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Prediction of oligodendroglial histology and LOH 1p/19q using dynamic [18F]FET-PET imaging in intracranial WHO grade II and III gliomas
Authors:Nathalie L. Jansen  Christoph Schwartz  Vera Graute  Sabina Eigenbrod  Jürgen Lutz  Rupert Egensperger  Gabriele P?pperl  Hans A. Kretzschmar  Paul Cumming  Peter Bartenstein  J?rg-Christian Tonn  Friedrich-Wilhelm Kreth  Christian la Fougère  Niklas Thon
Affiliation:Department of Nuclear Medicine (N.L.J., V.G., P.C., P.B., C.l.F.); Department of Neurosurgery (C.S., J.-C.T., F.-W.K., N.T.); Center for Neuropathology and Prion Research (S.E., R.E., H.A.K.); Department of Neuroradiology, Hospital of the Ludwig-Maximilians-University, Munich (J.L.); and Department of Nuclear Medicine, Katharinenhospital, Stuttgart, Germany (G.P.)
Abstract:Oligodendroglial components (OC) and loss of heterozygosity on chromosomes 1p and 19q (LOH 1p/19q) are associated with better outcome in patients with glioma. We aimed to assess the fitness of [18F]fluoroethyltyrosine positron-emission-tomography (FET-PET) for noninvasively identifying these important prognostic/predictive factors. One hundred forty-four patients with MRI-suspected WHO grade II and III glioma underwent FET-PET scans prior to histological diagnosis. FET-PET analyses included maximal tumoral uptake (SUVmax/BG), biological tumor volume (BTV), mean tumoral uptake (SUVmean/BG), total tumoral uptake (SUVtotal/BG), and kinetic analysis. Suspicion of OC was based on static and dynamic FET-uptake parameters. PET results were correlated with histology and 1p/19q status. OC tumors exhibited significantly higher uptake values, compared with astrocytomas (AC) (SUVmax/BG 3.1 vs 2.3, BTV 15.5 mL vs 7.2 mL, SUVtotal/BG 38.5 vs 17.4, P < .01 each; SUVmean/BG 2.2 vs 2.1, P < .05). These differences were more pronounced in WHO grade II gliomas. Comparable results were found with respect to 1p/19q status. Kinetic analysis misclassified 18 of 34 low-grade OC tumors as high-grade glioma but misclassified only 5 of 45 of the low-grade ACs. FET-based suspicion of OC resulted in concordance rates of both 76% for the prediction of OC and LOH 1p/19q. FET-uptake was significantly higher in gliomas with OC, compared with AC, and likewise in 1p/19q codeleted, compared with noncodeleted tumors. However, FET-PET analysis did not reliably predict the presence of OC/LOH 1p/19q in the individual patient, mostly because of an overlap in PET characteristics of OC tumors and high-grade AC. Histological examination is still required for an accurate diagnosis.
Keywords:FET-PET   FET uptake   glioma   kinetic analysis   LOH1p/19q   oligodendroglial tumor components
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