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Dopamine and Cognition

Sponsor
Donders Centre for Cognitive Neuroimaging (Other)
Overall Status
Completed
CT.gov ID
NCT05884671
Collaborator
Dr. Hanneke den Ouden, Donders Centre for Cognition, Radboud University (Other), Dr. Rebecca Calcott, Donders Centre for Cognitive Neuroimaging, Radboud University (Other), Prof. Dr. Robbert-Jan Verkes, Radboud University Medical Centre Department of Psychiatry (Other), Floortje Spronkers, Donders Centre for Cognition, Radboud University (Other), Funding: NWO + KNAW (Other)
47
Enrollment
1
Location
2
Arms
9.6
Actual Duration (Months)
4.9
Patients Per Site Per Month

Study Details

Study Description

Brief Summary

Rationale: To unravel the role of dopamine in gating of working memory, motivation and learning.

Objective: The primary objective of this study is to isolate effects of blocking D2 receptor stimulation on gating of working memory, reinforcement learning and reward-based motivation, and their associated physiological changes (measured with fMRI and eye tracking). The secondary objective is to assess the degree to which the effects of D2 receptor action vary as a function of proxy measures of baseline dopamine levels.

Study design: A double-blind placebo controlled within-subject design will be employed, in which young healthy participants are tested twice, once on placebo, and once on a low oral dose (400mg) of the D2 receptor antagonist sulpiride. This design and drug dose is commonly used in our lab without side effects (previously approved CMO protocols 2011/204, 2008/078 & 2016/2646).

Study population: Healthy human participants, 18 - 45 yr old. We will recruit 46 participants.

Intervention: Participants will receive both 400 mg sulpiride and placebo, in separate sessions in a counterbalanced order.

Main study parameters/endpoints: BOLD signal measured with fMRI, and behavioural performance on cognitive tasks.

Nature and extent of the burden and risks associated with participation, benefit and group relatedness: Participants will attend 3 study sessions: A screening session and 2 pharmaco-fMRI sessions (sulpiride and placebo). Participants will complete a baseline battery of tasks and questionnaires, a structural MRI scan, as well as a battery of tasks both in and outside the scanner. On the day preceding each pharmaco-fMRI session, participants will have to adhere to some simple restrictions with respect to medication, alcohol and drug intake. On the day of testing participants will have to refrain from smoking and stimulant-containing drinks. Sulpiride can be administered safely without any relevant risk of serious adverse events and has been approved for clinical use in the Netherlands.

Condition or Disease Intervention/Treatment Phase
  • Drug: Sulpiride 400 MG
  • Drug: Placebo
 N/A

Detailed Description

A more detailed description can be found in the approved research protocol as well as the pre-registrations. The links to the pre-registrations will be made available upon publication.

Study Design

Study Type:
Interventional
Actual Enrollment :
47 participants
Allocation:
Randomized
Intervention Model:
Crossover Assignment
Intervention Model Description:
This is a within-subjects (i.e., crossover), double-blind, randomized placebo-controlled study.This is a within-subjects (i.e., crossover), double-blind, randomized placebo-controlled study.
Masking:
Triple (Participant, Investigator, Outcomes Assessor)
Primary Purpose:
Basic Science
Official Title:
Dopaminergic Mechanisms of Gating Working Memory, Learning and Motivation: a Pharmaco-fMRI Study
Actual Study Start Date :
Sep 23, 2021
Actual Primary Completion Date :
Jul 12, 2022
Actual Study Completion Date :
Jul 12, 2022

Arms and Interventions

Arm Intervention/Treatment
Active Comparator: Sulpiride

All study participants receive both placebo and the active medication (sulpiride 400mg), in a within-subjects , double-blind, randomized design.

Drug: Sulpiride 400 MG
All participants will receive one single dose of 400mg sulpiride. None of the participants will receive repeated doses. In order for the fMRI data acquisition to coincide with the time-window of maximal drug effects represented by a combination of plasma kinetics and physiological effects we will administer the drug 90 minutes prior to fMRI data acquisition.
Other Names:
  • Dogmatil

    		•
    Placebo Comparator: Placebo

    All study participants receive both placebo and the active medication (sulpiride 400mg), in a within-subjects , double-blind, randomized design.

    Drug: Placebo
    All participants will receive placebo during one of the sessions.

    Outcome Measures

    Primary Outcome Measures

    1. Working memory gating task: Reaction time [Measured at intervention day 1, 115 min after the pharmacological intervention took place. Measurements are compared regarding intervention type (drug versus placebo).]

