcohol intoxications- is of special concern, as it has been associated with major neurocognitive impairments in the young brain. Recent studies indicate that alcohol may disrupt the gut microbiota (GM) and that these disruptions may lead to impairments in brain and behavior. Also, interventions with psychobiotics have been shown to result in reductions in alcohol-induced damage and in improvements on cognitive and brain functioning. Thus, the present proposal will explore the effects of BD on GM. Additionally, a GM intervention with psychobiotics both in-vivo and in-vitro, will determine whether improvements in GM composition/function may lead to reductions of alcohol-induced brain damage in BD-population, a barely unexplored research field with major clinical applications.
Status | Recruiting |
Enrollment | 82 |
Est. completion date | August 31, 2025 |
Est. primary completion date | June 30, 2024 |
Accepts healthy volunteers | Accepts Healthy Volunteers |
Gender | All |
Age group | 18 Years to 23 Years |
Eligibility | Inclusion Criteria: - College students whose native language is Portuguese; - Age 18-23 years; - Binge Drinkers: report (i) drinking 4 (for women)/5 (for men) or more drinks on one occasion at least once a month, (ii) drinking at a speed of at least two drinks per hour during these episodes (which brings blood alcohol concentration to 0.08 g/dL or above), and (iii) having an AUDIT score < 20. - Non/Low-Drinkers: report (i) never drinking 4/5 or more drinks on one occasion and (ii) having an AUDIT score = 4. Exclusion Criteria: - Use of illicit drugs as determined by the Drug Use Disorders Identification Test (DUDIT); - Alcohol abuse (i.e., AUDIT = 20); - Personal history of psychopathological disorders (according to DSM-V criteria); - History of traumatic brain injury or neurological disorder; - Family history (mother/father) of alcoholism diagnosis of substance abuse; - Occurrence of one or more episodes of loss of consciousness for more than 30 minutes; - Non-corrected sensory deficits; - Diagnosis of any gut disease/problems or other medical conditions: inflammatory bowel disease, irritable bowel syndrome, Crohn's Disease, celiac disease, lactose intolerance, autoimmune disease; - Consumption of medical drugs with psychoactive effects (e.g., antidepressants, anxiolytics or benzodiazepines) during the 4 weeks prior to the experiment; - Use of any of the following drugs in the last 4 weeks: laxatives, antibiotics, anticoagulants, non-steroidal anti-inflammatory drugs, analgesics, corticosteroids; - No type of metal object implanted in the body, especially in the head (orthodontic appliances are not excluded). |
Country | Name | City | State |
---|---|---|---|
Portugal | Psychological Neuroscience Laboratory, Psychology Research Center, University of Minho | Braga | Gualtar, Braga |
Lead Sponsor | Collaborator |
---|---|
University of Minho | Foundation for Science and Technology (FCT) |
Portugal,
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Lopez-Caneda E, Crego A, Campos AD, Gonzalez-Villar A, Sampaio A. The Think/No-Think Alcohol Task: A New Paradigm for Assessing Memory Suppression in Alcohol-Related Contexts. Alcohol Clin Exp Res. 2019 Jan;43(1):36-47. doi: 10.1111/acer.13916. Epub 2018 Nov 25. — View Citation
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* Note: There are 13 references in all — Click here to view all references
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Alcohol Consumption - Drinking pattern | The Alcohol Use Disorder Identification Test (AUDIT) will be administered to characterize the drinking pattern of the participants. AUDIT scores = 4 reveal low risk of alcohol use; scores between 5 and 20 represent excessive alcohol consumption; and scores = 20 indicate very high risk for alcohol dependence and warrant further diagnostic evaluation for alcohol dependence. | Screening visit (clinical interview) | |
Primary | Alcohol Consumption - Drinking pattern | The AUDIT will be administered to characterize the drinking pattern of the participants. AUDIT scores = 4 reveal low risk of alcohol use; scores between 5 and 20 represent excessive alcohol consumption; and scores = 20 indicate very high risk for alcohol dependence and warrant further diagnostic evaluation for alcohol dependence. | At baseline (pre-intervention) | |
Primary | Alcohol Consumption - Drinking pattern | The AUDIT will be administered to characterize the drinking pattern of the participants. AUDIT scores = 4 reveal low risk of alcohol use; scores between 5 and 20 represent excessive alcohol consumption; and scores = 20 indicate very high risk for alcohol dependence and warrant further diagnostic evaluation for alcohol dependence. | Immediately post-intervention | |
Primary | Alcohol Consumption - Drinking pattern | The AUDIT will be administered to characterize the drinking pattern of the participants. AUDIT scores = 4 reveal low risk of alcohol use; scores between 5 and 20 represent excessive alcohol consumption; and scores = 20 indicate very high risk for alcohol dependence and warrant further diagnostic evaluation for alcohol dependence. | 3 months post-intervention | |
Primary | Alcohol Craving - Short-term acute craving | Short-term alcohol craving levels will be assessed using the Alcohol Craving Questionnaire - Short form Revised (ACQ-SF-R) at the present moment. Total minimum score: 1 (low level of alcohol craving); Total maximum score: 7 (high level of alcohol craving). | Screening visit (clinical interview) | |
