Abstract

Pediatric Bipolar Disorder (PBD) is a serious public health concern associated with mood instability, high suicide rates, substance abuse, academic failure and poor interpersonal relationships. The illness is also associated with significant affect dysregulation and cognitive dysfunction. Onset of this bipolar diathesis early in life may adversely impact the development of brain structures affecting the regulation of mood and cognition known to mature during childhood and adolescence. For that reason, it is particularly important to understand pathophysiological processes affecting the affective and cognitive neural systems during development. Our preliminary findings in the PBD patients, relative to healthy controls, suggest reduced top down regulation of affective brain systems, indicated by decreased activation of dorsolateral and ventrolateral prefrontal cortex and increased activation of amygdala and peri-amygdaloid structures during emotional processing. Therefore, our first and central aim of the current study is to clarify the systems-level pathophysiology during manic states to better identify the interlinked affective and cognitive neural circuitry function. Our secondary aim is to examine the affective and cognitive circuitry function following symptomatic recovery. We plan to use a longitudinal study design, examining brain function in 100 narrowly defined medication naove PBD patients aged 13-16 years at two time points: (1) At baseline in manic state, and (2) After 8 weeks of treatment with the prototypic mood stabilizer lithium carbonate in medicated euthymic responders and non-responders. Additionally, at baseline and at the end of 8 weeks, we will also characterize the brain function in 50 typically developing IQ and demographically matched healthy youths who will be compared with the PBD patients. We will use innovative neurocognitive and fMRI paradigms to probe the affective and cognitive circuitry function at each time point. This work will help to establish a model that characterizes the functional pathophysiology of PBD and provides reliable and objective understanding of the neural systems in illness and on recovery. This model will serve as a prototype in providing future opportunities for preventive efforts by facilitating early identification, moving a step closer to safer, more effective and neurobiologically informed early interventions for youths that would potentially reverse the pathophysiology in PBD patients.

Public Health Relevance

Pediatric Bipolar Disorder (PBD) is a serious illness associated with significant affect dysregulation and cognitive dysfunction, affecting their interpersonal functioning and school achievement. Therefore, the proposed study aims to understand the functioning of the underlying and interfacing affective and cognitive neural circuitry in manic state and in recovery after treatment with lithium in 13 to 16 year old youths with bipolar disorder relative to healthy controls. This model will provide future opportunities for preventive efforts by facilitating early identification, moving a step closer to safer, more effective and neurobiologically informed early interventions for youths affected by PBD.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Research Project (R01)
Project #
5R01MH081019-04
Application #
8197809
Study Section
Child Psychopathology and Developmental Disabilities Study Section (CPDD)
Program Officer
Garvey, Marjorie A
Project Start
2009-01-01
Project End
2013-11-30
Budget Start
2011-12-01
Budget End
2012-11-30
Support Year
4
Fiscal Year
2012
Total Cost
$708,717
Indirect Cost
$257,305

  Institution

Name
University of Illinois at Chicago
Department
Psychiatry
Type
Schools of Medicine
DUNS #
098987217
City
Chicago
State
IL
Country
United States
Zip Code
60612

  Publications

Karaman, M Muge; Sui, Yi; Wang, He et al. (2016) Differentiating low- and high-grade pediatric brain tumors using a continuous-time random-walk diffusion model at high b-values. Magn Reson Med 76:1149-57
Pavuluri, Mani (2014) Trials and tribulations of conducting medication trials: pediatric bipolar disorder as prototype. Clin Investig (Lond) 4:993-996
Shankman, Stewart A; Katz, Andrea C; Passarotti, Alessandra M et al. (2013) Deficits in emotion recognition in pediatric bipolar disorder: the mediating effects of irritability. J Affect Disord 144:134-40
Passarotti, Alessandra M; Fitzgerald, Jacklynn M; Sweeney, John A et al. (2013) Negative emotion interference during a synonym matching task in pediatric bipolar disorder with and without attention deficit hyperactivity disorder. J Int Neuropsychol Soc 19:601-12
Yang, Hongyu; Lu, Lisa H; Wu, Minjie et al. (2013) Time course of recovery showing initial prefrontal cortex changes at 16 weeks, extending to subcortical changes by 3 years in pediatric bipolar disorder. J Affect Disord 150:571-7
Wegbreit, Ezra; Passarotti, Alessandra M; Ellis, James A et al. (2013) Where, when, how high, and how long? The hemodynamics of emotional response in psychotropic-naïve patients with adolescent bipolar disorder. J Affect Disord 147:304-11
Wu, Minjie; Lu, Lisa H; Passarotti, Alessandra M et al. (2013) Altered affective, executive and sensorimotor resting state networks in patients with pediatric mania. J Psychiatry Neurosci 38:232-40
Mayanil, T; Wegbreit, E; Fitzgerald, J et al. (2011) Emerging biosignature of brain function and intervention in pediatric bipolar disorder. Minerva Pediatr 63:183-200
Wegbreit, Ezra; Ellis, James A; Nandam, Aneesh et al. (2011) Amygdala functional connectivity predicts pharmacotherapy outcome in pediatric bipolar disorder. Brain Connect 1:411-22
Passarotti, Alessandra M; Pavuluri, Mani N (2011) Brain functional domains inform therapeutic interventions in attention-deficit/hyperactivity disorder and pediatric bipolar disorder. Expert Rev Neurother 11:897-914

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