Depression, Anxiety Clinical Trial
Official title:
Neurofeedback Training to Improve Prefrontal Functioning in Older Adults With Subclinical Depression and Anxiety: a Randomised Control Trial
Symptoms of depression and anxiety are common in older adults and are associated with poor outcomes and the risk of dementia. The prefrontal cortex (PFC) is crucial for emotion regulation. Poor PFC function may underlie subclinical depression and anxiety symptoms in older people, which could progress to clinical conditions. Neurofeedback training based on electroencephalography (EEG) or functional near-infrared spectroscopy (fNIRS) teaches individuals to self-regulate different aspects of brain activity and induce neurocognitive improvements. This proposed project will examine whether prefrontal EEG and fNIRS neurofeedback training programmes can enhance the mood and cognition of older adults with subclinical depression and anxiety.
Status | Recruiting |
Enrollment | 90 |
Est. completion date | October 31, 2024 |
Est. primary completion date | October 31, 2024 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 60 Years to 79 Years |
Eligibility | Inclusion Criteria: - (i) age of 60-79 years; - (ii) right-handedness as assessed using the short form of the Edinburgh Handedness Inventory (Veale, 2014); - (iii) a moderate or higher score on at least one of the depression and anxiety subscales (but not necessarily both) of the Depression Anxiety Stress Scale-21 (DASS-21), which has been shown to yield reliable and valid scores; - (iv) no history of neurological or psychiatric disorder; - (v) no history of traumatic brain injury requiring hospitalisation; - (vi) not currently using psychotropic medication; - (vii) ability to read Traditional Chinese text; - (viii) normal or corrected-to-normal vision; and - (ix) a score of at least 19 on the Hong Kong Montreal Cognitive Assessment Exclusion Criteria: - does not fulfill any of the above criteria |
Country | Name | City | State |
---|---|---|---|
Hong Kong | Faculty of Health and Social Sciences OF The Hong Kong Polytechnic University | Hong Kong |
Lead Sponsor | Collaborator |
---|---|
The Hong Kong Polytechnic University |
Hong Kong,
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* Note: There are 62 references in all — Click here to view all references
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Mood symptoms (post) | Change in the HADS depression score (The Hospital Anxiety and Depression Scale (HADS) depression score has a minimum value of 0 and a maximum value of 21. Higher scores indicate a worse outcome. A score of 0-7 indicates normal, 8-10 indicates mild depression, 11-14 indicates borderline depression, and 15-21 indicates depression.) | Within 1 week before the first training session, and within 1 week after the last training session | |
Primary | Mood symptoms (follow-up) | Change in the HADS depression score at follow up (The Hospital Anxiety and Depression Scale (HADS) depression score has a minimum value of 0 and a maximum value of 21. Higher scores indicate a worse outcome. A score of 0-7 indicates normal, 8-10 indicates mild depression, 11-14 indicates borderline depression, and 15-21 indicates depression.) | Within 1 week before the first training session, and within 1 month after the last training session | |
Primary | Anxiety symptoms (post) | Change in the HADS anxiety score (The Hospital Anxiety and Depression Scale (HADS) anxiety score has a minimum value of 0 and a maximum value of 21. Higher scores indicate a worse outcome. A score of 0-7 indicates normal, 8-10 indicates mild anxiety, 11-14 indicates borderline anxiety, and 15-21 indicates anxiety.) | Within 1 week before the first training session, and within 1 week after the last training session | |
Primary | Anxiety symptoms (follow-up) | Change in the HADS anxiety score at follow-up (The Hospital Anxiety and Depression Scale (HADS) anxiety score has a minimum value of 0 and a maximum value of 21. Higher scores indicate a worse outcome. A score of 0-7 indicates normal, 8-10 indicates mild anxiety, 11-14 indicates borderline anxiety, and 15-21 indicates anxiety.) | Within 1 week before the first training session, and within 1 month after the last training session | |
Secondary | Stroop (post; RT) | Change in Stroop mean reaction time | Within 1 week before the first training session, and within 1 week after the last training session | |
Secondary | Stroop (follow-up; RT) | Change in Stroop mean reaction time at follow-up | Within 1 week before the first training session, and within 1 month after the last training session | |
Secondary | Stroop (post; accuracy) | Change in Stroop accuracy | Within 1 week before the first training session, and within 1 week after the last training session | |
Secondary | Stroop (follow-up; accuracy) | Change in Stroop accuracy at follow-up | Within 1 week before the first training session, and within 1 month after the last training session | |
Secondary | Stroop (post; fNIRS) | Change in mean change in oxyhemoglobin concentration measured by fNIRS | Within 1 week before the first training session, and within 1 week after the last training session | |
Secondary | Stroop (follow-up; fNIRS) | Change in mean change in oxyhemoglobin concentration measured by fNIRS at follow-up | Within 1 week before the first training session, and within 1 month after the last training session | |
Secondary | Stroop (post; EEG) | Change in stimulus-locked N450 amplitude measured by EEG | Within 1 week before the first training session, and within 1 week after the last training session | |
Secondary | Stroop (follow-up; EEG) | Change in stimulus-locked N450 amplitude measured by EEG at follow-up | Within 1 week before the first training session, and within 1 month after the last training session | |
Secondary | n-back (post; RT) | Change in n-back mean reaction time | Within 1 week before the first training session, and within 1 week after the last training session | |
Secondary | n-back (follow-up; RT) | Change in n-back mean reaction time at follow-up | Within 1 week before the first training session, and within 1 month after the last training session | |
Secondary | n-back (post; accuracy) | Change in n-back accuracy | Within 1 week before the first training session, and within 1 week after the last training session | |
Secondary | n-back (follow-up; accuracy) | Change in n-back accuracy at follow-up | Within 1 week before the first training session, and within 1 month after the last training session | |
Secondary | n-back (post; fNIRS) | Change in mean change in oxyhemoglobin concentration measured by fNIRS | Within 1 week before the first training session, and within 1 week after the last training session | |
Secondary | n-back (follow-up; fNIRS) | Change in mean change in oxyhemoglobin concentration measured by fNIRS at follow-up | Within 1 week before the first training session, and within 1 month after the last training session | |
Secondary | n-back (post; EEG) | Change in stimulus-locked P300 amplitude measured by EEG at follow-up | Within 1 week before the first training session, and within 1 week after the last training session | |
Secondary | n-back (follow-up; EEG) | Change in stimulus-locked P300 amplitude measured by EEG at follow-up | Within 1 week before the first training session, and within 1 month after the last training session |
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