Primary | Alcohol Craving - Short-term acute craving | Short-term alcohol craving levels will be assessed using the Alcohol Craving Questionnaire - Short form Revised (ACQ-SF-R) at the present moment. Total minimum score: 1 (low level of alcohol craving); Total maximum score: 7 (high level of alcohol craving). | At baseline (pre-intervention) | |
Primary | Alcohol Craving - Short-term acute craving | Short-term alcohol craving levels will be assessed using the ACQ-SF-R at the present moment. Total minimum score: 1 (low level of alcohol craving); Total maximum score: 7 (high level of alcohol craving). | Immediately post-intervention | |
Primary | Alcohol Craving - Short-term acute craving | Short-term alcohol craving levels will be assessed using the ACQ-SF-R at the present moment. Total minimum score: 1 (low level of alcohol craving); Total maximum score: 7 (high level of alcohol craving). | 3 months post-intervention | |
Primary | Use of illicit drugs | The use of illicit drugs will be determined by the Drug Use Disorders Identification Test (DUDIT). DUDIT provides information on the level of drug intake and selected criteria for substance abuse/harmful use and dependence according to the ICD-10 and DSM-4 diagnostic systems. In this study, the use of sedative pills, analgesics and tobacco is not an exclusion criterion. | Screening visit (clinical interview) | |
Primary | Description of Food Frequency | Habitual dietary intake of each participant will be also measured using a Food Frequency Questionnaire. A detailed description, on average, of nutrients and food group values over the past 12 months will be obtained by classifying the frequency of consumption of each food/beverage type on a scale from never or less than once per month to =6 per day. | Screening visit (clinical interview) | |
Primary | Food Diary | During the intervention phase, each binge drinker should keep a record of everything they ate and drank during three days of each of the 6 weeks: two days a week and one at the weekend, according to their usual practice. They should also record the type of packaging of the food and drink and the place where they consumed them. | Intervention (6 weeks) | |
Primary | Impulsivity Assessment | The Barratt Impulsiveness Scale (BIS-11) will be used to assess the personality/behavioural construct of impulsiveness including motor (acting without thinking), attentional (an inability to focus attention or concentrate) and non-planning (lack of forethought), in different situations. | Screening visit (clinical interview) | |
Primary | Impulsivity Assessment | The Barratt Impulsiveness Scale (BIS-11) will be used to assess the personality/behavioural construct of impulsiveness including motor (acting without thinking), attentional (an inability to focus attention or concentrate) and non-planning (lack of forethought), in different situations. | 3 months post-intervention | |
Primary | Neuropsychological Evaluation - Memory | The Delayed Matching to Sample (DMS) from Cambridge Neuropsychological Test Automated Battery (CANTAB) will be used to assess both simultaneous visual matching ability and short-term visual recognition memory, for non-verbalisable patterns. | At baseline (pre-intervention) | |
Primary | Neuropsychological Evaluation - Memory | The Delayed Matching to Sample (DMS) from Cambridge Neuropsychological Test Automated Battery (CANTAB) will be used to assess both simultaneous visual matching ability and short-term visual recognition memory, for non-verbalisable patterns. | Immediately post-intervention | |
Primary | Neuropsychological Evaluation - Emotion and Social Cognition | The Emotion Recognition Task (ERT) from CANTAB will measure the ability to identify six basic emotions (sadness, happiness, fear, anger, disgust, and surprise) in facial expressions along a continuum of expression magnitude. | At baseline (pre-intervention) | |
Primary | Neuropsychological Evaluation - Emotion and Social Cognition | The Emotion Recognition Task (ERT) from CANTAB will measure the ability to identify six basic emotions (sadness, happiness, fear, anger, disgust, and surprise) in facial expressions along a continuum of expression magnitude. | Immediately post-intervention | |
Primary | Neuropsychological Evaluation - Executive Function | The performance of the cognitive domain comprising high-level thinking and decision-making will be assessed through CANTAB, namely the Cambridge Gambling Task (CGT, to assess decision-making and risk behaviour outside a learning context), Intra-Extra Dimensional Set Shift (IED, to assess cognitive flexibility), Spatial Working Memory (SWM, to identify working memory strategies and errors) and Stop Signal Task (SST, to measure response inhibition/impulse control). | At baseline (pre-intervention) | |
Primary | Neuropsychological Evaluation - Executive Function | The performance of the cognitive domain comprising high-level thinking and decision-making will be assessed through CANTAB, namely the Cambridge Gambling Task (CGT, to assess decision-making and risk behaviour outside a learning context), Intra-Extra Dimensional Set Shift (IED, to assess cognitive flexibility), Spatial Working Memory (SWM, to identify working memory strategies and errors) and Stop Signal Task (SST, to measure response inhibition/impulse control). | Immediately post-intervention | |
