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Research ArticleBrain
Open Access

Phase White Matter Signal Abnormalities in Patients with Clinically Isolated Syndrome and Other Neurologic Disorders

J. Hagemeier, M. Heininen-Brown, T. Gabelic, T. Guttuso, N. Silvestri, D. Lichter, L.E. Fugoso, N. Bergsland, E. Carl, J.J.G. Geurts, B. Weinstock-Guttman and R. Zivadinov
American Journal of Neuroradiology October 2014, 35 (10) 1916-1923; DOI: https://doi.org/10.3174/ajnr.A3969
J. Hagemeier
aFrom the Buffalo Neuroimaging Analysis Center (J.H., M.H.-B., T. Gabelic, N.B., E.C., R.Z.)
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M. Heininen-Brown
aFrom the Buffalo Neuroimaging Analysis Center (J.H., M.H.-B., T. Gabelic, N.B., E.C., R.Z.)
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T. Gabelic
aFrom the Buffalo Neuroimaging Analysis Center (J.H., M.H.-B., T. Gabelic, N.B., E.C., R.Z.)
cDepartment of Neurology (T. Gabelic), Referral Centre for Demyelinating Disease of the Central Nervous System, University Hospital Centre Zagreb, Zagreb, Croatia
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T. Guttuso Jr
bBaird MS Center (T. Guttuso, N.S., D.L., L.E.F., B.W.-G., R.Z.), Department of Neurology, University at Buffalo, Buffalo, New York
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N. Silvestri
bBaird MS Center (T. Guttuso, N.S., D.L., L.E.F., B.W.-G., R.Z.), Department of Neurology, University at Buffalo, Buffalo, New York
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D. Lichter
bBaird MS Center (T. Guttuso, N.S., D.L., L.E.F., B.W.-G., R.Z.), Department of Neurology, University at Buffalo, Buffalo, New York
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L.E. Fugoso
bBaird MS Center (T. Guttuso, N.S., D.L., L.E.F., B.W.-G., R.Z.), Department of Neurology, University at Buffalo, Buffalo, New York
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N. Bergsland
aFrom the Buffalo Neuroimaging Analysis Center (J.H., M.H.-B., T. Gabelic, N.B., E.C., R.Z.)
dIstituto Di Ricovero e Cura a Carattere Scientifico (N.B.), Don Gnocchi Foundation, Milan, Italy
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E. Carl
aFrom the Buffalo Neuroimaging Analysis Center (J.H., M.H.-B., T. Gabelic, N.B., E.C., R.Z.)
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J.J.G. Geurts
eDepartment of Anatomy and Neurosciences (J.J.G.G.), Section of Clinical Neuroscience, VU University Medical Center, Amsterdam, the Netherlands.
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B. Weinstock-Guttman
bBaird MS Center (T. Guttuso, N.S., D.L., L.E.F., B.W.-G., R.Z.), Department of Neurology, University at Buffalo, Buffalo, New York
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R. Zivadinov
aFrom the Buffalo Neuroimaging Analysis Center (J.H., M.H.-B., T. Gabelic, N.B., E.C., R.Z.)
bBaird MS Center (T. Guttuso, N.S., D.L., L.E.F., B.W.-G., R.Z.), Department of Neurology, University at Buffalo, Buffalo, New York
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Abstract

BACKGROUND AND PURPOSE: Identifying MRI biomarkers that can differentiate multiple sclerosis patients from other neurological disorders is a subject of intense research. Our aim was to investigate phase WM signal abnormalities for their presence, prevalence, location, and diagnostic value among patients with clinically isolated syndrome and other neurologic disorders and age-, sex-, and group-matched healthy controls.

MATERIALS AND METHODS: Forty-eight patients with clinically isolated syndrome and 30 patients with other neurologic diseases and a healthy control group (n = 47) were included in the study. Subjects were scanned at 3T by using SWI-filtered phase and T2WI, with WM signal abnormalities ≥3 mm being classified.

RESULTS: Patients with clinically isolated syndrome had significantly more phase and T2 WM signal abnormalities than healthy controls (P < .001). Phase WM signal abnormalities were more prevalent among patients with clinically isolated syndrome compared with patients with other neurologic disorders (4:1 ratio), whereas T2 WM signal abnormalities were more ubiquitous with a 2:1 ratio. The presence of phase WM signal abnormalities was sensitive for clinically isolated syndrome (70.8%) and achieved a moderate-to-high specificity for differentiating patients with clinically isolated syndrome and healthy controls, patients with other neurologic disorders, and patients with other neurologic disorders of other autoimmune origin (specificity, 70%–76.7%). Combining the presence of ≥2 phase lesions with the McDonald 2005 and 2010 criteria for dissemination in space improved the specificity (90%), but not the accuracy, in differentiating patients with clinically isolated syndrome from those with other neurologic disorders. In subanalyses among patients with clinically isolated syndrome who converted to clinically definite multiple sclerosis versus those who did not within a 3-year follow-up period, converters had significantly more phase (P = .008) but not T2 or T1 WM signal abnormalities.

CONCLUSIONS: Phase WM signal abnormalities are prevalent among patients with clinically isolated syndrome. The presence of (multiple) phase WM signal abnormalities tended to be more predictive of conversion to clinically definite multiple sclerosis and was specific in differentiating patients with clinically isolated syndrome and other neurologic disorders, compared with T2 WM signal abnormalities; however, the accuracy remains similar to that of the current McDonald criteria.

ABBREVIATIONS:

CDMS
clinically definite MS
CIS
clinically isolated syndrome
DIS
dissemination in space
HC
healthy control
OND
other neurologic disorders
ROC
receiver operating characteristic
SA
signal abnormality
  • © 2014 by American Journal of Neuroradiology

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American Journal of Neuroradiology: 35 (10)
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Cite this article
J. Hagemeier, M. Heininen-Brown, T. Gabelic, T. Guttuso, N. Silvestri, D. Lichter, L.E. Fugoso, N. Bergsland, E. Carl, J.J.G. Geurts, B. Weinstock-Guttman, R. Zivadinov
Phase White Matter Signal Abnormalities in Patients with Clinically Isolated Syndrome and Other Neurologic Disorders
American Journal of Neuroradiology Oct 2014, 35 (10) 1916-1923; DOI: 10.3174/ajnr.A3969

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Phase White Matter Signal Abnormalities in Patients with Clinically Isolated Syndrome and Other Neurologic Disorders
J. Hagemeier, M. Heininen-Brown, T. Gabelic, T. Guttuso, N. Silvestri, D. Lichter, L.E. Fugoso, N. Bergsland, E. Carl, J.J.G. Geurts, B. Weinstock-Guttman, R. Zivadinov
American Journal of Neuroradiology Oct 2014, 35 (10) 1916-1923; DOI: 10.3174/ajnr.A3969
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