Major Depressive Disorder Clinical Trial
Official title:
New Form of Brain Stimulation Targeting Dorsomedial Prefrontal Cortex in Treating Refractory Depression and the Predictive Biomarkers of Antidepressant Efficacy
Major depressive disorder (MDD) is a common and troublesome disorder, with high risk of physical and psychiatric comorbidity. At least one-third of patients could not achieve a response after several antidepressant trials, so-called treatment-refractory depression (TRD). The high-frequency repetitive transcranial magnetic stimulation (rTMS) or intermittent theta-burst stimulation (iTBS) at left-sided dorsolateral prefrontal cortex (DLPFC) have a response rate of 40-60%. Obviously, not all TRD patients achieve the remitted state after treatment with antidepressants or DLPFC-rTMS, which may result from the heterogeneity of MDD. More and more evidence, such as brain lesion studies, deep brain stimulation, open-labeled rTMS case series, and neuroimaging studies, suggests that dorsomedial prefrontal cortex (DMPFC) might play a more central role in the pathophysiology of major depression. The DMPFC demonstrated as a "dorsal nexus" phenomenon in depression, which means a unique brain region where cortical networks for affect regulation, default mode control and cognitive control coverage in depressed subjects but not in healthy persons. In addition, another meta-analysis of resting-state functional MRI (fMRI) demonstrated the abnormal functional connectivity from DMPFC. These abnormalities of networks were highly associated with several depressive symptoms such as anhedonia, emotional regulation, somatic markers, rumination, self-reflection, poor attention and poor decision-making. However, only a handful of studies investigated the brain stimulation targeting DMPFC and the further changes in brain functional connectivity. The clinical efficacy and the fMRI changes of prolonged intermittent theta-burst stimulation (piTBS) and 20Hz- rTMS targeting bilateral DMPFC were investigated, and the predictive value of baseline networks by fMRI for antidepressant responses was also assessed to find a reliable approach to gauge treatment response prospectively.
| Status | Recruiting |
| Enrollment | 75 |
| Est. completion date | December 31, 2025 |
| Est. primary completion date | September 30, 2025 |
| Accepts healthy volunteers | No |
| Gender | All |
| Age group | 21 Years to 70 Years |
| Eligibility | Inclusion Criteria: 1. Diagnosed with a recurrent major depressive disorder based on Diagnostic and Statistical Manual of Mental Disorders, Fourth Edition (DSM-IV) criteria. Diagnoses were established after taking a thorough medical history and conducting a semistructured interview by administering the Mini International Neuropsychiatric Interview (MINI); 2. Recruited participants had to have a Clinical Global Impression - Severity score of at least four and a total score of at least 18 on the 17-items Hamilton Depression Rating Scale (HDRS-17); 3. Patients were qualified if they failed to respond to at least one adequate antidepressant treatment in their current episode (for example, failed to achieve 50% improvement of depression to an equivalent daily dose of 10 to 20 mg of escitalopram for at least eight weeks); 4. Stabilized treatment: keeping current antidepressant drug treatment, including the dose at least for four weeks before this trial and during the trial period; keep the stabilized psychotherapy at least for three months and no anticipated adjustment of types of psychotherapy and the frequency. Exclusion Criteria: 1. Patients with Bipolar I and II disorder, schizophrenia, organic brain syndromes, or other major physical illnesses; 2. Patients who had received or will receive brain surgery or receive brain metal implantation (for example, neurostimulator) or received cardiac pacemakers; 3. Patients who had strong suicidal ideation within one week ( 3 points for third item of HDRS-suicidality) 4. Patients who had abnormal finding in the brain ( for example, brain tumor or arteriovenous malformation) or neurological disease ( for example, history of meningitis, encephalitis, epilepsy, stroke or neurodegenerative disease) 5. Pregnancy; 6. Patients who have metal implantation in the body, including cochlear implant, prosthetic heart valve, neurostimulator, clips.. etc 7. Patients who also failed to respond after receiving one completed course of electroconvulsive therapy (ECT) treatment or left dorsolateral prefrontal brain stimulation (adequate dose and adequate duration of ECT or DLPFC-rTMS and had followed up to monitor the efficacy at least for three months) 8. Claustrophobia for MRI screening; 9. Those who cannot follow the protocols, and did not sign informed consent proved by the institutional review board (IRB) |
| Country | Name | City | State |
|---|---|---|---|
| Taiwan | Taipei Veterans General Hospital, Taiwan | Taipei |
| Lead Sponsor | Collaborator |
|---|---|
| Taipei Veterans General Hospital, Taiwan |
Taiwan,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Change in 17-item Hamilton Depression Rating Scale | the altered 17-item Hamilton Depression Rating Scale (range, 0 to 52, with higher scores indicating more depression) | Time Frame: Baseline, Week 1, Week 2, Week 3 (one week after brain stimulation), Week 6, Week 14(three-month after brain stimulation) | |
| Primary | Change in anxiosomatic cluster symptoms derived 17-item Hamilton Depression Rating Scale | the altered anxiosomatic cluster symptoms (range, 0 to 26, with higher scores indicating more severe anxiosomatic symptoms).The anxiosomatic cluster symptoms comprised nine items derived from HDRS-17: early insomnia, middle insomnia, slowness or retardation, psychic anxiety, autonomic anxiety, gastrointestinal symptoms, somatic symptoms, genital symptoms, and hypochondriasis. | Time Frame: Baseline, Week 1, Week 2, Week 3 (one week after brain stimulation), Week 6, Week 14(three-month after brain stimulation) | |
