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Research ArticleAdult Brain
Open Access

Feasibility of Brain Atrophy Measurement in Clinical Routine without Prior Standardization of the MRI Protocol: Results from MS-MRIUS, a Longitudinal Observational, Multicenter Real-World Outcome Study in Patients with Relapsing-Remitting MS

R. Zivadinov, N. Bergsland, J.R. Korn, M.G. Dwyer, N. Khan, J. Medin, J.C. Price, B. Weinstock-Guttman and D. Silva on behalf of the MS-MRIUS Study Group
American Journal of Neuroradiology February 2018, 39 (2) 289-295; DOI: https://doi.org/10.3174/ajnr.A5442
R. Zivadinov
aFrom the Department of Neurology (R.Z., N.B., M.G.D.), Buffalo Neuroimaging Analysis Center
cTranslational Imaging Center at Clinical and Translational Science Institute (R.Z.), University of Buffalo, State University of New York, Buffalo, New York
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N. Bergsland
aFrom the Department of Neurology (R.Z., N.B., M.G.D.), Buffalo Neuroimaging Analysis Center
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J.R. Korn
dQuintilesIMS (J.R.K.), Burlington, Massachusetts
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M.G. Dwyer
aFrom the Department of Neurology (R.Z., N.B., M.G.D.), Buffalo Neuroimaging Analysis Center
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N. Khan
eQuintilesIMS (N.K., J.C.P.), Basel, Switzerland
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J. Medin
fNovartis Pharmaceuticals AG (J.M., D.S.), Basel, Switzerland.
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J.C. Price
eQuintilesIMS (N.K., J.C.P.), Basel, Switzerland
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B. Weinstock-Guttman
bDepartment of Neurology (B.W.-G.), Jacobs Multiple Sclerosis Center, Jacobs School of Medicine and Biomedical Sciences, University at Buffalo, State University of New York, Buffalo, New York
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D. Silva
fNovartis Pharmaceuticals AG (J.M., D.S.), Basel, Switzerland.
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Abstract

BACKGROUND AND PURPOSE: Feasibility of brain atrophy measurement in patients with MS in clinical routine, without prior standardization of the MRI protocol, is unknown. Our aim was to investigate the feasibility of brain atrophy measurement in patients with MS in clinical routine.

MATERIALS AND METHODS: Multiple Sclerosis and Clinical Outcome and MR Imaging in the United States (MS-MRIUS) is a multicenter (33 sites), retrospective study that included patients with relapsing-remitting MS who began treatment with fingolimod. Brain MR imaging examinations previously acquired at the baseline and follow-up periods on 1.5T or 3T scanners with no prior standardization were used, to resemble a real-world situation. Brain atrophy outcomes included the percentage brain volume change measured by structural image evaluation with normalization of atrophy on 2D-T1-weighted imaging and 3D-T1WI and the percentage lateral ventricle volume change, measured by VIENA on 2D-T1WI and 3D-T1WI and NeuroSTREAM on T2-fluid-attenuated inversion recovery examinations.

RESULTS: A total of 590 patients, followed for 16 months, were included. There were 585 (99.2%) T2-FLAIR, 425 (72%) 2D-T1WI, and 166 (28.2%) 3D-T1WI longitudinal pairs of examinations available. Excluding MR imaging examinations with scanner changes, the analyses were available on 388 (65.8%) patients on T2-FLAIR for the percentage lateral ventricle volume change, 259 and 257 (43.9% and 43.6%, respectively) on 2D-T1WI for the percentage brain volume change and the percentage lateral ventricle volume change, and 110 (18.6%) on 3D-T1WI for the percentage brain volume change and percentage lateral ventricle volume change. The median annualized percentage brain volume change was −0.31% on 2D-T1WI and −0.38% on 3D-T1WI. The median annualized percentage lateral ventricle volume change was 0.95% on 2D-T1WI, 1.47% on 3D-T1WI, and 0.90% on T2-FLAIR.

CONCLUSIONS: Brain atrophy was more readily assessed by estimating the percentage lateral ventricle volume change on T2-FLAIR compared with the percentage brain volume change or percentage lateral ventricle volume change using 2D- or 3D-T1WI in this observational retrospective study. Although measurement of the percentage brain volume change on 3D-T1WI remains the criterion standard and should be encouraged in future prospective studies, T2-FLAIR–derived percentage lateral ventricle volume change may be a more feasible surrogate when historical or other practical constraints limit the availability of percentage brain volume change on 3D-T1WI.

ABBREVIATIONS:

MS-MRIUS
Multiple Sclerosis and Clinical Outcome and MR Imaging in the United States
PBVC
percentage brain volume change
PLVVC
percentage lateral ventricle volume change
RRMS
relapsing-remitting MS
SIENA
structural image evaluation with normalization of atrophy
  • © 2018 by American Journal of Neuroradiology

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American Journal of Neuroradiology: 39 (2)
American Journal of Neuroradiology
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1 Feb 2018
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R. Zivadinov, N. Bergsland, J.R. Korn, M.G. Dwyer, N. Khan, J. Medin, J.C. Price, B. Weinstock-Guttman, D. Silva
Feasibility of Brain Atrophy Measurement in Clinical Routine without Prior Standardization of the MRI Protocol: Results from MS-MRIUS, a Longitudinal Observational, Multicenter Real-World Outcome Study in Patients with Relapsing-Remitting MS
American Journal of Neuroradiology Feb 2018, 39 (2) 289-295; DOI: 10.3174/ajnr.A5442

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Feasibility of Brain Atrophy Measurement in Clinical Routine without Prior Standardization of the MRI Protocol: Results from MS-MRIUS, a Longitudinal Observational, Multicenter Real-World Outcome Study in Patients with Relapsing-Remitting MS
R. Zivadinov, N. Bergsland, J.R. Korn, M.G. Dwyer, N. Khan, J. Medin, J.C. Price, B. Weinstock-Guttman, D. Silva
American Journal of Neuroradiology Feb 2018, 39 (2) 289-295; DOI: 10.3174/ajnr.A5442
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