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NCT05445466 Clinical Trial

Causal Lesion Network Guided Treatment of Bipolar Mania With Transcranial Electrical Stimulation

Bipolar Disorder Clinical Trial

Official title:
Causal Lesion Network Guided Treatment of Bipolar Mania With Transcranial Electrical Stimulation

Clinical Trial Details — Status: Recruiting

Administrative data
NCT number NCT05445466
Other study ID # 2022P000295
Secondary ID
Status Recruiting
Phase N/A
First received
Last updated
Start date December 16, 2022
Est. completion date August 1, 2024

Study information
Verified date February 2024
Source Beth Israel Deaconess Medical Center
Contact Paulo Lizano, MD, PhD
Phone (617) 754-1227
Email plizano@bidmc.harvard.edu
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

Mania is a core symptom of bipolar disorder involving periods of euphoria. Decreased inhibitory control, increased risk-taking behaviors, and aberrant reward processing are some of the more recognized symptoms of bipolar disorder and are included in the diagnostic criteria for mania. Current drug therapies for mania are frequently intolerable, ineffective, and carry significant risk for side effects. Presently there are no neurobiologically informed therapies that treat or prevent mania. However, using a newly validated technique termed lesion network mapping, researchers demonstrated that focal brain lesions having a causal role in the development of mania in people without a psychiatric history can occur in different brain locations, such as the right orbitofrontal cortex (OFC), right dorsolateral prefrontal cortex (DLPFC), and right inferior temporal gyrus (ITG). This lesion network evidence converges with existing cross-sectional and longitudinal observations in bipolar mania that have identified specific disruptions in network communication between the amygdala and ventro-lateral prefrontal cortex. The OFC is associated with inhibitory control, risk-taking behavior, and reward learning which are major components of bipolar mania. Thus, the association between OFC with mania symptoms, inhibitory control, risk-taking behavior, and reward processing suggests that this region could be targeted using non-invasive brain stimulation.

Description:

Mania is a core symptom of bipolar disorder involving periods of euphoria, delusions, and overactivity. Mania occurs in multiple medical and psychiatric illnesses and can be refractory to existing treatments. Two recent studies using brain lesion mapping of psychiatrically healthy individuals presenting with mania identified causal locations in the brain, including the orbitofrontal cortex (OFC), dorsolateral prefrontal cortex (DLPFC), and inferior temporal gyrus (ITG), that were associated with new onset mania symptoms. Moreover, these identified brain regions have also been implicated in bipolar mania with specific disruption in network communication between the amygdala and ventro-lateral prefrontal cortex. The OFC is of particular interest because it is a brain structure that is associated with inhibitory control, risk-taking behavior and reward, which are major behavioral components of mania. Thus, the association between OFC with mania symptoms, inhibitory control, risk-taking behavior and reward suggests that this region could be targeted using noninvasive brain stimulation. While several studies have non-invasively targeted the DLPFC for mania, no study to date has non-invasively stimulated the OFC with either transcranial direct current stimulation (tDCS) or alternating current (tACS) in bipolar disorder and examined its effects on mania, inhibitory control, or risk-taking behavior. However, a study in healthy volunteers showed that cathodal stimulation to the OFC enhanced inhibitory control and decreased risk-taking behavior. Recently, researches have showed that targeting the OFC with tACS, personalized to the individual's intrinsic beta-gamma frequency of the reward network, that individuals showed rapid, reversible, frequency-specific modulation of reward-guided choice behavior and learning. Here we aim to answer the question of whether noninvasive brain stimulation when optimally targeted and personalized to an individual's beta-gamma frequency to the OFC can improve emotional cognitive processing and mania symptoms compared to tDCS or sham targeting. The knowledge gained from this study will provide a marker for clinical response and allow personalized treatment for patients with bipolar disorder.

Recruitment information / eligibility
Status Recruiting
Enrollment 24
Est. completion date August 1, 2024
Est. primary completion date July 1, 2024
Accepts healthy volunteers No
Gender All
Age group 18 Years to 65 Years
Eligibility Inclusion Criteria: 1. Aged 18-65 years of age 2. Proficient in English 3. Able to give informed consent 4. Meet diagnostic criteria for bipolar disorder or schizoaffective disorder, bipolar type as verified by the SCID 5. History of mania ( >1 lifetime episode) 6. Experiencing mild to moderate symptoms of mania 7. No changes to mood stabilizing medications for a period of 2 weeks prior to participation 8. Has not recently participated in tES/TMS treatments Exclusion Criteria: 1. Substance abuse or dependence (w/in past 6 months) 2. Those who are pregnant/breastfeeding 3. History of head injury with > 15 minutes of loss of consciousness/mal sequelae 4. DSM-V intellectual disability 5. Having a non-removable ferromagnetic metal within the body (particularly in the head) 6. History of seizures