      Reaction time [ms] during selective vs. non-selective input- and output-gating to assess the ability (speed) to selectively input- and output-gate working memory representations at intervention (sulpiride) versus placebo.

    2. Working memory gating task: Reaction time [Measured at intervention day 2, 115 min after the pharmacological intervention took place. Measurements are compared regarding intervention type (drug versus placebo).]

      Reaction time [ms] during selective vs. non-selective input- and output-gating to assess the ability (speed) to selectively input- and output-gate working memory representations at intervention (sulpiride) versus placebo.

    3. Working memory gating task: Accuracy [Measured at intervention day 1, 115 min after the pharmacological intervention took place. Measurements are compared regarding intervention type (drug versus placebo).]

      Accuracy [%] during selective vs. non-selective input- and output-gating to assess the ability (correctness) to selectively input- and output-gate working memory representations at intervention (sulpiride) versus placebo.

    4. Working memory gating task: Accuracy [Measured at intervention day 2, 115 min after the pharmacological intervention took place. Measurements are compared regarding intervention type (drug versus placebo).]

      Accuracy [%] during selective vs. non-selective input- and output-gating to assess the ability (correctness) to selectively input- and output-gate working memory representations at intervention (sulpiride) versus placebo.

    5. Working memory gating task: BOLD-response [Measured at intervention day 1, 115 min after the pharmacological intervention took place. Measurements are compared regarding intervention type (drug versus placebo).]

      BOLD-response to selective vs. global cues, examined for both pre- and retro-cue conditions (i.e., input- and output-gating respectively) to assess the neural response to selective working memory gating at intervention (sulpiride) versus placebo.

    6. Working memory gating task: BOLD-response [Measured at intervention day 2, 115 min after the pharmacological intervention took place. Measurements are compared regarding intervention type (drug versus placebo).]

      BOLD-response to selective vs. global cues, examined for both pre- and retro-cue conditions (i.e., input- and output-gating respectively) to assess the neural response to selective working memory gating at intervention (sulpiride) versus placebo.

    7. Simon task: Accuracy [Measured at intervention day 1, 250 min after the pharmacological intervention took place. Measurements are compared regarding intervention type (drug versus placebo).]

      Accuracy [%] during high and low average reward rate congruent and incongruent trials to assess cognitive effort investment after intervention versus placebo.

    8. Simon task: Accuracy [Measured at intervention day 2, 250 min after the pharmacological intervention took place. Measurements are compared regarding intervention type (drug versus placebo).]

      Accuracy [%] during high and low average reward rate congruent and incongruent trials to assess cognitive effort investment after intervention versus placebo.

    9. Simon task: Reaction time [Measured at intervention day 1, 250 min after the pharmacological intervention took place. Measurements are compared regarding intervention type (drug versus placebo).]

      Reaction time [ms] during high and low average reward rate congruent and incongruent trials to assess cognitive effort investment after intervention versus placebo

    10. Simon task: Reaction time [Measured at intervention day 2, 250 min after the pharmacological intervention took place. Measurements are compared regarding intervention type (drug versus placebo).]

      Reaction time [ms] during high and low average reward rate congruent and incongruent trials to assess cognitive effort investment after intervention versus placebo

    11. Perceptual decision-making task: Accuracy [Measured at intervention day 1, 215 min after the pharmacological intervention took place. Measurements are compared regarding intervention type (drug versus placebo).]

      Accuracy [%] as a function of average reward rate to assess cognitive effort investment after intervention versus placebo.

    12. Perceptual decision-making task: Accuracy [Measured at intervention day 2, 215 min after the pharmacological intervention took place. Measurements are compared regarding intervention type (drug versus placebo).]

      Accuracy [%] as a function of average reward rate to assess cognitive effort investment after intervention versus placebo.

    13. Perceptual decision-making task: Reaction time [Measured at intervention day 1, 215 min after the pharmacological intervention took place. Measurements are compared regarding intervention type (drug versus placebo).]

      Reaction time [ms] as a function of average reward rate to assess cognitive effort investment after intervention versus placebo.

    14. Perceptual decision-making task: Reaction time [Measured at intervention day 2, 215 min after the pharmacological intervention took place. Measurements are compared regarding intervention type (drug versus placebo).]

      Reaction time [ms] as a function of average reward rate to assess cognitive effort investment after intervention versus placebo.

