PT - JOURNAL ARTICLE AU - Martin Bendszus AU - Monika Warmuth-Metz AU - Rüdiger Klein AU - Ralf Burger AU - Christian Schichor AU - Jörg C. Tonn AU - Laszlo Solymosi TI - MR Spectroscopy in Gliomatosis Cerebri DP - 2000 Feb 01 TA - American Journal of Neuroradiology PG - 375--380 VI - 21 IP - 2 4099 - http://www.ajnr.org/content/21/2/375.short 4100 - http://www.ajnr.org/content/21/2/375.full SO - Am. J. Neuroradiol.2000 Feb 01; 21 AB - BACKGROUND AND PURPOSE: The diagnosis of gliomatosis cerebri with MR imaging is known to be difficult. We report on the value of MR spectroscopy in the diagnosis, grading, and biopsy planing in eight patients with histopathologically proved gliomatosis cerebri.METHODS: Patients underwent MR imaging and MR spectroscopy (single-voxel point-resolved spectroscopy [PRESS] at 1500/135, and chemical-shift imaging [CSI] PRESS at 1500/135) before open (n = 4) or stereotactic (n = 4) biopsy. In six patients who underwent CSI, biopsy samples were taken from regions of maximally elevated levels of choline/N-acetylaspartate (Cho/NAA).RESULTS: All patients showed elevated Cho/creatine (Cr) and Cho/NAA levels as well as varying degrees of decreased NAA/Cr ratios, which were most pronounced in the anaplastic lesions. In low-grade lesions, there was a maximum Cho/NAA ratio of 1.3, whereas in anaplastic tumors, the maximum Cho/NAA level was at least 2.5. Spectra in two patients with grade III lesions revealed a lactate peak; lactate and lipid signals were seen in two patients with grade IV lesions. Biopsy specimens from regions with maximally elevated levels of Cho/NAA showed dense infiltration of tumor cells.CONCLUSION: MR spectroscopy might be used to classify gliomatosis cerebri as a stable or a progressive disease indicating its potential therapeutic relevance.