Study Design

Related Conditions & MeSH terms

Intervention

Device:
High-Definition Transcranial Electrical-Current Stimulation
Non-frequency dependent transcranial electrical stimulation condition for 5 days of twice a day treatment
High-Definition Transcranial Alternate-Current Stimulation
Active-control stimulation condition will target alpha (10 Hz) for 5 days of twice a day treatment
High-Definition Personalized Beta-Gamma Electrical Stimulation
Personalized beta-gamma electrical stimulation for 5 days of twice a day treatment

Locations
Country Name City State
United States Beth Israel Deaconess Medical Center Boston Massachusetts

Sponsors (1)
Lead Sponsor Collaborator
Beth Israel Deaconess Medical Center

Country where clinical trial is conducted

United States, 

Outcome
Type Measure Description Time frame Safety issue
Primary Young Mania Rating Scale (YMRS) Measuring total Mania scores; 11 items used to access severity of mania (total score 0-60); higher scores represent higher severity of symptoms Change from baseline to 5 Day follow-up
Primary Young Mania Rating Scale (YMRS) Measuring total Mania scores; 11 items used to access severity of mania (total score 0-60); higher scores represent higher severity of symptoms Change from baseline to 1-month follow-up
Primary Young Mania Rating Scale (YMRS) Measuring total Mania scores; 11 items used to access severity of mania (total score 0-60); higher scores represent higher severity of symptoms Change from baseline to 3-month follow-up
Primary Altman Self-Rating Mania Scale (ASRM) The ASRM is a 5-item self rating mania scale, assessing the presence and severity of manic symptoms. 6 or higher indicates a high probability of a manic or hypomanic condition. Change from baseline to 5 Day follow-up
Primary Altman Self-Rating Mania Scale (ASRM) The ASRM is a 5-item self rating mania scale, assessing the presence and severity of manic symptoms. 6 or higher indicates a high probability of a manic or hypomanic condition. Change from baseline to 1-month follow-up
Primary Altman Self-Rating Mania Scale (ASRM) The ASRM is a 5-item self rating mania scale, assessing the presence and severity of manic symptoms. 6 or higher indicates a high probability of a manic or hypomanic condition. Change from baseline to 3-month follow-up
Primary Psychiatric Hospitalization for Mania Psychiatric hospitalization for mania Average per year prior to study entry compared to 1 year post study completion
Secondary Balloon Analogue Risk Task (BART) The BART is a computerized task the measures risk-taking behavior. Change from baseline to 5 Day follow-up
Secondary Balloon Analogue Risk Task (BART) The BART is a computerized task the measures risk-taking behavior. Change from baseline to 1-month follow-up
Secondary Balloon Analogue Risk Task (BART) The BART is a computerized task the measures risk-taking behavior. Change from baseline to 3-month follow-up
Secondary The Go/No Go Task The Go/No Go Task is a computerized task that measures impulsiveness. Change from baseline to 5 Day follow-up
Secondary The Go/No Go Task The Go/No Go Task is a computerized task that measures impulsiveness. Change from baseline to 1-month follow-up
Secondary The Go/No Go Task The Go/No Go Task is a computerized task that measures impulsiveness. Change from baseline to 3-month follow-up
Secondary Electroencephalography (EEG) Resting State EEG measures neural activity recorded from electrodes placed on the scalp. Resting state measures include connectivity as well as oscillatory characteristics within delta, theta, alpha, beta, gamma bands. Change from baseline to 5 Day follow-up
Secondary Electroencephalography (EEG) Resting State EEG measures neural activity recorded from electrodes placed on the scalp. Resting state measures include connectivity as well as oscillatory characteristics within delta, theta, alpha, beta, gamma bands. Change from baseline to 1-month follow-up
Secondary Electroencephalography (EEG) Resting State EEG measures neural activity recorded from electrodes placed on the scalp. Resting state measures include connectivity as well as oscillatory characteristics within delta, theta, alpha, beta, gamma bands. Change from baseline to 3-month follow-up
Secondary Reinforcement Learning Task The reinforcement learning task is a monetary based learning tasks that included reward and punishment trails. Change from baseline to 5 Day follow-up
Secondary Reinforcement Learning Task The reinforcement learning task is a monetary based learning tasks that included reward and punishment trails. Change from baseline to 1-month follow-up
Secondary Reinforcement Learning Task The reinforcement learning task is a monetary based learning tasks that included reward and punishment trails. Change from baseline to 3-month follow-up
Secondary Social Functioning Scale (SFS) The SFS a self-report questionnaire initially designed for people diagnosed with Schizophrenia; consists of 79 items designed to reflect the social skills and performances in different areas of life. Total score of SFS ranges between 55 - 145 points. Higher scores mean better social functioning. Change from baseline to 5 Day follow-up
Secondary Social Functioning Scale (SFS) The SFS a self-report questionnaire initially designed for people diagnosed with Schizophrenia; consists of 79 items designed to reflect the social skills and performances in different areas of life. Total score of SFS ranges between 55 - 145 points. Higher scores mean better social functioning. Change from baseline to 1-month follow-up
