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March 13, 2013Article

Distinction of seropositive NMO spectrum disorder and MS brain lesion distribution

Lucy Matthews, Rita Marasco, Mark Jenkinson, Wilhelm Küker, Sebastian Luppe, Maria Isabel Leite, Antonio Giorgio, Nicola De Stefano, Neil Robertson, Heidi Johansen-Berg, Nikos Evangelou, Jacqueline Palace
First published March 13, 2013, DOI: https://doi.org/10.1212/WNL.0b013e3182887957
Lucy Matthews
From the Nuffield Department of Clinical Neurosciences (L.M., R.M., M.J., W.K., M.I.L., H.J.-B., J.P.), University of Oxford; Institute of Psychological Medicine and Clinical Neurosciences (S.L., N.R.), University of Cardiff; Department of Neurological and Behavioural Sciences (A.G., N.D.S.), University of Siena; and Faculty of Medicine & Health Sciences (N.E.), University of Nottingham, UK.
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Rita Marasco
From the Nuffield Department of Clinical Neurosciences (L.M., R.M., M.J., W.K., M.I.L., H.J.-B., J.P.), University of Oxford; Institute of Psychological Medicine and Clinical Neurosciences (S.L., N.R.), University of Cardiff; Department of Neurological and Behavioural Sciences (A.G., N.D.S.), University of Siena; and Faculty of Medicine & Health Sciences (N.E.), University of Nottingham, UK.
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Mark Jenkinson
From the Nuffield Department of Clinical Neurosciences (L.M., R.M., M.J., W.K., M.I.L., H.J.-B., J.P.), University of Oxford; Institute of Psychological Medicine and Clinical Neurosciences (S.L., N.R.), University of Cardiff; Department of Neurological and Behavioural Sciences (A.G., N.D.S.), University of Siena; and Faculty of Medicine & Health Sciences (N.E.), University of Nottingham, UK.
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Wilhelm Küker
From the Nuffield Department of Clinical Neurosciences (L.M., R.M., M.J., W.K., M.I.L., H.J.-B., J.P.), University of Oxford; Institute of Psychological Medicine and Clinical Neurosciences (S.L., N.R.), University of Cardiff; Department of Neurological and Behavioural Sciences (A.G., N.D.S.), University of Siena; and Faculty of Medicine & Health Sciences (N.E.), University of Nottingham, UK.
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Sebastian Luppe
From the Nuffield Department of Clinical Neurosciences (L.M., R.M., M.J., W.K., M.I.L., H.J.-B., J.P.), University of Oxford; Institute of Psychological Medicine and Clinical Neurosciences (S.L., N.R.), University of Cardiff; Department of Neurological and Behavioural Sciences (A.G., N.D.S.), University of Siena; and Faculty of Medicine & Health Sciences (N.E.), University of Nottingham, UK.
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Maria Isabel Leite
From the Nuffield Department of Clinical Neurosciences (L.M., R.M., M.J., W.K., M.I.L., H.J.-B., J.P.), University of Oxford; Institute of Psychological Medicine and Clinical Neurosciences (S.L., N.R.), University of Cardiff; Department of Neurological and Behavioural Sciences (A.G., N.D.S.), University of Siena; and Faculty of Medicine & Health Sciences (N.E.), University of Nottingham, UK.
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Antonio Giorgio
From the Nuffield Department of Clinical Neurosciences (L.M., R.M., M.J., W.K., M.I.L., H.J.-B., J.P.), University of Oxford; Institute of Psychological Medicine and Clinical Neurosciences (S.L., N.R.), University of Cardiff; Department of Neurological and Behavioural Sciences (A.G., N.D.S.), University of Siena; and Faculty of Medicine & Health Sciences (N.E.), University of Nottingham, UK.
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Nicola De Stefano
From the Nuffield Department of Clinical Neurosciences (L.M., R.M., M.J., W.K., M.I.L., H.J.-B., J.P.), University of Oxford; Institute of Psychological Medicine and Clinical Neurosciences (S.L., N.R.), University of Cardiff; Department of Neurological and Behavioural Sciences (A.G., N.D.S.), University of Siena; and Faculty of Medicine & Health Sciences (N.E.), University of Nottingham, UK.
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Neil Robertson
From the Nuffield Department of Clinical Neurosciences (L.M., R.M., M.J., W.K., M.I.L., H.J.-B., J.P.), University of Oxford; Institute of Psychological Medicine and Clinical Neurosciences (S.L., N.R.), University of Cardiff; Department of Neurological and Behavioural Sciences (A.G., N.D.S.), University of Siena; and Faculty of Medicine & Health Sciences (N.E.), University of Nottingham, UK.
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Heidi Johansen-Berg
From the Nuffield Department of Clinical Neurosciences (L.M., R.M., M.J., W.K., M.I.L., H.J.-B., J.P.), University of Oxford; Institute of Psychological Medicine and Clinical Neurosciences (S.L., N.R.), University of Cardiff; Department of Neurological and Behavioural Sciences (A.G., N.D.S.), University of Siena; and Faculty of Medicine & Health Sciences (N.E.), University of Nottingham, UK.
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Nikos Evangelou
From the Nuffield Department of Clinical Neurosciences (L.M., R.M., M.J., W.K., M.I.L., H.J.-B., J.P.), University of Oxford; Institute of Psychological Medicine and Clinical Neurosciences (S.L., N.R.), University of Cardiff; Department of Neurological and Behavioural Sciences (A.G., N.D.S.), University of Siena; and Faculty of Medicine & Health Sciences (N.E.), University of Nottingham, UK.
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Jacqueline Palace
From the Nuffield Department of Clinical Neurosciences (L.M., R.M., M.J., W.K., M.I.L., H.J.-B., J.P.), University of Oxford; Institute of Psychological Medicine and Clinical Neurosciences (S.L., N.R.), University of Cardiff; Department of Neurological and Behavioural Sciences (A.G., N.D.S.), University of Siena; and Faculty of Medicine & Health Sciences (N.E.), University of Nottingham, UK.
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Full PDF
Citation
Distinction of seropositive NMO spectrum disorder and MS brain lesion distribution
Lucy Matthews, Rita Marasco, Mark Jenkinson, Wilhelm Küker, Sebastian Luppe, Maria Isabel Leite, Antonio Giorgio, Nicola De Stefano, Neil Robertson, Heidi Johansen-Berg, Nikos Evangelou, Jacqueline Palace
Neurology Mar 2013, 10.1212/WNL.0b013e3182887957; DOI: 10.1212/WNL.0b013e3182887957

