Publication Type Academic Article
Authors Dyke J, Sondhi D, Voss H, Shungu D, Mao X, Yohay K, Worgall S, Hackett N, Hollmann C, Yeotsas M, Jeong A, Van de Graaf B, Cao I, Kaminsky S, Heier L, Rudser K, Souweidane M, Kaplitt M, Kosofsky B, Crystal R, Ballon D
Journal AJNR Am J Neuroradiol
Volume 34
Issue 4
Pagination 884-9
Date Published 10/04/2012
ISSN 1936-959X
Keywords Brain, Magnetic Resonance Imaging, Neuronal Ceroid-Lipofuscinoses, Severity of Illness Index
Abstract BACKGROUND AND PURPOSE: LINCL is a uniformly fatal lysosomal storage disease resulting from mutations in the CLN2 gene that encodes for tripeptidyl peptidase 1, a lysosomal enzyme necessary for the degradation of products of cellular metabolism. With the goal of developing quantitative noninvasive imaging biomarkers sensitive to disease progression, we evaluated a 5-component MR imaging metric and tested its correlation with a clinically derived disease-severity score. MATERIALS AND METHODS: MR imaging parameters were measured across the brain, including quantitative measures of the ADC, FA, nuclear spin-spin relaxation times (T2), volume percentage of CSF (%CSF), and NAA/Cr ratios. Thirty MR imaging datasets were prospectively acquired from 23 subjects with LINCL (2.5-8.4 years of age; 8 male/15 female). Whole-brain histograms were created, and the mode and mean values of the histograms were used to characterize disease severity. RESULTS: Correlation of single MR imaging parameters against the clinical disease-severity scale yielded linear regressions with R2 ranging from 0.25 to 0.70. Combinations of the 5 biomarkers were evaluated by using PCA. The best combination included ADC, %CSF, and NAA/Cr (R2=0.76, P<.001). CONCLUSIONS: The multiparametric disease-severity score obtained from the combination of ADC, %CSF, and NAA/Cr whole-brain MR imaging techniques provided a robust measure of disease severity, which may be useful in clinical therapeutic trials of LINCL in which an objective assessment of therapeutic response is desired.
DOI 10.3174/ajnr.A3297
PubMed ID 23042927
PubMed Central ID PMC3644851
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