Secondary Social Functioning Scale (SFS) The SFS a self-report questionnaire initially designed for people diagnosed with Schizophrenia; consists of 79 items designed to reflect the social skills and performances in different areas of life. Total score of SFS ranges between 55 - 145 points. Higher scores mean better social functioning. Change from baseline to 3-month follow-up
Secondary Global Assessment of Functioning (GAF) The GAF measures how symptoms affect individuals day-to-day life; scored from 0 to 100 Change from baseline to 5 Day follow-up
Secondary Global Assessment of Functioning (GAF) The GAF measures how symptoms affect individuals day-to-day life; scored from 0 to 100 Change from baseline to 1-month follow-up
Secondary Global Assessment of Functioning (GAF) The GAF measures how symptoms affect individuals day-to-day life; scored from 0 to 100 Change from baseline to 3-month follow-up
Secondary Positive and Negative Syndrome Scale (PANSS) 30 items included in the PANSS measuring positive, negative and general symptoms; 7 related to positive symptoms, 7 for negative symptoms, and 16 for general psychopathology Scale. Ranges are 7 to 49 for the Positive and Negative Scales, and 16 to 112 for the General Psychopathology Scale. Change from baseline to 5 Day follow-up
Secondary Positive and Negative Syndrome Scale (PANSS) 30 items included in the PANSS measuring positive, negative and general symptoms; 7 related to positive symptoms, 7 for negative symptoms, and 16 for general psychopathology Scale. Ranges are 7 to 49 for the Positive and Negative Scales, and 16 to 112 for the General Psychopathology Scale. Change from baseline to 1-month follow-up
Secondary Positive and Negative Syndrome Scale (PANSS) 30 items included in the PANSS measuring positive, negative and general symptoms; 7 related to positive symptoms, 7 for negative symptoms, and 16 for general psychopathology Scale. Ranges are 7 to 49 for the Positive and Negative Scales, and 16 to 112 for the General Psychopathology Scale. Change from baseline to 3-month follow-up
Secondary Montgomery-Åsberg Depression Rating Scale (MADRS) The MADRS is designed to measure depression and severity of symptoms; 0 to 6 indicates no depression, 7 to 19 indicates mild depression, 20 to 34 indicates moderate depression, 35 and greater indicates severe depression. Change from baseline to 5 Day follow-up
Secondary Montgomery-Åsberg Depression Rating Scale (MADRS) The MADRS is designed to measure depression and severity of symptoms; 0 to 6 indicates no depression, 7 to 19 indicates mild depression, 20 to 34 indicates moderate depression, 35 and greater indicates severe depression. Change from baseline to 1-month follow-up
Secondary Montgomery-Åsberg Depression Rating Scale (MADRS) The MADRS is designed to measure depression and severity of symptoms; 0 to 6 indicates no depression, 7 to 19 indicates mild depression, 20 to 34 indicates moderate depression, 35 and greater indicates severe depression. Change from baseline to 3-month follow-up
Secondary Barratt Impulsiveness Scale-11 (BIS-11) The BIS-11 is designed to assess the personality/behavioral impulsiveness. The BIS-11 has 30 items and is scored appropriately. Scored to yield a total score, three second-order factors, and six first-order factors. Each question has a 4-point scale ranging from 1 (rarely/never) to 4 (almost always/always). Higher scores mean more impulsive behavior. Change from baseline to 5 Day follow-up
Secondary Barratt Impulsiveness Scale-11 (BIS-11) The BIS-11 is designed to assess the personality/behavioral impulsiveness. The BIS-11 has 30 items and is scored appropriately. Scored to yield a total score, three second-order factors, and six first-order factors. Each question has a 4-point scale ranging from 1 (rarely/never) to 4 (almost always/always). Higher scores mean more impulsive behavior. Change from baseline to 1-month follow-up
Secondary Barratt Impulsiveness Scale-11 (BIS-11) The BIS-11 is designed to assess the personality/behavioral impulsiveness. The BIS-11 has 30 items and is scored appropriately. Scored to yield a total score, three second-order factors, and six first-order factors. Each question has a 4-point scale ranging from 1 (rarely/never) to 4 (almost always/always). Higher scores mean more impulsive behavior. Change from baseline to 3-month follow-up
Secondary Brief Assessment of Cognition (BACS) The BACS is designed to assess several domains of cognition; Verbal Memory; Processing Speed; Working Memory; Verbal Fluency; Motor Function; Executive Functioning. Higher scores indicate better cognitive functioning. Change from baseline to 5 Day follow-up
Secondary Brief Assessment of Cognition (BACS) The BACS is designed to assess several domains of cognition; Verbal Memory; Processing Speed; Working Memory; Verbal Fluency; Motor Function; Executive Functioning. Higher scores indicate better cognitive functioning. Change from baseline to 1-month follow-up
Secondary Brief Assessment of Cognition (BACS) The BACS is designed to assess several domains of cognition; Verbal Memory; Processing Speed; Working Memory; Verbal Fluency; Motor Function; Executive Functioning. Higher scores indicate better cognitive functioning. Change from baseline to 3-month follow-up
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