13:30 |
592. |
In Vivo 3D Lithium
MRI of the Human Brain
Fernando Emilio
Boada1, Yongxian Qian1, Ariel
Gildengers2, Mary Phillips2, David
Kupfer2
1MR
Research Center, University of Pittsburgh, Pittsburgh, PA,
United States; 2Psychiatry, University of
Pittsburgh, Pittsburgh, PA, United States
Bipolar Disorder (BPD) is a
devastating mental illness that is often treated using
Lithium Carbonate therapy. Unfortunately, lithium carbonate
therapy has life-threatening side effects. Moreover, its
mechanisms of action and preferred accumulation sites in the
in vivo brain continue to be unknown sixty years after its
original introduction. A methodology for studying the
spatial distribution of lithium carbonate in the brain of
BPD subjects could, therefore, be an invaluable tool for
studying this disease. In this work we present the first
demonstration of 3D lithium MRI in the in Vivo human Brain
at 7 Tesla. |
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13:42 |
593. |
4T 7Li
MRSI in the Brains of Bipolar Disorder Subjects
Jing-Huei Lee1,2,
Matthew M. Norris1, Caleb M. Adler2,3,
Elizabeth E. Macaluso2, Wen-Jang Chu2,3,
Richard A. Komoroski2,3, Stephen M. Strakowski2,3
1Biomedical
Engineering, University of Cincinnati, Cincinnati, OH,
United States; 2Center for Imaging Research,
University of Cincinnati, Cincinnati, OH, United States;
3Psychiatry, University of Cincinnati,
Cincinnati, OH, United
States
This work proposes and
compares two approaches for 7Li MRSI data
analysis: Method I: 1D-3D vs. Method II: 3D-1D approach. The
result shows that there is virtually no difference between
these two approaches. However, Method I is preferred for use
in future data analysis since it is simple in practice.
Furthermore, this study is the first demonstration of the
7Li distribution in the brain of bipolar patients
who are on lithium therapy. The distribution is not uniform
throughout the entire brain for all patients, which is
unexpected. Further investigations are ongoing. |
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13:54 |
594. |
Decreased PHi and
[ADP] in Anterior Cingulate Cortex of Bipolar Disorder:
Further Evidence of Mitochondrial Dysfunction
Jonathan Dudley1,
Wen-Jang Chu2,3, Xin Wang1, Matt
Norris1, Jing-Huei Lee1,3
1Biomedical
Engineering, University of Cincinnati, Cincinnati, OH,
United States; 2Psychiatry, University of
Cincinnati, Cincinnati, OH, United States; 3Center
for Imaging Research, University of Cincinnati, Cincinnati,
OH, United States
The theory of mitochondrial
dysfunction in bipolar disorder (BD) has been supported by
numerous MRS studies. However, the absolute quantitation of
phosphor metabolites in this disease has not been well
studied. This work is to determine phosphor metabolite
concentrations in the anterior cingulate cortex among
different subject groups. The results were in concordance
with the theory of mitochondrial dysfunction, showing a
decrease in intracellular pH and [ADP] in manic and mixed BD
patients relative to controls. |
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14:06 |
595. |
Metabolic Changes
in Medication-Free Patients with Bipolar and Unipolar
Disorder
Ulrike Dydak1,2, Jonathan M. Nixon1,
Mario Dzemidzic3, Harish Sai Karne4,
Amit Anand4
1School of Health Sciences,
Purdue University, West Lafayette, IN, United States; 2Department
of Radiology and Imaging Sciences, Indiana University School
of Medicine, Indianapolis, IN, United States; 3Department
of Neurology, Indiana University School of Medicine,
Indianapolis, IN, United States; 4Department of
Psychiatry, Indiana University School of Medicine,
Indianapolis, IN, United States
Changes in brain metabolism
were studied in medication-free patients with bipolar and
unipolar disorder and compared to matched healthy controls.
2D MRSI data acquired in an axial slice including thalamus,
anterior and posterior cingulate cortex (ACC & PCC) were
analyzed using LCModel. Significant decreases in NAA/
creatine were found in bipolar patients compared to healthy
controls in the right thalamus and right ACC. Furthermore,
when comparing bipolar to unipolar patients, significant
decreases in the choline/creatine ratio were observed in the
right thalamus. No significant group differences were found
in the PCC nor any of the left hemisphere regions of
interest.
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14:18 |
596. |
Dissociation of
Anterior Cingulate Glutamate and Induced Theta EEG Activity
in Schizophrenia
Antonio Napolitano1,
Kathrin Doege2, Mallikarjun Pavan2,
Peter Liddle2, Dorothee P. Auer1
1Academic Radiology, University
of Nottingham, Nottingham, Nottinghamshire, United Kingdom;
2Division of Psychiatry, University of
Nottingham, United Kingdom
The glutamate hypothesis
stimulated over the last two decades several MRS studies to
research alterations of glutamate levels in schizophrenia.
In this study, we used a combined EEG/MRS protocol to
investigate whether prefrontal glutamate levels are altered
in patients with early schizophrenia and whether there is an
interrelation between glutamate and theta activity in
schizophrenia. |
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14:30 |
597. |
Tissue Specific
Changes in Brain Phosphodiesters in Late Life Major
Depression
David G. Harper1,2, J.