    Secondary Outcome Measures

    1. Eye-blink rate [Measured at baseline during intake session]

      Number of spontaneous eye blinks per minute, as a clinically relevant biomarker of striatal dopamine function

    2. Operation Span test [Measured at baseline during intake session]

      Number of letters remembered while performing math problems, as a parameter for working memory capacity

    3. Digit Span test [Measured at baseline during intake session]

      Accuracy score [nr of correct responses] on forward span and backward span, as a parameter for working memory capacity

    4. Digit Span test [Measured during intervention day 1 (sessions at least 14 days apart), 290 min after the pharmacological intervention took place]

      Accuracy score [nr of correct responses] on forward span and backward span, as a parameter for working memory capacity

    5. Digit Span test [Measured during intervention day 2 (sessions at least 14 days apart), 290 min after the pharmacological intervention took place]

      Accuracy score [nr of correct responses] on forward span and backward span, as a parameter for working memory capacity

    6. Beck Depression Inventory [Baseline measure via online questionnaire in between first and second intervention session (these take place at least 14 days apart)]

      Average score as indicator of depressive symptoms

    7. Barratt Impulsiveness Scale [Baseline measure via online questionnaire in between first and second intervention session (these take place at least 14 days apart)]

      Average score as indicator of impulsivity (personality trait)

    8. Behavioural Inhibition Scale/Behavioural Activation Scale [Baseline measure via online questionnaire in between first and second intervention session (these take place at least 14 days apart)]

      Average score as indicator of behavioural activation and inhibition

    9. State and Trait Anxiety Inventory [Baseline measure via online questionnaire in between first and second intervention session (these take place at least 14 days apart)]

      Average score as indicator of state and trait anxiety

    10. Utrechtse Burnout Schaal/Maslach Burnout Inventory [Baseline measure via online questionnaire in between first and second intervention session (these take place at least 14 days apart)]

      Average score as indicator of burn out

    11. Covid-19 Stress Scales [Baseline measure via online questionnaire in between first and second intervention session (these take place at least 14 days apart)]

      Average score as indicator of COVID-related stress and anxiety

    Other Outcome Measures

    1. Diastolic blood pressure [Measured at baseline on intervention day 1 (before pharmacological intervention took place)]

      Unit of measurement: mmHG

    2. Diastolic blood pressure [Measured at baseline on intervention day 2 (before pharmacological intervention took place)]

      Unit of measurement: mmHG

    3. Diastolic blood pressure [Measured 90 min post drug/placebo intake on intervention day 1]

      Unit of measurement: mmHG

    4. Diastolic blood pressure [Measured 90 min post drug/placebo intake on intervention day 2]

      Unit of measurement: mmHG

    5. Diastolic blood pressure [Measured 300 min post drug/placebo intake on intervention day 1]

      Unit of measurement: mmHG

    6. Diastolic blood pressure [Measured 300 min post drug/placebo intake on intervention day 2]

      Unit of measurement: mmHG

    7. Systolic blood pressure [Measured at baseline on intervention day 1 (before pharmacological intervention took place)]

      Unit of measurement: mmHG

    8. Systolic blood pressure [Measured at baseline on intervention day 2 (before pharmacological intervention took place)]

      Unit of measurement: mmHG

    9. Systolic blood pressure [Measured 90 min post drug/placebo intake on intervention day 1]

      Unit of measurement: mmHG

    10. Systolic blood pressure [Measured 90 min post drug/placebo intake on intervention day 2]

      Unit of measurement: mmHG

    11. Systolic blood pressure [Measured 300 min post drug/placebo intake on intervention day 1]

      Unit of measurement: mmHG

    12. Systolic blood pressure [Measured 300 min post drug/placebo intake on intervention day 2]

      Unit of measurement: mmHG

    13. Heart rate [Measured at baseline on intervention day 1 (before pharmacological intervention took place)]

      Unit of measurement: beats per minute (bpm)

    14. Heart rate [Measured at baseline on intervention day 2 (before pharmacological intervention took place)]

      Unit of measurement: beats per minute (bpm)

    15. Heart rate [Measured 90 min post drug/placebo intake on intervention day 1]

      Unit of measurement: beats per minute (bpm)

    16. Heart rate [Measured 90 min post drug/placebo intake on intervention day 2]

      Unit of measurement: beats per minute (bpm)

    17. Heart rate [Measured 300 min post drug/placebo intake on intervention day 1]

      Unit of measurement: beats per minute (bpm)

    18. Heart rate [Measured 300 min post drug/placebo intake on intervention day 2]

      Unit of measurement: beats per minute (bpm)