Primary | Alcohol Cue Reactivity - Emotional measures | The reactivity to alcoholic cues will be assessed using the Alcohol Cue Reactivity (ACR) task. The full task includes a total of 80 trials with 40 alcoholic and 40 non-alcoholic images obtained from the Amsterdam Beverage Picture Set. The emotional responses for each image in terms of valence and arousal task, will be registered using the Self-Assessment Manikin (valence: from 1 = "very unpleasant" to 9 ="very pleasant"; arousal: from 1 = "not arousing" to 9 = "highly arousing") during the ACR task. | At baseline (pre-intervention) | |
Primary | Alcohol Cue Reactivity - Emotional measures | The reactivity to alcoholic cues will be assessed using the ACR task. The full task includes a total of 80 trials with 40 alcoholic and 40 non-alcoholic images obtained from the Amsterdam Beverage Picture Set. The emotional responses for each image in terms of valence and arousal task, will be registered using the Self-Assessment Manikin (valence: from 1 = "very unpleasant" to 9 ="very pleasant"; arousal: from 1 = "not arousing" to 9 = "highly arousing") during the ACR task. | Immediately post-intervention. | |
Primary | Memory Inhibition Performance | Memory Inhibition (MI), specifically alcohol-related MI, will be assessed using the Think/No-Think Alcohol (TNTA) task. Percentage of correct responses (for Think, No-Think and Baseline items) in the TNTA task will be computed according to the following formula: ((number of correctly recalled items)/(number of previously learned items))×100. Correct responses correspond to the items learned during the learning phase and correctly recalled during the memory test phase. | At baseline (pre-intervention) | |
Primary | Memory Inhibition Performance | MI, specifically alcohol-related MI, will be assessed using the TNTA task. Percentage of correct responses (for Think, No-Think and Baseline items) in the TNTA task will be computed according to the following formula: ((number of correctly recalled items)/(number of previously learned items))×100. Correct responses correspond to the items learned during the learning phase and correctly recalled during the memory test phase. | Immediately post-intervention. | |
Primary | Ability of Emotional Recognition | Emotional recognition capacity will be assessed through the Emotion Discrimination (ED) task. ED assesses the brain's preconscious and conscious responses to emotional faces. The complete task includes a total of 120 images of human faces (60 men and 60 women), showing the main negative emotions: angry, sadness and fear. | At baseline (pre-intervention) | |
Primary | Ability of Emotional Recognition | Emotional recognition capacity will be assessed through the ED task. ED assesses the brain's preconscious and conscious responses to emotional faces. The complete task includes a total of 120 images of human faces (60 men and 60 women), showing the main negative emotions: angry, sadness and fear. | Immediately post-intervention. | |
Primary | Fecal Microbiota - Species Richness | Faecal samples will be collected from all participants for microbiota a-diversity analysis by 16S rRNA metagenomics (Illumina sequencing). The Chao1 Index will be used as an estimator of nonparametric microbial species richness in each sample. | At baseline (pre-intervention) | |
Primary | Fecal Microbiota - Species Richness | Faecal samples will be collected only from binge drinkers subjected to the intervention for microbiota a-diversity analysis by 16S rRNA metagenomics (Illumina sequencing). The Chao1 Index will be used as an estimator of nonparametric microbial species richness in each sample. | Immediately post-intervention. | |
Primary | Fecal Microbiota - Species Diversity | Faecal samples will be collected from all participants for microbiota a-diversity analysis by 16S rRNA metagenomics (Illumina sequencing). The Shannon Diversity Index (metric combining richness and evenness, with equal weighting given to abundant and rare species) and the Simpson Diversity Index (metric of richness and evenness, in which more weighting is given to abundant species) will be used. | At baseline (pre-intervention) | |
Primary | Fecal Microbiota - Species Diversity | Faecal samples will be collected only from binge drinkers subjected to the intervention for microbiota a-diversity analysis by 16S rRNA metagenomics (Illumina sequencing). The Shannon Diversity Index (metric combining richness and evenness, with equal weighting given to abundant and rare species) and the Simpson Diversity Index (metric of richness and evenness, in which more weighting is given to abundant species) will be used. | Immediately post-intervention. | |
Primary | Fecal Microbiota - Quantification of SCFAs levels | The concentration of short-chain fatty acids (SCFAs) present in each collected faecal sample shall be quantified by High Performance Liquid Chromatography (HPLC). | At baseline (pre-intervention) | |
Primary | Fecal Microbiota - Quantification of SCFAs levels | The concentration of SCFAs present in each collected faecal sample shall be quantified by HPLC. | Immediately post-intervention. | |
Primary | Blood samples - Presence of Inflammatory Markers | Blood samples will be collected from all participants. The presence and abundance of the following cytokines will be analyzed: Tumour Necrosis Factor a (TNF-a) and Interleukins (IL-1ß, IL-6, IL-10). | At baseline (pre-intervention) | |
Primary | Blood samples - Presence of Inflammatory Markers | Blood samples will be collected only from binge drinkers subjected to the intervention. The presence and abundance of the following cytokines will be analyzed: Tumour Necrosis Factor a (TNF-a) and Interleukins (IL-1ß, IL-6, IL-10). | Immediately post-intervention. |
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