Eric Jensen2,3, Caitlin Ravichandran2,4,
E. Yusuf Sivrioglu5, Daniel Iosifescu6,7,
Perry Renshaw8, Brent Forester2,9
1Geriatric Psychiatry, McLean
Hospital, Belmont, MA, United States; 2Psychiatry,
Harvard Medical School, Belmont, MA, United States; 3Neuroimaging
Center, McLean Hospital, Belmont, MA, United States; 4Laboratory
for Psychiatric Biostatistics, McLean Hospital, Belmont, MA,
United States; 5Psychiatry, Uludag University,
Bursa, Turkey; 6Psychiatry, Massachusetts General
Hospital, Boston, MA, United States; 7Psychiatry,
Harvard Medical School, Boston, MA, United States; 8Psychiatry,
University of Utah, Salt Lake City, UT, United States;
9Geriatric Psychiatry, Mclean Hospital, Belmont, MA,
United States
Biological membranes serve
numerous, essential cellular functions. MRI findings in
late life depression include increased white matter
hyperintensities and reduced fractional anisotropy as
measured by diffusion tensor imaging suggesting that
membrane integrity, especially in white matter, may be
compromised. Phosphatidylethanolamine, in the inner
mitochondrial membrane, serves an essential function and is
synthesized via a unique pathway not involving
phosphoethanolamine. We hypothesized that
glycerophosphocholine (GPCho) and
glycerophosphoethanolamine (GPEtn), particularly in white
matter, will be increased in late-life depression, and we
hypothesized that GPEtn will be altered fundamentally
differently than GPCho due to the additional pathway of the
inner mitochondrial membrane and that GPEtn would therefore
show changes in gray matter. |
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14:42 |
598. |
1H MRS
Measurement of Brain Glutathione Supports Increased
Oxidative Stress in Major Depressive Disorder
Sanjay J. Mathewew1,
Xiangling Mao2, Sarah Pillemer1, James
W. Murrough1, Dikoma C. Shungu2
1Psychiatry,
Mount Sinai School of Medicine, New York, NY, United States;
2Radiology, Weill Cornell Medical College, New
York, NY, United States
A large body of anecdotal
evidence now implicates increased oxidative stress in a
number of pathophysiologic models of major depressive
disorder (MDD). In this study, the first in vivo
1H MRS measurements of the primary cellular
antioxidant glutathione (GSH) were made in the occipital
lobe of MDD patients and found to be significantly decreased
compared to healthy control subjects, which supports the
presence of increased oxidative stress in the disorder.
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14:54 |
599. |
Evidence of Age
Effects in Cortical Areas But Not in the Subcortex of ADHD
Children: A Multi-Voxel In Vivo 31P
Spectroscopy Study at 4 Tesla
Jeffrey A.
Stanley1, Dalal Khatib1, Rachel M.
Dick1, Olivia A. McGarragle1, Frank P.
MacMaster1, Vaibhav A. Diwadkar1,
Arthur L. Robin1, David R. Rosenberg1
1Psychiatry
and Behavioral Neurosciences, Wayne State University School
of Medicine, Detroit, MI, United States
Attention Deficit
Hyperactivity Disorder (ADHD) is a serious public health
problem that affects between 3 to 9% of children and
accounts for between 30 to 40% of child referrals to mental
health services. While the cause of this illness remains
poorly understood, ADHD is increasingly seen as a
neurodevelopmental disorder. In vivo 31P
spectroscopy is a neuroimaging method that is sensitive in
detecting biochemical changes as the brain develops. The
purpose of this study is to provide further evidence of a
developmental mechanism where early maldeveloped
corticostriatal pathways may impact the maturational
integration of prefrontal corticostriatal pathways in
pediatric ADHD. |
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15:06 |
600. |
Disruption of
Commissural White Matter Tracts in Pediatric Bipolar
Disorder
Hao Huang1,
Kirti Saxena2, Annie Walley2, Min Xu1,
Nancy Rollins3
1Advanced
Imaging Research Center, University of Texas Southwestern
Medical Center, Dallas, TX, United States; 2Department
of Psychiatry, University of Texas Southwestern Medical
Center, Dallas, TX, United States; 3Department of
Radiology, University of Texas Southwestern Medical Center,
Dallas, TX, United States
Identifying early signs of
bipolar disorder is important because it may enable health
care providers to intervene earlier and prevent progression
of increased morbidity and personal dysfunction. Commissural
tracts including corpus callosum (CC) and anterior
commissure (AC) are the research target in this study. In
our study, we acquired high resolution DTI from 10 pediatric
bipolar patients and 10 age matched control subjects. We
found that AC and anterior segment of CC has statistically
smaller FA. Compared to DTI results of adult BP, the
disruption pattern caused by BP demonstrates anterior to
posterior pattern from childhood to adult. |
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15:18 |
601. |
Atypical
Development of White Matter Microstructure in Adolescents
with Autism Spectrum Disorders
Kun-Hsien Chou1,
I-Yun Chen2, Ya-Wei Cheng2, Jean
Decety3, Yang-Teng Fan2, Ching-Po Lin2,4
1Institute
of Biomedical Engineering, National Yang-Ming University,
Taipei, Taiwan; 2Institute of Neuroscience,
National Yang-Ming University, Taipei, Taiwan; 3Departments
of Psychology and Psychiatry, The University of Chicago,
Chicago, United States; 4Institute of Biomedical
imaging and Radiological Sciences, National Yang-Ming
University, Taipei, Taiwan
Autism spectrum disorders is
a common brain developmental disorder that occurs in one in
150 children. It is characterized by early onset of impaired
social reciprocity and communication difficulties, along
with restricted interest and stereotyped behavior. Several
brain morphometry studies suggested that cascade failure of
neurodevelopment is the most likely the core deficit of ASD.
But whether aberrant WM development persisted into later
childhood and adolescence was a crucial issue to probe. The
aim of the present study was to examine WM microstructure
using diffusion tensor imaging (DTI) and to investigate its
relations to age in adolescents with ASD.
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