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Abstract

Objective: Neuromyelitis optica and its spectrum disorder (NMOSD) can present similarly to relapsing-remitting multiple sclerosis (RRMS). Using a quantitative lesion mapping approach, this research aimed to identify differences in MRI brain lesion distribution between aquaporin-4 antibody–positive NMOSD and RRMS, and to test their diagnostic potential.

Methods: Clinical brain MRI sequences for 44 patients with aquaporin-4 antibody–positive NMOSD and 50 patients with RRMS were examined for the distribution and morphology of brain lesions. T2 lesion maps were created for each subject allowing the quantitative comparison of the 2 conditions with lesion probability and voxel-wise analysis.

Results: Sixty-three percent of patients with NMOSD had brain lesions and of these 27% were diagnostic of multiple sclerosis. Patients with RRMS were significantly more likely to have lesions adjacent to the body of the lateral ventricle than patients with NMOSD. Direct comparison of the probability distributions and the morphologic attributes of the lesions in each group identified criteria of “at least 1 lesion adjacent to the body of the lateral ventricle and in the inferior temporal lobe; or the presence of a subcortical U-fiber lesion; or a Dawson's finger-type lesion,” which could distinguish patients with multiple sclerosis from those with NMOSD with 92% sensitivity, 96% specificity, 98% positive predictive value, and 86% negative predictive value.

Conclusion: Careful inspection of the distribution and morphology of MRI brain lesions can distinguish RRMS and NMOSD.

  • Received June 12, 2012.
  • Accepted December 12, 2012.
  • © 2013 American Academy of Neurology

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Letters: Rapid online correspondence

  • 'Dawson's fingers' and Neuromyelitis Optica
    • Ilya Kister, Neurologist, NYU School of Medicine, NYilya.kister@gmail.com
    • Ilya Kister, Yulin Ge, Joseph Herbert (New York, USA); Tim Sinnecker, Jens Wuerfel, Friedemann Paul (Berlin, Germany)
    Submitted May 07, 2013

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