Abstract

Bipolar disorder is a dynamic illness with constantly changing symptom and syndrome presentations that? confound interpretation of neuroimaging findings, as well as treatment response. This feature of the illness? raises the need to examine patients as the condition evolves over time in order to clarify interactions? between neuroimaging measures, clinical response and affective state. Careful longitudinal assessments? and subject retention are critical elements to the success of the BITREC and its proposed projects. The? Longitudinal Assessment Core (LAC) will serve this need and is a direct extension of over a decade of? experience following young bipolar patients. Specifically, our experience with longitudinal studies is? demonstrated by the success of a number of large, long-term projects. Our previous and ongoing projects? provide an infrastructure for the longitudinal study of bipolar disorder from which the LAC will be developed.? The LAC will be fully integrated with the other BITREC cores and projects as described in the Operational? Plan. Dr. Paul Keck, Professor of Psychiatry and Pharmacology and Vice-Chair for Research in the? Department of Psychiatry will direct the LAC. He will be responsible for overall core function and for? overseeing infrastructure development. He will be assisted by several clinicians and staff to provide excellent? clinical care and ongoing assessments to subjects enrolled in the BITREC. The LAC will hold staff meetings? every other week to ensure that recruitment benchmarks are being met and to review subjects who have? developed new affective episodes or symptoms in order to determine whether they qualify for additional? BITREC projects. Standard operating procedures will be developed to maximize efficiency and meet? objectives and benchmarks. Most decisions involving daily core function will be made by the personnel of the? core under the direction of Dr. Keck. These decisions will be guided by and reported to the BITREC Steering? Committee. Additionally, Dr. Keck will be integrated within the overall administrative structure of the BITREC? by serving on the Steering Committee. With this structure established the LAC will be able to meet its? primary functions which are: 1) to provide treatment to subjects actively participating in BITREC projects;? 2) to provide ongoing clinical evaluations and excellent clinical care to subjects enrolled in the BITREC? between projects; and 3) to identify subjects who meet criteria for a new BITREC project. By following and? managing subjects across project, the LAC helps to further integrate the various components of the BITREC,? assuring a cohesive and effective research center.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Specialized Center (P50)
Project #
5P50MH077138-02
Application #
7637869
Study Section
Special Emphasis Panel (ZMH1)
Project Start
Project End
Budget Start
2008-07-01
Budget End
2009-06-30
Support Year
2
Fiscal Year
2008
Total Cost
$311,833
Indirect Cost

  Institution

Name
University of Cincinnati
Department
Type
DUNS #
041064767
City
Cincinnati
State
OH
Country
United States
Zip Code
45221

  Publications

Nery, Fabiano G; Norris, Matthew; Eliassen, James C et al. (2017) White matter volumes in youth offspring of bipolar parents. J Affect Disord 209:246-253
Fleck, David E; Ernest, Nicholas; Adler, Caleb M et al. (2017) Prediction of lithium response in first-episode mania using the LITHium Intelligent Agent (LITHIA): Pilot data and proof-of-concept. Bipolar Disord 19:259-272
Welge, Jeffrey A; Saliba, Lawrence J; Strawn, Jeffrey R et al. (2016) Neurofunctional Differences Among Youth With and at Varying Risk for Developing Mania. J Am Acad Child Adolesc Psychiatry 55:980-989
Strakowski, Stephen M; Fleck, David E; Welge, Jeffrey et al. (2016) fMRI brain activation changes following treatment of a first bipolar manic episode. Bipolar Disord 18:490-501
McNamara, Robert K; Jandacek, Ronald; Tso, Patrick et al. (2016) Adolescents with or at ultra-high risk for bipolar disorder exhibit erythrocyte docosahexaenoic acid and eicosapentaenoic acid deficits: a candidate prodromal risk biomarker. Early Interv Psychiatry 10:203-11
McNamara, Robert K; Moser, Ann B; Jones, Richard I et al. (2016) Familial risk for bipolar disorder is not associated with impaired peroxisomal function: Dissociation from docosahexaenoic acid deficits. Psychiatry Res 246:803-807
McNamara, Robert K; Jandacek, Ronald; Tso, Patrick et al. (2015) First-episode bipolar disorder is associated with erythrocyte membrane docosahexaenoic acid deficits: Dissociation from clinical response to lithium or quetiapine. Psychiatry Res 230:447-53
Jacob, Shawna N; Shear, Paula K; Norris, Matthew et al. (2015) Impact of functional magnetic resonance imaging (fMRI) scanner noise on affective state and attentional performance. J Clin Exp Neuropsychol 37:563-70
Strawn, Jeffrey R; Adler, Caleb M; McNamara, Robert K et al. (2014) Antidepressant tolerability in anxious and depressed youth at high risk for bipolar disorder: a prospective naturalistic treatment study. Bipolar Disord 16:523-30
Cerullo, Michael A; Eliassen, James C; Smith, Christopher T et al. (2014) Bipolar I disorder and major depressive disorder show similar brain activation during depression. Bipolar Disord 16:703-12

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