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Improved Turnaround Times | Median time to first decision: 12 days

Research ArticleBrain
Open Access

Quantitative 7T Phase Imaging in Premanifest Huntington Disease

A.C. Apple, K.L. Possin, G. Satris, E. Johnson, J.M. Lupo, A. Jakary, K. Wong, D.A.C. Kelley, G.A. Kang, S.J. Sha, J.H. Kramer, M.D. Geschwind, S.J. Nelson and C.P. Hess
American Journal of Neuroradiology April 2014, DOI: https://doi.org/10.3174/ajnr.A3932
A.C. Apple
From the Departments of Radiology and Biomedical Imaging (A.C.A., J.M.L., A.J., S.J.N., C.P.H.) and Neurology (K.L.P., G.S., E.J., K.W., G.A.K., S.J.S., J.H.K., M.D.G.), University of California, San Francisco; and GE Healthcare (D.A.C.K.), Global Applied Sciences Laboratory, Menlo Park, California.
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K.L. Possin
From the Departments of Radiology and Biomedical Imaging (A.C.A., J.M.L., A.J., S.J.N., C.P.H.) and Neurology (K.L.P., G.S., E.J., K.W., G.A.K., S.J.S., J.H.K., M.D.G.), University of California, San Francisco; and GE Healthcare (D.A.C.K.), Global Applied Sciences Laboratory, Menlo Park, California.
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G. Satris
From the Departments of Radiology and Biomedical Imaging (A.C.A., J.M.L., A.J., S.J.N., C.P.H.) and Neurology (K.L.P., G.S., E.J., K.W., G.A.K., S.J.S., J.H.K., M.D.G.), University of California, San Francisco; and GE Healthcare (D.A.C.K.), Global Applied Sciences Laboratory, Menlo Park, California.
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E. Johnson
From the Departments of Radiology and Biomedical Imaging (A.C.A., J.M.L., A.J., S.J.N., C.P.H.) and Neurology (K.L.P., G.S., E.J., K.W., G.A.K., S.J.S., J.H.K., M.D.G.), University of California, San Francisco; and GE Healthcare (D.A.C.K.), Global Applied Sciences Laboratory, Menlo Park, California.
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J.M. Lupo
From the Departments of Radiology and Biomedical Imaging (A.C.A., J.M.L., A.J., S.J.N., C.P.H.) and Neurology (K.L.P., G.S., E.J., K.W., G.A.K., S.J.S., J.H.K., M.D.G.), University of California, San Francisco; and GE Healthcare (D.A.C.K.), Global Applied Sciences Laboratory, Menlo Park, California.
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A. Jakary
From the Departments of Radiology and Biomedical Imaging (A.C.A., J.M.L., A.J., S.J.N., C.P.H.) and Neurology (K.L.P., G.S., E.J., K.W., G.A.K., S.J.S., J.H.K., M.D.G.), University of California, San Francisco; and GE Healthcare (D.A.C.K.), Global Applied Sciences Laboratory, Menlo Park, California.
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K. Wong
From the Departments of Radiology and Biomedical Imaging (A.C.A., J.M.L., A.J., S.J.N., C.P.H.) and Neurology (K.L.P., G.S., E.J., K.W., G.A.K., S.J.S., J.H.K., M.D.G.), University of California, San Francisco; and GE Healthcare (D.A.C.K.), Global Applied Sciences Laboratory, Menlo Park, California.
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D.A.C. Kelley
From the Departments of Radiology and Biomedical Imaging (A.C.A., J.M.L., A.J., S.J.N., C.P.H.) and Neurology (K.L.P., G.S., E.J., K.W., G.A.K., S.J.S., J.H.K., M.D.G.), University of California, San Francisco; and GE Healthcare (D.A.C.K.), Global Applied Sciences Laboratory, Menlo Park, California.
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G.A. Kang
From the Departments of Radiology and Biomedical Imaging (A.C.A., J.M.L., A.J., S.J.N., C.P.H.) and Neurology (K.L.P., G.S., E.J., K.W., G.A.K., S.J.S., J.H.K., M.D.G.), University of California, San Francisco; and GE Healthcare (D.A.C.K.), Global Applied Sciences Laboratory, Menlo Park, California.
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S.J. Sha
From the Departments of Radiology and Biomedical Imaging (A.C.A., J.M.L., A.J., S.J.N., C.P.H.) and Neurology (K.L.P., G.S., E.J., K.W., G.A.K., S.J.S., J.H.K., M.D.G.), University of California, San Francisco; and GE Healthcare (D.A.C.K.), Global Applied Sciences Laboratory, Menlo Park, California.
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J.H. Kramer
From the Departments of Radiology and Biomedical Imaging (A.C.A., J.M.L., A.J., S.J.N., C.P.H.) and Neurology (K.L.P., G.S., E.J., K.W., G.A.K., S.J.S., J.H.K., M.D.G.), University of California, San Francisco; and GE Healthcare (D.A.C.K.), Global Applied Sciences Laboratory, Menlo Park, California.
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M.D. Geschwind
From the Departments of Radiology and Biomedical Imaging (A.C.A., J.M.L., A.J., S.J.N., C.P.H.) and Neurology (K.L.P., G.S., E.J., K.W., G.A.K., S.J.S., J.H.K., M.D.G.), University of California, San Francisco; and GE Healthcare (D.A.C.K.), Global Applied Sciences Laboratory, Menlo Park, California.
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S.J. Nelson
From the Departments of Radiology and Biomedical Imaging (A.C.A., J.M.L., A.J., S.J.N., C.P.H.) and Neurology (K.L.P., G.S., E.J., K.W., G.A.K., S.J.S., J.H.K., M.D.G.), University of California, San Francisco; and GE Healthcare (D.A.C.K.), Global Applied Sciences Laboratory, Menlo Park, California.
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C.P. Hess
From the Departments of Radiology and Biomedical Imaging (A.C.A., J.M.L., A.J., S.J.N., C.P.H.) and Neurology (K.L.P., G.S., E.J., K.W., G.A.K., S.J.S., J.H.K., M.D.G.), University of California, San Francisco; and GE Healthcare (D.A.C.K.), Global Applied Sciences Laboratory, Menlo Park, California.
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Abstract

