Free-breathing simultaneous water-fat separation and T1 mapping of the whole liver (SWALI) with isotropic resolution using 3D golden-angle radial trajectory

Background: Conventional liver T1 mapping techniques are typically performed under breath-holding conditions; they have limited slice coverage and often rely on multiple acquisitions. Furthermore, liver fat affects the accuracy of T1 quantification. Therefore, we aim to propose a free-breathing technique for simultaneous water-fat separation and T1 mapping of the whole liver (SWALI) in a single scan.Methods: The proposed SWALI sequence included an inversion recovery (IR) preparation pulse followed by a series of multiecho three-dimensional (3D) golden-angle radial acquisitions. For each echo time (TE), a series of images containing a mix of water and fat were reconstructed using a sliding window method. For each inversion time (TI), water and fat were separated, and then water and fat T1 estimation was conducted. The fat fraction (FF) was calculated based on the last TI image. The FF and water T1 quantification accuracy were compared with the gold standard sequences in the phantom. The in vivo feasibility was tested in 9 healthy volunteers, 2 patients with fatty liver, and 3 patients with hepatocellular carcinoma (HCC). The reproducibility was evaluated in the patients with fatty liver and in the healthy volunteers.Results: The mean FF and the mean water T1 values obtained by the SWALI sequence showed good agreements with chemical shift-encoded magnetic resonance imaging (CSE-MRI; r=0.998; P<0.001) and fat-suppressed (FS) IR-spin echo (SE; r=0.997; P<0.001) in the phantom. For the patients with fatty liver and the healthy volunteers, the SWALI sequence showed no significant difference with CSE-MRI in FF quantification (P=0.53). In T1 quantification, comparable T1 values were obtained with the SWALI sequence and modified Look-Locker inversion recovery (MOLLI; P=0.10) in healthy volunteers, while the water T1 estimated by the SWALI sequence was significantly lower than the water-fat compound T1 estimated by MOLLI (P<0.001) in patients with fatty liver. In the reproducibility study, the intraclass correlation coefficients (ICCs) for the estimated FF and water T1 were 0.997 and 0.943, respectively. Water T1 of the patients with HCC calculated using the SWALI sequence showed a significant reduction after the contrast administration (P<0.001). Conclusions: Free-breathing water-fat separation and T1 mapping of the whole liver with 2.5 mm isotropic spatial resolution were achieved simultaneously using the SWALI sequence in a 5-min scan.