Investigation of Cerebral O-(2-[$^{18}$F]Fluoroethyl)-L-Tyrosine Uptake in Rat Epilepsy Models

Stegmayr, Carina; Filß, Christian; Shah, N. Jon; Langen, Karl-Josef; Surges, Rainer; Burda, Nicole; Neumaier, Bernd; Choi, Chang-Hoon; Willuweit, Antje; Stoffels, Gabriele; Mottaghy, Felix M.; Heinzel, Alexander

doi:10.1007/s11307-020-01503-x

%0 Journal Article
%A Stegmayr, Carina
%A Surges, Rainer
%A Choi, Chang-Hoon
%A Burda, Nicole
%A Stoffels, Gabriele
%A Filß, Christian
%A Willuweit, Antje
%A Neumaier, Bernd
%A Heinzel, Alexander
%A Shah, N. Jon
%A Mottaghy, Felix M.
%A Langen, Karl-Josef
%T Investigation of Cerebral O-(2-[$^{18}$F]Fluoroethyl)-L-Tyrosine Uptake in Rat Epilepsy Models
%J Molecular imaging & biology
%V 22
%@ 1860-2002
%C New York [u.a.]
%I Springer
%M FZJ-2020-02050
%P 1255–1265
%D 2020
%X A recent study reported on high, longer lasting and finally reversible cerebral uptake of O-(2-[18F]fluoroethyl)-L-tyrosine ([18F]FET) induced by epileptic activity. Therefore, we examined cerebral [18F]FET uptake in two chemically induced rat epilepsy models and in patients with focal epilepsy to further investigate whether this phenomenon represents a major pitfall in brain tumor diagnostics and whether [18F]FET may be a potential marker to localize epileptic foci.Five rats underwent kainic acid titration to exhibit 3 to 3.5 h of class IV–V motor seizures (status epilepticus, SE). Rats underwent 4× [18F]FET PET and 4× MRI on the following 25 days. Six rats underwent kindling with pentylenetetrazol (PTZ) 3 to 8×/week over 10 weeks, and hence, seizures increased from class I to class IV. [18F]FET PET and MRI were performed regularly on days with and without seizures. Four rats served as healthy controls. Additionally, five patients with focal epilepsy underwent [18F]FET PET within 12 days after the last documented seizure.No abnormalities in [18F]FET PET or MRI were detected in the kindling model. The SE model showed significantly decreased [18F]FET uptake 3 days after SE in all examined brain regions, and especially in the amygdala region, which normalized within 2 weeks. Corresponding signal alterations in T2-weighted MRI were noted in the amygdala and hippocampus, which recovered 24 days post-SE. No abnormality of cerebral [18F]FET uptake was noted in the epilepsy patients.There was no evidence for increased cerebral [18F]FET uptake after epileptic seizures neither in the rat models nor in patients. The SE model even showed decreased [18F]FET uptake throughout the brain. We conclude that epileptic seizures per se do not cause a longer lasting increased [18F]FET accumulation and are unlikely to be a major cause of pitfall for brain tumor diagnostics.
%F PUB:(DE-HGF)16
%9 Journal Article
%$ pmid:32409931
%U <Go to ISI:>//WOS:000532879300001
%R 10.1007/s11307-020-01503-x
%U https://juser.fz-juelich.de/record/875458

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