    19. Body temperature [Measured at baseline on intervention day 1 (before pharmacological intervention took place)]

      Measured in degree Celsius by an in-ear thermometer

    20. Body temperature [Measured at baseline on intervention day 2 (before pharmacological intervention took place)]

      Measured in degree Celsius by an in-ear thermometer

    21. Body temperature [Measured 90 min post drug/placebo intake on intervention day 1]

      Measured in degree Celsius by an in-ear thermometer

    22. Body temperature [Measured 90 min post drug/placebo intake on intervention day 2]

      Measured in degree Celsius by an in-ear thermometer

    23. Body temperature [Measured 300 min post drug/placebo intake on intervention day 1]

      Measured in degree Celsius by an in-ear thermometer

    24. Body temperature [Measured 300 min post drug/placebo intake on intervention day 2]

      Measured in degree Celsius by an in-ear thermometer

    25. Respiration movements [Measured during the MRI scan (115 min post drug/placebo) on intervention day 1. The pharmacological intervention sessions take place at least 14 days apart)]

      Voltage change over time measured by a respiration belt around participants' abdomen during MRI scanning

    26. Respiration movements [Measured during the MRI scan (115 min post drug/placebo) on intervention day 2. The pharmacological intervention sessions take place at least 14 days apart)]

      Voltage change over time measured by a respiration belt around participants' abdomen during MRI scanning

    27. Visual Analogue Scale (VAS) [Measured at baseline on intervention day 1 (before pharmacological intervention took place)]

      Measured with 16 mood rating items measured on a continuous scale from 1 to 10 by self-report

    28. Visual Analogue Scale (VAS) [Measured at baseline on intervention day 2 (before pharmacological intervention took place)]

      Measured with 16 mood rating items measured on a continuous scale from 1 to 10 by self-report

    29. Visual Analogue Scale (VAS) [Measured 90 min post drug/placebo intake on intervention day 1]

      Measured with 16 mood rating items measured on a continuous scale from 1 to 10 by self-report

    30. Visual Analogue Scale (VAS) [Measured 90 min post drug/placebo intake on intervention day 2]

      Measured with 16 mood rating items measured on a continuous scale from 1 to 10 by self-report

    31. Visual Analogue Scale (VAS) [Measured 300 min post drug/placebo intake on intervention day 1]

      Measured with 16 mood rating items measured on a continuous scale from 1 to 10 by self-report

    32. Visual Analogue Scale (VAS) [Measured 300 min post drug/placebo intake on intervention day 2]

      Measured with 16 mood rating items measured on a continuous scale from 1 to 10 by self-report

    33. Positive and Negative Affect Scale (PANAS) [Measured at baseline on intervention day 1 (before pharmacological intervention took place)]

      Measured with 20 statements regarding feelings and emotions measured on a 5-point Likert scale by self-report

    34. Positive and Negative Affect Scale (PANAS) [Measured at baseline on intervention day 2 (before pharmacological intervention took place)]

      Measured with 20 statements regarding feelings and emotions measured on a 5-point Likert scale by self-report

    35. Positive and Negative Affect Scale (PANAS) [Measured 90 min post drug/placebo intake on intervention day 1]

      Measured with 20 statements regarding feelings and emotions measured on a 5-point Likert scale by self-report

    36. Positive and Negative Affect Scale (PANAS) [Measured 90 min post drug/placebo intake on intervention day 2]

      Measured with 20 statements regarding feelings and emotions measured on a 5-point Likert scale by self-report

    37. Positive and Negative Affect Scale (PANAS) [Measured 300 min post drug/placebo intake on intervention day 1]

      Measured with 20 statements regarding feelings and emotions measured on a 5-point Likert scale by self-report

    38. Positive and Negative Affect Scale (PANAS) [Measured 300 min post drug/placebo intake on intervention day 2]

      Measured with 20 statements regarding feelings and emotions measured on a 5-point Likert scale by self-report

    39. Menstrual cycle stage (for female participants) [Measured within the first 10 min of the intervention day 1 (i.e., 10 min pre drug/placebo)]

      Day of onset of last menstrual bleeding measured by self-report

    40. Menstrual cycle stage (for female participants) [Measured within the first 10 min of the intervention day 2 (i.e., 10 min pre drug/placebo)]

      Day of onset of last menstrual bleeding measured by self-report

    Eligibility Criteria

    Criteria

    Ages Eligible for Study:
    18 Years to 45 Years
    Sexes Eligible for Study:
    All
    Accepts Healthy Volunteers:
    Yes
    Inclusion Criteria:

    • Healthy volunteers between 18 and 45 years of age

    • Predominant right-handedness

    Exclusion Criteria:

    • Presence of prolactin-dependent tumors (e.g., pituitary prolactinoma or breast cancer)

    • (History of) autonomic failure (e.g., vasovagal reflex syncope).

