Tissue sodium concentration and sodium T 1 mapping of the human brain at 3 T using a Variable Flip Angle method

The state-of-the-art method to quantify sodium concentrations in vivo consists in a fully relaxed 3D spin-density (SD) weighted acquisition. Nevertheless, most sodium MRI clinical studies use short-TR SD acquisitions to reduce acquisition durations. We present a clinically viable implementation of t...

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Bibliographic Details
Published in:Magnetic resonance imaging Vol. 58; p. 116
Main Authors: Coste, Arthur, Boumezbeur, Fawzi, Vignaud, Alexandre, Madelin, Guillaume, Reetz, Kathrin, Le Bihan, Denis, Rabrait-Lerman, Cécile, Romanzetti, Sandro
Format: Journal Article
Language:English
Published: Netherlands 01.05.2019
Subjects:
Adult
Algorithms
Brain - diagnostic imaging
Brain Mapping - methods
Computer Simulation
Female
Fourier Analysis
Healthy Volunteers
Humans
Image Processing, Computer-Assisted - methods
Magnetic Resonance Imaging
Magnetics
Male
Middle Aged
Models, Statistical
Phantoms, Imaging
Sodium - chemistry
Software
Young Adult
Variable Flip Angle
Tissue sodium concentration
T mapping
Na MRI
ISSN:1873-5894
Online Access:Get full text
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Summary:The state-of-the-art method to quantify sodium concentrations in vivo consists in a fully relaxed 3D spin-density (SD) weighted acquisition. Nevertheless, most sodium MRI clinical studies use short-TR SD acquisitions to reduce acquisition durations. We present a clinically viable implementation of the Variable Flip Angle (VFA) method for robust and clinically viable quantification of total sodium concentration (TSC) and longitudinal relaxation rates in vivo in human brain at 3 T. Two non-Cartesian steady-state spoiled ultrashort echo time (UTE) scans, performed at optimized flip angles, repetition time and pulse length determined under specific absorption rate constraints, are used to simultaneously compute T and total sodium concentration (TSC) maps using the VFA method. Images are reconstructed using the non-uniform Fast Fourier Transform algorithm and TSC maps are corrected for possible inhomogeneity of coil transmission and reception profiles. Fractioned acquisitions are used to correct for potential patient motion. TSC quantifications obtained using the VFA method are validated at first in comparison with a fully-relaxed SD acquisition in a calibration phantom. The robustness of similar VFA acquisitions are compared to the short-TR SD approach in vivo on seven healthy volunteers. The VFA method resulted in consistent TSC and T estimates across our cohort of healthy subjects, with mean TSC of 38.1 ± 5.0 mmol/L and T of 39.2 ± 4.4 ms. These results are in agreement with previously reported values in literature TSC estimations and with the predictions of a 2-compartment model. However, the short-TR SD acquisition systematically underestimated the sodium concentration with a mean TSC of 31 ± 4.5 mmol/L. The VFA method can be applied successfully to image sodium at 3 T in about 20 min and provides robust and intrinsically T -corrected TSC maps.
ISSN:1873-5894
DOI:10.1016/j.mri.2019.01.015