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MEGA‐PRESS of GABA+: Influences of acquisition parameters
Author(s) -
Deelchand Dinesh K.,
Marjańska Małgorzata,
Henry PierreGilles,
Terpstra Melissa
Publication year - 2021
Publication title -
nmr in biomedicine
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.278
H-Index - 114
eISSN - 1099-1492
pISSN - 0952-3480
DOI - 10.1002/nbm.4199
Subject(s) - signal (programming language) , spectroscopy , computer science , perspective (graphical) , relaxation (psychology) , chemistry , nuclear magnetic resonance , biological system , physics , neuroscience , artificial intelligence , biology , quantum mechanics , programming language
γ‐aminobutyric acid (GABA) was the first molecule that was edited with MEGA‐PRESS. GABA edited spectroscopy is challenged by limited selectivity of editing pulses. Coediting of resonances from macromolecules (MM) is the greatest single limitation of GABA edited spectroscopy. In this contribution, relative signal contributions from GABA, MM and homocarnosine to the total MEGA‐PRESS edited signal at ~3 ppm, i.e., GABA+, are simulated at 3 tesla using several acquisition schemes. The base scheme is modeled after those currently supplied by vendors: it uses typical pulse shapes and lengths, it minimizes the first echo time (TE), and the delay between the editing pulses is kept at TE/2. Edited spectra are simulated for imperfect acquisition parameters such as incorrect frequency, larger chemical shift displacement, incorrect transmit B 1 ‐field calibration for localization and editing pulses, and longer TE. An alternative timing scheme and longer editing pulses are also considered. Additional simulations are performed for symmetric editing around the MM frequency to suppress the MM signal. The relative influences of these acquisition parameters on the constituents of GABA+ are examined from the perspective of modern experimental designs for investigating brain GABA concentration differences in healthy and diseased humans. Other factors that influence signal contributions, such as T 1 and T 2 relaxation times are also considered.

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