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@ARTICLE{Langen:155422,
author = {Langen, K. J. and Tonn, J. C. and Weller, M. and Galldiks,
N.},
title = {{L}etter to the {E}ditor: “{T}he role of imaging in the
management of progressive glioblastoma. {A} systematic
review and evidence-based clinical practice guideline”
[{J} {N}eurooncol 2014; 118:435–460]},
journal = {Journal of neuro-oncology},
volume = {120},
number = {3},
issn = {0167-594x},
address = {Dordrecht [u.a.]},
publisher = {Springer Science + Business Media B.V},
reportid = {FZJ-2014-04588},
pages = {665-666},
year = {2014},
abstract = {o the Editor,We have read with interest the review by Ryken
et al. about the role of imaging in the management of
progressive glioblastoma [1]. In general, we agree with this
review but we cannot support the opinion that the routine
use of Positron-Emission-Tomography (PET) to identify
progression of glioblastoma is not recommendable.The authors
have considered PET using the amino acid tracer
11C-methyl-l-methionine (MET), but the use of MET is limited
to PET centers with an on-site cyclotron due the short
half-life of 11C (20.4 min). In recent years, the clinical
application of 18F-labeled amino acids such as
O-(2-18F-fluoroethyl)-l-tyrosine (FET) or
3,4-dihydroxy-6-[18F]fluoro-l-phenylalanine (FDOPA) has
spread considerably due to the logistical advantages of the
18F label (half-life, 109.8 min) [2]. FET can be produced
with high yields similar to the widely used FDG and
distributed in a satellite concept [3]. In Europe, MET PET
has been replaced in many centers by the more convenie ...},
cin = {INM-3 / INM-4},
ddc = {610},
cid = {I:(DE-Juel1)INM-3-20090406 / I:(DE-Juel1)INM-4-20090406},
pnm = {333 - Pathophysiological Mechanisms of Neurological and
Psychiatric Diseases (POF2-333) / 89572 - (Dys-)function and
Plasticity (POF2-89572)},
pid = {G:(DE-HGF)POF2-333 / G:(DE-HGF)POF2-89572},
typ = {PUB:(DE-HGF)16},
UT = {WOS:000345286700028},
doi = {10.1007/s11060-014-1594-z},
url = {https://juser.fz-juelich.de/record/155422},
}