Deep Learning-Based Reconstruction: Model Comparison for Variable-Density GRAPPA 1H MRSI
Authors
Affiliations (1)
Affiliations (1)
- University of Texas Southwestern Medical Center
Abstract
Proton magnetic resonance spectroscopic imaging (1H MRSI) enables quantitative mapping of brain metabolites, but its clinical use remains limited by long acquisition time. The goal of this work to improve the applicability of high-resolution 1H FID-MRSI at 7T by enhancing GRAPPA-based acceleration through deep learning-driven k-space reconstruction. In particular, compared with conventional GRAPPA, MultiNet PyGRAPPA enables substantially higher in-plane acceleration while suppressing residual lipid aliasing and preserving metabolite map fidelity in non-lipid-suppressed MRSI. Building on the MultiNet PyGRAPPA framework, we introduce a comprehensive comparison of advanced machine-learning models for predicting missing k-space points. Multiple architectures--including multilayer perceptrons, convolutional neural networks, and several U-Net variants--were trained within a variable-density k-space undersampling scheme to support acceleration factors of R = 4, 6, and 7. The proposed U-Net model extends the MultiNet concept by leveraging nonlinear hierarchical feature extraction, thereby improving reconstruction fidelity while maintaining robustness to noise.The methods were evaluated in vivo using retrospectively undersampled 7T 1H FID-MRSI datasets from healthy volunteers and patients. Quantitative analyses demonstrate that the U-Net outperforms the original MultiNet approach, offering improved SNR retention rate, reduced lipid RMSE, and higher structural similarity of major metabolites. Metabolite maps reconstructed with the U-Net showed reduced lipid artifacts and improved anatomical consistency. In conclusion, integrating deep convolutional networks into GRAPPA-based k-space prediction provides a more reliable and higher-fidelity reconstruction pipeline. When combined with variable-density undersampling, this approach enables faster acquisition of high-resolution 1H MRSI without compromising spectral quality or metabolite quantification.