Simultaneous T1, T2, and T1? cardiac magnetic resonance fingerprinting for contrast agentfree myocardial tissue characterization
Revista : Magnetic Resonance in MedicineTipo de publicación : ISI Ir a publicación
Abstract
Purpose
To develop a simultaneous T1, T2, and T1? cardiac magnetic resonance fingerprinting (MRF) approach to enable comprehensive contrast agentfree myocardial tissue characterization in a single breath-hold scan.
Methods
A 2D gradient-echo electrocardiogram-triggered cardiac MRF sequence with low flip angles, varying magnetization preparation, and spiral trajectory was acquired at 1.5 T to encode T1, T2, and T1? simultaneously. The MRF images were reconstructed using low-rank inversion, regularized with a multicontrast patch-based higher-order reconstruction. Parametric maps were generated and matched in the singular value domain to extended phase graphbased dictionaries. The proposed approach was tested in phantoms and 10 healthy subjects and compared against conventional methods in terms of coefficients of determination and best fits for the phantom study, and in terms of Bland-Altman agreement, average values and coefficient of variation of T1, T2, and T1? for the healthy subjects study.
Results
The T1, T2, and T1? MRF values showed excellent correlation with conventional spin-echo and clinical mapping methods in phantom studies (r2 > 0.97). Measured MRF values in myocardial tissue (mean ± SD) were 1133 ± 33 ms, 38.8 ± 3.5 ms, and 52.0 ± 4.0 ms for T1, T2 and T1?, respectively, against 1053 ± 47 ms, 50.4 ± 3.9 ms, and 55.9 ± 3.3 ms for T1 modified Look-Locker inversion imaging, T2 gradient and spin echo, and T1? turbo field echo, respectively.
Conclusion
A cardiac MRF approach for simultaneous quantification of myocardial T1, T2, and T1? in a single breath-hold MR scan of about 16 seconds has been proposed. The approach has been investigated in phantoms and healthy subjects showing good agreement with reference spin echo measurements and conventional clinical maps.