Multimodal Neuroimaging of Treatment Effects in Adolescent Mania
Study Details
Study Description
Brief Summary
Specific Aim 1: To determine the effects of treatment with quetiapine or lithium on brain activation in adolescents. The investigators will use functional magnetic resonance imaging (fMRI) to examine brain activation during an attentional task.
Specific Aim 2: To determine the effects of treatment with quetiapine or lithium on neurometabolite measures, early in their illness course. The investigators will use 1H-MRS to identify myo-inositol (mI), N-acetyl aspartate (NAA), and glutamate (Glu) levels in prefrontal ALN regions.
Specific Aim 3: To determine the relationships among the changes in brain activation and neurometabolite measures, as well as symptomatic improvement in manic adolescents.
Condition or Disease | Intervention/Treatment | Phase |
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N/A |
Detailed Description
Hypotheses 1 & 2 predict that following 6 weeks of treatment with lithium or quetiapine, manic adolescents who demonstrate symptomatic improvement will exhibit normalized (decreased) VLPFC and ACC activation and increased activation of compensatory posterior attentional brain areas as well as normalization of VLPFC and ACC neurometabolite measures (increased NAA and decreased Glu levels) compared with those who do not experience symptomatic improvement and healthy adolescents.
Hypothesis 3 predicts significant associations between fMRI activation changes (i.e. decreased activation in VLPFC and ACC ROIs and increased activation in the posterior attention ROI) and MRS changes (increases in NAA and decreases in Glu levels in the VLPFC and ACC) for patients who exhibit symptomatic improvement with either treatment.
Hypothesis 4 predicts that decreases in mI levels at 1 week will be associated with lithium, but not quetiapine, response at endpoint.
In contrast, Hypothesis 5 predicts higher baseline Cho levels will be associated with quetiapine, but not lithium, response at endpoint.
Study Design
Arms and Interventions
Arm | Intervention/Treatment |
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Active Comparator: 1--Quetiapine & Placebo Quetiapine & Placebo in the place of Lithium |
Drug: Quetiapine & Placebo
Bipolar adolescents will be initiated on 100 mg per day of quetiapine (or placebo) and 30 mg/kg (maximum starting dose of 600 mg twice daily) of lithium carbonate (or placebo), depending on randomization assignment. Patients will be given placebo for the medication to which they were not assigned. Quetiapine will be adjusted based on tolerability and response to a target dose of 400-600 mg and lithium will be adjusted to a target dose based on achieving a serum level of 1.0-1.2 mEq/L.
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Active Comparator: 2-- Lithium & Placebo Lithium & Placebo in the place of Quetiapine |
Drug: Lithium and Placebo
Bipolar adolescents will be initiated on 100 mg per day of quetiapine (or placebo) and 30 mg/kg (maximum starting dose of 600 mg twice daily) of lithium carbonate (or placebo), depending on randomization assignment. Patients will be given placebo for the medication to which they were not assigned. Quetiapine will be adjusted based on tolerability and response to a target dose of 400-600 mg and lithium will be adjusted to a target dose based on achieving a serum level of 1.0-1.2 mEq/L.
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Placebo Comparator: Placebo Sugar Pill (Placebo) given to mimic drug |
Other: Healthy Controls
Healthy control (patients given placebo -- sugar pill intended to mimic drug)
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Outcome Measures
Primary Outcome Measures
- The purpose of this study is to use magnetic resonance imaging (MRI) to examine brain structure, function and chemistry in people with Bipolar I disorder (manic or mixed episodes) who are being treated with either quetiapine or lithium. [6 weeks]
Eligibility Criteria
Criteria
Inclusion/Exclusion Criteria
Inclusion - Bipolar Disorder Subjects:
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DSM-IV-TR12 criteria for bipolar disorder, type I, manic or mixed episode, diagnosed by the Washington University in St. Louis Kiddie Schedule for Affective Disorders and Schizophrenia (WASH-U-KSADS)166,101,102-103,104-105,108
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Baseline YMRS112-114 score > 20;
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Ages 12-17 years 11 months old;
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Fluent in English;
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Provision of written informed consent by a legal guardian and written assent by the subject;
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Tanner scale stages III-V167, in order to include only post-pubescent subjects and minimize brain changes associated with the onset of puberty;168-169
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Less than 2 years from onset of bipolar disorder, defined by age at onset of first DSM-IV-TR affective episode (mania, hypomania, depression or mixed), to establish that our sample is early in their illness course;
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No prior psychiatric hospitalizations, <3 months of lifetime psychotropic medication exposure (with the exception of psychostimulants, since excluding patients with psychostimulant exposure would significantly limit the generalizability of our findings), and no active psychotropic medication during the week (72 hours for psychostimulants and benzodiazepines) prior to the index assessment (no treatment with fluoxetine during the prior month). Please note that patients will NOT be taken off medications for the purpose of this study; instead, this criterion is to exclude subjects receiving treatment at the time of index assessment;
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Does not have a history of intolerance or non-response to lithium or quetiapine;
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Manic or depressive symptoms do not result entirely from acute medical illness or acute intoxication or withdrawal from drugs or alcohol as determined by medical evaluation and rapid symptom resolution;
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No lifetime DSM-IV-TR diagnosis of post-traumatic stress disorder (PTSD), since PTSD has been associated with abnormalities in prefrontal NAA and function170-171,172. Furthermore, bipolar patients with co-occurring PTSD are less likely to respond to lithium monotherapy, and often need a serotonin specific reuptake inhibitor (SSRI) as adjunctive treatment to a mood stabilizer.173,174 ;
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If female and of child bearing potential, agrees to use one of the following method of birth control: complete abstinence from sexual intercourse, barrier (diaphragm or condom), or oral/injectable contraceptive.
Inclusion - Healthy Controls:
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Ages of 12-17 years and 11 month;
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No history of any DSM-IV-TR Axis I disorder (nicotine dependence is permitted);
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No first- or second-degree relatives with an affective or psychotic disorder;
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No medications with central nervous system effects within 5 half-lives;
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Fluent in English;
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Tanner stage III-V;
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Provision of informed consent and assent.
Exclusion - Bipolar Subjects & Healthy Controls:
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Contraindication to an MRI scan (e.g., braces or claustrophobia);
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An unstable medical or neurological illness that could influence fMRI or MRS results;
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IQ < 70, as determined by The Wechsler Abbreviated Scale of Intelligence (WASI) ;
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A positive pregnancy test;
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A history of major medical or neurological illness or a significant episode (> 10 minutes) of loss of consciousness;
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Any lifetime DSM-IV-TR substance use disorder (nicotine dependence is permitted);
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A lifetime DSM-IV-TR diagnosis of any pervasive developmental disorder;
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The patient lives >100 miles from the University of Cincinnati or is not able to attend follow-up visits.
Contacts and Locations
Locations
Site | City | State | Country | Postal Code | |
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1 | University of Cincinnati | Cincinnati | Ohio | United States | 45219 |
Sponsors and Collaborators
- University of Cincinnati
- Children's Hospital Medical Center, Cincinnati
Investigators
- Principal Investigator: Melissa DelBello, MD, University of Cincinnati
Study Documents (Full-Text)
None provided.More Information
Publications
None provided.- DelBello MM NeuroImaging Study