What question did this study set out to answer?

This research aims to evaluate how hepatic fat content and MOLLI acquisition protocols affect liver T1 estimates.

April 3, 2026Open Access

Impact of hepatic steatosis and MOLLI acquisition parameters on liver T1 estimates

Key Points

This research aims to evaluate how hepatic fat content and MOLLI acquisition protocols affect liver T1 estimates.
Participants underwent MRI at 1.5T with MOLLI acquisitions in various conditions (bSSFP and SPGR, IP, OP, FS).
A multi-echo sequence was used for obtaining proton density fat fraction (PDFF) and T2* maps.
ROI-based measurements were analyzed by three blinded readers using ICC, Bland-Altman analysis, and ANOVA for agreement and differences.
Liver PDFF varied widely, with strong agreement (ICC ≥ 0.90) between bSSFP and SPGR T1 estimates, although SPGR yielded higher values.
A significant difference was found between T1-OP and both T1-IP and T1-FS, with correlations indicating the influence of PDFF on T1 estimates.
In participants without steatosis, T1 values remained consistent across all acquisition methods.

Abstract

Abstract Purpose To evaluate the influence of hepatic fat content and sequence acquisition parameters on Modified Look-Locker Inversion Recovery (MOLLI)-based liver T1 estimates, comparing balanced steady-state free precession (bSSFP) and spoiled gradient recalled echo (SPGR) readouts under in-phase (IP), opposed-phase (OP), and fat-suppressed (FS) conditions. Methods Twenty participants (5 controls, 11 with hepatic steatosis, 4 with other chronic liver diseases; median age 15 years, range 10–28) underwent abdominal MRI at 1.5T. Six single-slice MOLLI acquisitions (bSSFP and SPGR; IP, OP, FS) were performed to obtain hepatic T1 maps. A 3D multi-echo confounder-corrected chemical shift encoded (mDIXON Quant ® ) sequence was performed to obtain proton density fat fraction (PDFF), and T2* maps. ROI-based measurements were made by three blinded readers. Agreement and mean difference among MOLLI protocols were assessed using intraclass correlation coefficients (ICC), Bland-Altman analysis, and repeated-measures ANOVA. Correlations between PDFF and T1 differences were evaluated using weighted linear regression. Numerical simulations were implemented to model fat-related effects on MOLLI T1 estimates. Results Liver PDFF ranged from 1 to 43% (median 4.6%). Agreement between bSSFP and SPGR T1 estimates was excellent (ICC ≥ 0.90), though SPGR estimated higher T1 values than bSSFP by 30–60 ms, with greater variability. T1-OP differed significantly from T1-IP and T1-FS (both p < 0.0001) and showed significant PDFF-related mean difference, in line with simulation results, while T1-FS and T1-IP estimates showed excellent agreement (ICC ≥ 0.89). Regression analysis showed that bSSFP T1-OP correlated very strongly with PDFF ( r = 0.81; +7.8 ms/%PDFF), whereas T1-IP showed a strong negative correlation ( r = − 0.79; − 5.0 ms/%PDFF), and T1-FS demonstrated only a moderate negative correlation ( r =-0.48; -3.1ms/%PDFF). SPGR based T1 estimates exhibited similar correlations with PDFF. In participants without steatosis, T1 values were consistent across all acquisitions. Conclusion Liver MOLLI T1 estimates are strongly influenced by hepatic fat content and acquisition parameters, particularly for OP acquisitions. IP and FS MOLLI acquisitions provide more reliable estimates across fat fractions. These findings support prioritization of IP or FS strategies in clinical and research liver T1 mapping protocols and underscore the need for fat-corrected or water-specific approaches.

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