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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT01880957
Other study ID # 2012-1826-F
Secondary ID 7R01MH090276-03
Status Completed
Phase N/A
First received
Last updated
Start date November 8, 2011
Est. completion date June 23, 2017

Study information

Verified date July 2022
Source Stony Brook University
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The primary aims of this study are to: 1. Quantify serotonin transporter (5-HTT) binding potential (BP) in vivo in bipolar disorder patients (BPD) during a major depressive episode (MDE). 2. Assess the effect of lithium treatment of bipolar disorder on 5-HTT. 3. Assess the effect of lithium treatment of bipolar disorder on 5-HT1A BP. 4. Assess the effect of lamotrigine treatment of bipolar disorder on 5-HTT and 5-HT1A BP. 5. Assess the effect of lithium treatment of unipolar depression on 5-HTT BP.


Description:

PET and MRI imaging will be used to investigate the aims described above in patients who have bipolar disorder or unipolar depression and are currently experiencing a depressive episode. Both healthy controls and depressed participants with bipolar disorder or unipolar depression will be recruited. Patients who are on medication before enrolling in the study will have a three week washout. At baseline, healthy controls and patients will have an MRI consisting of both structural and functional sequences. Psychological measures will also be obtained at baseline. Within one week of the MRI, both patients and healthy controls will have one CUMI and one DASB PET scan. Following the baseline PET scans, patient participants will begin medication treatment with either lithium or lamotrigine, based on the clinical judgement of the treating psychiatrist. Psychological measures will be obtained every 2 weeks. After 6 weeks of medication treatment at a therapeutic dose, patients will be assessed for remission (defined as a 50% decrease in the HDRS score from baseline). If this criteria is met, patient participants will then have follow-up PET scans (one CUMI and one DASB). If this criteria is not met, the patient will be switched to the other medication under study and will be reevaluated after an additional 4 weeks of medication treatment. Patients who still do not demonstrate a 50% decrease in their HDRS will be considered non-responders and will have repeat CUMI and DASB scans.


