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Research ArticleFunctional

MR Spectroscopy Findings in Early Stages of Motor Neuron Disease

M.M. van der Graaff, C. Lavini, E.M. Akkerman, Ch.B. Majoie, A.J. Nederveen, A.H. Zwinderman, F. Brugman, L.H. van den Berg, J.M.B.V. de Jong and M. de Visser
American Journal of Neuroradiology November 2010, 31 (10) 1799-1806; DOI: https://doi.org/10.3174/ajnr.A2217
M.M. van der Graaff
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C. Lavini
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E.M. Akkerman
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Ch.B. Majoie
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A.J. Nederveen
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A.H. Zwinderman
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F. Brugman
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L.H. van den Berg
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J.M.B.V. de Jong
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M. de Visser
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Abstract

BACKGROUND AND PURPOSE: Upper motor neuron degeneration varies in different phenotypes of MND. We used single-voxel MR spectroscopy of the primary motor cortex to detect corticomotoneuron degeneration and glial hyperactivity in different phenotypes of MND with a relatively short disease duration, contributing to further delineation of the phenotypes.

MATERIALS AND METHODS: We prospectively included patients with ALS-B, ALS-L, and PMA and compared their data with those of patients with PLS and healthy controls. Each cohort consisted of 12 individuals. Disease duration was <1 year in ALS and PMA, but longer in PLS by definition. Follow-up examination was at 6 months. We measured ALSFRS-R, finger- and foot-tapping speed, and levels of the following: 1) NAAx, 2) mIns, and 3) Glx in the primary motor cortex.

RESULTS: At baseline, we found significantly decreased NAAx levels and increased mIns levels in PLS. Levels of NAAx and mIns in patients with ALS-L and ALS-B were not significantly different from those in controls, but NAAx levels were significantly lower compared with those in PMA. At follow-up, only in PMA was a decrease of NAAx demonstrated. Glx levels varied widely in all groups. Levels of NAAx and mIns correlated well with clinical variables.

CONCLUSIONS: Metabolite changes suggest neuronal dysfunction and active glial involvement in PLS. The corticomotoneuron is affected in early ALS-B and ALS-L, but at a later stage also in PMA. MR spectroscopy data are useful to obtain insight into the disease process at the level of the upper motor neuron in various phenotypes of MND.

Abbreviations

ALS
amyotrophic lateral sclerosis
ALS-B
bulbar onset ALS
ALSFRS-R
Revised ALS Functional Rating Scale
ALS-L
limb-onset ALS
CI
confidence interval
Glx
glutamate + glutamine
L
left
mIns
myo-inositol
MND
motor neuron disease
MRS
MR spectroscopy
NA
not applicable
NAA
N-acetylaspartate
NAAx
N-acetylaspartate + N-acetyl aspartylglutamate
NS
not significant
PLS
primary lateral sclerosis
PMA
progressive muscular atrophy
R
right
ROC
receiver operating characteristic analysis
VC
vital capacity
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American Journal of Neuroradiology: 31 (10)
American Journal of Neuroradiology
Vol. 31, Issue 10
1 Nov 2010
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Cite this article
M.M. van der Graaff, C. Lavini, E.M. Akkerman, Ch.B. Majoie, A.J. Nederveen, A.H. Zwinderman, F. Brugman, L.H. van den Berg, J.M.B.V. de Jong, M. de Visser
MR Spectroscopy Findings in Early Stages of Motor Neuron Disease
American Journal of Neuroradiology Nov 2010, 31 (10) 1799-1806; DOI: 10.3174/ajnr.A2217

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MR Spectroscopy Findings in Early Stages of Motor Neuron Disease
M.M. van der Graaff, C. Lavini, E.M. Akkerman, Ch.B. Majoie, A.J. Nederveen, A.H. Zwinderman, F. Brugman, L.H. van den Berg, J.M.B.V. de Jong, M. de Visser
American Journal of Neuroradiology Nov 2010, 31 (10) 1799-1806; DOI: 10.3174/ajnr.A2217
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