Literature DB >> 25196714

Automated whole-brain N-acetylaspartate proton MRS quantification.

Brian J Soher1, William E Wu, Assaf Tal, Pippa Storey, Ke Zhang, James S Babb, Ivan I Kirov, Yvonne W Lui, Oded Gonen.   

Abstract

Concentration of the neuronal marker, N-acetylaspartate (NAA), a quantitative metric for the health and density of neurons, is currently obtained by integration of the manually defined peak in whole-head proton ((1) H)-MRS. Our goal was to develop a full spectral modeling approach for the automatic estimation of the whole-brain NAA concentration (WBNAA) and to compare the performance of this approach with a manual frequency-range peak integration approach previously employed. MRI and whole-head (1) H-MRS from 18 healthy young adults were examined. Non-localized, whole-head (1) H-MRS obtained at 3 T yielded the NAA peak area through both manually defined frequency-range integration and the new, full spectral simulation. The NAA peak area was converted into an absolute amount with phantom replacement and normalized for brain volume (segmented from T1 -weighted MRI) to yield WBNAA. A paired-sample t test was used to compare the means of the WBNAA paradigms and a likelihood ratio test used to compare their coefficients of variation. While the between-subject WBNAA means were nearly identical (12.8 ± 2.5 mm for integration, 12.8 ± 1.4 mm for spectral modeling), the latter's standard deviation was significantly smaller (by ~50%, p = 0.026). The within-subject variability was 11.7% (±1.3 mm) for integration versus 7.0% (±0.8 mm) for spectral modeling, i.e., a 40% improvement. The (quantifiable) quality of the modeling approach was high, as reflected by Cramer-Rao lower bounds below 0.1% and vanishingly small (experimental - fitted) residuals. Modeling of the whole-head (1) H-MRS increases WBNAA quantification reliability by reducing its variability, its susceptibility to operator bias and baseline roll, and by providing quality-control feedback. Together, these enhance the usefulness of the technique for monitoring the diffuse progression and treatment response of neurological disorders.
Copyright © 2014 John Wiley & Sons, Ltd.

Entities:  

Keywords:  MRI segmentation; MRS quantification; N-acetylaspartate (NAA); whole-brain NAA concentration (WBNAA)

Mesh:

Substances:

Year:  2014        PMID: 25196714      PMCID: PMC4212831          DOI: 10.1002/nbm.3185

Source DB:  PubMed          Journal:  NMR Biomed        ISSN: 0952-3480            Impact factor:   4.044


  59 in total

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Review 8.  N-acetylaspartate in the vertebrate brain: metabolism and function.

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2.  Quantifying global-brain metabolite level changes with whole-head proton MR spectroscopy at 3T.

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3.  Whole brain neuronal abnormalities in focal epilepsy quantified with proton MR spectroscopy.

Authors:  Ivan I Kirov; Ruben Kuzniecky; Hoby P Hetherington; Brian J Soher; Matthew S Davitz; James S Babb; Heath R Pardoe; Jullie W Pan; Oded Gonen
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4.  Global brain metabolic quantification with whole-head proton MRS at 3 T.

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5.  Aberrant interactions of peripheral measures and neurometabolites with lipids in complex regional pain syndrome using magnetic resonance spectroscopy: A pilot study.

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  5 in total

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