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February 23, 2010; 74 (8) Articles

Brain-water diffusion coefficients reflect the severity of inherited prion disease

H. Hyare, S. Wroe, D. Siddique, T. Webb, N. C. Fox, J. Stevens, J. Collinge, T. Yousry, J. S. Thornton
First published February 22, 2010, DOI: https://doi.org/10.1212/WNL.0b013e3181d0cc47
H. Hyare
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S. Wroe
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D. Siddique
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T. Webb
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N. C. Fox
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J. Stevens
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Citation
Brain-water diffusion coefficients reflect the severity of inherited prion disease
H. Hyare, S. Wroe, D. Siddique, T. Webb, N. C. Fox, J. Stevens, J. Collinge, T. Yousry, J. S. Thornton
Neurology Feb 2010, 74 (8) 658-665; DOI: 10.1212/WNL.0b013e3181d0cc47

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Abstract

Objective: Inherited prion diseases are progressive neurodegenerative conditions, characterized by cerebral spongiosis, gliosis, and neuronal loss, caused by mutations within the prion protein (PRNP) gene. We wished to assess the potential of diffusion-weighted MRI as a biomarker of disease severity in inherited prion diseases.

Methods: Twenty-five subjects (mean age 45.2 years) with a known PRNP mutation including 19 symptomatic patients, 6 gene-positive asymptomatic subjects, and 7 controls (mean age 54.1 years) underwent conventional and diffusion-weighted MRI. An index of normalized brain volume (NBV) and region of interest (ROI) mean apparent diffusion coefficient (ADC) for the head of caudate, putamen, and pulvinar nuclei were recorded. ADC histograms were computed for whole brain (WB) and gray matter (GM) tissue fractions. Clinical assessment utilized standardized clinical scores. Mann-Whitney U test and regression analyses were performed.

Results: Symptomatic patients exhibited an increased WB mean ADC (p = 0.006) and GM mean ADC (p = 0.024) compared to controls. Decreased NBV and increased mean ADC measures significantly correlated with clinical measures of disease severity. Using a stepwise multivariate regression procedure, GM mean ADC was an independent predictor of Clinician's Dementia Rating score (p = 0.001), Barthel Index of activities of daily living (p = 0.001), and Rankin disability score (p = 0.019).

Conclusions: Brain volume loss in inherited prion diseases is accompanied by increased cerebral apparent diffusion coefficient (ADC), correlating with increased disease severity. The association between gray matter ADC and clinical neurologic status suggests this measure may prove a useful biomarker of disease activity in inherited prion diseases.

Glossary

ADAS-Cog=
Alzheimer's Disease Assessment Scale–Cognitive subscale;
ADC=
apparent diffusion coefficient;
ADL=
Barthel Activities of Daily Living scale;
BET=
brain extraction tool;
BPRS=
Brief Psychiatric Rating Scale;
BSE=
bovine spongiform encephalopathy;
CDR=
Clinician's Dementia Rating Scale;
CGIS=
Clinician's Global Impression of Disease;
CI=
confidence interval;
DWI=
diffusion-weighted imaging;
FLAIR=
fluid-attenuated inversion recovery;
FOV=
field of view;
GM=
gray matter;
LC=
left head of caudate;
LP=
left putamen;
LPu=
left pulvinar;
MMSE=
Mini-Mental State Examination;
NBV=
normalized brain volume;
PH=
peak height;
PL=
peak location;
RC=
right head of caudate;
RP=
right putamen;
RPu=
right pulvinar;
ROI=
region of interest;
sCJD=
sporadic Creutzfeldt-Jakob disease;
TE=
echo time;
TI=
inversion time;
TR=
repetition time;
vCJD=
variant Creutzfeldt-Jakob disease;
WB=
whole brain;
WM=
white matter.
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