Abstract

The GCAP Neuroimaging Core implements quality control procedures, optimizes and updates imaging protocols, and collects all clinical imaging data from the CBDB Sibling and inpatients studies, and maintains and analyzes all structural, spectroscopy, DTI, and large scale archival fMRI data used in these studies. The Neuroimaging Core covers the following neuroimaging domains: 1. Structural MRI: acquisition, quality control, segmentation, automated and manual regions-of-interest (ROI) definition and measurements, surface extraction; 2. Functional MRI: acquisition, quality control, preprocessing, standardized analyses; 3. Spectroscopy: acquisition, quality control, preprocessing, ROI-based and voxel-based; 4. DTI: acquisition, quality control, preprocessing;and 5. Implementing new MRI techniques. The Neuroimaging Core subserves the following functions: 1. Medical coverage and image acquisition, image quality control (for data acquired by the core); 2. Maintenance of stimulation equipment, liaison with other NIH imaging core facilities; 3. Implementing and maintaining acquisition of physiological measurements and interventions, (e.g. galvanic skin response, pupillometry, pulse pressure); 4. Creates and updates a manual of MR acquisition and data analysis methods; 5. Training and supervising of research assistants and fellows in neuroimaging methods and analysis; 6. Perform standardized analyses and analysis quality control;and 7. Data mining and distributing of raw and processed data to GCAP investigators;integration with genomic and other scientific data maintained within GCAP. It is expected that other imaging studies performed in GCAP may use the Neuroimaging Core protocols and facilities for those parts (such as structural MRI scanning) it can perform to facilitate integrating and relating these data to the larger archival datasets. To function clinically, the core requires the participation of several staff physicians to perform data mining and analysis functions;requires computer specialists, and a fairly large group of research assistants who rotate between imaging and image analyses and are trained to maintain a standard level of knowledge in imaging and analysis. Day-to-day operation of the core is overseen by the Director of the Neuroimaging Core. Neuroimaging Core's strategy and supervision is under the direction of the Director of the Genes, Cognition and Psychosis Program and a panel consisting of clinical investigators and the Clinical and Scientific Directors.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Scientific Cores Intramural Research (ZIC)
Project #
1ZICMH002905-03
Application #
7970156
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
3
Fiscal Year
2009
Total Cost
$745,598
Indirect Cost

  Institution

Name
U.S. National Institute of Mental Health
Department
Type
DUNS #
City
State
Country
Zip Code

  Publications

Lemaitre, Herve; Goldman, Aaron L; Sambataro, Fabio et al. (2012) Normal age-related brain morphometric changes: nonuniformity across cortical thickness, surface area and gray matter volume? Neurobiol Aging 33:617.e1-9
Nichols, Lisa M; Masdeu, Joseph C; Mattay, Venkata S et al. (2012) Interactive effect of apolipoprotein e genotype and age on hippocampal activation during memory processing in healthy adults. Arch Gen Psychiatry 69:804-13
Marenco, Stefano; Stein, Jason L; Savostyanova, Antonina A et al. (2012) Investigation of anatomical thalamo-cortical connectivity and FMRI activation in schizophrenia. Neuropsychopharmacology 37:499-507
Marenco, Stefano; Geramita, Matthew; van der Veen, Jan Willem et al. (2011) Genetic association of ErbB4 and human cortical GABA levels in vivo. J Neurosci 31:11628-32
Tost, Heike; Kolachana, Bhaskar; Verchinski, Beth A et al. (2011) Neurogenetic effects of OXTR rs2254298 in the extended limbic system of healthy Caucasian adults. Biol Psychiatry 70:e37-9; author reply e41-2
Tost, Heike; Kolachana, Bhaskar; Hakimi, Shabnam et al. (2010) A common allele in the oxytocin receptor gene (OXTR) impacts prosocial temperament and human hypothalamic-limbic structure and function. Proc Natl Acad Sci U S A 107:13936-41
Tost, Heike; Lipska, Barbara K; Vakkalanka, Radhakrishna et al. (2010) No effect of a common allelic variant in the reelin gene on intermediate phenotype measures of brain structure, brain function, and gene expression. Biol Psychiatry 68:105-7
Muñoz, Karen E; Meyer-Lindenberg, Andreas; Hariri, Ahmad R et al. (2010) Abnormalities in neural processing of emotional stimuli in Williams syndrome vary according to social vs. non-social content. Neuroimage 50:340-6
Sambataro, F; Murty, V P; Lemaitre, H S et al. (2010) BDNF modulates normal human hippocampal ageing [corrected]. Mol Psychiatry 15:116-8
Sambataro, Fabio; Murty, Vishnu P; Callicott, Joseph H et al. (2010) Age-related alterations in default mode network: impact on working memory performance. Neurobiol Aging 31:839-52

Showing the most recent 10 out of 33 publications