| Secondary | Response rate after 2-week treatment at the end of the trial, one month and three months after. | Improvement = 50 % of 17-item Hamilton Depression Rating Scale (range, 0 to 52, with higher scores indicating more depression) | Time Frame: Week 2, Week 6(one month after brain stimulation), Week 14(three-month after brain stimulation) | |
| Secondary | Remission rate after 2-week treatment at the end of the trial, one month and three months after. | 17-item Hamilton Depression Rating Scale =7 (range, 0 to 52, with higher scores indicating more depression) | Time Frame: Week 2, Week 6(one month after brain stimulation), Week 14(three-month after brain stimulation) | |
| Secondary | Changes in Clinical Global Index | Clinical Global Index, range from 1 to 7 with higher scores indicating worse clinical severity of illness. | Time Frame: Baseline, Week 1, Week 2, Week 3 (one week after brain stimulation), Week 6, Week 14(three-month after brain stimulation) | |
| Secondary | Changes in depression severity, rated by self-reported | including Depression and Somatic Symptoms sub-scales, range from 0 to 66 with higher scores indicating more depressive and somatic symptom. | Time Frame: Baseline, Week 1, Week 2, Week 3 (one week after brain stimulation), Week 6, Week 14(three-month after brain stimulation) | |
| Secondary | Changes in Young Mania Rating Scale | Young Mania Rating Scale, range from 0 to 60 with higher scores indicating more severe manic symptoms. | Time Frame: Baseline, Week 1, Week 2, Week 3 (one week after brain stimulation), Week 6, Week 14(three-month after brain stimulation) | |
| Secondary | Baseline treatment refractory level and the further antidepressant efficacy of brain stimulation | Maudsley staging method(MSM),, range from 3 to 15 with higher scores indicating higher treatment resistance. | Baseline and Week 2 | |
| Secondary | Baseline treatment refractory level(TRDSS) and the further antidepressant efficacy of brain stimulation | Treatment-resistant depression severity scale(TRDSS), range from 3 to 20 with higher scores indicating higher treatment resistance. | Baseline and Week 2 | |
| Secondary | Baseline Life event stress scale and the further clinical efficacy of brain stimulation | Life event stress scale,range from 0 to 1467 with higher scores indicating more life event stress. | Baseline and Week 2 | |
| Secondary | Changes in depression severity, rated by Montgomery-Asberg Depression Rating Scale (MADRS) | the altered MADRS (range, 0 to 60 , with higher scores representing greater severity of depressive symptoms. | Time Frame: Baseline, Week 1, Week 2, Week 3 (one week after brain stimulation), Week 6, Week 14(three-month after brain stimulation) | |
| Secondary | Change in Hamilton Anxiety Scale (HAMA) | the altered Hamilton Anxiety Scale (HAMA) (range, 0 to 56, with higher scores indicating more anxiety) | Time Frame: Baseline, Week 1, Week 2, Week 3 (one week after brain stimulation), Week 6, Week 14(three-month after brain stimulation) | |
| Secondary | Baseline Rumination response scale (RRS) and the further clinical efficacy of brain stimulation | RRS,range from 22 to 88 with higher scores indicating more rumination. | Baseline and Week 2 | |
| Secondary | Change in Rumination response scale (RRS) | RRS,range from 22 to 88 with higher scores indicating more rumination. | Time Frame: Baseline, Week 1, Week 2, Week 3 (one week after brain stimulation), Week 6, Week 14(three-month after brain stimulation) | |
| Secondary | Baseline Snaith-Hamilton Pleasure Scale and the further clinical efficacy of brain stimulation | The 14-item Snaith-Hamilton Pleasure Scale is a self-administered instrument. Each of the items has a set of four response categories--Definitely Agree, Agree, Disagree, and Strongly Disagree, with either of the Disagree responses receiving a score of 1 and either of the Agree responses receiving a score of 0. Thus, the SHAPS was scored as the sum of the 14 items so that total scores ranged from 0 to 14. A higher total SHAPS score indicated higher levels of present state of anhedonia. | Baseline and Week 2 | |
| Secondary | Change in Snaith-Hamilton Pleasure Scale | The 14-item Snaith-Hamilton Pleasure Scale is a self-administered instrument. Each of the items has a set of four response categories--Definitely Agree, Agree, Disagree, and Strongly Disagree, with either of the Disagree responses receiving a score of 1 and either of the Agree responses receiving a score of 0. Thus, the SHAPS was scored as the sum of the 14 items so that total scores ranged from 0 to 14. A higher total SHAPS score indicated higher levels of present state of anhedonia. | Baseline, Week 1, Week 2, Week 3 (one week after brain stimulation), Week 6, Week 14(three-month after brain stimulation) | |
| Secondary | Changes in EEG band before and after brain stimulation | The value changes of prefrontal alpha, beta, theta, delta wave before and after 2 weeks treatment | Baseline and Week 2 | |
| Secondary | Changes in brain connectivity before and after brain stimulation | the change in resting-state functional connectivity | Baseline and Week 2 | |
| Secondary | Changes in TMS-EEG/paired-pulse stimulation before and after brain stimulation | the change in TMS-EEG/paired-pulse stimulation | Baseline and Week 2 | |
| Secondary | Changes in cognitive performance of Taiwan Cognition Questionnaire | Evaluate by Taiwan Cognition Questionnaire, range from 0 to 15 with higher scores indicating higher cognitive impairment | Baseline and Week 2 | |
| Secondary | Changes in cognitive performance of word list recall. | Evaluate by word list recall. | Baseline and Week 2 | |
| Secondary | Changes in cognitive performance of Trail-Making Test | Evaluate by Trail-Making Test | Baseline and Week 2 | |
| Secondary | Changes in cognitive performance of Go/No-Go task | Evaluate by Go/No-Go task | Baseline and Week 2 | |
| Secondary | Changes in cognitive performance of Wisconsin Card Sorting Test | Evaluate by Wisconsin Card Sorting Test | Baseline and Week 2 |
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