Recruitment information / eligibility

Status Completed
Enrollment 76
Est. completion date June 23, 2017
Est. primary completion date June 23, 2017
Accepts healthy volunteers Accepts Healthy Volunteers
Gender All
Age group 18 Years to 65 Years
Eligibility PATIENTS BIPOLAR Inclusion Criteria: - Bipolar patients suffering from a major depressive episode currently or recently (in the month prior to scanning). Patients on psychiatric medication will have failed their current regimen for the treatment of their depression: they will meet criteria for depression, be seeking treatment for it, and have been on an adequate dose of antidepressant or mood stabilizer (as defined by the Antidepressant Treatment Form-see Oquendo et al., 2003) for 4 weeks or more. - Of sufficient severity to score at least 15 on the first 17 items of the Hamilton Depression Rating Scale or a score of 10 to 14 on the first 17 items of the Hamilton Depression Scale in conjunction with a score of at least 29 on the Beck Depression Inventory. - Age range 18-65 years. - Off all psychotropic and other types of drugs likely to interact with serotonin transporters and 5-HT1A receptors for at least 21 days. Allowed short-acting benzodiazepines for distressing anxiety or insomnia (up to 24 hours prior to each PET scan). Patients will be off neuroleptics for 3 weeks and off fluoxetine for 6 weeks prior to study. Off serotonin depleting drugs such as reserpine for 3 months. Patient will also be off anti-coagulant/anti-platelet treatment such as coumadin, with the exception of aspirin for 10 days. - Willing to travel for PET scanning Exclusion Criteria: - Other major psychiatric disorders such as schizophrenia, schizoaffective illness; current drug or alcohol abuse (within past 2 months), or drug or alcohol dependence <6mos ago; anorexia nervosa or bulimia nervosa in the past year; IV drug use or ecstasy use more than two times. - A first-degree family history of schizophrenia if the subject is less than 33 years old (mean age of onset for schizophrenia plus two standard deviations). - Significant active physical illness particularly those that may affect the brain or serotonergic system including blood dyscrasias lymphomas, hypersplenism, endocrinopathies, renal failure or chronic obstructive lung disease, autonomic neuropathies, peripheral vascular disease, diabetes, low hemoglobin and malignancy, significant anemic disease or blood loss and the lab parameters platelet count < 80,000. - Lacks capacity to consent. - Actively suicidal-begins expressing a plan for suicide during the washout phase or develop suicidal ideation that warrants admission or requires medication or treatment intervention. - Electroconvulsive therapy (ECT) within the past 6 months. - Pregnancy, currently lactating; planning to conceive during the course of study participation or abortion in the past two months. - Metal implants, pacemaker or metal prostheses or orthodontic appliances, the presence of shrapnel - Current, past or anticipated exposure to radiation, that may include: being badged for radiation exposure in the workplace, participation in nuclear medicine procedures, including research protocols in the last year. - A neurological disease or loss of consciousness for more than a few minutes - Medicinal Patch (participants will be asked to remove before MRI) - Patients who are responding satisfactorily to psychiatric medications, because they will not be washed-out for purposes of this study - A documented history of a lack of response to a trial of adequate dose and duration of both lithium and lamotrigine defined as minimal clinical response to lamotrigine 200 mgs for at least 4 weeks or lithium serum levels of at least 0.8 (or dose >= 900 mgs) for at least 4 weeks. - Patient is unlikely to be able to tolerate medication washout - Claustrophobia - Blood donation within 8 weeks of the start of the study. - History of bleeding disorder or are currently taking anticoagulants. UNIPOLAR Inclusion: - Unipolar patients suffering from a major depressive episode currently or recently (in the month prior to scanning). Patients on psychiatric medication will have failed their current regimen for the treatment of their depression: they will meet criteria for depression, be seeking treatment for it, and have been on an adequate dose of antidepressant or mood stabilizer (as defined by the Antidepressant Treatment Form-see Oquendo et al., 2003) for 4 weeks or more. - Of sufficient severity to score at least 15 on the first 17 items of the Hamilton Depression Rating Scale or a score of 10 to 14 on the first 17 items of the Hamilton Depression Scale in conjunction with a score of at least 29 on the Beck Depression Inventory. - Age range 18-65 years. - Off all psychotropic and other types of drugs likely to interact with serotonin transporters and 5-HT1A receptors for at least 21 days. Allowed short-acting benzodiazepines for distressing anxiety or insomnia (up to 24 hours prior to each PET scan). Patients will be off neuroleptics for 3 weeks and off fluoxetine for 6 weeks prior to study. Off serotonin depleting drugs such as reserpine for 3 months. Patient will also be off anti-coagulant/anti-platelet treatment such as coumadin, with the exception of aspirin for 10 days. - Willing to travel for PET scanning Exclusion: - Other major psychiatric disorders such as schizophrenia, schizoaffective illness; current drug or alcohol abuse (within past 2 months), or drug or alcohol dependence <6mos ago; anorexia nervosa or bulimia nervosa in the past year; IV drug use or ecstasy use more than two times. - A first-degree family history of schizophrenia if the subject is less than 33 years old (mean age of onset for schizophrenia plus two standard deviations). - Significant active physical illness particularly those that may affect the brain or serotonergic system including blood dyscrasias lymphomas, hypersplenism, endocrinopathies, renal failure or chronic obstructive lung disease, autonomic neuropathies, peripheral vascular disease, diabetes, low hemoglobin and malignancy, significant anemic disease or blood loss and the lab parameters platelet count < 80,000. - Lacks capacity to consent. - Actively suicidal-begins expressing a plan for suicide during the washout phase or develop suicidal ideation that warrants admission or requires medication or treatment intervention. - Electroconvulsive therapy (ECT) within the past 6 months. - Pregnancy, currently lactating; planning to conceive during the course of study participation or abortion in the past two months. - Metal implants, pacemaker or metal prostheses or orthodontic appliances, the presence of shrapnel - Current, past or anticipated exposure to radiation, that may include: being badged for radiation exposure in the workplace, participation in nuclear medicine procedures, including research protocols in the last year. - A neurological disease or loss of consciousness for more than a few minutes - Medicinal Patch (participants will be asked to remove before MRI) - Patients who are responding satisfactorily to psychiatric medications, because they will not be washed-out for purposes of this study - A documented history of a lack of response to a trial of adequate dose and duration of both lithium and lamotrigine defined as minimal clinical response to lamotrigine 200 mgs for at least 4 weeks or lithium serum levels of at least 0.8 (or dose >= 900 mgs) for at least 4 weeks. - Patient is unlikely to be able to tolerate medication washout - Claustrophobia - Blood donation within 8 weeks of the start of the study. - History of bleeding disorder or are currently taking anticoagulants. - Past unsuccessful treatment of Lithium of adequate dose and duration. HEALTHY CONTROLS Inclusion: - No lifetime history of Axis I disorders - Age range 18-65 years. - Willing to travel for PET scanning. Exclusion: - Past or present alcohol/substance abuse or dependence; IV drug use or ecstasy use more than two times. - A first-degree relative with history of major depression, schizophrenia, schizoaffective disorder, or suicide attempt; two or more first degree relatives with a history of substance dependence. - Significant active physical illness particularly those that may affect the brain or serotonergic system including blood dyscrasias lymphomas, hypersplenism, endocrinopathies, renal failure or chronic obstructive lung disease, autonomic neuropathies, peripheral vascular disease, diabetes, low hemoglobin and malignancy, significant anemic disease or blood loss, and the following lab parameters: platelet count < 80,000 - Lacks capacity to consent - Pregnancy, currently lactating; planning to conceive during the course of study participation or abortion in the past two months - Metal implants, pacemaker or metal prostheses or orthodontic appliances, the presence of shrapnel - Current, past or anticipated exposure to radiation, that may include: being badged for radiation exposure in the workplace, participation in nuclear medicine procedures, including research protocols in the last year. - A neurological disease or loss of consciousness for more than a few minutes - Medicinal Patch (participants will be asked to remove before MRI) - Subjects on drugs or medication that affect the serotonin system - Claustrophobia - Blood donation within 8 weeks of the start of the study. - History of bleeding disorder or are currently taking anticoagulants.