BACKGROUND AND PURPOSE: In vivo MR imaging and postmortem neuropathologic studies have demonstrated elevated iron concentration and atrophy within the striatum of patients with Huntington disease, implicating neuronal loss and iron accumulation in the pathogenesis of this neurodegenerative disorder. We used 7T MR imaging to determine whether quantitative phase, a measurement that reflects both iron content and tissue microstructure, is altered in subjects with premanifest Huntington disease.

MATERIALS AND METHODS: Local field shift, calculated from 7T MR phase images, was quantified in 13 subjects with premanifest Huntington disease and 13 age- and sex-matched controls. All participants underwent 3T and 7T MR imaging, including volumetric T1 and 7T gradient recalled-echo sequences. Local field shift maps were created from 7T phase data and registered to caudate ROIs automatically parcellated from the 3T T1 images. Huntington disease–specific disease burden and neurocognitive and motor evaluations were also performed and compared with local field shift.

RESULTS: Subjects with premanifest Huntington disease had smaller caudate volume and higher local field shift than controls. A significant correlation between these measurements was not detected, and prediction accuracy for disease state improved with inclusion of both variables. A positive correlation between local field shift and genetic disease burden was also found, and there was a trend toward significant correlations between local field shift and neurocognitive tests of working memory and executive function.

CONCLUSIONS: Subjects with premanifest Huntington disease exhibit differences in 7T MR imaging phase within the caudate nuclei that correlate with genetic disease burden and trend with neurocognitive assessments. Ultra-high-field MR imaging of quantitative phase may be a useful approach for monitoring neurodegeneration in premanifest Huntington disease.

Abbreviations

AUC
area under the curve
CAG
cytosine-adenine-guanine
CAPS
CAG-age-product scaled
eTIV
estimated total intracranial volume
HD
Huntington disease
LFS
local field shift
PLIC
posterior limb of the internal capsule
pmHD
premanifest Huntington disease
UHDRS
Unified Huntington's Disease Rating Scale
  • © 2014 American Society of Neuroradiology

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Cite this article
A.C. Apple, K.L. Possin, G. Satris, E. Johnson, J.M. Lupo, A. Jakary, K. Wong, D.A.C. Kelley, G.A. Kang, S.J. Sha, J.H. Kramer, M.D. Geschwind, S.J. Nelson, C.P. Hess
Quantitative 7T Phase Imaging in Premanifest Huntington Disease
American Journal of Neuroradiology Apr 2014, DOI: 10.3174/ajnr.A3932

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Quantitative 7T Phase Imaging in Premanifest Huntington Disease
A.C. Apple, K.L. Possin, G. Satris, E. Johnson, J.M. Lupo, A. Jakary, K. Wong, D.A.C. Kelley, G.A. Kang, S.J. Sha, J.H. Kramer, M.D. Geschwind, S.J. Nelson, C.P. Hess
American Journal of Neuroradiology Apr 2014, DOI: 10.3174/ajnr.A3932
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