Literature DB >> 22578557

Magnetic resonance Spectroscopy with Linear Algebraic Modeling (SLAM) for higher speed and sensitivity.

Yi Zhang1, Refaat E Gabr, Michael Schär, Robert G Weiss, Paul A Bottomley.   

Abstract

Speed and signal-to-noise ratio (SNR) are critical for localized magnetic resonance spectroscopy (MRS) of low-concentration metabolites. Matching voxels to anatomical compartments a priori yields better SNR than the spectra created by summing signals from constituent chemical-shift-imaging (CSI) voxels post-acquisition. Here, a new method of localized Spectroscopy using Linear Algebraic Modeling (SLAM) is presented, that can realize this additional SNR gain. Unlike prior methods, SLAM generates spectra from C signal-generating anatomic compartments utilizing a CSI sequence wherein essentially only the C central k-space phase-encoding gradient steps with highest SNR are retained. After MRI-based compartment segmentation, the spectra are reconstructed by solving a sub-set of linear simultaneous equations from the standard CSI algorithm. SLAM is demonstrated with one-dimensional CSI surface coil phosphorus MRS in phantoms, the human leg and the heart on a 3T clinical scanner. Its SNR performance, accuracy, sensitivity to registration errors and inhomogeneity, are evaluated. Compared to one-dimensional CSI, SLAM yielded quantitatively the same results 4-times faster in 24 cardiac patients and healthy subjects. SLAM is further extended with fractional phase-encoding gradients that optimize SNR and/or minimize both inter- and intra-compartmental contamination. In proactive cardiac phosphorus MRS of six healthy subjects, both SLAM and fractional-SLAM (fSLAM) produced results indistinguishable from CSI while preserving SNR gains of 36-45% in the same scan-time. Both SLAM and fSLAM are simple to implement and reduce the minimum scan-time for CSI, which otherwise limits the translation of higher SNR achievable at higher field strengths to faster scanning.
Copyright © 2012 Elsevier Inc. All rights reserved.

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Year:  2012        PMID: 22578557      PMCID: PMC3381802          DOI: 10.1016/j.jmr.2012.03.008

Source DB:  PubMed          Journal:  J Magn Reson        ISSN: 1090-7807            Impact factor:   2.229


  24 in total

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2.  Problems and expediencies in human 31P spectroscopy. The definition of localized volumes, dealing with saturation and the technique-dependence of quantification.

Authors:  P A Bottomley; C J Hardy; P B Roemer; R G Weiss
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9.  Concentrations of human cardiac phosphorus metabolites determined by SLOOP 31P NMR spectroscopy.

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10.  Localized spectroscopy from anatomically matched compartments: improved sensitivity and localization for cardiac 31P MRS in humans.

Authors:  R Löffler; R Sauter; H Kolem; A Haase; M von Kienlin
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  16 in total

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3.  Spectroscopy with linear algebraic modeling (SLAM): speed and quantification in brain tumor studies.

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Authors:  Yi Zhang; Xiaoyang Liu; Jinyuan Zhou; Paul A Bottomley
Journal:  Proc Int Soc Magn Reson Med Sci Meet Exhib Int Soc Magn Reson Med Sci Meet Exhib       Date:  2017-04

6.  Chemical exchange saturation transfer (CEST) imaging with fast variably-accelerated sensitivity encoding (vSENSE).

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Journal:  Magn Reson Med       Date:  2016-07-01       Impact factor: 4.668

7.  Highly accelerated chemical exchange saturation transfer (CEST) measurements with linear algebraic modeling.

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8.  Minimizing lipid signal bleed in brain (1) H chemical shift imaging by post-acquisition grid shifting.

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