Proton chemical shift imaging, metabolic maps, and single voxel spectroscopy of glial brain tumors

被引:38
作者
Mader, I
Roser, W
Hagberg, G
Schneider, M
Sauter, R
Seelig, J
Radue, EW
Steinbrich, W
机构
[1] UNIV BASEL HOSP, KANTONSSPITAL, DEPT MED RADIOL, CH-4031 BASEL, SWITZERLAND
[2] UNIV BASEL, MR CTR, BASEL, SWITZERLAND
[3] UNIV BASEL, BIOCTR, CH-4056 BASEL, SWITZERLAND
[4] SIEMENS AG, MED ENGN GRP, D-8520 ERLANGEN, GERMANY
关键词
proton; magnetic resonance spectroscopy; chemical shift imaging; glial tumor; myoinositol; glycine;
D O I
10.1007/BF01772521
中图分类号
R8 [特种医学]; R445 [影像诊断学];
学科分类号
1002 ; 100207 ; 1009 ;
摘要
Seventeen patients with presumed glial brain tumors were examined with proton chemical shift imaging and single voxel spectroscopy that used different echo times. Metabolite resonances were evaluated by metabolic ratios and absolutely by correcting for coil load and comparison to phantom measurements. Metabolic images were created to visualize the metabolic changes. All patients showed spectra that were different from those measured in healthy control subjects. Spectral changes were also present in normal-appearing matter (NAM) that was distant from lesions. The resonance at 3.55 ppm which is usually assigned to both myo-inositol and glycine, was the only one to allow a discrimination between healthy volunteers, astrocytoma grade III and glioblastoma multiforme (GEM) (p < 0.02). From the different echo times used we conclude that an increase in this resonance has to be assigned to glycine rather than Inyo-inositol. This resonance might be used to grade human gliomas more reliably. Total creatine (Cr) decreased more drastically with malignancy than N-acetylated metabolites (NA). This led to a higher NA/Cr ratio in GEM compared to astrocytoma grade II. NA/Cr was thus pseudonormal in GEM due to a change in both nominator and denominator. This study reveals the importance of comparing magnetic resonance spectroscopy data of lesions to spectra measured in identical localizations in healthy control subjects instead of NAM and the importance of quantifying single metabolic peaks instead of creating metabolic ratios in clinical magnetic resonance spectroscopy.
引用
收藏
页码:139 / 150
页数:12
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