AOD Effects and Consequences Clinical Trial
Official title:
Spectroscopic Imaging of GABA and Glutamate/Glutamine in Healthy Volunteers at 4T: A Double Blind, Crossover Drug Challenge Study
An advanced technique for rapid magnetic resonance proton spectroscopic imaging (1H-MRSI) will be employed in a drug challenge study in healthy volunteers to spatially map and measure acute changes in the brain chemicals GABA, glutamate and glutamine after administration of a drug. Three condition will be tested in a double-blind fashion, i)depressant, ii)stimulant, iii)placebo. It is hypothesized that unique and reproducible spatial and directional metabolic response patterns will be observed, unique to each condition within the brain.
Proton magnetic resonance spectroscopy (1H MRS) is a powerful tool for assessing
neurochemistry non-invasively in vivo. However, the primary shortcoming in most studies is
the lack of spatial coverage afforded by the typical single-voxel design. Limits on
participant tolerance and financial resources restrict single-voxel studies to an
examination of one or two carefully chosen voxels per scan, thus inadequately addressing the
question of focal vs. global pathophysiology. A secondary shortcoming is that most studies
report on either GABA or glutamate-glutamine (Glu-Gln) due to the technically demanding
spectral-editing techniques that must be implemented in order to resolve and quantify those
metabolites with any accuracy.
1H MRS imaging (MRSI) can partially overcome these limitations by providing a global picture
of brain chemistry rather than just the focal snapshot afforded by the single-voxel design.
However, the scan time necessary for collecting enough data for adequate spatial resolution
and signal-to-noise, particularly if also using specialized spectral-editing techniques, is
still too lengthy. We recently developed a method that combines Spectroscopic Imaging with
the MEGAPRESS-based difference-editing acquisition for optimal GABA detection as well as for
optimal detection of Glu and Gln. This MEGACSI sequence will permit us to obtain the maximum
amount of neurochemical information in a clinically sound scan time, while using the current
state-of-the-art MRS editing methods for optimal detection of GABA, Glu, and Gln.
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Intervention Model: Single Group Assignment, Masking: Double Blind (Subject, Investigator), Primary Purpose: Basic Science
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