Prognostic impact of postoperative, pre-irradiation 18F-fluoroethyl- l-tyrosine uptake in glioblastoma patients treated with radiochemotherapy

• Published in: Radiotherapy and oncology Vol. 99; no. 2; pp. 218 - 224
• Main Authors: Piroth, Marc D., Holy, Richard, Pinkawa, Michael, Stoffels, Gabriele, Kaiser, Hans J., Galldiks, Norbert, Herzog, Hans, Coenen, Heinz H., Eble, Michael J., Langen, Karl J.
• Format: Journal Article
• Language: English
• Published: Elsevier Ireland Ltd 2011
• Subjects: [ 18F]Fluoroethyl- l-tyrosine; Amino acid PET; FET; Glioblastoma; Hematology, Oncology, and Palliative Medicine; Prognosis; Radiotherapy; [ 18F]Fluoroethyl- l-tyrosine; Prognosis; Amino acid PET; FET; Radiotherapy; Glioblastoma
• ISSN: 0167-8140; 1879-0887
• DOI: 10.1016/j.radonc.2011.03.006

Resection is considered as essential for the efficacy of modern adjuvant treatment of glioblastoma multiforme (GBM). Previous studies have indicated that amino acid PET is more specific than contrast enhancement on MRI for detecting residual tumor tissue after surgery. In a prospective study we investigated the prognostic impact of postoperative tumor volume and tumor/brain ratios (TBR) in PET using O-(2-[ 18F]fluoroethyl)- l-tyrosine (FET) in comparison with MRI. Forty-four patients with GBM were investigated by FET PET and MRI after surgery. Tumor volume in FET PET with a tumor/brain ratio (TBR) > 1.6 and a TBR > 2, mean and maximum TBR and gadolinium contrast-enhancement on MRI (Gd-volume) were determined. Thereafter patients received a fractionated radiotherapy with concomitant temozolomide (RCX). The median follow-up was 15.4 (3–35) months. The prognostic value of postoperative residual tumor volume in FET PET, TBR mean, TBR max and Gd-volume was evaluated using Kaplan–Maier estimates for disease-free survival (DFS) and overall survival (OS). Postoperative tumor volume in FET PET had a significant independent influence on OS and DFS (OS 20.0 vs. 6.9 months; DFS 9.6 vs. 5.1 months, p < 0.001; cut-off 25 ml). Similar results were observed when a TBR ⩾ 2 (cut-off 10 ml) was used to define the tumor volume in 18F-FET PET. The TBR mean and TBR max of FET uptake had a significant influence on DFS ( p < 0.05). Gd-volume in MRI had significant effect on OS and DFS in the univariate analysis. No independent significant influence in OS or DFS could be observed for Gd-volume in MRI. Our data indicate that the tumor volume in FET PET after surgery of GBM has a strong prognostic impact for these patients. FET PET appears to be helpful to determine the residual tumor volume after surgery of GBM and may serve as a valuable tool for optimal planning of radiation treatment.