Impulsivity Clinical Trial
Official title:
Determining the Most Effective Training Region in ADHD Neurofeedback (NF) Therapy - Functional Near-infrared Spectroscopy NF of the Dorsolateral Prefrontal Cortex (DLPFC) vs. Inferior Frontal Gyrus (IFG) in Healthy Participants
Verified date | September 2022 |
Source | University Hospital Tuebingen |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
The aim of the following study is to investigate which is the best region of interest (ROI) for a functional near-infrared spectroscopy (fNIRS)-based neurofeedback (NF) training for highly-impulsive individuals (and consequently also patients with attention-deficit/hyperactivity disorder, ADHD): the dorsolateral prefrontal cortex (DLPFC) or the inferior frontal gyrus (IFG). Generally, NF trainings aim to improve the neurophysiological as well as cognitive-behavioral deficits observed in many neuropsychiatric disorders and were shown to constitute an effective complementary treatment option for patients with ADHD. Some previous studies used the DLPFC as a ROI for NF training, while others focused on the IFG as the main target region. However, so far, no study has directly compared the effectiveness of NF trainings targeting the DLPFC vs. IFG using the same protocol or the specificity of regulation efforts between these two areas using fNIRS. Therefore, the aim of the current study is to compare the effectiveness of fNIRS-NF using the DLPFC as a ROI with fNIRS-NF using the IFG as a ROI in a randomized controlled study design with highly-impulsive, healthy participants. Furthermore, the investigators aim to test the effect of fNIRS-NF training in the context of stress. Previous studies reported that there is a strong connection between ADHD and stress. However, the effect of fNIRS-NF training for the adaptation to stressful situations is uncertain. To this end, the investigators will assess the brain activity of participants before and after an fNIRS-NF training period during performance of a Go/NoGo task, an n-back task and The Trier Social Stress Test (TSST). It is hypothesized that both trainings will be successful in reducing impulsive behavior; however, in the pre/post testing, specific effects of fNIRS-based NF of the DLPFC are expected on working memory function and of fNIRS-based NF of the IFG on inhibitory control (Go/NoGo task). Correlations between both functions and impulsive symptoms will give an indication which training ROI may be more promising for the treatment of (specific subgroups of) ADHD. Correlations between regulation of different training ROIs will indicate the specificity of feedback regulation of circumscribed cortical areas.
Status | Completed |
Enrollment | 57 |
Est. completion date | July 12, 2021 |
Est. primary completion date | July 12, 2021 |
Accepts healthy volunteers | Accepts Healthy Volunteers |
Gender | All |
Age group | 18 Years to 50 Years |
Eligibility | Inclusion Criteria: - Informed written consent - ASRS score in subscale (Items 10 bis 18) "hyperactivity/impulsivity" >=17 - No additional serious physical, neurological or mental disorder. Exclusion Criteria: - ASRS score "hyperactivity/impulsivity"<17 - Self-reported diagnosis of one or more of the following - Serious physical or chronic illness such as lung disease, heart disease, diabetes (E10-E14 according to ICD-10), hypertension (I10.x according to ICD-10), and rheumatic diseases - Neurological disorders including stroke, multiple sclerosis and epilepsy - History of moderate or severe craniocerebral injury (GCS 3-12) / second or third degree craniocerebral injury with period of unconsciousness exceeding 30 minutes - Indicated psychiatric disorders including bipolar disorder, psychosis, obsessive-compulsive disorder, chronic tics, Tourette syndrome, and suicidal behavior; in addition to self-report, these will be screened for by using the SCID (Structured Clinical Interview for DSM-IV) screening questions - Prior participation in a NF training. - Other psychotherapeutic treatment or any kind of attention training, also in the course of an ergotherapeutic treatment, while participating in the study |
Country | Name | City | State |
---|---|---|---|
Germany | Department of Psychiatry and Psychotherapy, University Hospital Tuebingen | Tuebingen | Baden-Württemberg |
Lead Sponsor | Collaborator |
---|---|
University Hospital Tuebingen | Japan society for the promotion of science, Nakatani foundation and Japan foundation for pediatric research |
Germany,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Change of n-back reaction times after neurofeedback training compared to baseline | Reaction times (mean and standard deviation) obtained during a block-design n-back (working memory) task (0-back, 1-back, and 3-back condition) | Change from baseline to immediately after the 8th neurofeedback training session | |