Study Design


Intervention

Drug:
Lithium

Lamotrigine


Locations

Country Name City State
United States Stony Brook University Hospital Stony Brook New York

Sponsors (3)

Lead Sponsor Collaborator
Stony Brook University National Institute of Mental Health (NIMH), The Dana Foundation

Country where clinical trial is conducted

United States, 

Outcome

Type Measure Description Time frame Safety issue
Primary Post-Lithium Treatment Hamilton Depression Rating Scale (HDRS) Patients will have a Hamilton Depression Rating Scale-24 (HDRS) score obtained at baseline. Minimum score 0, maximum possible score 75; the higher the score on the scale, the more severe the degree of depression. Participants must have an HDRS score of at least 15 to be eligible. After eight weeks of medication treatment, the HDRS score will be reevaluated with the HDRS-24 (and rescanned with PET and MRI). Participants who have a 50% or greater decrease in their HDRS-24 score will be considered responders (to Lithium treatment). 8 weeks
Primary Prediction of Treatment Response Outcome measures were generated following LASSO linear regression analysis using pretreament HDRS-24 AND..
pre-treatment 5-HTT OR
pretreatment 5-HT1A OR
the combination of both 5-HTT and 5-HT1A binding potential
to predict post-treatment response defined by a dichotomous remission status variable (remitter vs. non-remitter, where remitter is defined a priori by HDRS-24 <10 post-treatment and a reduction of greater than or equal to 50% in HDRS-24 pre-to-post treatment). Outcome measure is reported as percent accuracy, sensitivity, or specificity in predicting remitter status outcomes.
8 Weeks
Secondary Group Differences in 5-HTT Binding Potential Differences in mean of 5-HTT binding potential between patients with depression pre-treatment, post-treatment, compared to healthy volunteers. Broadly, binding potential is defined as the ratio of the tracer concentration in tissue to the free plasma concentration. It is a measure of the density of "available" targets (e.g. 5-HTT) & the affinity of the ligand (tracer) to that target. 8 Weeks
Secondary Group Differences in 5-HT1A Binding Potential Differences in mean of 5-HT1A binding potential between patients with depression pre-treatment, post-treatment, compared to healthy volunteers. Broadly, binding potential is defined as the ratio of the tracer concentration in tissue to the free plasma concentration. It is a measure of the density of "available" targets (e.g. 5-HT1A) & the affinity of the ligand (tracer) to that target. 8 Weeks
Secondary Relationship Between Change in 5-HTT or 5-HT1A Binding Potential Pre- to Post Treatment and Lithium Treatment Response Linear regression & correlation to assess the relationship between between change in binding potential pre- to post treatment vs. treatment response 8 weeks
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