    • (History of) clinically significant hepatic, cardiac, obstructive respiratory, renal, cerebrovascular, cardiovascular, metabolic, ocular or pulmonary disease/disorders

    • (History of) epilepsy in adulthood (i.e. no insult after 18 years of age, no current medication for epilepsy and no insult in the last five years)

    • Diagnosis (or history of) endocrine treatment

    • Diagnosis (or history of) neuroendocrine treatment (e.g., phechromocytoma, hyperthyroidism, Cushing's syndrome)

    • (History of) melanoma

    • Hypersensitivity to sulpiride

    • One first degree or two or more second degree family members with a history of sudden death or ventricular arrhythmia

    • Abnormal QT interval (assessed via ECG)

    • Uncontrolled hypertension, defined as diastolic blood pressure at rest > 95 mmHg or systolic blood pressure at rest > 180 mmHg

    • Hypotension, defined as diastolic blood pressure < 50 mm Hg or systolic < 95 mm Hg

    • or resting pulse rate < 45 beats/min

    • Diabetes

    • History of prescribed medication within the last month prior to the start of the study.

    • History of 'over the counter' medication within the last two months (with exception of occasional use of paracetamol, acetylsalicylic acid, and ibuprofen).

    • Possible pregnancy or breastfeeding

    • No appropriate contraception

    • Undiagnosed skin lesions

    • Lactose intolerance

    • Glaucoma or increased risk for glaucoma

    • Possible pregnancy or breastfeeding

    • Metal objects in or around the body (braces, pacemaker, metal fragments, hearing devices)

    • Claustrophobia

    • Diagnosis (or history of) psychiatric treatment (e.g., severe depression, anorexia nervosa, severe mood disorders, mania, schizophrenia or borderline personality disorder)

    • Diagnosis (or history of) neurological treatment

    • (History of) drug dependence (opiate, LSD, (meth)amphetamine, cocaine, solvents, or barbiturate) or alcohol dependence

    • Suicidality

    • Use of MAO inhibitor, anaesthetic, antidepressant or antipsychotic drugs within the week prior to the start of the study.

    • Average use of psychotropic medication or recreational drugs weekly or more.

    • Cannabis use within 2 weeks prior to the start of the study, and periods of more than 3 months using weekly or more in the last 6 months

    • Use of psychotropic medication, or of recreational drugs over a period of 72 hours

    • prior to the test sessions, and use of alcohol within the last 24 hours before each measurement.

    • Average use of more than 3 alcohol beverages daily.

    • Average use of psychotropic medication or recreational drugs weekly or more.

    • Habitual smoking, i.e., more than a pack of cigarettes per week and/or a self-reported inability or unease to cease smoking for 24 hours to testing.

    • Regular use of corticosteroids.

    • Abnormal hearing or (uncorrected) vision.

    • First degree family member with schizophrenia or bipolar disorder

    • Irregular sleep/wake rhythm (e.g., regular nightshifts or cross timezone travel).

    • Left handedness (because lateralisations of brain activation may differ from right-handed people).

    Contacts and Locations

    Locations

    Site City State Country Postal Code
    1 Donders Centre for Cognition, Radboud University Nijmegen Gelderland Netherlands

    Sponsors and Collaborators

    • Donders Centre for Cognitive Neuroimaging
    • Dr. Hanneke den Ouden, Donders Centre for Cognition, Radboud University
    • Dr. Rebecca Calcott, Donders Centre for Cognitive Neuroimaging, Radboud University
    • Prof. Dr. Robbert-Jan Verkes, Radboud University Medical Centre Department of Psychiatry
    • Floortje Spronkers, Donders Centre for Cognition, Radboud University
    • Funding: NWO + KNAW

    Investigators

    None specified.

    Study Documents (Full-Text)

    None provided.

    More Information

    Publications

    None provided.
    Responsible Party:
    Roshan Cools, Prof. Dr., Donders Centre for Cognitive Neuroimaging
    ClinicalTrials.gov Identifier:
    NCT05884671
    Other Study ID Numbers:
    • 3017048.09
    First Posted:
    Jun 1, 2023
    Last Update Posted:
    Jun 1, 2023
    Last Verified:
    May 1, 2023
    Individual Participant Data (IPD) Sharing Statement:
    Yes
    Plan to Share IPD:
    Yes
    Studies a U.S. FDA-regulated Drug Product:
    No
    Studies a U.S. FDA-regulated Device Product:
    No
    Additional relevant MeSH terms:
    Sulpiride

    Study Results

    No Results Posted as of Jun 1, 2023