Objectives: Phosphorus-31 magnetic resonance spectroscopic imaging (P-MRSI) is a non-invasive tool for assessing cellular high-energy metabolism in-vivo. However, its acquisition suffers from a low sensitivity, which necessitates large voxel sizes or multiple averages to achieve an acceptable signal-to-noise ratio (SNR), resulting in long scan times.

Materials And Methods: To overcome these limitations, we propose an acquisition and reconstruction scheme for FID-MRSI sequences. Specifically, we employed Compressed Sensing (CS) and Low-Rank (LR) with Total Generalized Variation (TGV) regularization in a combined CS-LR framework. Additionally, we used a novel approach to k-space undersampling that utilizes distinct pseudo-random patterns for each average. To evaluate the proposed method's performance, we performed a retrospective analysis on healthy volunteers' brains and ex-vivo perfused kidneys.

Results: The presented method effectively improves the SNR two-to-threefold while preserving spectral and spatial quality even with threefold acceleration. We were able to recover signal attenuation of anatomical information, and the SNR improvement was obtained while maintaining the metabolites peaks linewidth.

Conclusions: We presented a novel combined CS-LR acceleration and reconstruction method for FID-MRSI sequences, utilizing a unique approach to k-space undersampling. Our proposed method has demonstrated promising results in enhancing the SNR making it applicable for reducing acquisition time.

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Source
http://dx.doi.org/10.1007/s10334-024-01218-yDOI Listing

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