Primary | Change of n-back error rates after neurofeedback training compared to baseline | Error rates (hits, misses, false alarms) obtained during a block-design n-back (working memory) task (0-back, 1-back, and 3-back condition) | Change from baseline to immediately after the 8th neurofeedback training session | |
Primary | Change of Go/NoGo reaction times after neurofeedback training compared to baseline | Reaction times (mean and standard deviation) obtained during a Go/NoGo task (Go and NoGo blocks) | Change from baseline to immediately after the 8th neurofeedback training session | |
Primary | Change of Go/NoGo error rates after neurofeedback training compared to baseline | Error rates (hits, misses, false alarms) obtained during a Go/NoGo task (Go and NoGo blocks) | Change from baseline to immediately after the 8th neurofeedback training session | |
Primary | Change of N-back brain activation data (fNIRS) after neurofeedback training compared to baseline | Oxygenation changes (fNIRS data) during the 3-back, 1-back, and 0-back condition of the n-back task in pre-defined regions of interest (DLPFC [Brodman area/BA9 and 46], IFG, temporal cortex) | Change from baseline to immediately after the 8th neurofeedback training session | |
Primary | Change of Go/NoGo brain activation data (fNIRS) after neurofeedback training compared to baseline | Oxygenation changes (fNIRS data) during the Go and NoGo condition of the go-nogo task in pre-defined regions of interest (DLPFC [BA9 and 46], IFG, temporal cortex) | Change from baseline to immediately after the 8th neurofeedback training session | |
Primary | Neurofeedback learning success based on the online feedback signal (number of correct trials) | Increase in the number of successful neurofeedback training trials from session 1 to session 8 (for feedback and transfer trials, up- and down-regulation) | Change from neurofeedback session 1 to session 8 | |
Primary | Neurofeedback learning success based on the online feedback signal (percentage of correct time-points) | Increase in the percentage of time-points (in the second half of all neurofeedback regulation trials) where the fNIRS feedback signal was regulated in the correct direction from session 1 to session 8 (for feedback and transfer trials, up- and down-regulation) | Change from neurofeedback session 1 to session 8 | |
Primary | Neurofeedback learning success based on an offline analysis of successful up- vs. down-regulation | Increase in the differentiation between up- and down-regulation of the fNIRS signal from session 1 to session 8 (for feedback, transfer and all trials; offline analysis) | Change from neurofeedback session 1 to session 8 | |
Secondary | Correlation of internal-external control beliefs with neurofeedback learning outcome | Correlation of internal control beliefs (IE-4 questionnaire: min value 2, max value 10) and external control beliefs (IE-4 questionnaire: min value 2, max value 10) with neurofeedback learning outcome (see Outcomes 7-9). Higher values on internal and external control subscale mean higher expression for external and internal beliefs.
Kovaleva, A., Beierlein, C., Kemper, C. J., & Rammstedt, B. (2012). Eine Kurzskala zur Messung von Kontrollüberzeugung: Die Skala Internale-Externale-Kontrollüberzeugung-4 (IE-4). |
Baseline/pre-intervention | |
Secondary | Correlation of trait impulsivity with neurofeedback learning outcome | Correlation of trait-impulsivity subscale (min value 0, max value 19) and venturesomeness subscale (min value 0 max value 16; both measured with I7 questionnaire) with neurofeedback learning outcome (see Outcomes 7-9). Higher values on impulsivity subscale and venturesomeness subscale mean higher expression for impulsivity and venturesomeness.
Eysenck, S. B., Daum, I., Schugens, M. M., & Diehl, J. M. (1990). A cross-cultural study of impulsiveness, venturesomeness and empathy: Germany and England. Zeitschrift für Differentielle und diagnostische Psychologie. |
Baseline/pre-intervention | |
Secondary | Correlation of general self-efficacy with neurofeedback learning outcome | Correlation of general self-efficacy measured with the SWE (min value 10, max value 40) questionnaire with neurofeedback learning outcome (see Outcomes 7-9). Higher values in SWE questionnaire mean higher expression for general sel-efficacy.
Hinz, A., Schumacher, J., Albani, C., Schmid, G., & Brähler, E. (2006). Bevölkerungsrepräsentative Normierung der Skala zur allgemeinen Selbstwirksamkeitserwartung. Diagnostica, 52(1), 26-32. |
Baseline/pre-intervention | |
Secondary | Correlation of trait anxiety with neurofeedback learning outcome | Correlation of trait anxiety (measured with the STAI trait questionnaire [min value 20, max value 80] with neurofeedback learning outcome (see Outcomes 7-9). Higher values in STAI-trait questionnaire mean higher expression for trait-anxiety.
Laux, L. (1981). Das State-Trait-Angstinventar (STAI): Theoretische Grundlagen und Handanweisung. |
Baseline/pre-intervention |
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